Mechanisms Affecting the Gut of Preterm Infants in Enteral Feeding Trials

Nicholas D. Embleton; Janet E. Berrington; Jon Dorling; Andrew K. Ewer; Edmund Juszczak; John A. Kirby; Christopher A. Lamb; Clare V. Lanyon; William McGuire; Christopher S. Probert; Stephen P. Rushton; Mark D. Shirley; Christopher J. Stewart; Stephen P. Cummings

doi:10.3389/fnut.2017.00014

Mechanisms Affecting the Gut of Preterm Infants in Enteral Feeding Trials

Nicholas D. Embleton, Janet E. Berrington, Jon Dorling, Andrew K. Ewer, Edmund Juszczak, John A. Kirby, Christopher A. Lamb, Clare V. Lanyon, William McGuire, Christopher S. Probert, Stephen P. Rushton, Mark D. Shirley, Christopher J. Stewart, Stephen P. Cummings

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53 Citas (Scopus)

Resumen

Large randomized controlled trials (RCTs) in preterm infants offer unique opportunities for mechanistic evaluation of the risk factors leading to serious diseases, as well as the actions of interventions designed to prevent them. Necrotizing enterocolitis (NEC) a serious inflammatory gut condition and late-onset sepsis (LOS) are common feeding and nutrition-related problems that may cause death or serious long-term morbidity and are key outcomes in two current UK National Institutes for Health Research (NIHR) trials. Speed of increasing milk feeds trial (SIFT) randomized preterm infants to different rates of increases in milk feeds with a primary outcome of survival without disability at 2 years corrected age. Enteral lactoferrin in neonates (ELFIN) randomizes infants to supplemental enteral lactoferrin or placebo with a primary outcome of LOS. This is a protocol for the mechanisms affecting the gut of preterm infants in enteral feeding trials (MAGPIE) study and is funded by the UK NIHR Efficacy and Mechanistic Evaluation programme. MAGPIE will recruit ~480 preterm infants who were enrolled in SIFT or ELFIN. Participation in MAGPIE does not change the main trial protocols and uses non-invasive sampling of stool and urine, along with any residual resected gut tissue if infants required surgery. Trial interventions may involve effects on gut microbes, metabolites (e.g., short-chain fatty acids), and aspects of host immune function. Current hypotheses suggest that NEC and/or LOS are due to a dysregulated immune system in the context of gut dysbiosis, but mechanisms have not been systematically studied within large RCTs. Microbiomic analysis will use next-generation sequencing, and metabolites will be assessed by mass spectrometry to detect volatile organic and other compounds produced by microbes or the host. We will explore differences between disease cases and controls, as well as exploring the actions of trial interventions. Impacts of this research are multiple: translation of knowledge of mechanisms promoting gut health may explain outcomes or suggest alternate strategies to improve health. Results may identify new non-invasive diagnostic or monitoring techniques, preventative or treatment strategies for NEC or LOS, or provide data useful for risk stratification in future studies. Mechanistic evaluation might be especially informative where there are not clear effects on the primary outcome (ISRCTN 12554594).

Idioma original	English
Número de artículo	14
Publicación	Frontiers in Nutrition
Volumen	4
DOI	https://doi.org/10.3389/fnut.2017.00014
Estado	Published - may. 8 2017
Publicado de forma externa	Sí

Nota bibliográfica

Funding Information:
We gratefully acknowledge the support of parents who have contributed toward the design and conduct of our research studies, and the participation of their infants in our research. We are also indebted to the many nurses, doctors, and other health professionals who help facilitate and recruit infants at individual sites, the support of NHS pathology teams, the Local Clinical Research Network and NIHR, and the research team members who have helped establish MAGPIE including Julie Groombridge, Tom Skeath, and Stefan Zalewski. We are grateful to the R&D Department at Newcastle Hospitals NHS Foundation Trust www.newcastle-hospitals.org.uk/and the Joint Research Office Newcastle University (Susan Ridge, Philip Mawson, Aaron Jackson, Layla McMullen, Nicola Brown, Andrew Johnston, and many others) for providing guidance and sponsorship for the study.

Funding Information:
SIFT and ELFIN are funded by the Health Technology Assessment programme of the UK NIHR. MAGPIE is funded by the Efficacy and Mechanistic Evaluation Programme (EME) of the UK NIHR (Project Reference Number 13/122/02).

Publisher Copyright:
© Copyright © 2017 Embleton, Berrington, Dorling, Ewer, Juszczak, Kirby, Lamb, Lanyon, McGuire, Probert, Rushton, Shirley, Stewart and Cummings.

ASJC Scopus Subject Areas

Food Science
Endocrinology, Diabetes and Metabolism
Nutrition and Dietetics

ODS de las Naciones Unidas

Este resultado contribuye a los siguientes Objetivos de Desarrollo Sostenible

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10.3389/fnut.2017.00014

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Embleton, N. D., Berrington, J. E., Dorling, J., Ewer, A. K., Juszczak, E., Kirby, J. A., Lamb, C. A., Lanyon, C. V., McGuire, W., Probert, C. S., Rushton, S. P., Shirley, M. D., Stewart, C. J., & Cummings, S. P. (2017). Mechanisms Affecting the Gut of Preterm Infants in Enteral Feeding Trials. Frontiers in Nutrition, 4, Artículo 14. https://doi.org/10.3389/fnut.2017.00014

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title = "Mechanisms Affecting the Gut of Preterm Infants in Enteral Feeding Trials",

abstract = "Large randomized controlled trials (RCTs) in preterm infants offer unique opportunities for mechanistic evaluation of the risk factors leading to serious diseases, as well as the actions of interventions designed to prevent them. Necrotizing enterocolitis (NEC) a serious inflammatory gut condition and late-onset sepsis (LOS) are common feeding and nutrition-related problems that may cause death or serious long-term morbidity and are key outcomes in two current UK National Institutes for Health Research (NIHR) trials. Speed of increasing milk feeds trial (SIFT) randomized preterm infants to different rates of increases in milk feeds with a primary outcome of survival without disability at 2 years corrected age. Enteral lactoferrin in neonates (ELFIN) randomizes infants to supplemental enteral lactoferrin or placebo with a primary outcome of LOS. This is a protocol for the mechanisms affecting the gut of preterm infants in enteral feeding trials (MAGPIE) study and is funded by the UK NIHR Efficacy and Mechanistic Evaluation programme. MAGPIE will recruit ~480 preterm infants who were enrolled in SIFT or ELFIN. Participation in MAGPIE does not change the main trial protocols and uses non-invasive sampling of stool and urine, along with any residual resected gut tissue if infants required surgery. Trial interventions may involve effects on gut microbes, metabolites (e.g., short-chain fatty acids), and aspects of host immune function. Current hypotheses suggest that NEC and/or LOS are due to a dysregulated immune system in the context of gut dysbiosis, but mechanisms have not been systematically studied within large RCTs. Microbiomic analysis will use next-generation sequencing, and metabolites will be assessed by mass spectrometry to detect volatile organic and other compounds produced by microbes or the host. We will explore differences between disease cases and controls, as well as exploring the actions of trial interventions. Impacts of this research are multiple: translation of knowledge of mechanisms promoting gut health may explain outcomes or suggest alternate strategies to improve health. Results may identify new non-invasive diagnostic or monitoring techniques, preventative or treatment strategies for NEC or LOS, or provide data useful for risk stratification in future studies. Mechanistic evaluation might be especially informative where there are not clear effects on the primary outcome (ISRCTN 12554594).",

author = "Embleton, {Nicholas D.} and Berrington, {Janet E.} and Jon Dorling and Ewer, {Andrew K.} and Edmund Juszczak and Kirby, {John A.} and Lamb, {Christopher A.} and Lanyon, {Clare V.} and William McGuire and Probert, {Christopher S.} and Rushton, {Stephen P.} and Shirley, {Mark D.} and Stewart, {Christopher J.} and Cummings, {Stephen P.}",

note = "Funding Information: We gratefully acknowledge the support of parents who have contributed toward the design and conduct of our research studies, and the participation of their infants in our research. We are also indebted to the many nurses, doctors, and other health professionals who help facilitate and recruit infants at individual sites, the support of NHS pathology teams, the Local Clinical Research Network and NIHR, and the research team members who have helped establish MAGPIE including Julie Groombridge, Tom Skeath, and Stefan Zalewski. We are grateful to the R&D Department at Newcastle Hospitals NHS Foundation Trust www.newcastle-hospitals.org.uk/and the Joint Research Office Newcastle University (Susan Ridge, Philip Mawson, Aaron Jackson, Layla McMullen, Nicola Brown, Andrew Johnston, and many others) for providing guidance and sponsorship for the study. Funding Information: SIFT and ELFIN are funded by the Health Technology Assessment programme of the UK NIHR. MAGPIE is funded by the Efficacy and Mechanistic Evaluation Programme (EME) of the UK NIHR (Project Reference Number 13/122/02). Publisher Copyright: {\textcopyright} Copyright {\textcopyright} 2017 Embleton, Berrington, Dorling, Ewer, Juszczak, Kirby, Lamb, Lanyon, McGuire, Probert, Rushton, Shirley, Stewart and Cummings.",

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AU - Embleton, Nicholas D.

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AU - Dorling, Jon

AU - Ewer, Andrew K.

AU - Juszczak, Edmund

AU - Kirby, John A.

AU - Lamb, Christopher A.

AU - Lanyon, Clare V.

AU - McGuire, William

AU - Probert, Christopher S.

AU - Rushton, Stephen P.

AU - Shirley, Mark D.

AU - Stewart, Christopher J.

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N1 - Funding Information: We gratefully acknowledge the support of parents who have contributed toward the design and conduct of our research studies, and the participation of their infants in our research. We are also indebted to the many nurses, doctors, and other health professionals who help facilitate and recruit infants at individual sites, the support of NHS pathology teams, the Local Clinical Research Network and NIHR, and the research team members who have helped establish MAGPIE including Julie Groombridge, Tom Skeath, and Stefan Zalewski. We are grateful to the R&D Department at Newcastle Hospitals NHS Foundation Trust www.newcastle-hospitals.org.uk/and the Joint Research Office Newcastle University (Susan Ridge, Philip Mawson, Aaron Jackson, Layla McMullen, Nicola Brown, Andrew Johnston, and many others) for providing guidance and sponsorship for the study. Funding Information: SIFT and ELFIN are funded by the Health Technology Assessment programme of the UK NIHR. MAGPIE is funded by the Efficacy and Mechanistic Evaluation Programme (EME) of the UK NIHR (Project Reference Number 13/122/02). Publisher Copyright: © Copyright © 2017 Embleton, Berrington, Dorling, Ewer, Juszczak, Kirby, Lamb, Lanyon, McGuire, Probert, Rushton, Shirley, Stewart and Cummings.

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N2 - Large randomized controlled trials (RCTs) in preterm infants offer unique opportunities for mechanistic evaluation of the risk factors leading to serious diseases, as well as the actions of interventions designed to prevent them. Necrotizing enterocolitis (NEC) a serious inflammatory gut condition and late-onset sepsis (LOS) are common feeding and nutrition-related problems that may cause death or serious long-term morbidity and are key outcomes in two current UK National Institutes for Health Research (NIHR) trials. Speed of increasing milk feeds trial (SIFT) randomized preterm infants to different rates of increases in milk feeds with a primary outcome of survival without disability at 2 years corrected age. Enteral lactoferrin in neonates (ELFIN) randomizes infants to supplemental enteral lactoferrin or placebo with a primary outcome of LOS. This is a protocol for the mechanisms affecting the gut of preterm infants in enteral feeding trials (MAGPIE) study and is funded by the UK NIHR Efficacy and Mechanistic Evaluation programme. MAGPIE will recruit ~480 preterm infants who were enrolled in SIFT or ELFIN. Participation in MAGPIE does not change the main trial protocols and uses non-invasive sampling of stool and urine, along with any residual resected gut tissue if infants required surgery. Trial interventions may involve effects on gut microbes, metabolites (e.g., short-chain fatty acids), and aspects of host immune function. Current hypotheses suggest that NEC and/or LOS are due to a dysregulated immune system in the context of gut dysbiosis, but mechanisms have not been systematically studied within large RCTs. Microbiomic analysis will use next-generation sequencing, and metabolites will be assessed by mass spectrometry to detect volatile organic and other compounds produced by microbes or the host. We will explore differences between disease cases and controls, as well as exploring the actions of trial interventions. Impacts of this research are multiple: translation of knowledge of mechanisms promoting gut health may explain outcomes or suggest alternate strategies to improve health. Results may identify new non-invasive diagnostic or monitoring techniques, preventative or treatment strategies for NEC or LOS, or provide data useful for risk stratification in future studies. Mechanistic evaluation might be especially informative where there are not clear effects on the primary outcome (ISRCTN 12554594).

AB - Large randomized controlled trials (RCTs) in preterm infants offer unique opportunities for mechanistic evaluation of the risk factors leading to serious diseases, as well as the actions of interventions designed to prevent them. Necrotizing enterocolitis (NEC) a serious inflammatory gut condition and late-onset sepsis (LOS) are common feeding and nutrition-related problems that may cause death or serious long-term morbidity and are key outcomes in two current UK National Institutes for Health Research (NIHR) trials. Speed of increasing milk feeds trial (SIFT) randomized preterm infants to different rates of increases in milk feeds with a primary outcome of survival without disability at 2 years corrected age. Enteral lactoferrin in neonates (ELFIN) randomizes infants to supplemental enteral lactoferrin or placebo with a primary outcome of LOS. This is a protocol for the mechanisms affecting the gut of preterm infants in enteral feeding trials (MAGPIE) study and is funded by the UK NIHR Efficacy and Mechanistic Evaluation programme. MAGPIE will recruit ~480 preterm infants who were enrolled in SIFT or ELFIN. Participation in MAGPIE does not change the main trial protocols and uses non-invasive sampling of stool and urine, along with any residual resected gut tissue if infants required surgery. Trial interventions may involve effects on gut microbes, metabolites (e.g., short-chain fatty acids), and aspects of host immune function. Current hypotheses suggest that NEC and/or LOS are due to a dysregulated immune system in the context of gut dysbiosis, but mechanisms have not been systematically studied within large RCTs. Microbiomic analysis will use next-generation sequencing, and metabolites will be assessed by mass spectrometry to detect volatile organic and other compounds produced by microbes or the host. We will explore differences between disease cases and controls, as well as exploring the actions of trial interventions. Impacts of this research are multiple: translation of knowledge of mechanisms promoting gut health may explain outcomes or suggest alternate strategies to improve health. Results may identify new non-invasive diagnostic or monitoring techniques, preventative or treatment strategies for NEC or LOS, or provide data useful for risk stratification in future studies. Mechanistic evaluation might be especially informative where there are not clear effects on the primary outcome (ISRCTN 12554594).

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Mechanisms Affecting the Gut of Preterm Infants in Enteral Feeding Trials

Resumen

Nota bibliográfica

ASJC Scopus Subject Areas

ODS de las Naciones Unidas

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