Mutational screening of AGRN, SLC39A5, SCO2, P4HA2, BSG, ZNF644, and CPSF1 in a Chinese cohort of 103 patients with nonsyndromic high myopia

PURPOSE: High myopia (HM) is one of the leading causes of irreversible vision loss in the world. Many myopia loci have been uncovered with linkage analysis, genome-wide association studies, and sequencing analysis. Numerous pathogenic genes within these loci have been detected in a portion of HM cas...

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Autores principales: Zheng, Yi-Han, Cai, Xue-Bi, Xia, Lu-Qi, Zhou, Fang-Yue, Wen, Xin-Ran, Chen, De-Fu, Han, Fang, Zhou, Kai-Jing, Jin, Zi-Bing, Zhuang, Wen-Juan, Lin, Bing
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Molecular Vision 2021
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8684808/
https://www.ncbi.nlm.nih.gov/pubmed/35002215
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author Zheng, Yi-Han
Cai, Xue-Bi
Xia, Lu-Qi
Zhou, Fang-Yue
Wen, Xin-Ran
Chen, De-Fu
Han, Fang
Zhou, Kai-Jing
Jin, Zi-Bing
Zhuang, Wen-Juan
Lin, Bing
author_facet Zheng, Yi-Han
Cai, Xue-Bi
Xia, Lu-Qi
Zhou, Fang-Yue
Wen, Xin-Ran
Chen, De-Fu
Han, Fang
Zhou, Kai-Jing
Jin, Zi-Bing
Zhuang, Wen-Juan
Lin, Bing
author_sort Zheng, Yi-Han
collection PubMed
description PURPOSE: High myopia (HM) is one of the leading causes of irreversible vision loss in the world. Many myopia loci have been uncovered with linkage analysis, genome-wide association studies, and sequencing analysis. Numerous pathogenic genes within these loci have been detected in a portion of HM cases. In the present study, we aimed to investigate the genetic basis of 103 patients with nonsyndromic HM, focusing on the reported causal genes. METHODS: A total of 103 affected individuals with nonsyndromic HM were recruited, including 101 patients with unrelated sporadic HM and a mother and son pair. All participants underwent comprehensive ophthalmic examinations, and genomic DNA samples were extracted from the peripheral blood. Whole exome sequencing was performed on the mother and son pair as well as on the unaffected father. Sanger sequencing was used to identify mutations in the remaining 101 patients. Bioinformatics analysis was subsequently applied to verify the mutations. RESULTS: An extremely rare mutation in AGRN (c.2627A>T, p.K876M) was identified in the mother and son pair but not in the unaffected father. Another two mutations in AGRN (c.4787C>T, p.P1596L/c.5056G>A, p.G1686S) were identified in two unrelated patients. A total of eight heterozygous variants potentially affecting the protein function were detected in eight of the remaining 99 patients, including c.1350delC, p.V451Cfs*76 and c.1023_1024insA, p.P342Tfs*41 in SLC39A5; c.244_246delAAG, p.K82del in SCO2; c.545A>G, p.Y182C in P4HA2; c.415C>T, p.P139S in BSG; c.3266A>G, p.Y1089C in ZNF644; and c.2252C>T, p.S751L and c.1708C>T, p.R570C in CPSF1. Multiple bioinformatics analyses were conducted, and a comparison to a group with geographically matched controls was performed, which supported the potential pathogenicity of these variants. CONCLUSIONS: We provide further evidence for the potential role of AGRN in HM inheritance and enlarged the current genetic spectrum of nonsyndromic HM by comprehensively screening the reported causal genes.
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spelling pubmed-86848082022-01-06 Mutational screening of AGRN, SLC39A5, SCO2, P4HA2, BSG, ZNF644, and CPSF1 in a Chinese cohort of 103 patients with nonsyndromic high myopia Zheng, Yi-Han Cai, Xue-Bi Xia, Lu-Qi Zhou, Fang-Yue Wen, Xin-Ran Chen, De-Fu Han, Fang Zhou, Kai-Jing Jin, Zi-Bing Zhuang, Wen-Juan Lin, Bing Mol Vis Research Article PURPOSE: High myopia (HM) is one of the leading causes of irreversible vision loss in the world. Many myopia loci have been uncovered with linkage analysis, genome-wide association studies, and sequencing analysis. Numerous pathogenic genes within these loci have been detected in a portion of HM cases. In the present study, we aimed to investigate the genetic basis of 103 patients with nonsyndromic HM, focusing on the reported causal genes. METHODS: A total of 103 affected individuals with nonsyndromic HM were recruited, including 101 patients with unrelated sporadic HM and a mother and son pair. All participants underwent comprehensive ophthalmic examinations, and genomic DNA samples were extracted from the peripheral blood. Whole exome sequencing was performed on the mother and son pair as well as on the unaffected father. Sanger sequencing was used to identify mutations in the remaining 101 patients. Bioinformatics analysis was subsequently applied to verify the mutations. RESULTS: An extremely rare mutation in AGRN (c.2627A>T, p.K876M) was identified in the mother and son pair but not in the unaffected father. Another two mutations in AGRN (c.4787C>T, p.P1596L/c.5056G>A, p.G1686S) were identified in two unrelated patients. A total of eight heterozygous variants potentially affecting the protein function were detected in eight of the remaining 99 patients, including c.1350delC, p.V451Cfs*76 and c.1023_1024insA, p.P342Tfs*41 in SLC39A5; c.244_246delAAG, p.K82del in SCO2; c.545A>G, p.Y182C in P4HA2; c.415C>T, p.P139S in BSG; c.3266A>G, p.Y1089C in ZNF644; and c.2252C>T, p.S751L and c.1708C>T, p.R570C in CPSF1. Multiple bioinformatics analyses were conducted, and a comparison to a group with geographically matched controls was performed, which supported the potential pathogenicity of these variants. CONCLUSIONS: We provide further evidence for the potential role of AGRN in HM inheritance and enlarged the current genetic spectrum of nonsyndromic HM by comprehensively screening the reported causal genes. Molecular Vision 2021-12-07 /pmc/articles/PMC8684808/ /pubmed/35002215 Text en Copyright © 2021 Molecular Vision. https://creativecommons.org/licenses/by-nc-nd/3.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited, used for non-commercial purposes, and is not altered or transformed.
spellingShingle Research Article
Zheng, Yi-Han
Cai, Xue-Bi
Xia, Lu-Qi
Zhou, Fang-Yue
Wen, Xin-Ran
Chen, De-Fu
Han, Fang
Zhou, Kai-Jing
Jin, Zi-Bing
Zhuang, Wen-Juan
Lin, Bing
Mutational screening of AGRN, SLC39A5, SCO2, P4HA2, BSG, ZNF644, and CPSF1 in a Chinese cohort of 103 patients with nonsyndromic high myopia
title Mutational screening of AGRN, SLC39A5, SCO2, P4HA2, BSG, ZNF644, and CPSF1 in a Chinese cohort of 103 patients with nonsyndromic high myopia
title_full Mutational screening of AGRN, SLC39A5, SCO2, P4HA2, BSG, ZNF644, and CPSF1 in a Chinese cohort of 103 patients with nonsyndromic high myopia
title_fullStr Mutational screening of AGRN, SLC39A5, SCO2, P4HA2, BSG, ZNF644, and CPSF1 in a Chinese cohort of 103 patients with nonsyndromic high myopia
title_full_unstemmed Mutational screening of AGRN, SLC39A5, SCO2, P4HA2, BSG, ZNF644, and CPSF1 in a Chinese cohort of 103 patients with nonsyndromic high myopia
title_short Mutational screening of AGRN, SLC39A5, SCO2, P4HA2, BSG, ZNF644, and CPSF1 in a Chinese cohort of 103 patients with nonsyndromic high myopia
title_sort mutational screening of agrn, slc39a5, sco2, p4ha2, bsg, znf644, and cpsf1 in a chinese cohort of 103 patients with nonsyndromic high myopia
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8684808/
https://www.ncbi.nlm.nih.gov/pubmed/35002215
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