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Structural Analysis of Potent Hybrid HIV-1 Protease Inhibitors Containing Bis-tetrahydrofuran in a Pseudosymmetric Dipeptide Isostere

机译:含有双 - 四氢呋喃的效率杂交HIV-1蛋白酶抑制剂的结构分析

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摘要

The design, synthesis, and X-ray structural analysis of hybrid HIV-1 protease inhibitors (PIs) containing bis-tetrahydrofuran (bis-THF) in a pseudo-C-2-symmetric dipeptide isostere are described. A series of PIs were synthesized by incorporating bis-THF of darunavir on either side of the Phe-Phe isostere of lopinavir in combination with hydrophobic amino acids on the opposite P2/P2' position. Structure-activity relationship studies indicated that the bis-THF moiety can be attached at either the P2 or P2' position without significantly affecting potency. However, the group on the opposite P2/P2' position had a dramatic effect on potency depending on the size and shape of the side chain. Cocrystal structures of inhibitors with wild-type HIV-1 protease revealed that the bis-THF moiety retained similar interactions as observed in the darunavir-protease complex regardless of the position on the Phe-Phe isostere. Analyses of cocrystal structures and molecular dynamics simulations provide insights into optimizing HIV-1 PIs containing bis-THF in non-sulfonamide dipeptide isosteres.
机译:描述了含有双 - 四氢呋喃(BIS-THF)的杂化HIV-1蛋白酶抑制剂(PS-THF)的设计,合成和X射线结构分析在伪-C-2-对称二肽等蹄酮中。通过在Lopinavir Phe-Phe等甾氏菌的两侧结合疏水氨基酸在相反的p2 / p2'位置结合嗜酸盐磷酸的两侧,合成了一系列PIS。结构 - 活性关系研究表明,BIS-THF部分可以在P2或P2'位置附着,而不会显着影响效力。然而,相反的P2 / P2'位置的组对级联的效力具有显着影响,这取决于侧链的尺寸和形状。具有野生型HIV-1蛋白酶的抑制剂的共聚物结构显示,无论pHE-PHE等甾氏棘甾饼等的位置如何,双-THF部分在达尔努韦蛋白酶复合物中所观察到的相互作用。 COCRYSTAL结构和分子动力学模拟的分析提供了在非磺酰胺二肽旁观者中优化含有BIS-THF的HIV-1 PIV-1的见解。

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  • 来源
    《Journal of Medicinal Chemistry》 |2020年第15期|共18页
  • 作者单位

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

    Univ North Carolina Chapel Hill Dept Biochem &

    Biophys Chapel Hill NC 27599 USA;

    Univ North Carolina Chapel Hill Dept Biochem &

    Biophys Chapel Hill NC 27599 USA;

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

    Univ North Carolina Chapel Hill Dept Biochem &

    Biophys Chapel Hill NC 27599 USA;

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

    Univ Massachusetts Med Sch Dept Biochem &

    Mol Pharmacol Worcester MA 01605 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学;
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