[Clinical and genetic characteristics of a case of primary ciliary dyskinesia caused by new frameshift mutation of the DNAH5 gene].

Q4 Medicine

中华男科学杂志 Pub Date : 2024-01-01

Meng-Yang Li, Shan Huang, Li-Na Ma, An-Cong Wang

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引用次数: 0

Abstract

Objective: To investigate the clinical and genetic characteristics of a case of primary ciliary dyskinesia (PCD).

Methods: We collected the clinical data on a case of PCD treated in the Department of Reproductive Medicine of Linyi People's Hospital in July 2020, detected the genes of the patient by whole-exome sequencing (WES), verified the candidate mutations by Sanger sequencing, and predicted the protein structure of the mutant gene by SWISS-MODEL.

Results: The proband was found with the clinical phenotypes of chronic rhinitis, bronchiectasis, visceral transposition and male infertility. WES revealed a homozygous frameshift variation of c.12890dup (p.N4297Kfs*13) in exon 74 of the DNAH5 gene, which led to the premature termination of polypeptide chain synthesis and affected the gene function. SWISS-MODEL prediction showed that some of the amino acid residues were deleted after mutation, resulting in a 3D conformational change of the protein. This variation was not recorded in the ClinVar, gnomAD and OMIM databases and, according to the relevant guidelines of the American College of Genetics and Genomics, was classified as a pathogenic variation (PVS1+PM2_P+PM3_P).

Conclusion: The homozygous variation of the DNAH5 gene c.12890dup (p.N4297Kfs*13) may be the cause of the clinical phenotype of this case of PCD, and the above findings have enriched the variation spectrum of the DNAH5 gene.

本刊更多论文

[由 DNAH5 基因新的框架移位突变引起的一例原发性睫状肌运动障碍的临床和遗传特征]。

目的：研究一例原发性睫状肌运动障碍（PCD）患者的临床和遗传特征：研究一例原发性睫状肌运动障碍（PCD）患者的临床和遗传特征：收集2020年7月临沂市人民医院生殖医学科收治的一例原发性睫状肌运动障碍（PCD）患者的临床资料，通过全外显子组测序（WES）检测患者基因，通过Sanger测序验证候选突变基因，通过SWISS-MODEL预测突变基因的蛋白结构：结果：发现该患者具有慢性鼻炎、支气管扩张、内脏移位和男性不育的临床表现。WES发现DNAH5基因第74外显子存在c.12890dup (p.N4297Kfs*13)的同源框架移位变异，导致多肽链合成提前终止，影响了基因功能。SWISS-MODEL 预测显示，突变后部分氨基酸残基被删除，导致蛋白质的三维构象发生变化。该变异在 ClinVar、gnomAD 和 OMIM 数据库中均无记录，根据美国遗传学和基因组学学院的相关指南，该变异被归类为致病性变异（PVS1+PM2_P+PM3_P）：结论：DNAH5基因c.12890dup（p.N4297Kfs*13）的同源变异可能是导致该例PCD临床表型的原因，上述发现丰富了DNAH5基因的变异谱。

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

中华男科学杂志 Medicine-Medicine (all)

CiteScore

0.40

自引率

0.00%

发文量

5367

期刊介绍： National journal of andrology was founded in June 1995. It is a core journal of andrology and reproductive medicine, published monthly, and is publicly distributed at home and abroad. The main columns include expert talks, monographs (basic research, clinical research, evidence-based medicine, traditional Chinese medicine), reviews, clinical experience exchanges, case reports, etc. Priority is given to various fund-funded projects, especially the 12th Five-Year National Support Plan and the National Natural Science Foundation funded projects. This journal is included in about 20 domestic databases, including the National Science and Technology Paper Statistical Source Journal (China Science and Technology Core Journal), the Source Journal of the China Science Citation Database, the Statistical Source Journal of the China Academic Journal Comprehensive Evaluation Database (CAJCED), the Full-text Collection Journal of the China Journal Full-text Database (CJFD), the Overview of the Chinese Core Journals (2017 Edition), and the Source Journal of the Top Academic Papers of China's Fine Science and Technology Journals (F5000). It has been included in the full text of the American Chemical Abstracts, the American MEDLINE, the American EBSCO, and the database.