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成年小鼠大脑中的祖细胞会对β-淀粉样蛋白产生反应,从而获得神经元表型。

Progenitor cells from the adult mouse brain acquire a neuronal phenotype in response to beta-amyloid.

作者信息

Calafiore M, Battaglia G, Zappalà A, Trovato-Salinaro E, Caraci F, Caruso M, Vancheri C, Sortino M A, Nicoletti F, Copani A

机构信息

Department of Pharmaceutical Sciences, University of Catania, Catania 95125, Italy.

出版信息

Neurobiol Aging. 2006 Apr;27(4):606-13. doi: 10.1016/j.neurobiolaging.2005.03.019. Epub 2005 Jun 16.

Abstract

Neurospheres from adult mouse subventricular zone (SVZ) were grown in suspension cultures for 12-15 days. Neurospheres consisted mainly of neural precursor cells (NPCs) immunoreactive for nestin and also contained nestin-negative precursors. We used these neurospheres to determine the effects of synthetic beta-amyloid fragments (both betaAP(1-42) and betaAP(25-35)) on NPC proliferation, differentiation and survival. We show that neurospheres exposed to 25 microM betaAP(25-35) or betaAP(1-42) for 24 h (a toxic condition for mature neurons) did not undergo apoptosis. Instead, betaAP(25-35) orientated nestin-negative precursors towards nestin-positive NPCs and turned nestin-positive NPCs into neuroblasts. Intracerebroventricular infusion of full-length betaAP(1-42) increased the population of PSA-NCAM-positive cells in the SVZ, without affecting proliferation. We conclude that betaAP influences the fate of progenitor cells, driving their differentiation towards a neuronal lineage.

摘要

来自成年小鼠脑室下区(SVZ)的神经球在悬浮培养中生长12 - 15天。神经球主要由对巢蛋白呈免疫反应性的神经前体细胞(NPCs)组成,也包含巢蛋白阴性的前体细胞。我们使用这些神经球来确定合成β-淀粉样蛋白片段(βAP(1 - 42)和βAP(25 - 35))对NPC增殖、分化和存活的影响。我们发现,暴露于25微摩尔βAP(25 - 35)或βAP(1 - 42) 24小时(对成熟神经元有毒性的条件)的神经球并未发生凋亡。相反,βAP(25 - 35)使巢蛋白阴性的前体细胞向巢蛋白阳性的NPCs定向分化,并将巢蛋白阳性的NPCs转变为神经母细胞。脑室内注入全长βAP(1 - 42)增加了SVZ中PSA - NCAM阳性细胞的数量,而不影响增殖。我们得出结论,βAP影响祖细胞的命运,促使它们向神经元谱系分化。

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