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在细胞松弛素介导的细胞铺展抑制过程中钙电蛋白和依钙结合蛋白I的合成

Synthesis of calelectrins and calpactin I during cytochalasin mediated cell spreading inhibition.

作者信息

Hom Y K, Marinkovich M P, Lozano J J, Rocha V

机构信息

Biology Board of Studies, University of California, Santa Cruz.

出版信息

Cell Calcium. 1989 Apr;10(3):135-44. doi: 10.1016/0143-4160(89)90067-5.

Abstract

Mammary epithelial cell spreading on collagen gels has previously been shown to be correlated with the synthesis of a group of calcium-binding proteins (CBPs) which we have identified as the calcium-binding proteins termed calelectrins and calpactin I monomer/p36. To determine whether cell spreading per se is required for CBP synthesis, we examined the effect of cytochalasin D on these two events. Concentrations of cytochalasin D that did not reduce total protein synthesis, caused inhibition of cell spreading in a dose-dependent manner, but did not cause inhibition of CBP synthesis. Synthesis of collagen also continued during cytochalasin inhibition of cell spreading. Removal of the inhibitor from the cultures initiated cell spreading and CBP synthesis continued. Membrane-cytoskeleton complexes from control and CD treated cells were identical in regard to binding CBPs in a calcium-dependent manner. Colchicine, which inhibited cell spreading, was shown to be toxic to general protein synthesis at 75 nM. The data clearly indicate that mere inhibition of epithelial cell spreading does not automatically suppress CBP synthesis.

摘要

先前已表明,乳腺上皮细胞在胶原蛋白凝胶上的铺展与一组钙结合蛋白(CBPs)的合成相关,我们已将这些钙结合蛋白鉴定为称为钙电蛋白和钙促凝血蛋白I单体/p36的钙结合蛋白。为了确定CBP合成本身是否需要细胞铺展,我们研究了细胞松弛素D对这两个事件的影响。细胞松弛素D的浓度在不降低总蛋白合成的情况下,以剂量依赖的方式抑制细胞铺展,但不抑制CBP合成。在细胞松弛素抑制细胞铺展期间,胶原蛋白的合成也持续进行。从培养物中去除抑制剂后,细胞开始铺展,CBP合成继续。对照细胞和经细胞松弛素D处理的细胞的膜 - 细胞骨架复合物在以钙依赖方式结合CBPs方面是相同的。秋水仙碱可抑制细胞铺展,在75 nM时对一般蛋白质合成具有毒性。数据清楚地表明,单纯抑制上皮细胞铺展不会自动抑制CBP合成。

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