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精浆核糖核酸酶抗肿瘤作用中的关键细胞外和细胞内步骤。

Key extracellular and intracellular steps in the antitumor action of seminal ribonuclease.

作者信息

Mastronicola M R, Piccoli R, D'Alessio G

机构信息

Department of Organic and Biological Chemistry, University of Naples, Federico II, Italy.

出版信息

Eur J Biochem. 1995 May 15;230(1):242-9. doi: 10.1111/j.1432-1033.1995.tb20557.x.

Abstract

Bovine seminal ribonuclease (RNase) is a cytotoxin with a selective action toward tumor cells. We report here the results of an investigation that elucidate key extracellular and intracellular steps of the mechanism of its antitumor action. Seminal RNase is found to bind specifically to a large number of binding sites on the extracellular matrix of target cells, whereas other homologous RNases, including a monomeric derivative of the protein, do not bind. The key role of the pericellular matrix is confirmed by the finding that malignant cells grown in suspension bind negligible amounts of protein, and are resistant to its toxic effects, whereas the same cells, grown in monolayers, bind high amounts of seminal RNase and are killed by the protein. Seminal RNase is internalized by malignant cells, where it degrades rRNA and inhibits protein synthesis. These effects are not detectable when catalytically inactivated enzyme, or a catalytically active, monomeric derivative of the enzymes, are employed. The enzyme is bound and internalized also by the corresponding non-malignant cells, but no effects are detectable on RNA stability and on protein synthesis in these cells. This might be attributed to a different intracellular management in normal cells of the cytotoxic protein.

摘要

牛精核糖核酸酶(RNase)是一种对肿瘤细胞具有选择性作用的细胞毒素。我们在此报告一项研究结果,该研究阐明了其抗肿瘤作用机制的关键细胞外和细胞内步骤。发现精浆RNase能特异性结合靶细胞细胞外基质上的大量结合位点,而其他同源核糖核酸酶,包括该蛋白的单体衍生物,则不结合。细胞周围基质的关键作用通过以下发现得到证实:悬浮培养的恶性细胞结合的蛋白量可忽略不计,并且对其毒性作用具有抗性,而单层培养的相同细胞则结合大量精浆RNase并被该蛋白杀死。精浆RNase被恶性细胞内化,在细胞内它降解rRNA并抑制蛋白质合成。当使用催化失活的酶或该酶的催化活性单体衍生物时,这些作用无法检测到。该酶也能被相应的非恶性细胞结合并内化,但在这些细胞中对RNA稳定性和蛋白质合成没有可检测到的影响。这可能归因于正常细胞中对细胞毒性蛋白的不同细胞内处理方式。

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