Brooke Army Medical Center, Houston, TX 78234, USA.
University of Texas at San Antonio, San Antonio, TX 78249, USA.
Mil Med. 2021 Feb 26;186(3-4):279-285. doi: 10.1093/milmed/usaa416.
Weight gain and obesity in people living with HIV have been associated with increased risk for non-AIDS-related comorbidities, and integrase strand transfer inhibitor (INSTI)-based regimens may lead to comparatively more weight gain than other regimens. We evaluated body mass index (BMI) following antiretroviral therapy (ART) initiation among participants in the U.S. Military HIV Natural History Study (NHS).
NHS participants with available baseline weight and height data initiating ART from 2006 to 2017 were considered for analysis. Antiretroviral therapy was categorized by anchor class to include INSTIs, non-nucleoside reverse transcriptase inhibitors (NNRTIs) and protease inhibitors (PIs). Linear growth-curve modeling was used to predict BMI changes from ART initiation through 2 years of follow-up in participants stratified by baseline BMI (<25 vs ≥25 kg/m2) at ART start and anchor drug class. These models were adjusted for demographic- and HIV-related characteristics.
Of 961 NHS participants started on initial ART between 2006 and 2017, 491 men who had available baseline BMI data and were virally suppressed (<200 c/mL) at 1 and 2 years of follow-up were included. Overall, the predicted BMI increased at each time point over 2 years regardless of baseline BMI. There was a trend toward less weight gain for non-INSTI regimens regardless of demographic- or HIV-related factors (-0.65 kg/m2/yr, P = .070). In participants with BMI <25, all regimens were associated with BMI gains except in those with high viral load (≥100,000 copies/mL) started on PI regimens (-1.91 kg/m2/yr, P = .000; n = 13). For those participants with BMI ≥25, only INSTI- and PI-based regimens were significantly associated with increased BMI (INSTI 0.54 kg/m2/y, P = .000; PI 0.39 kg/m2/yr, P = .006). Non-nucleoside reverse transcriptase inhibitors were not associated with weight gain regardless of race- or HIV-related characteristics. African Americans with BMI ≥25 were more likely to gain weight as compared to Whites (0.99 kg/m2/yr, P = .016). Specific anchor drug-based predictions revealed that only INSTI use among African Americans was significantly associated with BMI gains (1.85 kg/m2/yr, P = .007); NNRTI- and PI-related weight change was not significant as compared to Whites.
In our cohort of young military members with HIV infection, those with BMI <25 experienced BMI gains across all ART classes. Among those with BMI ≥25, African Americans on INSTI regimens had the greatest BMI gains. Further studies are needed to determine whether NNRTI regimens should be considered in certain individuals at risk for INSTI-associated weight gain.
在感染 HIV 的人群中,体重增加和肥胖与非艾滋病相关合并症的风险增加有关,基于整合酶链转移抑制剂(INSTI)的治疗方案可能比其他方案导致更多的体重增加。我们评估了美国军事 HIV 自然史研究(NHS)中接受抗逆转录病毒治疗(ART)的参与者开始接受治疗后的体重指数(BMI)。
对从 2006 年至 2017 年开始接受 ART 且有基线体重和身高数据的 NHS 参与者进行分析。根据锚定药物类别将抗逆转录病毒治疗分为 INSTI、非核苷类逆转录酶抑制剂(NNRTI)和蛋白酶抑制剂(PI)。线性增长曲线模型用于预测在开始 ART 后 2 年的 BMI 变化,参与者根据开始 ART 时的基线 BMI(<25 与≥25 kg/m2)和锚定药物类别进行分层。这些模型根据人口统计学和 HIV 相关特征进行了调整。
在 2006 年至 2017 年期间开始接受初始 ART 的 961 名 NHS 参与者中,有 491 名男性有可用的基线 BMI 数据,并且在 1 年和 2 年的随访时 HIV 抑制(<200 c/mL)。总的来说,无论基线 BMI 如何,在 2 年内的每个时间点,预测的 BMI 都在增加。无论人口统计学或 HIV 相关因素如何,非 INSTI 方案的体重增加趋势较小(-0.65 kg/m2/yr,P=0.070)。在 BMI<25 的参与者中,除了基线病毒载量高(≥100,000 拷贝/mL)的参与者接受 PI 方案外(-1.91 kg/m2/yr,P=0.000;n=13),所有方案都与 BMI 增加相关。对于 BMI≥25 的参与者,只有 INSTI 和 PI 方案与 BMI 增加显著相关(INSTI 0.54 kg/m2/y,P=0.000;PI 0.39 kg/m2/yr,P=0.006)。无论种族或 HIV 相关特征如何,NNRTI 均与体重增加无关。与白人相比,BMI≥25 的非裔美国人更有可能增加体重(0.99 kg/m2/yr,P=0.016)。基于特定锚定药物的预测显示,只有非裔美国人使用 INSTI 与 BMI 增加显著相关(1.85 kg/m2/yr,P=0.007);与白人相比,NNRTI 和 PI 相关的体重变化不显著。
在我们的年轻 HIV 感染军事人员队列中,BMI<25 的参与者在所有 ART 类别中都经历了 BMI 增加。在 BMI≥25 的参与者中,接受 INSTI 方案的非裔美国人 BMI 增加最多。需要进一步研究以确定在 INSTI 相关体重增加风险较高的特定人群中是否应考虑使用 NNRTI 方案。
