Pertussis Clinical Trial
— GaPsOfficial title:
Randomised, Double-blinded, Open Label Study in Pregnant Women, Exploring the Impact of Acellular Pertussis Vaccination in Pregnancy on the Immunogenicity in Infants Randomized to Receive Either an Acellular (aP) or Whole Cell Pertussis (wP) Vaccine Subsequently
Verified date | March 2022 |
Source | London School of Hygiene and Tropical Medicine |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
Currently, there are two types of vaccines available against pertussis (whooping cough), an infectious disease of the respiratory tract that can be extremely serious in very young children. Both have advantages and disadvantages: The acellular form (aP, mainly used in resource-rich countries) does not appear to offer as long lasting protection, but the whole cell vaccine (wP, mainly used in LMIC) appears to be generally more reactogenic. There is consensus that a "better pertussis vaccine" ought to be designed. The GaPs trial is part of a series of clinical trials performed by the PERtussIS COrrelates of Protection Europe (PERISCOPE) Consortium, an EU-funded group of investigators which aims to generate knowledge on immune responses to pertussis. A better understanding of human biomarkers of protective immune responses to B. pertussis and its waning immunity is needed to accelerate the design and testing of new pertussis vaccines with a longer duration of protection. This proposal describes the design and objectives of the clinical trial to be conducted in the Gambia, which is the only site in Africa involved in the consortium and involves the recruitment of 600 mother/infant pairs. Pregnant women will be randomised to receive either the usually recommended tetanus vaccination or a combination vaccine against whooping cough, diptheria, tetanus and polio. Their infants will receive either aP or wP as part of their EPI vaccines, and resulting immune responses will be characterized in detail up to the age of 9 months. The investigators will use immunological assays to investigate the functional humoral and cellular responses to pertussis in infants born to mothers who are randomized to receiving pertussis vaccine in pregnancy or not, and their infants who will receive either aP or wP vaccine. Our research questions are: Does vaccination against pertussis in pregnancy have impact on subsequent immune responses to pertussis vaccine and other EPI vaccines in the infants Does vaccination of infants with wP vaccine induce different levels and functionality of antibody and/or T cell responses than vaccination with aP vaccine What is the difference in innate and acquired immunity- as measured with novel systems vaccinology tools- between being vaccinated with wP versus aP?
Status | Active, not recruiting |
Enrollment | 600 |
Est. completion date | December 2022 |
Est. primary completion date | May 18, 2022 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | Female |
Age group | 18 Years to 40 Years |
Eligibility | Inclusion Criteria: - signed /thumb-printed informed consent for trial participation obtained - Pregnant women between 18 and 40 years of age inclusive on day of consent - Singleton pregnancy - From 28 to 34 weeks gestation inclusive as determined by USS on day of randomization. - Resident within easy reach of the clinical trial site (no fixed boundaries will be set and such judgements will be made on a case by case basis by members of the field team in discussion with the potential participant, taking into account knowledge of the local transport links and geography) - Intention to deliver at the health centre related to the Sukuta clinical trial site - Willingness and capacity to comply with all the study procedures, including those relating to the newborn infant, in the opinion of the principal investigator or delegee. Exclusion Criteria: - History of pre-eclampsia or eclampsia - Gestational diabetes in current pregnancy - Rhesus negative multigravida - Grandmultigravida (more than 5 previous pregnancies) - Previous late stillbirth (defined as loss of pregnancy at any time after 28 weeks gestation) - Previous low birth weight baby or premature delivery (defined as a delivery before 37 weeks gestation) - Previous neonatal death (defined as death of an infant within the first 28 days of life) - Previous delivery of an infant with a known or suspected genetic or chromosomal abnormality - History of other significant pregnancy related complications judged likely to affect the safety of the mother or infant or to significantly compromise the endpoint data collected - History of other significant neonatal complications judged likely to affect the safety of the mother or infant or to significantly compromise the endpoint data collected - Smoke cigarettes, alcohol consumption or use of illegal drugs during current pregnancy - Significant maternal chronic illness including but not limited to hypertension requiring treatment, heart disease, lung disease, neurological disorders including a history of epilepsy or recurrent afebrile seizures, kidney disease, liver disease, anaemia and other haematological disorders (including sickle cell), endocrine disorders including known diabetes mellitus, autoimmunity - Severe anaemia (less than 7.0g/dL) - Known Human Immunodeficiency Virus (HIV) or hepatitis B (HBV) virus positive or found to be HIV or HBV positive during screening - Positive result for syphilis infection on laboratory testing - Receipt of any vaccine during the current pregnancy or plans to receive any non-study vaccines during the current pregnancy (tetanus toxoid vaccination is not an exclusion and vaccines given during national campaigns if applicable will not generally be exclusions) - Any other condition judged to significantly increase the risks to either the mother or the infant within the current pregnancy (including relevant history from previous pregnancies) - History of anaphylactic or severe allergic reactions to previous vaccines or history of anaphylactic or severe allergic reactions in previous offspring (if applicable) - Receipt of any blood product including human immunoglobulins at any stage during the current pregnancy or plan to receive any blood products during the period or trial participation (receipt or blood products in an emergency or for obstetric reasons will not represent a protocol deviation given such situations are unplanned) - Receipt of immunosuppressive or immuno-modulatory medication at any stage during the current pregnancy or plan to receive any such medication during the period or trial participation - Clinically suspected or confirmed congenital or acquired clotting or bleeding disorders or the current receipt of medications known to alter clotting or bleeding - Current malaria infection (on the day of randomization and vaccination) - Any clinically significant signs or symptoms of acute illness, significant abnormalities in vital signs, an axillary temperature of greater than 38.0°C or any recorded fever (greater than 38.0°C) in the preceding 24 hours. - Two or more symptoms (nausea/vomiting, diarrhoea, headaches, fatigue and myalgia) rated as grade 2 and clinically significant on the maternal systemic reactogenicity scale (2 Table 5) present at baseline on the day of vaccination - Deprived of freedom by an administrative or court order, or in an emergency setting, or hospitalized - involuntarily - Participation in the 4 weeks preceding the trial vaccination or planned participation during the present trial period in another clinical trial investigating a vaccine, drug, medical device, or medical procedure |
Country | Name | City | State |
---|---|---|---|
Gambia | Sukuta Health Centre | Sukuta | Banjul |
Lead Sponsor | Collaborator |
---|---|
London School of Hygiene and Tropical Medicine | Imperial College London, Leiden University Medical Center, National Institute for Public Health and the Environment (RIVM), Radboud University Medical Center, University of Oxford, University of Turku |
Gambia,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | PT specific antibody GMC | PT-specific antibody GMC at 20 weeks in infants vaccinated with aP versus wP | 20 weeks | |
Primary | PT specific antibody GMC | PT-specific antibody GMC at 9 months in infants vaccinated with aP versus wP | 9 months | |
Secondary | PT specific antibody | PT-specific antibody GMC at 20 weeks and 9 months in infants vaccinated with aP versus wP following maternal vaccination with Boostrix ® Polio (GSK) or Tetanus Toxoid. | at 20 weeks and 9 months | |
Secondary | change in PT, FHA, and PRN antibody concentrations | Proportion with a 2-fold reduction in PT, FHA, and PRN antibody concentrations (measured in cord blood) from baseline at 8, 20 weeks and 9 months of age in aP versus wP primed infants following maternal immunisation with Boostrix ® Polio (GSK) or Tetanus Toxoid | at 8 and 20 weeks and at 9 months of age | |
Secondary | Pertussis antigen-specific memory B-cell | Pertussis antigen-specific memory B-cell frequencies at 8,16 weeks and 9 months of age measured by ELISpot in the aP versus wP group following maternal immunisation with aP or Boostrix ® Polio (GSK) or Tetanus Toxoid | at 8, 16 weeks and at 9 months of age | |
Secondary | Pertussis antigen-specific Th1, Th2 and Th17 responses | Pertussis antigen-specific Th1, Th2 and Th17 responses determined by flow-cytometry and cytokine analysis following antigen-specific culture (the 'Rapid T-cell assay'). | at 16 weeks of age of the infant | |
Secondary | PT, FHA and PRN-specific antibody GMC and GMR | PT, FHA and PRN-specific antibody GMC and GMR prior to immunisation (cord blood baseline) and at 8, 20 weeks and 9 months of age. | at baseline (cord blood baseline) and at 8, 20 weeks and at 9 months | |
Secondary | Hib, diphtheria, tetanus, pneumococcal and polio-specific antibody | Hib, diphtheria, tetanus, pneumococcal and polio-specific antibody concentrations | at 8, 20 weeks and 9 months | |
Secondary | Serious adverse events (SAE) in expectant mothers | Serious adverse events (SAE) in expectant mothers from enrollment at 28-34 weeks gestation up to eight weeks from the end of pregnancy. | at 28-34 weeks gestation up to eight weeks from the end of pregnancy. | |
Secondary | local and systemic reactogenicity | Proportion of mothers 28-34 weeks gestation with local and systemic reactogenicity within the first three days of aP administration | within first 3 days of aP administration | |
Secondary | PT specific antibody | PT-specific antibody GMC 9 months post delivery | at 9 months post delivery |
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