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动物细胞中葡萄糖摄取的调节。使用从未转化和猿猴病毒40转化的小鼠成纤维细胞培养物中分离的质膜囊泡进行的研究。

Modulation of glucose uptake in animal cells. Studies using plasma membrane vesicles isolated from nontransformed and simian virus 40-transformed mouse fibroblast cultures.

作者信息

Lever J E

出版信息

J Biol Chem. 1979 Apr 25;254(8):2961-7.

PMID:218958
Abstract

Plasma membrane vesicles isolated from nontransformed and Simian virus 40-transformed mouse fibroblast cultures catalyzed carrier-mediated D-glucose transport without detectable metabolic conversion to glucose 6-phosphate. Glucose transport activity was stereospecific, temperature-dependent, sensitive to inactivation by p-chloromercuriphenylsulfonate, and accompanied plasma membrane material during subcellular fractionation. D-Glucose efflux from vesicles was inhibited by phloretin, an inhibitor of glucose uptake in intact cells. Cytochalasin B, a potent inhibitor of glucose uptake when tested with the intact cells used for vesicle isolation did not inhibit glucose transport in vesicles despite the presence of high affinity cytochalasin binding sites in isolated membranes. The enhanced glucose uptake observed in intact cells after viral transformation was not expressed in vesicles: no significant differences in glucose transport specific activity could be detected in vesicle preparations from nontransformed and transformed mouse fibroblast cultures. These findings indicate that cellular components distinct from glucose carriers can mediate changes in glucose uptake in mouse fibroblast cultures in at least two cases: sensitivity to inhibition by cytochalasin B and the enhanced cellular sugar uptake observed after viral transformation.

摘要

从未转化和经猴病毒40转化的小鼠成纤维细胞培养物中分离出的质膜囊泡催化载体介导的D-葡萄糖转运,且未检测到代谢转化为6-磷酸葡萄糖的情况。葡萄糖转运活性具有立体特异性、温度依赖性,对对氯汞苯磺酸盐失活敏感,并且在亚细胞分级分离过程中与质膜物质相伴。泡囊中D-葡萄糖的外流受到根皮素的抑制,根皮素是完整细胞中葡萄糖摄取的抑制剂。细胞松弛素B在用其进行囊泡分离的完整细胞中测试时是一种有效的葡萄糖摄取抑制剂,但尽管分离的膜中存在高亲和力的细胞松弛素结合位点,它却不抑制囊泡中的葡萄糖转运。在病毒转化后完整细胞中观察到的葡萄糖摄取增强在囊泡中并未表现出来:从未转化和转化的小鼠成纤维细胞培养物制备的囊泡中,未检测到葡萄糖转运比活性有显著差异。这些发现表明,至少在两种情况下,与葡萄糖载体不同的细胞成分可以介导小鼠成纤维细胞培养物中葡萄糖摄取的变化:对细胞松弛素B抑制的敏感性以及病毒转化后观察到的细胞糖摄取增强。

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