Healthy Infants Clinical Trial
Official title:
Influence of Inflammation on Micronutrient Status Assessment
Inflammation can influence several biochemical measurements those commonly used to interpret micronutrient status in children. Our primary objective is to investigate the effects of inflammation on several biochemical measurements used to interpret micronutrient status in children. A total of 40 infants (9-18 mo of age) will participate in this study. Investigators will use PENTA vaccines as a means to induce controlled inflammation (closely mimic to natural infection). PENTA is a combination of five different vaccine antigens (Hepatitis B (HBV)/ Haemophilus influenza type b (Hib) / Tetanus-Diphtheria-whole cell Pertussis (TDwP)). The investigators will also use two different stable isotopic retinols for the assessment of total body vitamin A stores. Baseline blood samples (5 mL) will be obtained from all infants and then randomly selected 30 infants will receive PENTA vaccines, while the other 10 infants will receive no vaccines. 24 hours after vaccination a finger-prick blood sample will be obtained from the infants in the vaccinated group to measure CRP and on the same day, blood samples (5 mL) will be obtained from infants who develop inflammation (CRP> 5mg/L) in the vaccine group and also from infants in the control group. Thus estimated plasma micronutrients and vitamin A stores before and after inflammation will calculate the effects of inflammation on the interpretation of micronutrient deficiencies based on biochemical indicator assessment.
Background:
Subclinical micronutrient deficiencies remain a hidden aspect of malnutrition for which
comprehensive data are lacking. Defining subclinical micronutrient deficiencies requires
considering the prevalence of inflammation and its implications for the interpretation of
micronutrient deficiencies based on biochemical indicator assessment. This study will provide
a comprehensive profile of micronutrient status and antimicrobial resistance in a cohort of
young children living in the densely populated urban slum.
Hypothesis:
I. Inflammation can influence several biochemical measurements those commonly used to
interpret micronutrient status in children II. Micronutrient assessments can be performed
successfully using finger/heel prick blood samples with microsamplers, thus increasing the
ease of blood collection and reducing costs for cold storage and transport to the analytical
laboratory.
Specific Objectives:
Our primary objective is to investigate the effects of inflammation on several biochemical
measurements used to interpret micronutrient status in children. Our secondary aim is to test
the applicability of a blood spot device allowing the determination of micronutrient status
in field settings. Our exploratory objective is to make a comparative analysis of gut
antimicrobial resistance genes (AMR) and resistome profile in children.
Methods:
A total of 40 infants (9-18 mo of age) will participate in this study. In this study,
investigators will use two different stable isotopic vitamin A e.g., 13C10-retinyl acetate
and 13C4-retinyl acetate. 400 μg of these isotopes, dissolved in 0.5 mL of sunflower oil,
will be provided directly into the infant's mouth by using a direct replacement pipette.
Mothers will be asked to breastfeed their infant after oral dosing to enhance absorption of
the labeled vitamin A. Specific activity of 13C10- and 13C4- retinyl acetate in the blood
samples will be measured by liquid chromatography-tandem mass spectrometry (LC/MS/MS). On the
day of blood collection, a 24-h dietary recall and weekly morbidity questionnaires will be
used. Investigators will also use PENTA vaccines as a means to induce controlled inflammation
(closely mimic to natural infection). PENTA is a combination of five different vaccine
antigens (Hepatitis B (HBV)/ Haemophilus influenza type b (Hib) / Tetanus-Diphtheria-whole
cell Pertussis (TDwP)). This vaccination is beneficial to the infants since the World Health
Organization recommends a booster vaccination dose. At the end of the study, PENTA vaccines
will also be provided to the study infants in the "no-vaccine" group.
On day 0, all infants (n=40) will receive an oral dose of 13C10-retinyl acetate, and blood
samples (5 mL) will be taken on day 4. On day 7 all infants (n=40) will also receive another
oral dose of 13C4-retinyl acetate. 3-day later randomly selected 30 infants will receive
PENTA vaccines (day 10), while the other 10 infants will receive no vaccines. 24 hours after
vaccination a finger-prick blood sample will be obtained from the infants in the vaccinated
group to measure CRP (QuikRead go, Orion, Finland). On the same day (day 11), blood samples
(5 mL) will be obtained from infants who develop inflammation (CRP> 5mg/L) in the vaccine
group and also from infants in the control group (day 11). Thus plasma micronutrients and
vitamin A stores estimates on day 4 and day 11 will evaluate the effects of inflammation on
the plasma micronutrient status indicators and total body vitamin A store. Blood
microsamplers will be tested alongside venous blood collection to assess the feasibility of
finger/heel prick sampling. Fecal samples, local surface water, and wastewater samples will
be collected to test the prevalence of AMR resitomes in children and their environment.
Outcome measures/variables:
1. The following plasma biomarkers will be estimated before inflammation and 24 hours after
inflammation
- Inflammation markers: C-reactive protein (CRP) (mg/L) and α1-acid glycoprotein
(AGP) (g/L)
- Vitamin A status indicators: retinol (nmol/L), total body vitamin A stores (nmol),
Retinol binding protein (RBP) (mg/L) and beta-carotene (nmol/L)
- Iron status indicators: ferritin (ug/L) and soluble transferrin receptor (mg/L)
- Folate/B12 status indicators: folate (nmol/L), methylmalonic acid (umol/L) and
cobalamin (pmol/L)
- Trace element status indicators: selenium (ug/L), copper (ug/L) and thyroglobulin
(ug/L).
2. The usefulness of a microsampler device to collect blood samples for future
micronutrient assessments.
3. Assessment and contrast of AMR gene abundances and diversity to develop resistomes
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