CDK13-related障碍。

4区 生物学 Q2 Biochemistry, Genetics and Molecular Biology
Advances in Genetics Pub Date : 2019-01-01 Epub Date: 2018-12-11 DOI:10.1016/bs.adgen.2018.11.001
Mark James Hamilton, Mohnish Suri
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引用次数: 16

摘要

CDK13突变最近被确定为综合征性智力残疾的新原因。在本章中,我们回顾了迄今为止报道的44例cdk13相关疾病,重点介绍了该诊断的关键临床指标,包括特征性颅面特征,婴儿期喂养困难以及存在结构性心脏或大脑畸形。报告的突变谱也被描述,显示过量的错义突变产生在蛋白激酶结构域。对基因型-表型相关性的探索表明,预测导致CDK13单倍不足的突变患者的表型倾向较轻,而影响氨基酸残基842的错义突变似乎最有可能与结构畸形相关。错义变异体更大的表型影响被假设是由于显性-负性机制而发生的,通过这种机制,突变蛋白将细胞周期蛋白K隔离在无活性复合物中。然而,验证这一假设的功能性研究尚未开展。本文还描述了cdk13相关疾病患者的鉴别诊断和临床护理建议,强调基线超声心动图、对进食和吞咽困难的警惕以及定期的发育评估是护理的关键组成部分。最后,讨论了CDK13研究的未来方向,包括需要解决CDK13单倍不全致病性的不确定性,并从大型队列中收集进一步的纵向数据,以便为这种诊断的患者提供临床护理信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
CDK13-related disorder.

Mutations in CDK13 have recently been identified as a novel cause of syndromic intellectual disability. In this chapter, we review the 44 cases of CDK13-related disorder reported to date, highlighting key clinical pointers to this diagnosis including characteristic craniofacial features, feeding difficulties in infancy, and the presence of structural heart or brain malformations. The spectrum of reported mutations is also described, demonstrating an excess of missense mutations arising in the protein kinase domain. Exploration of genotype-phenotype correlations suggests a trend toward milder phenotypes in patients with mutations predicted to cause haploinsufficiency of CDK13, while missense mutations affecting amino acid residue 842 appear most likely to be associated with structural malformations. The greater phenotypic impact of missense variants is hypothesized to occur due to a dominant-negative mechanism, by which the mutant protein acts to sequester cyclin K in inactive complexes. Functional studies to validate this hypothesis have not yet been carried out, however. Differential diagnosis and recommendations for clinical care of patients with CDK13-related disorder are also described, emphasizing baseline echocardiography, vigilance for feeding and swallowing difficulties, and regular developmental evaluation as key components of care. Finally, future directions for CDK13 research are discussed, including the need to resolve uncertainty regarding pathogenicity of CDK13 haploinsufficiency, and to gather further longitudinal data from large cohorts in order to inform the clinical care of patients with this diagnosis.

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来源期刊
Advances in Genetics
Advances in Genetics 生物-遗传学
CiteScore
5.70
自引率
0.00%
发文量
1
审稿时长
1 months
期刊介绍: Advances in Genetics presents an eclectic mix of articles of use to all human and molecular geneticists. They are written and edited by recognized leaders in the field and make this an essential series of books for anyone in the genetics field.
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