Prediction of gestational diabetes in obese pregnant women from the UK Pregnancies Better Eating and Activity (UPBEAT) pilot trial

dc.contributor.authorMaitland, R. A
dc.contributor.authorSeed, Paul
dc.contributor.authorBriley, Annette L
dc.contributor.authorHomsy, M
dc.contributor.authorThomas, S
dc.contributor.authorPasupathy, D
dc.contributor.authorRobson, Stephen
dc.contributor.authorNelson, Scott M.
dc.contributor.authorSattar, Naveed
dc.contributor.authorPoston, Lucilla
dc.date.accessioned2023-05-17T01:40:25Z
dc.date.issued2014
dc.date.updated2022-03-13T07:17:11Z
dc.description.abstractAim : To examine the prediction of gestational diabetes in obese women using routine clinical measures and measurement of biomarkers related to insulin resistance in the early second trimester. Methods : A total of 117 obese pregnant women participating in a pilot trial of a complex intervention of dietary advice and physical activity were studied. Blood samples were obtained at recruitment (15+0–17+6 weeks' gestation) and demographic, clinical history and anthropometric measures recorded. The biomarkers analysed were plasma lipids (HDL cholesterol, LDL cholesterol, triglycerides), high-sensitivity C-reactive protein, alanine transaminase, aspartate transaminase, ferritin, fructosamine, insulin, adiponectin, tissue plasminogen activator, interleukin-6, visfatin and leptin. Univariate and logistic regression analyses were performed to determine independent predictors and area under the receiver-operating curve was calculated for the model. Results : Of the 106 participants included in the analysis, 29 (27.4%) developed gestational diabetes. Participants with gestational diabetes were older (P = 0.002), more often of parity ≥ 2, had higher systolic (P = 0.02) and diastolic blood pressure (P = 0.02) and were more likely to be black (P = 0.009). Amongst the blood biomarkers measured, plasma adiponectin alone remained independently associated with gestational diabetes in adjusted models (P = 0.002). The area under the receiver-operating curve for clinical factors alone (0.760) increased significantly (area under the curve 0.834, chi-square statistic (1) = 4.00, P = 0.046) with the addition of adiponectin. Conclusions : A combination of routinely measured clinical factors and adiponectin measured in the early second trimester in obese women may provide a useful approach to the prediction of gestational diabetes. Validation in a large prospective study is required to determine the usefulness of this algorithm in clinical practice. (Clinical Trial Registry No: ISRCTN89971375)en_AU
dc.description.sponsorshipThis paper presents independent research funded by theNational Institute for Health Research (NIHR) under theProgramme Grants for Applied Research funding stream(Ref: RP-0407-10452). The views expressed are those of theauthor(s) and not necessarily those of the NHS, the NIHR orthe Department of Health. The study was also supported byGuy’s and St. Thomas’ Charity; Reg Charity 251983, the UKChief Scientist Office, the Scottish Government HealthDirectorates, Edinburgh, UK and Tommy’s Charity; RegCharity 1060508, UK.en_AU
dc.format.mimetypeapplication/pdfen_AU
dc.identifier.issn0742-3071en_AU
dc.identifier.urihttp://hdl.handle.net/1885/291098
dc.language.isoen_AUen_AU
dc.publisherBlackwell Publishing Inc.en_AU
dc.rights© 2014 The Authors. Diabetic Medicine © 2014 Diabetes UKen_AU
dc.sourceDiabetic Medicineen_AU
dc.titlePrediction of gestational diabetes in obese pregnant women from the UK Pregnancies Better Eating and Activity (UPBEAT) pilot trialen_AU
dc.typeJournal articleen_AU
local.bibliographicCitation.issue8en_AU
local.bibliographicCitation.lastpage970en_AU
local.bibliographicCitation.startpage963en_AU
local.contributor.affiliationMaitland, R. A, King's Collegeen_AU
local.contributor.affiliationSeed, Paul, King's Collegeen_AU
local.contributor.affiliationBriley, Annette L, King's Collegeen_AU
local.contributor.affiliationHomsy, M, King's Collegeen_AU
local.contributor.affiliationThomas, S, Guy’s and St. Thomas’ NHS Foundation Trusten_AU
local.contributor.affiliationPasupathy, D, King's Collegeen_AU
local.contributor.affiliationRobson, Stephen, College of Health and Medicine, ANUen_AU
local.contributor.affiliationNelson, Scott M., University of Glasgowen_AU
local.contributor.affiliationSattar, Naveed, University of Glasgowen_AU
local.contributor.affiliationPoston, Lucilla, King's Collegeen_AU
local.contributor.authoruidRobson, Stephen, u4140897en_AU
local.description.embargo2099-12-31
local.description.notesImported from ARIES. The author was affiliated with Institute of Cellular Medicine, Newcastle University, UKen_AU
local.identifier.absfor000000 - Internal ANU use onlyen_AU
local.identifier.ariespublicationU3488905xPUB23899en_AU
local.identifier.citationvolume31en_AU
local.identifier.doi10.1111/dme.12482en_AU
local.identifier.scopusID2-s2.0-84904344219
local.identifier.thomsonID000340666600012
local.publisher.urlhttps://www.wiley.com/en-gben_AU
local.type.statusPublished Versionen_AU

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