Healthcare Workers (HCW) are at high risk for COVID-19. In addition to the risk of serious forms among HCW, significant absenteeism due to illness would have dramatic consequences in our ability to fight COVID-19. No coronavirus vaccine is available today and drug treatments are only at the start of clinical evaluation. Available since 1921, the bacillus Calmette and Guérin (BCG) is the most widely used vaccine in the world (> 3 billion doses administered) with an extremely low rate of adverse effects. BCG is indicated for the prevention of tuberculosis (TB), but more recent studies have shown that it also has nonspecific immune properties which may be interesting in the current COVID-19 epidemic. Data in mice and in humans have demonstrated protection conferred by BCG against viral respiratory infections such as influenza. In countries with high endemic TB, BCG decreases the incidence of acute respiratory infections by up to 80%, neonatal BCG vaccination has been shown to greatly reduce the risk of sepsis and of hospitalization of children for reasons other than TB. A recent study conducted in South Africa showed that re-vaccination with BCG in adults reduced the incidence of respiratory infections by 70% compared to unvaccinated controls. Beyond respiratory infections, BCG has also shown protective effects against inflammatory diseases. These non-specific beneficial effects are likely linked to the induction of "trained innate immunity", implying epigenetic and metabolic re-programming of innate immune cells. It is therefore possible that revaccination with BCG could significantly reduce the incidence and severity of COVID-19. Very recent ecological observations indeed suggest an inverse correlation between BCG vaccination coverage and the morbidity and mortality of COVID-19. In this context several trials began in Europe and Australia to evaluate the efficacy of BCG vaccination in populations at risk of exposure (HCW) or severe disease (elderly). This study is aligned with studies carried out in Australia, The Netherlands and Spain. In contrast to these latter studies, virtually all French study participants have been vaccinated in their childhood, since BCG vaccination was mandatory in France in neonates until 2007, and in HCW until recently. Therefore, the French study will be in a unique situation to evaluate the effect of re-vaccination with BCG in the context of BCG priming decades before revaccination.
Randomized, multicenter phase III controlled trial, in 2 parallel arms:
- One group vaccinated with BCG
- One group receiving placebo (0.9 % saline) Randomization in a 1: 1 ratio will be
stratified on the center. The study will be proposed to all heath care workers eligible.
At screening, the investigator will propose the study to the participant and explain the
details by providing an information letter. After signature of the consent, evaluations
specific for the study will be undertaken, such as clinical examination, blood sampling,
nasopharyngeal sampling in case of clinical signs.
At the inclusion visit, participants corresponding to the inclusion criteria will be
randomized to receive BCG or placebo.
Participants will receive a single dose of BCG vaccine (or placebo). The adult dose of BCG
vaccine (or placebo) is 0.1 mL injected intradermally over the distal insertion of the
deltoid muscle onto the humerus (approximately one third down the upper arm).
Follow-up visits will be done respectively at M3 and M6 and phone contacts between these two
visits.
Blood samples will be collected prior to randomization (V0) and at 3 and 6 months to
determine exposure to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Where
required, swab/blood samples will be taken at illness episodes to assess SARS-CoV-2
infection.
Participants will be followed for 6 months with regular mobile phone text messages 2 times
weekly to collect local and general reactions until 30 days after vaccination and during the
study to identify and detail COVID-19 infection.
Immunological studies will be conducted at a central Laboratory. Analysis will take place
after M6 visits.
A nested study will be carried out on blood samples of 72 study subjects in order to evaluate
the impact of COVID-19 on innate immunity. These blood samples will be collected at M6 among
6 groups, each containing 12 study subjects:
- One group of subjects vaccinated with BCG that have remained sero-negative for SARS CoV2
- One group of subjects having received placebo that have remained sero-negative for SARS
CoV2
- One group of symptomatic subjects vaccinated with BCG
- One group of symptomatic subjects having received placebo.
- One group without symptoms but sero-positive for SARS CoV2 vaccinated with BCG
- One group without symptoms but sero-positive for SARS CoV2 vaccinated with placebo
Biological: BCG GROUP
One intradermal injection of 0.1 ml of BCG vaccine (AJ Vaccine).Each 0.1 ml vaccine contains between 2 to 8 x 105 colony forming units.
Other Name: Experimental GROUP
Other: PLACEBO GROUP
One intradermal injection of 0.1ml NaCl
Other Name: Control GROUP
Inclusion Criteria:
- Individual (Male and female) aged 18 or over.
- Healthcare Worker (medical or non-medical) from hospitals in direct contact with
COVID-19 patients.
- Participants must give their written consent before any trial procedure.
- Participants covered by social security regimen (excepting AME).
- Healthy according to the opinion of the investigator.
Exclusion Criteria:
- Has any BCG vaccine contraindication, known allergy to the BCG vaccine or SAE to prior
BCG vaccination.
- History of tuberculosis
- People with acquired or innate immunodeficiency.
- People have already been infected with SARS Cov-2 (virological documentation or TDM or
seropositive if serology available).
- People who could not commit to follow-up for 6 months.
- People not in good general condition, as assessed by the investigator.
- People included in other clinical trials assessing treatment.
- Pregnant or breastfeeding or positive urine pregnancy at enrolment visit.
- BCG vaccine given within the last year.
- Another live vaccine administered in the month prior to randomization.
- History of anaphylaxis following vaccination.
- Receiving medical treatment that affects the immune response or other
immunosuppressive therapy in the last year. These therapies include systemic
corticosteroids (more than or equal to 10 mg for more than or equal to 2 weeks),
immunosuppressant, biological agents (such as monoclonal antibodies against tumour
necrosis factor (TNF)-alpha).
- Another vaccine administered in the month prior to inclusion and randomization.
- Fever > 38°C within the past 24 hours
- People with malignancies (e.g. lymphoma, leukemia, Hodgkin's disease or other tumors
of the reticuloendothelial system) or infected with HIV
- Receipt of immune globulins, blood or blood-derived products in the past 3 months
- Acute severe febrile illness
- Generalized infected skin conditions
- People under legal protection measure (tutorship, curatorship or safeguard measures)
I-REIVAC/CIC 1417 Cochin Hospital, APHP
Paris, France
Investigator: Odile LAUNAY, Professor
Contact: 01 58 41 28 58
odile.launay@aphp.fr
Odile LAUNAY, Professor
01 58 41 28 58
odile.launay@aphp.fr
Anne RADENNE
01 42 16 16 99
anne.radenne@aphp.fr