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[硫代磷酸α-异头寡脱氧核苷酸的体外抗HIV活性]

[In vitro anti-HIV activity of phosphorothioate alpha-anomeric oligodeoxynucleotides].

作者信息

Rayner B, Matsukura M, Morvan F, Cohen J S, Imbach J L

机构信息

Laboratoire de Chimie bio-organique, U.A. n 488, C.N.R.S., Université de Montpellier-II.

出版信息

C R Acad Sci III. 1989;310(3):61-4.

PMID:2516764
Abstract

Oligonucleotide analogs consisting exclusively of alpha-anomeric deoxynucleoside units bridged with phosphorothioate linkages have been synthesized and tested in vitro as antiviral agents against human immunodeficiency virus (HIV) in human T cells. Two 28-mers, an homopolymer alpha-S-dC28 and an oligomer alpha-S-anti-rev complementary to the initiation site of the regulatory viral gene rev exhibited antiviral activities comparable to those reported for the corresponding beta-anomeric phosphorothioate analogs. In contrast, a nuclease-resistant homopolymer, alpha-dC28 was inactive. Their preliminary results would indicate that the origin of oligonucleotide phosphorothioate anti-HIV activity is not exclusively correlated with their higher nuclease resistance.

摘要

已合成了仅由通过硫代磷酸酯键连接的α-异头脱氧核苷单元组成的寡核苷酸类似物,并在体外作为抗人类免疫缺陷病毒(HIV)的抗病毒剂在人T细胞中进行了测试。两种28聚体,一种均聚物α-S-dC28和一种与调节性病毒基因rev的起始位点互补的寡聚物α-S-抗rev,其抗病毒活性与报道的相应β-异头硫代磷酸酯类似物相当。相比之下,一种抗核酸酶的均聚物α-dC28没有活性。它们的初步结果表明,寡核苷酸硫代磷酸酯抗HIV活性的来源并不完全与其更高的抗核酸酶性相关。

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