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WDR62 基因突变导致脑回简化和皮质结构异常的小头畸形。

Mutations in WDR62, encoding a centrosome-associated protein, cause microcephaly with simplified gyri and abnormal cortical architecture.

机构信息

Division of Genetics, Department of Medicine, Children's Hospital Boston, Boston, Massachusetts, USA.

出版信息

Nat Genet. 2010 Nov;42(11):1015-20. doi: 10.1038/ng.683. Epub 2010 Oct 3.

Abstract

Genes associated with human microcephaly, a condition characterized by a small brain, include critical regulators of proliferation, cell fate and DNA repair. We describe a syndrome of congenital microcephaly and diverse defects in cerebral cortical architecture. Genome-wide linkage analysis in two families identified a 7.5-Mb locus on chromosome 19q13.12 containing 148 genes. Targeted high throughput sequence analysis of linked genes in each family yielded > 4,000 DNA variants and implicated a single gene, WDR62, as harboring potentially deleterious changes. We subsequently identified additional WDR62 mutations in four other families. Magnetic resonance imaging and postmortem brain analysis supports important roles for WDR62 in the proliferation and migration of neuronal precursors. WDR62 is a WD40 repeat-containing protein expressed in neuronal precursors as well as in postmitotic neurons in the developing brain and localizes to the spindle poles of dividing cells. The diverse phenotypes of WDR62 suggest it has central roles in many aspects of cerebral cortical development.

摘要

与人类小头畸形相关的基因,其特征是大脑较小,包括增殖、细胞命运和 DNA 修复的关键调节因子。我们描述了一种先天性小头畸形和大脑皮质结构多种缺陷的综合征。在两个家庭中进行的全基因组连锁分析确定了染色体 19q13.12 上的 7.5Mb 位点,该位点包含 148 个基因。对每个家族中连锁基因的靶向高通量序列分析产生了>4000 个 DNA 变体,并表明单个基因 WDR62 携带潜在的有害变化。随后,在另外四个家庭中发现了其他 WDR62 突变。磁共振成像和死后大脑分析支持 WDR62 在神经元前体的增殖和迁移中具有重要作用。WDR62 是一种 WD40 重复蛋白,在神经元前体以及发育中大脑的有丝分裂神经元中表达,并定位于分裂细胞的纺锤体极。WDR62 的多种表型表明它在大脑皮质发育的许多方面都具有核心作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9fe5/2969850/8fd281b5e536/nihms236207f1.jpg

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