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首页> 外文期刊>International journal of STD & AIDS >Changes in renal, bone, lipid, and inflammation markers in HIV-1 patients after combination antiretroviral therapy simplification to dolutegravir monotherapy
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Changes in renal, bone, lipid, and inflammation markers in HIV-1 patients after combination antiretroviral therapy simplification to dolutegravir monotherapy

机译:HIV-1患者肾,骨,脂质和炎症标志物的变化在组合抗逆转录病毒治疗后对DoluteGravir单药治疗

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摘要

Combination antiretroviral therapy (cART) can cause metabolic toxicities. How cART simplification to dual or monotherapies affects metabolic markers is unknown. We analyzed the metabolic effects of cART simplification to dolutegravir (DTG) monotherapy in the randomized clinical DOMONO (DOlutegravir MONOtherapy for HIV) trial including HIV-positive participants. Renal function, Framingham risk score (FRS), inflammation, and bone mineral density (BMD) with trabecular bone score (TBS) were measured during 48 weeks after simplification. The changes at 48 weeks by on-treatment analyses overall and for prior tenofovir disoproxil fumarate (TDF) exposure were analyzed separately, using Bonferroni corrected alpha (p = 0.00096). Ninety-five patients initiated DTG monotherapy, including 80 discontinuing TDF. At week 48, the switch to DTG monotherapy resulted in an expected -7.8 ml/min estimated glomerular filtration decline. In patients on prior TDF, proteinuria improved (p < 0.00096), but proximal tubular dysfunction proportions did not change. Fasting lipids, FRS, and the inflammation markers C-reactive protein and CD4:CD8 T-cell ratio remained stable. Lumbar spine BMD improved (+1.7%, p < 0.00096), while hip BMD and TBS remained comparable. Simplification of TDF-containing cART to DTG monotherapy ameliorated lumbar spine BMD and proteinuria with neutral effect on lipids and inflammation markers. Although DTG monotherapy should not be used in routine care and its role in strictly selected patients with primary HIV infection needs to be further elucidated, these observations remain relevant regarding DTG-based dual therapy without TDF. registration number: NCT02401828.
机译:组合抗逆转录病毒治疗(推车)可引起代谢毒性。如何简化双重或单疗法影响代谢标记的人是如何未知的。我们分析了随机临床Domono(Dolutegravir Monoherapy的DTUTURGRAVIR(DTG)单疗法(Dolututgravir Monotherapy的HIV)试验,包括艾滋病毒阳性参与者的代谢效应。在简化后48周期间测量肾功能,骨髓素风险评分(FRS),炎症和骨矿物密度(BMD),测定了小梁骨评分(TBS)。通过单独分析通过Bonferroni校正的α单独分析通过关于治疗分析48周的改变,并分别进行先前的Tenofovir Disoproxil umarate(TDF)暴露(P = 0.00096)。九十五名患者启动了DTG单一疗法,其中80例停止TDF。第48周,转换为DTG单疗法导致预期-7.8ml / min的估计肾小球过滤下降。在先前TDF的患者中,蛋白尿改善(P <0.00096),但近端管功能障碍比例没有变化。空腹脂质,FRS和炎症标志物C反应蛋白和CD4:CD8 T细胞比保持稳定。腰椎BMD改善(+ 1.7%,P <0.00096),而HIP BMD和TBS保持可比。简化含TDF的CART到DTG单疗法改善腰椎BMD和蛋白尿对脂质和炎症标志物的中性效果。虽然DTG单药治疗不应用于常规护理,但其在严格选择的患有原发性HIV感染患者中的作用需要进一步阐明,这些观察结果仍然有关于没有TDF的DTG的双重治疗。注册号:NCT02401828。

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