鼻内接种具有复制能力的仙台病毒载体1型人类免疫缺陷病毒(HIV-1) gag疫苗的安全性和免疫原性的首次人体评估:在初免-加强免疫方案中诱导强效T细胞或抗体反应
First-in-Human Evaluation of the Safety and Immunogenicity of an Intranasally Administered Replication-Competent Sendai Virus-Vectored HIV Type 1 Gag Vaccine: Induction of Potent T-Cell or Antibody Responses in Prime-Boost Regimens.
作者信息
Nyombayire Julien, Anzala Omu, Gazzard Brian, Karita Etienne, Bergin Philip, Hayes Peter, Kopycinski Jakub, Omosa-Manyonyi Gloria, Jackson Akil, Bizimana Jean, Farah Bashir, Sayeed Eddy, Parks Christopher L, Inoue Makoto, Hironaka Takashi, Hara Hiroto, Shu Tsugumine, Matano Tetsuro, Dally Len, Barin Burc, Park Harriet, Gilmour Jill, Lombardo Angela, Excler Jean-Louis, Fast Patricia, Laufer Dagna S, Cox Josephine H
机构信息
Projet San Francisco, Kigali, Rwanda.
Kenya AIDS Vaccine Initiative Institute of Clinical Research, Nairobi.
出版信息
J Infect Dis. 2017 Jan 1;215(1):95-104. doi: 10.1093/infdis/jiw500. Epub 2016 Oct 17.
BACKGROUND
We report the first-in-human safety and immunogenicity assessment of a prototype intranasally administered, replication-competent Sendai virus (SeV)-vectored, human immunodeficiency virus type 1 (HIV-1) vaccine.
METHODS
Sixty-five HIV-1-uninfected adults in Kenya, Rwanda, and the United Kingdom were assigned to receive 1 of 4 prime-boost regimens (administered at 0 and 4 months, respectively; ratio of vaccine to placebo recipients, 12:4): priming with a lower-dose SeV-Gag given intranasally, followed by boosting with an adenovirus 35-vectored vaccine encoding HIV-1 Gag, reverse transcriptase, integrase, and Nef (Ad35-GRIN) given intramuscularly (SA); priming with a higher-dose SeV-Gag given intranasally, followed by boosting with Ad35-GRIN given intramuscularly (SA); priming with Ad35-GRIN given intramuscularly, followed by boosting with a higher-dose SeV-Gag given intranasally (AS); and priming and boosting with a higher-dose SeV-Gag given intranasally (SS).
RESULTS
All vaccine regimens were well tolerated. Gag-specific IFN-γ enzyme-linked immunospot-determined response rates and geometric mean responses were higher (96% and 248 spot-forming units, respectively) in groups primed with SeV-Gag and boosted with Ad35-GRIN (SA and SA) than those after a single dose of Ad35-GRIN (56% and 54 spot-forming units, respectively) or SeV-Gag (55% and 59 spot-forming units, respectively); responses persisted for ≥8 months after completion of the prime-boost regimen. Functional CD8 T-cell responses with greater breadth, magnitude, and frequency in a viral inhibition assay were also seen in the SA and SA groups after Ad35-GRIN boost, compared with those who received either vaccine alone. SeV-Gag did not boost T-cell counts in the AS group. In contrast, the highest Gag-specific antibody titers were seen in the AS group. Mucosal antibody responses were sporadic.
CONCLUSIONS
SeV-Gag primed functional, durable HIV-specific T-cell responses and boosted antibody responses. The prime-boost sequence appears to determine which arm of the immune response is stimulated.
CLINICAL TRIALS REGISTRATION
NCT01705990.
背景
我们报告了首例对一种原型鼻内给药、具有复制能力的仙台病毒(SeV)载体的1型人类免疫缺陷病毒(HIV-1)疫苗进行的人体安全性和免疫原性评估。
方法
肯尼亚、卢旺达和英国的65名未感染HIV-1的成年人被分配接受4种初免-加强免疫方案中的1种(分别在0个月和4个月给药;疫苗与安慰剂接受者的比例为12:4):鼻内给予低剂量SeV-Gag进行初免,随后肌肉注射编码HIV-1 Gag、逆转录酶、整合酶和Nef的腺病毒35载体疫苗(Ad35-GRIN)进行加强免疫(SA);鼻内给予高剂量SeV-Gag进行初免,随后肌肉注射Ad35-GRIN进行加强免疫(SA);肌肉注射Ad35-GRIN进行初免,随后鼻内给予高剂量SeV-Gag进行加强免疫(AS);以及鼻内给予高剂量SeV-Gag进行初免和加强免疫(SS)。
结果
所有疫苗方案耐受性良好。用SeV-Gag初免并以Ad35-GRIN加强免疫的组(SA和SA)中,Gag特异性干扰素-γ酶联免疫斑点法测定的反应率和几何平均反应更高(分别为96%和248个斑点形成单位),高于单次注射Ad35-GRIN(分别为56%和54个斑点形成单位)或SeV-Gag(分别为55%和59个斑点形成单位)后的反应率和几何平均反应;在完成初免-加强免疫方案后,反应持续≥8个月。与单独接受任何一种疫苗的人相比,在Ad35-GRIN加强免疫后的SA和SA组中,在病毒抑制试验中还观察到具有更大广度、强度和频率的功能性CD8 T细胞反应。SeV-Gag在AS组中未提高T细胞计数。相比之下,AS组中观察到最高的Gag特异性抗体滴度。黏膜抗体反应是散发性的。
结论
SeV-Gag引发功能性、持久的HIV特异性T细胞反应并增强抗体反应。初免-加强免疫顺序似乎决定了刺激免疫反应的哪一方面。
临床试验注册
NCT01705990。
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