HudsonAlpha Institute for Biotechnology, Huntsville, Alabama, USA.
Department of Pediatrics, University of Louisville, Louisville, Kentucky, USA.
Genet Med. 2018 Dec;20(12):1635-1643. doi: 10.1038/gim.2018.53. Epub 2018 Apr 12.
Clinically relevant secondary variants were identified in parents enrolled with a child with developmental delay and intellectual disability.
Exome/genome sequencing and analysis of 789 "unaffected" parents was performed.
Pathogenic/likely pathogenic variants were identified in 21 genes within 25 individuals (3.2%), with 11 (1.4%) participants harboring variation in a gene defined as clinically actionable by the American College of Medical Genetics and Genomics. These 25 individuals self-reported either relevant clinical diagnoses (5); relevant family history or symptoms (13); or no relevant family history, symptoms, or clinical diagnoses (7). A limited carrier screen was performed yielding 15 variants in 48 (6.1%) parents. Parents were also analyzed as mate pairs (n = 365) to identify cases in which both parents were carriers for the same recessive disease, yielding three such cases (0.8%), two of which had children with the relevant recessive disease. Four participants had two findings (one carrier and one noncarrier variant). In total, 71 of the 789 enrolled parents (9.0%) received secondary findings.
We provide an overview of the rates and types of clinically relevant secondary findings, which may be useful in the design and implementation of research and clinical sequencing efforts to identify such findings.
在患有发育迟缓及智力障碍的儿童的父母中发现了具有临床相关性的二级变体。
对 789 名“无病”父母进行了外显子组/基因组测序和分析。
在 25 名个体的 21 个基因中发现了致病性/可能致病性变体,其中 11 名(1.4%)参与者携带美国医学遗传学与基因组学学院定义的具有临床可操作性的基因变异。这 25 名个体自我报告了相关的临床诊断(5 例);相关家族史或症状(13 例);或无相关家族史、症状或临床诊断(7 例)。进行了有限的携带者筛查,在 48 名(6.1%)父母中发现了 15 个变体。还对父母进行了伴侣对分析(n=365),以确定父母双方均为同一隐性疾病携带者的病例,发现了三个此类病例(0.8%),其中两个孩子患有相关的隐性疾病。四名参与者有两个发现(一个携带者和一个非携带者变体)。总共,789 名入组父母中有 71 名(9.0%)收到了二级发现。
我们提供了具有临床相关性的二级发现的发生率和类型的概述,这对于设计和实施研究和临床测序工作以识别此类发现可能是有用的。
Zotero 插件