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The role of the TCF4 gene in the phenotype of individuals with 18q segmental deletions

机译:TCF4基因在18q节段缺失的个体表型中的作用

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The goal of this study is to define the effects of TCF4 hemizygosity in the context of a larger segmental deletion of chromosome 18q. Our cohort included 37 individuals with deletions of 18q. Twenty-seven had deletions including TCF4 (TCF4 +/−); nine had deletions that did not include TCF4 (TCF4 +/+); and one individual had a microdeletion that included only the TCF4 gene. We compared phenotypic data from the participants’ medical records, survey responses, and in-person evaluations. Features unique to the TCF4 +/− individuals included abnormal corpus callosum, short neck, small penis, accessory and wide-spaced nipples, broad or clubbed fingers, and sacral dimple. The developmental data revealed that TCF4 +/+ individuals were only moderately developmentally delayed while TCF4 +/− individuals failed to reach developmental milestones beyond those typically acquired by 12 months of age. TCF4 hemizygosity also conferred an increased risk of early death principally due to aspiration-related complications. Hemizygosity for TCF4 confers a significant impact primarily with regard to cognitive and motor development, resulting in a very different prognosis for individuals hemizygous for TCF4 when compared to individuals hemizygous for other regions of distal 18q.
机译:这项研究的目的是在18q染色体更大的片段缺失的背景下确定TCF4半合子的影响。我们的研究对象包括37个缺失18q的个体。有27个删除,包括TCF4(TCF4 + /-/ ); 9个删除项不包含TCF4(TCF4 + / + );一个人的微缺失仅包含TCF4基因。我们比较了参与者的病历,调查回复和当面评价中的表型数据。 TCF4 +/- 个体的独特功能包括abnormal体异常,脖子短,阴茎小,乳头宽而附属的乳头,手指宽大或棒状以及ac骨酒窝。发育数据显示,TCF4 + / + 个体仅适度发育延迟,而TCF4 +/- 个体未能达到超过12个月大时通常获得的发展里程碑。 TCF4的半合子性也主要由于与抽吸有关的并发症而使早期死亡的风险增加。 TCF4的半合子性主要对认知和运动发育产生重大影响,与18q末梢其他区域的半合子个体相比,TCF4的半合子个体的预后非常不同。

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