利用全外显子组测序揭示非综合征性白化病的遗传学机制：TYR、TYRP1、OCA2 和 MC1R 基因在 17 个家系中的综合研究。

Unveiling genetics of non-syndromic albinism using whole exome sequencing: A comprehensive study of TYR, TYRP1, OCA2 and MC1R genes in 17 families.

机构信息

Department of Zoology, Government Postgraduate College Dargai, Malakand 23050, Pakistan; Higher Education Department, Peshawar 25120, Government of Khyber Pakhtunkhwa, Pakistan; Department of Zoology, Abdul Wali Khan University, Mardan 23200, Pakistan.

Department of Zoology, Government Postgraduate College Dargai, Malakand 23050, Pakistan.

出版信息

Gene. 2024 Feb 5;894:147986. doi: 10.1016/j.gene.2023.147986. Epub 2023 Nov 11.

DOI:10.1016/j.gene.2023.147986

PMID:37956964

Abstract

BACKGROUND

Oculocutaneous albinism (OCA) is a group of skin depigmentation disorders. Clinical presentation of OCA includes defects in melanocyte differentiation, melanin biosynthesis, and melanosome maturation and transport.

OBJECTIVES

A molecular diagnostics study of families presenting oculocutaneous albinism.

METHODS

In this study, 17 consanguineous OCA families consisting of 93 patients were investigated. Whole Exome Sequencing (WES) of the index patient in each family were performed. Short listed variants of WES were Sanger validated for Mendelian segregation in obligate carriers and other available family members. Variant prioritization and pathogenicity were classified as per the criteria of American College Medical Genetics and Genomics (ACMG). Comparative computational modelling was performed to predict the potential damaging effect of the altered proteins.

RESULTS

15 pathogenic variations: c.132 T > A, c.346C > T, c.488C > G, c.1037G > A in TYR, c.1211C > T, c.1441G > A, c.1706_1707insT, c.2020C > G, c.2402G > C, c.2430del, in OCA2, c.1067G > A in TYRP1 and c.451C > T, c.515G > T, c.766C > T, c.917G > A in MC1R genes were identified. Three variants in OCA2 gene were characterized: c.1706_1707insT, c.2430del, and c.2402G > C, all of which were not reported before in OCA families.

CONCLUSION

A few studies focusing on mutation screening of OCA patients have been reported before; however, this study has uniquely presents the Pakhtun ethnic population residing on the North-Western boarder. It explains that TYR, OCA2, TYRP1, and MC1R variations lead to non-syndromic OCA phenotype The overlapping phenotypes of OCA can precisely be diagnosed for its molecular pathogenicity using WES. This study recommends WES as a first-line molecular diagnostic tool, and provides a basis for developing customized genetic tests i.e. pre-marital screening to reduce the disease burden in the future generations.

摘要

背景

眼皮肤白化病（OCA）是一组皮肤色素减退疾病。OCA 的临床表现包括黑素细胞分化、黑色素生物合成以及黑素小体成熟和运输缺陷。

目的

对表现出眼皮肤白化病的家系进行分子诊断研究。

方法

本研究纳入了 17 个由 93 例患者组成的近亲白化病家系。对每个家系的先证者进行全外显子组测序（WES）。对 WES 的短名单变体进行 Sanger 测序，以验证强制性携带者和其他可利用的家族成员中的孟德尔分离。根据美国医学遗传学与基因组学学院（ACMG）的标准对变体进行优先级排序和致病性分类。进行比较计算建模以预测改变的蛋白质的潜在破坏性影响。

结果

发现 15 个致病性变异：TYR 基因中的 c.132T>A、c.346C>T、c.488C>G、c.1037G>A、c.1211C>T、c.1441G>A、c.1706_1707insT、c.2020C>G、c.2402G>C、c.2430del、OCA2 基因中的 c.1067G>A、TYRP1 基因中的 c.451C>T、c.515G>T、c.766C>T、c.917G>A，这是首次在 OCA 家系中发现。OCA2 基因中的 3 个变体 c.1706_1707insT、c.2430del 和 c.2402G>C 以前没有在 OCA 家系中报道过。

结论

以前有一些关于 OCA 患者突变筛查的研究，但本研究独特地呈现了居住在西北边境的普什图族人群。它表明 TYR、OCA2、TYRP1 和 MC1R 的变异导致非综合征性 OCA 表型。使用 WES 可以精确地对重叠的 OCA 表型进行分子发病机制诊断。本研究建议 WES 作为一线分子诊断工具，并为开发定制的遗传测试（例如婚前筛查）提供依据，以减少未来几代人的疾病负担。