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Boosting immunity by antiviral drug therapy: A simple relationship among timing efficacy and success

机译:通过抗病毒药物疗法增强免疫力:时间疗效和成功之间的简单关系

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摘要

Drug therapies against persistent human infections such as hepatitis C virus, hepatitis B virus, and HIV fail to consistently eradicate the infection from the host. Hence, recent emphasis has shifted to the study of antiviral therapy aimed at boosting specific immune responses. It was argued that structured therapy interruptions were required to achieve this, because such regimes have shown promising results in early HIV infection. Using mathematical models, we show that, contrary to this notion, a single phase of drug therapy can result in the establishment of sustained immunity. We present a simple relationship between timing of therapy and efficacy of the drugs required for success. In the presence of strong viral suppression, we show that therapy should be stopped relatively early, and that a longer duration of treatment leads to failure. On the other hand, in the presence of weaker viral suppression, stopping treatment too early is detrimental, and therapy has to be continued beyond a time threshold. We discuss our modeling results primarily in the context of HCV therapy during chronic infection. Although the therapy regimes explored here also have implications for HIV, virus-mediated destruction of specific immune cells renders success unlikely during the chronic phase of the infection.
机译:针对持续性人类感染(例如丙型肝炎病毒,乙型肝炎病毒和HIV)的药物治疗无法始终如一地从宿主中消除感染。因此,最近的重点已转移到旨在增强特异性免疫反应的抗病毒治疗研究上。有人认为需要中断结构性治疗才能实现这一目标,因为这种治疗方案已在早期HIV感染中显示出令人鼓舞的结果。使用数学模型,我们证明,与该概念相反,药物治疗的单个阶段可以导致建立持续的免疫力。我们提出了治疗时间和成功所需药物疗效之间的简单关系。在存在强大的病毒抑制作用的情况下,我们表明治疗应该相对早地停止,并且更长的治疗时间会导致失败。另一方面,在病毒抑制作用较弱的情况下,过早停止治疗是有害的,必须继续治疗超过时间阈值。我们主要在慢性感染期间的HCV治疗中讨论我们的建模结果。尽管此处探讨的治疗方案也对HIV有影响,但是病毒介导的特定免疫细胞的破坏使得在慢性感染阶段不太可能取得成功。

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