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对氯汞苯磺酸盐与人红细胞核苷转运体不对称结合的证据。

Evidence for the asymmetrical binding of p-chloromercuriphenyl sulphonate to the human erythrocyte nucleoside transporter.

作者信息

Tse C M, Wu J S, Young J D

出版信息

Biochim Biophys Acta. 1985 Sep 10;818(3):316-24. doi: 10.1016/0005-2736(85)90005-7.

Abstract

Nucleosides cross the human erythrocyte membrane by a facilitated-diffusion process which is selectively inhibited by nanomolar concentrations of nitrobenzylthioinosine (NBMPR). The chemical asymmetry of the transporter was investigated by studying the effects of p-chloromercuriphenyl sulphonate (PCMBS) on uridine transport and high-affinity NBMPR binding in inside-out and right-side-out membrane vesicles, unsealed erythrocyte ghosts and intact cells. PCMBS was an effective inhibitor of the transporter (50% inhibition at 30 microM), but only when the organomercurial had access to the cytoplasmic membrane surface. PCMBS inhibition of NBMPR binding to ghosts was reversed by incubation with dithiothreitol. Both uridine and NBMPR were able to protect the transporter against PCMBS inhibition.

摘要

核苷通过易化扩散过程穿过人红细胞膜,该过程可被纳摩尔浓度的硝基苄基硫代肌苷(NBMPR)选择性抑制。通过研究对氯汞苯磺酸盐(PCMBS)对翻转和正常取向的膜囊泡、未封闭的红细胞血影及完整细胞中尿苷转运和高亲和力NBMPR结合的影响,对转运体的化学不对称性进行了研究。PCMBS是转运体的有效抑制剂(30微摩尔时50%抑制),但只有当有机汞能够接触到细胞质膜表面时才起作用。用二硫苏糖醇孵育可逆转PCMBS对血影中NBMPR结合的抑制。尿苷和NBMPR都能够保护转运体免受PCMBS的抑制。

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