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Macaque studies of vaccine and microbicide combinations for preventing HIV-1 sexual transmission

机译:猕猴疫苗和杀微生物剂组合预防HIV-1性传播的研究

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摘要

Vaccination and the application of a vaginal microbicide have traditionally been considered independent methods to prevent the sexual transmission of HIV-1 to women. Both techniques can be effective in macaque models, and limited efficacy has been observed in clinical trials for each. Here, we have addressed whether vaccines and microbicides can be used together to provide reinforced protection against virus challenge of rhesus macaques. In two separate experiments, four groups of animals were vaccinated with a T-cell-based adenovirus (Ad) vectored vaccine aimed at reducing postinfection viral loads and/or a partially effective dose of a vaginal microbicide aimed at blocking infection of a high-dose vaginal challenge with SIVmac251 or SHIV-162P3. In the first study, the only two protected animals were in the group that received Ad26/Ad5HVR48 vaccine vectors combined with the fusion inhibitor T-1249 as the vaginal microbicide before SIV-mac251 challenge. In the second study, vaccination with Ad35/ Ad26 vectors combined with the CCR5 inhibitor maraviroc as the vaginal microbicide led to significant reductions of both acquisition of infection and postinfection viral loads following SHIV-SF162P3 challenge. As expected, the vaccine by itself reduced viral loads but had no acquisition effect, whereas the microbicide had a partial acquisition effect but minimal impact on viral loads. For both measures of protective efficacy, the vaccine-microbicide combination differed more from controls than did either separate intervention. Overall, the data suggest that vaccines and microbicides are complementary techniques that may protect better when used together than separately.
机译:疫苗接种和阴道杀菌剂的应用传统上一直被认为是防止HIV-1向女性性传播的独立方法。两种技术在猕猴模型中均有效,并且在每种临床试验中均观察到有限的功效。在这里,我们已经解决了疫苗和杀微生物剂是否可以一起使用以增强抵抗猕猴的病毒攻击的保护作用。在两个独立的实验中,四组动物分别接种了旨在减少感染后病毒载量的基于T细胞的腺病毒(Ad)载体疫苗和/或旨在阻止高剂量感染的部分有效剂量的阴道杀菌剂用SIVmac251或SHIV-162P3阴道攻击。在第一个研究中,只有两只受保护的动物在接受SIV-mac251攻击之前接受了Ad26 / Ad5HVR48疫苗载体与融合抑制剂T-1249组合作为阴道杀菌剂。在第二项研究中,将Ad35 / Ad26载体与CCR5抑制剂maraviroc结合作为阴道杀菌剂进行疫苗接种,可显着降低SHIV-SF162P3攻击后的感染获得率和感染后病毒载量。如预期的那样,疫苗本身降低了病毒载量,但没有获得效果,而杀菌剂具有部分获得效果,但对病毒载量的影响最小。对于这两种保护效力的措施,疫苗-杀微生物剂组合与对照的差异大于两种单独干预的差异。总体而言,数据表明,疫苗和杀菌剂是互补的技术,与单独使用相比,它们可能会得到更好的保护。

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    Beth Israel Deaconess Medical Center, Boston, MA 02115 Ragon Institute of MGH, MIT, and Harvard, Boston, MA 02114;

    Department of Microbiology and Immunology, Weill Cornell Medical College, New York, NY 10021;

    Tulane National Primate Research Center, Tulane University School of Medicine,Covington, LA 70433;

    Tulane National Primate Research Center, Tulane University School of Medicine,Covington, LA 70433;

    Department of Microbiology and Immunology, Weill Cornell Medical College, New York, NY 10021;

  • 收录信息 美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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  • 入库时间 2022-08-18 00:40:24

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