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p53 家族成员 p63 和 p73 在小鼠和人类大脑皮质发育和成年期的动态表达。

Dynamic expression of the p53 family members p63 and p73 in the mouse and human telencephalon during development and in adulthood.

机构信息

Depto Anatomía, Facultad de Medicina, 38071 La Laguna, Tenerife, Spain.

出版信息

Brain Res. 2011 Feb 4;1372:29-40. doi: 10.1016/j.brainres.2010.11.041. Epub 2010 Nov 27.

DOI:10.1016/j.brainres.2010.11.041
PMID:21114965
Abstract

p63 and p73, family members of the tumor suppressor p53, are critically involved in the life and death of mammalian cells. They display high homology and may act in concert. The p73 gene is relevant for brain development, and p73-deficient mice display important malformations of the telencephalon. In turn, p63 is essential for the development of stratified epithelia and may also play a part in neuronal survival and aging. We show here that p63 and p73 are dynamically expressed in the embryonic and adult mouse and human telencephalon. During embryonic stages, Cajal-Retzius cells derived from the cortical hem co-express p73 and p63. Comparison of the brain phenotypes of p63- and p73- deficient mice shows that only the loss of p73 function leads to the loss of Cajal-Retzius cells, whereas p63 is apparently not essential for brain development and Cajal-Retzius cell formation. In postnatal mice, p53, p63, and p73 are present in cells of the subventricular zone (SVZ) of the lateral ventricle, a site of continued neurogenesis. The neurogenetic niche is reduced in size in p73-deficient mice, and the numbers of young neurons near the ventricular wall, marked with doublecortin, Tbr1 and calretinin, are dramatically decreased, suggesting that p73 is important for SVZ proliferation. In contrast to their restricted expression during brain development, p73 and p63 are widely detected in pyramidal neurons of the adult human cortex and hippocampus at protein and mRNA levels, pointing to a role of both genes in neuronal maintenance in adulthood.

摘要

p63 和 p73 是肿瘤抑制因子 p53 的家族成员,它们在哺乳动物细胞的生死存亡中起着至关重要的作用。它们具有高度同源性,可能协同作用。p73 基因与大脑发育有关,p73 缺陷的小鼠表现出重要的端脑畸形。反过来,p63 对于分层上皮的发育是必需的,并且可能在神经元存活和衰老中起作用。我们在这里显示 p63 和 p73 在胚胎和成年小鼠和人脑中呈动态表达。在胚胎期,来自皮质半球的 Cajal-Retzius 细胞共同表达 p73 和 p63。比较 p63 和 p73 缺陷小鼠的脑表型表明,只有 p73 功能的丧失导致 Cajal-Retzius 细胞的丧失,而 p63显然不是大脑发育和 Cajal-Retzius 细胞形成所必需的。在出生后的小鼠中,p53、p63 和 p73 存在于侧脑室室下区 (SVZ) 的细胞中,SVZ 是持续神经发生的部位。p73 缺陷小鼠的神经发生龛体积减小,靠近脑室壁的年轻神经元数量明显减少,这些神经元用双皮质素、Tbr1 和钙视网膜蛋白标记,表明 p73 对 SVZ 增殖很重要。与它们在大脑发育过程中的受限表达相反,p73 和 p63 在成年人大脑皮层和海马体的锥体神经元中在蛋白质和 mRNA 水平上广泛表达,表明这两个基因在成年期神经元维持中起作用。

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