Anemia Clinical Trial
Official title:
The Non-specific Effects of Vaccination Related to Mortality and Morbidity in Nanoro Health and Demographic Surveillance System Cohort
It has long been recognized that the positive effects of vaccination on childhood mortality
cannot be solely attributed to a decline in the disease targeted by the vaccine. These
so-called non-specific effects of vaccination have so far mostly been linked to mortality.
However, it has been suggested that non-specific effects may also effect morbidity and
nutritional status. This study aims to further explore the correlation between vaccination,
susceptibility to infectious diseases (particularly malaria and bacterial infections),
nutritional status and immunity.
With this prospective cross sectional study among healthy individuals in rural west-Africa we
aim to address several research questions at the same time. This study will assess the
influence of (time-point of) vaccination on morbidity, mortality and immune status among
healthy individuals in a rural sub-Saharan African setting. Secondly, to explore the
prevalence of subclinical malaria, iron deficiency anemia, sickle cell anemia and thallasemia
among a healthy rural sub-Saharan African population. And finally to assess normal
hemocytometry values among a healthy rural sub-Saharan African population.
A cross sectional study among healthy participants randomly selected from the population
living in the Nanoro HDSS cohort to (a) study the relation between vaccination and morbidity
(including hemoglobin levels, subclinical malaria and stunting) (b) perform hemocytometry in
order to determine reference values for that population and estimate the prevalence and
causes of anemia, using reference values from other Sub-Sahara Africa countries and
industrialized countries.
In a cross sectional study among a healthy population in the Nanoro HDSS cohort,
hemocytometry will be performed in order to define normal values for that population. In
addition, hemoglobin levels can be related to the presence of iron deficiency, thalassemia
and malaria and be corrected for important confounding factors, such as the family income,
family composition, distance to a healthcare center and vaccination status. This study will
allow to assess simultaneously the normal range of hemoglobin values, the prevalence of
(different causes of) anemia, the prevalence of subclinical malaria parasitemia, as well as
the influence of (timepoint of) vaccination on all these issues. It is hypothized that early
vaccination with live attenuated vaccines has a protective effect against malaria and other
severe infectious diseases and will result in a better nutritional status, a higher
hemoglobin level and a higher threshold of subclinical parasitemia. The protective effect of
early vaccination with live attenuated vaccines may be due to the long-term modulation of the
immune system through epigenetic changes causing a right balance between the pro- and
anti-inflammatory responses. Such balance can be determined by ex-vivo stimulation of whole
blood by a variety of stimuli, including Mycobacterium tuberculosis and lipopolysaccharide
from Escherichia coli, followed by measurement of ex vivo cytokine production. Previous
studies among healthy volunteers in the Netherlands have shown that BCG is indeed capable to
induce epigenetic changes and influence immune response by influencing various pathways
including through genetic variations in mTOR, HK2, PFKP, GLS, and GLUD1/2 (ref).
The new Sysmex analysers are not only capable to determine hemocytometry, but are at the same
time capable to detect malaria parasites directly. Interestingly, not only the asexual stages
of the parasites are detected but the gametocytes as well. This may be very important as
gametocyte carriers are known to play a crucial role in malaria transmission. Gametocytes are
presently detected by light microscopy or by PCR, however these techniques are limited; the
sensitivity of light microscopy is relatively low and PCR is too complex to perform in most
rural sub-Saharan African settings. The new Sysmex hematology analysers are easy to operate
at low costs and may as such become an important tool for malaria elimination programs. No
data are presently available about gametocyte density in Burkina Faso in a large population,
nor is the lower level of detection of gametocytes using the sysmex analyzers known.
This research has four main objectives :
1. To perform hemocytometry among a healthy rural Burkina Faso population selected from the
Nanoro HDSS cohort, in order to determine reference values for that population.
2. To perform hemocytometry among a healthy rural Burkina Faso population selected from the
Nanoro HDSS cohort, in order to estimate the prevalence and causes of anemia, using
reference values from other Sub-Sahara Africa (SSA) countries and industrialized
countries.
3. To study the relation between (timepoint of) vaccination and morbidity (including
hemoglobin levels, subclinical malaria, bacterial infection and stunting) among a
healthy rural Burkina Faso population selected from the Nanoro HDSS cohort. For this
objective the population will be stratified by birth cohort.
4. To perform ex-vivo whole blood stimulation to assess differences in immune response
between patientgroups with a different vaccination status, within a healthy rural
Burkina Faso population selected from the Nanoro HDSS cohort
Seondary objectives
5. To assess the detection limit of gametocyte carriages for the new series Sysmex
hematology analyzers.
6. To assess if Salmonella resides in blood as a reservoir for invasive infection among a
rural Burkina Faso population selected from the Nanoro HDSS cohort.
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