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首页> 外文期刊>Nature Communications >BAFopathies’ DNA methylation epi-signatures demonstrate diagnostic utility and functional continuum of Coffin–Siris and Nicolaides–Baraitser syndromes
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BAFopathies’ DNA methylation epi-signatures demonstrate diagnostic utility and functional continuum of Coffin–Siris and Nicolaides–Baraitser syndromes

机译:BAFopathies的DNA甲基化后签名显示了Coffin-Siris和Nicolaides-Baraitser综合征的诊断效用和功能连续性

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Coffin–Siris and Nicolaides–Baraitser syndromes (CSS and NCBRS) are Mendelian disorders caused by mutations in subunits of the BAF chromatin remodeling complex. We report overlapping peripheral blood DNA methylation epi-signatures in individuals with various subtypes of CSS (ARID1B, SMARCB1, and SMARCA4) and NCBRS (SMARCA2). We demonstrate that the degree of similarity in the epi-signatures of some CSS subtypes and NCBRS can be greater than that within CSS, indicating a link in the functional basis of the two syndromes. We show that chromosome 6q25 microdeletion syndrome, harboring ARID1B deletions, exhibits a similar CSS/NCBRS methylation profile. Specificity of this epi-signature was confirmed across a wide range of neurodevelopmental conditions including other chromatin remodeling and epigenetic machinery disorders. We demonstrate that a machine-learning model trained on this DNA methylation profile can resolve ambiguous clinical cases, reclassify those with variants of unknown significance, and identify previously undiagnosed subjects through targeted population screening.
机译:棺材-西里斯和尼古拉德-巴里瑟特综合征(CSS和NCBRS)是由BAF染色质重塑复合体亚基突变引起的孟德尔疾病。我们报告了具有各种亚型的CSS(ARID1B,SMARCB1和SMARCA4)和NCBRS(SMARCA2)的个体中重叠的外周血DNA甲基化Epi-签名。我们证明,某些CSS亚型和NCBRS的Epi-Signatures的相似度可以大于CSS内的相似度,表明这两种综合征的功能基础存在联系。我们表明,染色体6q25微缺失综合征,藏有ARID1B缺失,表现出相似的CSS / NCBRS甲基化谱。在广泛的神经发育状况,包括其他染色质重塑和表观遗传机械障碍中,证实了这种表位签名的特异性。我们证明在这种DNA甲基化配置文件上训练的机器学习模型可以解决模棱两可的临床病例,对具有重要意义的变体的病例进行重新分类,并通过有针对性的人群筛选来识别以前未被诊断的受试者。

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