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哺乳动物细胞中腐胺和尸胺输出的表征:一种药理学方法

Characterization of putrescine and cadaverine export in mammalian cells. A pharmacological approach.

作者信息

Tjandrawinata R R, Hawel L, Byus C V

机构信息

Department of Biochemistry, University of California-Riverside 92521.

出版信息

Biochem Pharmacol. 1994 Dec 16;48(12):2237-49. doi: 10.1016/0006-2952(94)00420-x.

Abstract

We characterized the mechanism(s) involved in the efflux of putrescine/cadaverine from cultured mammalian cells using various pharmacological agents. Verapamil and quinine inhibited putrescine and cadaverine export in monocytic-leukemic RAW 264 and H35 hepatoma cells in a concentration-dependent manner with an IC50 in the micromolar range. Verapamil, which inhibits L-type calcium channels, inhibited putrescine export, regardless of whether calcium was present in the extracellular medium or not. Furthermore, the export of putrescine in the absence of verapamil did not appear to depend upon extracellular calcium. Neither intracellular calcium, external sodium, changes in intracellular pH nor phosphorylation affected the levels of putrescine export independently from changes in intracellular putrescine levels. The data suggest that verapamil and quinine inhibit putrescine/cadaverine efflux from the cell by binding directly to an integral membrane protein.

摘要

我们使用各种药理试剂,对培养的哺乳动物细胞中腐胺/尸胺外流所涉及的机制进行了表征。维拉帕米和奎宁以浓度依赖性方式抑制单核细胞白血病RAW 264和H35肝癌细胞中的腐胺和尸胺输出,IC50在微摩尔范围内。抑制L型钙通道的维拉帕米抑制了腐胺输出,无论细胞外培养基中是否存在钙。此外,在没有维拉帕米的情况下,腐胺的输出似乎不依赖于细胞外钙。细胞内钙、细胞外钠、细胞内pH值的变化以及磷酸化均未独立于细胞内腐胺水平的变化而影响腐胺输出水平。数据表明,维拉帕米和奎宁通过直接结合整合膜蛋白来抑制细胞中腐胺/尸胺的外流。

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