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神经干细胞的细胞连接病理学导致异常神经发生和脑积水。

A cell junction pathology of neural stem cells leads to abnormal neurogenesis and hydrocephalus.

机构信息

Instituto de Anatomía, Histología y Patología, Universidad Austral de Chile, Valdivia, Chile.

出版信息

Biol Res. 2012;45(3):231-42. doi: 10.4067/S0716-97602012000300005.

Abstract

Most cells of the developing mammalian brain derive from the ventricular (VZ) and the subventricular (SVZ) zones. The VZ is formed by the multipotent radial glia/neural stem cells (NSCs) while the SVZ harbors the rapidly proliferative neural precursor cells (NPCs). Evidence from human and animal models indicates that the common history of hydrocephalus and brain maldevelopment starts early in embryonic life with disruption of the VZ and SVZ. We propose that a "cell junction pathology" involving adherent and gap junctions is a final common outcome of a wide range of gene mutations resulting in proteins abnormally expressed by the VZ cells undergoing disruption. Disruption of the VZ during fetal development implies the loss of NSCs whereas VZ disruption during the perinatal period implies the loss of ependyma. The process of disruption occurs in specific regions of the ventricular system and at specific stages of brain development. This explains why only certain brain structures have an abnormal development, which in turn results in a specific neurological impairment of the newborn. Disruption of the VZ of the Sylvian aqueduct (SA) leads to aqueductal stenosis and hydrocephalus, while disruption of the VZ of telencephalon impairs neurogenesis. We are currently investigating whether grafting of NSCs/neurospheres from normal rats into the CSF of hydrocephalic mutants helps to diminish/repair the outcomes of VZ disruption.

摘要

哺乳动物大脑发育过程中的大多数细胞都来源于脑室(VZ)和侧脑室下区(SVZ)。VZ 由多能性放射状胶质细胞/神经干细胞(NSCs)组成,而 SVZ 则含有快速增殖的神经前体细胞(NPCs)。来自人类和动物模型的证据表明,脑积水和脑发育不良的共同病史始于胚胎早期,VZ 和 SVZ 受到干扰。我们提出,一种涉及黏附连接和缝隙连接的“细胞连接病理学”是广泛基因突变导致 VZ 细胞中异常表达的蛋白质的最终共同结果。胎儿发育过程中 VZ 的破坏意味着 NSCs 的丧失,而围产期 VZ 的破坏则意味着室管膜的丧失。破坏过程发生在脑室系统的特定区域和大脑发育的特定阶段。这解释了为什么只有某些脑结构会出现异常发育,从而导致新生儿特定的神经功能障碍。中脑导水管(SA)VZ 的破坏会导致导水管狭窄和脑积水,而端脑 VZ 的破坏会损害神经发生。我们目前正在研究将正常大鼠的 NSCs/神经球移植到脑积水突变体的脑脊液中是否有助于减轻/修复 VZ 破坏的后果。

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