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多烯增强聚肌苷酸-聚胞苷酸诱导干扰素产生的机制研究。

Mechanistic studies of polyene enhancement of interferon production by polyriboinosinic-polyribocytidylic acid.

作者信息

Borden E C, Booth B W, Leonhardt P H

出版信息

Antimicrob Agents Chemother. 1978 Feb;13(2):159-64. doi: 10.1128/AAC.13.2.159.

Abstract

The production of interferon by polyriboinosinic-polyribocytidylic acid [poly(I) . poly(C)] and poly(I) . poly(C)-diethylaminoethyl-dextran in L929 cells was enhanced from 10 to 100 times by polyene macrolides, including amphotericin B (AmB), AmB methyl ester, nystatin, and filipin. AmB and its water-soluble methyl ester were the most effective; retinol, a nonmacrolide polyene, was ineffective. Interferon induction by Newcastle disease virus was not enhanced by AmB. The kinetics of interferon production were not markedly altered by AmB. Polyenes and poly(I) . poly(C)-diethylaminoethyl-dextran did not need to be present on cells simultaneously to enhance interferon production. Pretreatment with polyenes was as effective as simultaneous addition. Even treatment of washed cells, several hours after removal of poly(I) . poly(C)-diethylaminoethyl-dextran, resulted in enhancement of interferon production. AmB did not appear to form a macromolecular complex with poly(I) . poly(C) in that neither the ultraviolet absorption spectrum nor the melting point of poly(I) . poly(C) was altered by mixing with AmB. Isotopic studies indicated that AmB did not enhance binding of poly(I) . poly(C) to cells. Since the macrolide polyenes have been demonstrated to bind to cell membrane sterols with subsequent alterations in membrane permeability barriers, they may enhance interferon production by increasing cell penetration of poly(I) . poly(C).

摘要

在L929细胞中,多聚肌苷酸-多聚胞苷酸[聚(I)·聚(C)]和聚(I)·聚(C)-二乙氨基乙基葡聚糖产生干扰素的能力,被包括两性霉素B(AmB)、两性霉素B甲酯、制霉菌素和菲律宾菌素在内的多烯大环内酯增强了10到100倍。AmB及其水溶性甲酯最为有效;视黄醇,一种非大环内酯多烯,没有效果。新城疫病毒诱导的干扰素产生未被AmB增强。AmB未显著改变干扰素产生的动力学。多烯和聚(I)·聚(C)-二乙氨基乙基葡聚糖不需要同时存在于细胞上就能增强干扰素的产生。用多烯预处理与同时添加一样有效。即使在去除聚(I)·聚(C)-二乙氨基乙基葡聚糖数小时后对洗涤过的细胞进行处理,也会导致干扰素产生增强。AmB似乎未与聚(I)·聚(C)形成大分子复合物,因为聚(I)·聚(C)的紫外吸收光谱和熔点都不会因与AmB混合而改变。同位素研究表明,AmB不会增强聚(I)·聚(C)与细胞的结合。由于大环内酯多烯已被证明可与细胞膜固醇结合,随后改变膜通透性屏障,它们可能通过增加聚(I)·聚(C)的细胞穿透性来增强干扰素的产生。

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Annu Rev Pharmacol. 1970;10:119-42. doi: 10.1146/annurev.pa.10.040170.001003.
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Brief communication: polyene potentiation of antitumor agents.
J Natl Cancer Inst. 1973 Apr;50(4):1047-50. doi: 10.1093/jnci/50.4.1047.
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Adv Appl Microbiol. 1974;17(0):109-34. doi: 10.1016/s0065-2164(08)70556-2.

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