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低细胞外钙足以维持小鼠中脑神经前体细胞的存活和增殖。

Low extracellular calcium is sufficient for survival and proliferation of murine mesencephalic neural precursor cells.

作者信息

Milosevic Javorina, Juch Franziska, Storch Alexander, Schwarz Johannes

机构信息

Department of Neurology, University of Leipzig, Leipzig, Germany.

出版信息

Cell Tissue Res. 2006 Jun;324(3):377-84. doi: 10.1007/s00441-005-0147-3. Epub 2006 Feb 24.

Abstract

Various media and Ca2+ concentrations are employed to culture neural progenitor cells (NPCs). We have therefore explored the effects of extracellular calcium concentrations on the survival, proliferation, spontaneous apoptosis and self-renewal capacity of mesencephalic NPCs grown adherently and as free-floating neurospheres. We employed EMEM supplemented with various concentrations of extracellular CaCl2 (0.1-1 mM). Raising the calcium concentration from 0.1 mM to 0.6 mM resulted in an increased number of NPCs growing as a monolayer and increased the protein yield of cells growing in neurospheres (24+/-3 microg total proteins in 0.1 mM Ca2+ medium vs. 316+/-34 microg proteins in 1 mM Ca2+ medium). Concentrations more than 0.6 mM did not result in a further improvement of proliferation or survival. Elimination of calcium from our control medium by 1 mM EGTA resulted in a decrease in cell number from 82+/-2 x 10(4) NPCs/ml observed in control medium to 62+/-2 x 10(4) NPCs/ml observed in calcium-free media. Protein yield dropped significantly in calcium-free media, accompanied by the decreased expression of the proliferation marker PCNA and the pro-survival marker Bcl-2. Two weeks of expansion as neurospheres caused spontaneous cell death in more than 90% of NPCs grown in 0.1 mM CaCl2 EMEM compared with 42% in 1 mM CaCl2 EMEM. Although the action of Ca2+ on NPCs appears to be complex, the presented data strongly suggest that extracellular calcium plays a crucial role in the maintenance of NPCs in a healthy and proliferating state; physiological concentrations (>1.0 mM) are not required, a concentration of 0.5 mM being adequate for cell maintenance.

摘要

人们采用各种培养基和钙离子浓度来培养神经祖细胞(NPCs)。因此,我们探究了细胞外钙浓度对贴壁生长和悬浮生长的中脑NPCs的存活、增殖、自发凋亡及自我更新能力的影响。我们使用添加了不同浓度细胞外氯化钙(0.1 - 1 mM)的伊格尔氏最低限度必需培养基(EMEM)。将钙浓度从0.1 mM提高到0.6 mM,导致单层生长的NPCs数量增加,且悬浮生长的细胞蛋白质产量提高(0.1 mM钙离子培养基中总蛋白质为24±3微克,而1 mM钙离子培养基中为316±34微克)。超过0.6 mM的浓度并未使增殖或存活进一步改善。通过1 mM乙二醇双四乙酸(EGTA)从我们的对照培养基中去除钙,导致细胞数量从对照培养基中观察到的82±2×10⁴个NPCs/毫升降至无钙培养基中观察到的62±2×10⁴个NPCs/毫升。无钙培养基中的蛋白质产量显著下降,同时增殖标志物增殖细胞核抗原(PCNA)和促存活标志物Bcl - 2的表达降低。作为神经球扩增两周后,在0.1 mM氯化钙EMEM中生长的NPCs中有超过90%发生自发细胞死亡,而在1 mM氯化钙EMEM中为42%。尽管钙离子对NPCs的作用似乎很复杂,但所呈现的数据强烈表明,细胞外钙在维持NPCs处于健康和增殖状态中起着关键作用;不需要生理浓度(>1.0 mM),0.5 mM的浓度足以维持细胞。

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