使用ClinGen指南重新评估意义不确定的纤维蛋白-1基因变体。

IF 4 2区 医学 Q1 MEDICAL LABORATORY TECHNOLOGY
Annals of Laboratory Medicine Pub Date : 2024-05-01 Epub Date: 2023-10-16 DOI:10.3343/alm.2023.0152
Seo Wan Kim, Boyeon Kim, Yoonjung Kim, Kyung-A Lee
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引用次数: 0

摘要

背景:马凡氏综合征(MFS)是由原纤维蛋白-1基因(FBN1)变异引起的。FBN1的突变热点和/或公认的关键功能结构域包括半胱氨酸残基、钙结合共有序列和与结构域间包装相关的氨基酸。以前的变异解释指南没有反映基因或相关疾病的特征。利用临床基因组资源(ClinGen)FBN1变异管理专家小组(VCEP),我们重新评估了作为不确定显著性变异(VUSs)报告的FBN1种系变异。我们检查了人类基因组突变数据库、ClinVar和VarSome数据库中的变体,并使用gnomAD数据库评估了它们的等位基因频率。回顾了患者的临床信息。结果:四种影响半胱氨酸的错义变体(c.460T>c,c.1006T>c、c.5330G>c和c.8020T>c)被重新归类为可能的致病性变体,并被分配为PM1_strong或PM1。通过授予BA1(独立),两个内含子变体被重新归类为良性。四个错义变体被重新分类为可能的良性变体。BP5标准适用于具有其他疾病分子基础的病例,其中一个(c.7231G>A)与致病性新发COL3A1变体(c.1988G>T,p.Gly633Val)一起被发现。结论:考虑到FBN1变体的高外显率和MFS的临床变异性,检测致病性变体很重要。ClinGen FBN1 VCEP包含突变热点和/或公认的关键功能域,并专门针对MFS调整标准;因此,它不仅有利于识别致病性FBN1变体,而且有利于将这些变体与引起其他具有重叠临床特征的结缔组织疾病的变体区分开来。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Re-evaluation of a Fibrillin-1 Gene Variant of Uncertain Significance Using the ClinGen Guidelines.

Background: Marfan syndrome (MFS) is caused by fibrillin-1 gene (FBN1) variants. Mutational hotspots and/or well-established critical functional domains of FBN1 include cysteine residues, calcium-binding consensus sequences, and amino acids related to interdomain packaging. Previous guidelines for variant interpretation do not reflect the features of genes or related diseases. Using the Clinical Genome Resource (ClinGen) FBN1 variant curation expert panel (VCEP), we re-evaluated FBN1 germline variants reported as variants of uncertain significance (VUSs).

Methods: We re-evaluated 26 VUSs in FBN1 reported in 161 patients with MFS. We checked the variants in the Human Genome Mutation Database, ClinVar, and VarSome databases and assessed their allele frequencies using the gnomAD database. Patients' clinical information was reviewed.

Results: Four missense variants affecting cysteines (c.460T>C, c.1006T>C, c.5330G>C, and c.8020T>C) were reclassified as likely pathogenic and were assigned PM1_strong or PM1. Two intronic variants were reclassified as benign by granting BA1 (stand-alone). Four missense variants were reclassified as likely benign. BP5 criteria were applied in cases with an alternate molecular basis for disease, one of which (c.7231G>A) was discovered alongside a pathogenic de novo COL3A1 variant (c.1988G>T, p.Gly633Val).

Conclusions: Considering the high penetrance of FBN1 variants and clinical variability of MFS, the detection of pathogenic variants is important. The ClinGen FBN1 VCEP encompasses mutational hotspots and/or well-established critical functional domains and adjusts the criteria specifically for MFS; therefore, it is beneficial not only for identifying pathogenic FBN1 variants but also for distinguishing these variants from those that cause other connective tissue disorders with overlapping clinical features.

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来源期刊
Annals of Laboratory Medicine
Annals of Laboratory Medicine MEDICAL LABORATORY TECHNOLOGY-
CiteScore
8.30
自引率
12.20%
发文量
100
审稿时长
6-12 weeks
期刊介绍: Annals of Laboratory Medicine is the official journal of Korean Society for Laboratory Medicine. The journal title has been recently changed from the Korean Journal of Laboratory Medicine (ISSN, 1598-6535) from the January issue of 2012. The JCR 2017 Impact factor of Ann Lab Med was 1.916.
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