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Immuno-activation with anti-CD3 and recombinant human IL-2 in HIV-1-infected patients on potent antiretroviral therapy

机译:抗CD3和重组人IL-2对HIV-1感染患者的有效抗逆转录病毒疗法免疫激活

摘要

BACKGROUND: A stable reservoir of latently infected, resting CD4 T cells has been demonstrated in HIV-1-infected patients despite prolonged antiretroviral treatment. This is a major barrier for the eradication of HIV by antiretroviral agents alone. Activation of these cells in the presence of antiretroviral therapy might be a strategy to increase the turnover rate of this reservoir. METHODS: Three HIV-1-positive patients on potent antiretroviral therapy, in whom plasma viremia had been suppressed to below 5 copies/ml for at least 26 weeks, were treated with a combination of OKT3 (days 1-5) and recombinant human IL-2 (days 2 6). RESULTS: The side-effects were fever, headache, nausea, diarrhea, and in one of the patients transient renal failure and seizures. The regimen resulted in profound T cell activation. In one patient plasma HIV-1 RNA transiently increased with a peak at 1500 copies/ml. In the other two patients plasma HIV-1 RNA levels remained below the detection limit, but HIV-1 RNA levels in the lymph nodes increased two- to threefold. All patients developed antibodies against OKT3. CONCLUSION: OKT3/IL-2 resulted in T cell activation and proliferation, and could stimulate HIV replication in patients having achieved prolonged suppression of plasma viremia. OKT3/IL-2 therapy was toxic and rapidly induced antibodies against OKT3
机译:背景:尽管经过长期的抗逆转录病毒治疗,但已在HIV-1感染的患者中证明了稳定的潜伏感染的静息CD4 T细胞库。这是仅通过抗逆转录病毒药物消灭艾滋病毒的主要障碍。在存在抗逆转录病毒疗法的情况下激活这些细胞可能是增加该储库周转率的策略。方法:对三名接受强力抗逆转录病毒治疗的HIV-1阳性患者进行了至少26周的血浆病毒血症抑制至低于5拷贝/ ml的治疗,采用OKT3(1-5天)和重组人IL联合治疗-2(第2 6天)。结果:副作用为发烧,头痛,恶心,腹泻,其中一名患者出现短暂性肾功能衰竭和癫痫发作。该方案导致深刻的T细胞活化。在一名患者的血浆中,HIV-1 RNA瞬时增加,峰值为1500拷贝/ ml。在其他两名患者中,血浆HIV-1 RNA水平仍低于检测极限,但淋巴结中的HIV-1 RNA水平增加了两倍至三倍。所有患者均产生了针对OKT3的抗体。结论:OKT3 / IL-2导致T细胞活化和增殖,并能刺激血浆病毒血症的长期抑制患者HIV复制。 OKT3 / IL-2治疗具有毒性,可快速诱导出针对OKT3的抗体

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