Cohort profile: the MUNICH Preterm and Term Clinical study (MUNICH-PreTCl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidity

Purpose The MUNICH Preterm and Term Clinical (MUNICH-PreTCl) birth cohort was established to uncover pathological processes contributing to infant/childhood morbidity and mortality. We collected comprehensive medical information of healthy and sick newborns and their families, together with infant b...

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Main Authors: Orsolya Genzel-Boroviczeny, Matthias Mann, Susanne Pangratz-Fuehrer, Robin Eisenburger, Janne Scharpenack, Philipp E Geyer, Johannes B Müller-Reif, Nadja van Hagen, Alina M Müller, Majken Karoline Jensen, Christoph Klein, Claudia Nussbaum, Wolfgang Bodensohn
Format: Article
Language:English
Published: BMJ Publishing Group 2021-06-01
Series:BMJ Open
Online Access:https://bmjopen.bmj.com/content/11/6/e050652.full
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author Orsolya Genzel-Boroviczeny
Matthias Mann
Susanne Pangratz-Fuehrer
Robin Eisenburger
Janne Scharpenack
Philipp E Geyer
Johannes B Müller-Reif
Nadja van Hagen
Alina M Müller
Majken Karoline Jensen
Christoph Klein
Claudia Nussbaum
Wolfgang Bodensohn
spellingShingle Orsolya Genzel-Boroviczeny
Matthias Mann
Susanne Pangratz-Fuehrer
Robin Eisenburger
Janne Scharpenack
Philipp E Geyer
Johannes B Müller-Reif
Nadja van Hagen
Alina M Müller
Majken Karoline Jensen
Christoph Klein
Claudia Nussbaum
Wolfgang Bodensohn
Cohort profile: the MUNICH Preterm and Term Clinical study (MUNICH-PreTCl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidity
BMJ Open
author_facet Orsolya Genzel-Boroviczeny
Matthias Mann
Susanne Pangratz-Fuehrer
Robin Eisenburger
Janne Scharpenack
Philipp E Geyer
Johannes B Müller-Reif
Nadja van Hagen
Alina M Müller
Majken Karoline Jensen
Christoph Klein
Claudia Nussbaum
Wolfgang Bodensohn
author_sort Orsolya Genzel-Boroviczeny
title Cohort profile: the MUNICH Preterm and Term Clinical study (MUNICH-PreTCl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidity
title_short Cohort profile: the MUNICH Preterm and Term Clinical study (MUNICH-PreTCl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidity
title_full Cohort profile: the MUNICH Preterm and Term Clinical study (MUNICH-PreTCl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidity
title_fullStr Cohort profile: the MUNICH Preterm and Term Clinical study (MUNICH-PreTCl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidity
title_full_unstemmed Cohort profile: the MUNICH Preterm and Term Clinical study (MUNICH-PreTCl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidity
title_sort cohort profile: the munich preterm and term clinical study (munich-pretcl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidity
publisher BMJ Publishing Group
series BMJ Open
issn 2044-6055
publishDate 2021-06-01
description Purpose The MUNICH Preterm and Term Clinical (MUNICH-PreTCl) birth cohort was established to uncover pathological processes contributing to infant/childhood morbidity and mortality. We collected comprehensive medical information of healthy and sick newborns and their families, together with infant blood samples for proteomic analysis. MUNICH-PreTCl aims to identify mechanism-based biomarkers in infant health and disease to deliver more precise diagnostic and predictive information for disease prevention. We particularly focused on risk factors for pregnancy complications, family history of genetically influenced health conditions such as diabetes and paediatric long-term health—all to be further monitored and correlated with proteomics data in the future.Participants Newborns and their parents were recruited from the Perinatal Center at the LMU University Hospital, Munich, between February 2017 and June 2019. Infants without congenital anomalies, delivered at 23–41 weeks of gestation, were eligible.Findings Findings to date concern the clinical data and extensive personal patient information. A total of 662 infants were recruited, 44% were female (36% in preterm, 46% in term). 90% of approached families agreed to participate. Neonates were grouped according to gestational age: extremely preterm (<28 weeks, N=28), very preterm (28 to <32 weeks, N=36), late preterm (32 to <37 weeks, N=97) and term infants (>37+0 weeks, N=501). We collected over 450 data points per child–parent set, (family history, demographics, pregnancy, birth and daily follow-ups throughout hospitalisation) and 841 blood samples longitudinally. The completion rates for medical examinations and blood samples were 100% and 95% for the questionnaire.Future plans The correlation of large clinical datasets with proteomic phenotypes, together with the use of medical registries, will enable future investigations aiming to decipher mechanisms of disorders in a systems biology perspective.Trial registration number DRKS (00024189); Pre-results.
url https://bmjopen.bmj.com/content/11/6/e050652.full
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spelling doaj-920aff25a9ee45c5a4f781ef8f9d6a2b2021-08-07T17:02:58ZengBMJ Publishing GroupBMJ Open2044-60552021-06-0111610.1136/bmjopen-2021-050652Cohort profile: the MUNICH Preterm and Term Clinical study (MUNICH-PreTCl), a neonatal birth cohort with focus on prenatal and postnatal determinants of infant and childhood morbidityOrsolya Genzel-Boroviczeny0Matthias Mann1Susanne Pangratz-Fuehrer2Robin Eisenburger3Janne Scharpenack4Philipp E Geyer5Johannes B Müller-Reif6Nadja van Hagen7Alina M Müller8Majken Karoline Jensen9Christoph Klein10Claudia Nussbaum11Wolfgang Bodensohn12Division of Neonatology Innenstadt, Department of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyProteomics and Signaltransduction, Max-Planck-Institute of Biochemistry, Martinsried, GermanyDivision of Neonatology Innenstadt, Department of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyDivision of Neonatology Innenstadt, Department of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyDivision of Neonatology Innenstadt, Department of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyProteomics and Signaltransduction, Max-Planck-Institute of Biochemistry, Martinsried, GermanyProteomics and Signaltransduction, Max-Planck-Institute of Biochemistry, Martinsried, GermanyDivision of Neonatology Innenstadt, Department of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyDivision of Neonatology Innenstadt, Department of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyNutrition and Epidemiology, Harvard University T H Chan School of Public Health, Boston, Massachusetts, USADepartment of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyDivision of Neonatology Innenstadt, Department of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyDivision of Neonatology Innenstadt, Department of Pediatrics, Dr von Hauner Children’s Hospital, University Hospital, LMU, Munich, GermanyPurpose The MUNICH Preterm and Term Clinical (MUNICH-PreTCl) birth cohort was established to uncover pathological processes contributing to infant/childhood morbidity and mortality. We collected comprehensive medical information of healthy and sick newborns and their families, together with infant blood samples for proteomic analysis. MUNICH-PreTCl aims to identify mechanism-based biomarkers in infant health and disease to deliver more precise diagnostic and predictive information for disease prevention. We particularly focused on risk factors for pregnancy complications, family history of genetically influenced health conditions such as diabetes and paediatric long-term health—all to be further monitored and correlated with proteomics data in the future.Participants Newborns and their parents were recruited from the Perinatal Center at the LMU University Hospital, Munich, between February 2017 and June 2019. Infants without congenital anomalies, delivered at 23–41 weeks of gestation, were eligible.Findings Findings to date concern the clinical data and extensive personal patient information. A total of 662 infants were recruited, 44% were female (36% in preterm, 46% in term). 90% of approached families agreed to participate. Neonates were grouped according to gestational age: extremely preterm (<28 weeks, N=28), very preterm (28 to <32 weeks, N=36), late preterm (32 to <37 weeks, N=97) and term infants (>37+0 weeks, N=501). We collected over 450 data points per child–parent set, (family history, demographics, pregnancy, birth and daily follow-ups throughout hospitalisation) and 841 blood samples longitudinally. The completion rates for medical examinations and blood samples were 100% and 95% for the questionnaire.Future plans The correlation of large clinical datasets with proteomic phenotypes, together with the use of medical registries, will enable future investigations aiming to decipher mechanisms of disorders in a systems biology perspective.Trial registration number DRKS (00024189); Pre-results.https://bmjopen.bmj.com/content/11/6/e050652.full