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候选杀微生物剂PPCM在细胞和组织培养中可阻断1型人类免疫缺陷病毒感染,并在小鼠模型中预防生殖器疱疹。

Candidate microbicide PPCM blocks human immunodeficiency virus type 1 infection in cell and tissue cultures and prevents genital herpes in a murine model.

作者信息

Mesquita Pedro M M, Wilson Sarah S, Manlow Philippe, Fischetti Lucia, Keller Marla J, Herold Betsy C, Shattock Robin J

机构信息

Department of Cellular and Molecular Medicine, St. George's University of London, London, United Kingdom.

出版信息

J Virol. 2008 Jul;82(13):6576-84. doi: 10.1128/JVI.00335-08. Epub 2008 Apr 23.

Abstract

A structurally novel candidate microbicide, PPCM, which is formed from the reaction of D,L-mandelic acid with sulfuric acid, provides activity against human immunodeficiency virus (HIV) and herpes simplex virus (HSV) and is not cytotoxic. The objectives of the current studies were to comprehensively evaluate the activity of PPCM in cell and explant cultures, explore the possibility of combining PPCM with HIV-specific reverse transcriptase inhibitors, and evaluate the efficacy of a formulated gel against genital herpes in a murine model. PPCM inhibited infection by laboratory and clinical R5 and X4 clade B and clade C HIV strains in cell culture. Ectocervical and endocervical tissue explants exposed to HIV-1(BaL) in the presence of PPCM were protected (50% inhibitory concentrations [IC(50)] of 3.9 microg/ml for ectocervix and 3.1 microg/ml for endocervix), and transfer of virus to target T cells via migratory cells was significantly impaired (IC(50) of 35.7 microg/ml for ectocervix and 54.6 microg/ml for endocervix). The drug also blocked infection by cell-associated virus. Combinations of PPCM with UC-781 or PMPA in vitro exhibited additive anti-HIV activity. PPCM was incorporated into stable, low-pH gel formulations at concentrations of 0.4% and 4%. Both gels prevented genital herpesvirus infection in mice, even when virus was introduced in human seminal plasma. The abilities of PPCM to inhibit primary HIV isolates, reduce infection by cell-associated virus, and transfer of HIV from migratory to T cells, combined with the complete protection provided by formulated gel against genital herpes, indicate that this drug is an excellent candidate for inclusion in a combination microbicide and would provide protection against both HIV and HSV.

摘要

一种结构新颖的候选杀微生物剂PPCM,由D,L-扁桃酸与硫酸反应形成,具有抗人类免疫缺陷病毒(HIV)和单纯疱疹病毒(HSV)的活性,且无细胞毒性。当前研究的目的是全面评估PPCM在细胞和外植体培养中的活性,探索将PPCM与HIV特异性逆转录酶抑制剂联合使用的可能性,并在小鼠模型中评估一种配方凝胶对生殖器疱疹的疗效。PPCM在细胞培养中抑制实验室和临床R5及X4 B亚型和C亚型HIV毒株的感染。在PPCM存在下暴露于HIV-1(BaL)的宫颈外组织和宫颈内组织外植体受到保护(宫颈外组织的50%抑制浓度[IC(50)]为3.9微克/毫升,宫颈内组织为3.1微克/毫升),并且通过迁移细胞将病毒转移至靶T细胞的过程受到显著损害(宫颈外组织的IC(50)为35.7微克/毫升,宫颈内组织为54.6微克/毫升)。该药物还可阻断细胞相关病毒的感染。PPCM与UC-781或替诺福韦酯在体外联合使用表现出相加的抗HIV活性。PPCM以0.4%和4%的浓度被掺入稳定的低pH凝胶配方中。两种凝胶均可预防小鼠的生殖器疱疹病毒感染,即使病毒是在人类精液中引入的。PPCM抑制原发性HIV分离株、减少细胞相关病毒感染以及HIV从迁移细胞向T细胞转移的能力,再加上配方凝胶对生殖器疱疹提供的完全保护,表明该药物是组合杀微生物剂中的优秀候选药物,可同时预防HIV和HSV感染。

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