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模拟改良的直接观察下抗逆转录病毒疗法对HIV抑制与耐药性、疾病进展及死亡的影响。

Modeling the impact of modified directly observed antiretroviral therapy on HIV suppression and resistance, disease progression, and death.

作者信息

Kagay C R, Porco T C, Liechty C A, Charlebois E, Clark R, Guzman D, Moss A R, Bangsberg D R

机构信息

University of California, San Francisco, School of Medicine, San Francisco, California 94110, USA.

出版信息

Clin Infect Dis. 2004 Jun 1;38 Suppl 5:S414-20. doi: 10.1086/421406.

Abstract

A simulation model that used Markov assumptions with Monte Carlo uncertainty analysis was evaluated 1500 times at 10,000 iterations. Modified directly observed therapy (MDOT) for human immunodeficiency virus was assumed to improve adherence to therapy to 90% of prescribed doses. The impact of MDOT interventions on modeled biological and clinical outcomes was compared for populations with mean rates of adherence (i.e., the mean percentage of prescribed doses taken by each member of the population who had not discontinued therapy) of 40%, 50%, 60%, and 70%. MDOT reduced the risk of virological failure, development of opportunistic infections, and death, yet increased the risk of drug resistance, for each adherence distribution among persons with detectable plasma virus loads. Over 1500 trials, for a population with 50% adherence to therapy and a 12-month period, MDOT increased the median rate of virological suppression from 13.2% to 37.0% of patients, decreased the rate of opportunistic infection from 5.7% to 4.3% of patients, and decreased the death rate from 2.9% to 2.2% of patients. In the same population, however, MDOT increased the rate of new drug resistance mutations from 1.00 to 1.41 per person during the 12-month period. The impact of MDOT was smaller in populations with higher levels of adherence. MDOT interventions will likely improve clinical outcomes in populations with low levels of adherence but may not be effective at preventing drug resistance in treatment-experienced populations. MDOT may be more effective in preventing drug resistance with potent regimens in treatment-naive patients.

摘要

一个使用马尔可夫假设并进行蒙特卡洛不确定性分析的模拟模型在10000次迭代下被评估了1500次。假设针对人类免疫缺陷病毒的改良直接观察治疗(MDOT)可将治疗依从性提高到规定剂量的90%。比较了MDOT干预措施对依从率平均为40%、50%、60%和70%的人群(即未中断治疗的人群中每个成员服用规定剂量的平均百分比)的模拟生物学和临床结果的影响。对于血浆病毒载量可检测的人群中的每种依从性分布情况,MDOT降低了病毒学失败、机会性感染发生和死亡的风险,但增加了耐药性风险。在1500次试验中,对于一个治疗依从率为50%且为期12个月的人群,MDOT使病毒学抑制的中位数率从患者的13.2%提高到37.0%,使机会性感染率从患者的5.7%降至4.3%,并使死亡率从患者的2.9%降至2.2%。然而,在同一人群中,MDOT在12个月期间使每人新出现的耐药性突变率从1.00提高到1.41。在依从性较高的人群中,MDOT的影响较小。MDOT干预措施可能会改善依从性较低人群的临床结果,但在预防有治疗经验人群的耐药性方面可能无效。MDOT在预防初治患者使用强效方案时的耐药性方面可能更有效。

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