Hamzah Lisa, Tiraboschi Juan M, Iveson Helen, Toby Martina, Mant Christine, Cason John, Burling Keith, Wandolo Emily, Jendrulek Isabelle, Taylor Chris, Ibrahim Fowzia, Kulasegaram Ranjababu, Teague Alastair, Post Frank A, Fox Julie
Department of HIV Research, King's College London, London, UK.
Antivir Ther. 2016;21(4):287-96. doi: 10.3851/IMP3000. Epub 2015 Oct 13.
Efavirenz (EFV) has been associated with reductions in vitamin D (25[OH]D) and tenofovir (TDF) with increased bone turnover, reductions in bone mineral density (BMD) and renal tubular dysfunction. We hypothesized that switching from fixed-dose TDF/emtricitabine (FTC)/EFV to darunavir/ritonavir monotherapy (DRV/r) might increase 25(OH)D and BMD, and improve renal tubular function.
Subjects with HIV RNA <50 copies/ml on TDF/FTC/EFV for ≥6 months were randomized 1:1 to ongoing TDF/FTC/EFV or DRV/r (800/100 mg once daily) for 48 weeks. The primary end point was change from baseline in 25(OH)D at week 48. Secondary end points included changes in BMD, bone turnover markers and renal tubular function.
A total of 64 subjects (86% male, 66% white, mean [sd] CD4(+) T-cell count 537.3 [191.5]/mm(3)) were analysed. After adjustment for baseline 25(OH)D and demographics, at week 48 DRV/r monotherapy was associated with a +3.6 (95% CI 0.6, 6.6) ng/ml increase in 25(OH)D compared to TDF/FTC/EFV (P=0.02). DRV/r monotherapy was associated with an increase in BMD (+2.9% versus -0.003% at the neck of femur and +2.6% versus +0.008% at the lumbar spine for DRV/r versus TDF/FTC/EFV; P<0.05 for all) and reductions in bone biomarkers compared with those remaining on TDF/FTC/EFV. No significant difference in renal tubular function was observed. Reasons for discontinuation in the DRV/r arm included side effects (n=4) and viral load rebound (n=3), all of which resolved with DRV/r discontinuation or regimen intensification.
Switching from TDF/FTC/EFV to DRV/r in patients with suppressed HIV RNA resulted in significant improvements in 25(OH)D and bone biomarkers, and a 2-3% increase in BMD.
依非韦伦(EFV)与维生素D(25[OH]D)水平降低有关,而替诺福韦(TDF)与骨转换增加、骨矿物质密度(BMD)降低及肾小管功能障碍有关。我们推测,从固定剂量的TDF/恩曲他滨(FTC)/EFV转换为达芦那韦/利托那韦单药治疗(DRV/r)可能会提高25(OH)D水平和BMD,并改善肾小管功能。
TDF/FTC/EFV治疗≥6个月且HIV RNA<50拷贝/ml的受试者按1:1随机分为继续接受TDF/FTC/EFV治疗或接受DRV/r(800/100mg每日一次)治疗48周。主要终点是第48周时25(OH)D相对于基线的变化。次要终点包括BMD、骨转换标志物和肾小管功能的变化。
共分析了64名受试者(86%为男性,66%为白人,平均[标准差]CD4(+)T细胞计数为537.3[191.5]/mm³)。在对基线25(OH)D和人口统计学因素进行调整后,与TDF/FTC/EFV相比,第48周时DRV/r单药治疗使25(OH)D增加了+3.6(95%CI 0.6,6.6)ng/ml(P=0.02)。与继续接受TDF/FTC/EFV治疗的受试者相比,DRV/r单药治疗使BMD增加(股骨颈处分别为+2.9%对-0.003%,腰椎处为+2.6%对+0.008%;所有比较P<0.05),并使骨生物标志物降低。未观察到肾小管功能有显著差异。DRV/r组停药的原因包括副作用(n=4)和病毒载量反弹(n=3),所有这些在停用DRV/r或加强治疗方案后均得到缓解。
在HIV RNA得到抑制的患者中,从TDF/FTC/EFV转换为DRV/r可使25(OH)D和骨生物标志物显著改善,BMD增加2 - 3%。
