Università Cattolica del Sacro Cuore, Dipartimento di Sicurezza e Bioetica Sezione Malattie Infettive, Rome, Italy.
Fondazione Policlinico Universitario A. Gemelli IRCCS, UOC Malattie Infettive, Rome, Italy.
J Antimicrob Chemother. 2020 Jun 1;75(6):1599-1603. doi: 10.1093/jac/dkaa058.
To assess the impact of switching to dolutegravir plus lamivudine maintenance therapy on the HIV cellular reservoir size.
This was a prospective, longitudinal, matched, controlled study. We enrolled virologically suppressed patients on stable three-drug ART who switched at baseline (BL) to dolutegravir/lamivudine (DT group) or maintained triple therapy (TT group); subjects in the TT group were matched 1:1 with those in the DT group according to age, gender, years since HIV diagnosis, years on ART and anchor drug. Total blood-associated HIV DNA levels were assessed by droplet digital PCR at BL and after 48 weeks (T48). Results were expressed as log10 HIV DNA copies/106 leucocytes.
We enrolled 40 patients in the DT group and 40 in the TT group; the two groups were homogeneous for all main characteristics except nadir CD4 cell count. At BL, HIV DNA levels were comparable between the DT and TT groups: 2.27 (IQR 1.97-2.47) and 2.26 (IQR 2.05-2.61) log10 HIV DNA copies/106 leucocytes, respectively. Change in HIV DNA load from BL to T48 was -0.105 (IQR -0.384 to 0.121, P = 0.041) in the DT group and -0.132 (IQR -0.362 to 0.046, P = 0.005) in the TT group, with a comparable decline observed between the two groups (P = 0.821). A higher HIV DNA decline was associated with higher BL CD4/CD8 ratio.
Maintenance therapy with dolutegravir/lamivudine had the same impact as the triple regimen on HIV DNA levels after 48 weeks of treatment. These data seem to support the effectiveness of a dolutegravir/lamivudine dual regimen in controlling the magnitude of the cellular reservoir (www.clinicaltrials.gov, number NCT02836782).
评估转换为多替拉韦/拉米夫定维持治疗对 HIV 细胞储库大小的影响。
这是一项前瞻性、纵向、匹配、对照研究。我们招募了在稳定的三药 ART 下病毒学抑制的患者,这些患者在基线(BL)时转换为多替拉韦/拉米夫定(DT 组)或维持三联疗法(TT 组);TT 组的患者根据年龄、性别、HIV 诊断后时间、ART 时间和锚定药物与 DT 组 1:1 匹配。BL 和 48 周(T48)时通过液滴数字 PCR 评估全血相关 HIV DNA 水平。结果表示为 log10 HIV DNA 拷贝/106 白细胞。
我们招募了 40 名 DT 组患者和 40 名 TT 组患者;除了最低 CD4 细胞计数外,两组在所有主要特征上均相似。BL 时,DT 组和 TT 组的 HIV DNA 水平相当:2.27(IQR 1.97-2.47)和 2.26(IQR 2.05-2.61)log10 HIV DNA 拷贝/106 白细胞。DT 组从 BL 到 T48 的 HIV DNA 载量变化为-0.105(IQR -0.384 至 0.121,P=0.041),TT 组为-0.132(IQR -0.362 至 0.046,P=0.005),两组之间观察到相似的下降(P=0.821)。较高的 HIV DNA 下降与较高的 BL CD4/CD8 比值相关。
多替拉韦/拉米夫定维持治疗与三联疗法在治疗 48 周后对 HIV DNA 水平的影响相同。这些数据似乎支持多替拉韦/拉米夫定双药方案在控制细胞储库大小方面的有效性(www.clinicaltrials.gov,编号 NCT02836782)。
