非编码变异是导致隐性发育障碍与编码变异反式的罕见原因。

IF 6.6 1区 医学 Q1 GENETICS & HEREDITY
Jenny Lord , Carolina J. Oquendo , Htoo A. Wai , John G. Holloway , Alexandra Martin-Geary , Alexander J.M. Blakes , Elena Arciero , Silvia Domcke , Anne-Marie Childs , Karen Low , Julia Rankin , Genomics England Research Consortium, Diana Baralle , Hilary C. Martin , Nicola Whiffin
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引用次数: 0

摘要

目的:识别致病性非编码变异具有挑战性。在发育障碍(DD)患者的隐性基因中,通常会发现一个改变蛋白质的变异体,但这些变异体中致病性非编码 "二次命中 "的发生率尚不清楚:方法:我们从 100,000 基因组项目中的 4,073 个未确诊罕见病三组探查者中,在隐性 DD 相关基因中发现了罕见的杂合蛋白改变变异。我们在内含子、非翻译区(UTR)、启动子和候选增强子区中发现了另一个单倍型上的罕见非编码变异。我们对最重要的候选基因进行了表型匹配临床评估,并在可能的情况下进行了功能测试:我们在 2430 名受试者的隐性 DD 相关基因中发现了 3761 个罕见的杂合子功能缺失变异或 ClinVar 致病变异。在其中的 1366 例(36.3%)中,我们发现了至少一种罕见的反式非编码变异。通过生物信息学筛选和临床审查,我们发现其中有 7 个临床匹配度较高。经过详细的特征描述,我们确定了三个病例的可能诊断(GAA、NPHP3 和 PKHD1)和另外三个病例的候选诊断(PAH、LAMA2 和 IGHMBP2):我们开发了一种系统方法来发现涉及复合杂合编码/非编码变异的新诊断,并得出结论:这种机制可能是导致 DDs 的罕见原因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Noncoding variants are a rare cause of recessive developmental disorders in trans with coding variants

Purpose

Identifying pathogenic noncoding variants is challenging. A single protein-altering variant is often identified in a recessive gene in individuals with developmental disorders (DD), but the prevalence of pathogenic noncoding “second hits” in trans with these is unknown.

Methods

In 4073 genetically undiagnosed rare-disease trio probands from the 100,000 Genomes project, we identified rare heterozygous protein-altering variants in recessive DD-associated genes. We identified rare noncoding variants on the other haplotype in introns, untranslated regions, promoters, and candidate enhancer regions. We clinically evaluated the top candidates for phenotypic fit and performed functional testing where possible.

Results

We identified 3761 rare heterozygous loss-of-function or ClinVar pathogenic variants in recessive DD-associated genes in 2430 probands. For 1366 (36.3%) of these, we identified at least 1 rare noncoding variant in trans. Bioinformatic filtering and clinical review, revealed 7 to be a good clinical fit. After detailed characterization, we identified likely diagnoses for 3 probands (in GAA, NPHP3, and PKHD1) and candidate diagnoses in a further 3 (PAH, LAMA2, and IGHMBP2).

Conclusion

We developed a systematic approach to uncover new diagnoses involving compound heterozygous coding/noncoding variants and conclude that this mechanism is likely to be a rare cause of DDs.
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来源期刊
Genetics in Medicine
Genetics in Medicine 医学-遗传学
CiteScore
15.20
自引率
6.80%
发文量
857
审稿时长
1.3 weeks
期刊介绍: Genetics in Medicine (GIM) is the official journal of the American College of Medical Genetics and Genomics. The journal''s mission is to enhance the knowledge, understanding, and practice of medical genetics and genomics through publications in clinical and laboratory genetics and genomics, including ethical, legal, and social issues as well as public health. GIM encourages research that combats racism, includes diverse populations and is written by authors from diverse and underrepresented backgrounds.
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