A genetic investigation in five Chinese families with keratoconus

Qinghong Lin; Xuejun Wang; Xiaoliao Peng; Tian Han; Ling Sun; Xiaoyu Zhang; Xingtao Zhou

doi:10.7717/peerj.18037

PeerJ (Sep 2024)

A genetic investigation in five Chinese families with keratoconus

Qinghong Lin,
Xuejun Wang,
Xiaoliao Peng,
Tian Han,
Ling Sun,
Xiaoyu Zhang,
Xingtao Zhou

Affiliations

Qinghong Lin: Department of Ophthalmology, Eye and ENT Hospital of Fudan University, Shanghai, China
Xuejun Wang: Department of Ophthalmology, Eye and ENT Hospital of Fudan University, Shanghai, China
Xiaoliao Peng: Department of Ophthalmology, Eye and ENT Hospital of Fudan University, Shanghai, China
Tian Han: Department of Ophthalmology, Eye and ENT Hospital of Fudan University, Shanghai, China
Ling Sun: Department of Ophthalmology, Eye and ENT Hospital of Fudan University, Shanghai, China
Xiaoyu Zhang: Department of Ophthalmology, Eye and ENT Hospital of Fudan University, Shanghai, China
Xingtao Zhou: Department of Ophthalmology, Eye and ENT Hospital of Fudan University, Shanghai, China

DOI: https://doi.org/10.7717/peerj.18037
Journal volume & issue: Vol. 12
p. e18037

Abstract

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Background This study investigated the genetic characteristics of five Chinese families with keratoconus (KC). Methods In the five families affected by KC, medical records, clinical observations, and blood samples were collected from all individuals. All KC family members (n = 20) underwent both whole exome sequencing of genomic DNA and Sanger sequencing to confirm the variants. Online software was utilized to analyze all variants, and the online server I-TASSER was employed for in silico predictions of the three-dimensional protein structures of the variants. The newly discovered variants and single nucleotide polymorphisms were further examined in 322 sporadic KC patients. Results The Pentacam tomographic composite index in those affected first-degree family members of the probands showed a pathological change. Five new variants were detected in the five probands and other affected members in their families: a heterozygous missense variant g.19043832C>T (p.Ser145Asn) in the homer scaffolding protein 3 (HOMER3) gene; a heterozygous missense variant g.99452113G>A (p.Gly483Arg) in the insulin-like growth factor 1 receptor (IGF1R) gene; a heterozygous missense variant g.55118280G>T (p.Trp843Leu) in the echinoderm microtubule-associated protein like 6 (EML6) gene; a heterozygous frameshift variant c. 1226_1227del (p.Gln410Glufs*17) in the DOP1 leucine zipper-like protein B (DOP1B) gene; and a heterozygous splice-site variant c.7776+2T>A in the neurobeachin-like protein 2 (NBEAL2) gene. These variations were predicted to be potentially pathogenic and associated with KC. Conclusion Five novel variants in HOMER3, IGF1R, EML6, DOP1B, and NBEAL2 genes were identified in this study and may be associated with the pathogenesis of KC. This study provides new information about the gene variants and their protein changes in KC patients. The findings should be explored further and could potentially be applied to the early diagnosis of KC before clinical onset.

Published in PeerJ

ISSN: 2167-8359 (Online)
Publisher: PeerJ Inc.
Country of publisher: United States
LCC subjects: Medicine; Science: Biology (General)
Website: https://peerj.com/

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