Active anti-interferon-alpha immunization: a European-Israeli, randomized, double-blind, placebo-controlled clinical trial in 242 HIV-1--infected patients (the EURIS study).

A Gringeri, M Musicco, P Hermans, Z Bentwich, M Cusini, A Bergamasco, E Santagostino, A Burny, B Bizzini, D Zagury
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引用次数: 69

Abstract

This randomized, double-blind, placebo-controlled, phase II/III study was designed to evaluate safety, immunogenicity, and efficacy of an active anti-interferon-alpha (anti-IFN-alpha) vaccine in asymptomatic HIV-1-infected patients. The active immunization was aimed at inducing anti-IFN-alpha antibodies to counteract IFN-alpha overproduction. In all, 242 patients, recruited between December 1995 and July 1996 in eight centers in Europe and Israel, with CD4+ counts from 100 to 634 cells/mm3 who were receiving or not receiving antiretroviral therapy (including protease inhibitors) were randomized to receive either anti-IFN-alpha vaccine or placebo. The anti-IFN-alpha immunization regimen consisted of three priming injections delivered intramuscularly at 1-month intervals in a water-in-oil emulsion of inactivated recombinant IFN-alpha-2b (i-IFN-alpha) followed by intramuscular booster injections of i-IFN-alpha adsorbed onto calcium phosphate every 3 months. Immunogenicity to vaccine was defined as an increase of anti-IFN-alpha antibody level of more than twofold the preimmunization value. Clinical progression, changes in antiretroviral treatment, and decrease of CD4+ counts to <200 cells/mm3 were considered endpoints for efficacy evaluation. Contrary to our previous experience, in which six to seven oil priming injections induced a >90% response rate, the three oil-adjuvanted injections in this trial were suboptimal because only 40 of 122 vaccinees (33%) had raised anti-IFN-alpha antibody following immunization. In vaccinees, both antibody responders (AbRV) and nonresponders (AbNRV), the tolerance to the vaccine was good and was without evidence of significant safety concerns. During the course of the trial, 62% of vaccine responders, 64% of nonresponders, and 63% of placebo patients elected to add protease inhibitor-containing regimens as new treatment guidelines were established, resulting in a marked decrease in clinical and laboratory progression such that the expected endpoints of the study could not be achieved and further follow-up was halted. Despite the unexpectedly low immunogenicity and fewer than expected endpoints, anti-IFN-alpha vaccine recipients, in comparison with placebo recipients, showed a lower rate of disease progression, nonelective treatment changes, and/or CD4+ count decrease to <200 cells/mm3, but the difference was not statistically significant. Nevertheless, the subgroup of patients immunized to IFN-alpha who experienced a rise in anti-IFN-alpha antibodies had a significantly lower rate of occurrence of HIV-1-related events and of any combination of the endpoints compared with those of either placebo patients or vaccinees who failed to develop anti-IFN-alpha antibodies, the latter two groups behaving similarly. Further studies of this approach are warranted because these data suggest a beneficial effect of this adjuvant approach.

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主动抗干扰素- α免疫:欧洲-以色列242例HIV-1感染患者的随机、双盲、安慰剂对照临床试验(EURIS研究)。
这项随机、双盲、安慰剂对照的II/III期研究旨在评估一种活性抗干扰素- α(抗ifn - α)疫苗在无症状hiv -1感染患者中的安全性、免疫原性和有效性。主动免疫的目的是诱导抗ifn - α抗体来抵消ifn - α的过量产生。在1995年12月至1996年7月期间,在欧洲和以色列的8个中心招募了242名患者,CD4+计数从100到634细胞/mm3不等,接受或未接受抗逆转录病毒治疗(包括蛋白酶抑制剂),随机接受抗ifn - α疫苗或安慰剂。抗ifn - α免疫方案包括:每隔1个月用灭活重组ifn - α -2b (i- ifn - α)的油包水乳剂肌内注射3次启动剂,然后每隔3个月肌内注射一次吸附在磷酸钙上的i- ifn - α加强剂。对疫苗的免疫原性定义为抗ifn - α抗体水平比免疫前增加两倍以上。临床进展,抗逆转录病毒治疗的变化,CD4+计数下降到90%的应答率,在本试验中,三种油佐剂注射是次优的,因为122名疫苗接种者中只有40名(33%)免疫后抗ifn - α抗体升高。在疫苗接种者中,无论是抗体应答者(AbRV)还是无应答者(AbNRV),对疫苗的耐受性都很好,没有证据表明存在重大的安全性问题。在试验过程中,62%的疫苗应答者、64%的无应答者和63%的安慰剂患者选择添加含有蛋白酶抑制剂的方案作为新的治疗指南,导致临床和实验室进展明显减少,以至于无法达到研究的预期终点,进一步的随访被停止。尽管免疫原性出乎意料地低,终点也少于预期,但与安慰剂受体相比,抗ifn - α疫苗受体显示出较低的疾病进展率、非选择性治疗改变和/或CD4+计数降至
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