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鉴定膜载体转运途径中的一个残基。

Identification of a residue in the translocation pathway of a membrane carrier.

作者信息

Yan R T, Maloney P C

机构信息

Department of Physiology, Johns Hopkins University Medical School, Baltimore, Maryland 21209.

出版信息

Cell. 1993 Oct 8;75(1):37-44.

PMID:8402899
Abstract

Preliminary work using directed mutagenesis proved that cysteine is not required for operation of UhpT, the anion exchange protein responsible for glucose 6-phosphate transport by E. coli. We then made a detailed study of C143 and C265, because these cysteines impart sensitivity to p-chloromercuribenzosulfonate (PCMBS), a sulfhydral agent resembling glucose 6-phosphate in size, shape, and charge. We showed that C143 was exposed to the cytoplasm, as expected from hydropathy analysis, but we found no sidedness for C265. Rather, C265 was accessible to PCMBS from both membrane surfaces. And since the attack at C265 was blocked by glucose 6-phosphate, position 265 must lie directly on the pathway taken by the substrate as it moves through this membrane carrier.

摘要

利用定向诱变进行的初步研究证明,大肠杆菌中负责转运6-磷酸葡萄糖的阴离子交换蛋白UhpT的运作并不需要半胱氨酸。然后我们对C143和C265进行了详细研究,因为这些半胱氨酸会使细胞对对氯汞苯磺酸盐(PCMBS)敏感,PCMBS是一种在大小、形状和电荷方面与6-磷酸葡萄糖类似的巯基试剂。我们发现,正如亲水性分析所预期的那样,C143暴露于细胞质中,但我们并未发现C265具有方向性。相反,PCMBS可以从膜的两个表面接触到C265。而且由于6-磷酸葡萄糖会阻止对C265的攻击,因此265位必定直接位于底物通过该膜载体时所经过的路径上。

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