经给药途径用 HIV 腺病毒载体加强 DNA 质粒疫苗初免后的安全性和免疫原性:一项随机临床试验。
Safety and immunogenicity of an HIV adenoviral vector boost after DNA plasmid vaccine prime by route of administration: a randomized clinical trial.
机构信息
Laboratory of Infectious Disease Prevention, New York Blood Center, New York, New York, United States of America.
出版信息
PLoS One. 2011;6(9):e24517. doi: 10.1371/journal.pone.0024517. Epub 2011 Sep 12.
BACKGROUND
In the development of HIV vaccines, improving immunogenicity while maintaining safety is critical. Route of administration can be an important factor.
METHODOLOGY/PRINCIPAL FINDINGS: This multicenter, open-label, randomized trial, HVTN 069, compared routes of administration on safety and immunogenicity of a DNA vaccine prime given intramuscularly at 0, 1 and 2 months and a recombinant replication-defective adenovirus type 5 (rAd5) vaccine boost given at 6 months by intramuscular (IM), intradermal (ID), or subcutaneous (SC) route. Randomization was computer-generated by a central data management center; participants and staff were not blinded to group assignment. The outcomes were vaccine reactogenicity and humoral and cellular immunogenicity. Ninety healthy, HIV-1 uninfected adults in the US and Peru, aged 18-50 were enrolled and randomized. Due to the results of the Step Study, injections with rAd5 vaccine were halted; thus 61 received the booster dose of rAd5 vaccine (IM: 20; ID:21; SC:20). After the rAd5 boost, significant differences by study arm were found in severity of headache, pain and erythema/induration. Immune responses (binding and neutralizing antibodies, IFN-γ ELISpot HIV-specific responses and CD4+ and CD8+ T-cell responses by ICS) at four weeks after the rAd5 booster were not significantly different by administration route of the rAd5 vaccine boost (Binding antibody responses: IM: 66.7%; ID: 70.0%; SC: 77.8%; neutralizing antibody responses: IM: 11.1%; ID: 0.0%; SC 16.7%; ELISpot responses: IM: 46.7%; ID: 35.3%; SC: 44.4%; CD4+ T-cell responses: IM: 29.4%; ID: 20.0%; SC: 35.3%; CD8+ T-cell responses: IM: 29.4%; ID: 16.7%; SC: 50.0%.)
CONCLUSIONS/SIGNIFICANCE: This study was limited by the reduced sample size. The higher frequency of local reactions after ID and SC administration and the lack of sufficient evidence to show that there were any differences in immunogenicity by route of administration do not support changing route of administration for the rAd5 boost.
TRIAL REGISTRATION
ClinicalTrials.gov NCT00384787.
背景
在 HIV 疫苗的研发过程中,提高免疫原性的同时保持安全性至关重要。接种途径可能是一个重要因素。
方法/主要发现:这项多中心、开放性、随机试验 HVTN069 比较了肌内注射(IM)、皮内(ID)和皮下(SC)途径接种 DNA 疫苗初免(分别于 0、1 和 2 个月)和复制缺陷型重组腺病毒 5 型(rAd5)疫苗加强针(分别于 6 个月)的安全性和免疫原性。中央数据管理中心采用计算机生成随机分组;参与者和工作人员对分组不知情。主要结局是疫苗反应原性和体液及细胞免疫原性。美国和秘鲁共 90 名健康、未感染 HIV-1 的 18-50 岁成年人入组并随机分组。由于 Step 研究的结果,rAd5 疫苗的注射停止;因此,61 人接受了 rAd5 疫苗加强针(IM:20 人;ID:21 人;SC:20 人)。在接受 rAd5 加强针后,研究组间在头痛、疼痛和红斑/硬结的严重程度上存在显著差异。在接受 rAd5 加强针四周后,rAd5 疫苗加强针的接种途径对免疫反应(结合和中和抗体、IFN-γ ELISpot HIV 特异性反应以及 ICS 检测的 CD4+和 CD8+T 细胞反应)无显著差异(结合抗体反应:IM:66.7%;ID:70.0%;SC:77.8%;中和抗体反应:IM:11.1%;ID:0.0%;SC:16.7%;ELISpot 反应:IM:46.7%;ID:35.3%;SC:44.4%;CD4+T 细胞反应:IM:29.4%;ID:20.0%;SC:35.3%;CD8+T 细胞反应:IM:29.4%;ID:16.7%;SC:50.0%)。
结论/意义:本研究因样本量减少而受到限制。ID 和 SC 给药后局部反应频率较高,且没有足够证据表明免疫原性因接种途径而异,因此不支持改变 rAd5 加强针的接种途径。
试验注册
ClinicalTrials.gov NCT00384787。
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