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HIV-1和HIV-2在猪尾猕猴中的差异复制及致病作用

Differential replication and pathogenic effects of HIV-1 and HIV-2 in Macaca nemestrina.

作者信息

Otten R A, Brown B G, Simon M, Lupo L D, Parekh B S, Lairmore M D, Schable C A, Schochetman G, Rayfield M A

机构信息

Division of HIV/AIDS, Centers for Disease Control and Prevention, Atlanta, GA 30333.

出版信息

AIDS. 1994 Mar;8(3):297-306. doi: 10.1097/00002030-199403000-00002.

Abstract

OBJECTIVE

HIV-1 and HIV-2 isolates representing various geographic regions and distinct viral subtypes were examined for their ability to establish both in vitro and in vivo productive infections of Macaca nemestrina (pigtail macaque) peripheral blood mononuclear cells.

METHODS

Animals were inoculated with either autologous cell-associated or cell-free viral preparations of selected isolates. HIV-specific immune responsiveness, hematologic changes, genetic variation, and virus burden were monitored as delineators of HIV pathogenesis.

RESULTS

HIV-2 replication in vitro and in vivo correlated with nascent antigen production and rising viral titers as determined by infectious center assays. Infection was detectable by polymerase chain reaction amplification of proviral sequences in macaque cells as early as 1 week postinoculation. Two distinct patterns of CD4+ cell depletion induced by HIV-2 infection were observed during the first month postinoculation and characterized by a moderate loss sustained through 20 weeks postinoculation or a substantial loss maintained long-term (> 90 weeks). Identity between inoculating viral stocks and subsequent viral isolates from animals was established comparatively by limited sequence analysis of specific domains within the HIV-2 pol and env genes. In contrast, replication of HIV-1 isolates was limited or only semipermissive in vitro. Intravenous inoculation of HIV-1 field isolates, using conditions successful for HIV-2 (for example, identical viral titers), failed to establish a productive viral infection leading to seroconversion of fluctuations in hematologic cell markers. Infection with a high-titer inoculum of a laboratory-adapted HIV-1 strain in vivo, as demonstrated by polymerase chain reaction analysis, produced seroconversion in the absence of overt viral replication or hematologic variations in one out of four animals.

CONCLUSIONS

This system provides for multifaceted modeling of HIV pathogenesis, primarily with HIV-2 and potentially with HIV-1/-2 chimerics, in support of immunotherapeutic developments and critical evaluation of intervention practices.

摘要

目的

对代表不同地理区域和不同病毒亚型的HIV-1和HIV-2分离株进行检测,以评估它们在体外和体内建立对豚尾猕猴外周血单个核细胞进行有效感染的能力。

方法

用所选分离株的自体细胞相关或无细胞病毒制剂接种动物。监测HIV特异性免疫反应性、血液学变化、基因变异和病毒载量,作为HIV发病机制的指标。

结果

通过感染中心试验确定,HIV-2在体外和体内的复制与新生抗原产生及病毒滴度升高相关。早在接种后1周,通过聚合酶链反应扩增猕猴细胞中的前病毒序列即可检测到感染。在接种后第一个月观察到HIV-2感染诱导的两种不同模式的CD4+细胞耗竭,其特征是接种后20周持续中度损失或长期(>90周)维持大量损失。通过对HIV-2 pol和env基因内特定结构域的有限序列分析,比较确定接种病毒株与动物随后的病毒分离株之间的一致性。相比之下,HIV-1分离株的复制在体外受到限制或仅为半允许性。使用对HIV-2成功的条件(例如,相同的病毒滴度)静脉接种HIV-1现场分离株,未能建立导致血液学细胞标志物波动的血清转化的有效病毒感染。通过聚合酶链反应分析证明,在体内用高滴度实验室适应的HIV-1毒株接种,四只动物中有一只在没有明显病毒复制或血液学变化的情况下产生了血清转化。

结论

该系统为HIV发病机制提供了多方面的模型,主要针对HIV-2,也可能针对HIV-1/-2嵌合体,以支持免疫治疗的发展和对干预措施的关键评估。

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