Use of biomarkers of sub-clinical infection, nutrition and neonatal maturity to interpret plasma retinol in Nigerian neonates

Use of biomarkers of sub-clinical infection, nutrition and neonatal maturity to interpret plasma retinol in Nigerian neonates

Using the World Health Organization criterion, the prevalence of sub-clinical vitamin A deficiency can be assessed using plasma retinol concentrations <0·7 μmol/l. However, plasma retinol can be depressed by infection; thus, the use of this criterion alone may overestimate deficiency. In the pres...

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Bibliographic Details
Published in:British journal of nutrition Vol. 90; no. 2; pp. 353 - 361
Main Authors: Adelekan, Delana A., Northrop-Clewes, Christine A., Owa, Joshua A., Oyedeji, Adesola O., Owoeye, Adedayo A., Thurnham, David I.
Format: Journal Article
Language:English
Published: Cambridge, UK Cambridge University Press 01-08-2003
Subjects:
Acids
Acute-phase proteins
alpha 1-Antichymotrypsin - blood
alpha-Tocopherol - blood
Babies
Biological and medical sciences
Biomarkers
Biomarkers - blood
Birth Weight
Body Weight
Carotenoids
Carotenoids - blood
Gestational Age
Glycoproteins
Humans
Infant, Newborn
Infection - blood
Infections
Lutein
Lutein - blood
Medical sciences
Metabolic diseases
Neonate
Neonates
Nigeria
Nutrition research
Nutritional Status - physiology
Orosomucoid - analysis
Other nutritional diseases (malnutrition, nutritional and vitamin deficiencies...)
Pediatrics
Plasma
Proteins
Public health
Retinol
Tropical medicine
Vitamin A
Vitamin A - blood
Vitamin A Deficiency - blood
Vitamin A Deficiency - diagnosis
α1-Acid glycoprotein
α1-Antichymotrypsin
Nigeria
Africa
South Africa
United Kingdom > UK
Northern Ireland
Neonate
Acute-phase proteins
α1-Antichymotrypsin
α1-Acid glycoprotein
Lutein
Nigeria
Retinol
Human
Prevalence
Retinol: Lutein: Acute-phase proteins: α1-Antichymotrypsin: α1-Acid glycoprotein: Nigeria: Neonate
Estimation
Nutrition disorder
Vitamin
Biological marker
Vitamin deficiency
Infant
Feeding
Infection
Acute phase protein
Newborn
α1-acid-Glycoprotein
Nutritional status
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Summary:Using the World Health Organization criterion, the prevalence of sub-clinical vitamin A deficiency can be assessed using plasma retinol concentrations <0·7 μmol/l. However, plasma retinol can be depressed by infection; thus, the use of this criterion alone may overestimate deficiency. In the present study, we investigated the usefulness of the acute-phase proteins (APP) α1-antichymotrypsin (ACT) and α1-acid glycoprotein (AGP), plasma carotenoids and anthropometric and gestational indices to interpret plasma retinol in the blood of 192 apparently healthy Nigerian neonates collected randomly during days 1–20 postpartum. The mean weight (2·64 kg) and length (0·458 m) of the neonates and plasma concentrations (geometric mean, μmol/l) of retinol (0·54), α-carotene (0·072), ß-carotene (0·076) and lutein (0·080) were low. The prevalence of vitamin A deficiency was 72 %, indicating a severe public health problem. Babies who were of low birth weight (P<0·003) or premature and low birth weight (P<0·023) had significantly lower retinol concentrations than full-term normal weight babies. Thirty-two neonates had abnormal ACT and forty-four abnormal AGP concentrations. Positive correlations between retinol and ACT (r 0·186, P=0·05) and AGP (r 0·31, P=0·0001) during days 1–5 may be due to the increasing plasma retinol from maternal milk and a coincidental increasing capacity to synthesise APP. Subsequently, negative correlations between retinol and ACT (r −0·28, P=0·02) and AGP (r −0·29, P=0·018) from day 6 onwards reflected the continuing increase in plasma retinol, but no further increase in the APP. Overall, weight, ACT, lutein and age explained 30 % of the variance in retinol, but lutein was the most significant (r2 0·18, P<0·0001). Hence, the distribution of plasma retinol concentrations in this group of neonates was more strongly linked with nutrition (via the surrogate marker lutein) than infection.
Bibliography:istex:E6761ED0BD450629AC6438F5AABB177BC683B21D
ArticleID:00135
PII:S0007114503001351
ark:/67375/6GQ-PMCLPJJB-T
ObjectType-Article-1
SourceType-Scholarly Journals-1
ObjectType-Feature-2
content type line 23
ISSN:0007-1145
1475-2662
DOI:10.1079/BJN2003907