Target 5000: a standardized all-Ireland pathway for the diagnosis and management of inherited retinal degenerations

Kirk A J Stephenson; Julia Zhu; Niamh Wynne; Adrian Dockery; Rebecca M Cairns; Emma Duignan; Laura Whelan; Conor P Malone; Hilary Dempsey; Karen Collins; Shana Routledge; Rajiv Pandey; Elaine Crossan; Jacqueline Turner; James J O'Byrne; Laura Brady; Giuliana Silvestri; Paul F Kenna; G Jane Farrar; David J Keegan

doi:10.1186/s13023-021-01841-1

Target 5000: a standardized all-Ireland pathway for the diagnosis and management of inherited retinal degenerations

Orphanet J Rare Dis. 2021 May 5;16(1):200. doi: 10.1186/s13023-021-01841-1.

Authors

Kirk A J Stephenson¹, Julia Zhu², Niamh Wynne³, Adrian Dockery⁴, Rebecca M Cairns⁵, Emma Duignan³, Laura Whelan⁴, Conor P Malone³, Hilary Dempsey³, Karen Collins³, Shana Routledge², Rajiv Pandey², Elaine Crossan^{2

6}, Jacqueline Turner², James J O'Byrne², Laura Brady⁷, Giuliana Silvestri⁵, Paul F Kenna^{3

4}, G Jane Farrar⁴, David J Keegan²

Affiliations

¹ Mater Clinical Ophthalmic Genetics Unit, Mater Misericordiae University Hospital, Dublin, Ireland. kirkstephenson@hotmail.com.
² Mater Clinical Ophthalmic Genetics Unit, Mater Misericordiae University Hospital, Dublin, Ireland.
³ The Research Foundation, Royal Victoria Eye and Ear Hospital, Dublin, Ireland.
⁴ Ocular Genetics Unit, Smurfit Institute of Genetics, Trinity College Dublin, Dublin, Ireland.
⁵ Belfast Health and Social Care Trust Hospitals, Belfast, Northern Ireland.
⁶ National Council for the Blind of Ireland, Whitworth Road, Dublin 9, Ireland.
⁷ Fighting Blindness Ireland, Ely Place, Dublin 2, Ireland.

Abstract

Introduction: Inherited retinal degenerations (IRD) are rare genetic disorders with > 300 known genetic loci, manifesting variably progressive visual dysfunction. IRDs were historically underserved due to lack of effective interventions. Many novel therapies will require accurate diagnosis (phenotype and genotype), thus an efficient and effective pathway for assessment and management is required.

Methods: Using surveys of existing practice patterns and advice from international experts, an all-Ireland IRD service (Target 5000) was designed. Detailed phenotyping was followed by next generation genetic sequencing in both a research and accredited laboratory. Unresolved pedigrees underwent further studies (whole gene/whole exome/whole genome sequencing). Novel variants were interrogated for pathogenicity (cascade screening, in silico analysis, functional studies). A multidisciplinary team (MDT; ophthalmologists, physicians, geneticists, genetic counsellors) reconciled phenotype with genotype. A bespoke care plan was created for each patient comprising supports, existing interventions, and novel therapies/clinical trials.

Results and discussion: Prior to Target 5000, a significant cohort of patients were not engaged with healthcare/support services due to lack of effective interventions. Pathogenic or likely pathogenic variants in IRD-associated genes were detected in 62.3%, with 11.6% having variants of unknown significance. The genotyping arm of Target 5000 allowed a 42.73% cost saving over independent testing, plus the value of MDT expertise/processing. Partial funding has transferred from charitable sources to government resources.

Conclusion: Target 5000 demonstrates efficacious and efficient clinical/genetic diagnosis, while discovering novel IRD-implicated genes/variants and investigating mechanisms of disease and avenues of intervention. This model could be used to develop similar IRD programmes in small/medium-sized nations.

Keywords: Clinical diagnostic algorithm; Genetic diagnosis; Inherited retinal degenerations; Ocular genetics; Public and patient involvement; Retinal dystrophy.

Publication types

Letter
Research Support, Non-U.S. Gov't

MeSH terms

Exome
Humans
Ireland
Mutation
Pedigree
Retinal Degeneration*
Retinal Dystrophies* / genetics