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细胞松弛素B的膜效应。对大鼠肝癌细胞和其他细胞系中易化扩散过程的竞争性抑制以及对功能性转运位点形成的影响。

Membrane effects of cytochalasin B. Competitive inhibition of facilitated diffusion processes in rat hepatoma cells and other cell lines and effect on formation of functional transport sites.

作者信息

Plagemann P G, Zylka J H, Erbe J, Estensen R D

出版信息

J Membr Biol. 1975 Aug 11;23(1):77-90. doi: 10.1007/BF01870245.

Abstract

Cytochalasin B competitively inhibits the transport of 2-deoxy-D-glucose and thymidine in a number of different cell lines (Novikoff rat hepatoma cells, mouse L, S180 and Ki-MSV-transformed BALB/3T3 cells, and human HeLa cells). The apparent Km values for the transport of these substrates as well as the apparent Ki values for the inhibition by cytochalasin B are very similar for the various cell lines, and the effect is readily and completely reversed by removal of the chemical. Thymidine transport by Chinese hamster ovary cells however, is little affected by cytochalasin B, whereas the transport of 2-deoxy-D-glucose, uridine and guanine by these cells is competitively inhibited to about the same extent as in other cell lines. In addition and concomitant with the inhibition of cytokinesis and an alteration in cell shape, cytochalasin B also impairs and delays the formation of functional transport sites for thymidine, guanine and choline in synchronized populations of Novikoff cells without affecting the apparent affinities of the transport systems for their substrates. This effect is unrelated to the direct inhibition of the transport processes, since the drug does not directly inhibit choline transport and has no effect on the formation of 2-deoxy-D-glucose transport sites in spite of the fact that it strongly inhibits the transport of this substrate. The inhibition of functional transport sites may be due to the induction of a structural alteration in the membrane by cytochalasin B which impairs the insertion of new proteins of certain but not all transport systems into the membrane.

摘要

细胞松弛素B竞争性抑制多种不同细胞系(诺维科夫大鼠肝癌细胞、小鼠L细胞、S180细胞以及Ki-MSV转化的BALB/3T3细胞和人宫颈癌细胞)中2-脱氧-D-葡萄糖和胸苷的转运。这些底物转运的表观Km值以及细胞松弛素B抑制作用的表观Ki值在各种细胞系中非常相似,并且通过去除该化学物质,这种作用很容易且完全逆转。然而,中国仓鼠卵巢细胞的胸苷转运受细胞松弛素B的影响很小,而这些细胞中2-脱氧-D-葡萄糖、尿苷和鸟嘌呤的转运受到的竞争性抑制程度与其他细胞系大致相同。此外,与胞质分裂的抑制和细胞形状的改变同时发生的是,细胞松弛素B还会损害并延迟诺维科夫细胞同步群体中胸苷、鸟嘌呤和胆碱功能性转运位点的形成,而不影响转运系统对其底物的表观亲和力。这种作用与转运过程的直接抑制无关,因为该药物并不直接抑制胆碱转运,并且尽管它强烈抑制这种底物的转运,但对2-脱氧-D-葡萄糖转运位点的形成没有影响。功能性转运位点的抑制可能是由于细胞松弛素B诱导膜结构改变,从而损害某些但不是所有转运系统的新蛋白质插入膜中。

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