首页> 美国卫生研究院文献>The Journal of Neuroscience >Modulation of calcium channels in human retinal glial cells by basic fibroblast growth factor: a possible role in retinal pathobiology
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Modulation of calcium channels in human retinal glial cells by basic fibroblast growth factor: a possible role in retinal pathobiology

机译:碱性成纤维细胞生长因子对人视网膜胶质细胞钙通道的调节:在视网膜病理生物学中的可能作用

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摘要

The objective of this study was to begin to examine the cellular and biophysical effects on human retinal glial cells of basic fibroblast growth factor (bFGF), which is endogenous to the retina and likely to play a role in retinal pathobiology. Experiments were performed on cultured glial cells derived from the adult postmortem retina. A proliferative response to bFGF established a sensitivity of the retinal glia to this growth factor. The possibility that bFGF alters calcium currents was assessed using the whole-cell recording configuration of the patch-clamp technique to analyze inward currents carried by barium. Two types of voltage-gated calcium channels could be expressed by the glial cells. One, similar to the T-type current described in various kinds of cells, had a low threshold of activation, a transient response, and an insensitivity to the dihydropyridine nifedipine. The other type of inward current, which closely resembles the L-type calcium current found in other cells, had a high threshold, had a long- lasting response, and was inhibited by nifedipine. When continuous whole-cell recordings were made from retinal glial cells, the L-type calcium current increased significantly within 20 min after exposure of the cells to bFGF. The physiological significance of this modulatory effect remains uncertain, though the observation that nifedipine inhibits both the L-type calcium current and the bFGF-induced proliferation is consistent with the hypothesis that dihydropyridine- sensitive channels may play a role in modulating the mitogenic response of retinal glial cells to this growth factor.
机译:这项研究的目的是开始研究碱性成纤维细胞生长因子(bFGF)对人视网膜胶质细胞的细胞和生物物理作用,它是视网膜内源性的,可能在视网膜病理生物学中起作用。对源自成年死后视网膜的培养的神经胶质细胞进行了实验。对bFGF的增殖反应建立了视网膜胶质对此生长因子的敏感性。使用膜片钳技术的全细胞记录配置来评估bFGF改变钙电流的可能性,以分析钡携带的内向电流。胶质细胞可以表达两种类型的电压门控钙通道。一种类似于在各种细胞中描述的T型电流,其活化阈值低,瞬态响应和对二氢吡啶硝苯地平不敏感。另一种内向电流与其他细胞中的L型钙电流非常相似,具有较高的阈值,具有长效响应,并被硝苯地平抑制。当从视网膜胶质细胞连续记录全细胞时,细胞暴露于bFGF后20分钟内L型钙电流显着增加。尽管观察到硝苯地平同时抑制L型钙电流和bFGF诱导的增殖,但这种调节作用的生理学意义仍不确定,这与二氢吡啶敏感通道可能在调节视网膜有丝分裂反应中起作用的假设一致。胶质细胞就是这种生长因子。

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