Measles Clinical Trial
Official title:
Trial of Two-Dose Standard Measles Vaccination Schedule: Long-Term Impact on Morbidity and Mortality of a Two-Dose Vaccination Schedule at 6 and 9 Months of Age Compared With a Standard Regimen of One Dose at 9 Months of Age
The general objectives of the proposed research work are:
A1) to reduce childhood mortality in developing countries through better control of measles
infection by finding the best immunization strategy, and A2) to investigate the hypothesis
that standard titre measles immunization is associated with non targeted beneficial effects
on childhood morbidity and mortality in developing countries.
The measurable, specific objectives of the present proposal are:
B1) to examine whether a two-dose strategy for measles immunization at 6 and 9 months of age
can reduce measles incidence by 50% through better coverage or improved seroconversion, and
B2) to examine whether a two-dose strategy for measles immunization at 6 and 9 months of age
can reduce childhood mortality by 20% through better coverage, better protection against
measles or non targeted beneficial effects, and B3) to determine the magnitude and duration
of non-measles related changes in morbidity patterns after standard titre measles
immunization, in particular to test whether measles immunization is associated with a 15%
reduction in the risk of diarrhoea, and B4) to determine non-measles related immunological
changes among recipients of measles vaccine in order to establish possible pathways for the
non targeted effects of standard titre measles immunization.
Background. Measles is the major killer among vaccine preventable diseases with an estimated
one million deaths/year in developing countries. Though a good vaccine exists, the current
immunization strategy of one dose at 9 months is far from optimal; too many children get
measles before the age of immunization, coverage is too low when immunization has to wait
until 9 months of age, and the protective efficacy is insufficient with the current vaccine
given at 9 months of age. There is therefore a need for alternative immunization strategies
or new vaccines.
Evaluations of vaccines have usually been based on a disease specific perspective; i.e.
evaluation of specific immunity, and protective efficacy against the specific disease, its
complications and mortality. However, our research from Guinea-Bissau, Senegal and
Bangladesh has indicated that measles immunization and measles infection may have
non-specific beneficial effects. The present protocol is an attempt to assess the magnitude
and possible mechanisms of the non targeted beneficial effects of measles immunization and
measles infection as well as an attempt to assess some of the practical implications of the
hypothesis about non-specific beneficial effects.
Approach and methodologies. We tested a two dose measles immunization strategy at 6 and 9
months compared with the currently recommended strategy of one dose at 9 months. The
children were be randomized to receive measles immunization at 6 and 9 months of age or
inactivated polio at 6 months and measles at 9 months of age.
The non targeted effects of measles immunization on mortality and morbidity are best studied
within a randomized trial comparing immunized and unimmunized children. In order to study
the impact on non-measles related morbidity, some children recruited for the immunization
trial will be included in weekly morbidity surveillance for diarrhoea, respiratory
infections and malaria which are the most important disease complexes for childhood
mortality in Guinea-Bissau.
Possible immunological differences between measles immunized and unimmunized children will
be examined through measurements of T-lymphocyte levels, neopterin, beta2-microglobulin,
delayed hypersensitivity (Multitest), allergic reactions (skin prick tests), antibody
responses to other antigens (tetanus) and thymus growth (by sonography). Functional
differences will be tested by response to a second vaccine antigen (HBV) at 7½ and 9 months
of age when only one group has received measles vaccine.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention
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