Combination Assessment Trial of COVID-19 Vaccines (COMBAT-COVID)
NCT ID: NCT05162482
Last Updated: 2022-02-18
Study Results
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Basic Information
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UNKNOWN
PHASE2
1680 participants
INTERVENTIONAL
2022-03-01
2024-06-30
Brief Summary
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Detailed Description
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The total duration of the trial will be approximately 2 ½ years. The study will enroll participants which will be divided into 2 cohorts, one for a more detailed immunological assessment and one for main immunology endpoints. The study will include 9 study groups with different combinations of COVID-19 vaccine schedule (6 heterologous combinations and 3 homologous combinations plus booster in homologous arms). The investigators will be measuring Anti-spike IgG antibodies by ELISA at week 14 (4 weeks post booster dose) and pseudo neutralizing antibodies against SARS-CoV-2 at day 0, and weeks 4, 14, 24, 28, 48, 60 and 96 as per schedule of events for the immunology cohort and at baseline and 4 weeks post second dose in general cohort. This is a pragmatic trial where the interval between the two doses will be kept longer than the conventional recommendations of 21/28 days. Additionally, the investigators will also be assessing safety and reactogenicity by recording serious adverse events (SAE), adverse events of special interest (AESI), solicited local and systemic reactions within 7 days post each dose, unsolicited reactions within 28 days post each dose, medically attended adverse reactions up to 3 months post booster dose and changes from baseline to 4 weeks post each dose in biochemical and hematological tests or safety measures throughout the study.
A trained person will administer the vaccine and draw blood samples under strict aseptic techniques to ensure minimum discomfort and reduce the risk of infection. There is a risk of adverse events associated with all vaccines and there can be some risks associated with vaccine administration and blood collection procedures like pain, redness, itch, swelling, fever, feverishness, chills, joint pains, muscle pains, fatigue, headache, malaise, nausea, vomiting, diarrhea etc. However, in most cases the adverse events are mild and self-limiting but can require medication and/or hospitalization in rare cases. Participants suffering from any adverse event causally related to the to the trial intervention will be facilitated and the cost of treatment including laboratory investigations will be provided to them. The participants will also be compensated for their time, the inconvenience of getting jabs and providing blood samples.
Confidentiality of all the data collected from the population is a top priority. All the names and personal information regarding any individual will not to be disclosed separately. The data will be published collectively. All the names present in the forms will be de linked and forms will be coded accordingly all the data files will be password protected. Data that will be shared with University of Oxford, International Vaccine Institute (IVI), Seoul, Republic of Korea, Ragon Institute, Harvard School of Medicine, USA, National Institute of Health (NIH) Pakistan will have multi-layered security with several layers of encryption to protect data. Blood samples from patients enrolled will be stored at our research office in Infectious disease research laboratory at Aga Khan University Karachi, labelled with identification numbers not participant name. During the storage, only dedicated members of our study team will have access to the samples. De-identified research data maybe be stored indefinitely. If volunteers consent to be contacted for future research, a record of this consent will be recorded, retained, and stored securely and separately from the research data. If volunteers consent to have their samples stored and used for future research, information about their consent form will be retained and stored securely as per Biobanking procedures and SOPs. Identifiable information such as contact details will be stored for a minimum of 5 years from the end of the study. This includes storage of consent forms. Storage of data will be reviewed every 5 years and files will be confidentially destroyed if storage is no longer required. During the storage, only the local PIs and researchers designated by them will have access to the data or samples.
Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
NONE
Study Groups
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Heterologous 1
BIBP (CNBG, Sinopharm) WIV (0.5ml) at baseline CanSinoBIO (0.5ml) after 70±7 days (10 wks±2)
(160 participants)
BIBP (CNBG, Sinopharm) WIV
BIBP (CNBG, Sinopharm) WIV (Whole Inactivated Virus in a single dose, prefilled syringe with a storage temperature of 2-8°C)
CanSinoBIO
CanSinoBIO (Viral Vector in a single dose, prefilled syringe with a storage temperature of 2-8°C)
Heterologous 2
BIBP (CNBG, Sinopharm) WIV (0.5ml) at baseline AstraZeneca ChAdOx (0.5ml) after 70±7 days (10 wks±2)
(160 participants)
BIBP (CNBG, Sinopharm) WIV
BIBP (CNBG, Sinopharm) WIV (Whole Inactivated Virus in a single dose, prefilled syringe with a storage temperature of 2-8°C)
AstraZeneca ChAdOx
AstraZeneca ChAdOx (Viral Vector in a multi-dose vial consisting of 10 doses with a storage temperature of 2-8°C)
Heterologous 3
CanSinoBIO (0.5ml) at baseline BIBP (CNBG, Sinopharm) WIV (0.5ml) after 70±7 days (10 wks±2)
(160 participants)
BIBP (CNBG, Sinopharm) WIV
BIBP (CNBG, Sinopharm) WIV (Whole Inactivated Virus in a single dose, prefilled syringe with a storage temperature of 2-8°C)
CanSinoBIO
CanSinoBIO (Viral Vector in a single dose, prefilled syringe with a storage temperature of 2-8°C)
Heterologous 4
CanSinoBIO (0.5ml) at baseline AstraZeneca ChAdOx (0.5ml) after 70±7 days (10 wks±2)
(160 participants)
CanSinoBIO
CanSinoBIO (Viral Vector in a single dose, prefilled syringe with a storage temperature of 2-8°C)
AstraZeneca ChAdOx
AstraZeneca ChAdOx (Viral Vector in a multi-dose vial consisting of 10 doses with a storage temperature of 2-8°C)
Heterologous 5
AstraZeneca ChAdOx (0.5ml) at baseline BIBP (CNBG, Sinopharm) WIV(0.5ml) after 70±7 days (10 wks±2)
(160 participants)
BIBP (CNBG, Sinopharm) WIV
BIBP (CNBG, Sinopharm) WIV (Whole Inactivated Virus in a single dose, prefilled syringe with a storage temperature of 2-8°C)
AstraZeneca ChAdOx
AstraZeneca ChAdOx (Viral Vector in a multi-dose vial consisting of 10 doses with a storage temperature of 2-8°C)
Heterologous 6
AstraZeneca ChAdOx (0.5ml) at baseline CanSinoBIO (0.5ml) after 70±7 days (10 wks±2)
(160 participants)
CanSinoBIO
CanSinoBIO (Viral Vector in a single dose, prefilled syringe with a storage temperature of 2-8°C)
AstraZeneca ChAdOx
AstraZeneca ChAdOx (Viral Vector in a multi-dose vial consisting of 10 doses with a storage temperature of 2-8°C)
Homologous 7
BIBP (CNBG, Sinopharm) WIV (0.5ml) at baseline BIBP (CNBG, Sinopharm) WIV (0.5ml) after 70±7 days (10 wks±2) Full dose booster: 80 participants (0.5ml) 6 months after second dose Fractional dose booster: 80 participants (dose to be decided) 6 months after second dose No booster: 80 participants
(240 participants)
BIBP (CNBG, Sinopharm) WIV
BIBP (CNBG, Sinopharm) WIV (Whole Inactivated Virus in a single dose, prefilled syringe with a storage temperature of 2-8°C)
Homologous 8
CanSinoBIO (0.5ml) at baseline CanSinoBIO (0.5ml) after 70±7 days (10 wks±2) Full dose booster: 80 participants (0.5ml) 6 months after second dose Fractional dose booster: 80 participants (dose to be decided) 6 months after second dose No booster: 80 participants
(240 participants)
CanSinoBIO
CanSinoBIO (Viral Vector in a single dose, prefilled syringe with a storage temperature of 2-8°C)
Homologous 9
AstraZeneca ChAdOx (0.5ml) at baseline AstraZeneca ChAdOx (0.5ml) after 70±7 days (10 wks±2) Full dose booster: 80 participants (0.5ml) 6 months after second dose Fractional dose booster: 80 participants (dose to be decided) 6 months after second dose No booster: 80 participants
(240 participants)
AstraZeneca ChAdOx
AstraZeneca ChAdOx (Viral Vector in a multi-dose vial consisting of 10 doses with a storage temperature of 2-8°C)
Interventions
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BIBP (CNBG, Sinopharm) WIV
BIBP (CNBG, Sinopharm) WIV (Whole Inactivated Virus in a single dose, prefilled syringe with a storage temperature of 2-8°C)
CanSinoBIO
CanSinoBIO (Viral Vector in a single dose, prefilled syringe with a storage temperature of 2-8°C)
AstraZeneca ChAdOx
AstraZeneca ChAdOx (Viral Vector in a multi-dose vial consisting of 10 doses with a storage temperature of 2-8°C)
Eligibility Criteria
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Inclusion Criteria
* Participant is willing and able to give written informed consent for participation in the trial.
* Male or Female aged 18 years or above and in good health as determined by a trial clinician. Participants may have well controlled mild-moderate comorbidity.
* In the Investigator's opinion, is able and willing to comply with all trial requirements.
* Residing in the study areas.
Exclusion Criteria
* Pregnant women or those who are planning to conceive within next 70 days.
* Women who are breast feeding
* Already received any COVID-19 vaccine or any other vaccine likely to impact on interpretation of the trial data (e.g., Adenovirus vectored vaccines).
* Administration of immunoglobulins and/or any blood products within the three months preceding the planned administration of the vaccines.
* Any confirmed or suspected immunosuppressive or immunodeficient state; asplenia; recurrent severe infections and use of immunosuppressant medication within the past 6 months, except topical steroids or short-term oral steroids (course lasting ≤14 days)
* History of allergic disease or reactions likely to be exacerbated by any component of study vaccines (e.g., hypersensitivity to the active substance of the COVID-19 vaccines included in the study groups
* Any history of anaphylaxis.
* Current diagnosis of or treatment for cancer (except basal cell carcinoma of the skin and cervical carcinoma in situ)
* Bleeding disorder (e.g., factor deficiency, coagulopathy, or platelet disorder), or prior history of thrombotic events and/or significant bleeding or bruising following IM injections or venipuncture.
* Continuous use of anticoagulants, such as coumarins and related anticoagulants (i.e., warfarin)
* Any other significant disease, disorder or finding which may significantly increase the risk to the volunteer because of participation in the study, affect the ability of the volunteer to participate in the study or impair interpretation of the study data.
* Severe and/or uncontrolled cardiovascular disease, respiratory disease, gastrointestinal disease, liver disease, renal disease, endocrine disorder, and neurological illness (mild/moderate well controlled comorbidities are allowed)
* History of active or previous auto-immune neurological disorders (e.g., multiple sclerosis, Guillain-Barre syndrome, transverse myelitis). Bell's palsy will not be an exclusion criterion.
* History of laboratory confirmed COVID-19 within 6 months prior to enrolment (history of SARS-CoV-2 detection by PCR or antibody to SARS-CoV-2).
* Scheduled elective surgery during the trial.
* Participants enrolled in any other research trial.
* Participants planning to migrate out of the study area within 2 years of the study.
If the volunteer has any of the following, they will not be enrolled that day.
* Acute respiratory illness (moderate or severe illness with or without fever)
* Fever (temperature greater than 38°C) They may be considered for enrolment later in the trial if they recover in sufficient time.
18 Years
ALL
Yes
Sponsors
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Coalition for Epidemic Preparedness Innovations
OTHER
University of Oxford
OTHER
International Vaccine Institute
OTHER
Harvard Medical School (HMS and HSDM)
OTHER
Chughtai Lab
UNKNOWN
National Institute of Health, Pakistan
UNKNOWN
Aga Khan University Hospital, Pakistan
OTHER
Responsible Party
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Dr. Farah Qamar
Associate Professor
Principal Investigators
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Farah Qamar
Role: PRINCIPAL_INVESTIGATOR
Aga Khan University Hospital, Pakistan (AKU)
Tahir Yousafzai
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Zahra Hassan
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Junaid Iqbal
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Kiran Iqbal
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Sonia Qureshi
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Maria Fletcher
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Najeeha Iqbal
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Momin Kazi
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Shazia Sultana
Role: STUDY_DIRECTOR
Aga Khan University Hospital, Pakistan (AKU)
Andrew Pollard
Role: STUDY_DIRECTOR
University of Oxford
Matthew Snape
Role: STUDY_DIRECTOR
University of Oxford
Teresa Lambe
Role: STUDY_DIRECTOR
University of Oxford
Xinxue Liu
Role: STUDY_DIRECTOR
University of Oxford
Anh Wartel
Role: STUDY_DIRECTOR
International Vaccine Institute (IVI), Korea
Jean-Louis Excler
Role: STUDY_DIRECTOR
International Vaccine Institute (IVI), Korea
Deok-Ryun Kim
Role: STUDY_DIRECTOR
International Vaccine Institute (IVI), Korea
Galit Alter
Role: STUDY_DIRECTOR
Ragon Institute, Harvard School of Medicine, USA
Aamir Ikram
Role: STUDY_DIRECTOR
National Institute of Health (NIH) Pakistan
Ghazala Parveen
Role: STUDY_DIRECTOR
National Institute of Health (NIH) Pakistan
Firdous Nawaz Khan
Role: STUDY_DIRECTOR
National Institute of Health (NIH) Pakistan
Omera Naseer
Role: STUDY_DIRECTOR
National Institute of Health (NIH) Pakistan
Locations
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National Institute of Health
Islamabad, Punjab Province, Pakistan
Chughtai Lab
Lahore, Punjab Province, Pakistan
Aga Khan University
Karachi, Sindh, Pakistan
Countries
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Central Contacts
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Facility Contacts
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Rakshanda Ambreen
Role: primary
References
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Saleem AF, Mach O, Yousafzai MT, Khan A, Weldon WC, Oberste MS, Sutter RW, Zaidi AKM. Needle adapters for intradermal administration of fractional dose of inactivated poliovirus vaccine: Evaluation of immunogenicity and programmatic feasibility in Pakistan. Vaccine. 2017 May 31;35(24):3209-3214. doi: 10.1016/j.vaccine.2017.04.075. Epub 2017 May 4.
Saleem AF, Mach O, Yousafzai MT, Khan A, Weldon WC, Steven Oberste M, Zaidi SS, Alam MM, Quadri F, Sutter RW, Zaidi AKM. Immunogenicity of Different Routine Poliovirus Vaccination Schedules: A Randomized, Controlled Trial in Karachi, Pakistan. J Infect Dis. 2018 Jan 17;217(3):443-450. doi: 10.1093/infdis/jix577.
Saleem AF, Yousafzai MT, Mach O, Khan A, Quadri F, Weldon WC, Oberste MS, Zaidi SS, Alam MM, Sutter RW, Zaidi AKM. Evaluation of vaccine derived poliovirus type 2 outbreak response options: A randomized controlled trial, Karachi, Pakistan. Vaccine. 2018 Mar 20;36(13):1766-1771. doi: 10.1016/j.vaccine.2018.02.051. Epub 2018 Feb 21.
Yousafzai MT, Saleem AF, Mach O, Baig A, Sutter RW, Zaidi AKM. Feasibility of conducting intradermal vaccination campaign with inactivated poliovirus vaccine using Tropis intradermal needle free injection system, Karachi, Pakistan. Heliyon. 2017 Sep 18;3(8):e00395. doi: 10.1016/j.heliyon.2017.e00395. eCollection 2017 Aug.
Saleem AF, Mach O, Yousafzai MT, Kazi Z, Baig A, Sajid M, Jeyaseelan V, Sutter RW, Zaidi AKM. One-Year Decline of Poliovirus Antibodies Following Fractional-Dose Inactivated Poliovirus Vaccine. J Infect Dis. 2021 Apr 8;223(7):1214-1221. doi: 10.1093/infdis/jiaa504.
Riaz A, Mohiuddin S, Husain S, Yousafzai MT, Sajid M, Kabir F, Rehman NU, Mirza W, Salam B, Nadeem N, Pardhan K, Khan KMA, Raza SJ, Arif F, Iqbal K, Zuberi HK, Whitney CG, Omer SB, Zaidi AKM, Ali A; Pakistan Pneumococcal Vaccine Study Group. Effectiveness of 10-valent pneumococcal conjugate vaccine against vaccine-type invasive pneumococcal disease in Pakistan. Int J Infect Dis. 2019 Mar;80:28-33. doi: 10.1016/j.ijid.2018.12.007. Epub 2018 Dec 18.
Qamar FN, Yousafzai MT, Khaliq A, Karim S, Memon H, Junejo A, Baig I, Rahman N, Bhurgry S, Afroz H, Sami U. Adverse events following immunization with typhoid conjugate vaccine in an outbreak setting in Hyderabad, Pakistan. Vaccine. 2020 Apr 23;38(19):3518-3523. doi: 10.1016/j.vaccine.2020.03.028. Epub 2020 Mar 20.
Qamar FN, Batool R, Qureshi S, Ali M, Sadaf T, Mehmood J, Iqbal K, Sultan A, Duff N, Yousafzai MT. Strategies to Improve Coverage of Typhoid Conjugate Vaccine (TCV) Immunization Campaign in Karachi, Pakistan. Vaccines (Basel). 2020 Nov 19;8(4):697. doi: 10.3390/vaccines8040697.
Provided Documents
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Document Type: Study Protocol and Statistical Analysis Plan
Document Type: Informed Consent Form
Related Links
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Patel D. Poverty in Pakistan: Numerous efforts, many numbers, not enough results 2015
Other Identifiers
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6739
Identifier Type: -
Identifier Source: org_study_id
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