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钙螯合剂可增强45Ca在通透突触体和微粒体中的积累。

Calcium chelators enhance 45Ca accumulation in permeablized synaptosomes and in microsomes.

作者信息

Moore J E, Abercrombie R F

机构信息

Department of Physiology, Emory University School of Medicine, Atlanta, Georgia 30322, USA.

出版信息

Am J Physiol. 1996 Feb;270(2 Pt 1):C628-35. doi: 10.1152/ajpcell.1996.270.2.C628.

Abstract

The study of intracellular Ca2+ regulation usually requires using calcium chelators to adjust [Ca2+]. We examined the effects of these chelators on calcium accumulation in microsomes and saponin-permeabilized synaptosomes to assess their influence on apparent transport properties. At a fixed free Ca2+ of 0.6 microM, increasing ethylene glycol-bis(beta-aminoethyl ether)-N,N,N', N'-tetraacetic acid (EGTA) and total Ca2+ enhanced ATP-dependent 45Ca sequestration in synaptosomes and microsomes. The EGTA-Ca complex did not change the maximal initial calcium uptake rate or maximal steady-state accumulation. Rather, EGTA/Ca increased the apparent affinity of the microsomal transporter for Ca2+. The presence of the organic anion transport inhibitor probenicid (2.5 mM) had no effect on 45Ca accumulation in the presence of EGTA. Replacing part of the Ca2+ with Ni2+ but maintaining [Ca2+] approximately constant reduced 45Ca uptake, suggesting that the Ni-EGTA complex did not stimulate 45Ca transport. Our results imply that EGTA is not actively transported across the endoplasmic reticulum membrane, nor does the divalent ion-bound form of EGTA change the properties of the transporter. EGTA, and other mobile calcium chelators with similar structures, e.g., 1,2-bis(2-aminophenoxy)ethane-N,N,N',N'-tetraacetic acid, indo 1, and fluo 3, may increase calcium uptake by delivering more Ca2+ to its transport site.

摘要

细胞内钙离子调节的研究通常需要使用钙螯合剂来调节[Ca2+]。我们研究了这些螯合剂对微粒体和皂素通透突触体中钙积累的影响,以评估它们对表观转运特性的影响。在固定的游离Ca2+浓度为0.6微摩尔时,增加乙二醇双(β-氨基乙基醚)-N,N,N',N'-四乙酸(EGTA)和总Ca2+可增强突触体和微粒体中ATP依赖的45Ca螯合。EGTA-Ca复合物并未改变最大初始钙摄取速率或最大稳态积累。相反,EGTA/Ca增加了微粒体转运体对Ca2+的表观亲和力。有机阴离子转运抑制剂丙磺舒(2.5毫摩尔)的存在对EGTA存在时的45Ca积累没有影响。用Ni2+替代部分Ca2+但保持[Ca2+]大致恒定会降低45Ca摄取,这表明Ni-EGTA复合物不会刺激45Ca转运。我们的结果表明,EGTA不会主动转运穿过内质网膜,EGTA的二价离子结合形式也不会改变转运体的特性。EGTA以及其他具有类似结构的可移动钙螯合剂,如1,2-双(2-氨基苯氧基)乙烷-N,N,N',N'-四乙酸、indo 1和fluo 3,可能通过将更多Ca2+输送到其转运位点来增加钙摄取。

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