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干扰素可增强胚胎癌细胞中的2-5A合成酶。

Interferon enhances 2-5A synthetase in embryonal carcinoma cells.

作者信息

Wood J N, Hovanessian A G

出版信息

Nature. 1979 Nov 1;282(5734):74-6. doi: 10.1038/282074a0.

Abstract

Mouse teratocarcinomas provide a useful model of mammalian differentiation, because the malignant embryonal carcinoma (EC) stem cells of such tumours may produce various differential cell types in vivo or in vitro. Many EC cell lines have now been established and classified on the basis of their ability to differentiate in vivo into cell types characteristically derived from any of the three germ layers. There is convincing evidence that EC cells can neither produce interferon, nor respond to it by becoming resistant to virus, whereas differentiated cells derived from EC lines behave normally in both respects. We investigated the lack of responsiveness of EC cells towards interferon by measuring the levels of two double-stranded RNA-dependent enzyme activities recently shown to be enhanced by interferon. We report here that on treatment with interferon, EC cells show increased 2-5A synthetase levels comparable to those found in differentiated cells, while there is little or no effect on kinase activity in EC cells, in contrast to their differentiated counterparts.

摘要

小鼠畸胎癌为哺乳动物分化提供了一个有用的模型,因为此类肿瘤的恶性胚胎癌(EC)干细胞在体内或体外可产生多种分化细胞类型。目前已建立了许多EC细胞系,并根据它们在体内分化为典型地源自三个胚层中任何一个胚层的细胞类型的能力进行分类。有确凿证据表明,EC细胞既不能产生干扰素,也不会通过对病毒产生抗性来对干扰素作出反应,而源自EC细胞系的分化细胞在这两方面表现正常。我们通过测量最近显示可被干扰素增强的两种双链RNA依赖性酶活性水平,研究了EC细胞对干扰素缺乏反应性的情况。我们在此报告,用干扰素处理后,EC细胞显示出与分化细胞中相当的2-5A合成酶水平升高,而与它们的分化对应物相比,对EC细胞中的激酶活性几乎没有影响。

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