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胰腺β细胞中含γ-氨基丁酸的突触样微囊泡的调节性胞吐作用。

Regulated exocytosis of GABA-containing synaptic-like microvesicles in pancreatic beta-cells.

作者信息

Braun Matthias, Wendt Anna, Birnir Bryndis, Broman Jonas, Eliasson Lena, Galvanovskis Juris, Gromada Jesper, Mulder Hindrik, Rorsman Patrik

机构信息

Department of Physiological Sciences, Lund University, BMC B11 SE-22184 Lund, Sweden.

出版信息

J Gen Physiol. 2004 Mar;123(3):191-204. doi: 10.1085/jgp.200308966. Epub 2004 Feb 9.

Abstract

We have explored whether gamma-aminobutyric acid (GABA) is released by regulated exocytosis of GABA-containing synaptic-like microvesicles (SLMVs) in insulin-releasing rat pancreatic beta-cells. To this end, beta-cells were engineered to express GABA(A)-receptor Cl(-)-channels at high density using adenoviral infection. Electron microscopy indicated that the average diameter of the SLMVs is 90 nm, that every beta-cell contains approximately 3,500 such vesicles, and that insulin-containing large dense core vesicles exclude GABA. Quantal release of GABA, seen as rapidly activating and deactivating Cl(-)-currents, was observed during membrane depolarizations from -70 mV to voltages beyond -40 mV or when Ca(2+) was dialysed into the cell interior. Depolarization-evoked GABA release was suppressed when Ca(2+) entry was inhibited using Cd(2+). Analysis of the kinetics of GABA release revealed that GABA-containing vesicles can be divided into a readily releasable pool and a reserve pool. Simultaneous measurements of GABA release and cell capacitance indicated that exocytosis of SLMVs contributes approximately 1% of the capacitance signal. Mathematical analysis of the release events suggests that every SLMV contains 0.36 amol of GABA. We conclude that there are two parallel pathways of exocytosis in pancreatic beta-cells and that release of GABA may accordingly be temporally and spatially separated from insulin secretion. This provides a basis for paracrine GABAergic signaling within the islet.

摘要

我们研究了在胰岛素释放的大鼠胰腺β细胞中,γ-氨基丁酸(GABA)是否通过含GABA的突触样微囊泡(SLMVs)的调节性胞吐作用释放。为此,利用腺病毒感染技术使β细胞高密度表达GABA(A)受体Cl(-)通道。电子显微镜显示,SLMVs的平均直径为90纳米,每个β细胞约含有3500个此类囊泡,且含胰岛素的大致密核心囊泡不含GABA。在膜电位从-70 mV去极化到-40 mV以上的电压时,或当Ca(2+)被透析到细胞内部时,观察到GABA的量子释放,表现为Cl(-)电流的快速激活和失活。当使用Cd(2+)抑制Ca(2+)内流时,去极化诱发的GABA释放受到抑制。对GABA释放动力学的分析表明,含GABA的囊泡可分为易释放池和储备池。同时测量GABA释放和细胞电容表明,SLMVs的胞吐作用对电容信号的贡献约为1%。对释放事件的数学分析表明,每个SLMV含有0.36 amol的GABA。我们得出结论,胰腺β细胞中有两条平行的胞吐途径,因此GABA的释放可能在时间和空间上与胰岛素分泌分开。这为胰岛内的旁分泌GABA能信号传导提供了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3631/2217446/cf64ab940812/200308966f1.jpg

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