APOL1 and APOL1-Associated Kidney Disease: A Common Disease, an Unusual Disease Gene - Proceedings of the Henry Shavelle Professorship.

Glomerular diseases Pub Date : 2023-01-01 DOI:10.1159/000529227

Martin R Pollak, David J Friedman

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引用次数: 3

Abstract

Background: Genetic variants in APOL1 are a major contributor to the increased risk of kidney disease in people of recent African ancestry.

Summary: Two alleles in the APOL1 gene, referred to as G1 and G2, confer increased risk of kidney disease under a recessive model of risk inheritance. Disease risk is inherited as a recessive trait: People with genotypes G1/G1, G2/G2, and G1/G2 (i.e., a risk allele from each parent) have increased risk for what we refer to here as APOL1-associated kidney disease. In the USA, about 13% of the self-identified African-American population has a high-risk genotype. As we discuss below, APOL1 is an unusual disease gene. Most studies to date have suggested that the G1 and G2 variants have toxic, gain-of-function effects on the encoded protein.

Key message: In this article, we review key concepts critical to understanding APOL1-associated kidney disease, emphasizing ways in which it is highly atypical for a human disease-causing gene.

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APOL1和APOL1相关的肾脏疾病:一种常见疾病，一种不寻常的疾病基因- Henry Shavelle教授会议记录。

背景:APOL1的遗传变异是近期非洲血统人群肾脏疾病风险增加的主要因素。摘要:APOL1基因中的两个等位基因G1和G2在风险遗传的隐性模型下增加了肾脏疾病的风险。疾病风险作为一种隐性特征遗传:基因型为G1/G1、G2/G2和G1/G2的人(即来自父母双方的风险等位基因)患apol1相关肾病的风险增加。在美国，大约13%的自我认定的非裔美国人有高风险基因型。正如我们下面讨论的，APOL1是一种不寻常的疾病基因。迄今为止，大多数研究表明G1和G2变异对编码蛋白具有毒性和功能获得效应。关键信息:在本文中，我们回顾了对理解apol1相关肾脏疾病至关重要的关键概念，强调了它在人类致病基因中是非典型的方式。

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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Glomerular diseases

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