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糖皮质激素对大鼠脂肪细胞中己糖转运的影响。质膜中转运体减少的证据。

Effect of glucocorticoids on hexose transport in rat adipocytes. Evidence for decreased transporters in the plasma membrane.

作者信息

Carter-Su C, Okamoto K

出版信息

J Biol Chem. 1985 Sep 15;260(20):11091-8.

PMID:4040912
Abstract

Glucocorticoids are known to rapidly inhibit glucose transport when added to isolated rat adipocytes. To determine whether this inhibition of transport persists following isolation of the plasma membranes, adipocytes were incubated in the absence or presence of a maximally inhibitory concentration of dexamethasone, a synthetic glucocorticoid, and plasma membrane vesicles were prepared. D-Glucose uptake into vesicles from steroid-treated cells was inhibited by an average of 40%. The ability of dexamethasone to inhibit transport depended upon pretreatment of cells with hormone prior to membrane isolation. Furthermore, the decreased rate of transport was prevented by the simultaneous addition to the cell of actinomycin D or cycloheximide with dexamethasone, indicating a requirement for RNA and protein synthesis. The effect of dexamethasone on glucose transport was further investigated using our recently developed cytochalasin B affinity-labeling protocol to identify the transporter on sodium dodecyl sulfate-polyacrylamide gels. A peak of radioactivity having Mr = 54,000 was identified which exhibited the properties expected for the glucose transporter, in that label incorporation was prevented by D-glucose and unlabeled cytochalasin B, but not by D-sorbitol or unlabeled cytochalasins A, D, or E. Dexamethasone was found to cause a significant (average 33%) decrease in the amount of labeled transporter in the plasma membrane which was prevented by the simultaneous addition of actinomycin D with dexamethasone to the cells. A similar percentage decrease was not found in a microsomal membrane fraction nor in a total cellular membrane fraction. These results suggest that glucocorticoids may decrease glucose transport in rat adipocytes by selectively decreasing the number of transporters in the plasma membrane.

摘要

已知将糖皮质激素添加到分离的大鼠脂肪细胞中时,能迅速抑制葡萄糖转运。为了确定在分离质膜后这种转运抑制是否持续存在,将脂肪细胞在不存在或存在最大抑制浓度的地塞米松(一种合成糖皮质激素)的情况下进行孵育,然后制备质膜囊泡。来自用类固醇处理过的细胞的囊泡对D-葡萄糖的摄取平均被抑制了40%。地塞米松抑制转运的能力取决于在膜分离之前用激素对细胞进行预处理。此外,通过在细胞中同时添加放线菌素D或环己酰亚胺与地塞米松,可防止转运速率降低,这表明需要RNA和蛋白质合成。使用我们最近开发的细胞松弛素B亲和标记方案,在地十二烷基硫酸钠-聚丙烯酰胺凝胶上鉴定转运体,进一步研究了地塞米松对葡萄糖转运的影响。鉴定出一个分子量为54,000的放射性峰值,其表现出葡萄糖转运体预期的特性,即D-葡萄糖和未标记的细胞松弛素B可阻止标记掺入,但D-山梨醇或未标记的细胞松弛素A、D或E则不能。发现地塞米松会导致质膜中标记的转运体数量显著减少(平均33%),而在细胞中同时添加放线菌素D与地塞米松可防止这种减少。在微粒体膜部分或总细胞膜部分未发现类似百分比的减少。这些结果表明,糖皮质激素可能通过选择性减少质膜中转运体的数量来降低大鼠脂肪细胞中的葡萄糖转运。

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