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首页> 外文期刊>American journal of medical genetics, Part A >Expanding the phenotype associated with 17q12 duplication: Case report and review of the literature
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Expanding the phenotype associated with 17q12 duplication: Case report and review of the literature

机译:扩展与17q12复制相关的表型:病例报告和文献复习

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摘要

The routine use of molecular karyotyping in the evaluation of patients with idiopathic developmental delay with/without dysmorphic features, has led to the delineation of several submicroscopic deletion/duplication syndromes. De novo copy number variations are often presumed to be pathogenic and inherited ones from a healthy parent likely to be not relevant for the phenotype. However, it is difficult to draw such a conclusion for an inherited copy number variation not known to be a common variation. We report on a child with developmental delay, seizures, microcephaly, hypotonia, unusual stereotypical movements, and changes in the white matter who inherited a 17q12 tandem duplication of ~1.4Mb from his healthy father. Copy number variations in this chromosomal region are thought to be pathogenic and associated with various phenotypes including developmental delay, growth retardation, seizures, renal disease, and diabetes mellitus. We review all reported cases with 17q12 duplication and discuss the novelty of the phenotype in the present case. We also share our thoughts on submicroscopic complexity that may underlie, at least in part, the wide range of phenotypes in patients with 17q12 duplication.
机译:分子核型分型在具有/不具有畸形特征的特发性发育迟缓患者的评估中的常规使用,导致了几种亚显微缺失/重复综合征的描述。从头算起的拷贝数变异通常被认为是致病的,并且是从健康的父母那里遗传下来的,可能与表型无关。但是,对于不知道是常见变异的遗传拷贝数变异,很难得出这样的结论。我们报告了一个发育迟缓,癫痫发作,小头畸形,肌张力低下,异常刻板印象运动以及白质变化的孩子,该孩子从他健康的父亲那里继承了17q12串联重复序列〜1.4Mb。该染色体区域的拷贝数变化被认为是致病的,并且与各种表型有关,包括发育延迟,生长迟缓,癫痫发作,肾脏疾病和糖尿病。我们审查与17q12重复的所有报告的病例,并讨论本例中表型的新颖性。我们还就亚显微复杂性分享了我们的想法,这种复杂性至少部分是17q12重复患者表型广泛的基础。

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