BCG Vaccine for Health Care Workers as Defense Against COVID 19
SARS-CoV-2 spreads rapidly throughout the world. A large epidemic would seriously challenge the available hospital capacity, and this would be augmented by infection of healthcare workers (HCW). Strategies to prevent infection and disease severity of HCW are, therefore, desperately needed to safeguard continuous patient care. Bacille Calmette-Guérin (BCG) is a vaccine against tuberculosis, with protective non-specific effects against other respiratory tract infections in in vitro and in vivo studies, and reported morbidity and mortality reductions as high as 70%. Furthermore, in our preliminary analysis, areas with existing BCG vaccination programs appear to have lower incidence and mortality from COVID191. The investigators hypothesize that BCG vaccination can reduce HCW infection and disease severity during the epidemic phase of SARS-CoV-2.
Inclusion Criteria
- Adult (≥18 years)
- Male or female
- Hospital personnel taking care for patients with known or suspected SARS-CoV-2 infection and providing, on average, at least 25 hours per week of direct patient care
Exclusion Criteria
- Known allergy to (components of) the BCG vaccine or serious adverse events to prior BCG administration
- Known active or latent Mycobacterium tuberculosis or with another mycobacterial species. A history with- or a suspicion of M. tuberculosis infection.
- Fever (>38 C) within the past 24 hours
- Age > 75 years
- Pregnancy or planning pregnancy within 30 days of study enrollment
- Breastfeeding
- Suspicion of active viral or bacterial infection
- Any Immunocompromised subjects. This exclusion category comprises: a) subjects with known infection by the human immunodeficiency virus (HIV-1); b) subjects with known neutropenic with less than 1500 neutrophils/mm3; c) subjects with solid organ transplantation; d) subjects with bone marrow transplantation; e) subjects under chemotherapy; f) subjects with primary immunodeficiency; g) known severe lymphopenia with less than 400 lymphocytes/mm3; h) treatment with any anti-cytokine therapies. i) treatment with oral or intravenous steroids defined as daily doses of 10mg prednisone or equivalent for longer than 3 months
- Living with someone who is immunosuppressed or taking immunosuppressive drugs
- Previous documented infection with COVID19
- Active solid or non-solid malignancy or lymphoma within the prior two years
- Direct involvement in the design or the execution of the study
- Expected absence from work of ≥4 of the following 12 weeks due to any reason (holidays, maternity leave, retirement, planned surgery etc)
- Not in possession of a smartphone
- Inability to keep the vaccine site covered in the case of a draining pustule.
Additional locations may be listed on ClinicalTrials.gov for NCT04348370.
See trial information on ClinicalTrials.gov for a list of participating sites.
Study design: A placebo-controlled adaptive multi-center randomized controlled trial.
Study population: High risk HCW with direct patient contacts, defined as physician
assistants, respiratory therapists, nurses, physicians or other HCWs working at emergency
rooms, ICUs and in locations within hospitals where COVID-infected patients are treated.
Intervention: Participants will be randomized between intradermal administration of BCG
vaccine or placebo in a 1:1 ratio.
Recruitment, Randomization, treatment allocation, and blinding
A standardized, IRB approved email will be sent to department chairs describing the
study. A research coordinator will reach out to interested participants via phone with
the help of an IRB-approved verbal script to introduce the study, confirm eligibility and
provide further instructions on how to access and sign the IRB-approved ICD via REDCap
using their own electronic devices. It is important that the investigators obtain the
consent via REDCAp to a) avoid direct person-to-person contact and comply with social
distancing imposed recommendations, and b) minimize the waste of reconstituted BCG by
allowing the research personnel to schedule vaccinations in a controlled fashion. Patient
registration into the trial will happen immediately after consent has been provided and
will involve entering of baseline information into an electronic data capture system
(RedCap).
Once the eligibility is confirmed and the ICD signed by the participant and stored in
REDCap, the research coordinator will randomize the participant and communicate the
treatment assignment to the nurse administering the vaccination. The nurse will
subsequently assign an appointment and communicate date and time of vaccination with the
participant. All eligible participants will receive intradermal injections of BCG:placebo
in a 1:1 ratio.
Both, participants and investigators will be blinded to the treatment assignments during
the study. However, in case of an emergency where it is important to know the treatment
received, the investigator and/or participant can reach out to the unblinded study
personnel who will provide the unblinded data. All participants will receive their
treatment allocation at the end of the study, after the data analysis is finalized.
Unblinded personnel will not be involved in the collection and analysis of study data
other than the baseline eligibility criteria.
The end of the study is defined as the last patient's last entry in the electronic data
capture system.
Informed Consent and Eligibility
The following types of procedures will be conducted as indicated below:
Medical history will be obtained from patient medical record/clinical chart. Informed
Consent will be obtained to access these records. When information cannot be obtained or
is not available from the patient medical record/clinical chart, it will be obtained via
patient interview. Physical examination will be conducted solely to look for existing BCG
vaccination scars.
Symptom evaluation will be conducted via an electronic survey administered to
participants every 1-3 days.
HIV and pregnancy will be collected as self-reported information. If unknown, a urine
pregnancy test will be performed.
Nasopharyngeal, oral and/ or rectal swabs will be collected for rt-PCR test for SARS-CoV2
infection if a study develops symptoms consistent with Covid-19.
If a participant does not know their PPD/IGRA status from within the last 24 months (all
health care providers should have this information), an IGRA can be performed to evaluate
eligibility.
Study participants have the option of donating blood via phlebotomy (for serological test
for Covid-19 disease and PBMCs for immune correlates) or providing a fingerstick and
dried blood spot (for serologic test for Covid-19).
Data will be collected at four time points/periods: (1) after consent, (2) at baseline,
(3) during follow-up period, and (4) at study end.
Data to be collected during screening includes medical history, physical exam results,
results of rt-PCR and serological test results.
Data to be collected during baseline enrollment includes eligibility confirmation,
demographic information, risk factors, randomization assignment, confirmation of BCG
vaccination/placebo, any immediate reactions to BCG vaccination/placebo.
Data to be collected during follow-up includes intermittent surveys about the presence of
flu-like symptoms, rt-PCR test results if done, serological test results, if testing
positive for Covid-19 information regarding their disease course, and disease outcome
status.
THE FOLLOWING IS COLLECTED AFTER CONSENT IS OBTAINED:
Date of signed Informed Consent Form
Role in hospital
Department in hospital
rt-PCR test for SARS-CoV2 result
Serological test for Covid-19 result
Number of BCG scars (by visual/physical examination)
Medical history*
Previous PPD and IGRA test results
History of TB disease
History of previous HIV testing
Urine Pregnancy test result (if applicable)
Plans of pregnancy in 30 days
Plan to stop working in 3 months/ leave facility in 6 months
Current diabetes mellitus
Current chronic kidney disease
Currently taking immunosuppressive drugs
Living with someone with HIV, immunocompromised, taking immunosuppressive drug
Chemotherapy in past 3 months
History of organ/bone marrow transplant
Access to smartphone
BASELINE DATA COLLECTION/PROCEDURES
The following procedures will be conducted and data collected as indicated below:
A questionnaire to obtain information about age, sex, demographic information, who they
live with, smoking status, any current medications they are on, and other comorbidities
Participants will then be randomized to either receive a single dose of BCG vaccination
or placebo.
BCG vaccination or placebo will be administered.
Eligibility screening data will carry forward into the trial.
The following additional data points will be collected:
Age
Sex
Race
Ethnicity
Nationality
Who they live with
Height
Weight
Smoking status/tobacco use
Alcohol use
Current list of medications
Current list of comorbidities
History of diabetes mellitus
History of hypertension
History of stroke
History of kidney disease
History of COPD
Randomization assignment
BCG/placebo administered
FOLLOW-UP PROCEDURES AND DATA COLLECTION:
Participants will be followed to assess whether they get infected with SARS-CoV2:
Participants will complete intermittent surveys via an electronic system every 1-3 days
to assess the presence of any flu-like symptom, including sore throat, fever, headache,
malaise, and cough. Note that this is part of routine surveillance for Covid-19 in health
workers at the United States site. Consent forms will ask for consent to access this
survey information.
Any positive response on the survey will trigger a nasopharyngeal, oral and/ or rectal
swab to be collected to test for Covid-19 via rt-PCR
All participants, regardless of survey responses, will have serology for Covid-19 tested
at 4 week intervals during the follow-up period (6 months)
If a participant completes the follow-up period and does not test positive for disease,
their study participation is complete
If a participant does test positive for disease, their disease status will be ascertained
for up to two months or until an outcome is available through one of the following
mechanisms: (1) an electronic survey if they are not admitted to the hospital, including
questions about the number of days they are ill, daily fever, and other symptoms; or (2)
(2) if they are admitted to the hospital, ordinal outcomes for disease severity will be
extracted from the hospital¿s electronic medical records system.
During the first week of follow-up, all participants will actively be asked about any
adverse events; thereafter, participants will report unsolicited AEs through the
electronic survey. Vaccine related adverse events will be graded using the FDA guidance
(https://www.fda.gov/media/73679/download) and noted using WHO-recommended Adverse event
following Immunization forms (AEFI;
https://vaccine-safety-training.org/classification-of-aefis.html).
Participants will have the option of donating 12 mL of blood for plasma (serology) and
PBMCs for secondary analysis of immune correlates and for future analysis based on
covid19-specific IgM and IgG. If they do not donate 12mL of blood, a fingerstick will be
required for baseline COVID19 serology.
Dried Blood Spot (DBS): all participants are HCWs and will self-collect DBS samples at
week 4, 8, 12, 16, 20 and 24. Envelopes to store the DBS are provided upon enrollment and
can be dropped off at work and picked up by study coordinators to minimize HCW
distractions.
COVID specific RNA is found in stool for ~21 days when an individual develops infection
(https://doi.org/10.1038/s41586-020-2196-x). Participants will have the option of
collecting stool swabs monthly if they are asymptomatic or weekly if they develop
symptoms. Nucleic acid testing will be performed in retrospect to support secondary
objectives.
If participants develop symptoms consistent with COVD19, will be PCR tested for COVID19.
They will be given the option of donating 12 mL of blood for plasma and PBMCs 2 weeks
after symptoms resolve.
Week 12 (+/- 2 Weeks), participants will be given the option to donate 12 mL of blood for
plasma and PBMCs for secondary analysis of immune correlates and for future secondary
analysis based on covid-specific IgM and IgG.
Week 24 (+/- 2 Weeks), participants will be given the option to donate 12 mL of blood for
plasma and
PBMCs for secondary analysis of immune correlates and for future secondary analysis based
on covid-specific IgM and IgG.
Except for the administration of BCG vaccine or placebo and the above mentioned DBS and
phlebotomy, participants will undergo no invasive procedures for study purposes.
The following data points will be collected during the follow-up period AND AT
END OF STUDY TIMEPOINT:
Sore throat (collected at multiple time points)
Fever (collected at multiple time points)
Headache (collected at multiple time points)
Malaise (collected at multiple time points)
Cough (collected at multiple time points)
rt-PCR test for SARS-CoV2 result (as indicated)
Serological test for Covid-19 result (every 2 weeks)
Number of days ill
Daily fever
Other Covid-19 symptoms
Admitted to hospital
Required oxygen
Treated in intensive care
Required ventilation
Death
Severe pneumonia
Respiratory failure
Acute respiratory distress syndrome
Sepsis
Septic shock
*Already being collected as part of routine surveillance of health care workers. Will
request access to this information in Informed Consent Form.
Subjects can leave the study at any time for any reason if they wish to do so without any
consequences. The investigator can decide to withdraw a subject from the study for urgent
medical reasons. Participants who received placebo will be unblinded at the end of the
study and pending a recommendation by the DSMB, they will be offered the option of
receiving the BCG intervention.
A participant will only be replaced in case of withdrawal before the administration of
BCG vaccine/placebo.
Trial PhasePhase IV
Trial Typeprevention
Lead OrganizationScott and White Memorial Hospital
- Primary ID2020-0432F
- Secondary IDsNCI-2020-03798
- ClinicalTrials.gov IDNCT04348370