Frans C. Stades - American College of Veterinary Ophthalmologists
Transcription
Frans C. Stades - American College of Veterinary Ophthalmologists
Strategies to target canine inherited ocular disordersa critical review of European approaches Frans C. Stades DVM, Ph.D., Dip. ECVO Assoc. Prof. Em. Vet. Ophthalmology, University Utrecht f.c.stades@uu.nl; stades@planet.nl Strategies to target (canine) presumed inherited ocular disorders-a critical review of ECVO approaches and differences from other Schemes ___________________________________ _________ Frans C. Stades DVM, Ph.D., Dip. ECVO Assoc. Prof. Em. Vet. Ophthalmology, University Utrecht f.c.stades@uu.nl; stades@planet.nl ECVO Hereditary Eye Disease Scheme 1. 2. 3. General aspects Organization and panels Panellists 1. 2. 4. 5. 6. 7. 8. 9. Training and examination of Eye Scheme Examiners Requirements to become and to maintain Panellist status Arrangements + procedure for the Eye Examination + Form Examination outside the Scheme Publication of Results Conflicting results on same animal + "Suspicious" cases Appeals Procedure Other Schemes European? EU = 27; Eur = 58? (e.g. Vatican, San Marino) Languages: 30 n panellists – (Dips) n cases (’08) n/panellist n Inhab x106 (’07) --------------------------------------------------------------------------------------------------------------1. N 19 (1) 5,500 289 4.6 2. Fin 24 (0) 19,000 791 5.2 3. DK 18 (0) 3,500 194 5.4 4. NL 8 (5) 7,000 875 16.3 5. D 80 (8) 12,000 150 82.3 6. Austria 15 (2) 1,512 100 8.3 7. CH 6 (4) 2,480 413 7.2 – Spain-Dips 2 (2) 221 110 44.5 – GB+IE-Dips 3 (11+1) 261 87 60.9 + 4.3 -------------------------------------------------------------------------------------------------------------------------------------------ECVO total 175 (34) 51,474 294 239 – (Isr) 1 (1) 300 5.5 – France-Dips 6 (8) starting 63.4 – Belgium problems with privacy laws (identity dog not public?) 10.6 – Ital = training (4) 59.1 -------------------------------------------------------------------------------------------------------------------------------------------• • Sweden BVA=GB+IE 31 28 (5) (11+1) 17,000 18,000 548 642 9 60.9 + 4.3 ECVO Hereditary Eye Disease Scheme: General aspects Purposes: diagnose + control PIED • PIED: – – – – (presumed Inherited Eye Disease) in Animals = HED Committee disabling painful disturbing to wellbeing necessitate surgical intervention or lifelong medication • Results made public: identity animal + free + not free of PIED CERF-ACVO: PIED: – potential compromise of vision or other ocular function • Diagnose + statistical summaries of PIED / breed in “blue book” • Provide a registry of purebred dogs certified free of PIED ECVO Hereditary Eye Disease Scheme: General aspects purpose concerning PIED: Scheme provides: • definitions • guidelines • recommendations • information Additional info: appendixes, Procedure notes, illustrations on website (www.ecvo.org/public/index.htm) Failing at moment: general breeding advice / PIED ECVO Hereditary Eye Disease Scheme: General aspects Tries to guarantee/provide (initial training + continuing education): • Ability examiners to: – recognize PIED – differentiate clinical signs of PIED + their significance • Authentication of – veterinary European Eye Specialists (Diplomates) – specifically trained veterinarians (ESE: European Eye Scheme Examiner) • Appropriate level of expertise + service for – – – – owners breeders Breed clubs+ Kennel clubs public in general, by providing an for the diagnosis of PIED. • rules + guidelines for the eye examination ECVO Hereditary Eye Disease Scheme: General aspects • General examination: eye + adnexa • Partly examination: not permitted • Certificate of the examination issued in respect of PIED – valid for one year from the date of examination – recommended: animal examined annually – inconclusive: re-examined sooner e.g. within 6 months • Litter screening can also be performed under the Scheme Certificate • National language + English • Readable + understandable for well informed breeder + owner 2. Organization and panels • ECVO Hereditary Eye Disease Committee (former Genetics Comm.) +Advisory Committee (panel representatives) • National ECVO Diplomates + ESE Nat. Panel – national rules and regulations (not violate ECVO-ConstitutionBylaws-Scheme • Panel Board, elected by its membership – consider business + policies of Panel – In absence of a National Panel: ECVO-HED-Committee will act in its place • National Panel must meet at least once per year 3. Panellists Panellists ECVO to perform examinations are: • Practising Diplomates of the ECVO (51); • Eye Scheme Examiners (ESE: 140): veterinarians, specifically trained and examined (contract may be extended ad infinitum by the ECVO) 3. Panellists Training and examination of Eye Scheme Examiners • Before training commences, the candidate must confirm normal stereoscopic, color vision (binocular, corrected for refractive errors) (first proposal: stereoscopic (at least 240 arc seconds) color vision (corrected for refractive errors, binocular vision of at least 1.0). • + Residents who want to do Scheme examinations! Before ESE-candidates can qualify to sit Scheme examination: must document: • examination ≥ 500 dogs under supervision 2 different ECVO panel members – ≥ 50 of these: under practicing ECVO Dip – 200 dogs may be under ACVO Dip – record of all examined • examination ≥ 100 cats – ≥ 10 of these: under practicing ECVO Diplomate or ESE – record of all examined. • examination certain specific breeds + diseases, in Appendix A (e.g.: PHTVL/PHPV Grade 1 (at least 1 in puppies ≤ 10weeks, Complete retinal detachment, RD focal/multifocal, CEA, ≤ 50 Sheltie-Collie puppies etc) Before ESE-candidates can qualify to sit Scheme examination: • must document: participation 3 ECVO recognized continuing education (anterior + posterior segments + basic genetic principles) • trained in direct + indirect ophthalmoscopy, slitlamp biomicroscopy + gonioscopy • literature concerning PIED: Appendix B ECVO-Eye Scheme Examiner (ESE)- exam Coordinated and directed by 2 ECVO members: • member 1x HED-Committee + 1x Examination Committee or Executive Committee of the ECVO Examination consist of 3 parts: 1. written section of multiple choice (50x; 3 min/question) PIED 2. images PIED (40x; 2 min/question) Passed: 3. live case evaluation (at least 5 cases) + oral examination Requirements for maintaining Panellist status Board of National Panel is responsible: • Panellist obliged to work under the rules; violation: Board entitled to expel • Proof of continuing misdiagnosis: re-examined or expel • Minimum number examinations: 100 / year or 300 / 3 years – less = re-qualification. Recently qualified: exempted first full year Requirements for maintaining Panellist status • Attend annual meeting Panel.absent 3 consec. meetings (without dispensation): can be expelled; • Attend related meetings Panel (e.g. arbitrary or appeal cases), absent more than half (over 3 consec. years), (without dispensation): can be expelled • Attend one annual scientific meeting ECVO / 3 years Absent (without dispensation): can be expelled • In special circumstances: exemption from: – minimum number examinations – attendance of meetings Requirements for maintaining Panellist status • Possess good eyesight: – minimum visual acuity of 0.7 (corrected for refractive errors) – certificate visual acuity every 5 years until 70, thereafter: every second year. • Expel Panellist: by Board Panel – appeal to entire National Panel or HED-Committee ECVO • Expelled: may be allowed by Board to sit new examination to re-qualify 5. Procedure for the Eye Examination • registration document / identifying document • any previous eye certification. – not available: examination can be undertaken but Certificate issued after provided with documentation • Certificates only issued: identified permanently (e.g. by tattoo, microchip or otherwise) • All animals: general examination eye + adnexa – including use mydriatic 5. Procedure for an ECVO-Eye Examination • according to the ECVO protocol – Preliminary or partial examinations are not permitted – Gonioscopy = additional (thus not separate) • certificate signed by owner before start examination • certificate is issued upon completion • patient: outside Scheme + PIED is recognized: – Panellist strongly recommended to issue: ECVO Certificate – recommended cost by Registry or Kennel Club – no certificate issued: Panellist obliged to keep record of such cases and report the number/disease to HED-Committee annually (due December 31, still weak point) Prior to the examination: • owner must sign completed first part of certificate – – – – verifying details are correct date last examination etc. available for publication + other ECVO approved use ______ Specific breeds (Procedure Notes): PPM, iris coloboma, pectinate ligament abnormality: examination before mydriatic v v minimum equipment: • slit-lamp biomicroscope ≥ 10 x (≥16x better?) • binocular indirect ophthalmoscope • other: optional (Certificate only valid: if accompanied by additional document specifying method) – ERG: standardized protocol (Narfstrom K, et Al. Doc Ophthalmol. 2002; 105: 83-92) __ __ __ Box: Pectinate ligament abnormality: • before mydriasis • gonioscopy completed bilaterally (Barkan, Franklin or Koeppe) • in all breeds primary glaucoma occurs (Proc. Notes) e.g. Bouvier, Bassets, Samoyed, Husky, Am.C Spaniel, E.Springer Spaniel, Flat Coated Ret. ,Chow, Dutch Shepherd (Rough Hair), Entlebucher, Viszla, Tatra, Leonberger, (Border Collie; not yet in PN) etc. V V Procedure notes: e.g. Instructions • Details of all lesions/conditions (whether relating to hereditary eye disease or not): recorded in: – descriptive comments – drawings – results – preferably in English PIED: criteria • scientific literature + genetic testing • incidence affected animals in the population – numbers in data bank national registry + CERF – numbers in data banks breed clubs – panel member experience Results Main Groups (8+8): More: Other (definitive: 1-8 + 11-18: 2 + 2 more can be added) Congenital Acquired Results possibilities: UNAFFECTED • displays no clinical evidence of the presumed inherited eye disease(s) specified l Results possibilities just drawing and/or comment OS corneal scar Results possibilities: N.B. • PIED, not yet proven in this breed • under investigation • to be included in data base Breed Club Results possibilities: UNDETERMINED • displays clinical features that could possibly fit the presumed inherited eye disease(s) mentioned, but the changes are inconclusive (e.g. do DNA test) Sheltie, lat optic disc ___ V Results possibilities: SUSPICIOUS • displays minor, but specific signs of the PIED mentioned. Further development will confirm the diagnosis. Re-examination in 6 …12 months __ Results possibilities: AFFECTED • displays clinical evidence of the presumed inherited eye disease(s) specified (+ specifying boxes) v --- Procedure notes ECVO Pectinate ligament abnormality 1. Fibrae latae (FL; fibre/trabecle: broadened [latae; Lat.: broad] also described as broad bands); 2. Lamina (LA.; plates/sheets continuous tissue, very short remaining fibres); 3. Occlusion (OC.; pectinate ligament closed, with flow holes. Gen.: + narrowed angle a/o shallow A.C.) Results possibilities: AFFECTED • displays clinical evidence of the presumed inherited eye disease(s) specified • severity is expressed using the boxes for mild, moderate or severe ____ v Procedure notes: e.g. specific breeds 1. Pectinate Ligament Abnor. gonioscopy : • American Cocker Spaniel • Bouvier des Flandres • Bassets (all) • Border Collie • Chow Chow • Dutch Shepherd (Rough Hair) • English Springer Spaniel • Entlebucher Mountain Dog • Flat Coated Retriever • Husky Siberian • Leonberger • Samoyed • Tatra • Viszla 2. Persistent Pupillary Membrane Airdale Terrier Basenji Chow Chow Cheaspeak bay Ret (Cerf) English Cocker Spaniel Mastiff Petit Basset Griffon Vendéen Welsh Corgi 3. Iris coloboma Australian shepherd Chinese crested dog Procedure notes • 1. 2. e.g.: PPM non-inherited or presumed inherited congenital eye disease in some breeds. Remnants of the embryological vascular network (pupillary membrane) which nourishes the anteri-or part of the developing lens (failing to regress in the first 4-5 weeks after birth). There can be tiny, more or less triangular shaped dots, centrally, on the anterior capsule of the lens. These are to be drawn into the figures in the “drawing area” and are not to be ticked-in in the undetermined or affected boxes in the “results area”. other forms of PPM: these are to be mentioned as 1. 2. 3. N.B…under investigation in the specific breeds (see list) in the box PPM: “affected” and the box of the parts which are involved; if more parts are involved, more boxes are to be ticked in If the examiner finds that vision impairment or blindness occurs, the animal has to be “ticked” as “affected” in all breeds. Distribution certificate copies: • top copy: National registry (Major disadv.: should be European) white + original signatures • yellow: Breed club or Kennel club Breed club; • pink: Panellist • white: owner • Litter Examination • younger than 12 weeks (after tattoo/chip) – Litter Screening Form – Separate certificate • Germany on line Registry + breed club • Norway starting 7. Publication of Results • name (only animal!), registration, identification + results: – appropriate National registration office – national Kennel Club + Breed Club (if sanctioned by the Members) • animal exported, all results examinations + pedigree to importing country • transferred from one registry to an other, the “exporting” registry provides all results of examinations on PIED + “importing” registry is obliged to include them Conflicting results eye examinations: on the same animal • conflict: most adverse judgment is valid until the animal is examined by the National Panel or Chief Panellist, whose decision will be final • found “affected” for PIED + transferred to other registry – “affected” not be changed, unless re-examined by the appeals authority of the new registry – “affected” not be changed: for conditions which may be changed artificially; theses results are definitive (e.g. distichiasis, entropion, etc.) 9. "Suspicious" cases after the prescribed period • re-examined by Panel or Chief Panellist • alternatively: by the first examiner or another Panellist: "affected“ = definitive, unless by Panel or Chief Panellist "unaffected“ = "suspicious" judgment remains valid until 1. National Panel or the Chief Panellist or if large distances: 2. after extra follow-up period of at least 1 year: by 2 panellists 3. after extra follow-up period of at least 2 year: by 1 panellists _________ 10. Appeals Procedure • Panel (regional e.g. Germany) meetings (at least 2 times/year), or a chief panellist (an ECVO-diplomate appointed by the National Panel) available for the evaluation of appeal cases. An owner has the right to appeal the results of an eye examination and the procedure is as follows: • Any appeal: in writing + within 60days: Panel /Chief Panellist. Decision is final – except: choroidal hypoplasia + retinal dysplasia: re-examination must be completed before 12 weeks of age or: • Animal + Certificate to second Panellist – second Panellist agreeing with the first Panellist: appeal deemed to have failed = informs Panel. Further appeal to Panel Meeting / Chief Panellist is possible – second Panellist disagreeing with the first Panellist: Panel Meeting/Chief Panellist. This decision will be final To be done: - list breed abnormalities - general breeding advice / abnormality e.g. distichiasis – ectopic cilia • Definition + discomfort to the animal + need to surgical intervention • Significance to ectopic cilia • Why PIED ( number cases data bases, literature, DNA test) • Hereditary basis (not been established – e.g. Cerf: recorded+ breeder’s option) • Breeding effects know: affected to unaffected dramatic drop = carriers (shown in Havaneser) + spread into population, unrecognized. Breed clubs could decide the following: • In case there is a low number of cases of distichiasis in a breed, or in breeds where the type of hairs are stiff and irritating, it is wiser for a breed club to decide not to use affected dogs for breeding • If really necessary to use affected: more advisable to breed affected to affected, until, in future, a DNA test is available. Differences to other Schemes: • BVA: Chip-tattoo not obligatory + no identification check Kennel Club: 2010 chip obligatory • none use categories of “undetermined” and “suspicious” (cases which are inconclusive (BVA), respectively where further development may confirm the diagnosis) • Sweden + BVA – no adnexa – abnormalities mentioned only in breeds in which ≈ proven (Signs of PRA in the Sahara ice dog breed is no PRA!) Differences to other Schemes: • Most European countries: Kennel club issues pedigree; Breed club issues breeding advice /rules – puppy registry! • Sweden + Switzerland: result eye examination may have direct consequence: – PIED no further pedigrees (National Kennel club) BVA scheme (GB+Ierland) • Self trained examiners + British Diploma + European specialists® [28 (12 Dips)] • certificate is readable and understandable for well informed owner – list of specified congenital and of required PIED’s is given Pass or fail the dog • Issued for pedigree dogs, regardless if can be identified! (2010 all chipped) • Certifies for inherited non-adnexal + include general examination eye+adnexa BVA scheme (GB+Ierland) • Eleven different inherited eye conditions are only certified in specific breeds (approximately 50), in other specified breeds (some 45), the eye conditions are listed as “under investigation”. • In the remaining breeds they are identified, but not listed under the BVA-scheme. Labrador BVA scheme (GB+Ierland) • In doubt, or in cases where it is likely that the appearance will change with time, a re-examination in 6 months is recommended, or the dog is examined by a second panellist. • If two panellists disagree or in case of appeal, the dog is referred to the Chief panellist, whose decision is final SSVO scheme (Sweden) • Self trained examiners + ECVO-recognized specialists [total 31 (5 Dips)] – Training + continuing education: shared 4 Nordic countries – To sit examination: animals to be examined under direct supervision doubles ECVO Scheme. • identification obligatory (tattoo or microchip) • Only inherited non-adnexal eye disease + include general examination • readable and understandable for the well informed Swedish-reading owner • Signs of eye disease: specified in handwriting by the examiner no specific boxes SSVO scheme (Sweden) • examiner considers this disease inherited or not • The different (non-adnexal) inherited eye diseases are certified only in specified breeds (approximately 55). • Appeal, dog referred to Swedish ECVO Diplomate (decision is final) • Registration of offspring of several specified breeds will be refused by the Swedish Kennel Club, unless both parents have been examined or if one or both parents is/are affected with specified PIED (mainly PRA and lens luxation). CERF scheme • Only recognized specialists (Dip’s ACVO) as examiners • computer readable certificate • dog should be microchipped or tattooed – non-compatible systems – currently not require examiner to verify permanent identification himself. • All abnormalities recorded, no matter the significance. If an abnormality is detected that is not considered to be inherited, it should be described in the comment section. • All data are collected by the CERF, which publishes the overall results. • Individual dogs’ identities are confidential • registration number American Kennel Club + for advertising – For a fee, thus no stimulus to publication of affected to breed club! – Annual renewal is required Appendix A • • • • • • • • The following list of diseases/variations should have been seen and recorded (at the discretion of the national panel) Iris Disease Number Persistent pupillary membrane 5 Iris atrophy2, coloboma Lens Perinuclear ring (cortex)5 Nuclear fibrillar opacities 5 Pigment on anterior lens capsule; 5 Cataract, complete2 Cataract, posterior cortical, including posterior polar10 Cataract, anterior cortical / subcapsular5 Cataract, anterior suture lines5 Cataract, other (e.g. suture tips, equatorial)5Cataract, nuclear5 Lens (sub)luxation (can be seen without supervision)5 Vitreous Asteroid hyalosis2 Persistent tunica vasculosa lentis posterior1PHTVL/PHPV Grade 1 (at least 1 in puppy ≤ 10weeks)3 Fundus Complete retinal detachment2 Partial retinal detachment2 RD focal/multifokal5 CEA, CRD30 CEA, coloboma 5PRA early stage3 PRA late stage3Non-inherited retinopathies 5Other: Glaucoma (can be seen without supervision)2 Of the 500 dogs examined at least 50 should be collie/Shetland sheepdog puppies ≤ 10 weeks of age. Of these, at least 10 should be merle dogs. Appendix B List of relevant literature 1. Anatomy, embryology and histology, physiology, immunology, pharmacology and vision 2. Gelatt Veterinary Ophthalmology 4th ed. 2007 Blackwell Synergy 3. Pathology 4. Pathology of domestic animals (Jubb & Kennedy) , 4th ed., 3 volumes, London Academic Press, 1993.(chapters on eye and related structures) Neuro-ophthalmology 1. DeLahunta & Glass: Veterinary neuroanatomy and clinical neurology 3rd Ed. Saunders/Elsevier 2009 (chapters related to the eye and adnexa and vision) Clinical ophthalmology 1. Gelatt Veterinary Ophthalmology 4th ed. 2007 Blackwell Synergy 2. Slatter’s Fundamentals of Veterinary Ophthalmology (Maggs, Milelr & Ofri), 4th ed. , Saunders/Elsevier, 2009 3. Ophthalmology for the veterinary practitioner (Stades F,Wyman, Boevé, Neumann, Spiess) , Schlütersche Hannover, 2007 4. Small animal ophthalmology, a problem oriented approach (Peiffer R. & Peterson – Jones S.), 2009, 4th ed., Saunders/Elsevier. 5. Canine ophthalmology: an atlas and text (Barnett KC ,Heinrich C & Samson J), 2002, WB Saunders. 6. Manual of small animal ophthalmology (Peterson – Jones S. et al.), BSAVA Publications Cheltenham, 2002. 7. Feline ophthalmology, an atlas and text ( Barnett KC & Crispin SM), WB Saunders, 1998 8. Genetics 9. Inherited eye diseases in purebred dogs (Rubin L) Williams & Wilkins, 1989. 10. ACVO Genetics Committee : Ocular disorders proven or suspected to be hereditary in dogs , Vet.Pract.Publishing Cy ed 11. http:// www.optigen.com: testing for inherited eye diseases of purebred dogs Recommended articles 1. Acland, G.M., and Aguirre, G.D.: Retinal degenerations in the dog: IV. Early retinal degeneration (erd) in Norwegian Elkhounds. Exp. Eye Res., 44:491, 1987. 2. Aguirre, G.D., and Acland, G.M.: Variations in retinal degeneration phenotype inherited at the prcd. locus. Exp. Eye. Res. 46:663,1988. 3. Aguirre, G.D., and Rubin, L.F.: Progressive retinal atrophy (rod dysplasia) in the Norwegian elkhound: J. Am. Vet. Med. Assoc., 158:208,1971. 4. Aguirre, GD; Rubin, LF; Pathology of hemeralopia in the Alaskan Malamute dog. Invest Ophthalmol1974;13, 231-235. 5. Albert, D.M., et al: Canine herpes-induced retinal dysplasia and associated ocular anomalies. Invest. Ophthalmol. Vis. Sci., 15:267, 1976. 6. Barnett KC, Curtis R. Lens luxation and progressive retinal atrophy in the Tibetan Terrier. Vet Rec 1978; 103: 160. 7. Barnett KC. Curtis R. Autosomal dominant progressive retinal atrophy in Abyssinian cats. J Hered 1985; 76: 168-70. 8. Bedford PGC. Gonioscopy in the dog. J Small Anim Pract 1977; 18: 615-29 9. Bedford PGC. A gonioscopic study of the iridocorneal angle in the English and American breeds of cocker spaniel and the basset hound. Journal of Small Animal Practice 1977; 18: 631-642. 10. Bedford PGC. Collie eye anomaly in the United Kingdom Vet Rec 1982. 111: 263-70. 11. Bergsjø T, Arnesen K, Heim P, Nes N. Congenital blindness with ocular developmental anomalies including retinal dysplasia, in Doberman Pinscher dogs. J Am Vet Med Ass 1984; 184: 1383-86. 12. Bjerkås E, Bergsjø T. Hereditary cataract in the rottweiler dog. Progr Vet Comp Ophthalmol 1991; 1: 7-10. 13. Bjerkås E, Haaland M. Pulverulent nuclear cataract in th Norwegian buhund. J Small Anim Pract 1995; 36: 471-74. 14. Bjerkås E, Ekesten B, Farstad W. Pectinate ligament dysplasia and narrowing of the iridocorneal angle associated with glaucoma in the English springer spaniel. Vet Ophthalmol 2002; 5: 49-54. 15. Boevé MH, Stades FC, van der Linde-Sipman, Vrensen GFJM. Persistent hyperplastic tunica vasculosa lentis and primary vitreous (PHTVL/PHPV) in the dog: A comparative review. Progr Vet Comp Ophthalmol 1992; 2: 163-72. 16. Carrig CB, Sponenberg DP, Schmidt GM, Tvedten HW. Inheritance of associated ocular and skeletal dysplasia in Labrador retrievers. J Am Vet Med Assoc 1988; 193: 1269-72 17. Cottrell BD, Barnett KC. Primary glaucoma in the Welsh springer spaniel. J Small Anim Pract 1988; 29: 185-99. 18. Crispin S, Long SE, Wheeler CA. Incidence and ocular manifestations of multifocal retinal dysplasia in the golden retriever in the UK. Vet Rec 1999; 145:669-672. 19. Curtis R. Aetiopathological aspects of inherited lens dislocation in the Tibetan Terrier. J Comp Path 1983; 93: 151-163. 20. Curtis R, Barnett KC. Primary lens luxation in the miniature bull terrier. Vet Rec 1983; 112: 328-329. 21. Curtis R. Late-onset cataract in the Boston terrier. Vet Rec 1984; 115: 577-78. 22. Curtis R, Barnett KC. A survey of cataracts in golden and Labrador retrievers. J Small Anim Pract 1989; 30: 277-86. 23. Curtis R. Lens luxation in the dog and cat. Vet Clin North Am: Small Anim Pract 1990; 20: 755-773. 24. Curtis R, Barnett KC. Progressive retinal atrophy in miniature longhaired dachshund dogs. Br Vet J 1993; 149: 71-85. 25. Dekomien G, Runte M, Gödde R, Epplen JT. Generalized progressive retinal atrophy of Sloughi dogs is due to an 8-bp insertion in exon 21 of the PDE6B gene. Cytogenet Cell Genet 2000; 90: 261-267. 26. Djajadiningrat-Laanen SC, Boevé MH, Stades FC, van Oost BA. Familial non-rcd 1 generalised retinal degeneration in Irish setters J Sm Anim Pract 2003; 44:113-116. 27. Ekesten B, Narfström K. Age-related changes in intraocular pressure and iridocorneal angle in samoyeds. Prog Vet Comp Ophthalmol 1991; 2: 37-40. 28. Ekesten B. Correlation of intraocular distances to the iridocorneal angle in samoyeds with special reference to angle-closure. Prog Vet Comp Ophthalmol 1992; 3: 67-73. 29. Ekesten B, Bjerkås E, Kongsengen K, Narfström K. Primary glaucoma in the Norwegian elkhound. Vet Comp Ophthalmol 1997; 7: 14-18. 30. Foster SJ, Curtis R, Barnett KC. Primary lens luxation in the Border Collie. J Small Anim Pract 1986; 27: 1-6. 31. Gelatt, K.N. et al.: Animal models for inherited cataracts: A review. Curr. Eye Res., 3(5):765-778, 1984. 1. 2. 3. 4. 5. 6. 7. 8. 9. 10. 11. 12. 13. 14. 15. 16. 17. 18. 19. 20. 21. 22. 40. Grahn BH, Cullen CL Retinopathy of Great Pyrenees dogs: fluorescein angiography, light microscopy and transmitting and scanning electron microscopy. Vet Ophth 2001 4: 191-199. Holle DM, Stankovics ME, Sarna CS, Aguirre GD. The geographic form of retinal dysplasia is not always a congenital abnormality. Vet Ophth 1999; 2: 61-66. Lazarus JA, Pickett JP, Champagne ES. Primary lens luxation in the chinese Shar Pei: Clinical and hereditary characteristics. Vet Ophthalmol 1998; 1: 101-107. Leon A, Curtis R, Barnett KC. Hereditary persistent hyperplastic primary vitreous in the Staffordshire bull terrier. J Am Anim Hosp Assoc 1986; 22: 765-74. Leppanen M, Mårtenson J, Mäki K. Results of ophthalmologic screening examinations of German Pinschers in Finland – a retrospective study. Vet Ophth 2001; 4: 165-169. Long, SE; Crispin, SM. Inheritance of multifocal retinal dysplasia in the golden retriever in the UK. Vet Rec 1999; 145: 702-204 MacMillan, AD; Lipton, DE. Heritability of multifocal retinal dysplasia in American cocker spaniels. J Am Vet Med Assoc 1978; 172: 568-572. Martin CL, Wyman M. Glaucoma in the basset hound. Journal of the American Veterinary Medical Association 1968; 153: 1320-1327. Martin, C.L., and Chambreau, T.: Cataract production in experimentally orphaned puppies fed a commercial replacement for bitch's milk. J. Am. Anim. Hosp. Assoc., 18:115, 1982. Martin, C.L.: Development of pectinate ligament structure of the dog: Study by scanning electron microscopy. Am. J. Vet. Res., 35:1433, 1974. Martin, C.L.: Gonioscopy and anatomical correlations of the drainage angle of the dog. J. Small Anim. Prac., 10:171, 1969. Martin, C.L.: Scanning electron microscopic examination of selected canine iridocorneal angle abnormalities. J. Am. Anim. Hosp. Assoc., 11:300, 1975. Martin, C.L.: Slit lamp examination of the normal canine anterior ocular segment. Part I: Introduction and technique. J. Small Anim. Pract., 10:143, 1969. Martin, C.L.: Slit lamp examination of the normal canine anterior ocular segment. Part II: Description. J. Small Anim. Pract., 10:151, 1969. Martin, C.L.: Slit lamp examination of the normal canine anterior ocular segment. Part III: Description and summary. J. Small Anim. Pract. 10:163, 1969. Martin, C.L.: The normal canine iridocorneal angle as viewed with the scanning electron microscope. J. Am. Anim. Hosp. Assoc., 11:180, 1975. McLellan GJ, Elks R, Lybaert P, Watte C, Moore DL, Bedford PG. (2002) Vitamin E deficiency in dogs with retinal pigment epithelial dystrophy. Vet Rec 151(22):663-7 Narfstrom, K.: Progressive retinal atrophy in the Abyssinian cat: Clinical characteristics. Invest. Ophthalmol. Vis. Sci., 26:193, 1985. Narfström K, Dubielzig R. Posterior lenticonus, cataracts and microphthalmia; congenital ocular defects in the cavalier king charles spaniel. J Small Anim Pract 1984; 25: 669-77. Narfström K. Cataract in the West Highland white terrier. J Small Anim Pract 1981; 22: 467-71. Narfström K, Wrigstad A, Ekesten B, Nilsson SEG. Hereditary retinal dystrophy in the briard dog: Clinical and hereditary characteristics. Prog Vet Comp Ophthalmol 1994; 4: 85-92. Narfstrom K, Ekesten B, Rosolen SG, Spiess BM, Percicot CL, Ofri R; Committee for a Harmonized ERG Protocol, European College of Veterinary Ophthalmology. Guidelines for clinical electroretinography in the dog. Doc Ophthalmol. 2002; 105: 83-92. Parshall CJ, Wyman M, Nitroy S et al. Photoreceptor dysplasia: An inherited progressive retinal dystrophy of miniature schnauzer dogs. Prog Vet Comp Ophthalmol 1991; 1: 187-203. Petersen-Jones SM, Clemens PJM, Barnett KC et al. Incidence of the gene mutation causal for rod-cone dysplasia type 1 in Irish setters in the UK. J Small Anim Pract 1995; 36: 310-14. Petersen-Jones S.M. Abnormal ocular pigment deposition associated with glaucoma in the Cairn terrier. J Small Anim Pract 1991; 32: 19-22. Read RA, Wood JLN, Lakhani KH. Pectinate ligament dysplasia (PLD) and glaucoma in flat coated retrievers. I. Objectives, technique and results of a PLD study. Veterinary Ophthalmology 1998; 1: 85-90. Roberts, S.R., and Dellaporta, A., and Winter, F.C.: The collie ectasia syndrome. Pathology of the eyes of young and adult dogs. Am. J. Ophthalmol., 62:728, 1966. Roberts, S.R., Dellaporta, A., and Winter, F.C.: The collie ectasia syndrome. Pathologic alterations of the eyes of pups one to fourteen days of age. Am. J. Ophthalmol., 61:1458, 1966. Roberts, S.R.: The Collie eye anomaly. J. Am. Vet. Med. Assoc., 155:859, 1969. Schmidt, GM; Ellersieck, MR; et al. Inheritance of retinal dysplasia in the English springer spaniel. 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Journals Veterinary Ophthalmology (2002 onwards) Relevant articles in (2002 onwards) Journal of Small Animal Practice Veterinary Record 23. 24. 25. 26. 27. 28. 29. 30. 31. 32. 33. 34. 35. 36. 37. 38. 39. Procedure notes: Texts e.g. • • • • Cataract Either presumed inherited or non-inherited, congenital or acquired, non-physiological opacity of the lens and/or its capsule. Cataracts diagnosed in the period between birth and the 8th week of age are to be ticked in as congenital. Cataracts diagnosed at older age are to be ticked in as non-congenital (acquired). If there is distinct proof the cataract is congenital in origin (e.g. associated PPM),. the boxes for congenital and non-congenital cataracts can be ticked in. It is strongly recommended to draw the cataract in the "predrawings" on the certificate, as seen from the front (see separate instructions for drawing and filling the form). For the Scheme it is advised all bilateral or unilateral cataracts and especially cortical cataracts are presumed hereditary (see fig. 1 and 2), except: Procedure notes: • Cataract minor, clearly circumscribed cataracts e.g. located in the (posterior) suture lines (other than specifically described to be hereditary), or distinctly in the nucleus e.g. fibreglass/crystal-like (see fig. 3) cataracts in the nucleus (not to be confused with pulverulent-like cataracts, see fig. 4), or located, in/on (the back) of the posterior capsule as whitish "scar-ghosts" of the tunica vasculosa lentis, or in/on the anterior capsule associated with persistent pupillary membrane. In case of doubt (e.g. very minor cataracts in the cortex, in the posterior pole etc., only barely visible by the naked eye [thus not a microscope], using a slit lamp light beam) at least suspicious is given; this means the animal displays minor, but specific signs of the inherited disease(s) mentioned. Further change may confirm the diagnosis. Re-examination in .... months is advised. At least 6 months, but usually 12 months later the animal is re-examined, or, preferably examined at a panel meeting for further judgement. Procedure notes: Cataract • Unilateral minor, circumscribed cataracts located in the cortex, (such as e.g. punctate cataracts), developing at the age of 6 years, or later (with proof that the animal was unaffected at 5 years of age) are given “suspicious” and re-examination after 12 months. If there is no progression at that re-examination, the animal can be given unaffected for presumed inherited cataract. • To describe the type of cataract, the general box for presumed hereditary cataract and, if available, the specifying box for the type of cataract should be ticked. If there is e.g. a punctate cataract or a posterior polar cataract, (which both are generally cortical), the specifying box for that type is also to be ticked in. If there is e.g. a cortical and a nuclear cataract, all three boxes have to be ticked in. Lids Stades Lids • • • • • • ≈≡≠ ≥ ©®@≤ ≠♀♂≈