Research Article
Recombinant Receptor Binding Domain Protein Induces Partial Protective Immunity in Rhesus Macaques Against Middle East Respiratory Syndrome Coronavirus Challenge ☆- Jiaming Lana, d, 1,
- Yanfeng Yaob, 1,
- Yao Denga, 1,
- Hong Chena,
- Guangwen Luc,
- Wen Wanga,
- Linlin Baob,
- Wei Dengb,
- Qiang Weib,
- George F. Gaoc,
- Chuan Qinb, , ,
- Wenjie Tana, ,
Received 24 June 2015, Revised 16 August 2015, Accepted 17 August 2015, Available online 18 August 2015
Highlights
•In this study, we evaluated a recombinant receptor binding domain(rRBD) based subunit vaccine in a rhesus macaque model. •Significant and sustained immunuity in a rhesus macaque model were elicited by the rRBD vaccination. •Partial protection was observed in the vaccinated monkeys against the MERS-CoV challenge. •We suggest the partial protection in monkey against the MERS-CoV challenge may be conferred by neutralizing antibodies induced by rRBD immunity. •The study provided useful information for the development of a human vaccine against MERS-CoV infection. AbstractBackgroundDevelopment an effective vaccine against Middle East respiratory syndrome coronavirus (MERS-CoV) is urgent and limited information is available on vaccination in nonhuman primate (NHP) model. We herein report of evaluating a recombinant receptor-binding domain (rRBD) protein vaccine in a rhesus macaque model. MethodsNine monkeys were randomly assigned to high-dose, low-dose and mock groups,which were immunized with different doses of rRBD plus alum adjuvant or adjuvant alone at different time points (0, 8, 25 weeks). Immunological analysis was conducted after each immunisation. Monkeys were challenged with MERS-CoV at 14 days after the final immunisation followed by observation for clinical signs and chest X-rays. Nasal, oropharyngeal and rectal swabs were also collected for analyses. Monkeys were euthanized 3 days after challenge and multiple specimens from tissues were collected for pathological, virological and immunological tests. ConclusionRobust and sustained immunological responses (including neutralisation antibody) were elicited by the rRBD vaccination. Besides, rRBD vaccination alleviated pneumonia with evidence of reduced tissue impairment and clinical manifestation in monkeys. Furthermore, the rRBD vaccine decreased viral load of lung, trachea and oropharyngeal swabs of monkeys. These data in NHP paves a way for further development of an effective human vaccine against MERS-CoV infection.
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