转换为马拉维若+达芦那韦/利托那韦300/800/100毫克每日一次治疗48周后的骨矿物质密度改善情况,GUSTA研究的初步结果
Bone mineral density improvement after 48 weeks of switch to maraviroc+darunavir/ritonavir 300/800/100 mg QD, preliminary results of GUSTA study.
作者信息
Bianco Claudia, Rossetti Barbara, Gagliardini Roberta, Lamonica Silvia, Fanti Luri, Lombardi Francesca, Cauda Roberto, Di Giambenedetto Simona, De Luca Andrea
机构信息
Infectious Diseases Unit, Azienda Ospedaliera Universitaria Senese, Siena, Italy.
Clinic of Infectious Diseases, Catholic University of Sacred Heart, Roma, Italy.
出版信息
J Int AIDS Soc. 2014 Nov 2;17(4 Suppl 3):19816. doi: 10.7448/IAS.17.4.19816. eCollection 2014.
INTRODUCTION
Low bone mineral density (BMD) and osteoporosis are prevalent in HIV-infected patients and were associated with HIV infection and tenofovir-containing ART.
MATERIALS AND METHODS
The GUSTA study (GUided Simplification with Tropism Assay) is a two-arm, prospective, multicenter, 1:1 randomized controlled trial designed to demonstrate the non-inferiority of therapeutic switch to maraviroc+darunavir/ritonavir (MVC+DRV/r) 300/800/100 mg QD against the continuation of previous triple cART in patients with stable virological suppression. Enrolment criteria include HIV1-RNA <50 copies/mL for >6 months, R5 tropism and CD4>200 cells/µL for >3 months. Dual energy X-ray absorptiometry scans of proximal femur and lumbar spine were performed at baseline and week 48. Bone composition was evaluated using L2-L4 lumbar column and proximal femoral BMD, T-score and the Z-score. At the same timepoints, plasma bone metabolism biomarkers were measured. Linear regression was used to compare means of differences between arms. The association between BMD changes and the baseline variables was assessed by linear regression.
RESULTS
27 patients were included, 13 from study group and 14 from control group, 74.1% were males, 44.4% heterosexuals, 81.5% Caucasian, median age was 47 years (IQR 41-53), time from HIV diagnosis 13.4 years (9-19), CD4 553/µL (406-739), nadir CD4 201/µL (76-283). At baseline, median ART duration was 10.5 years (5.7-15.3), the majority of patients (70.4%) was on tenofovir, 63% was on a PI-based regimen and 14,8% on an NNRTI-based regimen. Mean proximal femur BMD from baseline increased over 48 weeks by 2.06% (SD 2.24) in the study arm and decreased by -2.77% (SD 4.63) in control arm (p=0.003). The change over 48 weeks in proximal femur T-score was significantly different between the study (+0.11, SD 0.22) and control arm (-1.14, SD 0.27, p=0.016). Also the changes in total alkalin phosphatase (-20 U/L vs -1.5, p=0.003) was significant between the two groups. After adjusting for time from HIV diagnosis and years of ART, study group was the only factor associated to higher mean percentage change from baseline femoral BMD (MVC+DRV/r +4.83, p=0.044).
CONCLUSIONS
The study demonstrated a significant improvement in femoral BMD and T-score after treatment simplification with MVC+DRV/r.
引言
低骨矿物质密度(BMD)和骨质疏松在HIV感染患者中普遍存在,且与HIV感染及含替诺福韦的抗逆转录病毒治疗(ART)有关。
材料与方法
GUSTA研究(病毒嗜性检测引导下的简化治疗)是一项双臂、前瞻性、多中心、1:1随机对照试验,旨在证明对于病毒学抑制稳定的患者,改用马拉维罗+达芦那韦/利托那韦(MVC+DRV/r)300/800/100毫克每日一次的治疗方案不劣于继续使用之前的三联cART方案。入选标准包括HIV-1 RNA<50拷贝/毫升超过6个月、R5嗜性以及CD4>200细胞/微升超过3个月。在基线和第48周时对股骨近端和腰椎进行双能X线吸收测定扫描。使用L2-L4腰椎柱和股骨近端的骨密度、T值和Z值评估骨成分。在相同时间点,测量血浆骨代谢生物标志物。采用线性回归比较两组间差异的均值。通过线性回归评估骨密度变化与基线变量之间的关联。
结果
共纳入27例患者,研究组13例,对照组14例,74.1%为男性,44.4%为异性恋,81.5%为白种人,中位年龄47岁(四分位间距41-53岁),自HIV诊断以来的时间为13.4年(9-19年),CD4为553/微升(406-739),最低CD4为201/微升(76-283)。基线时,ART的中位持续时间为10.5年(5.7-15.3年),大多数患者(70.4%)使用替诺福韦,63%使用基于蛋白酶抑制剂(PI)的方案,14.8%使用基于非核苷类逆转录酶抑制剂(NNRTI)的方案。研究组股骨近端骨密度自基线起在48周内平均增加2.06%(标准差2.24),而对照组下降了-2.77%(标准差4.63)(p=0.003)。股骨近端T值在48周内的变化在研究组(+0.11,标准差0.22)和对照组(-1.14,标准差0.27,p=0.016)之间有显著差异。两组间总碱性磷酸酶的变化(-20 U/L对-1.5,p=0.003)也有显著差异。在调整了自HIV诊断以来的时间和ART年限后,研究组是与股骨骨密度自基线起平均百分比变化较高相关的唯一因素(MVC+DRV/r为+4.83,p=0.044)。
结论
该研究表明,使用MVC+DRV/r简化治疗后,股骨骨密度和T值有显著改善。
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