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J Am Soc Nephrol. 2021 Sep;32(9):2273-2290. doi: 10.1681/ASN.2020071065. Epub 2021 Jun 18.
2
Pathogenic Variants in the Genes Affected in Alport Syndrome (COL4A3-COL4A5) and Their Association With Other Kidney Conditions: A Review.致病变异在 Alport 综合征(COL4A3-COL4A5)相关基因中的作用及其与其他肾脏疾病的关系:综述。
Am J Kidney Dis. 2021 Dec;78(6):857-864. doi: 10.1053/j.ajkd.2021.04.017. Epub 2021 Jul 8.
3
Consensus statement on standards and guidelines for the molecular diagnostics of Alport syndrome: refining the ACMG criteria.关于 Alport 综合征分子诊断标准和指南的共识声明:完善 ACMG 标准。
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杂合致病性变异(常染色体显性遗传性阿尔波特综合征)很常见,且通常与终末期肾衰竭、听力损失或眼部异常无关。

Heterozygous Pathogenic and Variants (Autosomal Dominant Alport Syndrome) Are Common, and Not Typically Associated With End-Stage Kidney Failure, Hearing Loss, or Ocular Abnormalities.

作者信息

Savige Judy

机构信息

Department of Medicine (Melbourne Health and Northern Health), Royal Melbourne Hospital, The University of Melbourne, Parkville, Victoria, Australia.

出版信息

Kidney Int Rep. 2022 Jun 7;7(9):1933-1938. doi: 10.1016/j.ekir.2022.06.001. eCollection 2022 Sep.

DOI:10.1016/j.ekir.2022.06.001
PMID:36090501
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9458992/
Abstract

The term "autosomal dominant (AD) Alport syndrome" is often used to describe the condition associated with heterozygous pathogenic or variants and has largely replaced "thin basement membrane nephropathy (TBMN)." AD Alport syndrome implies that affected individuals develop end-stage kidney failure (ESKF) as well as the typical Alport hearing loss and ocular abnormalities, but these features have been considered rare with TBMN. Recent studies suggest that ESKF occurs in 14% to 30% of those with heterozygous pathogenic or variants but confirm that the hearing loss and ocular defects occur uncommonly if at all. Uncertainty over the risk of ESKF has persisted. However all the cited studies of heterozygous pathogenic or variants and kidney failure are from hospital-based patients and thus biased toward more severe disease. Multiple unselected cohorts with ESKF have found heterozygous pathogenic variants in and occur about as often as variants, which suggests that AD Alport syndrome causes ESKF as often as X-linked (XL) disease. In the normal population, heterozygous pathogenic and variants are present 20 times more often than variants. Therefore, AD Alport syndrome is complicated by ESKF 20 times often than XL disease and occurs in fewer than 3% of those with pathogenic or variants by the age of 60. Nevertheless, individuals with heterozygous pathogenic or variants referred to a hospital are still more likely to develop impaired kidney function than those who remain at home undiagnosed.

摘要

术语“常染色体显性(AD)遗传性肾炎综合征”常用于描述与杂合致病性或变异相关的病症,并且在很大程度上已取代了“薄基底膜肾病(TBMN)”。AD遗传性肾炎综合征意味着受影响的个体发展为终末期肾衰竭(ESKF)以及典型的遗传性肾炎听力损失和眼部异常,但这些特征在TBMN中被认为是罕见的。最近的研究表明,14%至30%的杂合致病性或变异患者会出现ESKF,但证实听力损失和眼部缺陷即使出现也不常见。ESKF风险的不确定性一直存在。然而,所有引用的关于杂合致病性或变异与肾衰竭的研究均来自住院患者,因此偏向于病情更严重的疾病。多个未经选择的ESKF队列发现,杂合致病性变异在[具体基因名称1]和[具体基因名称2]中的出现频率与[另一基因名称]变异大致相同,这表明AD遗传性肾炎综合征导致ESKF的频率与X连锁(XL)疾病相同。在正常人群中,杂合致病性[具体基因名称1]和[具体基因名称2]变异的出现频率比[另一基因名称]变异高20倍。因此,AD遗传性肾炎综合征并发ESKF的频率是XL疾病的20倍,并且在60岁时,致病性或变异患者中不到3%会出现这种情况。然而,转诊至医院的杂合致病性或变异个体仍比未被诊断而居家的个体更有可能出现肾功能损害。