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A combinatorial ledge: reverse transcriptase fidelity, total body viral burden, and the implications of multiple-drug HIV therapy for the evolution of antiviral resistance.

机译:一个组合的壁架:逆转录酶保真度,全身病毒载量以及多种药物HIV治疗对抗病毒耐药性演变的影响。

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The chronicity, high mutation rates, and high circulating titers of HIV during the 'stable' phase of infection make rapid evolution of resistance mutations a key predictor of antiretroviral efficacy. Recent advances in measurement of viral RNA titers, turnover dynamics and the in vivo spectrum of resistance mutations allow realistic in vivo estimates of important kinetic parameters of within-patient evolution of viral resistance. First-order estimates of the frequency of viral genotypes necessary for resistance to many antiretroviral combination regimens indicate that many such genotypes pre-exist in patients prior to initiation of therapy. The combinatorial nature of observed multiply-resistant genotypes, however, along with current estimates of total-body viral load and viral turnover dynamics, imply a strikingly sharp transition associated with the change from two-drug to three-drug antiretroviral regimens: pre-existing resistance being near-certain in the first instance but highly unlikely in the second. This abrupt change, a 'combinatorial ledge', carries with it a number of important implications for the understanding and control of HIV infection and other potential targets of antiviral therapy.
机译:在感染的“稳定”阶段,HIV的长期性,高突变率和高循环滴度使耐药性突变的迅速发展成为抗逆转录病毒疗效的关键预测指标。病毒RNA滴度,代谢动力学和耐药性突变体内谱的测量方面的最新进展使得可以对病毒耐药性患者体内进化的重要动力学参数进行实际的体内估计。对许多抗逆转录病毒联合治疗方案耐药所必需的病毒基因型频率的一级估计表明,许多此类基因型在治疗开始之前就已存在于患者体内。然而,观察到的多重耐药基因型的组合性质,以及当前对全身病毒载量和病毒更新动态的估计,暗示了与从两药到三药抗逆转录病毒疗法的变化相关的惊人的急剧转变:预先存在阻力在第一时间几乎是确定的,但在第二时间极不可能。这种突然的变化,即“组合壁架”,对理解和控制HIV感染以及抗病毒治疗的其他潜在目标具有许多重要意义。

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