Lecture 06 Antibiotics I 2013 [Kompatibilitási mód]
Transcription
Lecture 06 Antibiotics I 2013 [Kompatibilitási mód]
Resistance: Antibiotics Principle: inhibit growth of bacteria without harming the host – Drug must penetrate body tissue to reach bacteria (exception: GI infection) – Bacteria targeted must be within the spectrum of the AB – Drug can be bactericidal or bacteriostatic – Different agents can be combined for synergistic effect Identification of the invasive microorganism necessary for optimal treatment General side effect: Alteration in normal body flora – GI tract harbors symbiotic bacteria which are killed by AB => resistant bacteria repopulate the niche = secondary or superinfection (most common: overgrowth of Clostridium difficile) Resistance avoided/delayed by: Using AB only when absolutely needed and indicated: AB often abused for viral infections (diarrhea, flusymptoms, etc.) Starting with narrow-spectrum drugs Limiting use of newer drugs Minimizing giving antibiotics to livestock Identifying the infecting organism Defining the drug sensitivity of the infecting organism Considering all host factors: site of infection, inability of drug of choice to penetrate the site of infection, etc. Using AB combinations only when indicated: Severe or mixed infections, prevention of resistance (tuberculosis) Cell wall inhibitors beta-lactams, glycopeptides, cycloserine, bacitracin Protein synthesis inhibitors erythromycins, clindamycin, aminoglycosides, tetracyclins, chloramphenicol, linezolid, streptogramins Nucleic acid synthesis inhibitors quinolones, sulfonamides, trimethoprim, rifampin Alteration of cell membrane function Polymyxins, lipopetides Miscellaneous metronidazole, isoniazid, ethambutol loss of efficacy of a given AB against a particular strain – Frequently: Staphylococcus aureus, Pseudomonas aeruginosa, Mycobacterium tuberculosis Acquisition: – Spontaneous mutation – Adaption: drug metabolism (β-lactamase); alternative metabolic pathways – Gene transfer: plasmids (via conjugation and transduction); transposons The more ABs are used, the greater the chance of resistance !!! •RANGE OF ANTIBACTERIAL ACTIVITY broad spectrum – narrow spectrum Major groups of pathogenic bacteria used for characterization of antibacterial spectrum non-fermentative Gram– rods fermentative Gram– bacteria Gram+ bacteria obligate intracellular & cell wall defective Mycobacteria e.g. Pseudomonas e.g. E. coli Salmonella e.g. Staphylococcus e.g. Chlamydia Mycoplasma e.g. causative agents of tuberculosis Inhibitors of Cell Wall Synthesis Beta– Beta–lactam antibiotics -Penicillin and derivates -Cephalosporins -Monobactams -Carbapenems Glycopeptides Other Cell Wall- or Membrane-Active Agents 1 Beta lactam antibiotics In 1928, Alexander Fleming was researching vaccines and noticed a culture of staphlococci had undergone lysis from contamination with a mold Fleming finally isolated the mold, Penicillium notatum, notatum, and found that the fluid beneath it possessed antibacterial properties Basic structure consists of thiazolidine ring connected to β-lactam ring, to which is attached a side chain Dosing: 22-4 times per day Combination with aminoglycosides is useful (Synergy) Mechanism of Action Interferes with last step of bacterial cell wall synthesis, causing cell lysis Bactericidal Only effective against rapidly growing organisms that synthesize a peptidoglycan cell wall Inactive against Chlamydia, Mycoplasma, mycobacteria, fungi, viruses β-lactamase resistant β-lactam antibiotics Semisynthetic Methicillin (1958), (1958), Nafcillin, Oxacillin, Oxacillin, Dicloxacillin All are penicillinasepenicillinase-resistant penicillins used in penicillinasepenicillinase-producing staphylococci; narrow spectrum Methicillin--resistant Staphylococcus Methicillin Staphylococcus aureus=MRSA (PBP change) (1961) Mechanism of action way of being bactericide Penicillin binding proteins: proteins: Enzymes involved in forming cross linkages between peptidoglycan chains inactivated by penicillin Inhibition of transpeptidase transpeptidase:: Hinders last step in formation of cross links needed for cell wall integrity Autolysins:: Normally degrade cell wall, but penicillin Autolysins prevents new synthesis Natural Penicillins (basic penicillin) Penicillin G (Benzylpenicillin) Gram +/+/- cocci, Gram + bacilli, spirochetes, anaerobes (Narrow Narrow--spectrum spectrum)) Susceptible to inactivation by β -lactamase (i.e. Staphylococcus aureus) aureus) Penicillin V More acid stable than Pen G For the treatment of meningitis caused by susceptible organism Aminopenicillins (ampicillin and amoxicillin) Broader spectrum against GramGram-negatives (plus as in case of basic penicillin penicillin)) Klebsiella species show primarily resistance to aminopenicillins Resistance due to plasmid mediated penicillinase May use clavulanic acid or sulbactam to extend/maintain the antibacterial activity Reach therapeutic concentration in the CSF 2 Ureidopenicillins Piperacillin Carbenicillin, Ticarcillin Azlocillin,, Mezlocillin Azlocillin Effective against Pseudomonas Pseudomonas aeruginosa Reach therapeutic concentration in the CSF Allergic Reactions Acute (< 30 min) Urticaria, angioedema, bronchoconstriction, GI, shock Accelerated (30 minmin-48 hrs) Urticaria, pruritis, wheezing, mild laryngeal edema, local inflammatory reactions Delayed (> 2 days) Skin rash Oral glossitis, flurred tongue, black and brown tongue, cheilosis, severe stomatitis with loss buccal mucosa Cephalosporins Cephalosporium acremonium, first source, isolated in 1948 β-lactam antibiotics Related to penicillins structurally and functionally More resistant to βlactamases Beta-lactamase inhibitors Irreversible inhibitor of β-lactamase Clavulanic acid Sulbactam Tazobactam Large molecules, do not penetrate into the CSF Ampicillin+sulbactam=Unazyn (for newborn babies) Amoxicillin+ Clavulanic acid=Augmentin Piperacillin+tazobactam=Tazocin (against P. aeruginosa), iv. All combinations are effective against G+ and G- negative anaerobes Carbapenems Meropenem (Meronem): penetrates well into the CSF Imipenem (Tienam), Doripenem; Ertapenem (Invanz): No activity against P. aeruginosa Synthetic β-lactam antibiotics sulfur atom in the thiazolidine ring Resists β -lactamase hydrolysis Good efficacy against facultative anaerob GramGram-negatives, Pseudomonas, Gram+ and Gram – anaerobes Effective against ESBL producing GrGr-negatives They are ineffective: MRSA, Stenotrophomonas maltophilia, E. faecium, B. cepacia (for the second written test) Antibacterial Spectrum Five generations Increased generation number: number: -increased gram negative bacterial susceptibility -increased β-lactamase resistance -decreased efficacy against gram + No effect against: MRSA, Enterococci, Listeria, anaerobic bacteria (except: cefoxitin),, Rickettsia, L. pneumophila, cefoxitin) Chlamydia, Mycoplasma (for the second written test) 3 First Generation Cefazolin, Cephalexin, Cefadroxil, Gram + cocci, some gram – bacilli (E. coli), coli), They are effective for treating Staphylococcal (Meticillin sensitive =MSSA) and Streptococcal infections Do not penetrate into the CSF Second generation Cefaclor (Ceclor), Cefuroxime axetil (Zinnat)(iv. (Zinnat)(iv. and oral oral)) Cefoxitin (Mefoxin) is effective against against:: -anaerobes -ESBL producing GramGram-negatives Their antibacterial spectrum is broader than that of 1st generation cephalosporins and includes some gram -ve pathogens (H. influenzae, Neisseria) Neisseria) They are also more resistant to beta-lactamase They are useful agents for treating upper and lower respiratory tract infections and sinusitis Do not penetrate into the CSF Third Generation Cefixime (Oral) (Suprax) Cebtibuten (oral) (Cedax) Cefotaxime (Claforane) Ceftriaxone (Rocephine) Ceftazidime (Fortum) Cefoperazone (Cefobid) Cefotaxime and cefriaxone are used for the blind treatment of meningitis Fourth Generation Cefepime (Maxipime), Cefpirome (Cefir) They have a greater resistance to betalactamases than the third generation cephalosporins. Many can cross blood brain barrier and are effective in meningitis. Active against P. aeruginosa. Only for severe infections Third Generation They have an extended spectrum of action against Gram -ve organisms (i.e. Haemophylus influenza, Neisseria meningitidis, E.coli, Neisseria gonorrhea, Enterobacter spp., most Klebsiella) P. aeruginosae, Resistant to most beta-lactamases Ceftriaxone and cefotaxime have excellent activity against Streptococcus pneumoniae, but never effective against Pseudomonas aeruginosa Ceftazidime is effective against Pseudomonas Ceftriaxone, cefotaxime and ceftazidime reach therapeutic concentration in the CSF Cephalosporins Active Against MethicillinResistant Staphylococci (fifth generation) Ceftaroline fosamil (Teflaro) Ceftobiprole medocaril (Zeftera) strong affinity for the PBP2a and PBP2x, responsible for resistance in staphylococci and pneumococci, respectively Look effective against MRSA, S. pneumoniae, Pseudomonas Enter into the CSF 4 Bacterial Resistance to β-lactams Monobactams Narrow spectrumspectrum- enterobacteriaceae, pseudomonas; no gram + or anaerobic activity Resistant to β-lactamase Aztreonam IV or IM β-lactamase activity 1. • • 2. 3. Hydrolyzes cyclic amide bond of β -lactam ring Usually acquired by transfer of plasmids Decreased permeability to drug Altered penicillin binding proteins (MRSA, S. pneumoniae) 4. Active efflux efflux Staphylococcus resistance to beta lactams 1.beta-lactamase penicillinase only Resistant to -penicillin-G, -aminopenicillins, -ureidopenicillins Susceptible: - beta-lactamase resistant penicillins (methicillin), -First and second gen. cephalosporins, Augmentin, Unazyn -carbapenems Alternative cell wall synthesis altered PBP e.g. MRSA ! Because of the new, PBP2a is produced, this strains are resistant to practically all betalactams ! Susceptible: fifth gen. cephalosp (clinically looks effective). Extended-Spectrum β-Lactamases (ESBL) β-lactamases capable of conferring bacterial resistance to All beta-lactams, but not the cephamycins (cefoxitime) or carbapenems Only in cases of Gram-negatives (i.e. E. coli, Klebsiella pneumoniae) Alteration of PBPs Mosaic gene structure develops (PBP2x) Recombination between Streptococcus pneumoniae and other α-hemolytic Streptococci Penicillin MIC will be increased and other β-lactam MICs also will be increased This resistance is not inhibited by β-lactam inhibitors Glycopeptides (Vancomycine, teicoplanine) It binds firmly to the DD-Ala Ala--D-Ala terminus and inhibits transglycosylase. No effect against GrGr-negatives Narrow--spectrum, against MRSA, penicillin resistant Streptoccus Narrow pneumoniae,, Corynebacterium jeikeium, pneumoniae jeikeium, pseudomembranous colitis caused by Clostridium difficile i. v., oral ral route only for C. difficile Synergy with aminoglycosides Toxic to the ears and to the kidneys Once per day Side effects: red man syndrome or red neck syndrome. 5 Primary resistance against some, lesser important species: -Leuconostoc -Pediococcus -Lactobacillus species Acquired resistance -S. aureus -Enterococci -Clostridium difficile NAM/NAG-peptide subunits, normally D-alanyl-D-alanine, which vancomycin binds to D-alanyl-D-lactate and D-alanyl-Dserine result in resistance agricultural use of avoparcin , another similar glycopeptide antibiotic, has contributed to the emergence of vancomycin-resistant organisms. Newer glycopeptide antibiotics Dalbavancin Derived from teicoplanin Effective on methicillin-resistant and vancomycinintermediate S aureus Telavancin Derived from vancomycin active versus gram-positive bacteria including strains with reduced susceptibility to vancomycin Other Cell Wall- or Membrane-Active Agents Daptomycin Novel cyclic lipopeptide Similar to that of vancomycin Active against vancomycin-resistant strains of enterococci and S aureus Fosfomycin Analog of phosphoenolpyruvate Active against both gram-positive and gram-negative Cycloserine Bacitracin: -inhibits cell wall synthesis -Effective against Gram positive microorganisms -Topical application due to nephrotoxicity -Often used for traumatic abrasions 6