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在肌膜大囊泡中研究肌肉乳酸转运。

Muscle lactate transport studied in sarcolemmal giant vesicles.

作者信息

Juel C

机构信息

August Krogh Institute, University of Copenhagen, Denmark.

出版信息

Biochim Biophys Acta. 1991 May 31;1065(1):15-20. doi: 10.1016/0005-2736(91)90004-r.

Abstract

Lactate transport was studied in giant (median diameter 6.3 microns) sarcolemmal vesicles obtained by collagenase treatment of rat skeletal muscle. The lactate transport displayed stereospecificity, had a high temperature coefficient, and could be inhibited up to 90% with known transport inhibitors (PCMBS and cinnamate). In equilibrium exchange experiments, the L-lactate flux demonstrated saturation kinetics with Km = 23.7 mM and Vmax = 108 pmol cm-2 s-1. With lactate present on only one side of the membrane, (zero trans conditions), Vmax was reduced to 48 pmol cm-2 s-1. The flux rate displayed transacceleration. The lactate flux was coupled to a parallel H+ flux. Under equilibrium exchange conditions, the carrier-mediated lactate flux was not pH-dependent. In the zero trans experiments, H+ on the trans side acted as an inhibitor. The loaded form of the carrier reorients faster than the unloaded form, and the protonated form with no lactate bound reorients slowly or is immobile. When compared to intact muscles, the giant sarcolemmal vesicles retain their transport characteristics both qualitatively and quantitatively.

摘要

采用胶原酶处理大鼠骨骼肌获得巨型(中位直径6.3微米)肌膜囊泡,对其中的乳酸转运进行了研究。乳酸转运具有立体特异性,温度系数较高,且已知的转运抑制剂(对氯汞苯甲酸和肉桂酸)可将其抑制达90%。在平衡交换实验中,L-乳酸通量呈现饱和动力学,米氏常数(Km)为23.7 mM,最大反应速率(Vmax)为108 pmol cm-2 s-1。当乳酸仅存在于膜的一侧(零转条件)时,Vmax降至48 pmol cm-2 s-1。通量速率显示出转位加速现象。乳酸通量与平行的H+通量偶联。在平衡交换条件下,载体介导的乳酸通量不依赖于pH值。在零转实验中,转位侧的H+起抑制剂作用。载体的负载形式比未负载形式重新定向更快,而未结合乳酸的质子化形式重新定向缓慢或不移动。与完整肌肉相比,巨型肌膜囊泡在定性和定量方面均保留其转运特性。

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