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3-马来酰亚胺基丙基磺酸酯修饰的肽融合抑制剂 albuvirtide 的生物物理特性和广谱抗 HIV 活性。

Biophysical property and broad anti-HIV activity of albuvirtide, a 3-maleimimidopropionic acid-modified peptide fusion inhibitor.

机构信息

Institute of Pathogen Biology, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing, China.

出版信息

PLoS One. 2012;7(3):e32599. doi: 10.1371/journal.pone.0032599. Epub 2012 Mar 5.

Abstract

Albuvirtide (ABT) is a 3-maleimimidopropionic acid (MPA)-modified peptide HIV fusion inhibitor that can irreversibly conjugate to serum albumin. Previous studies demonstrated its in vivo long half-life and potent anti-HIV activity. Here, we focused to characterize its biophysical properties and evaluate its antiviral spectrum. In contrast to T20 (Enfuvirtide, Fuzeon), ABT was able to form a stable α-helical conformation with the target sequence and block the fusion-active six-helix bundle (6-HB) formation in a dominant-negative manner. It efficiently inhibited HIV-1 Env-mediated cell membrane fusion and virus entry. A large panel of 42 HIV-1 pseudoviruses with different genotypes were constructed and used for the antiviral evaluation. The results showed that ABT had potent inhibitory activity against the subtypes A, B and C that predominate the worldwide AIDS epidemics, and subtype B', CRF07_BC and CRF01_AE recombinants that are currently circulating in China. Furthermore, ABT was also highly effective against HIV-1 variants resistant to T20. Taken together, our data indicate that the chemically modified peptide ABT can serve as an ideal HIV-1 fusion inhibitor.

摘要

阿比乌替肽(ABT)是一种 3-马来酰亚胺基丙酸(MPA)修饰的肽类 HIV 融合抑制剂,可与血清白蛋白不可逆结合。先前的研究表明其具有体内长半衰期和强大的抗 HIV 活性。在此,我们专注于研究其生物物理特性并评估其抗病毒谱。与 T20(恩夫韦肽,Fuzeon)不同,ABT 能够与靶序列形成稳定的α-螺旋构象,并以显性负性方式阻断融合活性的六螺旋束(6-HB)形成。它能够有效抑制 HIV-1 Env 介导的细胞膜融合和病毒进入。我们构建了一个包含 42 种具有不同基因型的 HIV-1 假病毒的大型面板,并用于抗病毒评估。结果表明,ABT 对目前在全球 AIDS 流行中占主导地位的亚型 A、B 和 C,以及在中国流行的亚型 B'、CRF07_BC 和 CRF01_AE 重组病毒具有强大的抑制活性。此外,ABT 对耐 T20 的 HIV-1 变异体也具有高度疗效。综上所述,我们的数据表明,经过化学修饰的肽 ABT 可以作为一种理想的 HIV-1 融合抑制剂。

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