CONCOMITANT MUTATIONS IN INHERITED RETINAL DYSTROPHIES

先证者 ABCA4型 复合杂合度 基因检测 基因 系谱图 色素性视网膜炎 生物 突变 遗传咨询 遗传学 表型
作者
Ana Rodríguez‐Muñoz,Belén García‐Bohórquez,Patricia Udaondo,Ana Hervás-Ontiveros,David G. Charteris,Elena Aller,Teresa Jaijo,Gema García‐García,José M. Millán
出处
期刊:Retina-the Journal of Retinal and Vitreous Diseases [Ovid Technologies (Wolters Kluwer)]
卷期号:41 (9): 1966-1975 被引量:2
标识
DOI:10.1097/iae.0000000000003103
摘要

Purpose: To highlight the challenge of correct reproductive and therapeutic counseling in complex pedigrees with different inherited retinal dystrophies (IRD). Methods: Two hundred eight patients diagnosed with nonsyndromic IRD underwent full ophthalmologic examination and molecular analysis using targeted next-generation sequencing. Results: Five families (4%) carried mutations in more than one gene that contribute to different IRD. Family fRPN-NB had a dominant mutation in SNRNP200 , which was present in nine affected individuals and four unaffected, and a mutation in RP2 among 11 family members. Family fRPN-142 carried a mutation in RPGR that cosegregated with the disease in all affected individuals. In addition, the proband also harbored two disease-causing mutations in the genes BEST1 and SNRNP200 . Family fRPN-169 beared compound heterozygous mutations in USH2A and a dominant mutation in RP1 . Genetic testing of fRPN-194 determined compound heterozygous mutations in CNGA3 and a dominant mutation in PRPF8 only in the proband. Finally, fRPN-219 carried compound heterozygous mutations in the genes ABCA4 and TYR . Conclusion: These findings reinforce the complexity of IRD and underscore the need for the combination of high-throughput genetic testing and clinical characterization. Because of these features, the reproductive and therapeutic counseling for IRD must be approached with caution.
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