Malaria Clinical Trial
Official title:
A Phase 1 Trial of the Malaria Candidate Vaccines FP9 CS and MVA CS in Adult Gambian Men Aged 18 - 45 Years
Animal and human studies have shown that the prime-boost immunization strategy using malaria antigens expressed in plasmid or viral vectors induces strong cellular immune responses. An immunization regimen with the malaria vaccines DNA ME-TRAP followed by MVA ME-TRAP induced strong T cell responses in adults in the United Kingdom (UK) and in the Gambia but did not provide significant clinical protection against infection. The investigators assessed two new vaccines which utilize a similar immunization strategy but a different malaria antigen, a circumsporozoite (CS) protein. The entire CS protein was expressed either in a modified vaccinia virus Ankara (MVA) CS, or an attenuated fowlpox virus strain (FP9) CS.
Objectives:
The primary aim was the assessment of safety and reactogenicity of these vaccines in Gambian
adults. The secondary aim was the assessment of immunogenicity and comparison with UK adults
given the same vaccines.
Study Area:
The study was conducted in the town of Farafenni, about 200km east of the capital city,
Banjul. In this area, malaria is highly seasonal with an entomological inoculation rate
between 10-50 bites per year. This study was carried out from January to June, when the
incidence of malaria is low.
Study Population:
The study involved 32 healthy Gambian adults aged 18-45 years. Volunteers were subjected to
a thorough physical and medical examination. Exclusion criteria included a low PCV (< 30%);
raised plasma creatinine or ALT levels; and HIV positivity, as determined by ELISA assays.
Study Procedure:
After prior consultations with community leaders, public meetings were held to inform the
community of the planned study. Volunteers aged 18-45 years were then invited to take part
in the study after written informed consent was obtained in the presence of the principal
investigator. Prior to the start of the screening exercise, the investigators checked the
age and identity of each volunteer and conducted pre-HIV test counselling. Screening
involved a thorough physical examination, blood sampling for haematological (full blood
count, packed cell volume [PCV]), renal (plasma creatinine) and hepatic (alanine
aminotransferase) tests and HIV 1 and 2 testing by ELISA. All eligible volunteers were
issued unique study numbers and photo identification cards.
The initial part of the study was designed to determine the dose and safety of the
individual vaccines using an open-label dose escalation method. Study volunteers were
randomly allocated to two groups of four that received 5 x 10^7 pfu id of either FP9 CS or
MVA CS. When a good safety profile was evident one week after this dose, another set of four
volunteers per group received a higher dose (1 x 10^8 pfu id) of FP9 CS or MVA CS. After the
investigators had achieved a satisfactory safety profile with a higher dose of both vaccines
given alone, they proceeded to administer the vaccines in combination using the heterologous
prime-boost regime. The vaccines were administered at 4-week intervals. Eight volunteers
received FP9 CS at week 0 followed by MVA CS at week 4 (FM group). Another set of 8
volunteers received FP9 CS at weeks 0 and 4, followed by MVA CS at week 8 (FFM). Following
vaccination, volunteers were observed for 1 hour and given a course of antipyretic
(paracetamol) to take if required. A physician and a study nurse could be contacted by the
volunteers at anytime during the course of the study. In addition, home visits were made by
field workers on days 1, 2, 7 and 28, after each vaccination, to record adverse events using
a standard questionnaire.
Sample Size:
Sample size was determined by the requirement to make a preliminary evaluation of
inter-group and inter-individual variability, to avoid excessive risk and to allow for a
realistic workload. Statistical significance may not be reached in this study with low
power, but a non-significant finding would provide justification for the need for a study
with greater power.
Data Safety Monitoring Board (DSMB):
An international DSMB was established to monitor the conduct of the trial and to approve the
analytical plan. The trial was conducted in line with the ICH Good Clinical Practices
guidelines and with the Medical Research Council (MRC) rules and regulations for the conduct
of clinical trials.
;
Allocation: Non-Randomized, Endpoint Classification: Safety Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Prevention
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