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正常细胞与恶性转化细胞中的膜变化及三磷酸腺苷含量

Membrane changes and adenosine triphosphate content in normal and malignant transformed cells.

作者信息

Vlodavsky I, Inbar M, Sachs L

出版信息

Proc Natl Acad Sci U S A. 1973 Jun;70(6):1780-4. doi: 10.1073/pnas.70.6.1780.

Abstract

Transformed fibroblasts had a low content of ATP when grown at a high cell density and a high content of ATP when grown at a low cell density. Concanavalin A agglutinated transformed cells with a low, but not those with a high, ATP content. Transformed cells with a high ATP content gained agglutinability after ATP depletion by inhibitors of the energy-generating systems, and those with a low ATP content lost their agglutinability after restoration of a high ATP content by glucose. Fixation of the surface membrane by formaldehyde, glutaraldehyde, or LaCl(3), inhibited agglutination of cells with an ATP content that allows agglutination. Normal fibroblasts grown at a high or a low cell density were not agglutinated by concanavalin A. Depletion of the cellular ATP content of normal cells induced agglutination only in cells grown at a high, but not at a low, cell density. A similar number of concanavalin A molecules was bound to the surface membrane of agglutinating and nonagglutinating fibroblasts. It is suggested that a high content of ATP inhibits the movement of concanavalin A binding sites, and that a low content of ATP allows, in transformed cells, a new distribution of binding sites to form the clusters required for cell agglutination. Agglutinability of transformed cells is determined by ATP content, and in normal cells changes in the content of ATP are by themselves not sufficient to induce agglutination. Transformed cells, therefore, do not have a control, presumably for membrane stability, that exists in normal cells.

摘要

转化的成纤维细胞在高细胞密度下生长时ATP含量低,而在低细胞密度下生长时ATP含量高。伴刀豆球蛋白A能凝集ATP含量低的转化细胞,但不能凝集ATP含量高的转化细胞。ATP含量高的转化细胞在能量产生系统的抑制剂使ATP耗竭后获得凝集性,而ATP含量低的转化细胞在通过葡萄糖恢复高ATP含量后失去凝集性。用甲醛、戊二醛或LaCl₃固定表面膜,抑制了具有允许凝集的ATP含量的细胞的凝集。在高或低细胞密度下生长的正常成纤维细胞不会被伴刀豆球蛋白A凝集。正常细胞的细胞ATP含量耗竭仅在高细胞密度而非低细胞密度下生长的细胞中诱导凝集。相同数量的伴刀豆球蛋白A分子与可凝集和不可凝集的成纤维细胞的表面膜结合。有人提出,高ATP含量会抑制伴刀豆球蛋白A结合位点的移动,而低ATP含量在转化细胞中允许结合位点重新分布以形成细胞凝集所需的簇。转化细胞的凝集性由ATP含量决定,而在正常细胞中,ATP含量的变化本身不足以诱导凝集。因此,转化细胞没有正常细胞中存在的可能用于膜稳定性的调控机制。

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