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首页> 外文期刊>Stem cell research >Multiple mechanisms mediate the taurine-induced proliferation of neural stem/progenitor cells from the subventricular zone of the adult mouse - ScienceDirect
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Multiple mechanisms mediate the taurine-induced proliferation of neural stem/progenitor cells from the subventricular zone of the adult mouse - ScienceDirect

机译:多种机制介导牛磺酸诱导成年小鼠脑室下区神经干/祖细胞的增殖-ScienceDirect

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摘要

Taurine was previously reported to increase the proliferation of neural precursor cells (NPCs) from subventricular zone of the mouse brain. The results of a study that aimed to understand the mechanisms of this effect are presented here. Because taurine was not found in NPC nuclei, direct interactions with nuclear elements seem unlikely. A gene expression profile analysis indicated that genes that are regulated by taurine have roles in i) proliferation, including the Shh and Wnt pathways; ii) cellular adhesion; iii) cell survival; and iv) mitochondrial functioning. Cell cycle analysis of propidium iodide and CFSE-labeled cells using flow cytometry revealed an increase in the number of cells in the S-phase and a decrease in those in the G0/G1 phase in taurine-treated cultures. No changes in the length of the cell cycle were observed. Quantification of the viable, apoptotic, and necrotic cells in cultures using flow cytometry and calcein-AM, annexin-V, and propidium iodide staining showed reductions in the number of apoptotic and necrotic cells (18% to 11% and 13% to 10%, respectively) and increases in the number of viable cells (61% to 69%) in the taurine-treated cultures. Examination of the relative mitochondrial potential values by flow cytometry and rhodamine123 or JC-1 staining showed a 44% increase in the number of cells with higher mitochondrial potential and a 38% increase in the mitochondrial membrane potential in taurine cultures compared with those of controls. Taken together, the results suggest that taurine provides more favorable conditions for cell proliferation by improving mitochondrial functioning.
机译:以前曾报道牛磺酸可增加小鼠脑室下区域神经前体细胞(NPC)的增殖。本文介绍了旨在了解这种作用机理的研究结果。由于在NPC核中未发现牛磺酸,因此与核元素的直接相互作用似乎不太可能。基因表达谱分析表明,牛磺酸调节的基因在i)增殖中起作用,包括Shh和Wnt途径; ii)细胞粘附; iii)细胞存活; iv)线粒体功能。使用流式细胞术对碘化丙啶和CFSE标记的细胞进行细胞周期分析,结果显示,牛磺酸处理的培养物中S期细胞数量增加,而G0 / G1期细胞数量减少。没有观察到细胞周期长度的变化。使用流式细胞仪和钙黄绿素-AM,膜联蛋白-V和碘化丙锭染色对培养物中的存活,凋亡和坏死细胞进行定量,结果显示凋亡和坏死细胞的数量减少了(18%至11%和13%至10%分别)和牛磺酸处理的培养物中活细胞数量的增加(61%至69%)。通过流式细胞术和若丹明123或JC-1染色检查相对线粒体电位值,与对照相比,牛磺酸培养物中具有较高线粒体电位的细胞数量增加了44%,线粒体膜电位增加了38%。两者合计,结果表明牛磺酸通过改善线粒体功能为细胞增殖提供了更有利的条件。

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