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Human Immunodeficiency Virus Type 1 Fitness Is a Determining Factor in Viral Rebound and Set Point in Chronic Infection

机译:人类免疫缺陷病毒1型适应度是病毒感染和慢性感染设定点的决定因素

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摘要

Human immunodeficiency virus type 1 (HIV-1) isolates from 20 chronically infected patients who participated in a structured treatment interruption (STI) trial were studied to determine whether viral fitness influences reestablishment of viremia. Viruses derived from individuals who spontaneously controlled viremia had significantly lower in vitro replication capacities than viruses derived from individuals that did not control viremia after interruption of antiretroviral therapy (ART), and replication capacities correlated with pre-ART and post-STI viral set points. Of note, no clinically relevant improvement of viral loads upon STI occurred. Virus isolates from controlling and noncontrolling patients were indistinguishable in terms of coreceptor usage, genetic subtype, and sensitivity to neutralizing antibodies. In contrast, viruses from controlling patients exhibited increased sensitivity to inhibition by chemokines. Sensitivity to inhibition by RANTES correlated strongly with slower replication kinetics of the virus isolates, suggesting a marked dependency of these virus isolates on high coreceptor densities on the target cells. In summary, our data indicate that viral fitness is a driving factor in determining the magnitude of viral rebound and viral set point in chronic HIV-1 infection, and thus fitness should be considered as a parameter influencing the outcome of therapeutic intervention in chronic infection.
机译:研究人员从参与结构性治疗中断(STI)试验的20名慢性感染患者中分离出1型人类免疫缺陷病毒(HIV-1),以确定病毒适应性是否影响病毒血症的重建。自发控制病毒血症的个体产生的病毒的体外复制能力比抗逆转录病毒疗法(ART)中断后不控制病毒血症的个体产生的病毒低得多,复制能力与ART之前和STI后的病毒设定值相关。值得注意的是,没有发生与性传播感染有关的病毒载量的临床相关改善。在共受体使用,遗传亚型和对中和抗体的敏感性方面,从控制患者和非控制患者中分离出的病毒是无法区分的。相反,来自控制患者的病毒对趋化因子抑制的敏感性更高。 RANTES抑制的敏感性与病毒分离株的复制动力学较慢密切相关,表明这些病毒分离株对靶细胞上高共受体密度具有显着依赖性。总之,我们的数据表明,病毒适应度是确定慢性HIV-1感染的病毒反弹和病毒设定点的驱动因素,因此,适应度应被视为影响慢性感染治疗干预结果的参数。

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