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首页> 外文期刊>Journal of medical primatology >Robust suppression of env-SHIV viremia in Macaca nemestrina by 3-drug ART is independent of timing of initiation during chronic infection
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Robust suppression of env-SHIV viremia in Macaca nemestrina by 3-drug ART is independent of timing of initiation during chronic infection

机译:用3药ART强烈抑制猕猴中的env-SHIV病毒血症与慢性感染期间的起始时间无关

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摘要

Background Nonhuman primates (NHPs) are an important model organism for studies of HIV pathogenesis and preclinical evaluation of anti-HIV therapies. The successful translation of NHP-derived data to clinically relevant anti-HIV studies will require better understanding of the viral strains and NHP species used and their responses to existing antiretroviral therapies (ART). Methods Five pigtailed macaques (Macaca nemestrina) were productively infected with the SIV/HIV chimeric virus SHIV-1157 ipd3N4 following intravenous challenge. After 8 or 27 weeks, ART (PMPA, FTC, raltegravir) was initiated. Viral load, T-cell counts, and production of SHIV-specific antibodies were monitored throughout the course of infection and ART. Results ART led to a rapid and sustained decrease in plasma viral load. Suppression of plasma viremia by ART was independent of the timing of initiation during chronic infection. Conclusions We present a new NHP model of HIV infection on antiretroviral therapy, which should prove applicable to multiple clinically relevant anti-HIV approaches.
机译:背景技术非人类灵长类动物(NHPs)是研究HIV发病机理和抗HIV治疗的临床前评估的重要模型生物。要成功地将NHP来源的数据转换为临床相关的抗HIV研究,将需要更好地了解所使用的病毒株和NHP种类及其对现有抗逆转录病毒疗法(ART)的反应。方法在静脉内攻击后,将5只猪尾猕猴(Macaca nemestrina)有效地感染了SIV / HIV嵌合病毒SHIV-1157 ipd3N4。 8或27周后,开始使用ART(PMPA,FTC,raltegravir)。在整个感染和抗病毒治疗过程中,监测病毒载量,T细胞计数和SHIV特异性抗体的产生。结果ART导致血浆病毒载量快速持续下降。 ART对血浆病毒血症的抑制作用与慢性感染期间的起始时间无关。结论我们提出了一种抗逆转录病毒疗法治疗HIV感染的NHP新模型,该模型应证明适用于多种临床相关的抗HIV方法。

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