2016 BSMC syllabus - Friday - Therapeutics Education Collaboration
Transcription
2016 BSMC syllabus - Friday - Therapeutics Education Collaboration
27th Annual Best Science Medicine Course Formerly the Drug Therapy Decision Making Course – 25 years May 6th and 7th, 2016 Fairmont Waterfront Hotel Vancouver, B.C. FRIDAY Syllabus Presented by The Therapeutics Education Collaboration, The St. Paul’s Hospital Department of Family and Community Medicine In Cooperation with the Department of Family Medicine, University of British Columbia COURSE DIRECTORS Drs. James McCormack and Robert Rangno COMMITTEE MEMBERS Drs. Rita McCracken and Tracey Monk "It is an art of no little importance to administer medicines properly; but it is an art of much greater and more difficult acquisition to know when to suspend or altogether omit them." Philippe Pinel 1745‐1826 The New Therapeutic Commandments Thou shalt 1. Have no aim except to help patients according to their goals 2. Always seek knowledge of the benefits, harms, and costs of treatment 3. If all else fails consider watchful waiting 4. Honour balanced sources of knowledge 5. Treat according to level of risk and not to level of risk factor 6. Not bow down to treatment targets 7. Honour thy elderly patient 8. Not pile one treatment upon another 9. Diligently try to find the best treatment for the individual 10. Start with the lowest dose possible Written by R Lehman, J McCormack, T Perry, A Tejani, J Yudkin Best Science Medicine Course 2016 FACULTY Course Committee Co-Chairs: Bob Rangno, Emeritus Prof., Medicine, Pharmacology, UBC & PHC James McCormack, Prof., Pharmaceutical Sciences, UBC G. Michael Allan, Prof., Family Medicine, University of Alberta & Director, Evidence and CPD Program, Alberta College of Family Physicians Committee: Rita McCracken, Clin. Assist. Prof., Medicine and Associate Head, Family Medicine, PHC Tracy Monk, Clin. Assist. Prof., Medicine, UBC Guest Faculty Alan Cassels, Adj Prof., Human and Social Development, University of Victoria Mike Kolber, Assoc. Prof., Family Medicine, University of Alberta Tina Korownyk, Assoc. Prof., Family Medicine, University of Alberta Dee Mangin, Assoc. Prof., Family Medicine, McMaster University, Hamilton, Ontario Local Faculty Ric Arseneau, Clin. Assoc. Prof., Medicine, UBC, PHC & BCWH Jason Crookham, Clin. Instructor, Medicine, UBC Kit Fairgrieve, St. Paul’s Hospital Goldcorp Addiction Medicine Fellow, PHC Peter Loewen, Asst. Prof., Pharm. Sciences, UBC & VGH Natasha Press, Clin. Assoc. Prof., Medicine, Infectious Diseases, UBC & PHC Kam Shojania, Clin. Prof., Medicine, Head, Rheumatology, UBC & PHC Aaron M Tejani, Clin. Asst. Prof., Pharmaceutical Sciences, UBC BCWH – BC Women’s Hospital PHC – Providence Health Care UBC – University of British Columbia VGH – Vancouver General Hospital BSMC BEST SCIENCE MEDICINE COURSE 27th Annual Best Science Medicine Course Formerly The Drug Therapy Decision Making Course – 25 years Friday, May 6, 2016 07:00 Registration (Muffins & Coffee) Chairs – Bob Rangno and James McCormack “I’ve Got The Music In Me” 08:00 Welcome 08:10 “Everybody’s Talking At Me” 08:30 “The Bare Necessities” of evidence-based practice and how to “Rule The World” Bob Rangno Bob Rangno and James McCormack Mike Allan and James McCormack “Start Me Up” 08:50 09:10 09:20 09:40 10:10 10:20 Do we need to prevent “Bad Blood” with prophylactic antibiotics? Questions Stopping SSRIs – “I Can’t Fight This Feeling” Stories from the Cochrane Collaboration – “Everyday I Write the Book” Questions Refreshment Break “Hurts So Good” 10:40 CentralSensitivitySyndromes(CSS)–“DoYouFeelLikeIDo?" 11:00 Osteoarthritiscanbe“BadTo The Bone” 11:20 Questions 11:30 Concussionsandwhattodowhenyou“Bang yourHead” 11:50 Questions 12:00 Lice Treatment - "I've Got You Under My Skin" 12:10 Lunch Natasha Press Dee Mangin Alan Cassels Ric Arseneau Mike Allan Jason Crookham Mike Kolber “Bad Case Of Loving You” 13:00 Male and female sexual dysfunction – can we create “Paradise By The Dashboard Light?” Tina Korownyk 13:20 Moisturizers and anti-aging creams, can they change the fact that we are “Born This Way” James McCormack 13:40 There is no “Black Or White” when it comes to drug interactions Dee Mangin 14:00 Questions 14:20 Refreshment Break “Helter Skelter” 14:40 15:00 15:20 15:40 16:00 COPD treatments – “All I Need Is The Air That I Breathe” Antidotes for anticoagulants – are they a case of “Take The Money And Run”? Polymyalgia rheumatica – relieving “The King Of Pain” Questions Adjourn Mike Allan Peter Loewen Kam Shojania Bob Rangno, James McCormack and Mike Allan “Whoa-oh-whoa, Listen To The Music” The Doobie Brothers Welcome!! “I Got The Music In Me” Kiki Dee band Robert Rangno, MSc, MD Professor Emeritus Medicine and Pharmacology, UBC, Vancouver, BC James McCormack, BSc (Pharm), PharmD Professor Faculty of Pharmaceutical Sciences, UBC, Vancouver, BC Please let the world, or at least your world, know about the course and what you’ve learned #bsmc2016 @medmyths G. Michael Allan, MD, CCFP Professor University of Alberta, Edmonton, Alberta You can find a pdf of the handouts at http://therapeuticseducation.org/dtc therapeuticseducation.org medicationmythbusters.com “I Can See Clearly Now” Johnny Nash DisclosureofCommercial Support LearningOutcomeObjec8veSlide Tobeabletolookatpublishedstudyresultsandteaseoutthe rela8vebenefit,theabsolutebenefitedtheNNT/NNH Thisprogramhasreceived NOfinancialsupportfromANYBODY JM - Entire salary comes through the UBC Faculty of Pharmaceutical Sciences - also some legal/ educational work BR - retired from UBC MA – U of A & Alberta Health - (Alberta College of Family Physicians, etc) We have received no honorarium or research money from the drug industry in the last 25 or so years iOS apps (iPad/iPhone) KidneyCalc and MyStudies - mystudies.org Premium podcast subscription Best Science (BS) Medicine podcast - therapeuticseducation.org l l a re a E e G W D E L W O s r N e K brok 14 Bob Rangno, James McCormack and Mike Allan Have no aim except to help patients according to their goals 2. Always seek knowledge of the benefits, harms, and costs of treatment 3. If all else fails consider watchful waiting 4. Honour balanced sources of knowledge 5. Treat according to level of risk and not to level of risk factor 6. Not bow down to treatment targets 7. Honour thy elderly patient 8. Not pile one treatment upon another 9. Diligently try to find the best treatment for the individual 10. Start with the lowest dose possible 1. A lot of bullshit Relevant and useful information I JUST KNOW Systematic review/ meta-analysis RCT Which is either A)purposeful B)based in ignorance Cohort Case Control Case Report “Expert” Opinion BEST AVAILABLE EVIDENCE PYRAMID Need different evidence for different questions The Bullshit Asymmetry Recovered Data 2013 The amount of energy needed to refute bullshit is an order of magnitude bigger than to produce it. 2016 CHD mortality Randomized controlled trials of replacing saturated fat with vegetable oil rich in linoleic acid (corn oil) RECOVERED DATA Blinded RCT 9,423 (M/F) - 4 years 458 (M) - 3 years 36 hard (non-surrogate) outcomes were reported 1 outcome showed a statistically significant difference in combined cardiovascular events 0.86 (0.77-0.96) CHD mortality “the totality of evidence no longer provides support for the traditional diet-heart hypothesis” If true - 1% absolute reduction in risk CD002137 James McCormack and G. Michael Allan The “Bare Necessities” The “Numbers” Surrogate markers/ thresholds The Numbers Low doses Shared decision making/ values and preferences Sources of information Polypharmacy/ Polytesting Relative Risk and Absolute Benefit Intensive therapy Standard therapy Relative risk Relative risk 95% CI nonfatal myocardial infarction or nonfatal stroke or death from cardiovascular causes 6.9 7.2 0.95 0.80-1.05 Death (%) 5 4 1.25 1.01-1.50 Non-fatal MI (%) 3.6 4.6 0.8 0.6-0.9 Non-fatal stroke (%) 1.3 1.2 1.1 0.75-1.50 CHF (%) 3 2.4 1.2 0.95-1.50 Primary outcome (%) 5 is 25% greater than 4 RR - 1.25 The CI represents a plausible range of values for the effect but not a probability of its magnitude 25% relative increase 1.25 minus1.00 = 0.25 1% relative increase 1.01minus1.00 = 0.01 50% relative increase 1.50 minus1.00 = 0.50 5%-4% = 1% 1% = 1/100 NNH = 100 Baseline Risk of a heart attack = 50% over 5 years RR - Relative benefit = 0.8 or 20% reduction With Treatment = 40% Absolute difference = 10% NNT = 10 Baseline Risk of a stroke = 2% per year RR - Relative benefit = 0.25 or 75% reduction With Treatment = 0.5% Absolute difference = 1.5% NNT = 67 Baseline risk of cancer = 10% lifetime RR - Relative harm = 2.5 or 150% increase With Treatment = 25% Absolute difference = 15% NNH = 7 20 “NEGATIVE” STUDIES IN A ROW LIPIDS Surrogate markers/ thresholds AIM-HIGH, HPS2-THRIVE (niacin) BLOOD PRESSURE ALTITUDE (aliskiren) ACCORD (fibrates) VALISH, AASK, ACCORD dalOUTCOMES (dalcetrapib) ME Hg) O C (aggressive BP lowering) m T STABILITY (darapladib) OU 140m G s E v R Hg YES nefit PADIABETES EM 20mm tatins o GENERAL be s en T (1VADT (irbesartan/afib) 3 - suACTIVE r N ACCORD, ADVANCE, I E SPR HOP d pres CRESCENDO (rimonabant) (aggressive A1c lowering) bloo VISTA-16 (varespladib) BUT ROADMAP (olmesartan) ORIGIN (insulin) SAVOR-TIMI 53 (saxagliptin) 182,000+ EXAMINE (alogliptin) patients ALECARDIO (aleglitazar) !! FIN Y!!! L L A James McCormack and G. Michael Allan European Association for the Study of Diabetes conference in Stockholm, Sweden Sept 2015 “The packed conference hall listened intently as the investigators announced the results of the primary outcome (a composite of cardiovascular mortality, non-fatal myocardial infarction, and non-fatal stroke), showing superiority of the drug over placebo, and burst into impromptu applause when strong effects were shown” www.thelancet.com/diabetes-endocrinology November 2015 EMPA-REG OUTCOME 3.1yr - 63 y/o, 71% male, 100% prev CVD, A1c 8.1% All deaths CVD (%) death (%) Death from cardiovascular causes, nonfatal myocardial infarction, or nonfatal stroke (%) Genital infections (%) Empagliflozin 5.7 3.7 10.5 6.4 Placebo 8.3 5.9 12.1 1.8 RR ARR NNT/NNH 31 2.6 39 38 2.2 45 14 1.6 61 260 4.6 22 NEJM 2015;DOI: 10.1056/NEJMoa1504720 SPRINT HOPE-3 CHOLESTEROL 3.3yr - 68 y/o, 64% male, 17% prev CVD, 140/78 mmHg, statin 44% All deaths (%) Myocardial infarction, acute coronary syndrome, stroke, heart failure, or death from cardiovascular causes (%) Acute kidney injury or acute renal failure(%) Serious syncope (%) Intensive (120mmHg) Regular (140 mmHg) 3.3 5.2 4.4 2.3 4.5 6.8 2.6 1.7 RR 35 24 41 25 ARR NNT /NNH 1.2 85 1.6 62 1.8 56 0.6 173 5.6yr - 66 y/o, 54% male, 0% prev CVD, 138/82mmHg, Total chol 5.2/200 All deaths (%) Total MI (%) Death from cardiovascular causes, nonfatal myocardial infarction, nonfatal stroke, resuscitated cardiac arrest, heart failure, or revascularization (%) Muscle symptoms (%) Rosuvastatin Placebo 5.3 5.6 0.7 1.1 4.4 5.7 5.8 4.7 RR ARR NNT/NNH No statistical diff 35 0.4 263 24 1.4 73 24 1.1 91 NEJM 2016 NEJM 2015 HOPE-3 BP Pre-Med/Pre-Pharmacy 5.6yr - 66 y/o, 54% male, 0% prev CVD, 138/82mmHg, Total chol 5.2/200 All deaths (%) Total stroke (%) Cardiovascular death, nonfatal myocardial infarction, nonfatal stroke, resuscitated cardiac arrest, heart failure, revascularization, or angina with objective evidence of ischemia (%) Symptomatic hypotension, dizziness, lightheadedness (%) Candesartan/ HCTZ 5.4 1.2 5.3 3.4 Placebo 5.5 1.5 5.7 2.0 RR ARR NNT/NNH No statistical differences 67 1.4 73 NEJM 2016 = PRESUMPTUOUS Definition - too confident especially in a way that is rude : done or made without permission, right, or good reason James McCormack and G. Michael Allan DPP-4 inhibitors lower A1c by 0.3-0.8% but they do not modify CVD or mortality Adverse events were generally uncommon, but a risk of pancreatitis remains possible, and saxagliptin increased hypoglycemia (~1 in 50) and heart failure (~1 in 150) Normal (20-25) to overweight (25-30) BMI carries the lowest risk of mortality ~25 appearing lowest (in elderly ~27.5) Mortality increases when BMI is below “lownormal” (BMI <20) and obese (BMI ≥30), more at the extremes When to Measure/Re-measure Bone density Cholesterol If pt would consider If pt would consider treatment treatment one time one time measurement Before measurement translate cholesterol into treatment translate T-score into 1010-year CVD risk year fracture risk “fire and forget” approach After treatment Don’t bother as the test Don’t bother because all you just isn’t precise enough can do is raise the statin dose - that decision should be based on magnitude of CVD reduction not cholesterol Blood pressure Easy to measure BUT many, many repeat measurements unless VERY high Low doses “fire and forget” approach???? A sample of RCT Evidence 6.25 mg hydrochlorothiazide first marketed at 50 to 200 mg daily 6.25 mg captopril 25 mg PO TID is still a commonly recommended initial starting dose for hypertension 25 mg sildenafil (Viagra) effective dose for erectile dysfunction 25 mg sumatriptan (Imitrex) works as well as100 mg 5 mg daily fluoxetine (Prozac) similar effects to those seen at 20 mg and 40 mg daily 0.25 mg ezetimibe (Ezetrol) 1/40th of the recommended initial starting dose provides 50% of the LDL lowering effect 15 mg elemental iron daily as effective for anemia in the elderly as 50 mg and 150 mg with a lower incidence of side effects 150 mg daily bupropion (Zyban) 0.5 mg BID varenicline (Champix) produces the same rate of smoking cessation at one year as 300 mg daily (1.0 mg BID) 10 mg atorvastatin produces 2/3 of the effect on cholesterol as that seen with an 80 mg (8-fold increase) dose 200 mg ibuprofen (Motrin) as effective as 400 mg for migraine headache 25 mg ranitidine (Zantac) as effective as 125 mg for heartburn relief 1.8 mg colchicine as effective as 4.8mg for acute gout with less adverse events low-dose (~20mg/day) isotretinoin improves acne similar to conventional dosing low-dose may reduce common side effects (chapped lips, dry skin, epistaxis) by 16-35% may be associated with increased relapse rates (~20%) particularly with severe acne James McCormack and G. Michael Allan % reduction in LDL cholesterol 60 45 Shared decision making/ values and preferences 30 10mg 20mg 40mg 80mg 15 0 Rosuvastatin Atorvastatin Simvastatin Pravastatin It’s all about figuring out The Chance WITH NO TREATMENT Recommended approaches • • • VS • The Chance WITH TREATMENT • • GENERAL SUGGESTIONS - these are “relative” use percentages or natural frequencies(numerator/denominator) use absolute terms add bar graphs or icon arrays use incremental risk format with icon arrays in the same array avoid use of NNTs if use relative risks add baseline risks Ann Intern Med 2014;161:270-80 Conditions requiring risk assessment The main ones are hypertension, cholesterol, glucose/diabetes, osteoporosis/BMD, atrial fibrillation, cancer Can Fam Physician 2007;53:1326-27 5 Canadian Guidelines for blood pressure, cholesterol, glucose, and bone density Figure out risk Then figure out benefit Include harm and costs and inconvenience 197 PAGES - 90,000 Words 99 (0.1%) words - relevant to patients’ values and preferences James McCormack and G. Michael Allan Risk of future illness CVD risk/benefit (most people don’t benefit despite a lifetime of treatment) Assume a person’s lifetime risk of CVD is that of a male with two CVD risk factors - roughly 50% (NEJM 2012;366:321-9) Assume that with multiple risk factor modification we can reduce that risk relatively by 60% (VERY optimistic) Sources of information Risk goes from 50% ➡ 20% 30% of individuals BENEFIT 70% DO NOT despite a LIFETIME of treatment A FEW USEFUL PLACES Cochrane Library thennt.com AHRQ treatment options University of Laval decision box Best Science (BS) Medicine Podcast Tool For Practice Therapeutics Initiative RxFiles My Studies Centre for Evidence Based Medicine (UK) Prescrire Ottawa Hospital Decision Aids Less is More Medicine http://www.therapeuticcommandments.org Golden Pill Award Major therapeutic advance Clear advantage Modest improvement 2011 0 0 2012 0 0 0 2 2013 0 0 2014 2015 1 cholic acid (hereditary bile acid deficiency) 1 meningococcal conjugate vaccine (infant immunization) 3 imatinib (ALL artesunate (malaria) sofosbuvir (HepC) conjugate vaccine (infant immunization) 0 abiraterone (prostate CA) boceprevir (Hep C) 1 propranolol (severe infantile hemangioma) 1 sodium phenylbutyrate coated granules (urea cycle disorders) 2 permethrin (scabies) ketoconazole HRA (endogenous Cushing’s syndrome) Prioritize the medications Polypharmacy/ Polytesting a)Will it Reduce Symptoms? Is it actually helping? b)Will it Reduce the Risk of Future Illness? Is the size of the effect big enough to justify the potential side effects, costs and inconvenience? c)Will it Cause Harm? Are any of their symptoms being caused by their medication? James McCormack and G. Michael Allan MEDSTOPPER DON’T: Seven Deadly (PHE) Sins 1) Review of Systems (Mike’s rule) 2) Screen for depression (or virtual anything) 3) Urinalysis, CBC, LFT, creatinine, any biomarker, etc 4) Chest x-ray, ECG, virtual anything 5) Cholesterol or sugar in “young” (<40) healthy 6) Other time wasters: like waist circumference - or even mention metabolic syndrome. 7) Don’t recommend Vitamins, ASA, low salt, etc canadiantaskforce.ca medstopper.com What do Normal Backs Look Like 33 studies (3110 pts, no Hx of any back pain) of CT/MRI findings. Anti-CCP, with ~96% specificity and ~14 positive likelihood ratio, is good for assisting with the diagnosis of RA Anti- CCP is present in only 1⁄4 to 1⁄2 of patients before or at diagnosis, so a negative test does NOT rule out RA can also predict more aggressive joint erosion AJNR Am J Neuroradiol. 2015 Apr;36(4):811-6 Variability in glucose measurements Seasonal variation 0.2-0.5% Higher in winter Am J Epi 2004;161:565-74 The A1c Test and Diabetes National Diabetes Information Clearinghouse We Are All Individuals Every patient is an “n of 1” study Every treatment is an experiment Natasha Press Faculty/Presenter Disclosure Do we need to prevent “Bad Blood” with prophylactic antibiotics? Natasha Press Division of Infectious Diseases St. Paul’s Hospital May 6, 2016. Disclosure of Commercial Support • Potential for conflict of interest: none • Mitigating Potential Bias: • I will not be discussing any products from companies from whom I have received commercial support Endocarditis prophylaxis guidelines • Timeline: • 1955: first AHA (American Heart Association) guidelines recommend penicillin • 2007: AHA limits prophylaxis to highest‐risk patients undergoing highest‐risk procedures • 2008: UK recommends no endocarditis prophylaxis • Faculty: Natasha Press • • • • • Relationships with commercial interests: Grants/Research Support: none Speakers Bureau/Honoraria: Pfizer, Merck Consulting Fees: none Other: Advisory board (Pfizer) Objectives • When to use prophylactic antibiotics: • 1. Cardiac indications – To prevent endocarditis • 2. Orthopedic indications – To prevent prosthetic joint infection Evolution of endocarditis prophylaxis • Rationale for antibiotic prophylaxis before dental procedures: Eliminate bacteremia that could cause endocarditis • No firm scientific evidence to support this • Daily activities cause transient bacteremia • No randomized control trial – cost, numbers, medicolegal issues • Pro: prevents cases of infective endocarditis • Con: unproved, expensive, potentially harmful Natasha Press AHA 2007: Highest risk patients 1. Prosthetic heart valves • mechanical and tissue 2. Prior history of Infective endocarditis 3. Cardiac transplant valvulopathy (leaflet pathology and regurgitation) 4. Congenital heart disease – Unrepaired cyanotic – Repaired with prosthetic material within 6 months – Repaired with residual defects at site of prosthetic device Non‐dental procedures • Respiratory procedures: Incision/biopsy of respiratory tract mucosa – e.g. tonsillectomy, bronchoscopy with biopsy • No prophylaxis for: – GU procedures – GI procedures – Skin/MSK procedures – (unless procedure is in ongoing infection) Who should get prophylaxis? • Patient with an implantable cardiac defibrillator undergoing dental root canal AHA 2007: Highest risk procedures • Dental: Manipulation of gingival tissue or oral mucosa • Not for: – Routine cleaning – Anaesthetic injection through tissue – Placement of orthodontic appliances • Single‐dose amoxicillin 2g • cephalexin 2g, azithromycin 500mg, clindamycin 600mg Cases • Who should get antibiotic prophylaxis? • Patient with an implantable cardiac defibrillator undergoing dental root canal Who should get prophylaxis? • Patient with a bioprosthetic aortic valve replacement undergoing dental root canal • • • • NO NO prophylaxis for patients with ICD or pacemakers Not a high‐risk patient (prosthetic valve, previous IE, transplant valvulopathy, congenital heart) Natasha Press Who should get prophylaxis? • Patient with a bioprosthetic aortic valve replacement undergoing dental root canal • • • • YES High‐risk patient High‐risk procedure (gingival tissue, periapical, oral mucosa) Who should get prophylaxis? Who should get prophylaxis? • Pediatric patient with recently repaired congenital heart disease (prosthetic material used) undergoing tonsillectomy Current recommendations • Pediatric patient with recently repaired congenital heart disease (prosthetic material used) undergoing tonsillectomy • YES • High‐risk patient • Congenital heart disease – Unrepaired cyanotic – Repaired with prosthetic material within 6 m – Residual defects at prosthetic device • High‐risk procedure – Incision/biopsy of respiratory tract mucosa UK Before and After Study: 5 years later • In Canada: we follow the AHA guidelines • In UK: no endocarditis prophylaxis since 2008 • Retrospective before and after study: • Change in antibiotic prescribing • Change in rates of endocarditis Thornhill MH et al. BMJ 2011; 342:d2392 UK Before and After Study • Change in rates of endocarditis – Significant increase in endocarditis • Change in antibiotic prescribing: – 419 cases more than expected (95% CI 95‐743) – Single‐dose of amoxicillin or clindamycin – Suggests 66 extra deaths (95% CI 15‐117) – 88 % decrease – NNT: 1 in 277 – 277 prescriptions to prevent one case of endocarditis Thornhill MH et al. British Dental Journal; 28 (11) June 2015 Thornhill MH et al. British Dental Journal; 28 (11) June 2015 Lancet 2015; 385: 1219 Natasha Press Adverse events to prophylaxis • Amoxicillin: Let’s do what Canada does! Prophylaxis for high‐risk patients! – NO fatal adverse reactions in 35 years – Very safe (safer than we thought!) • Clindamycin: – 1 fatal reaction every 3 years (C. difficile) – We need a different alternative to amoxicillin We will not be influenced by the colonies! Thornhill M et al. J Antimicrob Chemother 2015 UK Updated Guidelines (2015) Follow‐up for AHA guidelines • No increase in endocarditis (VGS) since 2007 • No antibiotic prophylaxis • Amoxicillin 2 g • Good oral health • Clindamycin 600 mg • Cephalexin 2g Fine Print: “The application of the recommendations in this guideline are not mandatory and the guideline does not override the responsibility of healthcare professionals to make decisions appropriate to the circumstances of the individual patient” Orthopedic devices • Azithromycin or clarithromycin 500 mg Mayo Clin Proc 2015: 90(7); 874. Orthopedic devices • No prophylaxis for dental procedures • Low rate of late prosthetic joint infections (1‐2%) • Paucity of data to support/refute prophylaxis • Antibiotic prophylaxis debate • “Recommendations for Antibiotics in Patients with Joint Prosthesis Are Irresponsible and Indefensible”. J Can Dent Assoc. 2009;75 (7). • New in 2013 • Canadian Dental Association Position Statement “routine antibiotic prophylaxis is not indicated for dental patients with total joint replacement”. • Similar to American Dental Association (ADA)/American Academy of Orthopedic Surgeons (AAOS) Natasha Press Who should get prophylaxis? • Patient with multiple prosthetic joints Who should get prophylaxis? • Patient with multiple prosthetic joints undergoing root canal on every tooth undergoing root canal on every tooth • NO • No antibiotic prophylaxis for patients with prosthetic joints undergoing dental procedures Final case • Patient with prosthetic joints do not require antibiotic prophylaxis prior to: – Dental procedures – GI procedures – Urologic procedures Final case • Patient with prosthetic aortic valve and total knee replacement undergoing: • 1. excision of a suspicious nevus • 2. skin biopsy of an area of cellulitis Final case • Patient with prosthetic valve and total knee replacement undergoing: • Patient with prosthetic valve and total knee replacement undergoing: • 1. excision of a suspicious nevus • NO prophylaxis • 2. skin biopsy of an area of cellulitis • YES prophylaxis, but not amoxicillin! • Cover skin pathogens likely to cause bacteremia and endocarditis Natasha Press Conclusions • 1. Cardiac indications: • We follow AHA 2007 guidelines: Amoxicillin to patients at highest risk undergoing high‐risk procedures • UK has abandoned prophylaxis because of lack of evidence • 2. Orthopedic indications: • Everyone agrees no prophylaxis required References • • • • • • • • Wilson W et al. Prevention of infective endocarditis. Guidelines from the American Heart Association…Circulation 2007;116:1736‐54 Thornhill M et al. Impact of the NICE guideline recommending cessation of antibiotic prophylaxis for prevention of infective endocarditis: before and after study. BMJ 2011; 342 d2392 Thornhill M et al. NICE and antibiotic prophylaxis to prevent endocarditis. British Dental Journal; 28 (11) June 2015 Thornhill M et al. Incidence and nature of adverse reactions to antibiotics used as endocarditis prophylaxis. J Antimicrob Chemother 2015. Dayer M et al. Incidence of infective endocarditis in England, 200‐13, a secular trend, interrupted time‐series analysis. Lancet 2015; 385: 1219. DeSimone DC et al. Incidence of Infective Endocarditis Due to Viridans Group Streptococci…Inpatient Sample. Mayo Clin Proc. 2015; 90(7); 874‐81. 2013 CDA Position on Dental Patients with Prosthetic Joint Replacement. J Can Dent Assoc 2013;79 d126 Watters W 3rd et al. Prevention of orthopaedic implant infection in patients undergoing dental procedures. J Am Acad Orthop Surg March 2013 ; 21:180‐189. Conclusions • ID, cardiologists, dentists, orthopaedic surgeons… agree: • 1. Excellent dental hygiene • 2. Antimicrobial stewardship Dee Mangin CFPC CoI Templates Slide 1 I Can’t Fight this Feeling: Stopping SSRIs Faculty/Presenter Disclosure • Faculty/Presenter: Dee Mangin • Relationships with commercial interests: • No funding gifts or food from drug or diagnostic industries • Consulting Fees: I have occasionally provided expert witness reports for the plaintiff in class action legal cases taken against pharmaceutical companies. Any fees are donated to an independent patient drug side effect information and reporting website RxISK.org Dee Mangin David Braley Nancy Gordon Chair in Family Medicine Learning objectives • Understand the issues around prescribing of antidepressants • Understand the strengths and weaknesses of the evidence around long term maintenance treatment to prevent depression recurrence • Have evidence to inform shared decision making (conversations with patients!) around discontinuation vs continuation of maintenance SSRIs (Absolute risk difference, NNT, NNH, NNTrial…..) • Learn practical approaches to tapering and stopping SSRIs Where’s the harm? • • • • • • • • • • • Increased bleeding risk Increased risk of falls in seniors Serotonin syndrome in combination with other drugs Drug interactions Sleep disturbance Reduced bone density Reduced emotional reactivity Tolerance to effects (“Poop out”) Sexual dysfunction Accidental pregnancy exposure …………… Summary of The Problem • Many guidelines for primary care recommend maintenance treatment with SSRIs in certain patients: • There is little evidence to support this but it is driving widespread SSRI use • There are increasing reports of adverse effects of long term use Examining the evidence base • Meta‐analysis of maintenance treatment after initial response to SSRIs show relapse rate 41% on placebo vs 18% on active treatment • Absolute difference 23% NNT 4‐5 Geddes et al Lancet 2005 Dee Mangin What we know about publication bias in studies of acute treatment is likely to apply to studies of long term use as well With permission of Dr Erick Turner 2010 With permission of Dr Erick Turner 2010 Benefit (trial) Trial design flaws outcome threshold • Almost all trials before need for tapering known • Many short duration or still during the acute treatment phase • Outcome measures inadequate (‘return of symptoms’) • No trials in primary care population where 90% of prescription occurs Benefit (attenuated) harm Low Severity / risk high Trial Patients Patients in Practice Primary Care S condary Care Kend ck Hega ty Glasz ou BMJ 2008 Oct 24 337 Current maintenance treatment recommendations ‘3 or more episodes’ ‘additional risk factors for recurrence (e.g. ongoing psychosocial stressors)’ ‘patient preference’ ‘comorbid conditions’ Antidepressant Cessation Trial • Multicentre double blinded placebo controlled RCT of long term maintenance SSRI vs gradual withdrawal to placebo in primary care • 18 month follow up • Primary outcome: occurrence of moderately severe depression • standard DSM based diagnosis based on the interviewer administered MADRS • validated cutpoint = 24 (100% agreement with clinician rating) ‘In many patients…….. treatment will be required indefinitely’ American Psychiatric Association Australasian Clinical Trials Registry 2008 ACTRN12608000613303 Dee Mangin Was there any harm in trying? Source population • Secondary outcomes: • At 18 months a comparison of: interviewer and patient reported mood, overall quality of life and functioning, overall psychological distress / symptoms, social and occupation functioning….. • Depression diagnosed and treated in primary care • On treatment with fluoxetine for at least 12 months (15 months or greater) as maintenance to prevent recurrence of acute depression • Currently in remission Who took part? Results: Primary Outcome • 33% (419/1273) responded to a mailed invitation to participate People want to try stopping • Randomised to Placebo masked taper over 4 weeks if 20 mg (longer if higher dose) vs Continuation at current dose • Absolute difference in recurrences 12.8% (96% CI 3.4%‐22.3%, p=0.005) 23.3% depression recurrences in the taper arm 10.5% depression recurrences in the continuation arm • Most dated their depression onset back to at least 5 years previously • The majority of the difference: 6‐16 weeks after taper • Most had had multiple episodes • No difference in subthreshold symptoms (‘not so well’) Summary What happened next: Were patients worse off for trying to stop? Maintenance antidepressants prevent an episode of depression in the subsequent 18 months in 12 8% of patients. NNT (18 months) is 8 7/8 patients taking long term medication experience no benefit For every 16 taking medication one is unable to discontinue because of intolerable withdrawal symptoms. (NNH 16) It seems reasonable to trial withdrawal NNTrial = 2 On measures of interviewer and patients reported mood, overall quality of life and functioning, overall psychological distress / symptoms, social and occupation functioning….. No suggestion of poorer outcomes at 18 months for those who trial discontinuation Dee Mangin Domains of withdrawal symptoms Observations Somatic • disequilibrium (e.g. dizziness, ataxia, vertigo), • gastrointestinal symptoms (e.g. nausea, vomiting) • flu‐like symptoms (e.g. fatigue, lethargy, myalgia, chills) • sensory disturbances (e.g. parasthesiae, electric shock sensations) • sleep disturbances (e.g. insomnia, vivid dreams) Psychological • Given the mean number of long term medications older patients take in most developed countries is 7, evidence is needed about the effects of continuation vs discontinuation • Pragmatic discontinuation trials are ideal for assessing drug effectiveness and safety, against a background of short term industry trials subject to bias • The high response rate of eligible patients for this trial carried out in routine practice indicates significant patient desire for such trials of discontinuation in a ‘safe’ setting. • anxiety/agitation, irritability and bouts of crying Do sometimes result in a change in depression rating scale scores (i.e. they look like the original indication) From Discontinuation Emergent Signs and Symptoms Scale How to stop Leaping into the void…. • Little evidence to guide best way to stop SSRIs • Evidence that some have more significant discontinuation symptoms than others (paroxetine, venlafaxine): an important consideration when you are choosing a treatment to start • Various approaches advocated (evidence free) practical suggestions • Switch to longer half life (as with benzos: NO EVIDENCE THIS IS HELPFUL) • Taper off (seems rational but no evidence for rate of taper) • Alternating days: unhelpful especially with shorter half life drugs P‐E‐T 1 Preparation 2 Engagement • Explain to the patient that stopping can be easy or more difficult • Patients on antidepressants for longer may need a longer taper: • Let patients know they will be no worse off for trying to discontinue • Suggest they engage family and friends as supports • Optimise non pharmacological management options • On them for months – take weeks to stop • On them for years – take months to stop • Prepare the patient for discontinuation effects, and reassure them they (especially unusual sensations) are not harmful or life threatening • Rare but important: Warn specifically about emergent suicidal ideation and akathisia and what to do Dee Mangin 3 Taper Taper ‐ monitoring • All SSRIs need tapering (yes fluoxetine too) • A test drop in dose of say 10% may signal the required rate of taper • Put control of the taper rate in the patients hands • Suggest: Have a clear plan about • If 10% is OK try dropping by 25% steps • If not stay at 10% or less increments • Some patients have trouble with the final drop – if this appears to be happening suggest an exponential decay rather than linear drop (e.g. halve or quarter the previous dose each time) • For those needing smaller increment drops you can tablet split or get a liquid preparation (find a compounding pharmacy near you) • If the patient cannot afford compounding, most SSRIs can be dissolved and a proportion of the resultant (well shaken) liquid can be calculated (Consult a pharmacist near you to confirm solubility) • Some people may not be able to discontinue completely and the lowest dose required to control discontinuation symptoms will minimise harms ( “Dose size does matter” McCormack, J) • • • • What to monitor Who will monitor How often What the agreed criteria for considering restarting are going to be • patients will feel more reassured about trialling a taper if it is framed as ‘pause and monitor’ knowing they can restart. This is one of patient’s expressed fears about deprescribing of any medication. Alan Cassels CFPC CoI Templates: Slide 1 Faculty/Presenter Disclosure The Cochrane Collaboration “Everyday I write the book” Faculty/Presenter: Alan Cassels Alan Cassels, Best Science Medicine Course The Fairmont Waterfront, Vancouver BC May 6, 2016 Relationships with commercial interests: Grants/Research Support: CIHR Knowledge Translation grant (Medstopper) Speakers Bureau/Honoraria: None Consulting Fees: DECA Consulting; Quizzify.com; Other: Book royalties: Agio Publishing; Greystone Publishing Twitter: @akecassels CFPC CoI Templates: Slide 2 CFPC CoI Templates: Slide 3 Disclosure of Commercial Support Potential for conflict(s) of interest: Alan Cassels has received (or will receive) funding from Agio Publishing and Greystone Publishing whose product(s) are being discussed in this program. Mitigating Potential Bias I have no commercial interest (shares, research consultancies, etc) and am not dependent on the success or failure of the pharmaceutical industry (Selling Sickness), the medical screening industry (Seeking Sickness) or the Cochrane Collaboration. I don’t expect you to purchase any of my books, nor do I expect you to recommend them to your patients. My books are available on Amazon, in libraries and the discard pile of your local bookstore. 27th Annual Best Science Medicine Course: Slide 4 Learning Outcome Objective Slide I expect attendees to my lecture will learn something about the origins and creation of the Cochrane Collaboration so that when they Google “Cochrane Library” they will be able to search a vast storehouse of systematic reviews on almost all areas of healthcare. Elvis Costello “I'm a man with a mission in two or three editions, And I'm giving you a longing look. Everyday, everyday, everyday I write the book…” “Don't tell me you don't know the difference, Between a lover and a fighter. With my pen and my electric typewriter…” Alan Cassels Archie Cochrane (1909-1988) “How can we have a rational health service if we don’t know which of the things being done are useful and which are useless or possibly even harmful?” Sir Iain Chalmers “People don’t need islands unconnected to any continent, they want something that tells them: ‘What does it mean?’” Effectiveness and Efficiency: Random Reflections on Health Services, 1972 “Humans need clean, clear health information like they need clean, clear water.” The Cochrane Collaboration (under construction) What determines if a healthcare intervention ‘works’? Alan’s water fountain --Sir Muir Gray Who is Cochrane? People asking hard questions and questioning answers http //vancouverisland ctvnews.ca/video?clipId=766895 Alan Cassels What the heck does this symbol mean? Systematic Reviews. • Each line is one trial (the shorter the line, the more certain the result); • The vertical line indicates the position if the two treatments compared in the trials had similar effects; • A line touching the vertical line, means that that particular trial found no clear difference. • The diamond represents their combined results. • The diamond to the left of the vertical line indicates that the treatment is beneficial. • If the diamond is to the right of the line would show that the treatment did more harm than good. “The notion of systematic review — looking at the totality of evidence — is quietly one of the most important innovations in medicine over the past 30 years.” Goldacre, B. Forward to Evans I, Thornton H, Chalmers I, et al. Testing Treatments Better Research for Better Healthcare. 2nd edition. London Pinter & Martin; 2011. Who is out there producing gold standard evidence? “Like all great ideas, it’s so simple and obvious that it just had to be done.” Page 37. p. ix Kay Dickersin What kinds of questions has Cochrane tackled? Was High Dose Chemotherapy with Autologous Bone Marrow Transplantation HDC/ ABMT beneficial to treat breast cancer? p.4 Alan Cassels Peter Gøtzsche What is the effectiveness of mammography screening? How many do you have to screen to save a single life? Lives saved: 1 in 2,100 women False positives: 690 in 2100 You have high blood pressure: How low do you need to go? Alan Cassels The SPRINT TRIAL: “Aiming lower saves more lives when it comes to controlling blood pressure…” Cochrane Hypertension Group Patricia Crowley For premature infants do steroids work to prevent respiratory distress and save lives? p.76 There are REAL human costs resulting from failure to perform systematic, up-to-date reviews of RCTs of health care: The case of steroids and prematurity. • First RCT in 1972. • By 1991, seven more trials had been reported, • Corticosteroids reduces the odds of the babies of these women dying from the complications of immaturity by 30 to 50 per cent. • Patricia Crowley published her systematic review in1989. • Up to then most obstetricians didn’t realize that the treatment was so effective. • Tens of thousands of premature babies have probably suffered and died unnecessarily (and needed more expensive treatment than was necessary). Tom Jefferson Do people need to get a flu shot every year? Does it make sense for governments to be stockpiling billions of dollars worth of antivirals? Alan Cassels What do we mean when we say flu vaccines ‘work?’ Flu vaccines are effective in reducing infection and in slightly reducing absence from work in adults, but there is no evidence that they reduce transmission, hospitalization, pneumonia, or death. There is poor‐quality evidence from cohort studies that vaccines are effective in elderly people living in institutions, but there is little good‐quality evidence for the elderly population in general. A 2007 systematic review of 274 influenza vaccine studies found: Industry‐funded studies were published in more prestigious journals and cited more than other studies independently from methodological quality and size. Studies funded from public sources were significantly less likely to report conclusions favourable to the vaccines. Generally reliable evidence on influenza vaccines is thin but there is evidence of widespread manipulation of conclusions and spurious notoriety of the studies. T Jefferson C Di Pietrantonj M G Debalini A Rivetti V Demicheli Relation of study qua ity concordance take home message funding and impact in studies of influenza vaccines: systematic review BMJ. 2009; 338: b354. Published online 2009 February 12. http //www ncbi nlm nih gov/pmc/articles/PMC2643439/?tool pubmed Jefferson TO Rivetti D Di Pietrantonj C Rivetti A Demicheli V. Vaccines for preventing influenza in healthy adults. Cochrane Database Syst Rev. 2007 Apr 18;(2):CD001269. http://www.ncbi.nlm.nih.gov/pubmed/17443504 Alan vs Perry Alan Cassels, flu agent provacateur “the Why does some vaccine research rise to the top? science is on my side” Sir Ian Chalmers Dr. Perry Kendall, flu aficionado “the science is on our side” Shouldn’t we be absolutely rigorous about the science? Sir Iain Geoffrey Chalmers By Ju ia Fullerton-Batten, 27 Feb 2006 – National Portrait Gallery “Be careful of reading health books. You may die of a misprint.” --Mark Twain What is the question to which you’d like a Cochrane-level answer? cassels@uvic ca @AKEcassels (250) 361-3120 Feedback and criticism: cassels@uvic ca Ric Arseneau CENTRAL SENSITIVITY SYNDROMES: “DO YOU FEEL LIKE I DO?” FACULTY/PRESENTER DISCLOSURE ๏ Faculty/Presenter: Ric Arseneau Ric Arseneau, MD FRCPC MA(Ed) MBA FACP CGP Clinical Associate Professor Division of General Internal Medicine St. Paul's Hospital & BC Women’s Hospital Director of Program Planning Complex Chronic Diseases Program University of British Columbia ๏ Relationships with commercial interests: ๏ None DISCLOSURE OF COMMERCIAL SUPPORT MITIGATING POTENTIAL BIAS ๏ This program has received NO financial support. ๏Treatment ๏ This program has received NO in-kind support. ๏ Potential for conflict(s) of interest: ๏ None LEARNING OUTCOME OBJECTIVE Participants should be able to: 1. Identify clinical presentations that should include CSS in the differential 2. Name the predisposing, precipitating, and perpetuating factors for these conditions 3. Explain to patients the basic physiology involved in these conditions 4. Access physician and patient resources to manage these conditions recommendations are approved by the Clinical Advisory Committee at the Complex Chronic Diseases Program, BC Women’s Hospital, UBC Ric Arseneau 501534 MEDICALLY UNEXPLAINED SYMPTOMS 2013 HPQ0010.1177/1359105313501534Journal of Health PsychologyStenhoff et al. Article Understanding medical students’ views of chronic fatigue syndrome: A qualitative study IS IT REAL ? Journal of Health Psychology 2015, Vol. 20(2) 198–209 © The Author(s) 2013 Reprints and permissions: sagepub.co.uk/journalsPermissions.nav DOI: 10.1177/1359105313501534 hpq.sagepub.com Alexandra Laura Stenhoff, Shireen Sadreddini, Sarah Peters and Alison Wearden Medicalization ? Malingering ? Psychiatric ? Abstract Chronic fatigue syndrome receives little attention in the medical curriculum. This study explores UK medical students’ knowledge of and attitudes towards chronic fatigue syndrome. Semi-structured interviews (average length 22 minutes) were conducted with 21 participants (7 females and 14 males) in years 3 (n = 4), 4 (n = 11) and 5 (n = 6) of their studies. Inductive thematic analysis taking a realist perspective produced three themes: limited knowledge, influences on attitudes and training needs. Students acquired their knowledge and attitudes largely from informal sources and expressed difficulty understanding chronic fatigue syndrome within a traditional biomedical framework. Incorporating teaching about chronic fatigue syndrome into the medical curriculum within the context of a biopsychosocial understanding of illness could encourage more positive attitudes towards chronic fatigue syndrome. Free-association exercise with housestaff Keywords beliefs, chronic fatigue syndrome, health education, models, qualitative methods 4 OVERLAPPING GROUPS Pain Fatigue Unexplained Symptoms Sleep Dysfunction Noncardiac Chest Pain and Fibromyalgia CENTRAL SENSITIVITY SYNDROMES Fig. 1. Central sensitization syndromes share a common etiologic mechanism of central sensitization and frequently present with overlapping epidemiologic, clinical, and psychological features. (Adapted from Yunus MB. Role of central sensitization in symptoms beyond muscle pain, and the evaluation of a patient with widespread pain. Best Pract Res Clin Rheumatol 2007;21:481–97; with permission.) Introduction Chronic fatigue syndrome, also named myalgic and Hotopf, 2005) and often results in substanencephalomyelitis (CFS/ME), is a debilitating tial impairment and high levels of health-care condition affecting 0.2–0.4 per cent of the UK use (McCrone et al., 2003). Indeed, it has been population (CFS/ME WG, 2002). It is charac- shown that CFS/ME intrudes into more life terised by severe, disabling fatigue, not domains (i.e. work, recreation and health), and explained by other medical conditions, and pre- to a greater degree, than other chronic illnesses sent for 6 months or more, usually in conjunction with other symptoms (Fukuda et al., 1994; Sharpe et al., 1994). In the absence of labora- B. University of Manchester, UK Muhammad Yunus, MD tory tests or blood tests, diagnosis is made based on history and exclusion of other possible Corresponding author: Alexandra Laura Stenhoff, University of Manchester, 11 causes for the fatigue (National Institute for Macintosh Mills, 4 Cambridge Street, Manchester Semin Arthritis Rheum 36:339-356 Health and Clinical Excellence (NICE), 2007). M15GG, UK. CFS/ME has an uncertain prognosis (Cairns Email: stenhoff.alexandra@gmail.com Fibromyalgia and Overlapping Disorders: The Unifying Concept of Central Sensitivity Syndromes Downloaded from hpq.sagepub.com at University of British Columbia Library on September 12, 2015 277 M.B. Yunus Semin Arthritis Rheum 36:339-356 Figure 2 Simplified suggested biopsychosocial mechanisms for CS and CSS with interacting factors. ANS, autonomic nervous system. The relationship between central sensitization and CSS may be bidirectional; chronicity of CSS may accentuate central sensitization. Ric Arseneau CENTRAL SENSITIVITY SYNDROMES The 3 P’s Predisposing ๏ Precipitating ๏ Perpetuating ๏ PRECIPITATING ๏ Precipitant vs. “Cause” ๏ Stressor ๏ Physical ๏ Psychological ๏ Infectious ๏ Forest Fire Analogy ๏ ? Lightning strike ๏ ? Camp fire ๏ ? Cigarette ๏ ? Arson ๏ Can’t go back and “undo” or “fix” ๏ Deal with the problem - now PREDISPOSING ๏Genetic predisposition ๏ Twin studies ๏ Identical - 50% ๏ Fraternal - 25% ๏ Family members ๏Childhood PRECIPITANT / STRESSOR Physical Psychological Infectious ๏ ๏ ๏ ๏ Trauma (PTSD) ๏ “Burn out” ๏ Other ๏ Viral ๏ Bacterial ๏ Other Car accident Surgery Other injury PERPETUATING... NIH Public Access Author Manuscript J Behav Neurosci Res. Author manuscript; available in PMC 2011 January 18. Published in final edited form as: J Behav Neurosci Res. 2009 January 1; 7(2): 1–17. trauma Poor Sleep Over-exertion Reduced Activity Depression Anxiety Stress Kindling and Oxidative Stress as Contributors to Myalgic Encephalomyelitis/Chronic Fatigue Syndrome L. A. Jason1,*, N. Porter1, J. Herrington1, M. Sorenson1, and S. Kubow2 DePaul University 1 2 McGill University KINDLING THEORY: UPREGULATION ๏ Prolonged stimulation of the limbic-hypothalamic-pituitary axis ๏ High-intensity ๏ Chronically ๏ stimulation repeated low- intensity stimulation Exceeds “threshold limits” ๏ Resulting in persistent hypersensitivity / low activation threshold firing ๏ Spontaneous ๏ Neuroplastic changes Ric Arseneau PAIN PATHWAY CHRONIC PAIN Sensitization & Amplification CHRONIC PAIN: SENSITIVITY SHIFT ! PAIN 154 (2013) S10–S28 www.elsevier.com/locate/pain Review Glia and pain: Is chronic pain a gliopathy? Ru-Rong Ji a,⇑, Temugin Berta a, Maiken Nedergaard b a b Department of Anesthesiology and Neurobiology, Duke University Medical Center, Durham, NC, USA Division of Glial Disease and Therapeutics, Center for Translational Neuromedicine, University of Rochester, Rochester, NY, USA ๏ Opioids ๏ Glial and gliopathy health ๏ Low Dose Naltrexone (LDN) ๏ PEA (palmitoyethanolamide) bs_bs_banner FIBROMYALGIA Pain Medicine 2013; 14: 895–915 Wiley Periodicals, Inc. MUSCULOSKELETAL SECTION Original Research Article Excessive Peptidergic Sensory Innervation of Cutaneous Arteriole–Venule Shunts (AVS) in the Palmar Glabrous Skin of Fibromyalgia Patients: Implications for Widespread Deep Tissue Pain and Fatigue Phillip J. Albrecht, PhD,*,† Quanzhi Hou, MD PhD,*,† Charles E. Argoff, MD,‡ James R. Storey, MD,§ James P. Wymer, MD PhD,‡ and Frank L. Rice, PhD*,† Conclusions. The excessive sensory innervation to the glabrous skin AVS is a likely source of severe pain and tenderness in the hands of FM patients. Importantly, glabrous AVS regulate blood flow to the skin in humans for thermoregulation and to other tissues such as skeletal muscle during periods of increased metabolic demand. Therefore, blood flow dysregulation as a result of excessive innervation to AVS would likely contribute to the widespread deep pain and fatigue of FM. SNRI compounds may provide partial therapeutic benefit by enhancing the impact of sympathetically mediated inhibitory modulation of the excess sensory innervation. ๏ Excessive sensory innervation to A-V shunts ๏ Blood flow dysregulation ๏ Symptoms Ric Arseneau EPIDEMIOLOGY OF FIBROMYALGIA Clinical Review & Education Clinical Crossroads Fibromyalgia A Clinical Review Daniel J. Clauw, MD • • After OA • 2% to 8% of the population • Treatment Almost all women Cost Grades of Recommendations General Newer criteria: symptom based and do not require tender points • • Clinical Reviewreview & Education Clinical Crossroads 1: Systematic of randomized trials or n-of-1 trial 2: Randomized trial or (exceptionally) observational studies with dramatic effect 3: Non-randomized controlled cohort/follow-up study 4: Systematic review of case-control studies, historically controlled studies Table. Summary of Treatment Guidelines34 5: Opinion Diagnostic criteria (1990): chronic widespread pain with tender points • Centralized pain state therapies Graded exercise36 Cognitive behavioral therapy (CBT)37 Low principles of of Incorporate principles self-management including including aa self-management approach multimodal approach Adverse Effects Aerobic exercise has been best studied but strengthening and stretching have also been shown to be of value Fibromyalgia Fibromyalgia 1A Worsening of symp when program is b rapidly Low Pain-based CBT programs have been shown to be effective in one-on-one settings, small groups, and via the Internet 1A Most CAM therapies have not been rigorously studied 1A No significant adve effects of CBT per s patient acceptance poor when viewed “psychological” int Generally safe 34 Table. Summary of Treatment Guidelines34 Details Evidence Level Low Clinical Review & Education Clinical Crossroads Cost Details A:recommendations Consistent level 1 studies B: Consistent level 235or 3 Low studies or extrapolations level of 1 studies 1A Patient education Incorporatefrom principles including a C: Level 4 studies or extrapolations fromself-management level 2 or 3 studies multimodal approach D: Level 5 evidence or troublingly inconsistent or inconclusive studies of any level Consensus Nonpharmacological Female:Male ratio of 2:1 Treatment General recommendations Patient education35 1547 Level of evidence Second most common “rheumatic” disorder • JAMA April 16, 2014 Volume 311, Number 15 Evidence Evidence Level Level Adverse Effects Effects Adverse Complementary and Variable Trusted(Patient(Resources:( Clinical Pearls Clinical Pearls alternative medicine Fibromyalgia(( 38 (CAM) therapies UpToDate) 1A 1A Followinginitial initialdiagnosis, diagnosis,spend spendseveral several Following CFIDS)&)Fibromyalgia)Self7Help) visits(or (oruse useseparate separateeducational educational visits Pain)BC) sessions)to toexplain explainthe thecondition conditionand andset set sessions) treatmentexpectations expectations treatment Headache Central ME|FM)Society)of)BC) nervous Several types of CNS neusystem (CNS) rostimulatory therapies have Nonpharmacological ME/FM)Action)Network) neurostimulatory been effective in fibromyalgia therapies therapies39 and other chronic pain states Counselpatients patientsto to“start “startlow, low, 1A Worseningof ofsymptoms symptoms exercise has has been been best best Counsel 1A Worsening Graded exercise36 Low Aerobic exercise National)Fibromyalgia)Association)(US) (( 5, Consensus Pharmacological Therapies best chosen based goslow” slow” whenprogram programisisbegun begun too go strengthening and and when too studied but strengthening therapies on predominant symptoms and rapidly have also also been been shown shown rapidly stretching have Formany manypatients, patients,focusing focusingfirst firston on For initiated in low doses with slow to be of value increasingdaily daily“activity” “activity”isishelpful helpful increasing Dr.)Arseneau’s)St.)Paul’s)Hospital)Grand)Rounds)presentation)Sept)2015) dose escalation Central)Sensitivity)Syndromes beforeactually actuallystarting startingexercise exercise before 1A Dry mouth, weight Tricyclic Amitriptyline, 10-70 mg once Internet-based programsare aregaining gaining 1A Nosignificant significantadverse adverse CBT programs programs have have Internet-based programs 1A No Cognitive behavioral Low Pain-based CBT 40,41 constipation, “grog compounds daily before bedtime acceptanceand andare aremore moreconvenient convenientfor for effectsof ofCBT CBTper perse sebut but be effective effective in in acceptance effects therapy (CBT)37 been shown to be or drugged feeling Cyclobenzaprine, 5-20 mg once workingpatients patients patientacceptance acceptanceisisoften often settings, small small working patient one-on-one settings, daily before bedtime poorwhen whenviewed viewedas asaa via the the Internet Internet poor groups, and via “psychological”intervention intervention “psychological” Duloxetine, 30-120 mg/d 1A Nausea, palpitation Serotonin norepiDuloxetine therapies have have not not 1A Generallysafe safe Evidenceemerging emerging thatCAM CAMtreatments treatments Complementary and Variable Most CAM therapies 1A Generally Evidence that Milnacipran, headache, fatigue, nephrine reuptake generic; rigorously studied studied suchas astai taichi, chi,isyoga, yoga, balneotherapy, and 100-200 mg/d alternative medicine been rigorously such balneotherapy, and 40 tachycardia, hyper inhibitors acupuncture milnacipran acupuncturemay may beeffective effective (CAM) therapies38 be is not Allowingpatients patientsto tochoose choosewhich whichCAM CAM Allowing therapiesto toincorporate incorporateinto intoan anactive active therapies treatmentprogram programcan can treatment increaseself-efficacy self-efficacy increase Clinical Review & Education Clinical Crossroads Fibromyalgia Clinical Review & Education Clinical Crossroads Headache These treatments Central nervous Several types of Headache These treatmentscontinue continueto tobe be of CNS CNS neuneu42 1A Sedation, weight g Gabapentin, 800-2400 mg/d Gabapentinoids Gabapentin is targets, refined stimulation system (CNS) rostimulatory therapies refinedas asoptimal optimal stimulation targets, therapies have have dizziness in divided doses “dosing,” become neurostimulatory been effective in “dosing,”etc, etc,generic, becomeunderstood understood in fibromyalgia fibromyalgia 39 pregabalin not therapies and other chronic chronic pain pain states states Pregabalin, up to 600 mg/d in34divided 34 5, Prescribing patients aadrug that Pharmacological Therapies best chosen 5, Consensus Consensus Prescribing patientsGuidelines drugregimen regimen that doses chosen based based Table. Summary of Treatment Table. Summary of Treatment Guidelines 43 helps symptoms therapies on predominant helpsimprove improveFor symptoms priorto to predominant symptoms symptoms and and 4.5-6.0 g per night in divided 1A Sedation, respirato γ-Hydroxybutyrate treatingprior initiating therapies initiated in low initiatingnonpharmacological nonpharmacological therapies low doses doses with with slow slow doses depression, and de narcolepsy/ Evidence Evidence help improve dose escalation can helpPearls improve adherence Details escalation cataplexy Costadherence Level Adverse Effects Treatment Cost Details Level Adverse Effects Treatment can Clinical 44 When can 1A Dry gain, Tricyclic Amitriptyline, 10-70 Wheneffective, effective, canimprove improveaawide widemg/d 1A Drymouth, mouth,weight weightLow-dose gain, 10-70 mg mg once once naltrexone Low 4.5 2 small General General 40,41 range constipation, compounds daily before bedtime rangeof ofsymptoms symptomsincluding includingpain, pain,sleep, sleep, constipation,“groggy” “groggy” bedtime single-center recommendations recommendations bowel, and bladder symptoms or bowel, andinitial bladder symptoms ordrugged druggedfeeling feeling Patient education randomized 35 Cyclobenzaprine, 5-20 Cyclobenzaprine, 5-20 mg mg once 1A Low Incorporate 1A Following diagnosis, spend several principles of Patient education35 Low Incorporate principles of once trialsa Taking several hours to daily before bedtime Taking several hoursprior prior tobedtime bedtime bedtime self-management including a visits (or use separate educational self-management including a 45 improves adverse effect profile improves adverse effect profile Cannabanoids NA the condition Nabilone, mg orally at 1Aa Sedation, dizziness multimodal sessions) to explain and set0.5approach multimodal approach bedtime to 1.0 mg twice daily mouth treatment expectations Warning patients about Duloxetine, 30-120 1A Nausea, Serotonin norepiDuloxetine Warning patients abouttransient transient 30-120 mg/d mg/d 1A Nausea,palpitations, palpitations, nausea, taking with food, and slowly Milnacipran, 100-200 mg/d headache, fatigue, nephrine reuptake is generic; nausea, taking with food, and slowly 100-200 mg/d headache, fatigue, Fluoxetine, sertraline, 1A Nausea, sexual dys Selective serotonin SSRIs that Nonpharmacological Nonpharmacological 40 increasing can tolerability tachycardia, inhibitors milnacipran increasingdose dose canincrease increase tolerability tachycardia,hypertension hypertension paroxetine weight gain, sleep reuptake inhibitors should be therapies therapies 40 is not disturbance (SSRIs) used in 36 36 Milnacipran might be slightly more Milnacipran might be slightly more 1A Worsening of symp Graded exercise Lowto “start low, Aerobic exercise has been best Counsel patients 1A Worsening of symptoms Graded exercise Low Aerobic exercise has been best fibromyalgia than noradrenergic thanduloxetine duloxetineand andthus thusbut strengthening and when program is b studied go slow” when program is begun too noradrenergic studied but strengthening and arehelpful all generic potentially more for and potentially more helpful forfatigue fatigue rapidly stretching rapidly stretching have also been shown For many patients, focusing first on and have also been shown memory problems but more memory problems butalso alsois more likely tolikely be of value to be of value increasing daily “activity” helpful to cause hypertension to causeactually hypertension before starting exercise 1A Sedation, weight gain, Giving most or all of the dose at bedtime mg/d Gabapentinoids42 Gabapentin is Gabapentin, 800-2400 1A Sedation, weight gain, Giving most or all of the dose at bedtime 800-2400 mg/d 5D Gastrointestinal, Nonsteroidal antiNo evidenceCBT of efficacy; can be 1A No significant advre Cognitive behavioral Pain-based programs have Internet-basedLow programs are gaining 1A No significant adverse Cognitive behavioral Low Pain-based CBT programs have dizziness can increase tolerability in divided doses generic, dizziness can increaseand tolerability doses 37 cardiac eff drugs helpful for comorbid “peripheral effects adverse of CBT per therapy (CBT) been shown to be effective in acceptance are more convenient for effects of CBT per se inflammatory but therapy (CBT)37 been shown to be effective in pregabalin not Pregabalin, up to pain generators” mg/d to 600 600small mg/d patient acceptance one-on-one settings, small working patients patient acceptance is often one-on-one settings, in divided doses doses 5D Sedation, Tramadol with without poor whenaddiction viewed groups, and viaorthe Internet poor when viewed asOpioids a groups, and via the Internet tolerance, opioid-i acetaminophen, 50-100 mg “psychological” in “psychological” intervention Shown 4.5-6.0 g per night 1A Sedation, γ-Hydroxybutyrate43 For treating night in in divided divided 1A Sedation,respiratory respiratory Shownas asefficacious efficaciousbut butnot notapproved approved hyperalgesia every 6 h doses depression, and by Food and Drug Administration narcolepsy/ depression, anddeath death by Food and Drug Administration Complementary and Variable Most CAM therapies have not 1A Generally safe Complementary and Variable Most CAM therapies have not 1A Generally safe Evidence emerging that CAM treatments because of safety concerns cataplexy because of safety concerns No evidence alternativesuch medicine been rigorously studiedfor alternative medicine been rigorously studied as tai chi, yoga, balneotherapy, and of efficacy 38 38 44 (CAM) therapies (CAM) therapies acupuncture may be effective stronger opioids Low-dose naltrexone Low 4.5 mg/d 22 small small single-center single-center Allowing patients to choose which CAM a Evidence rated by author; not rated by Canadian randomized randomized therapies to incorporate into an activeNational Fibromyalgia Guideline Advisory Panel. trials trialsaa treatment program can 45 aa Ric Arseneau www.bcwomens.ca/health-professionals/professional-resources/complex-chronic-disease COMPLEX CHRONIC DISEASES PROGRAM Fibromyalgia and Chronic Pain in Related Disorders Clinical Protocol Date: Dec 25, 2015 Clinical Protocol: Fibromyalgia and Chronic Pain in Related Disorders PREAMBLE The recommendations below are supported by strong evidence (level A) unless stated otherwise We have added practical “tips” The drugs are presented in the order (more or less) to try them The actual order of use will depend on prior treatment, patient preference, etc. Look for “two fors” (drugs that benefit two or more problems) Provide patient with information/dose adjustment handout Given the different mechanisms of action, patients often end up on 2 or more drugs Patients with ME/CFS may need to be titrated more slowly, and may not tolerate higher doses of medications It is expected that physicians would educate themselves about these drugs beyond the outline provided below The treatments described below may occur one-on-one or in a group setting depending on resources • • • • • • • • • • 1. PATIENT EDUCATION Level A evidence Incorporated into multiple offerings (e.g., handouts, web-based resources) Incorporated into core group: Living with Complex Chronic Diseases “Family and Friends” evening session • • • • 2. PHYSICAL ACTIVITY • • • Level A evidence Offered in group setting and individual sessions with PT and OT Tai-Chi and mild Yoga o Suggested o Offerings in community rather than CCDP 3. SLEEP • • Sleep disturbance is a major component of FM and pain See sleep protocol for details 4. DIET • • Emerging evidence; some RCT data Offered in group setting and individual sessions with dietitian 5. ALTERNATIVE AND COMPLEMENTARY THERAPIES • Some agents have a strong theoretical rational and early evidence o Co-enzyme, D-Ribose 5 g, magnesium Malate, NADH, Vitamin D 5.1 Co-enzyme Q • 200 mg TID Page 1 G. Michael Allan Faculty/Presenter Disclosure Osteoarthritis can be Bad to the Bone • Faculty/Presenter: G. Michael Allan • Relationships with commercial interests: – – – – G. Michael Allan Professor & Director of EBM, Dept of Family Med, U of A Director of Evidence and CPD, Alberta College of Family Physicians Grants/Research Support: Not applicable Speakers Bureau/Honoraria: Not applicable Consulting Fees: Not applicable Other: – Employed by University of Alberta, Alberta Health – Non-profit sources including Alberta College of Family Physicians, TOP, IHE, CADTH, etc. Activity 27th Annual Best Science Medicine Course Learning Objectives • >10 sys revs, focus on last 5 yrs & Cochrane – Largest 60 RCTs with 8218 patients2 – Overall quality moderate We will review and learn about Osteoarthritis Knee Osteoarthritis •Non-Pharmaceutical Management Outcome2 – Exercise, Braces, Taping •Pharmaceutical Management – Acetaminophen, Topical NSAIDs, Oral NSAIDs (including Cox-2’s), Opioids, Glucosamine & Chondroitin, Intraarticular injections (steroid or hylanuronan product) Short-Term Long term (2-6 months) SMD Scores (0-100) SMD Scores Pain 0.49 (0 39-0 59) 44 vs 32 (Ex) 0.24 (0.140.35) 6 pts better Function 0 52 (0 39-0 64) 38 vs 28 (Ex) 0.15 (0.040.26) 3 pts better Quality of Life 0 28 (0.15-0.40) 43 vs 47 Hip similar: estimated NNT 6. Maybe slightly better long-term?3 •NSAID risks (including Cox-2 anti-inflammatories) 1) Cochrane 2008; 4: CD004376. 2) with update 2015 Jan 9;1:CD004376. 3) Cochrane 2014; 4: CD007912. 4) BMJ 2013;347:f5555 doi: 10.1136/bmj.f5555. 5) Arthritis Rheumatol. 2014;66(3):622-36. 6) BMC Musculoskeletal Disorders2011,12:123. 7) Cochrane 2007; 4: CD005523. 8) Arch Phys Med Rehabil 2012;93:1269-85. 9 ) Clin Rehabil. 2013;27:1059-71. 10) J Rheumatol 2009;36:1109–17 Acetaminophen: First do no harm Activity • Acetaminophen (≤10 RCTs, 1712 pts)1,2 • Types of exercise: Generally no diff – Pain, SMD ≤ 0.2 (0.02-0.41) – Pain NNT=16 (any pain relief)2 – But mean pain score diff=3 (from 54/100)4 – Example effect on Pain: Quad strengthening (SMD 0.29); Lower limb strengthening (0.53); strength & aerobic (0.40); walking (0.48); Other (0.32).1 – Subtle diff not consistent5,9 (e.g. Quad > lower limb5) • Others6 (3-7 RCTS, 1336-2355 pts): short-medium term pain/disability 1.7-3.7/100 • Aquatic exercise: 0.26- 0.68 pain,7,4 0.34 function4 – 10 RCTs, aquatic vs Land: No diff in any outcome6 • Effect Size small and NNT poor for a pain • Likely Supervised & more often better (e.g 3/wk)5 • No more research required (had enough by – In most comparative studies, acetaminophen the least effective3-5 & likely not be meaningful4,6 • But harm (except LFTs) similar to placebo1,2,4,6 2002)4 1) Cochrane 2008; 4: CD004376. 2) with update 2015 Jan 9;1:CD004376. 3) Cochrane 2014; 4: CD007912. 4) BMJ 2013;347:f5555 doi: 10.1136/bmj.f5555. 5) Arthritis Rheumatol. 2014;66(3):622-36. 6) BMC Musculoskeletal Disorders2011,12:123. 7) Cochrane 2007; 4: CD005523. 8) Arch Phys Med Rehabil 2012;93:1269-85. 9 ) Clin Rehabil. 2013;27:1059-71. 10) J Rheumatol 2009;36:1109–17 1. Ann Rheum Dis. 2004;63:901-7. 2. Cochrane 2006;1:CD004257. 3. Ann Intern Med. 2015;162: 46-54. 4. Euro J Pain 2007;11:125–38. 5. Osteoarthritis Cartilage. 2010;18:476-99. 6. BMJ 2014;350:h1225 G. Michael Allan Oral NSAIDs: The Balancing Act Oral NSAIDs: The Balancing Act • NSAID vs Acetaminophen3 • Traditional NSAIDs vs Cox-2 selective – No efficacy difference Cox-2 & traditional NSAIDs1 • Meta-analysis2: 23 RCTs, 10,845 pts – Global improve (pt) = 57% NSAID vs 39% NNT 6 – GI AE: Traditional NSAID, 19% vs 13%, NNH=12 • Withdrawal due to GI AE, 8% vs 4%, NNT 25. – VA improved 10.1mm or 15.6%. SMD 0.32. – Exclude run-in bias trials (10 left), SMD 0.23. • Sys Rev5: 25 RCTs, 9964 pts – 10.2 better out of 100 (from baseline of 64) • Network Meta:6 0.33 (celecoxib)- 0.52 (diclofenac) 1. NICE OA Guideline (http://www.rcplondon.ac.uk/pubs/contents/d87b4537-b333-4b8a-a2d8-5e96b7f4b65a.pdf ) 2. BMJ 2004; 329 (7478):1317. 3 Cochrane 2006 (1):CD004257. 4. Ann Rheum Dis. 2004;63(8):901-7. 5. Euro J Pain 2007; 11: 125-38. 6. Ann Intern Med. 2015;162:46-54. Topical NSAIDs: benefit over risk • ≥5 Sys Rev, Most recent from Cochrane – 34 RCTs (7688 pts). RCT quality moderate-good Duration % better on % better on Topical NSAID Placebo RR (95% CI) NNT 2-3 weeks 37% 19% 1 9 (1.6-2.4) 5-6 4-6 weeks 42% 24% 1.7 (1.4-2.1) 6 8-12 weeks 60% 50% 1 2 (1.1-1.3) 10 • Topical = Oral with 15% circulating NSAID level • Topical NSAID Adverse events – No diff between Topical NSAID & placebo in systemic or GI – Local AE: Topical 12.6%vs placebo 7.8%, NNH 21 – Withdrawal due to AE: Topical 5.4% vs Placebo 3.8%, NNH 63 1. BMJ 2004;329(7461):324. 2. J Rheumatol 2006;33:1841–4. 3. www.Bandolier.com March 05. 4. NICE OA Guideline (http://www.rcplondon.ac.uk/pubs/contents/d87b4537-b333-4b8a-a2d8-5e96b7f4b65a.pdf ) 5. J Rheumatolo 2004;31(10): 2002-12. 6. Tools for Practice #40, Jan 24, 2011. Cochrane 2012; 9: CD007400. Chondroitin: More of the Same • Sys Rev1: 43 RCTs, 9110 pts (9 low risk of bias) – 20% improvement on WOMAC: NNT 17, – Pain NNT 4-5 (but my calculation is 10-12) • Pts prefer NSAIDs (RR 2.34) but more GI AE4 • n-of-1 RCT, Celecoxib vs Acetaminophen5 – 80% no preference in 2 Tx; – 17% picked Celebrex (5% sure it was better) – 3% picked Acetaminophen 1. NICE OA Guideline (http://www.rcplondon.ac.uk/pubs/contents/d87b4537-b333-4b8a-a2d8-5e96b7f4b65a.pdf ) 2. BMJ 2004; 329 (7478):1317. 3 Cochrane 2006 (1):CD004257. 4. Ann Rheum Dis. 2004;63(8):901-7. 5 Rheumatology 2007;46:135-140 Glucosamine: Harm=0 (? Benefit) • Sys reviews in last 5 yrs + Cochrane – 7 Sys rev with 2-25 RCTs (414 - 4963 pts). • Pain: Results very widely, SMD 0.16 (ns) to 0.51 (sign) – Some subgroups higher:1-4,7 Rotta brand SMD 1.11 (sign).7 – In larger studies:1 Change in pain scale 0.4 / 10 (Sign). • Clinically meaningful change=0 9 • Function: Vary by trial duration & assessment tool, SMD 0.08 (NS) to 0.54 (sign).2,7 • Adverse effects: None.7 • Approximate yearly cost is $60 at 500mg TID. 1) BMJ. 2010; 341:c4675. 2) Int J Clin Pract. 2013; 67:585-94. 3) Arthritis Care Res (Hoboken). 2014 Jun 6. 4) Osteoarthritis Cartilage. 2010; 18(4):476-99. 5) Rheumatol Int. 2010; 30(3):357-63. 6) Am J Sports Med. 2014 May 27. [Epub ahead of print] 7) Cochrane 2005; (2):CD002946. Viscosupplementation: • ≥7 sys revs. Best = Rutjes 2012:1 89 RCTs – 12,667 patients (mean age 63), ~16 weeks. • Pain reduced (at 3 months) SMD -0.37 (-0.46, -0.28) • Heavily dependent on quality markers • Others find similar: Sys Rev2 (22 RCTs, 4056 pt) PAIN Sensitivity Variable 1 Outcome 1 RCT Size n<100 0.59 (0.31, 0.88) Variable 2 Outcome 2 n≥100 Drug Co Yes 0.52 (0.24, 0.80) No 0.0 (-0.16, 0.15) Study year 1990-99 0.89 (0.66, 1.13) ≥2010 0.06 (-0.13, 0.25) Allocation Concealment Unclear 0.67 (0.40, 0.93) Yes 0.06 (-0.24, 0.37) 0.14 (-0.17, 0.45) Cochrane 2015; 1: CD005614. Ann Intern Med. 2007;146:580-90. – MCID benefit (-0.37 = 9mm on 100mm pain scale). • BUT many issues, – High quality RCTs (>100 pts, proper randomization, blind outcome assessor): no meaningful effect on pain/function – Publication bias: Negative trials less l kely to be published. 5/6 unpublished studies showed no effect. • Dropouts due to AE, RR 1.33 (1.01, 1.74) • Viscosupplementation (1-3 injections) ~$285-500. 1) Ann Intern Med. 2012; 157:180-91. 2) CMAJ 2005;172:1039-43. 3) JAMA 2003; 290:3115-21 4) Cochrane 2006; 2: CD005321. 5) J Fam Pract 2006; 55:669-75. 6) J Fam Pract 2005; 54: 758-67. 7) J Bone Joint Surg 2004; 86:538-45. G. Michael Allan Steroid Injection (knee) for OA • 6 Systematic Reviews: 5-13 RCTs with 207-648 patients. – Corticosteroid (triamcinolone 20-40mg mostly, then methylprednisolone 40-120mg & others) vs placebo injections. • Pain: Using 100 point Visual analog scale, ~54 baseline,4 Steroids reduced pain more than placebo: – 21-22 points lower at one week,1,2 16.5 points lower at two weeks,3 7.4 points at 3-4 weeks1 • Average ~15 points better between 1-4 weeks4 • Maximal effect may occur at 1.5 weeks4 – At later time points, difference is non-statistically significant1 – Compared to baseline, pain was reduced 29 points at 3 months.5 1. Can Fam Physician. 2004;50:241-8. 2. Cochrane. 2006;2:CD005328. 3. BMJ. 2004;328:869. 4. Eur J Pain. 2007;11:125-38. 5. Ann Intern Med. 2015;162:46-54. 6. J Am Acad Orthop Surg. 2009;17:638-46. Opioids • Sys Rev: 22 RCTs1 (8275 pts) (publication bias) – Pain: SMD 0.28 (0.20-0.35), 0.7/10 – Function: SMD 0.26 (0.17-0.35), 0.6/10, NNT ~10-12 – AE: Oxycodone (e.g.): Any AE: 87% vs 52%, NNH 3 • Withdrawal due to AE: 32% vs 6%, NNH 4 • 18 RCT2, 4856 pts, (12 wks), SMD 0.58 (0.52-0.64) – Opioid sub-groups: Strong 0.69 vs weak 0.52 – Withdrawal rates = 7% Placebo, 19% weak opioids (NNH=9), 31% strong opioids (NNH 5) – Increased withdrawal confirmed by others.3 • 6 RCTs (1057 pts),4 10.5 /100 1. Cochrane 2014; 9: CD003115. 2. OsteoArthritis & Cartilage 2007;15:957-965 3. Schmerz. 2011;25(3):296-3053. 4. European J of Pain 2007; 11:125–138 Platelet Rich Plasma Injections Steroid Injection (knee) for OA • Pain: Reaching pain target or global improvement – 74-78% steroid vs 45-54% placebo:1-3 NNT 3-5, at 1-4 weeks.1-3 – Results at >4weeks inconsistent: 2 no effect,1,2 one reports NNT 5 at 16-24 weeks.3 • Function and stiffness not reliably changed.5 • Sensitivity mostly unclear (e.g. if steroids vary7) but maybe – Worse radiographic severity ≈ reduced effectiveness8 – Higher clinical severity ≈ improve effectiveness8 • Joint infection 1/14,000-77,000 with intra-articular injection9 • Maximum frequency ~4/year.10 – RCT injected steroids 4x/year for two years without any harms. – Cohort of ≥4 injections/year found no harm. 1. Can Fam Physician 2004;50 241-8. 2. Cochrane 2006;(2) CD005328. 3. BMJ 2004;328(7444) 869. 4. Eur J Pain 2007;11 125-38. 5. Ann Intern Med 2015;162 46-54. 6. J Am Acad Orthop Surg 2009;17 638-46. 7. Clin Rheumatol 2014;33 1695-706. 8. Rheumatology 2013;52 1022-32. 9. Am Fam Physician. 2014;90 115-6. 10. TFP Opioids (Tramadol) • Tramadol, Sys rev: 11 RCTs, (1939 pts) – Pain Scale: 8.5 better out of 100. – Pain (% ≥Mod Improve): RR 1.37 (1.22-1.55), 71%% vs 51%, NNT 5 – Adverse Events: minor 20% vs 8%, NNH 9 • Withdrawal due to AE: 28% vs 12%, NNH 7 • Bottom-Line: Opioids work, NNT ~5-10 but it’s similar to NSAID and lots of adverse events (NNH 5-10) Cochrane 2006; 3: CD005522. Miscellaneous 1 • 5 sys revs of 2-6 RCTs (257-609 pts).1-5 Best5: – 50% pain reduction: 43.8% PRP vs 19.3%, NNT 5 – Pain: SMD 0.53 (0.28-0.77) & Function: 1.24 out of 25. • Highest quality RCT (176 pts) in Meta.6 – At 6 months, 14 outcomes, 1 statistically significant: – 50% pain reduction: 38.2% PRP vs 24.1% HA, NNT 8 • New Largest, well designed RCT7 with 192 pts – 33 outcomes (11 outcomes at 2, 6 12 months): No diff. • Bottom-Line: Likely not effective. 1. Arthroscopy. 2013;29:2037-48. 2. Knee Surg Sports Traumatol Arthrosc. 2013 Nov 26. [Epub ahead of print] 3. Arch Phys Med Rehabil. 2014;95:562-75. 4. PM R. 2015;7:637-648. 5. Br J Sports Med. 2015;49:657-72. 6. Arthroscopy. 2012;28:1070-8. 7. Am J Sports Med 2015 43: 1575 • Acupuncture: 16 RCTs (3498 pts), For pain, – Vs Sham: SMD 0.28 (0.11-0.45) ≈ 4.5mm out of 100mm. – Better trials (e.g. good blinding): even less effect • Ultrasound: 5 RCTs (341 pts), For Pain – SMD 0.49 (0.23-0.76) ≈ 12 out of 100 – Unreliable: poor quality RCTs (Mean score 0.8 / 8) • Thermal Therapy: 3 RCTs (179 pts) – Unreliable: poor, small, diff outcomes (?quad strength) Cochrane 2010;1:CD001977. Cochrane 2010;1:CD003132. Cochrane 2003;4:CD004522. G. Michael Allan Miscellaneous 2 • Transcutaneous electrostimulation:18 RCT (813 pts) – Pain SMD 0.86 (0.49-1.23); 2.1 / 10 – Poor quality (1.4/8) & bigger studies, SMD = 0.07 • Electromagnetic Field Therapy: 9 RCTs (636pts) – Pain: 15.1/100 but Function & Quality of Life: No diff • Braces & Orthoses (insole): 13 RCTs (1356 pts) – Knee brace: At 12 months, no effect (more quit with brace due to lack of effect). Shorter, some mixed benefit – Lateral Wedge Insoles: no effect 1. Cochrane 2009; 4: CD002823. 2. Cochrane 2013; 12: CD003523 3. Cochrane 2015;3:CD004020. Miscellaneous Summary • • • • No: acupuncture, joint lavage, braces or insoles Very unlikely: Ultrasound, thermal, TENS Unlikely: Diacerein, ginger. Maybe (?): electromagnetic field therapy. Miscellaneous 3 • Diacerein (10 RCTs, 2210 pts): Natural Health Prod2 – Anthraquinone synthesized, interferes with interleukin- 1, – Pain VAS 8.6mm (1.7-15.6) & Function not sign – Diarrhea = 37.3% vs 10.2% (NNH 4). • Ginger: 5 RCTs (757 patients) on 500-1000/d – Pain SMD 0.30 (0.09-0.50) but allocation concealment: Yes SMD 0.14 vs unclear SMD 0.42 – Withdrawal due to AE: NNH 15 (Mostly bad taste & GI upset) • Joint Lavage: 7 RCTs with 567 patients – Pain SMD 0.11 (-0.21-0.42) = 3mm to 100mm – Function SMD 0.10 (-0.11-0.30) = 2mm to 100mm 1. Osteoarthritis Cartilage. 2015;23:13-21. 2. Cochrane. 2010;5:CD007320. 3. Cochrane 2014;2:CD005117. American Academy of Orthopedic Surgeons CPG Strong recommendations For Moderate Recommendations For Activity. Weight loss (if BMI >25)* NSAIDs & Tramadol Inconclusive Recommendation Electrotherapeutic modalities Manual Therapy Unloader type braces. Acetaminophen, Opioids, Patches • Overall: None, at least yet. Intra-articular corticosteroids Articular growth factor/plasma-rich protein • Two Promising therapies based on single RCTs: Strong Recommendations Against Moderate Recommendations Against – Prednisone 7.5 mg OD x 6 weeks (lasts 6 more weeks) – Methotrexate 10-25mg OD x 12 weeks. J Rheumatol 2014;41;53-59. Ann Rheum Dis. 2014 Mar 27. doi: 10.1136/annrheumdis-2013-204856. Acupuncture. Lateral Wedge Insoles Glucosamine or Chondroitin Needle Lavage Hyaluronic * Insufficient evidence to support: Open Rheumatol J. 2014;8 89-95. Jason Crookham Faculty/Presenter Disclosure Faculty/Presenter: Jason Crookham DO CCFP(SEM) Concussions and what to do when you “bang you head”. Jason Crookham DO CCFP(SEM) Clinical Instructor UBC Relationships with commercial interests: None Potential for conflict(s) of interest: None Disclosure of Commercial Support None Mitigating Potential Bias None 27th Annual Best Science Medicine Course Learning Outcome Objective Slide 1. Describe signs, symptoms and pathophysiology of concussion 2. Be aware of consensus statement and management guidelines for concussion 3. Understand the therapeutic goals of concussion management and limitations of guidelines 4th International Consensus Conference on Concussion in Sport Zurich, Switzerland November 1‐2nd, 2012. TRAUMATIC BRAIN INJURY Glasgow Coma Sca e 5th International Consensus Conference on Concussion in Sport Berlin, Germany October 26‐27th, 2016. “Minimal” Mild ? Sports concussion Mod Severe Jason Crookham DEFINITION INJURY DEFINITION: SPORTS CONCUSSION 1. Concussion may be caused either by a direct blow to the head, face, neck or elsewhere on the body with an ‘‘impulsive’’ force transmitted to the head. 2. Concussion typically results in the rapid onset of short- lived impairment of neurologic function that resolves spontaneously. However in some cases symptoms and signs may evolve over a number of minutes to hours. 3. Concussion may result in neuropathological changes but the acute clinical symptoms largely reflect a functional disturbance rather than a structural injury and as such, no abnormality is seen on standard structural neuroimaging studies. 4. Concussion results in a graded set of clinical symptoms that may or may not involve loss of consciousness. Resolution of the clinical and cognitive symptoms typically follows a sequential course. However it is important to note that in some cases, post-concussive symptoms may be prolonged. “Concussion is a brain injury and is defined as a complex pathophysiological process affecting the brain, induced by biomechanical forces. Several common features that incorporate clinical, pathologic and biomechanical injury constructs that may be utilized in defining the nature of a concussive head injury include…” DETAILED CLINICAL ASSESSMENT OUTLINED IN SCAT3 AND CHILD SCAT3 NOTE Develop d by CAT3 Subcommittee (M verson, Johnston McC GRADUATED RTP PROTOCOL Rehabilitation stage Functional exercise at each stage of rehabilitation Objective of each stage 1 No activity Symptom limited physical and cognitive rest Recovery 2 Light aerobic exercise Walking, swimming or stationary cycling keeping intensity < 70% MPHR No resistance training Increase HR 3 Sport-specific exercise Skating drills in ice hockey, running drills in soccer No head impact activities Add movement 4 Non-contact training drills Progression to more complex training drills e g passing drills in football and ice hockey May start progressive resistance training Exercise, coordination, and cognitive load 5 Full contact practice Following medical clearance participate in normal training activities Restore confidence and assess functional skills by coaching staff 6 Return to play Normal game play • 24 hours per step (therefore about 1 week for full protocol) • If recurrence of symptoms at any stage, return to previous asymptomatic level and resume after further 24 hr period of rest uwisse, McCrory, Dvorak Echemendia, Guskiew Putukian, Raftery, Schneider) SAME DAY RETURN TO PLAY? • Unanimously agreed that no RTP should occur on the day of concussive injury Jason Crookham ON-FIELD OR SIDELINE EVALUATION OF ACUTE CONCUSSION-WHEN A PLAYER SHOWS ANY FEATURES OF A CONCUSSION • The player should be evaluated by a physician or other licensed healthcare provider onsite using standard emergency management principles and particular attention should be given to excluding a cervical spine injury. • The appropriate disposition of the player must be determined by the treating healthcare provider in a timely manner. If no healthcare provider is available the player should be safely removed from practice or play and urgent referral to a physician arranged. • Once the first aid issues are addressed an assessment of the concussive injury should be made using the SCAT3 or other sideline assessment tools. Dilemmas in Concussion Management • • • • On field evaluation In office evaluation Follow-up Late Follow-up • The player should not be left alone following the injury and serial monitoring for deterioration is essential over the initial few hours following injury. • A player with diagnosed concussion should not be allowed to return to play on the day of injury. On Field Evaluation • Witness / injury report • SCAT-3 • Monitor for symptoms • Thinking/Rememberi ng • Physical • Emotional • Physical / mental rest 48 hours In Office Evaluation • Symptom severity • SCAT 3 • Evaluate for symptoms better explanted by alternative causes • Introduce Return to Play guideline MANAGEMENT • CORNERSTONE = initial period of rest until acute symptoms resolve Physical Rest No training, playing, exercise, weights Beware of exertion with activities of daily living Cognitive Rest No television, extensive reading, video games? Caution re: daytime sleep MANAGEMENT • Expect gradual resolution within 7-10 days • Gradual return to school and social activities that does not result in significant exacerbation of symptoms • Proceed through step-wise return to sport / play (RTP) strategy Jason Crookham 2 week follow up 3 month follow up • Symptom evaluation • Consider referral to concussion specialist • Consider multidisciplinary team • Consider specific symptom management • Discuss “significant exacerbation of symptoms” SCAT3 – 4 PAGE LAYOUT 4. Patient Information 2. Scoring 3. Instructions 1. Sideline Assessment Jason Crookham Mike Kolber Faculty/Presenter Disclosure • Faculty/Presenter(s): Michael Kolber • Rela:onships with commercial interests: “Lice Lice Baby” – Pay from University of Alberta and Alberta Health • Research and Speaking Fees Mike Kolber MD, CCFP MSc University of Alberta Department of Family Medicine Winter 2015-‐16 Lice Learning ObjecSves • AWer the session, delegates should be able to: – Understand epidemiology / transmission of lice – Understand how to diagnose lice – Learn why older tradiSonal treatments fail and potenSally more efficacious treatment opSons – Explain reasons for failure of therapy – Non-‐Profit Sources (Alberta College of Family Physicians, Towards OpSmized PracSce) – No funding from industry What is Head Lice? • 6 leg parasiSc insect found on human head • Live louse = ½ size of match head – Nit (egg) = size of sesame seed • AcSve lice, nits: < 5mm from scalp on hair shaW: (survive on blood: close to food source) – Nits >1 cm from scalp = non-‐viable • Most developed countries: < 10 per infestaSon • Lives only on humans: < 48 hours off host • Do not spread diseases Centers for Disease Control and PrevenSon; 2015. www.cdc.gov/parasites/lice/head Lice Epidemiology • Found world wide: irrespecSve of: – Socioeconomic climate,1,2 cleanliness1 – Low SE status à ↑ risk of treatment failure • Common: ~1 million cases / year CAN • Predominantly: Day care, school aged children3 – 5-‐20% of school kids have lice at any Sme4,5 • Girls > boys: longer hair and sharing combs6 1Pediatrics 2015;135;e1355-‐65, 2Emerg Infect Dis 2008;14(9) 1493-‐4. 3Center for Disease Control and PrevenSon 2015 available at www.cdc.gov/parasites/lice/head/treatment.html. Lice Transmission Yes -‐ able to transmit No – Cannot Transmit • Sleeping in same bed • InSmate play • Sharing combs, hats, toques • From your dog / cat • From non-‐inSmate play (they do not fly) • Toilet seat Pillows of infected paSents have live lice 4% of Sme2 Pediatrics 2015;135(5) e1355-‐65. 2Interna2onal Journal of Dermatology 2003, 42, 626–629 Mike Kolber 2 days to mate Lice Symptoms • Many asymptomaSc • Scalp itch Treatment #1 Adult Female Louse – especially behind ears, worse at night – ReacSon to louse saliva in bite (anScoagulant)1 • Scalp impeSgo à think fungal or lice Lay eggs (5-‐10/day) 8-‐9 days 10 days Treatment #2 Eggs Hatch Only mate once (stores sperm) Untreated, cycle repeats every 21 days One lice live span 30 days Pediatrics 2015;135(5) e1355-‐65. Diagnosing Lice Teaching Point #1: Only when see live louse TreaSng Lice: SystemaSc Review • Only 20% with nits à acSve lice1 • Wet combing à superior to visual inspecSon2 – 300 children: 100 had lice (21) or nits (79) – 21 lice: 6 found via inspecSon, 19 w wet combing • Other studies; wet combing 3-‐4 Smes more likely and 2xs as fast to find lice3,4 Teaching Point #2: Use wet combing to diagnose 1Pediatrics 2001;107 1011-‐5, 2Arch Dermatol 2009;145(3) 309-‐13. 3Epidemiol Infect. (2008), 136, 1425. 4Pediatric Dermatology Vol. 18 No. 1 9–12, 2001 Treatment Principles • Treat only those with live lice – Check household contacts /schoolmates when cases • Most treatments: topical and OTC • Pediculicide (kills lice) but not ovicidal (eggs) à repeat in 9 days (when eggs hatch) • AEs: skin and eye irritant • Do not use condiSoner before /aWer treatment (may ↓ treatment effecSveness) Ideal Treatment Product • • • • 1 applicaSon Kills louse + nits No Adverse Effects Minimal cost Mike Kolber Issues with TradiSonal Pediculicides • Resistance: – 98% N. American have genes for resistance to classic pediculicides – Likely why pediculicide studies show ↓ efficacy • Need 2 applicaSons • Neurotoxin = chemical: “I want natural treatment” Lice Treatments CANADA 2016 Class Names Mechanism Applica:on Pros and Cons Cost Combing + Picking Bug Buster LiceMeister Mechanical Removal Q 3-‐4 days x 2 weeks No chemicals Less effecSve $ Permethrin Nix, Kwellada Neurotoxic Leave 10 min rinse off. REPEAT 7-‐10 d Resistance $$ CI ragweed allergy, Approved 2 month old Pyrethrins R&C Neurotoxic Leave 10 min rinse off. REPEAT 7-‐10 d Resistance $$ Approved > 2 years old Silicone DimeScone Nyda 4% Hydrin 92% “suffocates” Leave x 30 min, comb then rinse in 8 hours High efficacy, ovicidal Flammable at high % Silicone-‐ like Isopropyl myristrate (Resultz) Dissolves Exoskeleton 2-‐3 applicaSons 7 days apart Appears beyer than $$ tradiSonal pediculicide Use in ≥ 4 years old $$ J Med Entomol 2014;51 450-‐7. Price Comparisons of Commonly Prescribed PharmaceuScals Alberta 2016 “Bug BusSng” (Wet Combing) Not Available, Too Toxic or Too Costly Product Reasons to not use Lindane AEs (neurotoxicity, marrow suppression, lymphoma) Banned for agriculture, removed US and CAN1 Malathion (Ovide) Not available in CAN, organophosphate pesScide Septra AnSbioSc stewardship, Stevens Johnson Syndrome Pyrethrins + piperonyl butoxide (RID) Not available in CAN IvermecSn (oral) Unavailable in CAN for lice unless Special Access, neurotoxic if use in < 15kg children, pregnant mothers, cost IvermecSn (topical) Cost (200$ / 60 grams), indicated for rosacea Mobile Heat Units Unavailable in CAN, cost 1. 2. 3. 4. Shampoo CondiSoner and comb wet hair (detangle) Lice comb: base of hair shaWs Wipe off comb (lice) at every pass 1Lancet Oncology 2015, doi.org/10.1016/ S1470-‐2045(15)00081-‐9 CFP 2012; 58 840, N Engl J Med 2010;362 896-‐905, CADTH 2010, Clinical Evidence 2010 Pediatrics 2006 118 1963 Bug BusSng vs Pediculicides • • • • RCT BB vs malathion or permethrin: 133 UK kids BB treatment: q 3 days x 12 days, pediculicide once Cure: 52% BB vs 13% (ARD = 39%, NNT = 3) Issues: – Inadequate comparator: pediculicide once – Differing baseline: age, previous infestaSons – DifferenSal FU: day 5 pediculicide vs day 15 BB BMJ 2005; doi:10.1136 Other Bug BusSng Studies RCT 74 UK children (70% ♀) • BB (4xs in 2 weeks) vs malathion (repeated once) • Quality: AC, blinded, PP analysis 7 day cure: BB 38% vs 78% malathion: NNH= 3 • Issues: detecSon based on dry hair inspecSon Conclusion: Bug Bus:ng Less Efficacious than Pediculicide Lancet 2000; 356: 540 Mike Kolber Wet combing added to Pediculicide • 95 US paSents (kids + adults), all treated w 1% permethrin (most repeat @ day 8) • Randomized to adjunct combing (or not) • Day 15 cure: 78% vs 73% combing (NSS) • Issues: lice diagnosis: dry or “wet rinsing” – Some state “need plasSc (not metal) comb” J Pediatr 2002; 141 665 DimeScone Evidence Products Popula:on Outcome No Lice Results NNT DimeScone 4% vs Malathion 0.5% (repeated 1 week)1 73 UK aged 1-‐48) Day 9 AND 14 Dime:cone 70% Malathion 33% 3 DimeScone 92% vs Permethrin 1% (repeated 1 week)2 145 Brazilian children Day 9 Dime:cone 97% Permethrin 68% 4 DimeScone 4% (once) Permethrin 1% (repeated 1 week)3 90 UK children and adults Day 9 Dime:cone 80% Permethrin 36% 3 DimeScone 4% Phenothrin 0.5% (repeated 1 week)4 253 UK peds / adults 66% with lice > 3/12 and 50% > 1 year Day 9 AND 14 DimeScone 70% Phenothrin 75% NSS DimeScone 100% (cohort study)5 58 US children Day 14 Dime:cone 97% NA 1PLoS ONE 2007; 2: e1127, 2BMC Inf Dis 2008; 8:115, 3BMC Derm 2013;13:5, 4BMJ 2005; 330: 1423 5BMC Pediatrics 2015; 15:70 DimeScone (Nyda) Product Monograph • Avoid in pregnant women, ok > 2 years • Leave x 30 minutes, comb, then let dry overnight • Repeat in 8-‐10 days • PotenSally Flammable Results for Resultz (Isopropyl myristate) Products Popula:on Outcome Lice Free Results NNT IPM (1-‐3xs 7 days apart) RID (pyrethrin) 2-‐3xs (43% used IPM 3 Smes)1 60 paSents Florida Day 21 40% IPM 17% RID 5 IPM /cyclomethicone (Full Marks) vs Permethrin 1% Each given twice2 168 UK Day 14 (mostly kids) 82% IPM 19% RID 2 IPM vs Malathion Each given 3 Smes3 216 kids 54% IPM 42% malathion NSS Day 21 Resultz appears superior to pyrethrins / Permethrin G. Pohl-‐Boskamp GmbH & Co. KG. Product Monograph NYDA DimeScone 100 cSt SoluSon, 50% w/w. September 11, 2012 Approach to Treatment Failures 1. RepeaSng treatment < 8-‐10 days: -‐ ie. prior to nits (eggs) hatching) 2. Hair condiSoner use: prevents tx from adhering 3. Pediculicide resistance: -‐ if suspect resistance à try different product 4. Re-‐infestaSon from close contact J Cutaneous Medicine Surgery; 2007; 161, 2Pharma J 2009;280 371–375, Clinical Evidence 2015; 01 1703 3Australasian J of Derm (2010) 51, 175–182 What about the clothes, bed sheets? • Lice can only survive off scalp ~2 days – Only deal with clothes / linens from last 2 days • Wash clothes and linens in hot water and dry hot [or dry clean] • For un-‐washables: plasSc bag for 2 weeks (freeze not necessary) – lice / eggs will die (no food source) Int J Dermatol 2003;42(8) 626, CDC 2015 CDC 2015, J Med Entomol 2014; 51 450-‐7, CFP 2016; 62 (4) 322 Mike Kolber No-‐nit is Non-‐sense • Only 20% eggs à acSve lice • No nits = many days off school for no reason • Should replace no nits with: – “please ensure child treated before coming back” Pediatrics 2001;107(5) 1011-‐5. Lice Summary • 5-‐20% school children have lice • Only treat live lice (diagnosis by wet combing) • Resistance to tradiSonal tx common – Consider: dimeScone, isopropyl myristate • Wash clothes, linens from last 48 hours • Put non-‐washables in plasSc bag x 2 weeks • Tx failures: retreat aWer 9 days, avoid condiSoners, look for re-‐infestaSon, try different product Tina Korownyk Faculty/Presenter Disclosure Male and Female Sexual Dysfunction can we create “Paradise By the Dashboard Light?” • Faculty/Presenter: Tina Korownyk • Relationships with commercial interests: None – Grants/Research Support: – Speakers Bureau/Honoraria: – Consulting Fees: – Other: Tina Korownyk Disclosure of Commercial Support • This program has received financial support from University of Alberta in the form of my salary • This program has received in‐kind support from BS Medicine in the form of travel & accommodation in order to attend this conference. Mitigating Potential Bias • I will not let BS Medicine influence my thinking • Potential for conflict(s) of interest: None 27th Annual Best Science Medicine Course Learning Outcome Objective Slide Be aware of effectiveness of various pharmacologic interventions in male & female sexual dysfunction Increase awareness of possible effects on sexual function of commonly used drugs Can alcohol contribute to poor choices in sex? • Meta‐analysis of 12 observational studies. • Adjusted analysis: – linear relationship: Alcohol & unprotected sex – Each 0.1 blood alcohol level = ~3% increase in unprotected sex. • Bottom‐Line: Country says it best • “I Ain't Never Gone To Bed With An Ugly Man, But I Sure Woke Up With a Few” Addiction. 2012 Jan;107(1):51‐9. Tina Korownyk PDE 5 Inhibitors for Erectile Dysfunction A “Hyposexuality Crisis?” • Variable incidence of “sexual dysfunction” cited – 9‐43%1 – Highest values from papers2 with probable conflicts of interest3,4 • 283 College students assessed how frequently they think about sex6: • The market for a drug that enhances female sexual desire has been to be worth up to $2bn in the U.S.5 (3.2 billion for men by 2019) (Headache, flushing, runny nose) Duration Cost/4 tabs Sildenafil (Viagra) 100mg 30‐60 mins 4‐5 hours $50 Tadalafil (Cialis) 20mg 35‐45 mins 24‐36 hours $80 g Vardenafil (Levitra) 20mg 30‐60 mins 4‐5 hours $75 Vardena il (Staxyn) 10 mg bli l) 30 60 mins 5 hou s $43 http://www.health.harvard.edu/mens‐health/which‐drug‐for‐erectile‐dysfunction Its not the same for females (Sildenafil) Efficacy of PDE 5 Inhibitors for ED NNT = 3‐4 NNH = 5 Onset ) – Males Median 19x/day (Range 1‐388) – Females 10x/day (Range 1‐140) 1) NEJM 2008;359(19) 2005‐2017. 2) JAMA. 1999;281(6) 537‐44) 3) Spinal Cord. 2011;49(2) 273‐9. 4) J Sex Med. 2009;8 2143‐53. 5) BMJ 2010;341:c5701 6) J Sex Res. 2012 49(1) 69‐77. Medication • • • • 2002 RCT1 781pts, FSAD, 4 wk run‐in, PP analysis Pre & postmenopausal women No difference for any end point – (two GEQ, sexual event log, the LSC, and the SFQ) • Main AE were headache, flushing, rhinitis, nausea, visual disturbances, and dyspepsia 1) J Womens Health Gend Based Med. 2002;11(4):367‐77. 1) Eur Urol. 2015 Oct 68(4) 674‐80.2 2) Indian J Endocrinol Metab. 2015 Jul‐Aug 19(4) 451‐61 Success in obtaining FDA approval for Female Sexual Dysfunction 1 – 1994 efforts for sildenafil abandoned – 2004 testosterone patch failed to win approval due to safety concerns. – 2010 flibanserin withdrawn from development Leonore Tiefer, associate clinical professor of psychiatry at New York University School of Medicine and Albert Einstein College of Medicine BMJ 2010;341:c5701 Tina Korownyk Drugs that Affect Female (and male) Sexual Desire? Flirting with Flibanserin • FDA Approved for HSDD Aug 2015 : Previously Rejected 3x – 2 Early RCTS = satisfying sexual events ~0 8/mo, no desire – 2013 RCTs: monthly desire 0 3 out of 6 – Excluded all women taking benzos, sleep aids, narcotics… SSRIs1 – 13%‐76% report sexual dysfunction • Any A/E NNH 6, Dizziness 14, Somnolence 15, Nausea 20, Fatigue 42, Serious A/E 100‐334, Syncope 500 • Risks ?worse with Etoh, CYP3A4 inhibitors (OCPs, fluconazole) Oral Contraceptives2 • 2013 Systematic Review, 36 studies (6 rcts) – At least one death from Etoh poisoning – Etoh interaction study =25 healthy volunteers (23 men), – 22% reported increase in desire – 15% reported decrease in desire – 64% no change • 3 more requested by FDA • Bottom‐Line: 5% change in desire and <1 additional “satisfying” sexual event in 30 days for frequent adverse events. 1) J Psychopharmacol. 2010 Apr 24(4) 489‐96 2) Eur J Contracept Reprod Health Care. 2013 Feb 18(1) 27‐43 Strategies for managing antidepressant induced sexual dysfunction • Cochrane Sys Review, 23 RCTs, 1886 pts1 • 22 added medications, 1 switched • Medications that demonstrated benefit: – Sildenafil (3 rcts) – Tadalafil (1 rct) – Buproprion 150mg bid (3 rcts)2 • Unclear effect – Buproprion150mg qd (2 rcts) – Switching antidepressants • Estimates of effect could be affected by unpublished trials Cochrane Database Syst Rev. 2013 May 31 5:CD003382 2) J Psychopharmacol. 2011 Mar 25(3):370‐8. Do Oral Contraceptives Impact Sexual Function? • 2612 online questionnaires, female medical students ≤ 30 yrs in German, Austria and Switzerland • Using FSFI score 26.55 for “at risk sexual dysfunction”: – – – – 54% using nothing 37% oral hormonal contraceptives 31% non‐oral hormone contraceptives 27% non hormonal contraceptives • No significant difference in scores for EE doses or progestins Arch Gynecol Obstet (2015) 292 883–890 Buproprion for Female Sexual Dysfunction? • 232 women, 29 yrs, HSDD. All failed at least one other tx – Buproprion SR 150mg/d vs placebo x 12 weeks. • Findings: Significant improvement with buproprion – 65.3% buproprion responded ‘Definitely yes’ to Global efficacy question vs 4.3% placebo (p=0.001) – 71.8% in buproprion were definitely satisfied with tx vs 3.7% placebo (p=0.001) • Limits: One “specialty” site in Iran, + exclusion criteria • Comments: Impressive numbers, however definite limitations. Most common A/E was headache. • Improvement in some outcomes supported by other trials2 • Side efffects of buproprion may outweigh benefits. 1) BJU Int. 2010 Feb 11. [Epub ahead of print] 2) (J Clin Psychopharmacol 2004;24:339–342) Systematic Review ‐ RCTs RCTs Graham 1992 Women seeking help for PMS Oranratanaphan 2006 OC vs placebo Placebo Sexual Desire YES Decrease ~15‐20 points VAS over placebo 2 difference OC NO Increase FSFI* 2 different OC NO Increase Increase FSFI from ~29 to 30 Women sterilized COC vs progestin vs placebo YES Decrease Edinburgh consistent in all measures, trend for Manila Sabatini 2006 Women in need of OC 2 different OC, vaginal ring NO Mean not reported** 40% reported decrease in desire with OC, 12% with VR Caruso 2011 159 women seeking OCs 2 different OC NO Improved in newer OC SPEQ 0.5 points Redmond 1999 Re‐analysis of RCT for acne OC vs Placebo YES No effect Not an outcome of the study Strufaldi 2010 Women in 1 yr relationship wanting OC Graham 1995 Eur J Contracept Reprod Health Care. 2013 Feb 18(1):27‐43 Tina Korownyk Change in Sexual Interest Scores for OC and Placebo Is one better than another? A circular argument Depends on where you read: • Vaginal ring better1 • Ultra‐low estrogen (EE < 20μg) reduces sexual desire more than higher estrogen (EE ≥20 μ g)2. • Post hoc analysis3 CHOICE study – Biggest risk: depo‐provera, vaginal ring, implant (~30% lacked interest in sex) – Industry study by makers of OCP, no placebo J Sex Med 2014;11 471–480 2) Eur J Contracept Reprod Health Care. 2013 Feb 18(1) 27‐43 3) Obstet Gynecol. 2016 Mar 127(3) 563‐72. Psychoneuroendocrinology. 1993 18(4):273‐81 What about Side Effects of 5‐ARIs? NNH Decreased Libido 181 ‐ 1673 Erectile Dysfunction 111 ‐ 2003 Ejaculatory Dysfunction 81 ‐ 1673 Composite Cardiac Failure 334 (one trial)* Gynecomastia Case reports Systematic review NNH Bottom Line 822 No strong evidence of one being superior. Industry funded papers each cite their drug has less s/es 1) CMAJ. 1996 Nov 1;155(9):1251‐9. 2) Arch Dermatol. 2010 Oct;146(10):1141‐50. 3) J Am Acad Dermatol 1998;39:578‐89. 4) Review of s/es The Dark Side of 5α‐reductase inhibitors’ therapy: Korean J Urol. 2014 Jun;55(6):367‐79 James McCormack Moisturizers Faculty/Presenter Disclosure JamesMcCormack Norela/onshipswithcommercialinterests James McCormack, BSc (Pharm), PharmD Professor Faculty of Pharmaceutical Sciences, UBC, Vancouver, BC LearningOutcomeObjec1veSlide Tobeabletorecommendanevidence-basedmoisturizer "Preservation of a youthful complexion has been the goal of aging humans for thousands of years" Ann Intern Med 2013;158:781-90 289 ads variety of claims - superiority, scientific, performance, subjective OVERALL Vague 42% Omission 17% False 23% Acceptable 18% J Glob Fas Mark 2015:6:194-206 James McCormack AGE and SUN Most (90%+) changes associated with skin aging are due to photoaging from sun exposure and chronologic aging • • • • • Unregulated terms These terms can mean ANYTHING or NOTHING AT ALL Dermatologist recommended Clinically proven Hypoallergenic Non-comedogenic Alcohol-free 24-hour anything Non-irritating Repairing Detoxifying Contouring Healing Dermatologist tested Dermatologist approved Proven formula Chemical free FDA has no authority to require companies to test cosmetic products for safety most cosmetic marketing claims are unregulated, and companies are rarely, if ever, required to back them up, even for children’s products companies are allowed to leave some chemical ingredients off product labels “Fragrance” may include any number of the industry’s 3,100 stock chemicals FDA does not have the resources or authority for premarket approval of cosmetic product labelling Cosmetic Myths creams designed for different body parts expensive creams hydrating serums age reversing products toners body-firming products sunscreen > 50 SPF facial masks Ingredients essential to all moisturizers April 2012 7 creams studied Garnier, L'Oreal Paris, Lancome Paris, Olay, Aveeno, Neutrogena August 2009 13 products studied Nivea, L'Oreal, Simple Kind to Skin, Olay, Dr Brandt, Logona, Clarins, Clinique, StriVectin, Garnier, Boots, Avon, RoC "After 6 weeks ... no product was even slightly better than the rest, including the control." "Simple moisturiser worked just as well as more expensive creams" 80% WATER 10-30% Oils/lipids/fats (emollients) Decreases Evaporation Typically from plants and animals - PETROLATUM (petroleum jelly), beeswax, lanolin, mineral oil, shea butter, cocoa butter, olive oil, coconut oil, sesame oil, squalene 5% Emulsifiers - Allows Oils to Mix with Water Beeswax/borax, cetearyl alcohol, polysorbate 60, PEG-150 stearate, steareth-20, lecithin, glyceryl monostearate 0.5% Preservatives Parabens, phenoxyethanol, MCI/MI James McCormack Other ingredients 5% Humectants - Attracts Water GLYCEROL (glycerin), propylene glycol, butylene glycol,alpha-hydroxy acids (glycolic acid, lactic acid), urea 1% Silicones DIMETHICONE 2% Herbal extracts - Most Added with No Clinical Evidence They Do Anything and often the reason for allergic reactions 0.2% Fragrance - 100s used Often the reason for allergic reactions MOST IMPORTANT INGREDIENT Sunscreen! INGREDIENTS TOUTED AS "Antiaging/ antiwrinkle” retinoids niacinamide hyaluronic acid alpha hydroxy acids ceramides Tretinoin overall Wrinkles are typically evaluated (looking at just the doses that worked >0.01%) APPLYING TO FACE FOR 6 MONTHS Retin-A Avita Altinac Tretin-X Refissa Renova Stieva-A Airol Atralin People using People using THE ACTUAL CREAM with TRETINOIN CREAM ALONE DIFFERENCE using a 9 point scale "Topical tretinoin [Retin-A and others] is considered the GOLD standard to treat photoaged skin" Journal of Cosmetic Dermatology 2015;14:40-6 Average change from using tretinoin 0.5-1.0 % OF PEOPLE IMPROVED Investigator’s assessment 75% 40% Patient’s assessment 85% 60% Fine wrinkles 65% 35% Coarse wrinkles 45% 25% Uneven skin discolouration 70% 45% 35% 25% 30% 20% 25% % OF PEOPLE HARMED Redness 30% 5% Scaling/dryness 55% 20% Burning/stinging 30% 10% 25% 35% 20% IN 6 MONTHS ADAPTATION OF DATA FROM A COCHRANE REVIEW - NUMBERS ROUNDED OFF Before and after images in adverts Other “active” ingredients PRESCRIPTION tretinoin (Retin-A, Avita, Altinac, Tretin-X, Refissa, Stieva-A, Airol, Atralin) isotretinoin (Isotrex) Less well studied but tazarotene (Tazorac, Avage, Zorac) likely similar to tretinoin adapalene (Differin) NON-PRESCRIPTION - many OTC products retinol ceramide Have less retinol acetate niacinamide effect than retinyl palmitate tretinoin but glycolic acid better tolerated retinaldehyde ‘lactic acid James McCormack BEST EVIDENCE A Randomised Trial Any other type of study has too many limitations/biases Does a cream actually “WORK” for you? 1) Don’t look at any adverts for moisturizers 50 people Preferably they aren’t told which group they are in 2) Start by choosing an inexpensive moisturizer 50 people PLUS an “active ingredient After 3-6 months objectively assess if there is a difference in “wrinkles” between the groups 3) If you actually want an effect on wrinkles chose one that contains ingredients shown in well-designed studies to actually do something 4) Do a patch test - small amount - wait 24 hours and if no reaction then continue to use it for a few weeks ALMOST NO CREAMS HAVE THIS TYPE OF EVIDENCE Does a cream actually “WORK” for you? 5) If it contains an active ingredient use it very sparingly at most once a day for a few weeks 6) If after a few weeks you like the way it makes your skin feel, the texture, the fragrance - USE IT 7) Because even the GOLD standard treatments have such a small effect you will never be able to objectively assess the impact Smiling is the best anti-aging “cream” Try ones like these first Are these the best? - no one knows. But they contain reasonable ingredients. Notice they come in BIG sizes Dee Mangin CFPC CoI Templates: Slide 1 Faculty/Presenter Disclosure Dangerous Caring How good medicines can be bad for your health and how to avoid it Or: There is no “Black Or White” when it comes to drug interactions • Faculty/Presenter: Dee Mangin • Relationships with commercial interests: – No funding gifts or food from drug or diagnostic industries – Consulting Fees: I have occasionally provided expert witness reports for the plaintiff in class action legal cases taken against pharmaceutical companies. Any fees are donated to an independent patient drug side effect information and reporting website RxISK.org Dee Mangin David Braley Nancy Gordon Chair in Family Medicine Learning objectives • Understand the scope and importance of drug interaction issues • Become familiar with some important drug interactions with medicines we prescribe commonly • Be excited by the possibilities of sniffing out drug interactions • Not be confused by any talk of enzymes, substrates, inhibitors and cytochromes The invisible pandemic • Hospitalisation from inappropriate medication use in older adults estimated at 17% • 70 000 admissions a year in Canada due to preventable drug adverse reactions • Adverse drug reactions 4‐6th most common cause of death (US) • Rate goes up sharply with the number of drugs taken Breaking News Prescribing in UTIs – dangerous? • Cotrimoxazole associated with an increased risk of sudden death when combined with ACE inhibitors and angiotensin receptor blockers • The mechanism is thought to be a sudden hyperkalemia • There is also an increased risk when Cotrimoxazole is prescribed with spironolactone, thought to be the same mechanism • A smaller but significant increased risk was also seen with ciprofloxacin in the ACE/ARB study. Mechanism unclear • Effect was not seen with nitrofurantoin or norfloxacin Dangerous Caring This kills more people every year than – Breast cancer – Colon cancer – Lung cancer Dee Mangin ADR Risks in polypharmacy 13% with the use of two medications 58% with five medications 82% with seven or more medications 7 [Patterson 2012] 1000 older adults • Annual healthcare costs of ADR’s $65,631 • $27,365 of this associated with preventable events – that is $27 million for every million older adults in the community • Common reason for medical misadventure claims Reducing patient harms • The “triple whammy” – ACEI + NSAID + diuretic • Do you routinely warn your patients about over the counter NSAIDs? Case One – Sarah, 28y • Presents after a very odd weekend experience — Agitation and restlessness — Sweating, shivering, muscle twitching — Headache, diarrhoea • Previous MVA with severe head injury • On venlafaxine (high dose) and carbamazepine ? What would you ask Sarah? ? What is the provisional diagnosis? Dee Mangin Serotonin Toxicity ‐ Is dose related and may include: Serotonin Toxicity ‐ Is dose related and may include: Neuromuscular effects Autonomic effects Mental status changes Neuromuscular effects Autonomic effects Mental status changes Hyperreflexia Tachycardia Agitation Hyperreflexia Tachycard a Agitation Clonus Hyperthermia Hypomania Clonus Myoclonus Sweating Anxiety Myoclonus Shivering Flushing Confusion Shivering OLDER ADULTS Tremor Mydriasis Tremor Mydriasis Hypertonia/rigidity [M Hunter Serotonin Toxicity Criteria Hypertonia/rigidity Hypomania Anxiety Confusion [ Drugs with potential for serotonin toxicity when used in combination • • SSRIs, SNRIs • • Some TCAs • • Opioids – especially tramadol • • Illicit substances • Rizatriptan, sumatriptan • OTC & complementary – St John’s Wort, cough mixtures Lithium MAOIs Buspirone Isoniazid Isbister 2007 Case Two – Lucy, 21y • Presented 3/7 ago with skin infection, prescribed erythromycin • Now feeling unwell – palpitations, light headed What further information do you need? What might have triggered this? • Erythromycin 400mg, two twice daily • Citalopram 40mg, once daily Drugs associated with QT prolongation Antimicrobials Antidepressants Antipsychotics Antiarrythmics Methadone Dee Mangin [Owens 2006] How is QT interval accurately measured? [adapted from Heist 2005] How often do you do an ECG prior to prescribing a QT prolonging drug? In at risk patients, assess QTc interval before and after starting/adding/increasing a medicine that may affect QT The cardiac action potential [Owens 2006] Drugs withdrawn due to QT prolongation and arrhythmias • Sibutramine (2010) • Cisapride (2000) Vanessas Law • Terfenadine (2010) Dee Mangin We are high prescribers of antidepressants • There is a global increase in antidepressant prescribing • Most developed countries have prevalence rates of antidepressant prescribing of 10% or more • One of the drivers of this growth is long term use Potential for harm: A year in the life of 18 Family Doctors Macrolide scripts per Family Doc Number of patients dispensed a macrolide already on one of the following drug classes SSRI/SNRI/ Mirtazapine TCA‡ SSRI/SNRI/ Mirtazapine + TCA‡ 24 21 8 10 1 18 18 14 16 17 6 22 6 11 15 12 1 5 14 5 3 6 6 5 2 5 5 1 9 1 0 2 2 0 2 5 2 0 0 0 1 1 3 3 1 1 1 0 0 0 0 107 82 30 61 31 194 100 64 139 67 25 162 28 36 69 49 14 Ted’s details Case 3 – Ted, 55y • Increasing general weakness over past 2 weeks • Initially had numbness in his hands and difficulty getting dressed • Fatigued ‐ was unable to walk further than next room • Increasing unsteadiness and fallen once What other information would you want? • Long term conditions: – Hypertension, hyperlipidaemia, asthma • Medications: – – – – – Cilazapril 5mg/day ‐ Bendrofluazide 5mg/day Diltiazem CD 120mg/day ‐ Aspirin 100mg/day Simvastatin 40mg/day Fluticasone/salmeterol and salbutamol inhalers Erythromycin (2 weeks prior) for chest infection • Physical exam: – increasing weakness and numbness – no specific muscle tenderness Statin‐induced myopathy • Uncommon with statins alone – myalgia 2‐11% – myositits 0.5% – rhabdomyolysis < 0.1% • Dose‐dependent adverse event • BUT Increased risk if co‐prescribed with drugs that: – are myotoxic (e.g. fibrates, colchicine) – increase simvastatin plasma levels (e g. CYP3A4 inhibitors, diltiazem) • Simvastatin (and atorvastatin) more likely to be affected by CYP3A4 inhibitors than pravastatin or rosuvastatin Simvastatin‐induced myopathy Avoid simvastatin with moderate/strong CYP3A4 inhibitors: (Refer to NZ Formulary or Medsafe Data Sheet for a full list) – Macrolide antibiotics ‐ erythromycin, clarithromycin – Grapefruit – Azole antifungals ‐ itraconazole, fluconazole, ketoconazole, posaconazole, voriconazole – Ciclosporin – Protease inhibitors (HIV and Hep C antivirals) ‐ e.g. ritonavir Reduce simvastatin dose with weak CYP3A4 inhibitors: – Verapamil, diltiazem, amiodarone – Monitor for muscle toxicity Dee Mangin What should you do in all 3 cases? • Place a patient alert in Medication module How could Ted have been managed better? • Report to Health Canada (patient can do this via www.rxisk.org which will populate a report form and also has a free interaction checker patients can use): – If serious, unexpected, concerning, new medicine – If in doubt, report it! Consider query builders to look for at‐risk patients Careful Combinations There are some uncommon (but potentially life‐threatening) disorders that can occur with combinations of medicines we prescribe freely: Take home messages (1) Some uncommon (but life‐threatening) disorders can occur with certain common medicine combinations • Serotonin toxicity – High dose or combination serotonergic agents • Serotonin toxicity – High dose or combination serotonergic agents • QT prolongation – Usually dose related, many medicines associated – Some patient factors may increase risk • Myopathy/rhabdomyolysis with statin use – Dose‐dependent – usually due to combination with medicines that inhibit statin metabolism Take home messages (2) • The risks of polypharmacy can outweigh the benefits of individual medicines • A complete and current list of medications is important • Patients may be taking other medicines • From other prescribers • Purchased Over The Counter • Obtained for recreational use • Make patients aware of risks of interactions and document discussions – engage them in checking for interactions / checking side effects / adverse event reporting • QT prolongation – Usually dose related, patient factors may increase risk – Consider ECG in at risk patients • Myopathy/rhabdomyolysis with statin use – Dose‐dependent: usually due to combination with medicines that inhibit statin metabolism – Do not use potent CYP3A4 inhibitors with simvastatin (e g. erythromycin, itraconazole, grapefruit) G. Michael Allan COPD Treatments: “All I need is the Air that I Breathe” G. Michael Allan Professor, Department of Family Med, U of A Director Evidence & CPD Program, ACFP Faculty/Presenter Disclosure • Faculty/Presenter: G Michael Allan • Relationships with commercial interests: – – – – Grants/Research Support None Speakers Bureau/Honoraria None Consulting Fees None Other None 27th Annual Best Science Medicine Course Learning Outcome Objective Slide Mitigating Potential Bias • N/A We will review and learn about COPD treatment • Refer to “Quick Tips” document. 1. Inhaled Medications (outcomes include Exacerbations, hospitalization and mortality) • Short-Acting Bronchodilators, Long-Acting Beta-Agonists, Long Acting Anticholinergic, Inhaled Corticosteroids, Combinations 2. Oral Medications and other interventions • Theophylline, Corticosteroid, Oxygen, Vaccinations, Exacerbations Therapy: Specific Outcomes After smoking cessation • There are many choices of Outcomes • Focus on Patient Orient Evidence that Matters – In order: FEV1, St George’s Respiratory Questionnaire (SGRQ), Exacerbations (Hospitalizations) & Mortality (Only intervention to slow ↓ lung function FEV1 loss from 60ml /year to 30ml ) • RCT’s that found effect treat mostly – Symptomatic AND FEV1<60% – 2011 ACP may consider with 60-80 + Sx • If mild, start with short acting puffers. 1.. JAMA 2003 290: 2301-2312. Ann Intern Med. 2007;147:639-653. Ann Intern Med 2011;155:179-191. G. Michael Allan The More the Scarier Drug Device Single Agents Class Dose & Delivery (1 month) Cost Agent FEV1 ml SGRQ Mean SGRQ Exacerbation Death NNT NNT Serious AE Formoterol (Foradil) Aerolizer LABA BID 12μg $70 (Y) Indacaterol 149 3.6 9 30 ns ns Formoterol (Oxeze) Turbuhaler LABA BID 6-12μg $65 (Y) Formoterol 45 2.66 4 ns ns Withdrawal (NNT 19) Salmeterol (Servent) Diskus LABA BID 50μg $78 (Y) Salmeterol 101 1.64 15 22 ns Withdrawal (NNT 15) Indacaterol (Onbrez) Breezhaler LABA OD 75μg $69 (Y) Aclidinium 90 2.3 11 ns ns Withdrawal (29‐77)* Aclidinium (Tudorza) Genuair LAMA BID 400μg $75 (Y) Glycopyrronium Glycopyrronium (Seebri) Breezhaler LAMA OD 50μg $75 (Y) Umeclidinium Tiotropium (Spiriva) LAMA OD 18μg $89 (Y) Handihaler Tiotropium (Respimat) Soft Mist LAMA OD 5μg $89 (N) Umeclidinium (Incruse) Ellipta LAMA OD 62 5μg $65 ? Respiratory Research 2013, 14:49. The Lung Association & Lung Association Ontario http://www.on.lung ca/document doc?id=2231 Tony Nickonchukhttps://www.lung ca/lung-health/lung-disease/copd/medication Hospitalization • LABA2 – TORCH= 32 (may be exaggerated) • Same for LABA + steroid • Tiotropium3,4 – NNT= 25 or 30 • ICS – only one study & ns 1. NEJM. 2007;356:775-89 3. JG M 2006; 21: 1011-9. 4. Cochrane 2005, 2: CD002876. Mortality • LABA+Steroid1 vs – Placebo NNT 56 – Steroid NNT 44 • Tiotropium: Not significant1 OR – Per protocol analysis NNT=53 (for 4 yrs)4 1. Ann Intern Med. 2007;147:639-653. 2. JGIM 2006; 21: 1011-9. 3. NEJM. 2007;356:775-89. 4. NEJM. 2008;359:1543-54. Tiotropium & Mortality 3.32 10 14 ns Less with drug 4.7‐7.9 ns ns ns ns Tiotropium 119 2.89 10 16 ns** Inhaled Steroids 70 1.22 n.a. 22 ns Withdrawal (NNT 14) Many*** * Aclidinium causes Diarrhea NNH 91 ** Mortality: Handihaler OR 0.92 (0.80‐1.05) vs Respimat OR 1.47 (1.04‐2.08), NNH 143 *** Inhaled Steroids Oral Candidiasis (NNH 27), Voice change (NNH 34), Bruising (NNH 32), Pneumonia (NNH 30) Adverse events: Inhaled Steroids • Fracture – One RCT showed decreased bone density1 – Meta of RCTs: ~NNH 83-172 over 3 yrs.2 • Pneumonia – From TORCH: 18.9% vs 12.8% = 6.1% (NNH 17)3 – >4 Meta-analysis find similar (NNH 13-25)4-8 • 47 for Severe pneumonia (1 yr)3 – Date not perfect (many no x-ray, budesonide less, etc) • Bottom-Line: Over 3 years, both fracture (NNH ~100) & pneumonia (NNH ~30) more common 1) NEJM 2000;343:1902-9. 2) Thorax 2011;66:699-708. 3) NEJM. 2007;356:775-89 4) JAMA. 2008;300:2407-16. 5) Arch Intern Med. 2009;169: 219- 29. 6) Cochrane 2007;4:CD003794. 7) Cochrane 2014;3: CD010115. 8) Lancet 2009; 374: 712–19 So, which puffer first • Tiotropium vs LABA: 2 publications • Sys Rev: 22 RCTs (23,309), Mortality: – Handihaler OR 0.92 (0.80-1.05), 4.9% vs 6.1% – Respimat: OR 1.47 (1.04-2.08), 2.4% vs 1.7%, NNH 143 • Other Respimat vs Handihaler (Sys Rev) 112 90‐140 mortality2 – Handihaler (UPLIFT, meta, cohorts): ≤ death – Respimat (Cohort & meta): Increased mortality (dose effect) – TIOSPIR (2 3 yrs, 17,135): respimat=handihaler; but healthy pop • Bottom-Line: Avoid tiotropium in respimat or soft mist inhaler. Use of Tiotropium in handihaler (classic “spiriva” inhaler) encouraged. Cochrane Database Syst Rev. 2014;7:CD009285. 2) Pulm Pharmacol Ther. 2014;;28 91-7 – 7384 x1 yr, tiotropium 18ug vs salmeterol 50ug BID1 • Patients with ≥1 exacerbations: 34% vs 39%, NNT 19 – 1207 pts, ½ yr: tiotropium>placebo but salmeterol not2 • LABA/steroid (50/500 BID) vs tiotropium3: 1323 x 2 yrs – Very high drop-out (39%) but No diff exacerbations or quality of life3 • LABA vs Steroid: Review (7 RCTs, 5997 pts)5 – No difference except Steroids more pneumonia & poss ble increased mortality (OR 1.17; 0.97 to 1.42) • Bottom-line: Tiotropium likely best first long-acting puffer but LABA like salmeterol, not far behind 1) NEJM 2011; 364:1093-103. 2) Thorax 2003;58:399-404. 3) Am J Respir Crit Care Med. 2008;177:19-26. 4) Cochrane 2010;5:CD007891. 5) Cochrane 2011;12: CD007033. 6) Ann Intern Med. 2011;155:179-191. G. Michael Allan Combo puffers (1+1≈1.1) Vaccinations • Guidelines Support use of Influenza yearly and Pneumococcal q 5-10 yrs.1 Influenza2: • Less Exacerbations & Flu • Pneumococcal4: No proven benefit (Exacerbation, pneumonia, hospitalization or mortality) in COPD 1. Can Respir J. 2003 May-Jun;10 Suppl A:11A-65A Can Respir J 2008; 15(Suppl A) 1A - 8A. 2. Cochrane 2006; 1: CD002733 3. Cochrane 2006;(4):CD001390. Dual Agents Agent FEV1 ml SGRQ Mean Serious AE 90‐160 2.9‐4.1 ? 22 53 Pneumonia NNH~70 ICS/LABA vs ICS 50‐110 0.3‐2.8 ? ns 75 none ? 23 ns Pneumonia NNH~48 70 High withdrawal and very inconsistent results ICS/LABA vs Tio Tio/LABA vs either 1.58 70 60‐110 Umeclidinium/ Vilanterol (vs either) 1.61 ? ns ns ns ? 16-∞ ~42 ns Withdrawal NNT~19 19-25 ns ns Rate down ~0.14-0.26 ? **Pneumonia, local effects, fractures up Glycopyrronium/ Indacaterol v Tio* 60‐100 2.22.6 ~12 Fluticasone + Vilanterol vs Vil 10‐20 ? ? * Vs Tiotropium or Glycopyrronium ** Increased numbers of Pneumonia, local effects (e.g. thrush) & fractures Adding Fluticasone/Salmeterol to Tiotropium • 6 RCTs, 1268 patients, Follow-up 35 weeks – – – – Device Class Dose Cost Salmeterol+fluticasone (Advair) Diskus LABA + ICS B D 50+ 100, 250, 500μg $108-127 (Y) Salmeterol+fluticasone (Advair) MDI LABA + ICS B D 25+ 125, 250μg $63-87 (Y) Formoterol+budesonide (Symbicort) Turbuhaler LABA + ICS OD or B D 5 + 100, 200μg $55 (Y) Formoterol+Mometasone (Zenhale) Breezhaler LABA+ ICS B D 5 + 50, 100, $58-69 200μg (N) Vilanterol+Fluticasone (Breo) Ellipta LABA +ICS OD 25 + 100μg Vilanterol+Umeclidinium (Anoro) Ellipta LABA + LAMA OD 25 + 62.5μg $107 (SA) Indacaterol+Glycopyrronium (Ultibro) Breezhaler LABA + LAMA OD 110 + 50μg $153 (SA) $107 (SA) Respiratory Research 2013, 14:49. The Lung Association & Lung Association Ontario http://www.on.lung.ca/document.doc?id=2231 https://www.lung.ca/lung-health/lung-disease/copd/medication Treating AECOPD (“Lung Attack”) SGRQ Exacerbation Death NNT NNT ICS/LABA vs Plac ICS/LABA vs LABA Drug Exacerbation: OR 0.73; (0.55-0.96); 31% vs 37%, NNT 18 SGRQ: 4.63 (4.26-5.01); No # provided for ≥4. Any Adverse Events: OR 1.24 (0.98-1.57), 39% vs 34%, Serious AE: OR 0.95 (0.58-1.52). • Oral Steroids1: – Treatment Failure (return to care) NNT = 9 – Dose ranges from 30-60mg prednisone, 4-14 days. • Antibiotics2 – Mortality reduction = NNT 8 – Treatment Failure (return to Care) NNT 3 • Abx choice really doesn’t matter 2,3 – In Uncomplicated: 1st Line: Amoxicillin, doxycycline, Sulpha, 2nd or 3rd generation cephalosporins, extended spectrum macrolides. – In complicated: Beta-lactam/beta-lactamase inh bitor, fluoroquinolone 1. Cocrhane 2005; 1: CD001288. 2. Cochrane 2006; 2: CD004403. 3 Can Respir J. 2003 10 Suppl A:11A-65A Daily antibiotics or Rolfumilast • Daily Antibiotic:1 1142 severe, zithro 250mg OD vs placebo • ≥1 exacerbation: 57% vs 68%, NNT 10 • SGRQ: ≥4 was 43% vs 36%, NNT 15 • 5% hearing & macrolide res (81% vs 41%) nasopharyngeal – Erythromycin 250mg BID found similar – 1157 Moxifloxacin (as 5 days q8 weeks): less effective • Roflumilast: Meta2 (9 RCTs, 9211 pts) + severe RCT3 (1935) • Bottom-Line: Adding dual therapy to Tiotropium will improve COPD quality of life to small level. For 18 people over ¾ of year, one will avoid an exacerbation. European J Internal Med 2014; 25: 491–495 – ≥1 COPD exacerbations : 20.8% vs 24.1%, NNT 31 – Harms: Weight loss (NNH 15 & Weight loss ~2kg x0.5-1 yr), Diarrhea (NNH 17), Nausea (NNH 34), Headache (NNH 50) – Severe: ≥1 Exacerbation 39.2% vs 44.7%, NNT 18 • ≥1 exacerbation hospitalization, 15.5% vs 19.7%, NNT 24 Tools for Practice #62, Feb 21, 2012. 2) Cochrane Database Syst Rev. 2011;(5):CD002309. 3) Lancet 2015; 385: 857–66 G. Michael Allan Adjunct Measures • Pulmonary Rehab: (if Sx & FEV1<50%) – Better SGRQ (6.9) & exercise (walks +44m in 6 min)3 – Hospitalization & mortality trend better but not stat sign.1 • Oxygen: RCTs3 used FEV1 <30% & PaO2 ≤55mmHg – O2 reduced death (RR 0.61, 0.46-0.82), NNT ~18 x 3 yrs – TOP4 & Can5: if Sx severe or FEV1<40%, do PaO2 – If PaO2 is ≤55mmHg, then Supplemental Oxygen • Give 15 or more hr/d to keep PaO2 >60 mm Hg (or sat ≥ 90%)3,5 1) Cochrane Database Syst Rev. 2015;2:CD003793. 2) Ann Intern Med 2007;147:633-8 & 639-53 3) Ann Intern Med. 2007;147: 633-38, & 639-53. 4) TOP COPD CPG. 5) Can Respir J 2008; 15(Suppl A): 1A-8A. Adjunctive Treatments • Theophylline1: Very few POEM outcomes – Exercise tolerance: No diff – Exacerbations: No diff • Oral Steroids (in Chronic)2: No POEM evidence. • Nutritional supplementation3: No evidence to support • Methylxanthines in AECOPD4: No Help 1. Cochrane 2002; 3: CD003902. 2. Cochrane 2005; 3: CD005374. 3. Cochrane 2005; 2:CD000998 4. BMJ. 2003;327:643-8. Peter Loewen Antidotes for Anticoagulants “Take The Money And Run”? No conflicts of interest. Dr. Peter Loewen B.Sc.(Pharm), ACPR, Pharm.D., FCSHP, RPh University of British Columbia Vancouver General Hospital peter.loewen@ubc.ca Major Bleeding in AF Trials Objectives % per year 5.0 After the session and upon reflection, participants will be able to: 1.Describe to their patients the probability and implication of major bleeding with OAC therapy. 2.Appropriately discuss the relevance of antidotes to OAC therapy with their patients. NS NNT 147 x 1y NS NNT 308 x 1h NNT 105 x 1y 2.5 0.0 RE-LY warfarin NOAC hi dose NOAC low dose ROCKET-AF ARISTOTLE NNT 56 x 1y ENGAGE AF RE-LY, ROCKET-AF, ARISTOTLE, ENGAGE AF ICH in AF Trials % per year 5.0 First 30 days of warfarin: “major hemorrhage” 11.8% per person-year 16.7% if CHADS2 > 3 warfarin NOAC hi dose NOAC low dose 2.5 0.0 Over the 5-year study period: 8.7% visited the hospital for bleeding HR 0.40 NNH 500 HR 0.31 x 1y NNH 500 x 1y RE-LY HR 0.67 NNH 500 x 1y ROCKET-AF HR 0.42 NNT 213 x 1y ARISTOTLE HR 0.48 NNT 218 HR 0.3 x 1y NNT 170 x 1y 18% of those died in hospital or within 7 days of discharge ENGAGE AF RE-LY, ROCKET-AF, ARISTOTLE, ENGAGE AF Gomes T, et al. CMAJ. 2013;185(2):E121–7 Peter Loewen Major Bleeding Case-Fatality Major Bleeding Case-Fatality Extracranial Bleeding Intracranial Bleeding warfarin 11-20%2 ~50%3 rivaroxaban 5-10%2 dabigatran ~9%1 apixaban ? 13 RCTs (n=27,419 treated 6-36 mos, 1121 major bleed in 1034 individuals) AF & VTE, all NOACs Case fatality for major bleeding: 1. Majeed A, et al. Circulation 2013;128:2325–32 2. Beyer-Westendorf J, et al. Blood [Internet] 2014;124:955–62 3. Fang MC, et al. Am J Med 2007;120:700–5 NOAC: 7.6% warfarin: 11% RR 0.53 (0.43-0.64) Chai-Adisaksopha C, et al. J Thromb Haemost 2015;13:2012–20 Managing OAC-associated bleeding site-specific therapy endoscopy, neurosurgery, etc volume, cryosupernatant plasma CPD (CSP), FFP, prothrombin complex concentrates (PCC), antidote Holbrook A, CHEST 2012;141:e152S–84S. Fawole A, et al. Cleve Clin J Med 2013;80:443–51. HOW DOES Vit.K AFFECT OUTCOMES IN WARFARIN-ASSOCIATED MAJOR BLEEDS? Johansen M, et al. Cochrane Database Syst Rev 2015;7:CD010555. Peter Loewen “Serious bleeding, although rare, can occur in your brain or in your gut. If this happens the doctor can give you an antidote that reverses the anticoagulation and gets the blood back to normal.” Palacio AM, et al. Patient Prefer Adherence 2015;9:133–8. WHAT WOULD AN IDEAL ANTIDOTE DO? “… if a severe bleeding event does occur, the antidote can be used to reduce the duration and severity of the bleeding event.” Ghijben P, et al. Pharmacoeconomics 2014;32:1115–27. www.praxbind.com Pollack CV Jr., et al. N Engl J Med 2015;373:511–20. www.clinicaltrials.gov NCT02104947 Peter Loewen www.clinicaltrials.gov NCT02329327 Siegal DM, et al. N Engl J Med 2015;373:2413–24. Managing OAC-associated bleeding site-specific therapy endoscopy, neurosurgery, etc Restart OAC? When? volume, cryosupernatant plasma CPD (CSP), FFP, prothrombin complex concentrates (PCC), antidote Restart OAC? When? Witt DM, et al. Arch Intern Med. 2012;172(19):1484–91. Restart OAC? When? Restart OAC? When? “restarting warfarin after 7 days was not associated with increased risk of GIB but was associated with decreased risk of mortality and thromboembolism compared with resuming after 30 days of interruption.” Qureshi W, et al. Am J Cardiol. 2013;113(4):662–8. n=4602 AF patients discharged from hospital following antithromboticassociated GI bleed. 5 years followup. HR for restarting antithrombotic treatment vs. not restarting Staerk L, et al. BMJ 2015;16;351:h5876. Peter Loewen Restart OAC? When? Restart OAC? When? Claassen DO, et al. Arch Neurol. 2008;65(10):1313–8. Restart OAC? When? Kuramatsu JB, et al. JAMA 2015;313:824–36. Restart OAC? When? Kuramatsu JB, et al. JAMA 2015;313:824–36. HAS-BLED Kuramatsu JB, et al. JAMA 2015;313:824–36. HAS-BLED performance based on LRs strong moderate 0.43 weak 00.81 moderate 1 1.14 2 2.12 3 3.73 3.36 1.6 4 5 >=2 vs <2 3.34 0.1 Pisters et al. CHEST 2010; 138(5):1093–1100 0.2 strong 1 LR+ >=4 vs. <4 5 10 Loewen P, Dahri K. Ann Hematol. 2011;90:1191–200. Peter Loewen Bleeding CPRs - C statistics clinically useless How to HAS-BLED limited modest clinically value value useful OBRI Kuijer Shireman HEMMOR2HAGES RIETE HAS-BLED ATRIA Clinician judgement 0.5 0.6 0.7 0.8 Ohman et al. JAMA 2000;284:876-8 Donzé J et al. Am J Med 2012;125:1095–102 How to HAS-BLED www.acc.org/anticoagevaluator www.sparctool.com Kam Shojania PMR – Polymyalgia Rheumatica Faculty/Presenter Disclosure • • Faculty: Kam Shojania Polymyalgia Rheumatica • Relationships with commercial interests: – – – – – Grants/Research Support: Indirectly, via faculty: Janssen, BMS, Abbvie, Pfizer, Roche, UCB, Amgen. Speakers Bureau/Honoraria: Two industry talks last year. Consulting Fees: Two times in the past year Other: UBC salary, Ministry of Health contract for IVIG management. Arthritis Research Centre, CHEOS, Arthritis Society Investments relevant to this talk: None Kam Shojania, MD, FRCPC Chief, UBC Division of Rheumatology Disclosure of Commercial Support • This program has received financial support from Nobody in the form of Nothing. • This program has received in‐kind support from Nothing in the form of Nobody. • Potential for conflict(s) of interest: • • • Mitigating Potential Bias • I won’t be talking about biologics for PMR because they are off label. In particular, I won’t be discussing Tocilizumab because we very rarely would consider it for PMR. Off label. Don’t do it. None really. Nobody can make money on PMR. Oh wait! There might be a biologic useful for PMR called tocilizumab (made by Roche). Stay tuned for lot’s of ‘CME’ . 27th Annual Best Science Medicine Course Learning Outcome Objective Slide 1. Don’t use high dose prednisone for PMR. Max 20mg daily. Try 15mg daily for most patients 2. About 10% of PMR may have a normal ESR or CRP. If one is normal, check the other. Consider repeating in a week or two if both normal. 3. Would be rare to have PMR under 60 yo. 3. Infection and malignancy can mimic PMR 4. Fibromyalgia can mimic PMR (what is fibromyalgia? Ask James) 5. All patients will get steroid side effects so consider MTX as a steroid‐sparing agent in PMR. Case 1 • 75 yo man with 1 week of proximal muscle pain and stiffness in the AM. Very fatigued. No features of GCA. • On exam mild tachycardia, reduced shoulder and hip ROM. • Anemic. WBC 13, elevated neutrophils, CRP 160. • What is the DDx? Kam Shojania Case 1 continued • Infection, PMR, vasculitis, malignancy. • Infection! • If you treat with prednisone you would likely kill him. Case 2 • 59 yo woman with 12 weeks of proximal muscle pain and stiffness in the AM. Very fatigued. Wt gain of 15 lbs. Depressive symptoms. • On exam tired‐looking and no obvious findings. No joint pain. • Anemic. WBC 8, CRP 12. • What is the DDx? Case 2 • Hypothyroid • Fibromyalgia • Depression • Prednisone 50mg daily would help her quite a bit at the beginning and the CRP would normalize. What is PMR? • Proximal myalgia of the hip and shoulder girdles associated with morning stiffness (at least 1 hour) • Etiology is largely unknown • Associated with HLA‐DR4 • Some series show higher prevalence of antibodies to Adenovirus and RSV Epidemiology • Elderly patients, >50 years of age (mostly >60) – Incidence 52.5/100000 – Prevalence 0.5‐0.7% • • • • Females 2:1 White, European (highest rates in Northern Europe) Some evidence of genetic susceptibility 50% Temporal arteritis patients will have PMR (15% of PMR patients will develop TA) Clinical Picture Often previously healthy, >50 Bilateral proximal muscle pain and stiffness ESR >40, CRP elevation Prompt response to steroids Low grade fevers, weight loss Malaise, fatigue, depression Difficulty getting out of bed, rising from sitting, performing ADLs • Rarely can have high spiking fevers • • • • • • • Kam Shojania Exam findings • Low grade temp • Muscle strength is NORMAL • Pain specifically in shoulder and hip girdle despite lack of clinically significant swelling • Tenderness to palpation and diminished ROM in shoulders and hips • Can get a transient synovitis (usually knee, wrist, sternoclavicular joints) Treatment • Rule out infectious/autoimmune process – – – – – • Low dose prednisone (10‐15mg/d) for 2‐4 weeks. Then can start trying to taper. • Vitamin D/Calcium • Steroid sparing agents (MTX usually) Few points about steroid therapy • Starting >10mg fewer relapses, shorter treatment periods than compared to <10mg • Starting >15mg lead to higher cumulative doses and more steroid adverse affects • Tapering lead to more successful treatment, fewer relapses, when done slowly (1mg/mo) Endocarditis RA Lupus Systemic Infection Myositis Prognosis ‐ good • But prednisone is the big problem • Self limited and most resolve within 1‐3 years, however patients experience significant decrease in quality of life • 50% of patients can often be weaned off all steroids by 2 years – If relapse, often occurs within 12 months of weaning steroids • Need to be monitored for GCA Other differentials to consider • • • • • • • Amyloidosis (inflammatory) Fibromyalgia Osteoarthritis Shoulder disorders – bilat rotator cuff Cervical spondylosis Parkinson’s Disease Multiple Myeloma Tests to order • • • • • ESR (typically >40, sometimes >100), CRP ANA, RF, Blood cultures CBC CK NORMAL! No imaging necessary but Xrays should not show erosive disease or osteopenia. – MRI if done will often show bursitis. • TA biopsy only done if you suspect TA Kam Shojania ESR vs CRP? – choose the CRP ESR CRP Watch blood separate in a tube mm/hr Increases with age and anemia, females, renal disease. Cheap Acute phase reactant made by liver. More specific. More sensitive to change. Previously more expensive and now cheaper. We often see inappropriate treatment of PMR: • Prednisone 50mg daily! • Rapid taper and re‐initiation of prednisone: Yo‐yo • Steroid withdrawal symptoms mimic PMR flare. Also responds to steroids. Taper long and slow. • Rheumatoid arthritis can start out as looking like PMR initially. And often RF, CCP negative in elderly onset RA. If symptoms more to hands/wrists/feet, then reconsider RA as the diagnosis and consider DMARD. Some tips to make you look good (or at least not bad) Make sure you look for PMR mimics right away. Missing infection and malignancy would not be good. Review all prednisone S/E verbally and in writing and chart it. Do not use NSAIDs Temporal Arteritis • • • • • • • • Visual loss, Headache Scalp tenderness Jaw claudication CVA Aortic arch syndrome Thoracic aorta aneurysm Dissection A few rules for PMR • Start with prednisone 15mg daily (not 50mg). • Taper to 10mg within 4‐8 weeks then by 1mg/month • A good response to prednisone (90% better in 48h) is a good diagnostic test. • Watch for GCA symptoms. • Follow up every month at least during the 1st year. Perhaps every 2 months in the 2nd year. • Recommend low dose MTX at 10‐15mg PO weekly • Exercise, fall‐prevention, osteoporosis management including bisphosphonates Kam Shojania Medical co‐morbidities! • Hypertension • Diabetes • Osteoporosis • Obesity • Cardiovascular risks • Sleep apnea When to refer? • Atypical presentation such as less than 60yo or not responsive to steroids • Co‐morbidities that make prednisone worrisome. • Inflammatory arthritis • Very high inflammatory markers • Features of GCA • Early MTX use will reduce prednisone requirements. 27th Annual Best Science Medicine Course Learning Outcome Objective Slide 1. Don’t use high dose prednisone for PMR. Max 20mg daily. Try 15mg daily for most patients 2. About 10% of PMR may have a normal ESR or CRP. If one is normal, check the other. Consider repeating in a week or two if both normal. 3. Would be rare to have PMR under 60 yo. 3. Infection and malignancy can mimic PMR 4. Fibromyalgia can mimic PMR (what is fibromyalgia? Ask James) 5. All patients will get steroid side effects so consider MTX as a steroid‐sparing agent in PMR. Bringing Best Evidence to Clinicians: Combining Evidence and Clinical Pharmacology to Improve Drug Therapy Mark the date: Friday, 29 October 2016 Where: Surrey Memorial Hospital, 13750 96 Ave, Surrey BC What: Bringing Best Evidence to Clinicians: Combining Evidence and Clinical Pharmacology to Improve Drug Therapy Overview This popular conference put on every year by the UBC Therapeutics Initiative in collaboration with UBC Continuing Professional Development is designed to provide physicians, pharmacists, and other health professionals with up-to-date, evidence-based, practical information on prescription drug therapy. Although primarily aimed at prescribers (MD’s, NP’s) and pharmacists, this course will appeal to any health professional who wants to learn and think about the scientific evidence behind what we should or should not be doing with prescription drugs. CCCEP and Mainpro M1/MOC Section 1 credits will be available. Note that this conference is not supported by industry funding. Comments from last year: “Excellent, thought-provoking, evidence-based content.“ “Unbiased speakers who strongly believe in practicing evidence-based medicine.“ “Promotes critical thinking and provides powerful messages that will stick with me.“ “Probing questions make you examine your beliefs and how you practice.“ “Always an excellent course.“ Speakers & Topics What is the Evidence For or Against Using Opioids for Chronic Pain? Dr. Jason Busse, National Pain Centre, McMaster University; Chair, Canadian Opioid Guideline Update; Author of forthcoming systematic review on opioids for chronic pain. Hamilton, ON Dogma vs. Evidence in Management of Atrial Fibrillation, and Treatments to Prevent Atherosclerotic Events Dr. John Mandrola, Cardiac electrophysiologist, endurance athlete, and chief cardiology correspondent for Medscape. Louisville, KY Is Evidence Available to Guide Palliative Care? Dr. Staci Mandrola, Internist, hospice/palliative care physician, and cyclist. Louisville, KY Guidelines we can trust? Understanding pitfalls, limitations, and conflict of interest in clinical guidelines Sarah Burgess, PharmD, Dalhousie University What do we Now Know about the Benefits/Harms of Drugs for Type 2 Diabetes? Cait O’Sullivan, PharmD, Provincial Academic Detailing Program and UBC Therapeutics Initiative How can you Tell Whether your Patient is Benefiting from Drug Treatment of COPD? Aaron Tejani, PharmD, UBC Therapeutics Initiative New Evidence about Hypertension Targets and Statins for Primary Prevention Dr. James M. Wright, UBC Therapeutics Initiative Workshops: Dealing with difficult chronic pain and palliative care Incorporating evidence about preventive therapies into patient informed consent Making decisions about anticoagulants for atrial fibrillation or VTE Difficult hypertension Practical deprescribing Registration opening soon at: http://ubccpd.ca/course/BestEvidence2016 Thanks for your questions and discussion. Thanks for completing your course evaluations.