When is it MODY? Challenges in the Interpretation of Sequence Variants in MODY Genes.

Q3 Medicine Review of Diabetic Studies Pub Date : 2015-09-01 Epub Date: 2016-02-10 DOI:10.1900/RDS.2015.12.330
Sara Althari, Anna L Gloyn
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引用次数: 21

Abstract

The genomics revolution has raised more questions than it has provided answers. Big data from large population-scale resequencing studies are increasingly deconstructing classic notions of Mendelian disease genetics, which support a simplistic correlation between mutational severity and phenotypic outcome. The boundaries are being blurred as the body of evidence showing monogenic disease-causing alleles in healthy genomes, and in the genomes of individu-als with increased common complex disease risk, continues to grow. In this review, we focus on the newly emerging challenges which pertain to the interpretation of sequence variants in genes implicated in the pathogenesis of maturity-onset diabetes of the young (MODY), a presumed mono-genic form of diabetes characterized by Mendelian inheritance. These challenges highlight the complexities surrounding the assignments of pathogenicity, in particular to rare protein-alerting variants, and bring to the forefront some profound clinical diagnostic implications. As MODY is both genetically and clinically heterogeneous, an accurate molecular diagnosis and cautious extrapolation of sequence data are critical to effective disease management and treatment. The biological and translational value of sequence information can only be attained by adopting a multitude of confirmatory analyses, which interrogate variant implication in disease from every possible angle. Indeed, studies which have effectively detected rare damaging variants in known MODY genes in normoglycemic individuals question the existence of a sin-gle gene mutation scenario: does monogenic diabetes exist when the genetic culprits of MODY have been systematical-ly identified in individuals without MODY?

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什么时候是莫迪?MODY基因序列变异解释的挑战。
基因组学革命提出的问题比它提供的答案要多。来自大规模人群重测序研究的大数据正日益解构孟德尔疾病遗传学的经典概念,孟德尔疾病遗传学支持突变严重程度与表型结果之间的简单相关性。随着显示健康基因组和常见复杂疾病风险增加的个体基因组中存在单基因致病等位基因的证据不断增加,界限正在变得模糊。在这篇综述中,我们将重点关注与年轻人成熟型糖尿病(MODY)发病机制相关的基因序列变异解释相关的新挑战,MODY是一种以孟德尔遗传为特征的单基因糖尿病。这些挑战突出了围绕致病性分配的复杂性,特别是罕见的蛋白质警报变异体,并将一些深刻的临床诊断意义带到了最前沿。由于MODY具有遗传和临床异质性,准确的分子诊断和谨慎的序列数据外推对于有效的疾病管理和治疗至关重要。序列信息的生物学和翻译价值只能通过采用大量的验证性分析来获得,这些分析从各个可能的角度询问变异在疾病中的含义。事实上,在血糖正常的个体中有效检测到已知MODY基因中罕见的破坏性变异的研究质疑了单基因突变的存在:当在没有MODY的个体中系统地确定了MODY的遗传罪魁祸首时,是否存在单基因糖尿病?
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Review of Diabetic Studies
Review of Diabetic Studies Medicine-Internal Medicine
CiteScore
1.80
自引率
0.00%
发文量
28
期刊介绍: The Review of Diabetic Studies (RDS) is the society"s peer-reviewed journal published quarterly. The purpose of The RDS is to support and encourage research in biomedical diabetes-related science including areas such as endocrinology, immunology, epidemiology, genetics, cell-based research, developmental research, bioengineering and disease management.
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