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Estimation of HIV treatment-efficacy by combining structural nested mean models with pharmacokinetic models of antiretroviral drug exposure

机译:通过将结构嵌套均值模型与抗逆转录病毒药物暴露的药代动力学模型相结合来评估HIV的治疗效果

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The aim of treating HIV-1-infected patients is to achieve and maintain suppression of viral load (VL). Achievement of this aim is thwarted by variable adherence to prescribed anti-retroviral drugs. Variable adherence to an antiretroviral regimen creates variability in the patient’s internal exposure to the drugs. Structural nested mean models (SNMMs) enabled us to estimate, during the initial phase of treatment, the relationship between variable internal exposure and VL, accounting for measured time-varying confounders and feedback relations using an antiretroviral regimen containing lopinavir/ritonavir (LPV/RTV, LPV/r). Our final SNMM predicts that the short term effect of treatment is modified by the most recent past VL, with higher initial VL’s being associated with larger treatment-induced reductions in VL for a given internal exposure to the drugs. Variation in internal exposure to LPV/r in the interquartile interval (P25%–P75%) only slightly affects the overall reduction in VL, supporting the conclusion that the relatively long duration of action of LPV/r lessens the impact on VL of the most frequently recurring intermittent lapses in dosing.
机译:治疗感染HIV-1的患者的目的是实现并维持对病毒载量(VL)的抑制。对处方抗逆转录病毒药物的依从性参差不齐,阻碍了这一目标的实现。对抗逆转录病毒疗法方案的依从性可变会导致患者内部暴露于药物的变异性。结构嵌套均值模型(SNMM)使我们能够在治疗的初始阶段估计变量内部暴露量与VL之间的关系,并考虑使用含洛匹那韦/利托那韦(LPV / RTV)的抗逆转录病毒疗法,测量了随时间变化的混杂因素和反馈关系,LPV / r)。我们的最终SNMM预测,近期的VL会改变短期治疗效果,对于给定的内部暴露量,较高的初始VL与更大的治疗诱导的VL降低相关。在四分位数间隔内(P25%–P75%),内部暴露于LPV / r的变化仅轻微影响VL的总体下降,支持以下结论:相对较长的LPV / r作用时间减轻了对大多数人对VL的影响频繁反复间歇给药。

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