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蛋白质与干扰素反应增强子的结合,与正常及对干扰素耐药的Friend细胞中2'-5'-寡腺苷酸合成酶的干扰素诱导作用相关。

Protein binding to the interferon response enhancer correlates with interferon induction of 2'-5'-oligoadenylate synthetase in normal and interferon-resistant Friend cells.

作者信息

Coccia E M, Vaiman D, Raber J, Marziali G, Fiorucci G, Orsatti R, Cohen B, Nissim N, Romeo G, Affabris E

机构信息

Laboratorio di Virologia, Istituto Superiore di Sanità, Rome, Italy.

出版信息

J Virol. 1991 Apr;65(4):2081-7. doi: 10.1128/JVI.65.4.2081-2087.1991.

Abstract

The induction of transcription of the 2'-5'-oligoadenylate (2-5A) synthetase gene by type I (alpha/beta) and type II (gamma) interferons (IFNs) has been studied in wild-type (w.t.) and IFN-resistant Friend leukemia cells (FLC). Following IFN treatment, new complexes are formed in vitro between the IFN-responsive sequence (IRS) of the 2-5A synthetase gene and cellular proteins. Within minutes after IFN-alpha/beta addition to w.t. FLC, an IRS-protein complex, designated F1, is detected, as already observed in several human cell lines. In response to IFN-gamma, a novel complex, designated Fg, is observed in w.t. FLC. The Fg complex appears within 3 h, while an F1-like complex is faintly visible 10 to 24 h later. In the IFN-alpha/beta-resistant FLC, IFN-gamma induces only the Fg complex and fails to induce F1. Fg formation is correlated with the IFN-gamma-induced transcription of the 2-5A synthetase gene and the appearance of the corresponding enzymatic activity in both w.t. and IFN-alpha/beta-resistant FLC. These findings suggest that F1 and Fg represent two distinct effector complexes by which type I and type II IFNs, respectively, induce 2-5A synthetase.

摘要

在野生型(w.t.)和对干扰素(IFN)耐药的弗瑞德白血病细胞(FLC)中,研究了I型(α/β)和II型(γ)干扰素(IFN)对2'-5'-寡腺苷酸(2-5A)合成酶基因转录的诱导作用。IFN处理后,2-5A合成酶基因的IFN反应序列(IRS)与细胞蛋白在体外形成新的复合物。在向野生型FLC添加IFN-α/β后的几分钟内,检测到一种IRS-蛋白复合物,命名为F1,这在几种人类细胞系中已观察到。对IFN-γ的反应中,在野生型FLC中观察到一种新的复合物,命名为Fg。Fg复合物在3小时内出现,而一种类似F1的复合物在10至24小时后微弱可见。在对IFN-α/β耐药的FLC中,IFN-γ仅诱导Fg复合物,而不能诱导F1。Fg的形成与IFN-γ诱导的2-5A合成酶基因转录以及野生型和对IFN-α/β耐药的FLC中相应酶活性的出现相关。这些发现表明,F1和Fg代表两种不同的效应复合物,I型和II型IFN分别通过它们诱导2-5A合成酶。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/98e0/240065/1b1cf95553b6/jvirol00047-0427-a.jpg

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