首页> 外文期刊>Molecular syndromology >Microcephaly/Trigonocephaly, Intellectual Disability, Autism Spectrum Disorder, and Atypical Dysmorphic Features in a Boy with Xp22.31 Duplication
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Microcephaly/Trigonocephaly, Intellectual Disability, Autism Spectrum Disorder, and Atypical Dysmorphic Features in a Boy with Xp22.31 Duplication

机译:Xp22.31复制男孩中的小头畸形/三角头畸形,智力障碍,自闭症谱系障碍和非典型畸形特征

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摘要

The Xp22.31 segment of the short arm of the human X chromosome is a region of high instability with frequent rearrangement. The duplication of this region has been found in healthy people as well as in individuals with varying degrees of neurological impairment. The incidence has been reported in a range of 0.4-0.44% of the patients with neurological impairment. Moreover, there is evidence that Xp22.31 duplication may cause a common phenotype including developmental delay, intellectual disability, feeding difficulty, autistic spectrum disorders, hypotonia, seizures, and talipes. We report on a patient with microcephaly and trigonocephaly, moderate intellectual disability, speech and language delay, and poor social interaction in addition to minor but atypical dysmorphic features. This report provides further insight into the pathogenicity of the Xp22.31 duplication by extending knowledge of its clinical features. This case, in association with those reported in the literature, indicates that the Xp22.31 duplication may contribute to cause pathological phenotypes with minor facial dysmorphisms, microcephaly, and intellectual disability as main features.
机译:人类X染色体短臂的Xp22.31节段是高度不稳定的区域,经常发生重排。在健康人群以及神经功能受损程度不同的人中都发现了该区域的重复。据报道,神经功能障碍患者的发病率在0.4-0.44%的范围内。此外,有证据表明Xp22.31复制可能引起常见的表型,包括发育迟缓,智力残疾,进食困难,自闭症谱系障碍,肌张力低下,癫痫发作和滑石粉。我们报告了一个小头畸形和三角畸形,中度智力残疾,言语和语言障碍,社交互动不良以及轻微但非典型的畸形特征的患者。该报告通过扩展Xp22.31的临床特征知识,为Xp22.31复制的致病性提供了进一步的见解。该病例与文献报道的病例有关,表明Xp22.31重复可能导致病理表型,主要表现为面部畸形,小头畸形和智力障碍。

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