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首页> 外文期刊>JAIDS: Journal of acquired immune deficiency syndromes >Isoniazid Preventive Therapy for People With HIV Who Are Heavy Alcohol Drinkers in High TB-/HIV-Burden Countries: A Risk-Benefit Analysis
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Isoniazid Preventive Therapy for People With HIV Who Are Heavy Alcohol Drinkers in High TB-/HIV-Burden Countries: A Risk-Benefit Analysis

机译:Isoniazid用于艾滋病毒患者的Isoniazid预防疗法,谁是高TB / HIV - 负担国家的沉重酒精饮酒者:风险效益分析

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Background: Isoniazid preventive therapy (IPT) reduces mortality among people living with HIV (PLHIV) and is recommended for those without active tuberculosis (TB) symptoms. Heavy alcohol use, however, is contraindicated for liver toxicity concerns. We evaluated the risks and benefits of IPT at antiretroviral therapy (ART) initiation to ART alone for PLHIV who are heavy drinkers in 3 high TB-/HIV-burden countries.Methods: We developed a Markov simulation model to compare ART alone to ART with cither 6 or 36 months of IPT for heavy drinking PLHIV enrolling in care in Brazil, India, and Uganda. Outcomes included nonfatal toxicity, fatal toxicity, life expectancy, TB cases, and TB death.Results: In this simulation, 6 months of IPT + ART (1PT6) extended life expectancy over both ART alone and 36 months of IPT + ART (IPT36) in India and Uganda, but ART alone dominated in Brazil in 51.5% of simulations. Toxicity occurred in 160/1000 persons on IPT6 and 415/1000 persons on IPT36, with fatal toxicity in 8/1000 on 1PT6 and 21/1000 on IPT36. Sensitivity analyses favored IPT6 in India and Uganda with high toxicity thresholds.Conclusions: The benefits of IPT for heavy drinkers outweighed its risks in India and Uganda when given for a 6-month course. The toxicity/efficacy trade-off was less in Brazil where TB incidence is lower. IPT6 resulted in fatal toxicity in 8/1000 people, whereas even higher toxicities of IPT36 negated its benefits in all countries. Data to better characterize IPT toxicity among HIV-infected drinkers are needed to improve guidance.
机译:背景:Isoniazid预防疗法(IPT)降低了艾滋病毒(PlHIV)的人们的死亡率,并建议那些没有活跃结核病(TB)症状的人。然而,对肝脏毒性令人禁忌的饮酒是禁忌的。我们评估了IPT在抗逆转录病毒治疗(艺术)对艺术的风险和益处,仅为Plhiv为3个高TB-/ HIV-HORDEN国家的批重饮酒者。方法:我们开发了一个马尔可夫模拟模型,以将艺术与艺术进行比较在巴西,印度和乌干达招募沉重的饮酒Plhiv的IPT 6或36个月。结果包括非毒性,致命的毒性,预期衰竭,结核病病例和结核病死亡。结果:在这个模拟中,6个月的IPT +艺术(1PT6)单独延长寿命和IPT +艺术36个月(IPT36)在印度和乌干达,但艺术独自在巴西占据了51.5%的模拟。在IPT6和IPT36的IPT6和415/1000人的160/1000人上发生毒性,在1PT6和IPT36上的8/1000致致命毒性。敏感性分析在印度和乌干达具有高毒性阈值的人们青睐巴西的毒性/功效折衷较少,其中TB发病率降低。 IPT6导致8/1000人致命的毒性,而IPT36的毒性甚至更高的毒性否定了所有国家的利益。为了改善指导,需要更好地表征IPT毒性的IPT毒性。

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