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Long-range enhancers regulating Myc expression are required for normal facial morphogenesis

机译:正常面部形态发生需要远程调节Myc表达的增强子

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摘要

Cleft lip with or without cleft palate (CL/P) is one of the most common congenital malformations observed in humans, with 1 occurrence in every 500-1,000 births. A 640-kb noncoding interval at 8q24 has been associated with increased risk of non-syndromic CL/P in humans, but the genes and pathways involved in this genetic susceptibility have remained elusive. Using a large series of rearrangements engineered over the syntenic mouse region, we show that this interval contains very remote cis-acting enhancers that control Myc expression in the developing face. Deletion of this interval leads to mild alteration of facial morphology in mice and, sporadically, to CL/P. At the molecular level, we identify misexpression of several downstream genes, highlighting combined impact on the craniofacial developmental network and the general metabolic capacity of cells contributing to the future upper lip. This dual molecular etiology may account for the prominent influence of variants in the 8q24 region on human facial dysmorphologies.
机译:有或没有c裂(CL / P)的唇裂是人类中观察到的最常见的先天畸形之一,每500-1,000例新生儿中就有1例发生。在8q24处640-kb的非编码间隔与人类非综合征性CL / P的风险增加有关,但与这种遗传易感性有关的基因和途径仍然难以捉摸。使用在同位小鼠区域上进行工程改造的一系列重排,我们显示该间隔包含非常遥远的顺式作用增强子,可控制发育中的Myc表达。间隔时间的删除会导致小鼠面部形态的轻度改变,偶尔会导致CL / P。在分子水平上,我们确定了几个下游基因的错误表达,突出了对颅面发育网络的综合影响以及对未来上唇作出贡献的细胞的总体代谢能力。这种双重分子病因可能解释了8q24区域中的变异对人类面部畸形的显着影响。

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