Malaria Clinical Trial
Official title:
Randomized, Controlled, Dose Escalation Phase Ib Trial of MSP 3 LSP Adjuvanted in Aluminium Hydroxide Versus Hepatitis Bin 12 to 24 Month Old Children in Burkina Faso.
This will be a study of the safety of MSP 3 LSP candidate malaria vaccine in children aged 1-2 years in Burkina Faso. Three imminizations at 28 day intervals will be administratered subcuteneously on the shoulder region. The study will compare MSP3 with Engerix B vaccine to evaluate whether it is just as safe to give to children in malaria endemic country. The study will also evaluate whether the vaccine induces the expected immune responses. Two dose levels of MSP 3 will be evaluated; 15µg and 30µg to determine the one with the best safety and immune response profile.
The study is a single centre randomized controlled and blinded study (observer blind). It
will be conducted at the CNRFP Vaccinology unit located in Balonghin. Children in the
catchments area within the 1-2 years age group, whose parents consent will be screened to
randomise 45 eligible participants. Two MSP 3 dose levels will be evaluated; 15µg and 30µg.
The study will start with immunizing older children with the lowest dose observing safety
parameters closely, then proceed to to the higher dose with a two week of observation apart.
Clinical, biological and immune response data gathered after vaccination with 15µg and 30µg
MSP 3 LSP will be compared to:
- The children's baseline data before vaccinations, and
- The post vaccination data of children in the control group.
Randomization will ensure that the comparison groups are similar in relevant characteristics
at baseline. The concealment of allocation before enrolment will further enforce the
randomisation. Individuals who will make the assessment of the study end points will be
completely blinded of the vaccine administered. This will ensure that there is no observer
bias. Further, reporting or information bias will be minimised, because the recipients will
also not be aware of which vaccine they have been administered. This is possible because the
selected control vaccine has not been in routine use in this area, and has only now been
recommended by the Ministry of Health. Cross over immunisation at the end of the trial will
involve only those children who will received the study vaccine; they will be administered
the control vaccine in the interest of public health benefits for them.
The schedule of vaccination at 0, 1 and 2 months has been adopted because it is suitable for
the target group. The idea is to eventually deploy the vaccine through the expanded
programme on immunisation should the vaccine become registered for public use. For the EPI
age group, it is not only an efficient delivery mechanism, but they are also the most
vulnerable group to malaria.
In brief, the groups will be allocated as follows:
- Group 1: 23 participants (15 receiving MSP-3 vaccine 15 µg and 8 receiving Hepatitis B
vaccine).
- Group 2: 22 participants (15 receiving MSP-3 vaccine 30 µg and 7 receiving Hepatitis B
vaccine)
Immunization schedule will be 0, 1, and 2 months for all cohorts and provisionally as
following for each group:
Study days 0, 28 and 56 for group 1; and Study days 14, 42, 70 for group 2 Vaccinations of
groups 1 and 2 will be staggered: immunization in group 2 will start 2 weeks after group 1.
This interval may be extended if deemed necessary due to SAEs or other safety
concerns.Randomization will be done for each group at the times of first vaccinations.Route
of inoculation will be by subcutaneous injection into right or left deltoid (alternately).
Each child will be observed for at least 60 minutes after vaccination to evaluate and treat
any acute adverse events (AEs). Study duration will be approximately 13 months per
participant. There will be a seven (7) day follow-up period for solicited adverse events
(day of vaccination plus 6 subsequent days); and twenty eight (28) day follow-up period for
unsolicited adverse events (Vaccination day plus 27 subsequent days). The follow-up for
serious adverse events (SAE's) will be for 12 months following the first dose of study
vaccine (9 months after dose 3).
At the end of the follow-up period for unsolicited AEs (i.e., one month after the third
dose), participants will be followed by field workers at home at monthly intervals to record
SAEs. For data collection, conventional paper Case Report Forms (in triplicate copies) will
be used.
An interim analysis is foreseen after day 84 of follow up. At this stage decision will be
considered whether to proceed to a phase 2b study or not, and with which dosage of MSP 3,
based on the safety and immunogenicity profile.
;
Allocation: Randomized, Endpoint Classification: Safety Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Prevention
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