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来自可移植大鼠胰岛素瘤的细胞和分泌颗粒中的5-羟色胺转运

5-Hydroxytryptamine transport in cells and secretory granules from a transplantable rat insulinoma.

作者信息

Hutton J C, Peshavaria M, Tooke N E

出版信息

Biochem J. 1983 Mar 15;210(3):803-10. doi: 10.1042/bj2100803.

Abstract

Mechanisms of transport of 5-hydroxytryptamine in the pancreatic B-cell were investigated by using cell suspensions and secretory granules prepared from a transplantable rat insulinoma. (1) Cells incubated with 5-hydroxy[G-3H]tryptamine at concentrations ranging from 0.1 microM to 5 mM accumulated the radioisotope principally by a simple diffusion process. The incorporated radioactivity was recovered principally as the parent molecule and was recovered predominantly in soluble protein and secretory-granule fractions prepared from the tissue. (2) Isolated granules incubated in buffered iso-osmotic medium without ATP accumulated the amine to concentrations up to 38-fold that of the medium. This process was insensitive to reserpine and occurred over a wide range of 5-hydroxytryptamine concentrations (0.075 microM-25 mM). Above 5 mM, 5-hydroxytryptamine accumulation decreased in parallel with the breakdown of the delta pH across the granule membrane. Uptake was favoured by alkaline media and was reduced by the addition of (NH4)2SO4. In both cases a close correlation was observed between uptake and the transmembrane delta pH, a finding that suggested that 5-hydroxytryptamine permeated the membrane as the free base and equilibrated across the membrane with the delta pH. Binding of 5-hydroxytryptamine to granule constituents also played a part in this process. ATP caused a further doubling of granule 5-hydroxytryptamine uptake by a process that was sensitive to reserpine (0.5 microM). Inhibitor studies suggested that amine transport in this instance was linked to the activity of the granule membrane proton-translocating ATPase. (3) It was concluded that the uptake of amines driven by proton gradients across the insulin-granule membrane could account for the accumulation in vivo of amines in the B-cell.

摘要

利用从可移植大鼠胰岛素瘤制备的细胞悬液和分泌颗粒,研究了5-羟色胺在胰腺β细胞中的转运机制。(1) 用浓度范围为0.1微摩尔/升至5毫摩尔/升的5-羟[G-3H]色胺孵育细胞,放射性同位素主要通过简单扩散过程积累。掺入的放射性主要以母体分子形式回收,并且主要在从组织制备的可溶性蛋白质和分泌颗粒组分中回收。(2) 在无ATP的缓冲等渗介质中孵育的分离颗粒将胺积累到高达介质浓度38倍的浓度。这个过程对利血平不敏感,并且在很宽的5-羟色胺浓度范围(0.075微摩尔/升 - 25毫摩尔/升)内发生。高于5毫摩尔/升时,5-羟色胺的积累与颗粒膜两侧ΔpH的破坏平行下降。碱性介质有利于摄取,添加(NH4)2SO4会降低摄取。在这两种情况下,摄取与跨膜ΔpH之间都观察到密切相关性,这一发现表明5-羟色胺以游离碱形式渗透膜并与ΔpH跨膜平衡。5-羟色胺与颗粒成分的结合在这个过程中也起作用。ATP通过对利血平(0.5微摩尔/升)敏感的过程使颗粒5-羟色胺摄取进一步加倍。抑制剂研究表明,在这种情况下胺转运与颗粒膜质子转运ATP酶的活性有关。(3) 得出的结论是,由质子梯度驱动的胺跨胰岛素颗粒膜的摄取可以解释体内胺在β细胞中的积累。

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