Phadke Varun K, Gromer Daniel J, Rebolledo Paulina A, Graciaa Daniel S, Wiley Zanthia, Sherman Amy C, Scherer Erin M, Leary Maranda, Girmay Tigisty, McCullough Michele P, Min Ji-Young, Capone Stefania, Sommella Andrea, Vitelli Alessandra, Retallick Jamie, Seetahal Janine, Koller Mark, Tsong Rachel, Neill-Gubitz Hannah, Mulligan Mark J, Rouphael Nadine G
Hope Clinic, Division of Infectious Diseases, Emory University School of Medicine, Atlanta, GA, USA.
Hope Clinic, Division of Infectious Diseases, Emory University School of Medicine, Atlanta, GA, USA.
Vaccine. 2024 Dec 2;42(26):126441. doi: 10.1016/j.vaccine.2024.126441. Epub 2024 Oct 16.
Rabies is a zoonotic viral encephalitis that is endemic in many countries and confers a high mortality. Licensed vaccines require several doses to ensure efficacy. To investigate a logistically favorable approach, we assessed the safety and immunogenicity of ChAd155-RG, a novel investigational rabies vaccine using a replication-defective chimpanzee adenovirus vector.
We conducted a first-in-human, phase 1, randomized, double-blind, dose-escalation trial comparing ChAd155-RG with a licensed inactivated vaccine (RabAvert) in healthy adults. Participants received either RabAvert at standard dosing or ChAd155-RG at a low dose for one immunization or a high dose for one or two immunizations. To assess safety, we evaluated reactogenicity, unsolicited adverse events, and thrombotic events. To measure immunogenicity, we measured rabies viral neutralizing antibody (VNA) titers and anti-ChAd155 neutralizing antibodies.
Mild to moderate systemic reactogenicity and transient lymphopenia and neutropenia were more common among recipients of ChAd155-RG compared with those who received RabAvert. No thrombotic events or serious adverse events were reported. Only the groups receiving RabAvert or two doses of high-dose ChAd155-RG achieved 100 % seroconversion, and seroprotection was most durable in the RabAvert group. Most participants had preexisting anti-vector antibodies, which were boosted by ChAd155-RG. Baseline and post-vaccination anti-vector antibody titers were negatively associated with post-vaccination rabies VNA titers.
In this phase 1 clinical trial, a novel rabies vaccine using a simian adenovirus vector was safe and tolerable, but generated lower, less durable rabies VNA titers than a standard inactivated rabies virus vaccine, which may be due to preexisting, anti-vector immunity.
狂犬病是一种人畜共患的病毒性脑炎,在许多国家流行,死亡率很高。已获许可的疫苗需要多剂接种以确保疗效。为了研究一种在后勤方面有利的方法,我们评估了ChAd155-RG的安全性和免疫原性,ChAd155-RG是一种使用复制缺陷型黑猩猩腺病毒载体的新型研究性狂犬病疫苗。
我们在健康成年人中进行了一项首次人体1期随机双盲剂量递增试验,将ChAd155-RG与一种已获许可的灭活疫苗(RabAvert)进行比较。参与者接受标准剂量的RabAvert,或低剂量的ChAd155-RG进行一次免疫接种,或高剂量的ChAd155-RG进行一次或两次免疫接种。为了评估安全性,我们评估了反应原性、自发不良事件和血栓形成事件。为了测量免疫原性,我们测量了狂犬病病毒中和抗体(VNA)滴度和抗ChAd155中和抗体。
与接受RabAvert的人相比,ChAd155-RG的接受者中轻度至中度全身反应原性以及短暂性淋巴细胞减少和中性粒细胞减少更为常见。未报告血栓形成事件或严重不良事件。只有接受RabAvert或两剂高剂量ChAd155-RG的组实现了100%的血清转化,并且RabAvert组的血清保护最持久。大多数参与者预先存在抗载体抗体,ChAd155-RG使其增强。基线和接种疫苗后的抗载体抗体滴度与接种疫苗后的狂犬病VNA滴度呈负相关。
在这项1期临床试验中,一种使用猿猴腺病毒载体的新型狂犬病疫苗是安全且可耐受的,但产生的狂犬病VNA滴度低于标准灭活狂犬病病毒疫苗,且持久性较差,这可能是由于预先存在的抗载体免疫所致。
