在最后一次免疫接种4年后进行晚期MVA-B加强免疫后,健康志愿者的安全性及疫苗诱导的HIV-1免疫反应。
Safety and vaccine-induced HIV-1 immune responses in healthy volunteers following a late MVA-B boost 4 years after the last immunization.
作者信息
Guardo Alberto C, Gómez Carmen Elena, Díaz-Brito Vicens, Pich Judit, Arnaiz Joan Albert, Perdiguero Beatriz, García-Arriaza Juan, González Nuria, Sorzano Carlos O S, Jiménez Laura, Jiménez José Luis, Muñoz-Fernández María Ángeles, Gatell José M, Alcamí José, Esteban Mariano, López Bernaldo de Quirós Juan Carlos, García Felipe, Plana Montserrat
机构信息
Immunopathology and Cellular Immunology, AIDS Research Group, IDIBAPS, Hospital Clínic, University of Barcelona, Barcelona, Spain.
Centro Nacional de Biotecnología, CSIC, Madrid, Spain.
出版信息
PLoS One. 2017 Oct 24;12(10):e0186602. doi: 10.1371/journal.pone.0186602. eCollection 2017.
BACKGROUND
We have previously shown that an HIV vaccine regimen including three doses of HIV-modified vaccinia virus Ankara vector expressing HIV-1 antigens from clade B (MVA-B) was safe and elicited moderate and durable (1 year) T-cell and antibody responses in 75% and 95% of HIV-negative volunteers (n = 24), respectively (RISVAC02 study). Here, we describe the long-term durability of vaccine-induced responses and the safety and immunogenicity of an additional MVA-B boost.
METHODS
13 volunteers from the RISVAC02 trial were recruited to receive a fourth dose of MVA-B 4 years after the last immunization. End-points were safety, cellular and humoral immune responses to HIV-1 and vector antigens assessed by ELISPOT, intracellular cytokine staining (ICS) and ELISA performed before and 2, 4 and 12 weeks after receiving the boost.
RESULTS
Volunteers reported 64 adverse events (AEs), although none was a vaccine-related serious AE. After 4 years from the 1st dose of the vaccine, only 2 volunteers maintained low HIV-specific T-cell responses. After the late MVA-B boost, a modest increase in IFN-γ T-cell responses, mainly directed against Env, was detected by ELISPOT in 5/13 (38%) volunteers. ICS confirmed similar results with 45% of volunteers showing that CD4+ T-cell responses were mainly directed against Env, whereas CD8+ T cell-responses were similarly distributed against Env, Gag and GPN. In terms of antibody responses, 23.1% of the vaccinees had detectable Env-specific binding antibodies 4 years after the last MVA-B immunization with a mean titer of 96.5. The late MVA-B boost significantly improved both the response rate (92.3%) and the magnitude of the systemic binding antibodies to gp120 (mean titer of 11460). HIV-1 neutralizing antibodies were also enhanced and detected in 77% of volunteers. Moreover, MVA vector-specific T cell and antibody responses were boosted in 80% and 100% of volunteers respectively.
CONCLUSIONS
One boost of MVA-B four years after receiving 3 doses of the same vaccine was safe, induced moderate increases in HIV-specific T cell responses in 38% of volunteers but significantly boosted the binding and neutralizing antibody responses to HIV-1 and to the MVA vector.
TRIAL REGISTRATION
ClinicalTrials.gov NCT01923610.
背景
我们之前已经表明,一种包含三剂表达B亚型HIV-1抗原的改良安卡拉痘苗病毒载体(MVA-B)的HIV疫苗方案是安全的,并且在75%和95%的HIV阴性志愿者(n = 24)中分别引发了适度且持久(1年)的T细胞和抗体反应(RISVAC02研究)。在此,我们描述了疫苗诱导反应的长期持续性以及额外一剂MVA-B加强免疫的安全性和免疫原性。
方法
招募了13名来自RISVAC02试验的志愿者,在最后一次免疫后4年接受第四剂MVA-B。终点指标为安全性、通过ELISPOT、细胞内细胞因子染色(ICS)和ELISA评估的对HIV-1和载体抗原的细胞免疫和体液免疫反应,分别在接受加强免疫前以及加强免疫后2、4和12周进行检测。
结果
志愿者报告了64起不良事件(AE),但无一为与疫苗相关的严重AE。自第一剂疫苗接种4年后,只有2名志愿者维持了低水平的HIV特异性T细胞反应。在晚期MVA-B加强免疫后,通过ELISPOT在5/13(38%)的志愿者中检测到IFN-γ T细胞反应适度增加,主要针对Env。ICS证实了类似结果,45%的志愿者显示CD4 + T细胞反应主要针对Env,而CD8 + T细胞反应同样针对Env、Gag和GPN分布。在抗体反应方面,23.1%的疫苗接种者在最后一次MVA-B免疫4年后可检测到Env特异性结合抗体,平均滴度为96.5。晚期MVA-B加强免疫显著提高了反应率(92.3%)以及针对gp120的全身结合抗体的幅度(平均滴度为11460)。HIV-1中和抗体也得到增强,在77%的志愿者中检测到。此外,MVA载体特异性T细胞和抗体反应分别在80%和100%的志愿者中得到增强。
结论
在接种三剂相同疫苗4年后进行一剂MVA-B加强免疫是安全的,在38%的志愿者中诱导HIV特异性T细胞反应适度增加,但显著增强了对HIV-1和MVA载体的结合及中和抗体反应。
试验注册
ClinicalTrials.gov NCT01923610。
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