Pathonign variants in recessive disorders: How extremely hypomorphic variants can be pathogenic and benign depending on the allele in trans.

IF 1.6 Q2 MEDICINE, GENERAL & INTERNAL

Intractable & rare diseases research Pub Date : 2025-05-31 DOI:10.5582/irdr.2025.01014

Alexandre Fabre, Paul Guerry

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引用次数: 0

Abstract

In recessive monogenic diseases, individuals with a single pathogenic variant are typically asymptomatic and symptomatic disease is only observed in patients with two pathogenic variants. Assuming that disease only occurs where protein concentrations or activity are below 50% of normal (since in recessive diseases, most carriers are asymptomatic) some hypomorphic variants could be deleterious in association with a LoF variant, but nevertheless yield > 50% protein activity/concentration when homozygous. These types of variants would be very weakly eliminated by natural selection, if at all, and thus their frequency in the population could increase by genetic drift. Thus the population frequency criterion often used to qualify variants as benign would be misleading. One such variant may be c.5603A>T (p.Asn1868Ile), in ABCA4 (which causes Stargardt disease-1). This variant is pathogenic in trans with a null or missense variant but not when homozygous. We refer to these variants using the blend word "pathonign", since they are simultaneously pathogenic and benign in the population.

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隐性疾病的致病变异：如何根据反式中的等位基因极端次形变异可能是致病的和良性的。

在隐性单基因疾病中，具有单一致病变异的个体通常无症状，只有在具有两种致病变异的患者中才观察到有症状的疾病。假设疾病只发生在蛋白质浓度或活性低于正常水平50%的地方（因为在隐性疾病中，大多数携带者是无症状的），一些与LoF变异相关的半胚变异可能是有害的，但当纯合子时，蛋白质活性/浓度仍为50%。如果有的话，这些类型的变异在自然选择中会被非常微弱地消除，因此它们在种群中的频率可能会通过遗传漂变而增加。因此，通常用于将变异限定为良性的种群频率标准将具有误导性。其中一种变异可能是ABCA4中的c.5603A >t (p.Asn1868Ile)（引起Stargardt病1）。这种变异与空或错义变异反式致病，但纯合时不致病。我们使用混合词“致病”来指代这些变异，因为它们在人群中同时具有致病性和良性。

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

Intractable & rare diseases research MEDICINE, GENERAL & INTERNAL-

CiteScore

2.10

自引率

0.00%

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