大鼠星形胶质细胞中的全细胞氯电流伴随着细胞形态的变化。
Whole-cell chloride currents in rat astrocytes accompany changes in cell morphology.
作者信息
Lascola C D, Kraig R P
机构信息
Committee on Neurobiology, University of Chicago, Illinois 60637, USA.
出版信息
J Neurosci. 1996 Apr 15;16(8):2532-45. doi: 10.1523/JNEUROSCI.16-08-02532.1996.
Astrocytes can change shape dramatically in response to increased physiological and pathological demands, yet the functional consequences of morphological change are unknown. We report the expression of Cl- currents after manipulations that alter astrocyte morphology. Whole-cell Cl- currents were elicited after (1) rounding up cells by brief exposure to trypsin; (2) converting cells from a flat polygonal to a process-bearing (stellate) morphology by exposure to serum-free Ringer's solution; and (3) swelling cells by exposure to hypo-osmotic solution. Zero-current potentials approximated the Nernst for Cl-, and rectification usually followed that predicted by the constant-field equation. We observed heterogeneity in the activation and inactivation kinetics, as well as in the relative degree of outward versus inward rectification. Cl- conductances were inhibited by 4, 4-diisothiocyanostilbene-2,2'-disulfonic acid (200 microM) and by Zn2+ (1 mM). Whole-cell Cl- currents were not expressed in cells without structural change. We investigated whether changes in cytoskeletal actin accompanying changes in astrocytic morphology play a role in the induction of shape-dependent Cl- currents. Cytochalasins, which disrupt actin polymers by enhancing actin-ATP hydrolysis, elicited whole-cell Cl- conductances in flat, polygonal astrocytes. In stellate cells, elevated intracellular Ca2+ (2 microM), which can depolymerize actin, enhanced Cl- currents, and high intracellular ATP (5 mM), required for repolymerization, reduced Cl- currents. Modulation of Cl- current by Ca2+ and ATP was blocked by concurrent whole-cell dialysis with phalloidin and DNase, respectively. Phalloidin stabilizes actin polymers and DNase inhibits actin polymerization. Dialysis with phalloidin also prevented hypo-osmotically activated Cl- currents. These results demonstrate how the expression of astrocyte Cl- currents can be dependent on cell morphology, the structure of actin, Ca2+ homeostasis, and metabolism.
星形胶质细胞可根据生理和病理需求的增加而显著改变形状,但其形态变化的功能后果尚不清楚。我们报告了在改变星形胶质细胞形态的操作后氯离子电流的表达情况。在以下三种情况下可诱发全细胞氯离子电流:(1)通过短暂暴露于胰蛋白酶使细胞变圆;(2)通过暴露于无血清林格氏液将细胞从扁平多边形形态转变为有突起的(星状)形态;(3)通过暴露于低渗溶液使细胞肿胀。零电流电位接近氯离子的能斯特电位,整流通常遵循恒场方程的预测。我们观察到激活和失活动力学以及外向与内向整流的相对程度存在异质性。氯离子电导受到4,4-二异硫氰基芪-2,2'-二磺酸(200微摩尔)和锌离子(1毫摩尔)的抑制。在没有结构变化的细胞中未表达全细胞氯离子电流。我们研究了伴随星形胶质细胞形态变化的细胞骨架肌动蛋白的变化是否在形状依赖性氯离子电流的诱导中起作用。细胞松弛素通过增强肌动蛋白-ATP水解来破坏肌动蛋白聚合物,在扁平的多边形星形胶质细胞中引发全细胞氯离子电导。在星状细胞中,可使肌动蛋白解聚的细胞内钙离子升高(2微摩尔)会增强氯离子电流,而肌动蛋白重新聚合所需的高细胞内ATP(5毫摩尔)会降低氯离子电流。钙离子和ATP对氯离子电流的调节分别被同时用鬼笔环肽和脱氧核糖核酸酶进行全细胞透析所阻断。鬼笔环肽可稳定肌动蛋白聚合物,脱氧核糖核酸酶可抑制肌动蛋白聚合。用鬼笔环肽透析也可防止低渗激活的氯离子电流。这些结果表明星形胶质细胞氯离子电流的表达如何依赖于细胞形态、肌动蛋白结构、钙离子稳态和代谢。
Zotero 插件