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3. Bump2Baby and Me: protocol for a randomised trial of mHealth coaching for healthy gestational weight gain and improved postnatal outcomes in high-risk women and their children

Author

O’Reilly, Sharleen L., Burden, Christy, Campoy, Cristina, McAuliffe, Fionnuala M., Teede, Helena, Andresen, Jesper, Campbell, Karen J., Geraghty, Aisling A., Harrison, Cheryce L., Laws, Rachel, Norman, Jane E., Maindal, Helle T., Vrangbæk, Karsten, Segurado, Ricardo, Versace, Vincent L., and Skinner, Timothy C.

Published
2021
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4. C-STICH2: emergency cervical cerclage to prevent miscarriage and preterm birth—study protocol for a randomised controlled trial

Author

Hodgetts-Morton, Victoria, Hewitt, Catherine A., Jones, Laura, Leighton, Lisa, Pilarski, Nicole, Molloy, Eleanor, Hinshaw, Kim, Norman, Jane, Waugh, Jason, Stock, Sarah, Thornton, Jim, Toozs-Hobson, Philip, Johnston, Tracey, Coomarasamy, Arri, Thangaratinam, Shakila, Mol, Ben, Pajkrt, Eva, Marlow, Neil, Roberts, Tracy, Middleton, Lee, Brocklehurst, Peter, and Morris, Katie

Published
2021
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6. Bump2Baby and Me: protocol for a randomised trial of mHealth coaching for healthy gestational weight gain and improved postnatal outcomes in high-risk women and their children.

Author

O'Reilly, Sharleen L., Burden, Christy, Campoy, Cristina, McAuliffe, Fionnuala M., Teede, Helena, Andresen, Jesper, Campbell, Karen J., Geraghty, Aisling A., Harrison, Cheryce L., Laws, Rachel, Norman, Jane E., Maindal, Helle T., Vrangbæk, Karsten, Segurado, Ricardo, Versace, Vincent L., Skinner, Timothy C., and IMPACT DIABETES B2B Collaboration Group

Subjects
GESTATIONAL diabetes, WEIGHT gain, COACHING psychology, MOBILE health, MULTIMEDIA messaging, PREGNANCY outcomes, TYPE 2 diabetes, RESEARCH, CLINICAL trials, MEDICAL cooperation, PREGNANCY complications, RESEARCH funding, TELEMEDICINE
Abstract

Background: Gestational diabetes (GDM) impacts 8-18% of pregnancies and greatly increases both maternal and child risk of developing non-communicable diseases such as type 2 diabetes and obesity. Whilst lifestyle interventions in pregnancy and postpartum reduce this risk, a research translation gap remains around delivering implementable interventions with adequate population penetration and participation. Impact Diabetes Bump2Baby is an implementation project of an evidence-based system of care for the prevention of overweight and obesity. Bump2Baby and Me is the multicentre randomised controlled trial investigating the effectiveness of a mHealth coaching programme in pregnancy and postpartum for women at high risk of developing GDM.Methods: Eight hundred women will be recruited in early pregnancy from 4 clinical sites within Ireland, the UK, Spain, and Australia. Women will be screened for eligibility using the validated Monash GDM screening tool. Participants will be enrolled from 12 to 24 weeks' gestation and randomised on a 1:1 basis into the intervention or control arm. Alongside usual care, the intervention involves mHealth coaching via a smartphone application, which uses a combination of synchronous and asynchronous video and text messaging, and allows for personalised support and goal setting with a trained health coach. The control arm receives usual care. All women and their children will be followed from early pregnancy until 12 months postpartum. The primary outcome will be a difference in maternal body mass index (BMI) of 0.8 kg/m2 at 12 months postpartum. Secondary maternal and infant outcomes include the development of GDM, gestational weight gain, pregnancy outcomes, improvements in diet, physical activity, sleep, and neonatal weight and infant growth patterns. The 5-year project is funded by the EU Commission Horizon 2020 and the Australian National Health and Medical Research Council. Ethical approval has been received.Discussion: Previous interventions have not moved beyond tightly controlled efficacy trials into routine service delivery. This project aims to provide evidence-based, sustainable support that could be incorporated into usual care for women during pregnancy and postpartum. This study will contribute evidence to inform the early prevention of non-communicable diseases like obesity and diabetes in mothers and the next generation.Trial Registration: Australian New Zealand Clinical Trials Registry ACTRN12620001240932 . Registered on 19 November 2020. [ABSTRACT FROM AUTHOR]

Published
2021
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7. Glibenclamide and metfoRmin versus stAndard care in gEstational diabeteS (GRACES): a feasibility open label randomised trial.

Author

Reynolds, Rebecca M., Denison, Fiona C., Juszczak, Ed, Bell, Jennifer L., Penneycard, Jessica, Strachan, Mark W. J., Lindsay, Robert S., Alexander, Claire I., Love, Corinne D. B., Whyte, Sonia, Mackenzie, Fiona, Stenson, Ben, and Norman, Jane E.

Subjects
GESTATIONAL diabetes, GLIBENCLAMIDE, METFORMIN, HYPERGLYCEMIA, GLYCEMIC control, RANDOMIZED controlled trials, THERAPEUTICS, HYPOGLYCEMIC sulfonylureas, INSULIN therapy, HYPOGLYCEMIC agents, BLOOD sugar, COMBINATION drug therapy, COMPARATIVE studies, DRUGS, RESEARCH methodology, MEDICAL cooperation, PATIENT compliance, RESEARCH, PILOT projects, EVALUATION research, PATIENT selection
Abstract

Background: Metformin is widely used to treat gestational diabetes (GDM), but many women remain hyperglycaemic and require additional therapy. We aimed to determine recruitment rate and participant throughput in a randomised trial of glibenclamide compared with standard therapy insulin (added to maximum tolerated metformin) for treatment of GDM.Methods: We conducted an open label feasibility study in 5 UK antenatal clinics among pregnant women 16 to 36 weeks' gestation with metformin-treated GDM. Women failing to achieve adequate glycaemic control on metformin monotherapy were randomised to additional glibenclamide or insulin. The primary outcome was recruitment rate. We explored feasibility with uptake, retention, adherence, safety, glycaemic control, participant satisfaction and clinical outcomes.Results: Records of 197 women were screened and 23 women randomised to metformin and glibenclamide (n = 13) or metformin and insulin (n = 10). Mean (SD) recruitment rate was 0.39 (0.62) women/centre/month. 9/13 (69.2%, 95%CI 38.6-90.9%) women adhered to glibenclamide and all provided outcome data (100% retention). There were no episodes of severe hypoglycaemia, but metformin and insulin gave superior glycaemic control to metformin and glibenclamide, with fewer blood glucose readings <3.5 mmol/l (median [IQR] difference/woman/week of treatment 0.58 [0.03-1.87]).Conclusions: A large randomised controlled trial comparing glibenclamide or insulin in combination with metformin for women with GDM would be feasible but is unlikely to be worthwhile, given the poorer glycaemic control with glibenclamide and metformin in this pilot study. The combination of metformin and glibenclamide should be reserved for women with GDM with true needle phobia or inability to use insulin therapy.Trial Registration: www.clinicaltrials.gov registration number:NCT02080377 February 11th 2014. [ABSTRACT FROM AUTHOR]

Published
2017
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8. Sedentary behaviours during pregnancy: a systematic review.

Author

Fazzi, Caterina, Saunders, David H., Linton, Kathryn, Norman, Jane E., and Reynolds, Rebecca M.

Subjects
ACCELEROMETERS, BEHAVIOR modification, BIRTH weight, C-reactive protein, CINAHL database, HEALTH, HEALTH behavior, INFORMATION storage & retrieval systems, MEDICAL information storage & retrieval systems, LOW density lipoproteins, EVALUATION of medical care, MEDLINE, PREGNANCY complications, THIRD trimester of pregnancy, PRENATAL care, QUESTIONNAIRES, RESEARCH funding, RISK assessment, SPORTS, WEIGHT gain, SYSTEMATIC reviews, BIBLIOGRAPHIC databases, DISEASE prevalence, SEDENTARY lifestyles, PHYSICAL activity, PREGNANCY
Abstract

Background: In the general population, at least 50% of time awake is spent in sedentary behaviours. Sedentary behaviours are activities that expend less energy than 1.5 metabolic equivalents, such as sitting. The amount of time spent in sedentary behaviours is a risk factor for diseases such as type 2 diabetes, cardiovascular disease, and death from all causes. Even individuals meeting physical activity guidelines are at a higher risk of premature death and adverse metabolic outcomes if they sit for extended intervals. The associations between sedentary behaviour with type 2 diabetes and with impaired glucose tolerance are stronger for women than for men. It is not known whether sedentary behaviour in pregnancy influences pregnancy outcomes, but if those negative outcomes observed in general adult population also occur in pregnancy, this could have implications for adverse outcomes for mothers and offspring. We aimed to determine the proportion of time spent in sedentary behaviours among pregnant women, and the association of sedentary behaviour with pregnancy outcomes in mothers and offspring. Methods: Two researchers independently performed the literature search using 5 different electronic bibliographic databases. Studies were included if sedentary behaviours were assessed during pregnancy. Two reviewers independently assessed the articles for quality and bias, and extracted the relevant information. Results: We identified 26 studies meeting the inclusion criteria. Pregnant women spent more than 50% of their time in sedentary behaviours. Increased time in sedentary behaviour was significantly associated with higher levels of C Reactive Protein and LDL Cholesterol, and a larger newborn abdominal circumference. Sedentary behaviours were significantly higher among women who delivered macrosomic infants. Discrepancies were found in associations of sedentary behaviour with gestational weight gain, hypertensive disorders, and birth weight. No consistent associations were found between sedentary behaviour and other variables such as gestational diabetes. There was considerable variability in study design and methods of assessing sedentary behaviour. Conclusions: Our review highlights the significant time spent in sedentary behaviour during pregnancy, and that sedentary behaviour may impact on pregnancy outcomes for both mother and child. The considerable heterogeneity in the literature suggests future studies should use robust methodology for quantifying sedentary behaviour. [ABSTRACT FROM AUTHOR]

Published
2017
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9. The role of therapeutic optimism in recruitment to a clinical trial in a peripartum setting: balancing hope and uncertainty.

Author

Hallowell, Nina, Snowdon, Claire, Morrow, Susan, Norman, Jane E., Denison, Fiona C., and Lawton, Julia

Subjects
CLINICAL trials, PERIPARTUM cardiomyopathy, EXERCISE therapy, NITROGLYCERIN, MEDICAL care, CHILDBIRTH, EXPERIMENTAL design, UNCERTAINTY, QUALITATIVE research, PATIENT selection
Abstract

Background: Hope has therapeutic value because it enables people to cope with uncertainty about their future health. Indeed, hope, or therapeutic optimism (TO), is seen as an essential aspect of the provision and experience of medical care. The role of TO in clinical research has been briefly discussed, but the concept, and whether it can be transferred from care to research and from patients to clinicians, has not been fully investigated. The role played by TO in research emerged during interviews with staff involved in a peripartum trial. This paper unpacks the concept of TO in this setting and considers the role it may play in the wider delivery of clinical trials.Methods: The Got-it trial is a UK-based, randomised placebo-controlled trial that investigates the use of sublingual glyceryl trinitrate (GTN) spray to treat retained placenta. Qualitative data were collected in open-ended interviews with obstetricians, research and clinical midwives (n =27) involved in trial recruitment. Data were analysed using the method of constant comparison.Results: TO influenced staff engagement with Got-it at different points in the trial and in different ways. Prior knowledge of, and familiarity with, GTN meant that from the outset staff perceived the trial as low risk. TO facilitated staff involvement in the trial; staff who already understood GTN's effects were optimistic that it would work, and staff collaborated because they hoped that the trial would address what they identified as an important clinical need. TO could fluctuate over the course of the trial, and was sustained or undermined by unofficial observation of clinical outcomes and speculations about treatment allocation. Thus, TO appeared to be influenced by key situational factors: prior knowledge and experience, clinical need and observed participant outcomes.Conclusions: Situational TO plays a role in facilitating staff engagement with clinical research. TO may affect trial recruitment by enabling staff to sustain the levels of uncertainty, or individual equipoise, necessary to collaborate with research while also responding to patients' clinical needs. Staff may benefit from training to deal with fluctuations in TO.Trial Registration: ISCRTN88609453 . Registered on 26 March 2014. [ABSTRACT FROM AUTHOR]

Published
2016
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10. Recruiting and consenting into a peripartum trial in an emergency setting: a qualitative study of the experiences and views of women and healthcare professionals.

Author

Lawton, Julia, Snowdon, Claire, Morrow, Susan, Norman, Jane E., Denison, Fiona C., and Hallowell, Nina

Subjects
CLINICAL trials, PERIPARTUM cardiomyopathy, PREGNANCY complications, PATIENT-professional relations, PATIENT participation, ATTITUDE (Psychology), COMPARATIVE studies, DECISION making, EMERGENCY medical services, HEALTH attitudes, INFORMED consent (Medical law), INTERVIEWING, LABOR complications (Obstetrics), RESEARCH methodology, MEDICAL cooperation, MEDICAL personnel, SENSORY perception, PLACENTA diseases, READABILITY (Literary style), RESEARCH, STATISTICAL sampling, QUALITATIVE research, PILOT projects, EVALUATION research, RANDOMIZED controlled trials, BLIND experiment, PATIENT selection, PSYCHOLOGY of human research subjects, DIAGNOSIS
Abstract

Background: Recruiting and consenting women to peripartum trials can be challenging as the women concerned may be anxious, in pain, and exhausted; there may also be limited time for discussion and decision-making to occur. To address these potential difficulties, we undertook a qualitative evaluation of the internal pilot of a trial (Got-it) involving women who had a retained placenta (RP). We explored the experiences and views of women and staff about the information and consent pathway used within the pilot, in order to provide recommendations for use in future peripartum trials involving recruitment in emergency situations.Methods: In-depth interviews were undertaken with staff (n = 27) and participating women (n = 22). Interviews were analysed thematically. The accounts of women and staff were compared to identify differences and similarities in their views about recruitment and consent procedures.Results: Women and staff regarded recruitment as having been straightforward and facilitated by the use of simplified (verbal and written) summaries of trial information. Both parties, however, conveyed discordant views about whether fully informed consent had been obtained. These differences in perspectives appeared to arise from the different factors and considerations impinging on women and staff at the time of recruitment. While staff placed emphasis on promoting understanding in the emergency situation of RP by imparting information in clear and succinct ways, women highlighted the experiential realities of their pre- and post-birthing situations, and how these had led to quick decisions being made without full engagement with the potential risks of trial participation. To facilitate informed consent, women suggested that trial information should be given during the antenatal period, and, in doing so, articulated a rights-based discourse. Staff, however, voiced opposition to this approach by emphasising a duty of care to all pregnant women, and raising concerns about causing undue distress to the majority of individuals who would not subsequently develop a RP.Conclusions: By drawing upon the perspectives of women and staff involved in the same trial we have shown that they may operate within different experiential and ethical paradigms. In doing so, we argue for the potential benefits of drawing upon multiple perspectives when developing information and consent pathways used in future (peripartum) trials.Trial Registration: ISCRTN 88609453 . [ABSTRACT FROM AUTHOR]

Published
2016
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11. Post-weaning diet determines metabolic risk in mice exposed to overnutrition in early life.

Author

King, Vicky, Norman, Jane E., Seckl, Jonathan R., and Drake, Amanda J.

Subjects
*METABOLIC disorders, *ANIMAL weaning, *ANIMAL nutrition, *MATERNAL health, *OBESITY treatment
Abstract

Background: Maternal overnutrition during pregnancy is associated with an increased risk of obesity and cardiometabolic disease in the offspring; a phenomenon attributed to 'developmental programming'. The post-weaning development of obesity may associate with exacerbation of the programmed metabolic phenotype. In mice, we have previously shown that exposure to maternal overnutrition causes increased weight gain in offspring before weaning, but exerts no persistent effects on weight or glucose tolerance in adulthood. In order to determine whether post-weaning exposure to a cafeteria diet might lead to an exacerbation of programmed effects, offspring born and raised by mothers on control (CON) or cafeteria (DIO) diets were transferred onto either CON or DIO diets at weaning. Findings: Post-weaning DIO caused the development of obesity, with hyperglycaemia and hyperinsulinaemia in males; and obesity with hyperinsulinaemia in females and with increased cholesterol levels in both sexes. Exposure to maternal overnutrition during pregnancy and lactation caused only subtle additional effects on offspring phenotype. Conclusions: These results suggest that post-weaning exposure to a high-fat high-sugar diet has a more profound effect on offspring weight gain and glucose tolerance than exposure to maternal overnutrition. These data emphasise the importance of optimising early life nutrition in offspring of both obese and lean mothers. [ABSTRACT FROM AUTHOR]

Published
2014
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12. Trial protocol OPPTIMUM-- Does progesterone prophylaxis for the prevention of preterm labour improve outcome?

Author

Norman, Jane E., Shennan, Andrew, Bennett, Phillip, Thornton, Steven, Robson, Stephen, Marlow, Neil, Norrie, John, Petrou, Stavros, Sebire, Neil, Lavender, Tina, and Whyte, Sonia

Subjects
*PREMATURE labor, *PREMATURE infants, *OVARIES, *PROGESTERONE, *CONCEPTION
Abstract

Background: Preterm birth is a global problem, with a prevalence of 8 to 12% depending on location.. Several large trials and systematic reviews have shown progestogens to be effective in preventing or delaying preterm birth in selected high risk women with a singleton pregnancy (including those with a short cervix or previous preterm birth). Although an improvement in short term neonatal outcomes has been shown in some trials these have not consistently been confirmed in meta-analyses. Additionally data on longer term outcomes is limited to a single trial where no difference in outcomes was demonstrated at four years of age of the child, despite those in the "progesterone" group having a lower incidence of preterm birth. Methods/Design: The OPPTIMUM study is a double blind randomized placebo controlled trial to determine whether progesterone prophylaxis to prevent preterm birth has long term neonatal or infant benefit. Specifically it will study whether, in women with singleton pregnancy and at high risk of preterm labour, prophylactic vaginal natural progesterone, 200 mg daily from 22 - 34 weeks gestation, compared to placebo, improves obstetric outcome by lengthening pregnancy thus reducing the incidence of preterm delivery (before 34 weeks), improves neonatal outcome by reducing a composite of death and major morbidity, and leads to improved childhood cognitive and neurosensory outcomes at two years of age. Recruitment began in 2009 and is scheduled to close in Spring 2013. As of May 2012, over 800 women had been randomized in 60 sites. Discussion: OPPTIMUM will provide further evidence on the effectiveness of vaginal progesterone for prevention of preterm birth and improvement of neonatal outcomes in selected groups of women with singleton pregnancy at high risk of preterm birth. Additionally it will determine whether any reduction in the incidence of preterm birth is accompanied by improved childhood outcome. Trial registration: ISRCTN14568373 [ABSTRACT FROM AUTHOR]

Published
2012
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13. Inflammatory pathways in the mechanism of parturition.

Author

Norman, Jane E., Bollapragada, Shrikant, Mei Yuan, and Nelson, Scott M.

Subjects
*PARTURITION, *REPRODUCTION, *LABOR complications (Obstetrics), *PREGNANCY, *CHILDBIRTH
Abstract

Increasing evidence suggests that parturition is an inflammatory process. In this brief overview, inflammatory events occurring in association with parturition, and the mechanism by which they may contribute to labour and delivery will be discussed. Mention will be made of how this information may be of use in regulating the timing and the onset of parturition. [ABSTRACT FROM AUTHOR]

Published
2007
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14. IMOP: randomised placebo controlled trial of outpatient cervical ripening with isosorbide mononitrate (IMN) prior to induction of labour -- clinical trial with analyses of efficacy, cost effectiveness and acceptability.

Author

Bollapragada, Shrikant, Mackenzie, Fiona, Norrie, John, Petrou, Stavros, Reid, Margaret, Greer, Ian, Osman, Inass, and Norman, Jane E.

Subjects
CLINICAL medicine, PLACEBOS, MEDICAL care costs, BEHAVIORAL medicine, MEDICAL experimentation on humans, MEDICAL research
Abstract

Background: There is increasing interest in carrying out pre-induction cervical ripening on an outpatient basis. However, there are concerns about the use of prostaglandins, the agents commonly used in hospital settings for this indication, because prostaglandins induce uterine contractions that may lead to fetal hypoxia. Indeed, in a recent study we demonstrated abnormalities in 9% of fetal heart rate tracings performed following prostaglandin induced cervical ripening at term. In contrast, we confirmed in the same study that isosorbide mononitrate (IMN) (administered on an inpatient basis) was both effective in inducing cervical ripening at term, and was associated with no associated fetal heart rate abnormalities. Methods/design: The aim of this study is to determine whether IMN self administered by women on an outpatient basis improves the process of induction of labour. Specifically, we hypothesise that the use of outpatient IMN will result in a shorter inpatient stay before delivery, decreased costs to the health service and greater maternal satisfaction with ripening and induction of labour, compared with placebo treatment. In the study described here (the "IMOP" study), women scheduled for induction of labour at term, and who require pre-induction cervical ripening will be randomised to self-administer at home either IMN 40 mg, or a placebo, each vaginally, at 48 hours, 32 hours and 16 hours before scheduled hospital admission. After admission to hospital, treatment will revert to the usual induction of labour protocol. We will compare the primary outcomes of the elapsed time interval from hospital admission to vaginal delivery, the costs to the health service of induction of labour, and women's experience of induction of labour in the two groups. Discussion: This trial will provide evidence on the efficacy of outpatient IMN for pre-induction cervical ripening at term. We will study a formulation of IMN which is cheap and widely available. If the treatment is effective, acceptable to women, and cost effective, it could be implemented into obstetric practice worldwide. Trial registration: The trial has been registered on the International Standard Randomised Controlled Trial Number Register (ISRCTN) and given the registration number ISRTN39772441. [ABSTRACT FROM AUTHOR]

Published
2006
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15. Progestogens to prevent preterm birth in twin pregnancies: an individual participant data meta-analysis of randomized trials.

Author

Schuit, Ewoud, Stock, Sarah, Groenwold, Rolf H H, Maurel, Kimberly, Combs, C Andrew, Garite, Thomas, Spong, Cathy Y, Thom, Elizabeth A, Rouse, Dwight J, Caritis, Steve N, Saade, George R, Zachary, Julia M, Norman, Jane E, Rode, Line, Klein, Katharina, Tabor, Ann, Cetingöz, Elçin, Morrison, John C, Magann, Everett F, and Briery, Christian M

Abstract

Background: Preterm birth is the principal factor contributing to adverse outcomes in multiple pregnancies. Randomized controlled trials of progestogens to prevent preterm birth in twin pregnancies have shown no clear benefits. However, individual studies have not had sufficient power to evaluate potential benefits in women at particular high risk of early delivery (for example, women with a previous preterm birth or short cervix) or to determine adverse effects for rare outcomes such as intrauterine death.Methods/design: We propose an individual participant data meta-analysis of high quality randomized, double-blind, placebo-controlled trials of progestogen treatment in women with a twin pregnancy. The primary outcome will be adverse perinatal outcome (a composite measure of perinatal mortality and significant neonatal morbidity). Missing data will be imputed within each original study, before data of the individual studies are pooled. The effects of 17-hydroxyprogesterone caproate or vaginal progesterone treatment in women with twin pregnancies will be estimated by means of a random effects log-binomial model. Analyses will be adjusted for variables used in stratified randomization as appropriate. Pre-specified subgroup analysis will be performed to explore the effect of progestogen treatment in high-risk groups.Discussion: Combining individual patient data from different randomized trials has potential to provide valuable, clinically useful information regarding the benefits and potential harms of progestogens in women with twin pregnancy overall and in relevant subgroups. [ABSTRACT FROM AUTHOR]

Published
2012
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16. External validation of prognostic models predicting pre-eclampsia: individual participant data meta-analysis.

Author

Snell KIE, Allotey J, Smuk M, Hooper R, Chan C, Ahmed A, Chappell LC, Von Dadelszen P, Green M, Kenny L, Khalil A, Khan KS, Mol BW, Myers J, Poston L, Thilaganathan B, Staff AC, Smith GCS, Ganzevoort W, Laivuori H, Odibo AO, Arenas Ramírez J, Kingdom J, Daskalakis G, Farrar D, Baschat AA, Seed PT, Prefumo F, da Silva Costa F, Groen H, Audibert F, Masse J, Skråstad RB, Salvesen KÅ, Haavaldsen C, Nagata C, Rumbold AR, Heinonen S, Askie LM, Smits LJM, Vinter CA, Magnus P, Eero K, Villa PM, Jenum AK, Andersen LB, Norman JE, Ohkuchi A, Eskild A, Bhattacharya S, McAuliffe FM, Galindo A, Herraiz I, Carbillon L, Klipstein-Grobusch K, Yeo SA, Browne JL, Moons KGM, Riley RD, and Thangaratinam S

Subjects
Female, Humans, Pregnancy, Prognosis, Reproducibility of Results, Research Design, Risk Assessment, Pre-Eclampsia diagnosis, Pregnancy Complications diagnosis
Abstract

Background: Pre-eclampsia is a leading cause of maternal and perinatal mortality and morbidity. Early identification of women at risk during pregnancy is required to plan management. Although there are many published prediction models for pre-eclampsia, few have been validated in external data. Our objective was to externally validate published prediction models for pre-eclampsia using individual participant data (IPD) from UK studies, to evaluate whether any of the models can accurately predict the condition when used within the UK healthcare setting., Methods: IPD from 11 UK cohort studies (217,415 pregnant women) within the International Prediction of Pregnancy Complications (IPPIC) pre-eclampsia network contributed to external validation of published prediction models, identified by systematic review. Cohorts that measured all predictor variables in at least one of the identified models and reported pre-eclampsia as an outcome were included for validation. We reported the model predictive performance as discrimination (C-statistic), calibration (calibration plots, calibration slope, calibration-in-the-large), and net benefit. Performance measures were estimated separately in each available study and then, where possible, combined across studies in a random-effects meta-analysis., Results: Of 131 published models, 67 provided the full model equation and 24 could be validated in 11 UK cohorts. Most of the models showed modest discrimination with summary C-statistics between 0.6 and 0.7. The calibration of the predicted compared to observed risk was generally poor for most models with observed calibration slopes less than 1, indicating that predictions were generally too extreme, although confidence intervals were wide. There was large between-study heterogeneity in each model's calibration-in-the-large, suggesting poor calibration of the predicted overall risk across populations. In a subset of models, the net benefit of using the models to inform clinical decisions appeared small and limited to probability thresholds between 5 and 7%., Conclusions: The evaluated models had modest predictive performance, with key limitations such as poor calibration (likely due to overfitting in the original development datasets), substantial heterogeneity, and small net benefit across settings. The evidence to support the use of these prediction models for pre-eclampsia in clinical decision-making is limited. Any models that we could not validate should be examined in terms of their predictive performance, net benefit, and heterogeneity across multiple UK settings before consideration for use in practice., Trial Registration: PROSPERO ID: CRD42015029349 .

Published
2020
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