遗传学决策的复杂性:PKD1 和 PKD2 基因中三种新型变异的注释。

IF 2.3 4区 医学 Q2 UROLOGY & NEPHROLOGY Nephron Pub Date : 2024-01-01 Epub Date: 2024-01-24 DOI:10.1159/000534969
Rui Barata, Liliana Rocha, Isabel Tavares, Odete Pereira, Filipa Carvalho, João Paulo Oliveira
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引用次数: 0

摘要

随着肾脏病学实践向精准医疗方向发展,基因检测越来越普及,临床肾脏病学家对基本基因知识的要求也越来越高。然而,根据基因检测结果做出决定却很少是简单明了的。我们报告了一名患有常染色体显性多囊肾病(ADPKD)的 37 岁女性,她被转诊接受单基因植入前基因检测(PGT-M)进行医学辅助生殖。对 PKD1 和 PKD2 基因进行了致病变异筛选。测序分析发现了三个新型错义单核苷酸变异,其中两个位于 PKD1 基因 - c.349T>G,p.(Leu117Val) 和 c.1736C>T,p.(Pro579Leu);第三个位于 PKD2 基因 - c.1124A>G,p.(Asn375Ser)。不同软件工具对这三个错义变异功能影响的生物信息学预测并不一致。家系分离分析是确定 PGT-M 相关变异的必备条件,它有力地证明了致病变异是 PKD1 c.349T>G p.(Leu117Val),而其他两个变异是非致病的,或最多是表型调节剂。证明新型变异体的致病性通常很复杂,但对于指导遗传咨询和筛查至关重要,尤其是在讨论高危夫妇后代一级预防的生殖替代方案时。本文报告的这个家族说明了 ADPKD 所面临的挑战,以及详细的家族史和分离分析对于正确注释新型变异体临床意义的重要性。遗传性肾脏疾病相关基因中的新型等位基因变异的基础遗传学知识和正确的临床注释对当代临床肾脏病学的实践越来越必要。
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The Complexity of Decisions in Genetics: Annotation of Three Novel Variants in the PKD1 and PKD2 Genes.

As nephrology practice is evolving toward precision medicine, and genetic tests are becoming widely available, basic genetic literacy is increasingly required for clinical nephrologists. Yet, decisions based on results of genetic tests are seldom straightforward. We report a 37-year-old woman with autosomal dominant polycystic kidney disease (ADPKD) who was referred for medically assisted reproduction with monogenic preimplantation genetic testing (PGT-M). The PKD1 and PKD2 genes were screened for pathogenic variants. Sequencing analysis revealed the presence of three novel missense single nucleotide variants, two in the PKD1 gene - c.349T>G, p.(Leu117Val) and c.1736C>T, p.(Pro579Leu); and the third in the PKD2 gene - c.1124A>G, p.(Asn375Ser). Bioinformatic predictions of the functional effects of those three missense variants were inconsistent across different software tools. The family segregation analysis, which was mandatory to identify the relevant variant(s) for PGT-M, strongly supported that the disease-causing variant was PKD1 c.349T>G p.(Leu117Val), while the other two were nonpathogenic or, at most, phenotypic modulators. Proving the pathogenicity of novel variants is often complex but is critical to guide genetic counseling and screening, particularly when discussing reproductive alternatives for primary prevention in the progeny of at-risk couples. The family reported herein illustrates those challenges in the setting of ADPKD, and the invaluable importance of a detailed family history and segregation analysis for proper clinical annotation of novel variants. Basic genetic knowledge and proper clinical annotation of novel allelic variants in genes associated with hereditary kidney disorders are increasingly necessary for the contemporary practice of clinical nephrology.

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来源期刊
Nephron
Nephron UROLOGY & NEPHROLOGY-
CiteScore
5.00
自引率
0.00%
发文量
80
期刊介绍: ''Nephron'' comprises three sections, which are each under the editorship of internationally recognized leaders and served by specialized Associate Editors. Apart from high-quality original research, ''Nephron'' publishes invited reviews/minireviews on up-to-date topics. Papers undergo an innovative and transparent peer review process encompassing a Presentation Report which assesses and summarizes the presentation of the paper in an unbiased and standardized way.
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