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Mutations in CUL4B which encodes a ubiquitin E3 ligase subunit cause an X-linked mental retardation syndrome associated with aggressive outbursts seizures relative macrocephaly central obesity hypogonadism pes cavus and tremor

机译:编码遍在蛋白E3连接酶亚基的CUL4B突变导致与相关性巨噬细胞中枢性肥胖性腺功能减退症相关的X连锁精神发育迟滞综合征相关性脑卒中和震颤

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摘要

We have identified three truncating, two splice-site, and three missense variants at conserved amino acids in the CUL4B gene on Xq24 in 8 of 250 families with X-linked mental retardation (XLMR). During affected subjects' adolescence, a syndrome emerged with delayed puberty, hypogonadism, relative macrocephaly, moderate short stature, central obesity, unprovoked aggressive outbursts, fine intention tremor, pes cavus, and abnormalities of the toes. This syndrome was first described by Cazebas et al., in a family that was included in our study and that carried a CUL4B missense variant. CUL4B is a ubiquitin E3 ligase subunit implicated in the regulation of several biological processes, and CUL4B is the first XLMR gene that encodes an E3 ubiquitin ligase. The relatively high frequency of CUL4B mutations in this series indicates that it is one of the most commonly mutated genes underlying XLMR and suggests that its introduction into clinical diagnostics should be a high priority.
机译:我们已经确定了X连锁智力低下(XLMR)的250个家庭中的8个家庭中Xq24上CUL4B基因保守氨基酸的三个截短,两个剪接位点和三个错义变体。在受影响受试者的青春期期间,出现了一种综合征,其中包括青春期延迟,性腺功能减退,相对头畸形,中度矮小身材,中枢性肥胖,无端发情的爆发,好意的震颤,阴茎凹陷和脚趾异常。该综合征首先由Cazebas等人描述,属于我们的研究中的一个家族,该家族携带CUL4B错义变体。 CUL4B是一个泛素E3连接酶亚基,涉及几个生物学过程的调控,CUL4B是第一个编码E3泛素连接酶的XLMR基因。该系列中相对较高的CUL4B突变频率表明,它是XLMR基础上最常见的突变基因之一,并建议将其引入临床诊断应该是高度优先的工作。

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