Department of Pediatrics, UT Health Science Center, 7703 Floyd Curl Dive, San Antonio, TX 78229, USA.
Hum Genet. 2011 Dec;130(6):777-87. doi: 10.1007/s00439-011-1020-y. Epub 2011 Jun 14.
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.
本研究旨在明确 TCF4 半合子在更大的 18q 染色体片段缺失背景下的影响。我们的队列包括 37 名 18q 缺失患者。27 名患者的缺失包括 TCF4(TCF4(+/-));9 名患者的缺失不包括 TCF4(TCF4(+/));1 名患者的缺失仅包括 TCF4 基因。我们比较了参与者病历、调查回复和面对面评估中的表型数据。TCF4(+/-)个体特有的特征包括胼胝体异常、短颈、小阴茎、副乳和宽距乳头、宽或棒状手指和骶骨凹陷。发育数据显示,TCF4(+/)个体仅存在中度发育延迟,而 TCF4(+/-)个体未能达到 12 个月大时通常获得的发育里程碑。TCF4 半合子还增加了早逝的风险,主要是由于与吸入相关的并发症。TCF4 的半合子状态主要对认知和运动发育有显著影响,与其他 18q 远端区域的半合子个体相比,TCF4 半合子个体的预后明显不同。
