Gagliardini Roberta, Ciccullo Arturo, Borghetti Alberto, Maggiolo Franco, Bartolozzi Dario, Borghi Vanni, Pecorari Monica, Di Biagio Antonio, Callegaro Anna Paola, Bruzzone Bianca, Saladini Francesco, Paolucci Stefania, Maserati Renato, Zazzi Maurizio, Di Giambenedetto Simona, De Luca Andrea
Infectious Diseases Unit, AOU Senese, Siena, Italy.
Institute of Infectious Diseases, Catholic University of Sacred Heart, Rome, Italy.
Open Forum Infect Dis. 2018 May 15;5(6):ofy113. doi: 10.1093/ofid/ofy113. eCollection 2018 Jun.
Dual therapy (DT) with boosted protease inhibitors (bPIs) plus lamivudine has been shown to be superior to bPI monotherapy in virologically suppressed patients despite previous selection of the lamivudine resistance M184V mutation. We compared the virological efficacy of lamivudine-based DT in patients with and without a history of M184V detection.
We retrospectively analyzed patients with HIV-RNA ≤50 copies/mL switching to DT with at least 1 previous resistance genotype in the ARCA database. Time to virological failure (VF; HIV-RNA ≥200 copies/mL or 2 consecutive HIV-RNA >50 copies/mL) and to treatment discontinuation (TD) was analyzed by survival analysis.
Four hundred thirty-six patients switching to lamivudine plus bPIs (70%) or integrase inhibitors (30%) were included. Patients with M184V (n = 87) were older, had lower nadir CD4+ cell count, longer duration of antiretroviral therapy and of virologic suppression, and higher rate of hepatitis C virus infection compared with patients without M184V. The 3-year probability of remaining free from VF was 91.9% (95% confidence interval [CI], 86.6-97.2) without M184V and 87.8% (95% CI, 78.4-97.2) with M184V ( = .323). The time to TD did not differ between groups. Multivariate analysis adjusting for baseline variables differing between groups also did not detect M184V as being associated with VF or TD; however, the 3-year probability of remaining free of viral blips (isolated HIV-RNA 51-199 copies/mL) was 79.8% (95% CI, 67.8%-91.8%) with M184V vs 90.1% (95% CI, 84.0%-96.2%) without M184V ( = .016).
Previous selection of M184V did not increase the risk of VF or TD with lamivudine-based DT but was associated with a higher probability of viral blips.
对于病毒学抑制的患者,尽管先前已选择了拉米夫定耐药的M184V突变,但使用增强型蛋白酶抑制剂(bPIs)加拉米夫定的联合治疗(DT)已被证明优于bPI单药治疗。我们比较了有和没有M184V检测史的患者中基于拉米夫定的DT的病毒学疗效。
我们回顾性分析了ARCA数据库中HIV-RNA≤50拷贝/mL且至少有1次先前耐药基因型记录、转而接受DT治疗的患者。通过生存分析来分析病毒学失败(VF;HIV-RNA≥200拷贝/mL或连续2次HIV-RNA>50拷贝/mL)和治疗中断(TD)的时间。
纳入了436名转而接受拉米夫定加bPIs(70%)或整合酶抑制剂(30%)治疗的患者。与没有M184V的患者相比,有M184V的患者(n = 87)年龄更大,最低点CD4 +细胞计数更低,抗逆转录病毒治疗和病毒学抑制的持续时间更长,丙型肝炎病毒感染率更高。没有M184V的患者3年无VF的概率为91.9%(95%置信区间[CI],86.6 - 97.2),有M184V的患者为87.8%(95%CI,78.4 - 97.2)(P = 0.323)。两组之间的TD时间没有差异。对组间不同的基线变量进行调整的多变量分析也未发现M184V与VF或TD相关;然而,有M184V的患者3年无病毒波动(孤立的HIV-RNA 51 - 199拷贝/mL)概率为79.8%(95%CI,67.8% - 91.8%),而没有M184V的患者为90.1%(95%CI,84.0% - 96.2%)(P = 0.016)。
先前选择M184V不会增加基于拉米夫定的DT发生VF或TD的风险,但与更高的病毒波动概率相关。
