Growth and metabolic outcome in adolescents born preterm (GROWMORE): follow-up protocol for the Newcastle preterm birth growth study (PTBGS)

BACKGROUND: Preterm infants represent up to 10% of births worldwide and have an increased risk of adverse metabolic outcomes in later life. Early life exposures are key factors in determining later health but current lifestyle factors such as diet and physical activity are also extremely important a...

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Autores principales: Wood, Claire L, Tinnion, Robert J, Korada, S Murthy, Cheetham, Timothy D, Relton, Caroline L, Cooke, Richard J, Pearce, Mark S, Hollingsworth, Kieren G, Trenell, Michael I, Embleton, Nicholas D
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Study Protocol
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3898006/
https://www.ncbi.nlm.nih.gov/pubmed/24359608
http://dx.doi.org/10.1186/1471-2431-13-213
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author Wood, Claire L
Tinnion, Robert J
Korada, S Murthy
Cheetham, Timothy D
Relton, Caroline L
Cooke, Richard J
Pearce, Mark S
Hollingsworth, Kieren G
Trenell, Michael I
Embleton, Nicholas D
author_facet Wood, Claire L
Tinnion, Robert J
Korada, S Murthy
Cheetham, Timothy D
Relton, Caroline L
Cooke, Richard J
Pearce, Mark S
Hollingsworth, Kieren G
Trenell, Michael I
Embleton, Nicholas D
author_sort Wood, Claire L
collection PubMed
description BACKGROUND: Preterm infants represent up to 10% of births worldwide and have an increased risk of adverse metabolic outcomes in later life. Early life exposures are key factors in determining later health but current lifestyle factors such as diet and physical activity are also extremely important and provide an opportunity for targeted intervention. METHODS/DESIGN: This current study, GROWMORE, is the fourth phase of the Newcastle Preterm Birth Growth Study (PTBGS), which was formed from two randomised controlled trials of nutrition in early life in preterm (24–34 weeks gestation) and low birthweight infants. 247 infants were recruited prior to hospital discharge. Infant follow-up included detailed measures of growth, nutritional intake, morbidities and body composition (Dual X Ray Absorptiometry, DXA) along with demographic data until 2 years corrected age. Developmental assessment was performed at 18 months corrected age, and cognitive assessment at 9–10 years of age. Growth, body composition (DXA), blood pressure and metabolic function (insulin resistance and lipid profile) were assessed at 9–13 years of age, and samples obtained for epigenetic analysis. In GROWMORE, we will follow up a representative cohort using established techniques and novel metabolic biomarkers and correlate these with current lifestyle factors including physical activity and dietary intake. We will assess auxology, body composition (BODPOD™), insulin resistance, daily activity levels using Actigraph™ software and use (31)P and (1)H magnetic resonance spectroscopy to assess mitochondrial function and intra-hepatic lipid content. DISCUSSION: The Newcastle PTBGS is a unique cohort of children born preterm in the late 1990’s. The major strengths are the high level of detail of early nutritional and growth exposures, and the comprehensive assessment over time. This study aims to examine the associations between early life exposures in preterm infants and metabolic outcomes in adolescence, which represents an area of major translational importance.
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spelling pubmed-38980062014-01-23 Growth and metabolic outcome in adolescents born preterm (GROWMORE): follow-up protocol for the Newcastle preterm birth growth study (PTBGS) Wood, Claire L Tinnion, Robert J Korada, S Murthy Cheetham, Timothy D Relton, Caroline L Cooke, Richard J Pearce, Mark S Hollingsworth, Kieren G Trenell, Michael I Embleton, Nicholas D BMC Pediatr Study Protocol BACKGROUND: Preterm infants represent up to 10% of births worldwide and have an increased risk of adverse metabolic outcomes in later life. Early life exposures are key factors in determining later health but current lifestyle factors such as diet and physical activity are also extremely important and provide an opportunity for targeted intervention. METHODS/DESIGN: This current study, GROWMORE, is the fourth phase of the Newcastle Preterm Birth Growth Study (PTBGS), which was formed from two randomised controlled trials of nutrition in early life in preterm (24–34 weeks gestation) and low birthweight infants. 247 infants were recruited prior to hospital discharge. Infant follow-up included detailed measures of growth, nutritional intake, morbidities and body composition (Dual X Ray Absorptiometry, DXA) along with demographic data until 2 years corrected age. Developmental assessment was performed at 18 months corrected age, and cognitive assessment at 9–10 years of age. Growth, body composition (DXA), blood pressure and metabolic function (insulin resistance and lipid profile) were assessed at 9–13 years of age, and samples obtained for epigenetic analysis. In GROWMORE, we will follow up a representative cohort using established techniques and novel metabolic biomarkers and correlate these with current lifestyle factors including physical activity and dietary intake. We will assess auxology, body composition (BODPOD™), insulin resistance, daily activity levels using Actigraph™ software and use (31)P and (1)H magnetic resonance spectroscopy to assess mitochondrial function and intra-hepatic lipid content. DISCUSSION: The Newcastle PTBGS is a unique cohort of children born preterm in the late 1990’s. The major strengths are the high level of detail of early nutritional and growth exposures, and the comprehensive assessment over time. This study aims to examine the associations between early life exposures in preterm infants and metabolic outcomes in adolescence, which represents an area of major translational importance. BioMed Central 2013-12-20 /pmc/articles/PMC3898006/ /pubmed/24359608 http://dx.doi.org/10.1186/1471-2431-13-213 Text en Copyright © 2013 Wood et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Study Protocol
Wood, Claire L
Tinnion, Robert J
Korada, S Murthy
Cheetham, Timothy D
Relton, Caroline L
Cooke, Richard J
Pearce, Mark S
Hollingsworth, Kieren G
Trenell, Michael I
Embleton, Nicholas D
Growth and metabolic outcome in adolescents born preterm (GROWMORE): follow-up protocol for the Newcastle preterm birth growth study (PTBGS)
title Growth and metabolic outcome in adolescents born preterm (GROWMORE): follow-up protocol for the Newcastle preterm birth growth study (PTBGS)
title_full Growth and metabolic outcome in adolescents born preterm (GROWMORE): follow-up protocol for the Newcastle preterm birth growth study (PTBGS)
title_fullStr Growth and metabolic outcome in adolescents born preterm (GROWMORE): follow-up protocol for the Newcastle preterm birth growth study (PTBGS)
title_full_unstemmed Growth and metabolic outcome in adolescents born preterm (GROWMORE): follow-up protocol for the Newcastle preterm birth growth study (PTBGS)
title_short Growth and metabolic outcome in adolescents born preterm (GROWMORE): follow-up protocol for the Newcastle preterm birth growth study (PTBGS)
title_sort growth and metabolic outcome in adolescents born preterm (growmore): follow-up protocol for the newcastle preterm birth growth study (ptbgs)
topic Study Protocol
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3898006/
https://www.ncbi.nlm.nih.gov/pubmed/24359608
http://dx.doi.org/10.1186/1471-2431-13-213
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