OBJECTIVE:Evaluate immunogenicity and clinical efficacy of two immunization strategies with the ALVAC-HIV-recombinant canarypox vaccine (vCP1452) in treated HIV-infected patients. DESIGN:Randomized, double-blind, placebo-controlled, phase II study of vCP1452 immunization in chronically HIV-infected patients on therapy with CD4 T-cell count more than 350 cells/microl, CD4 nadir less than 400 cells/microl and pHIV-RNA less than 400 copies/ml. Patients were equally randomized to four injections at weeks 0, 4, 8, 20; three injections at weeks 4, 8, 20; and placebo. The primary endpoint was vaccine immunogenicity at week 24 measured by enzyme-linked immunospot-interferon-gamma against the HIV-gag-reverse transcriptase-nef vaccine sequences. Secondary endpoints included time to treatment resumption and viral quantitation following treatment interruption at week 24. Criteria to resume therapy included CD4 T-cell count decline less than 250 cells/microl or 50% decrease from baseline or pHIV-RNA more than 50,000 copies/ml. RESULTS:Sixty-five patients enrolled. Changes from baseline in HIV-specific T cells in the four injection arms (+480 spot-forming cells/M-peripheral blood mononuclear cell) were significant compared to placebo (+8; P = 0.014), but not in the three injection arms (+322). The week 36 pHIV-RNA (log10 copies/ml) after treatment interruption was higher in the four (4.71; P = 0.023) and three (4.82; P = 0.009) injection arms compared to placebo (4.40). Percentages of patients reaching treatment resumption criteria by week 48 were 74, 55 and 23% in the three respective arms (P = 0.013). Two independent factors influenced time to therapy resumption: immunization (hazards ratio = 2.7, P = 0.048 for three injections; hazards ratio = 4.1, P = 0.003 for four injections) and CD4 nadir (hazards ratio = 0.4, P = 0.002). CONCLUSIONS:Significant immunogenicity was induced by vCP1452; however, this strategy was independently associated with a shorter time to resume therapy and higher viral rebound.

译文

目的:评估两种ALVAC-HIV重组金丝雀痘疫苗(vCP1452)的免疫策略的免疫原性和临床疗效。
设计:对慢性HIV感染患者进行vCP1452免疫的随机,双盲,安慰剂对照II期研究,接受CD4 T细胞计数大于350细胞/微升,CD4最低点小于400细胞/微升和pHIV- RNA小于400拷贝/ ml。在第0、4、8、20周,患者被随机分为四次注射。在第4、8、20周进行3次注射;和安慰剂。主要终点是在第24周时通过针对HIV-gag-逆转录酶-nef疫苗序列的酶联免疫斑点-干扰素-γ测得的疫苗免疫原性。次要终点包括在治疗的第24周后恢复治疗的时间和病毒定量。恢复治疗的标准包括CD4 T细胞计数下降小于250细胞/微升或比基线下降50%或pHIV-RNA超过50,000个拷贝/毫升。
结果:65例患者入组。与安慰剂相比,四个注射臂(480个点形成细胞/ M外周血单核细胞)中HIV特异性T细胞的基线变化较安慰剂(8; P = 0.014)显着,但三个注射臂中的HIV特异性T细胞的基线变化却不明显(322 )。与安慰剂(4.40)相比,治疗中断后第36周的pHIV-RNA(log10拷贝/ ml)在四个(4.71; P = 0.023)和三个(4.82; P = 0.009)注射组中更高。到第48周时,在三个相应组中达到恢复治疗标准的患者百分比分别为74%,55%和23%(P = 0.013)。有两个独立的因素影响恢复治疗的时间:免疫(三次注射的危险比= 2.7,P = 0.048;四次注射的危险比= 4.1,P = 0.003)和CD4最低点(危险比= 0.4,P = 0.002)。
结论:vCP1452可诱导明显的免疫原性。但是,这种策略与恢复治疗时间较短和病毒反弹较高有关。

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