在RNA外泌体中建模致病变异。

RNA & disease (Houston, Tex.) Pub Date : 2020-01-01
Julia de Amorim, Anne Slavotinek, Milo B Fasken, Anita H Corbett, Derrick J Morton
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引用次数: 0

摘要

外泌体病是由编码RNA外泌体复合物(EXOSC)结构亚基的基因突变引起的一系列罕见疾病。RNA外泌体对于加工和降解许多RNA靶标至关重要。单个RNA外泌体亚基基因(称为EXOSC基因)的突变与多种不同的疾病有关。这些外泌体病不是由纯合子功能丧失或EXOSC基因的大量缺失引起的,可能是因为某种水平的RNA外泌体活性对生存能力至关重要。因此,迄今为止所描述的所有患者至少有一个等位基因具有编码RNA外泌体亚基的错义突变,该突变具有与疾病相关的单个致病性氨基酸变化。了解这些变化如何导致这类疾病的不同临床表现,需要研究个体致病性错义变异体如何改变RNA外泌体功能。这样的研究将需要获得患者样本,这对这些非常罕见的疾病来说是一个挑战,再加上对患者变异进行建模。在这里,我们重点介绍了最近的五项研究,这些研究模拟了EXOSC3、EXOSC2和EXOSC5的致病变异。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Modeling Pathogenic Variants in the RNA Exosome.

Exosomopathies are a collection of rare diseases caused by mutations in genes that encode structural subunits of the RNA exosome complex (EXOSC). The RNA exosome is critical for both processing and degrading many RNA targets. Mutations in individual RNA exosome subunit genes (termed EXOSC genes) are linked to a variety of distinct diseases. These exosomopathies do not arise from homozygous loss-of-function or large deletions in the EXOSC genes likely because some level of RNA exosome activity is essential for viability. Thus, all patients described so far have at least one allele with a missense mutation encoding an RNA exosome subunit with a single pathogenic amino acid change linked to disease. Understanding how these changes lead to the disparate clinical presentations that have been reported for this class of diseases necessitates investigation of how individual pathogenic missense variants alter RNA exosome function. Such studies will require access to patient samples, a challenge for these very rare diseases, coupled with modeling the patient variants. Here, we highlight five recent studies that model pathogenic variants in EXOSC3, EXOSC2, and EXOSC5.

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