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Identification of Two Novel Variants in the LRP5 Gene that Cause Familial Exudative Vitreoretinopathy.

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Background: Familial exudative vitreoretinopathy (FEVR, OMIM 133780) is a severe inherited eye disease characterized by abnormal development of the retinal vasculature. Variants in the reported genes account for ∼50% of… Click to show full abstract

Background: Familial exudative vitreoretinopathy (FEVR, OMIM 133780) is a severe inherited eye disease characterized by abnormal development of the retinal vasculature. Variants in the reported genes account for ∼50% of total FEVR cases. However, the pathogenesis of other 50% of FEVR cases remains unclear. Therefore, it is crucial to identify novel variants responsible for the pathogenesis of FEVR. Aims: To find causative variants responsible for FEVR in two Han Chinses families. Materials and Methods: We recruited two families with two FEVR patients and applied exome sequencing on the genomic DNA samples from the probands. Sanger sequencing was performed for variant validation. Western blot analysis and luciferase assays were performed to test the expression levels and activity of mutant proteins. Results: We identified two novel missense variants in the LRP5 gene (NM_002335), namely c.1176 C > A (p.Asp392Glu) and c.2435 A>C (p.Asp812Ala), inherited in an autosomal dominant manner. Both variants significantly reduced Norrin/β-catenin signaling activity without affecting the expression of the LRP5 protein. Conclusion: This study expands the variant spectrum of the LRP5 gene for FEVR, providing valuable information for prenatal counseling and molecular diagnosis of FEVR.

Keywords: exudative vitreoretinopathy; novel variants; familial exudative; lrp5 gene; two novel; gene

Journal Title: Genetic testing and molecular biomarkers
Year Published: 2022

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