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两种干扰素诱导的翻译抑制剂的分离:一种蛋白激酶和一种寡聚异腺苷酸合成酶。

Isolation of two interferon-induced translational inhibitors: a protein kinase and an oligo-isoadenylate synthetase.

作者信息

Zilberstein A, Kimchi A, Schmidt A, Revel M

出版信息

Proc Natl Acad Sci U S A. 1978 Oct;75(10):4734-8. doi: 10.1073/pnas.75.10.4734.

Abstract

Large-scale purification of translational inhibitors present in interferon-treated mouse L cells, but not in untreated cells, led to the isolation of two interferon-induced activities. One is a protein kinase system that is activatable by double-stranded RNA and ATP and that phosphorylates a Mr 67,000 protein and the smallest subunit of eukaryotic initiation factor-2. The purified protein kinase is a strong translational inhibitor. The second activity is an enzyme that, with double-stranded RNA, slowly polymerizes ATP into oligoadenylate with a 2'-5' phosphodiester linkage. The oligo-isoadenylate in turn activates a potent inhibitor of mRNA translation.

摘要

对经干扰素处理的小鼠L细胞(而非未处理的细胞)中存在的翻译抑制剂进行大规模纯化,从而分离出两种干扰素诱导活性。一种是蛋白激酶系统,可被双链RNA和ATP激活,能使分子量为67,000的蛋白质和真核起始因子-2的最小亚基磷酸化。纯化后的蛋白激酶是一种强效翻译抑制剂。第二种活性是一种酶,它与双链RNA一起能缓慢地将ATP聚合成具有2'-5'磷酸二酯键的寡腺苷酸。寡异腺苷酸继而激活一种强效的mRNA翻译抑制剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/572a/336194/9e6d4f43722d/pnas00669-0109-a.jpg

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