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视网膜双极细胞中递质释放的两个组成部分:胞吐作用和突触小泡的动员。

Two components of transmitter release in retinal bipolar cells: exocytosis and mobilization of synaptic vesicles.

作者信息

Sakaba T, Tachibana M, Matsui K, Minami N

机构信息

Department of Psychology, Graduate School of Humanities and Sociology, The University of Tokyo, Bunkyo-ku, Japan.

出版信息

Neurosci Res. 1997 Apr;27(4):357-70. doi: 10.1016/s0168-0102(97)01168-1.

Abstract

Ca2+-transmitter release coupling was examined using bipolar cells with large presynaptic terminals dissociated from the goldfish retina. Presynaptic Ca2+ current (I(Ca)) was recorded under the whole-cell voltage clamp. Release of excitatory amino acid transmitter was simultaneously monitored as the current through N-methyl-D-asperate (NMDA) receptors of reporter cells or as the membrane capacitance (C(m)) change associated with exocytosis. When I(Ca) was activated by a long depolarizing pulse, a double-peaked transmitter-induced current (I(tr)) was elicited in reporter cells. The rapid component of I(tr) was evoked immediately after the onset of depolarization, and was affected only slightly by intracellularly applied Ca2+ chelators. The delayed slow component of I(tr) was elicited during depolarization once a fixed amount of Ca2+ was accumulated in presynaptic terminals, and its appearance was suppressed or retarded by Ca2+ chelators. Two components of transmitter release were also recognized by monitoring C(m) changes elicited by the activation of I(Ca). These results suggest that bipolar cells have at least two pools of synaptic vesicles; a small, immediately releasable pool and a large releasable pool. The rapid and the delayed slow components of transmitter release may reflect exocytosis and mobilization of synaptic vesicles, respectively.

摘要

利用从金鱼视网膜分离出的具有大的突触前终末的双极细胞,研究了Ca2+与递质释放的偶联。在全细胞电压钳制下记录突触前Ca2+电流(I(Ca))。兴奋性氨基酸递质的释放通过报告细胞N-甲基-D-天冬氨酸(NMDA)受体的电流或与胞吐作用相关的膜电容(C(m))变化同时进行监测。当I(Ca)由长去极化脉冲激活时,报告细胞中会诱发一个双峰递质诱导电流(I(tr))。I(tr)的快速成分在去极化开始后立即诱发,并且仅受到细胞内应用的Ca2+螯合剂的轻微影响。I(tr)的延迟慢成分在去极化过程中,一旦突触前终末积累了一定量的Ca2+就会诱发,并且其出现会被Ca2+螯合剂抑制或延迟。通过监测由I(Ca)激活引起的C(m)变化,也识别出了递质释放的两个成分。这些结果表明双极细胞至少有两群突触小泡;一群小的、可立即释放的小泡和一群大的可释放小泡。递质释放的快速和延迟慢成分可能分别反映了突触小泡的胞吐作用和动员。

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