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利用促甲状腺激素和霍乱毒素探究干扰素启动其抗病毒活性的机制。

Use of thyrotropin and cholera toxin to probe the mechanism by which interferon initiates its antiviral activity.

作者信息

Kohn L D, Friedman R M, Holmes J M, Lee G

出版信息

Proc Natl Acad Sci U S A. 1976 Oct;73(10):3695-9. doi: 10.1073/pnas.73.10.3695.

Abstract

Thyrotropin (10 muM) inhibited the antiviral activity of interferon. When added after interferon, thyrotropin (TSH) had no effect on antiviral activity. There was also no inhibition of interferon action in cells washed with medium between incubations with TSH and interferon. 125I-Labeled TSH and 125I-labeled cholera toxin could bind to preparations of mouse L-cell plasma membranes. The binding was specific in that it was prevented by unlabeled thyrotropin or cholera toxin, but not by insulin, glucagon, prolactin, growth hormone, human chorionic gonadotropin, or luteinizing hormone. Mouse interferon inhibited 125I-labeled TSH binding to L-cell plasma membranes. The effect of mouse interferon on 125I-labeled cholera toxon binding was more complex, inhibition occurring only after an initial enhancement at low interferon concentrations. A 10-fold higher concentration of interferon was required to inhibit 125I-labeled TSH binding. Mouse interferon was also able to displace bound 125I-labeled TSH, but not bound 125I-labeled cholera toxin. The interferon interaction with cell membranes was temperature-sensitive. Human interferon could induce changes in binding of 125I-labeled TSH and 125I-labeled cholera toxin to mouse L-cell plasma membranes similar to those induced by mouse interferon. Mouse interferon induced similar changes in plasma membranes of human KB-3 cells, which are insensitive to both human and mouse interferons. In view of these results, the species specificity of interferons does not appear to reside solely at the point of the initial interaction with their binding sites.

摘要

促甲状腺激素(10微摩尔)可抑制干扰素的抗病毒活性。在干扰素之后添加时,促甲状腺激素(TSH)对抗病毒活性没有影响。在用促甲状腺激素和干扰素孵育之间用培养基洗涤的细胞中,也没有对干扰素作用的抑制。125I标记的促甲状腺激素和125I标记的霍乱毒素可与小鼠L细胞膜制剂结合。这种结合具有特异性,因为未标记的促甲状腺激素或霍乱毒素可阻止其结合,但胰岛素、胰高血糖素、催乳素、生长激素、人绒毛膜促性腺激素或促黄体生成素则不能。小鼠干扰素可抑制125I标记的促甲状腺激素与L细胞膜的结合。小鼠干扰素对125I标记的霍乱毒素结合的影响更为复杂,仅在低干扰素浓度下最初增强后才出现抑制。抑制125I标记的促甲状腺激素结合需要高10倍的干扰素浓度。小鼠干扰素也能够置换结合的125I标记的促甲状腺激素,但不能置换结合的125I标记的霍乱毒素。干扰素与细胞膜的相互作用对温度敏感。人干扰素可诱导125I标记的促甲状腺激素和125I标记的霍乱毒素与小鼠L细胞膜结合的变化,类似于小鼠干扰素所诱导的变化。小鼠干扰素在人KB - 3细胞的细胞膜中诱导类似的变化,而人KB - 3细胞对人干扰素和小鼠干扰素均不敏感。鉴于这些结果,干扰素的种属特异性似乎并不完全存在于其与结合位点的初始相互作用点上。

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本文引用的文献

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Cellular binding characteristics of human interferon.人类干扰素的细胞结合特性
Virology. 1974 Feb;57(2):378-86. doi: 10.1016/0042-6822(74)90177-9.
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Inhibition of interferon action by plant lectins.
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