The efficacy, safety and immunogenicity Nanocovax: results of a randomized, double-blind, placebo-controlled Phase 3 trial.
Thuy Phuong Nguyen; Quyet Do; Lan Trong Phan; Dang Duc Anh; Hiep Khong; Duc Viet Dinh; Luong Van Hoang; Thuong Vu Nguyen; Hung Ngoc Pham; Men Van Chu; Toan Trong Nguyen; Tri Minh Le; Tuyen Thi Ngoc Trang; Thanh Thi Dinh; Thuong Van Vo; Thao Thi Vu; Quynh Bao Phuong Nguyen; Vuong Tan Phan; Luong Viet Nguyen; Giang Truong Nguyen; Phong Minh Tran; Thuan Duc Nghiem; Tien Viet Tran; Tien Gia Nguyen; Tuynh Quang Tran; Linh Tung Nguyen; Anh Tuan Do; Dung Dang Nguyen; Son Anh Ho; Viet Thanh Nguyen; Dung T Pham; Hieu B Tran; Son T Vu; Su Xuan Hoang; Trung Minh Do; Xuan Thanh Nguyen; Giang Quynh Le; Ton Tran; Thang Minh Cao; Huy Manh Dao; Thao Thi Thanh Nguyen; Uyen Y Doan; Vy Thi Tuong Le; Linh Phuong Tran; Ngoc Minh Nguyen; Ngoc Thu Nguyen; Hang Thi Thu Pham; Quan Hoang Nguyen; Quang Duy Pham; Hieu Trung Nguyen; Hang Le Khanh Nguyen; Nguyen Van Trang; Lan Anh Thi Nguyen; Linh Thuy Nguyen; Nhung Thi Hong Trinh; Ly Thi Khanh Le; Van Thi Bao Tran; Mai Thi Ngoc Chu; My Ha Phan; Hoa Thi Hong Nguyen; Vinh The Tran; Mai Thi Nhu Tran; Truc Thi Thanh Nguyen; Phat Tan Ha; Hieu Trong Huynh; Khanh Duy Nguyen; Thuan Trong Ung; Nghia Hoang Trong Duong; Chung Chinh Doan; Si Minh Do.
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| PREPRINT-MEDRXIV | ID: ppmedrxiv-22272739
BackgroundNanocovax is a recombinant severe acute respiratory syndrome coronavirus 2 subunit vaccine composed of full-length prefusion stabilized recombinant SARS-CoV-2 spike glycoproteins (S-2P) and aluminum hydroxide adjuvant. In a Phase 1 and 2 studies, (NCT04683484) the vaccine was found to be safe and induce a robust immune response in healthy adult participants. MethodsWe conducted a multicenter, randomized, double-blind, placebo-controlled study to evaluate the safety, immunogenicity, and protective efficacy of the Nanocovax vaccine against Covid-19 in approximately 13,007 volunteers aged 18 years and over. The immunogenicity was assessed based on Anti-S IgG antibody response, surrogate virus neutralization, wild-type SARS-CoV-2 neutralization and the types of helper T-cell response by intracellular staining (ICS) for interferon gamma (IFNg) and interleukin-4 (IL-4). The vaccine efficacy (VE) was calculated basing on serologically confirmed cases of Covid-19. FindingsUp to day 180, incidences of solicited and unsolicited adverse events (AE) were similar between vaccine and placebo groups. 100 serious adverse events (SAE) were observed in both vaccine and placebo groups (out of total 13007 participants). 96 out of these 100 SAEs were determined to be unrelated to the investigational products. 4 SAEs were possibly related, as determined by the Data and Safety Monitoring Board (DSMB) and investigators. Reactogenicity was absent or mild in the majority of participants and of short duration. These findings highlight the excellent safety profile of Nanocovax. Regarding immunogenicity, Nanocovax induced robust IgG and neutralizing antibody responses. Importantly, Anti S-IgG levels and neutralizing antibody titers on day 42 were higher than those of natural infected cases. Nanocovax was found to induce Th2 polarization rather than Th1. Post-hoc analysis showed that the VE against symptomatic disease was 51.5% (95% confidence interval [CI] was [34.4%-64.1%]. VE against severe illness and death were 93.3% [62.2-98.1]. Notably, the dominant strain during the period of this study was Delta variant. InterpretationNanocovax 25 microgram (mcg) was found to be safe with the efficacy against symptomatic infection of Delta variant of 51.5%. FundingResearch was funded by Nanogen Pharmaceutical Biotechnology JSC., and the Ministry of Science and Technology of Vietnam; ClinicalTrials.gov number, NCT04922788.
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