Covid-19 Living Data

Trial RPCEC00000346
Publication Hernandez-Bernal, EClinicalMedicine, 2022
Dates: 2020-12-07 to 2021-02-09
Funding: Public/non profit (Center for Genetic Engineering and Biotechnology (CIGB), Havana (products, reagents); the Ministry of Public Health of Cuba (hospital facilities and general medical care of the participants))
Conflict of interest: Yes

Methods
	RCT
	Location : Single center / Cuba Follow-up duration (months): 2.33
	25 mcg CIGB-66 (RBD) Abdala D0/14/28 (n = 22) 50 mcg CIGB-66 (RBD) Abdala D0/14/28 (n = 22) Placebo D0/14/28 (n = 22) 25 mcg CIGB-66 (RBD) Abdala D0/28/56 (n = 22) 50 mcg CIGB-66 (RBD) Abdala D0/28/56 (n = 22) Placebo D0/28/56 (n = 22)
Inclusion criteria	Aged between 19 and 54 years healthy adults written informed consent to participate
Exclusion criteria	Virological diagnosis by RT-PCR of infection to SARS-CoV-2 contact or suspect of COVID-19 subjects at high risk of exposure to SARS-CoV-2 infection (health workers in 1st line of medical care) acute infection in the last 15 days autoimmune or endocrine-metabolic diseases decompensated at the time of inclusion treated in the last three months or with any medical condition that requires an immunomodulator, steroid (except topical or inhaled) or cytostatic during the study body mass index ≤18 or ≥35 Kg/m2 tattoos in both deltoid regions administration of any research product in the last three months allergy to thiomersal or any other component of the medicament pregnancy or breastfeeding mental disorders
Interventions
	Intervention 3 IM doses 25 mcg CIGB, each 14 days apart 3 IM doses 50 mcg CIGB, each 14 days apart 3 IM doses 25 mcg CIGB, each 28 days apart 3 IM doses 50 mcg CIGB, each 28 days apart
	Control 3 IM doses adjuvant placebo, each 14 days apart3 IM doses adjuvant placebo, each 28 days apart
Participants
	Randomized 132 participants
	Characteristics of participants Type of participants: Healthy adults N=132 72 males Children: 0 Pregnant women: 0 Immunocompromized patients: 0 Mean age: Age range: NR
	Description of participants Healthy adults that were SARS-CoV-2 infection-free and with no recent contact or high-risk of exposure to COVID-19 at a single center in Cuba
Primary outcome
	In the register 1) Adverse clinical events [at 24, 48 and 72 hours, and on the 7th day]; 2) Seroconversion of anti-RBD IgG antibodies to SARS-CoV-2 [on days 28 and 42 (for the short scheme 0-14-28) and 28, 56 and 70 (for the long scheme 0-28-56)]
	In the report Safety of the candidate (the non-occurrence of serious adverse events with a causal relationship attributable to the research product in no more than 5% of the subjects)
Documents available	Protocol Yes. In English Statistical plan Yes Data-sharing stated: Yes, When the trial is complete, upon requests directed to the corresponding author and after approval of a proposal Data accessibility: hernandez.bernal@cigb.edu.cu data can be shared through a secure online platform after signing a data access agreement.
Risk of bias Overall The overall risk of bias reported in the table corresponds to the highest risk of bias for the outcomes assessed for the systematic review	Some concerns
General comment	In addition to the published and pre-print articles, the prospective study registry was used in data extraction and risk of bias assessment. Neither protocol nor statistical analysis plan was available. The target sample size specified was achieved (n=132). There is no change from the trial registration in the intervention and control interventions. The primary outcomes reported in the article reflect those in the registry. Some reported outcomes were not planned in the registry (neutralizing antibody seroconversion and GMTs). The participants in the 3 short schedule arms (n=66) were also included in the phase 1-2 report. This study has been updated on June 21st, 2022 after publication of the trial report.