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Cohort profile: molecular signature in pregnancy (MSP): longitudinal high-frequency sampling to characterise cross-omic trajectories in pregnancy in a resource-constrained setting
JournalArticle (Originalarbeit in einer wissenschaftlichen Zeitschrift)
 
ID 4616832
Author(s) Brummaier, Tobias; Syed Ahamed Kabeer, Basirudeen; Wilaisrisak, Pornpimon; Pimanpanarak, Mupawjay; Win, Aye Kyi; Pukrittayakamee, Sasithon; Marr, Alexandra K.; Kino, Tomoshige; Al Khodor, Souhaila; Terranegra, Annalisa; Carrara, Verena I.; Nosten, Francois; Utzinger, Jürg; Chaussabel, Damien; Paris, Daniel H.; McGready, Rose
Author(s) at UniBasel Brummaier, Tobias
Paris, Daniel Henry
Utzinger, Jürg
Year 2020
Title Cohort profile: molecular signature in pregnancy (MSP): longitudinal high-frequency sampling to characterise cross-omic trajectories in pregnancy in a resource-constrained setting
Journal BMJ open
Volume 10
Number 10
Pages / Article-Number e041631
Keywords clinical physiology; epidemiology; fetal medicine; maternal medicine; reproductive medicine
Mesh terms Adult; Female; Humans; Infant, Newborn; Pregnancy; Pregnancy Complications, epidemiology; Pregnancy Outcome, epidemiology; Pregnancy Trimester, First; Premature Birth, epidemiology; Prenatal Care; Young Adult
Abstract A successful pregnancy relies on the interplay of various biological systems. Deviations from the norm within a system or intersystemic interactions may result in pregnancy-associated complications and adverse pregnancy outcomes. Systems biology approaches provide an avenue of unbiased, in-depth phenotyping in health and disease. The molecular signature in pregnancy (MSP) cohort was established to characterise longitudinal, cross-omic trajectories in pregnant women from a resource constrained setting. Downstream analysis will focus on characterising physiological perturbations in uneventful pregnancies, pregnancy-associated complications and adverse outcomes.; First trimester pregnant women of Karen or Burman ethnicity were followed prospectively throughout pregnancy, at delivery and until 3 months post partum. Serial high-frequency sampling to assess whole blood transcriptomics and microbiome composition of the gut, vagina and oral cavity, in conjunction with assessment of gene expression and microbial colonisation of gestational tissue, was done for all cohort participants.; 381 women with live born singletons averaged 16 (IQR 15-18) antenatal visits (13 094 biological samples were collected). At 5% (19/381) the preterm birth rate was low. Other adverse events such as maternal febrile illness 7.1% (27/381), gestational diabetes 13.1% (50/381), maternal anaemia 16.3% (62/381), maternal underweight 19.2% (73/381) and a neonate born small for gestational age 20.2% (77/381) were more often observed than preterm birth.; Results from the MSP cohort will enable in-depth characterisation of cross-omic molecular trajectories in pregnancies from a population in a resource-constrained setting. Moreover, pregnancy-associated complications and unfavourable pregnancy outcomes will be investigated at the same granular level, with a particular focus on population relevant needs such as effect of tropical infections on pregnancy. More detailed knowledge on multiomic perturbations will ideally result in the development of diagnostic tools and ultimately lead to targeted interventions that may disproportionally benefit pregnant women from this resource-limited population.; NCT02797327.
ISSN/ISBN 2044-6055
edoc-URL https://edoc.unibas.ch/82064/
Full Text on edoc Available
Digital Object Identifier DOI 10.1136/bmjopen-2020-041631
PubMed ID http://www.ncbi.nlm.nih.gov/pubmed/33040018
ISI-Number WOS:000582256700038
Document type (ISI) Journal Article, Randomized Controlled Trial
 
   

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