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临床外显子组测序揭示了黏连蛋白病的基因座异质性和表型变异性。

Clinical exome sequencing reveals locus heterogeneity and phenotypic variability of cohesinopathies.

机构信息

Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, Texas, 77030, USA.

Baylor Genetics, Houston, Texas, 77021, USA.

出版信息

Genet Med. 2019 Mar;21(3):663-675. doi: 10.1038/s41436-018-0085-6. Epub 2018 Aug 30.

DOI:10.1038/s41436-018-0085-6
PMID:30158690
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6395558/
Abstract

PURPOSE

Defects in the cohesin pathway are associated with cohesinopathies, notably Cornelia de Lange syndrome (CdLS). We aimed to delineate pathogenic variants in known and candidate cohesinopathy genes from a clinical exome perspective.

METHODS

We retrospectively studied patients referred for clinical exome sequencing (CES, N = 10,698). Patients with causative variants in novel or recently described cohesinopathy genes were enrolled for phenotypic characterization.

RESULTS

Pathogenic or likely pathogenic single-nucleotide and insertion/deletion variants (SNVs/indels) were identified in established disease genes including NIPBL (N = 5), SMC1A (N = 14), SMC3 (N = 4), RAD21 (N = 2), and HDAC8 (N = 8). The phenotypes in this genetically defined cohort skew towards the mild end of CdLS spectrum as compared with phenotype-driven cohorts. Candidate or recently reported cohesinopathy genes were supported by de novo SNVs/indels in STAG1 (N = 3), STAG2 (N = 5), PDS5A (N = 1), and WAPL (N = 1), and one inherited SNV in PDS5A. We also identified copy-number deletions affecting STAG1 (two de novo, one of unknown inheritance) and STAG2 (one of unknown inheritance). Patients with STAG1 and STAG2 variants presented with overlapping features yet without characteristic facial features of CdLS.

CONCLUSION

CES effectively identified disease-causing alleles at the mild end of the cohensinopathy spectrum and enabled characterization of candidate disease genes.

摘要

目的

黏连蛋白通路缺陷与黏连蛋白病相关,尤其是Cornelia de Lange 综合征(CdLS)。我们旨在从临床外显子组的角度描绘已知和候选黏连蛋白病基因中的致病性变异。

方法

我们回顾性研究了接受临床外显子组测序(CES,N=10698)的患者。患有新型或最近描述的黏连蛋白病基因中致病或可能致病的单核苷酸和插入/缺失变异(SNVs/indels)的患者被纳入进行表型特征描述。

结果

在已建立的疾病基因中发现了致病性或可能致病性的单核苷酸和插入/缺失变异(SNVs/indels),包括 NIPBL(N=5)、SMC1A(N=14)、SMC3(N=4)、RAD21(N=2)和 HDAC8(N=8)。与表型驱动的队列相比,在这个基因定义的队列中,疾病表型倾向于 CdLS 谱的轻度端。候选或最近报道的黏连蛋白病基因得到了 STAG1(N=3)、STAG2(N=5)、PDS5A(N=1)和 WAPL(N=1)中新生 SNVs/indels 的支持,以及 PDS5A 中一个遗传 SNV。我们还发现了影响 STAG1(两个新生,一个未知遗传)和 STAG2(一个未知遗传)的拷贝数缺失。携带 STAG1 和 STAG2 变异的患者表现出重叠的特征,但没有 CdLS 的特征性面部特征。

结论

CES 有效地在黏连蛋白病谱的轻度端识别出致病等位基因,并使候选疾病基因的特征描述成为可能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1278/6395558/66ce2503014b/nihms-973104-f0002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1278/6395558/4e678429ef59/nihms-973104-f0001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1278/6395558/66ce2503014b/nihms-973104-f0002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1278/6395558/4e678429ef59/nihms-973104-f0001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1278/6395558/66ce2503014b/nihms-973104-f0002.jpg

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