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HIV Reservoirs and Immune Surveillance Evasion Cause the Failure of Structured Treatment Interruptions: A Computational Study

机译:HIV水库和免疫监视规避导致结构化治疗中断失败:一项计算研究

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摘要

Continuous antiretroviral therapy is currently the most effective way to treat HIV infection. Unstructured interruptions are quite common due to side effects and toxicity, among others, and cannot be prevented. Several attempts to structure these interruptions failed due to an increased morbidity compared to continuous treatment. The cause of this failure is poorly understood and often attributed to drug resistance. Here we show that structured treatment interruptions would fail regardless of the emergence of drug resistance. Our computational model of the HIV infection dynamics in lymphoid tissue inside lymph nodes, demonstrates that HIV reservoirs and evasion from immune surveillance themselves are sufficient to cause the failure of structured interruptions. We validate our model with data from a clinical trial and show that it is possible to optimize the schedule of interruptions to perform as well as the continuous treatment in the absence of drug resistance. Our methodology enables studying the problem of treatment optimization without having impact on human beings. We anticipate that it is feasible to steer new clinical trials using computational models.
机译:持续的抗逆转录病毒疗法是目前治疗HIV感染的最有效方法。由于副作用和毒性等原因,非结构性中断非常普遍,无法避免。与持续治疗相比,由于发病率增加,几次构造这些干扰的尝试均以失败告终。失败的原因了解甚少,通常归因于耐药性。在这里,我们表明,无论是否出现耐药性,结构性治疗中断都将失败。我们对淋巴结内淋巴组织中HIV感染动力学的计算模型表明,HIV储库和免疫监视自身的逃避足以引起结构性中断的失败。我们使用来自临床试验的数据验证了我们的模型,并表明可以优化中断时间表,以在没有耐药性的情况下执行以及进行连续治疗。我们的方法可以研究治疗优化问题,而不会影响人类。我们预计使用计算模型指导新的临床试验是可行的。

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