Atypical splicing variants in PKD1 explain most undiagnosed typical familial ADPKD.

IF 4.7 2区 医学 Q1 GENETICS & HEREDITY NPJ Genomic Medicine Pub Date : 2023-07-07 DOI:10.1038/s41525-023-00362-z
Yvonne Hort, Patricia Sullivan, Laura Wedd, Lindsay Fowles, Igor Stevanovski, Ira Deveson, Cas Simons, Andrew Mallett, Chirag Patel, Timothy Furlong, Mark J Cowley, John Shine, Amali Mallawaarachchi
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Abstract

Autosomal dominant polycystic kidney disease (ADPKD) is the most common monogenic cause of kidney failure and is primarily associated with PKD1 or PKD2. Approximately 10% of patients remain undiagnosed after standard genetic testing. We aimed to utilise short and long-read genome sequencing and RNA studies to investigate undiagnosed families. Patients with typical ADPKD phenotype and undiagnosed after genetic diagnostics were recruited. Probands underwent short-read genome sequencing, PKD1 and PKD2 coding and non-coding analyses and then genome-wide analysis. Targeted RNA studies investigated variants suspected to impact splicing. Those undiagnosed then underwent Oxford Nanopore Technologies long-read genome sequencing. From over 172 probands, 9 met inclusion criteria and consented. A genetic diagnosis was made in 8 of 9 (89%) families undiagnosed on prior genetic testing. Six had variants impacting splicing, five in non-coding regions of PKD1. Short-read genome sequencing identified novel branchpoint, AG-exclusion zone and missense variants generating cryptic splice sites and a deletion causing critical intron shortening. Long-read sequencing confirmed the diagnosis in one family. Most undiagnosed families with typical ADPKD have splice-impacting variants in PKD1. We describe a pragmatic method for diagnostic laboratories to assess PKD1 and PKD2 non-coding regions and validate suspected splicing variants through targeted RNA studies.

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PKD1的非典型剪接变异解释了大多数未确诊的典型家族性ADPKD。
常染色体显性多囊肾病(ADPKD)是肾衰竭最常见的单基因原因,主要与PKD1或PKD2相关。大约10%的患者在标准基因检测后仍未得到诊断。我们的目标是利用短读和长读基因组测序和RNA研究来调查未确诊的家庭。招募具有典型ADPKD表型且基因诊断后未确诊的患者。先证物进行短读基因组测序,PKD1和PKD2编码和非编码分析,然后进行全基因组分析。靶向RNA研究调查了可能影响剪接的变异。随后,未确诊的患者接受了牛津纳米孔技术公司的长读基因组测序。在172个先证者中,9个符合纳入标准并同意。9个未进行基因检测的家庭中有8个(89%)进行了基因诊断。6个变体影响剪接,5个在PKD1的非编码区。短读基因组测序鉴定出新的分支点、ag排斥区和错义变异,产生隐剪接位点和导致关键内含子缩短的缺失。长读测序证实了一个家庭的诊断。大多数未确诊的典型ADPKD家庭都有PKD1剪接影响变异。我们描述了一种实用的方法,用于诊断实验室评估PKD1和PKD2非编码区,并通过靶向RNA研究验证可疑的剪接变体。
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来源期刊
NPJ Genomic Medicine
NPJ Genomic Medicine Biochemistry, Genetics and Molecular Biology-Molecular Biology
CiteScore
9.40
自引率
1.90%
发文量
67
审稿时长
17 weeks
期刊介绍: npj Genomic Medicine is an international, peer-reviewed journal dedicated to publishing the most important scientific advances in all aspects of genomics and its application in the practice of medicine. The journal defines genomic medicine as "diagnosis, prognosis, prevention and/or treatment of disease and disorders of the mind and body, using approaches informed or enabled by knowledge of the genome and the molecules it encodes." Relevant and high-impact papers that encompass studies of individuals, families, or populations are considered for publication. An emphasis will include coupling detailed phenotype and genome sequencing information, both enabled by new technologies and informatics, to delineate the underlying aetiology of disease. Clinical recommendations and/or guidelines of how that data should be used in the clinical management of those patients in the study, and others, are also encouraged.
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