一项初步研究，评估抗逆转录病毒治疗±白细胞介素-2后中断治疗至CD4 T细胞计数<350个细胞/mm³的时间：ACTG A5102研究结果

A pilot study evaluating time to CD4 T-cell count <350 cells/mm(3) after treatment interruption following antiretroviral therapy +/- interleukin 2: results of ACTG A5102.

作者信息

Henry Keith, Katzenstein David, Cherng Deborah Weng, Valdez Hernan, Powderly William, Vargas Michelle Blanchard, Jahed Nasreen C, Jacobson Jeffrey M, Myers Laurie S, Schmitz John L, Winters Mark, Tebas Pablo

机构信息

HIV Program, Hennepin County Medical Center and the University of Minnesota, Minneapolis, MN 55415, USA.

出版信息

J Acquir Immune Defic Syndr. 2006 Jun;42(2):140-8. doi: 10.1097/01.qai.0000225319.59652.1e.

DOI:10.1097/01.qai.0000225319.59652.1e

PMID:16760795

Abstract

BACKGROUND

Although an intermittent antiviral treatment (ART) strategy may limit long-term toxicity and cost, there is concern about the risk for virologic failure, selection of drug resistance mutations, and disease progression. By boosting CD4 T-cell counts, interleukin 2 (IL-2) could safely prolong the duration of treatment interruption (TI) in a CD4-driven strategy.

METHODS

The AIDS Clinical Trials Group (ACTG) study A5102 evaluated 3 cycles of IL-2 before TI, on clinical and immunologic outcomes, using a CD4 T-cell count of <350 cells/mm as the threshold for restarting ART. Forty-seven HIV-infected subjects on potent ART with CD4 T-cell counts of > or =500 cells/mm or more and HIV RNA levels of less than 200 copies/mL were randomized to arm A (ART + three 5-day cycles of IL-2 at 4.5 million U, Sc, BID every 8 weeks, n = 23) or arm B (ART alone, n = 24) for 18 weeks (step 1). At the end of step 1, subjects with a CD4 T-cell count of > or =500 cells/mm or more stopped ART until a CD4 count of <350 cells/mm (step 2). CD4 T-cell count, time to return of viremia, and the emergence of drug resistance mutations after TI were compared between study arms.

RESULTS

IL-2 recipients maintained higher CD4 counts during TI for 48 weeks with a waning of the CD4 effect by 72 weeks. A sustained CD4 T-cell count of more than 350 cells/mm and more durable TI were associated with a higher nadir CD4 T-cell count before ART and higher naive CD4 T-cell count at entry. After TI, a higher viral set point and drug resistance mutations at virologic rebound were associated with a shorter time to CD4 T-cell count of less than 350 cell/mm. There were no differences in the magnitude of virologic rebound (at week 8 of step 2, median log10 HIV RNA level was 4.23 for arm A and 4.21 for arm B) or the steady-state HIV-1 RNA level after week 8.

CONCLUSIONS

IL-2 before TI did not prolong time to CD4 of less than 350 cells/mm. A TI strategy utilizing a CD4 T-cell threshold of less than 350 cells/mm for restarting ART appears generally safe with most subjects in both arms remaining off ART for more than 1 year. Implications of our results for TI strategies include the potential advantage of starting ART at higher CD4 T-cell levels while avoiding any drug resistance and evaluating immunomodulators or drugs to reduce T-cell activation and HIV-1 RNA rebound during the TI.

摘要

背景

尽管间歇性抗逆转录病毒治疗（ART）策略可能会限制长期毒性和成本，但人们担心病毒学失败、耐药突变的选择以及疾病进展的风险。通过提高CD4 T细胞计数，白细胞介素2（IL-2）可以在以CD4为驱动的策略中安全地延长治疗中断（TI）的持续时间。

方法

艾滋病临床试验组（ACTG）的A5102研究评估了TI前3个周期的IL-2对临床和免疫结果的影响，使用CD4 T细胞计数<350个细胞/mm³作为重新开始ART的阈值。47名接受高效ART治疗、CD4 T细胞计数≥500个细胞/mm³且HIV RNA水平低于200拷贝/mL的HIV感染者被随机分为A组（ART + 每8周进行3个5天周期的IL-2，剂量为450万U，皮下注射，每日2次，n = 23）或B组（仅ART，n = 24），为期18周（第1步）。在第1步结束时，CD4 T细胞计数≥500个细胞/mm³的受试者停止ART，直至CD4计数<350个细胞/mm³（第2步）。比较研究组之间TI后的CD4 T细胞计数、病毒血症恢复时间和耐药突变的出现情况。

结果

IL-2接受者在TI期间48周内维持较高的CD4计数，到72周时CD4效应减弱。持续的CD4 T细胞计数超过350个细胞/mm³和更持久的TI与ART前较低的CD4 T细胞最低点计数和入组时较高的初始CD4 T细胞计数相关。TI后，病毒载量反弹时较高的病毒设定点和耐药突变与CD4 T细胞计数低于350个细胞/mm³的时间较短相关。病毒学反弹的幅度（在第2步的第8周，A组的中位log10 HIV RNA水平为4.23，B组为4.21）或第8周后的稳态HIV-1 RNA水平没有差异。

结论

TI前使用IL-2并未延长CD4计数低于350个细胞/mm³的时间。以CD4 T细胞阈值<350个细胞/mm³作为重新开始ART的TI策略总体上似乎是安全的，两组中的大多数受试者停用ART超过1年。我们的结果对TI策略的意义包括在较高的CD4 T细胞水平开始ART的潜在优势，同时避免任何耐药性，并评估免疫调节剂或药物以减少TI期间的T细胞活化和HIV-1 RNA反弹。