Search

Your search keyword '"Godfrey, K.M."' showing total 187 results
Start Over Author "Godfrey, K.M."
187 results on '"Godfrey, K.M."'

2. Comparison of body composition assessment tools in infancy

Author

Lyons-Reid, J., primary, Derraik, J.G.B., additional, Albert, B.B., additional, Kenealy, T., additional, Cutfield, W.S., additional, Ward, L.C., additional, Tint, M-T., additional, Chan, S-Y., additional, Monnard, C.R., additional, Ramos Nieves, J.M., additional, and Godfrey, K.M., additional

Published
2024
Full Text
View/download PDF

5. Pregnancy vitamin D supplementation and childhood bone mass at age 4 years : findings from the Maternal Vitamin D Osteoporosis Study (MAVIDOS) randomized controlled trial

Author

Curtis, E.M., Moon, R.J., D'Angelo, S., Crozier, S.R., Bishop, N.J., Gopal‐Kothandapani, J.S., Kennedy, S.H., Papageorghiou, A.T., Fraser, R., Gandhi, S.V., Schoenmakers, I., Prentice, A., Inskip, H.M., Godfrey, K.M., Javaid, M.K., Eastell, R., Cooper, C., Harvey, N.C., Arden, N.K., Carr, A., Dennison, E.M., Clynes, M., Woolford, S.J., and Mughal, M.Z.

Abstract

In the Maternal Vitamin D Osteoporosis Study (MAVIDOS) randomized trial, vitamin D supplementation in pregnancy did not lead to greater neonatal bone mass across the trial as a whole, but, in a prespecified secondary analysis by season of birth, led to greater neonatal bone mass among winter-born babies. Demonstrating persistence of this effect into childhood would increase confidence in a long-term benefit of this intervention. We investigated whether antenatal vitamin D supplementation increases offspring bone mineralization in early childhood in a prespecified, single-center follow-up of a double-blinded, multicenter, randomized controlled clinical trial based in the UK (MAVIDOS). A total of 1123 women in early pregnancy with a baseline 25-hydroxyvitamin D level 25–100 nmol/L from three research centers (2008–2014) were randomized to 1000 IU/d cholecalciferol or matched placebo from 14 weeks of gestation to delivery. Offspring born at the Southampton, UK research center were assessed at age 4 years (2013–2018). Anthropometry and dual-energy X-ray absorptiometry (DXA) were performed (yielding whole body less head [WBLH] bone mineral content [BMC], areal bone mineral density [aBMD], bone area [BA], and body composition). Of 723 children, 564 (78.0%) children attended the 4-year visit, 452 of whom had a useable DXA. Maternal vitamin D supplementation led to greater WBLH aBMD in the children compared with placebo (mean [95% confidence interval {CI}]: supplemented group: 0.477 (95% CI, 0.472–0.481) g/cm2; placebo group: 0.470 (95% CI, 0.466–0.475) g/cm2, p = 0.048). Associations were consistent for BMC and lean mass, and in age- and sex-adjusted models. Effects were observed across the whole cohort irrespective of season of birth. Maternal-child interactions were observed, with a greater effect size among children with low milk intake and low levels of physical activity. Child weight, height, and body mass index (BMI) were similar by maternal randomization group. These findings suggest a sustained beneficial effect of maternal vitamin D supplementation in pregnancy on offspring aBMD at age 4 years, but will require replication in other trials.

Published
2022

12. Body fat in Singaporean infants: development of body fat prediction equations in Asian newborns

Author

Aris, I.M., Soh, S.E., Tint, M.T., Liang, S., Chinnadurai, A., Saw, S.M., Kwek, K., Godfrey, K.M., Gluckman, P.D., Chong, Y.S., Yap, F.K.P., and Lee, Y.S.

Subjects
Population biology -- Research, Adipose tissues -- Physiological aspects -- Health aspects, Infants (Newborn) -- Physiological aspects -- Health aspects, Food/cooking/nutrition, Health
Abstract

BACKGROUND/OBJECTIVES: Prediction equations are commonly used to estimate body fat from anthropometric measurements, but are population specific. We aimed to establish and validate a body composition prediction formula for Asian newborns, and compared the performance of this formula with that of a published equation. SUBJECTS/METHODS: Among 262 neonates (174 from day 0, 88 from days 1-3 post delivery) from a prospective cohort study, body composition was measured using air-displacement plethysmography (PEA POD), with standard anthropometric measurements, including triceps and subscapular skinfolds. Using fat mass measurement by PEA POD as a reference, stepwise linear regression was utilized to develop a prediction equation in a randomly selected subgroup of 62 infants measured on days 1-3, which was then validated in another subgroup of 200 infants measured on days 0-3. RESULTS: Regression analyses revealed subscapular skinfolds, weight, gender and gestational age were significant predictors of neonatal fat mass, explaining 81.1% of the variance, but not triceps skinfold or ethnicity. By Bland-Altman analyses, our prediction equation revealed a non-significant bias with limits of agreement (LOA) similar to those of a published equation for infants measured on days 1-3 (95% LOA: (- 0.25, 0.26) kg vs (- 0.23, 0.21) kg) and on day 0 (95% LOA: (- 0.19, 0.17) kg vs (- 0.17, 0.18) kg). The published equation, however, exhibited a systematic bias in our sample. CONCLUSIONS: Our equation requires only one skinfold site measurement, which can significantly reduce time and effort. It does not require the input of ethnicity and, thus, aid its application to other Asian neonatal populations. European Journal of Clinical Nutrition (2013) 67, 922-927;doi: 10.1038/ejcn.2013.69;published online 3 April 2013 Keywords: body composition; neonatal fat mass; prediction equation; skinfolds, INTRODUCTION Excess adiposity is a major risk factor for adverse health outcomes and chronic diseases. (1) Body fat assessment in infants is important not only as an indicator of nutritional [...]

Published
2013
Full Text
View/download PDF

13. Natural products in drug discovery: advances and opportunities

Author

Atanasov, A.G. Zotchev, S.B. Dirsch, V.M. Orhan, I.E. Banach, M. Rollinger, J.M. Barreca, D. Weckwerth, W. Bauer, R. Bayer, E.A. Majeed, M. Bishayee, A. Bochkov, V. Bonn, G.K. Braidy, N. Bucar, F. Cifuentes, A. D’Onofrio, G. Bodkin, M. Diederich, M. Dinkova-Kostova, A.T. Efferth, T. El Bairi, K. Arkells, N. Fan, T.-P. Fiebich, B.L. Freissmuth, M. Georgiev, M.I. Gibbons, S. Godfrey, K.M. Gruber, C.W. Heer, J. Huber, L.A. Ibanez, E. Kijjoa, A. Kiss, A.K. Lu, A. Macias, F.A. Miller, M.J.S. Mocan, A. Müller, R. Nicoletti, F. Perry, G. Pittalà, V. Rastrelli, L. Ristow, M. Russo, G.L. Silva, A.S. Schuster, D. Sheridan, H. Skalicka-Woźniak, K. Skaltsounis, L. Sobarzo-Sánchez, E. Bredt, D.S. Stuppner, H. Sureda, A. Tzvetkov, N.T. Vacca, R.A. Aggarwal, B.B. Battino, M. Giampieri, F. Wink, M. Wolfender, J.-L. Xiao, J. Yeung, A.W.K. Lizard, G. Popp, M.A. Heinrich, M. Berindan-Neagoe, I. Stadler, M. Daglia, M. Verpoorte, R. Supuran, C.T. the International Natural Product Sciences Taskforce

Abstract

Natural products and their structural analogues have historically made a major contribution to pharmacotherapy, especially for cancer and infectious diseases. Nevertheless, natural products also present challenges for drug discovery, such as technical barriers to screening, isolation, characterization and optimization, which contributed to a decline in their pursuit by the pharmaceutical industry from the 1990s onwards. In recent years, several technological and scientific developments — including improved analytical tools, genome mining and engineering strategies, and microbial culturing advances — are addressing such challenges and opening up new opportunities. Consequently, interest in natural products as drug leads is being revitalized, particularly for tackling antimicrobial resistance. Here, we summarize recent technological developments that are enabling natural product-based drug discovery, highlight selected applications and discuss key opportunities. © 2021, Springer Nature Limited.

Published
2021

14. Adiposity associated DNA methylation signatures in adolescents are related to leptin and perinatal factors.

Author

Huang, R.C., Melton, P.E., Burton, M.A., Beilin, L.J., Clarke-Harris, R, Cook, E, Godfrey, K.M., Burdge, G.C., Mori, T.A., Anderson, D, Rauschert, S., Craig, J. M., Kobor, M.S., MacIsaac, J.L., Morin, A.M., Oddy, W.H., Pennell, C.E., Holbrook, J.D., and Lillycrop, K.A.

Subjects
DNA methylation, LEPTIN, ADIPOKINES, METHYLATION, OBESITY, RNA-binding proteins, BODY mass index, WEIGHT gain
Abstract

Epigenetics links perinatal influences with later obesity. We identifed differentially methylated CpG (dmCpG) loci measured at 17 years associated with concurrent adiposity measures and examined whether these were associated with hsCRP, adipokines, and early life environmental factors. Genome-wide DNA methylation from 1192 Raine Study participants at 17 years, identified 29 dmCpGs (Bonferroni corrected p < 1.06E-07) associated with body mass index (BMI), 10 with waist circumference (WC) and 9 with subcutaneous fat thickness. DmCpGs within Ras Association (RalGDS/AF-6), Pleckstrin Homology Domains 1 (RAPH1), Musashi RNA-Binding Protein 2 (MSI2), and solute carrier family 25 member 10 (SLC25A10) are associated with both BMI and WC. Validation by pyrosequencing confirmed these associations and showed that MSI2 , SLC25A10 , and RAPH1 methylation was positively associated with serum leptin. These were also associated with the early environment; MSI2 methylation (β = 0.81, p = 0.0004) was associated with pregnancy maternal smoking, SLC25A10 (CpG2 β = 0.12, p = 0.002) with pre- and early pregnancy BMI, and RAPH1 (β = −1.49, p = 0.036) with gestational weight gain. Adjusting for perinatal factors, methylation of the dmCpGs within MSI2, RAPH1, and SLC25A10 independently predicted BMI, accounting for 24% of variance. MSI2 methylation was additionally associated with BMI over time (17 years old β = 0.026, p = 0.0025; 20 years old β = 0.027, p = 0.0029) and between generations (mother β = 0.044, p = 7.5e-04). Overall findings suggest that DNA methylation in MSI2, RAPH1, and SLC25A10 in blood may be robust markers, mediating through early life factors. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

15. Changes in parental smoking during pregnancy and risks of adverse birth outcomes and childhood overweight in Europe and North America: An individual participant data meta-analysis of 229,000 singleton births

Author

Philips, E.M. Santos, S. Trasande, L. Aurrekoetxea, J.J. Barros, H. von Berg, A. Bergström, A. Bird, P.K. Brescianini, S. Chaoimh, C.N. Charles, M.-A. Chatzi, L. Chevrier, C. Chrousos, G.P. Costet, N. Criswell, R. Crozier, S. Eggesbø, M. Fantini, M.P. Farchi, S. Forastiere, F. van Gelder, M.M.H.J. Georgiu, V. Godfrey, K.M. Gori, D. Hanke, W. Heude, B. Hryhorczuk, D. Iñiguez, C. Inskip, H. Karvonen, A.M. Kenny, L.C. Kull, I. Lawlor, D.A. Lehmann, I. Magnus, P. Manios, Y. Melén, E. Mommers, M. Morgen, C.S. Moschonis, G. Murray, D. Nohr, E.A. Nybo Andersen, A.-M. Oken, E. Oostvogels, A.J.J.M. Papadopoulou, E. Pekkanen, J. Pizzi, C. Polanska, K. Porta, D. Richiardi, L. Rifas-Shiman, S.L. Roeleveld, N. Rusconi, F. Santos, A.C. Sørensen, T.I.A. Standl, M. Stoltenberg, C. Sunyer, J. Thiering, E. Thijs, C. Torrent, M. Vrijkotte, T.G.M. Wright, J. Zvinchuk, O. Gaillard, R. Jaddoe, V.W.V.

Abstract

Background Fetal smoke exposure is a common and key avoidable risk factor for birth complications and seems to influence later risk of overweight. It is unclear whether this increased risk is also present if mothers smoke during the first trimester only or reduce the number of cigarettes during pregnancy, or when only fathers smoke. We aimed to assess the associations of parental smoking during pregnancy, specifically of quitting or reducing smoking and maternal and paternal smoking combined, with preterm birth, small size for gestational age, and childhood overweight. Methods and findings We performed an individual participant data meta-analysis among 229,158 families from 28 pregnancy/birth cohorts from Europe and North America. All 28 cohorts had information on maternal smoking, and 16 also had information on paternal smoking. In total, 22 cohorts were population-based, with birth years ranging from 1991 to 2015. The mothers’ median age was 30.0 years, and most mothers were medium or highly educated. We used multilevel binary logistic regression models adjusted for maternal and paternal sociodemographic and lifestyle-related characteristics. Compared with nonsmoking mothers, maternal first trimester smoking only was not associated with adverse birth outcomes but was associated with a higher risk of childhood overweight (odds ratio [OR] 1.17 [95% CI 1.02–1.35], P value = 0.030). Children from mothers who continued smoking during pregnancy had higher risks of preterm birth (OR 1.08 [95% CI 1.02–1.15], P value = 0.012), small size for gestational age (OR 2.15 [95% CI 2.07–2.23], P value < 0.001), and childhood overweight (OR 1.42 [95% CI 1.35–1.48], P value < 0.001). Mothers who reduced the number of cigarettes between the first and third trimester, without quitting, still had a higher risk of small size for gestational age. However, the corresponding risk estimates were smaller than for women who continued the same amount of cigarettes throughout pregnancy (OR 1.89 [95% CI 1.52–2.34] instead of OR 2.20 [95% CI 2.02–2.42] when reducing from 5–9 to ≤4 cigarettes/day; OR 2.79 [95% CI 2.39–3.25] and OR 1.93 [95% CI 1.46–2.57] instead of OR 2.95 [95% CI 2.75–3.15] when reducing from ≥10 to 5–9 and ≤4 cigarettes/day, respectively [P values < 0.001]). Reducing the number of cigarettes during pregnancy did not affect the risks of preterm birth and childhood overweight. Among nonsmoking mothers, paternal smoking was associated with childhood overweight (OR 1.21 [95% CI 1.16–1.27], P value < 0.001) but not with adverse birth outcomes. Limitations of this study include the self-report of parental smoking information and the possibility of residual confounding. As this study only included participants from Europe and North America, results need to be carefully interpreted regarding other populations. Conclusions We observed that as compared to nonsmoking during pregnancy, quitting smoking in the first trimester is associated with the same risk of preterm birth and small size for gestational age, but with a higher risk of childhood overweight. Reducing the number of cigarettes, without quitting, has limited beneficial effects. Paternal smoking seems to be associated, independently of maternal smoking, with the risk of childhood overweight. Population strategies should focus on parental smoking prevention before or at the start, rather than during, pregnancy. © 2020 Philips et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Published
2020

16. Caries Risk Prediction Models in a Medical Health Care Setting

Author

Kalhan, T.A., Lam, C., Karunakaran, B., Chay, P.L., Chng, C.K., Nair, R., Lee, Y.S., Fong, M.C.F., Chong, Y.S., Kwek, K., Saw, S.M., Shek, L., Yap, F., Tan, K.H., Godfrey, K.M., Huang, J., Hsu, C.S., Kalhan, T.A., Lam, C., Karunakaran, B., Chay, P.L., Chng, C.K., Nair, R., Lee, Y.S., Fong, M.C.F., Chong, Y.S., Kwek, K., Saw, S.M., Shek, L., Yap, F., Tan, K.H., Godfrey, K.M., Huang, J., and Hsu, C.S.

Abstract

Contains fulltext : 225413.pdf (Publisher’s version ) (Closed access), Despite development of new technologies for caries control, tooth decay in primary teeth remains a major global health problem. Caries risk assessment (CRA) models for toddlers and preschoolers are rare. Among them, almost all models use dental factors (e.g., past caries experience) to predict future caries risk, with limited clinical/community applicability owing to relatively uncommon dental visits compared to frequent medical visits during the first year of life. The objective of this study was to construct and evaluate risk prediction models using information easily accessible to medical practitioners to forecast caries at 2 and 3 y of age. Data were obtained from the Growing Up in Singapore Towards Healthy Outcomes (GUSTO) mother-offspring cohort. Caries was diagnosed using modified International Caries Detection and Assessment System criteria. Risk prediction models were constructed using multivariable logistic regression coupled with receiver operating characteristic analyses. Imputation was performed using multiple imputation by chained equations to assess effect of missing data. Caries rates at ages 2 y (n = 535) and 3 y (n = 721) were 17.8% and 42.9%, respectively. Risk prediction models predicting overall caries risk at 2 and 3 y demonstrated area under the curve (AUC) (95% confidence interval) of 0.81 (0.75-0.87) and 0.79 (0.74-0.84), respectively, while those predicting moderate to extensive lesions showed 0.91 (0.85-0.97) and 0.79 (0.73-0.85), respectively. Postimputation results showed reduced AUC of 0.75 (0.74-0.81) and 0.71 (0.67-0.75) at years 2 and 3, respectively, for overall caries risk, while AUC was 0.84 (0.76-0.92) and 0.75 (0.70-0.80), respectively, for moderate to extensive caries. Addition of anterior caries significantly increased AUC in all year 3 models with or without imputation (all P < 0.05). Significant predictors/protectors were identified, including ethnicity, prenatal tobacco smoke exposure, history of allergies before 12 mo, his

Published
2020

17. Changes in parental smoking during pregnancy and risks of adverse birth outcomes and childhood overweight in Europe and North America: An individual participant data meta-analysis of 229,000 singleton births

Author

Philips, E.M., Santos, S., Trasande, L., Aurrekoetxea, J.J., Barros, H., von Berg, A., Bergström, A., Bird, P.K., Brescianini, S., Ní Chaoimh, C., Charles, M.-A., Chatzi, L., Chevrier, C., Chrousos, G.P., Costet, N., Criswell, R., Crozier, S., Eggesbø, M., Fantini, M.P., Farchi, S., Forastiere, F., van Gelder, M.M.H.J., Georgiu, V., Godfrey, K.M., Gori, D., Hanke, W., Heude, B., Hryhorczuk, D., Iñiguez, C., Inskip, H., Karvonen, A.M., Kenny, L.C., Kull, I., Lawlor, D.A., Lehmann, Irina, Magnus, P., Manios, Y., Melén, E., Mommers, M., Morgen, C.S., Moschonis, G., Murray, D., Nohr, E.A., Nybo Andersen, A.-M., Oken, E., Oostvogels, A.J.J.M., Papadopoulou, E., Pekkanen, J., Pizzi, C., Polanska, K., Porta, D., Richiardi, L., Rifas‐Shiman, S.L., Roeleveld, N., Rusconi, F., Santos, A.C., Sørensen, T.I.A., Standl, M., Stoltenberg, C., Sunyer, J., Thiering, E., Thijs, C., Torrent, M., Vrijkotte, T.G.M., Wright, J., Zvinchuk, O., Gaillard, R., Jaddoe, V.W.V., Philips, E.M., Santos, S., Trasande, L., Aurrekoetxea, J.J., Barros, H., von Berg, A., Bergström, A., Bird, P.K., Brescianini, S., Ní Chaoimh, C., Charles, M.-A., Chatzi, L., Chevrier, C., Chrousos, G.P., Costet, N., Criswell, R., Crozier, S., Eggesbø, M., Fantini, M.P., Farchi, S., Forastiere, F., van Gelder, M.M.H.J., Georgiu, V., Godfrey, K.M., Gori, D., Hanke, W., Heude, B., Hryhorczuk, D., Iñiguez, C., Inskip, H., Karvonen, A.M., Kenny, L.C., Kull, I., Lawlor, D.A., Lehmann, Irina, Magnus, P., Manios, Y., Melén, E., Mommers, M., Morgen, C.S., Moschonis, G., Murray, D., Nohr, E.A., Nybo Andersen, A.-M., Oken, E., Oostvogels, A.J.J.M., Papadopoulou, E., Pekkanen, J., Pizzi, C., Polanska, K., Porta, D., Richiardi, L., Rifas‐Shiman, S.L., Roeleveld, N., Rusconi, F., Santos, A.C., Sørensen, T.I.A., Standl, M., Stoltenberg, C., Sunyer, J., Thiering, E., Thijs, C., Torrent, M., Vrijkotte, T.G.M., Wright, J., Zvinchuk, O., Gaillard, R., and Jaddoe, V.W.V.

Abstract

Background Fetal smoke exposure is a common and key avoidable risk factor for birth complications and seems to influence later risk of overweight. It is unclear whether this increased risk is also present if mothers smoke during the first trimester only or reduce the number of cigarettes during pregnancy, or when only fathers smoke. We aimed to assess the associations of parental smoking during pregnancy, specifically of quitting or reducing smoking and maternal and paternal smoking combined, with preterm birth, small size for gestational age, and childhood overweight. Methods and findings We performed an individual participant data meta-analysis among 229,158 families from 28 pregnancy/birth cohorts from Europe and North America. All 28 cohorts had information on maternal smoking, and 16 also had information on paternal smoking. In total, 22 cohorts were population-based, with birth years ranging from 1991 to 2015. The mothers’ median age was 30.0 years, and most mothers were medium or highly educated. We used multilevel binary logistic regression models adjusted for maternal and paternal sociodemographic and lifestyle-related characteristics. Compared with nonsmoking mothers, maternal first trimester smoking only was not associated with adverse birth outcomes but was associated with a higher risk of childhood overweight (odds ratio [OR] 1.17 [95% CI 1.02–1.35], P value = 0.030). Children from mothers who continued smoking during pregnancy had higher risks of preterm birth (OR 1.08 [95% CI 1.02–1.15], P value = 0.012), small size for gestational age (OR 2.15 [95% CI 2.07–2.23], P value < 0.001), and childhood overweight (OR 1.42 [95% CI 1.35–1.48], P value < 0.001). Mothers who reduced the number of cigarettes between the first and third trimester, without quitting, still had a higher risk of small size for gestational age. However, the corresponding risk estimates were smaller than for women who continued the same amount of cigarettes throughout preg

Published
2020

20. Maternal vitamin D status during pregnancy and childhood bone mass at age 9 years: a longitudinal study

Author

Javaid, M.K., Crozier, S.R., Harvey, N.C., Gale, C.R., Dennison, E.M., Boucher, B.J., Arden, N.K., Godfrey, K.M., and Cooper, C.

Subjects
Alfacalcidol -- Dosage and administration, Calcifediol -- Dosage and administration, Vitamin D -- Dosage and administration, Pregnant women -- Health aspects, Vitamin D deficiency -- Complications and side effects, Bones -- Density, Bones -- Measurement
Published
2006

21. Adiposity associated DNA methylation signatures in adolescents are related to leptin and perinatal factors

Author

Huang, R.C., primary, Melton, P.E., additional, Burton, M.A., additional, Beilin, L.J., additional, Clarke-Harris, R, additional, Cook, E, additional, Godfrey, K.M., additional, Burdge, G.C., additional, Mori, T.A., additional, Anderson, D, additional, Rauschert, S., additional, Craig, J. M., additional, Kobor, M.S., additional, MacIsaac, J.L., additional, Morin, A.M., additional, Oddy, W.H., additional, Pennell, C.E., additional, Holbrook, J.D., additional, and Lillycrop, K.A., additional

Published
2021
Full Text
View/download PDF

24. Antimicrobial treatment in diabetic women with asymptomatic bacteriuria

Author

Harding, Godfrey K.M., Zhanel, George G., Nicolle, Lindsay E., and Cheang, Mary

Subjects
Urinary tract infections -- Prevention, Bacteria in the urine -- Drug therapy, Diabetes -- Complications
Abstract

Treating diabetic women who have asymptomatic bacteriuria with antibiotics will not necessarily prevent them from developing a urinary tract infection, according to a study of 105 women. Asymptomatic bacteriuria means the woman has bacteria in her urine, but no symptoms of infection. Diabetic women are three times more likely to have this condition as healthy women.

Published
2002

25. An outbreak of necrotizing enterocolitis associated with a novel Clostridium species in a neonatal intensive care unit. (Supplement Article)

Author

Alfa, Michelle J., Robson, Diane, Davi, Maria, Bernard, Kathy, Caeseele, Paul Van, and Harding, Godfrey K.M.

Subjects
Enterocolitis, Pseudomembranous -- Care and treatment, Enterocolitis, Neonatal necrotizing, Clostridium infections -- Care and treatment, Cross infection -- Care and treatment, Nosocomial infections, Health, Health care industry
Published
2002

27. Caries Risk Prediction Models in a Medical Health Care Setting

Author

Kalhan, T.A., primary, Un Lam, C., additional, Karunakaran, B., additional, Chay, P.L., additional, Chng, C.K., additional, Nair, R., additional, Lee, Y.S., additional, Fong, M.C.F., additional, Chong, Y.S., additional, Kwek, K., additional, Saw, S.M., additional, Shek, L., additional, Yap, F., additional, Tan, K.H., additional, Godfrey, K.M., additional, Huang, J., additional, and Hsu, C.-Y.S., additional

Published
2020
Full Text
View/download PDF

28. Impact of maternal body mass index and gestational weight gain on pregnancy complications: an individual participant data meta-analysis of European, North American and Australian cohorts

Author

Santos, S. Voerman, E. Amiano, P. Barros, H. Beilin, L.J. Bergström, A. Charles, M.-A. Chatzi, L. Chevrier, C. Chrousos, G.P. Corpeleijn, E. Costa, O. Costet, N. Crozier, S. Devereux, G. Doyon, M. Eggesbø, M. Fantini, M.P. Farchi, S. Forastiere, F. Georgiu, V. Godfrey, K.M. Gori, D. Grote, V. Hanke, W. Hertz-Picciotto, I. Heude, B. Hivert, M.-F. Hryhorczuk, D. Huang, R.-C. Inskip, H. Karvonen, A.M. Kenny, L.C. Koletzko, B. Küpers, L.K. Lagström, H. Lehmann, I. Magnus, P. Majewska, R. Mäkelä, J. Manios, Y. McAuliffe, F.M. McDonald, S.W. Mehegan, J. Melén, E. Mommers, M. Morgen, C.S. Moschonis, G. Murray, D. Ní Chaoimh, C. Nohr, E.A. Nybo Andersen, A.-M. Oken, E. Oostvogels, A.J.J.M. Pac, A. Papadopoulou, E. Pekkanen, J. Pizzi, C. Polanska, K. Porta, D. Richiardi, L. Rifas-Shiman, S.L. Roeleveld, N. Ronfani, L. Santos, A.C. Standl, M. Stigum, H. Stoltenberg, C. Thiering, E. Thijs, C. Torrent, M. Tough, S.C. Trnovec, T. Turner, S. van Gelder, M.M.H.J. van Rossem, L. von Berg, A. Vrijheid, M. Vrijkotte, T.G.M. West, J. Wijga, A.H. Wright, J. Zvinchuk, O. Sørensen, T.I.A. Lawlor, D.A. Gaillard, R. Jaddoe, V.W.V.

Abstract

Objective: To assess the separate and combined associations of maternal pre-pregnancy body mass index (BMI) and gestational weight gain with the risks of pregnancy complications and their population impact. Design: Individual participant data meta-analysis of 39 cohorts. Setting: Europe, North America, and Oceania. Population: 265 270 births. Methods: Information on maternal pre-pregnancy BMI, gestational weight gain, and pregnancy complications was obtained. Multilevel binary logistic regression models were used. Main outcome measures: Gestational hypertension, pre-eclampsia, gestational diabetes, preterm birth, small and large for gestational age at birth. Results: Higher maternal pre-pregnancy BMI and gestational weight gain were, across their full ranges, associated with higher risks of gestational hypertensive disorders, gestational diabetes, and large for gestational age at birth. Preterm birth risk was higher at lower and higher BMI and weight gain. Compared with normal weight mothers with medium gestational weight gain, obese mothers with high gestational weight gain had the highest risk of any pregnancy complication (odds ratio 2.51, 95% CI 2.31– 2.74). We estimated that 23.9% of any pregnancy complication was attributable to maternal overweight/obesity and 31.6% of large for gestational age infants was attributable to excessive gestational weight gain. Conclusions: Maternal pre-pregnancy BMI and gestational weight gain are, across their full ranges, associated with risks of pregnancy complications. Obese mothers with high gestational weight gain are at the highest risk of pregnancy complications. Promoting a healthy pre-pregnancy BMI and gestational weight gain may reduce the burden of pregnancy complications and ultimately the risk of maternal and neonatal morbidity. Tweetable abstract: Promoting a healthy body mass index and gestational weight gain might reduce the population burden of pregnancy complications. © 2019 Royal College of Obstetricians and Gynaecologists

Published
2019

31. Impact of maternal body mass index and gestational weight gain on pregnancy complications: An individual participant data meta‐analysis of European, North American and Australian cohorts

Author

Santos, S., Voerman, E., Amiano, P., Barros, H., Beilin, L.J., Bergström, A., Charles, M.-A., Chatzi, L., Chevrier, C., Chrousos, G.P., Corpeleijn, E., Costa, O., Costet, N., Crozier, S., Devereux, G., Doyon, M., Eggesbø, M., Fantini, M.P., Farchi, S., Forastiere, F., Georgiu, V., Godfrey, K.M., Gori, D., Grote, V., Hanke, W., Hertz‐Picciotto, I., Heude, B., Hivert, M.-F., Hryhorczuk, D., Huang, R.-C., Inskip, H., Karvonen, A.M., Kenny, L.C., Koletzko, B., Küpers, L.K., Lagström, H., Lehmann, Irina, Magnus, P., Majewska, R., Mäkelä, J., Manios, Y., McAuliffe, F.M., McDonald, S.W., Mehegan, J., Melén, E., Mommers, M., Morgen, C.S., Moschonis, G., Murray, D., Ní Chaoimh, C., Nohr, E.A., Nybo Andersen, A.-M., Oken, E., Oostvogels, A.J.J.M., Pac, A., Papadopoulou, E., Pekkanen, J., Pizzi, C., Polanska, K., Porta, D., Richiardi, L., Rifas‐Shiman, S.L., Roeleveld, N., Ronfani, L., Santos, A.C., Standl, M., Stigum, H., Stoltenberg, C., Thiering, E., Thijs, C., Torrent, M., Tough, S.C., Trnovec, T., Turner, S., van Gelder, M.M.H.J., van Rossem, L., von Berg, A., Vrijheid, M., Vrijkotte, T.G.M., West, J., Wijga, A.H., Wright, J., Zvinchuk, O., Sørensen, T.I.A., Lawlor, D.A., Gaillard, R., Jaddoe, V.W.V., Santos, S., Voerman, E., Amiano, P., Barros, H., Beilin, L.J., Bergström, A., Charles, M.-A., Chatzi, L., Chevrier, C., Chrousos, G.P., Corpeleijn, E., Costa, O., Costet, N., Crozier, S., Devereux, G., Doyon, M., Eggesbø, M., Fantini, M.P., Farchi, S., Forastiere, F., Georgiu, V., Godfrey, K.M., Gori, D., Grote, V., Hanke, W., Hertz‐Picciotto, I., Heude, B., Hivert, M.-F., Hryhorczuk, D., Huang, R.-C., Inskip, H., Karvonen, A.M., Kenny, L.C., Koletzko, B., Küpers, L.K., Lagström, H., Lehmann, Irina, Magnus, P., Majewska, R., Mäkelä, J., Manios, Y., McAuliffe, F.M., McDonald, S.W., Mehegan, J., Melén, E., Mommers, M., Morgen, C.S., Moschonis, G., Murray, D., Ní Chaoimh, C., Nohr, E.A., Nybo Andersen, A.-M., Oken, E., Oostvogels, A.J.J.M., Pac, A., Papadopoulou, E., Pekkanen, J., Pizzi, C., Polanska, K., Porta, D., Richiardi, L., Rifas‐Shiman, S.L., Roeleveld, N., Ronfani, L., Santos, A.C., Standl, M., Stigum, H., Stoltenberg, C., Thiering, E., Thijs, C., Torrent, M., Tough, S.C., Trnovec, T., Turner, S., van Gelder, M.M.H.J., van Rossem, L., von Berg, A., Vrijheid, M., Vrijkotte, T.G.M., West, J., Wijga, A.H., Wright, J., Zvinchuk, O., Sørensen, T.I.A., Lawlor, D.A., Gaillard, R., and Jaddoe, V.W.V.

Abstract

Objective To assess the separate and combined associations of maternal pre‐pregnancy BMI and gestational weight gain with the risks of pregnancy complications and their population impact.Design Individual participant data meta‐analysis of 39 cohorts.SettingEurope, North America and Oceania. Population 265,270 births. Methods Information on maternal pre‐pregnancy BMI, gestational weight gain, and pregnancy complications was obtained. Multilevel binary logistic regression models were used. Main outcome measures Gestational hypertension, pre‐eclampsia, gestational diabetes, preterm birth, small and large size for gestational age at birth. Results Higher maternal pre‐pregnancy BMI and gestational weight gain were, across their full ranges, associated with higher risks of gestational hypertensive disorders, gestational diabetes and large size for gestational age at birth. Preterm birth risk was higher at lower and higher BMI and weight gain. Compared to normal weight mothers with medium gestational weight gain, obese mothers with high gestational weight gain had the highest risk of any pregnancy complication (Odds Ratio 2.51 (95% Confidence Interval 2.31, 2.74)). We estimated that 23.9% of any pregnancy complication was attributable to maternal overweight/obesity and 31.6% of large size for gestational age infants was attributable to excessive gestational weight gain. Conclusions Maternal pre‐pregnancy BMI and gestational weight gain are, across their full ranges, associated with the risks of pregnancy complications. Obese mothers with high gestational weight gain are at the highest risk of pregnancy complications. Promoting a healthy pre‐pregnancy BMI and gestational weight gain may reduce the burden of pregnancy complications and ultimately the risk of maternal and neonatal morbidity.

Published
2019

32. Maternal body mass index, gestational weight gain, and the risk of overweight and obesity across childhood: An individual participant data meta-analysis

Author

Voerman, E., Santos, S., Patro Golab, B., Amiano, P., Ballester, F., Barros, H., Bergström, A., Charles, M.-A., Chatzi, L., Chevrier, C., Chrousos, G.P., Corpeleijn, E., Costet, N., Crozier, S., Devereux, G., Eggesbø, M., Ekström, S., Fantini, M.P., Farchi, S., Forastiere, F., Georgiu, V., Godfrey, K.M., Gori, D., Grote, V., Hanke, W., Hertz-Picciotto, I., Heude, B., Hryhorczuk, D., Huang, R.-C., Inskip, H., Iszatt, N., Karvonen, A.M., Kenny, L.C., Koletzko, B., Küpers, L.K., Lagström, H., Lehmann, Irina, Magnus, P., Majewska, R., Mäkelä, J., Manios, Y., McAuliffe, F.M., McDonald, S.W., Mehegan, J., Mommers, M., Morgen, C.S., Mori, T.A., Moschonis, G., Murray, D., Ní Chaoimh, C., Nohr, E.A., Nybo Andersen, A.-M., Oken, E., Oostvogels, A.J.J.M., Pac, A., Papadopoulou, E., Pekkanen, J., Pizzi, C., Polanska, K., Porta, D., Richiardi, L., Rifas-Shiman, S.-L., Ronfani, L., Santos, A.C., Standl, M., Stoltenberg, C., Thiering, E., Thijs, C., Torrent, M., Tough, S.C., Trnovec, T., Turner, S., van Rossem, L., von Berg, A., Vrijheid, M., Vrijkotte, T.G.M., West, J., Wijga, A., Wright, J., Zvinchuk, O., Sørensen, T.I.A., Lawlor, D.A., Gaillard, R., Jaddoe, V.W.V., Voerman, E., Santos, S., Patro Golab, B., Amiano, P., Ballester, F., Barros, H., Bergström, A., Charles, M.-A., Chatzi, L., Chevrier, C., Chrousos, G.P., Corpeleijn, E., Costet, N., Crozier, S., Devereux, G., Eggesbø, M., Ekström, S., Fantini, M.P., Farchi, S., Forastiere, F., Georgiu, V., Godfrey, K.M., Gori, D., Grote, V., Hanke, W., Hertz-Picciotto, I., Heude, B., Hryhorczuk, D., Huang, R.-C., Inskip, H., Iszatt, N., Karvonen, A.M., Kenny, L.C., Koletzko, B., Küpers, L.K., Lagström, H., Lehmann, Irina, Magnus, P., Majewska, R., Mäkelä, J., Manios, Y., McAuliffe, F.M., McDonald, S.W., Mehegan, J., Mommers, M., Morgen, C.S., Mori, T.A., Moschonis, G., Murray, D., Ní Chaoimh, C., Nohr, E.A., Nybo Andersen, A.-M., Oken, E., Oostvogels, A.J.J.M., Pac, A., Papadopoulou, E., Pekkanen, J., Pizzi, C., Polanska, K., Porta, D., Richiardi, L., Rifas-Shiman, S.-L., Ronfani, L., Santos, A.C., Standl, M., Stoltenberg, C., Thiering, E., Thijs, C., Torrent, M., Tough, S.C., Trnovec, T., Turner, S., van Rossem, L., von Berg, A., Vrijheid, M., Vrijkotte, T.G.M., West, J., Wijga, A., Wright, J., Zvinchuk, O., Sørensen, T.I.A., Lawlor, D.A., Gaillard, R., and Jaddoe, V.W.V.

Abstract

BackgroundMaternal obesity and excessive gestational weight gain may have persistent effects on offspring fat development. However, it remains unclear whether these effects differ by severity of obesity, and whether these effects are restricted to the extremes of maternal body mass index (BMI) and gestational weight gain. We aimed to assess the separate and combined associations of maternal BMI and gestational weight gain with the risk of overweight/obesity throughout childhood, and their population impact. Methods and findingsWe conducted an individual participant data meta-analysis of data from 162,129 mothers and their children from 37 pregnancy and birth cohort studies from Europe, North America, and Australia. We assessed the individual and combined associations of maternal pre-pregnancy BMI and gestational weight gain, both in clinical categories and across their full ranges, with the risks of overweight/obesity in early (2.0–5.0 years), mid (5.0–10.0 years) and late childhood (10.0–18.0 years), using multilevel binary logistic regression models with a random intercept at cohort level adjusted for maternal sociodemographic and lifestyle-related characteristics. We observed that higher maternal pre-pregnancy BMI and gestational weight gain both in clinical categories and across their full ranges were associated with higher risks of childhood overweight/obesity, with the strongest effects in late childhood (odds ratios [ORs] for overweight/obesity in early, mid, and late childhood, respectively: OR 1.66 [95% CI: 1.56, 1.78], OR 1.91 [95% CI: 1.85, 1.98], and OR 2.28 [95% CI: 2.08, 2.50] for maternal overweight; OR 2.43 [95% CI: 2.24, 2.64], OR 3.12 [95% CI: 2.98, 3.27], and OR 4.47 [95% CI: 3.99, 5.23] for maternal obesity; and OR 1.39 [95% CI: 1.30, 1.49], OR 1.55 [95% CI: 1.49, 1.60], and OR 1.72 [95% CI: 1.56, 1.91] for excessive gestational weight gain). The proportions of childhood overweight/obesity prevalence attributable to maternal overweight, maternal

Published
2019

34. Fetal nutrition and cardiovascular disease in adult life

Author

Barker, D.J.P., Gluckman, P.D., Godfrey, K.M., Harding, J.E., Owens, J.A., and Robinson, J.S.

Subjects
Fetal malnutrition -- Physiological aspects, Cardiovascular diseases -- Risk factors, Birth weight, Low -- Physiological aspects, Diabetes -- Risk factors
Published
1993

35. Relation of FTO gene variants to fetal growth trajectories: Findings from the Southampton Women's survey

Author

Barton, S.J., Mosquera, M., Cleal, J.K., Fuller, A.S., Crozier, S.R., Cooper, C., Inskip, H.M., Holloway, J.W., Lewis, R.M., and Godfrey, K.M.

Subjects
Placental amino acid transporter expression, endocrine system diseases, Reproductive Medicine, Fetal growth trajectories, Obstetrics and Gynaecology, nutritional and metabolic diseases, MC4R genotype, pathological conditions, signs and symptoms, Placental FTO expression, FTO genotype, Developmental Biology
Abstract

IntroductionPlacental function is an important determinant of fetal growth, and fetal growth influences obesity risk in childhood and adult life. Here we investigated how FTO and MC4R gene variants linked with obesity relate to patterns of fetal growth and to placental FTO expression.MethodsSouthampton Women's Survey children (n = 1990) with measurements of fetal growth from 11 to 34 weeks gestation were genotyped for common gene variants in FTO (rs9939609, rs1421085) and MC4R (rs17782313). Linear mixed-effect models were used to analyse relations of gene variants with fetal growth.ResultsFetuses with the rs9939609 A:A FTO genotype had faster biparietal diameter and head circumference growth velocities between 11 and 34 weeks gestation (by 0.012 (95% CI 0.005 to 0.019) and 0.008 (0.002–0.015) standard deviations per week, respectively) compared to fetuses with the T:T FTO genotype; abdominal circumference growth velocity did not differ between genotypes. FTO genotype was not associated with placental FTO expression, but higher placental FTO expression was independently associated with larger fetal size and higher placental ASCT2, EAAT2 and y + LAT2 amino acid transporter expression. Findings were similar for FTO rs1421085, and the MC4R gene variant was associated with the fetal growth velocity of head circumference.DiscussionFTO gene variants are known to associate with obesity but this is the first time that the risk alleles and placental FTO expression have been linked with fetal growth trajectories. The lack of an association between FTO genotype and placental FTO expression adds to emerging evidence of complex biology underlying the association between FTO genotype and obesity.

Published
2016
Full Text
View/download PDF

36. Gestational weight gain charts for different body mass index groups for women in Europe, North America, and Oceania

Author

Santos, S. Eekhout, I. Voerman, E. Gaillard, R. Barros, H. Charles, M.-A. Chatzi, L. Chevrier, C. Chrousos, G.P. Corpeleijn, E. Costet, N. Crozier, S. Doyon, M. Eggesbø, M. Fantini, M.P. Farchi, S. Forastiere, F. Gagliardi, L. Georgiu, V. Godfrey, K.M. Gori, D. Grote, V. Hanke, W. Hertz-Picciotto, I. Heude, B. Hivert, M.-F. Hryhorczuk, D. Huang, R.-C. Inskip, H. Jusko, T.A. Karvonen, A.M. Koletzko, B. Küpers, L.K. Lagström, H. Lawlor, D.A. Lehmann, I. Lopez-Espinosa, M.-J. Magnus, P. Majewska, R. Mäkelä, J. Manios, Y. McDonald, S.W. Mommers, M. Morgen, C.S. Moschonis, G. Murínová, L. Newnham, J. Nohr, E.A. Andersen, A.-M.N. Oken, E. Oostvogels, A.J.J.M. Pac, A. Papadopoulou, E. Pekkanen, J. Pizzi, C. Polanska, K. Porta, D. Richiardi, L. Rifas-Shiman, S.L. Roeleveld, N. Santa-Marina, L. Santos, A.C. Smit, H.A. Sørensen, T.I.A. Standl, M. Stanislawski, M. Stoltenberg, C. Thiering, E. Thijs, C. Torrent, M. Tough, S.C. Trnovec, T. Van Gelder, M.M.H.J. Van Rossem, L. Von Berg, A. Vrijheid, M. Vrijkotte, T.G.M. Zvinchuk, O. Van Buuren, S. Jaddoe, V.W.V.

Abstract

Background: Gestational weight gain differs according to pre-pregnancy body mass index and is related to the risks of adverse maternal and child health outcomes. Gestational weight gain charts for women in different pre-pregnancy body mass index groups enable identification of women and offspring at risk for adverse health outcomes. We aimed to construct gestational weight gain reference charts for underweight, normal weight, overweight, and grades 1, 2 and 3 obese women and to compare these charts with those obtained in women with uncomplicated term pregnancies. Methods: We used individual participant data from 218,216 pregnant women participating in 33 cohorts from Europe, North America, and Oceania. Of these women, 9065 (4.2%), 148,697 (68.1%), 42,678 (19.6%), 13,084 (6.0%), 3597 (1.6%), and 1095 (0.5%) were underweight, normal weight, overweight, and grades 1, 2, and 3 obese women, respectively. A total of 138, 517 women from 26 cohorts had pregnancies with no hypertensive or diabetic disorders and with term deliveries of appropriate for gestational age at birth infants. Gestational weight gain charts for underweight, normal weight, overweight, and grade 1, 2, and 3 obese women were derived by the Box-Cox t method using the generalized additive model for location, scale, and shape. Results: We observed that gestational weight gain strongly differed per maternal pre-pregnancy body mass index group. The median (interquartile range) gestational weight gain at 40 weeks was 14.2 kg (11.4-17.4) for underweight women, 14.5 kg (11.5-17.7) for normal weight women, 13.9 kg (10.1-17.9) for overweight women, and 11.2 kg (7.0-15.7), 8.7 kg (4.3-13.4) and 6.3 kg (1.9-11.1) for grades 1, 2, and 3 obese women, respectively. The rate of weight gain was lower in the first half than in the second half of pregnancy. No differences in the patterns of weight gain were observed between cohorts or countries. Similar weight gain patterns were observed in mothers without pregnancy complications. Conclusions: Gestational weight gain patterns are strongly related to pre-pregnancy body mass index. The derived charts can be used to assess gestational weight gain in etiological research and as a monitoring tool for weight gain during pregnancy in clinical practice. © 2018 The Author(s).

Published
2018

38. Gestational weight gain charts for different body mass index groups for women in Europe, North America, and Oceania

Author

Santos, S. (Susana), Eekhout, I. (Iris), Voerman, E. (Ellis), Gaillard, R. (Romy), Barros, A.I. (Ana), Charles, M.A., Chatzi, L. (Leda), Chevrier, C. (Cécile), Chrousos, G.P. (George P.), Corpeleijn, W.E. (Willemijn), Costet, N. (Nathalie), Crozier, S. (Sarah), Doyon, M. (Myriam), Eggesbø, M. (Merete), Fantini, M.P. (Maria), Farchi, S. (Sara), Forastiere, F. (Francesco), Gagliardi, L. (Luigi), Georgiu, V. (Vagelis), Godfrey, K.M. (Keith M.), Gori, D. (Davide), Grote, V. (Veit), Hanke, W. (Wojciech), Hertz-Picciotto, I. (Irva), Heude, B. (Barbara), Hivert, M.-F. (Marie-France), Hryhorczuk, D.O. (Daniel), Huang, R.-C. (Rae-Chi), Inskip, H.M. (Hazel), Jusko, T.A. (Todd A), Karvonen, A.M. (Anne M.), Koletzko, B. (Berthold), Küpers, A.M. (Marlijn), Lagström, H. (Hanna), Lawlor, D.A. (Debbie A.), Lehmann, I. (Irina), Lopez-Espinosa, M.-J. (Maria-Jose), Magnus, P. (Per), Majewska, R. (Renata), Mäkelä, J. (Johanna), Manios, Y., McDonald, S.W. (Sheila W.), Mommers, M. (Monique), Morgen, C.S. (Camilla S.), Moschonis, G., Murinova, L.P. (Lubica Palkovicova), Newnham, J.P. (John), Nohr, C. (Christian), Andersen, A-M.N. (Anne-Marie Nybo), Oken, E. (Emily), Oostvogels, A.J.J.M. (Adriëtte J. J. M.), Pac, A. (Agnieszka), Papadopoulou, E. (Eleni), Pekkanen, J. (Juha), Pizzi, C. (Costanza), Polanska, K. (Kinga), Porta, D. (Daniela), Richiardi, L. (Lorenzo), Rifas-Shiman, S.L. (Sheryl), Roeleveld, N. (Nel), Santa-Marina, L. (Loreto), Santos, A.C. (Ana Cristina), Smit, H.A. (Henriëtte), Sørensen, T.I.A. (Thorkild), Standl, M. (Marie), Stanislawski, M. (Maggie), Stoltenberg, C. (Camilla), Thiering, E. (Elisabeth), Thijs, C. (Carel), Torrent, M. (Maties), Tough, S.C. (Suzanne C.), Trnovec, T. (Tomáš), Van Gelder, M.M.H.J. (Marleen M. H. J.), Rossem, L. (Lenie) van, Berg, A. (Andrea) von, Vrijheid, M. (Martine), Vrijkotte, T.G.M. (Tanja), Zvinchuk, O. (Oleksandr), Buuren, S. (Stef) van, Jaddoe, V.W.V. (Vincent), Santos, S. (Susana), Eekhout, I. (Iris), Voerman, E. (Ellis), Gaillard, R. (Romy), Barros, A.I. (Ana), Charles, M.A., Chatzi, L. (Leda), Chevrier, C. (Cécile), Chrousos, G.P. (George P.), Corpeleijn, W.E. (Willemijn), Costet, N. (Nathalie), Crozier, S. (Sarah), Doyon, M. (Myriam), Eggesbø, M. (Merete), Fantini, M.P. (Maria), Farchi, S. (Sara), Forastiere, F. (Francesco), Gagliardi, L. (Luigi), Georgiu, V. (Vagelis), Godfrey, K.M. (Keith M.), Gori, D. (Davide), Grote, V. (Veit), Hanke, W. (Wojciech), Hertz-Picciotto, I. (Irva), Heude, B. (Barbara), Hivert, M.-F. (Marie-France), Hryhorczuk, D.O. (Daniel), Huang, R.-C. (Rae-Chi), Inskip, H.M. (Hazel), Jusko, T.A. (Todd A), Karvonen, A.M. (Anne M.), Koletzko, B. (Berthold), Küpers, A.M. (Marlijn), Lagström, H. (Hanna), Lawlor, D.A. (Debbie A.), Lehmann, I. (Irina), Lopez-Espinosa, M.-J. (Maria-Jose), Magnus, P. (Per), Majewska, R. (Renata), Mäkelä, J. (Johanna), Manios, Y., McDonald, S.W. (Sheila W.), Mommers, M. (Monique), Morgen, C.S. (Camilla S.), Moschonis, G., Murinova, L.P. (Lubica Palkovicova), Newnham, J.P. (John), Nohr, C. (Christian), Andersen, A-M.N. (Anne-Marie Nybo), Oken, E. (Emily), Oostvogels, A.J.J.M. (Adriëtte J. J. M.), Pac, A. (Agnieszka), Papadopoulou, E. (Eleni), Pekkanen, J. (Juha), Pizzi, C. (Costanza), Polanska, K. (Kinga), Porta, D. (Daniela), Richiardi, L. (Lorenzo), Rifas-Shiman, S.L. (Sheryl), Roeleveld, N. (Nel), Santa-Marina, L. (Loreto), Santos, A.C. (Ana Cristina), Smit, H.A. (Henriëtte), Sørensen, T.I.A. (Thorkild), Standl, M. (Marie), Stanislawski, M. (Maggie), Stoltenberg, C. (Camilla), Thiering, E. (Elisabeth), Thijs, C. (Carel), Torrent, M. (Maties), Tough, S.C. (Suzanne C.), Trnovec, T. (Tomáš), Van Gelder, M.M.H.J. (Marleen M. H. J.), Rossem, L. (Lenie) van, Berg, A. (Andrea) von, Vrijheid, M. (Martine), Vrijkotte, T.G.M. (Tanja), Zvinchuk, O. (Oleksandr), Buuren, S. (Stef) van, and Jaddoe, V.W.V. (Vincent)

Abstract

Background: Gestational weight gain differs according to pre-pregnancy body mass index and is related to the risks of adverse maternal and child health outcomes. Gestational weight gain charts for women in different pre-pregnancy body mass index groups enable identification of women and offspring at risk for adverse health outcomes. We aimed to construct gestational weight gain reference charts for underweight, normal weight, overweight, and grades 1, 2 and 3 obese women and to compare these charts with those obtained in women with uncomplicated term pregnancies. Methods: We used individual participant data from 218,216 pregnant women participating in 33 cohorts from Europe, North America, and Oceania. Of these women, 9065 (4.2%), 148,697 (68.1%), 42,678 (19.6%), 13,084 (6.0%), 3597 (1.6%), and 1095 (0.5%) were underweight, normal weight, overweight, and grades 1, 2, and 3 obese women, respectively. A total of 138, 517 women from 26 cohorts had pregnancies with no hypertensive or diabetic disorders and with term deliveries of appropriate for gestational age at birth infants. Gestational weight gain charts for underweight, normal weight, overweight, and grade 1, 2, and 3 obese women were derived by the Box-Cox t method using the generalized additive model for location, scale, and shape. Results: We observed that gestational weight gain strongly differed per maternal pre-pregnancy body mass index group. The median (interquartile range) gestational weight gain at 40 weeks was 14.2 kg (11.4-17.4) for underweight women, 14.5 kg (11.5-17.7) for normal weight women, 13.9 kg (10.1-17.9) for overweight women, and 11.2 kg (7.0-15.7), 8.7 kg (4.3-13.4) and 6.3 kg (1.9-11.1) for grades 1, 2, and 3 obese women, respectively. The rate of weight gain was lower in the first half than in the second half of pregnancy. No differences in the patterns of weight gain were observed between cohorts or countries. Similar weight gain patterns were observed in mothers without pregnancy compli

Published
2018
Full Text
View/download PDF

39. Gestational weight gain charts for different body mass index groups for women in Europe, North America, and Oceania

Author

Santos, S., Eekhout, I., Voerman, I., Gaillard, R., Barros, H., Charles, M.-A., Chatzi, L., Chevrier, C., Chrousos, G.P., Corpeleijn, E., Costet, N., Crozier, S., Doyon, M., Eggesbø, M., Fantini, M.P., Farchi, S., Forastiere, F., Gagliardi, L., Georgiu, V., Godfrey, K.M., Gori, D., Grote, V., Hanke, W., Hertz-Picciotto, I., Heude, B., Hivert, M.-F., Hryhorczuk, D., Huang, R.-C., Inskip, H., Jusko, T.A., Karvonen, A.M., Koletzko, B., Küpers, L.K., Lagström, H., Lawlor, D.A., Lehmann, Irina, Lopez-Espinosa, M.-J., Magnus, P., Majewska, R., Mäkelä, J., Manios, Y., McDonald, S.W., Mommers, M., Morgen, C.S., Moschonis, G., Murínová, L., Newnham, J., Nohr, E.A., Nybo Andersen, A.-M., Oken, E., Oostvogels, A.J.J.M., Pac, A., Papadopoulou, E., Pekkanen, J., Pizzi, C., Polanska, K., Porta, D., Richiardi, L., Rifas-Shiman, S.-L., Roeleveld, N., Santa-Marina, L., Santos, A.C., Smit, H.A., Sørensen, T.I.A., Standl, M., Stanislawski, M., Stoltenberg, C., Thiering, E., Thijs, C., Torrent, M., Tough, S.C., Trnovec, T., van Gelder, M.M.H.J., van Rossem, L., von Berg, A., Vrijheid, M., Vrijkotte, T.G.M., Zvinchuk, O., van Buuren, S., Jaddoe, V.W.V., Santos, S., Eekhout, I., Voerman, I., Gaillard, R., Barros, H., Charles, M.-A., Chatzi, L., Chevrier, C., Chrousos, G.P., Corpeleijn, E., Costet, N., Crozier, S., Doyon, M., Eggesbø, M., Fantini, M.P., Farchi, S., Forastiere, F., Gagliardi, L., Georgiu, V., Godfrey, K.M., Gori, D., Grote, V., Hanke, W., Hertz-Picciotto, I., Heude, B., Hivert, M.-F., Hryhorczuk, D., Huang, R.-C., Inskip, H., Jusko, T.A., Karvonen, A.M., Koletzko, B., Küpers, L.K., Lagström, H., Lawlor, D.A., Lehmann, Irina, Lopez-Espinosa, M.-J., Magnus, P., Majewska, R., Mäkelä, J., Manios, Y., McDonald, S.W., Mommers, M., Morgen, C.S., Moschonis, G., Murínová, L., Newnham, J., Nohr, E.A., Nybo Andersen, A.-M., Oken, E., Oostvogels, A.J.J.M., Pac, A., Papadopoulou, E., Pekkanen, J., Pizzi, C., Polanska, K., Porta, D., Richiardi, L., Rifas-Shiman, S.-L., Roeleveld, N., Santa-Marina, L., Santos, A.C., Smit, H.A., Sørensen, T.I.A., Standl, M., Stanislawski, M., Stoltenberg, C., Thiering, E., Thijs, C., Torrent, M., Tough, S.C., Trnovec, T., van Gelder, M.M.H.J., van Rossem, L., von Berg, A., Vrijheid, M., Vrijkotte, T.G.M., Zvinchuk, O., van Buuren, S., and Jaddoe, V.W.V.

Abstract

BackgroundGestational weight gain differs according to pre-pregnancy body mass index and is related to the risks of adverse maternal and child health outcomes. Gestational weight gain charts for women in different pre-pregnancy body mass index groups enable identification of women and offspring at risk for adverse health outcomes. We aimed to construct gestational weight gain reference charts for underweight, normal weight, overweight, and grades 1, 2 and 3 obese women and to compare these charts with those obtained in women with uncomplicated term pregnancies.MethodsWe used individual participant data from 218,216 pregnant women participating in 33 cohorts from Europe, North America, and Oceania. Of these women, 9065 (4.2%), 148,697 (68.1%), 42,678 (19.6%), 13,084 (6.0%), 3597 (1.6%), and 1095 (0.5%) were underweight, normal weight, overweight, and grades 1, 2, and 3 obese women, respectively. A total of 138, 517 women from 26 cohorts had pregnancies with no hypertensive or diabetic disorders and with term deliveries of appropriate for gestational age at birth infants. Gestational weight gain charts for underweight, normal weight, overweight, and grade 1, 2, and 3 obese women were derived by the Box-Cox t method using the generalized additive model for location, scale, and shape.ResultsWe observed that gestational weight gain strongly differed per maternal pre-pregnancy body mass index group. The median (interquartile range) gestational weight gain at 40 weeks was 14.2 kg (11.4–17.4) for underweight women, 14.5 kg (11.5–17.7) for normal weight women, 13.9 kg (10.1–17.9) for overweight women, and 11.2 kg (7.0–15.7), 8.7 kg (4.3–13.4) and 6.3 kg (1.9–11.1) for grades 1, 2, and 3 obese women, respectively. The rate of weight gain was lower in the first half than in the second half of pregnancy. No differences in the patterns of weight gain were observed between cohorts or countries. Similar weight gain pat

Published
2018

40. Relation of fingerprints and shape of the palm to fetal growth and adult blood pressure

Author

Godfrey, K.M., Barker, D.J.P., Peace, J., Cloke, J., and Osmond, C.

Subjects
Fetus -- Growth, Fingerprints -- Measurement -- Physiological aspects, Hypertension -- Physiological aspects -- Measurement, Health, Company growth, Physiological aspects, Growth, Measurement
Abstract

Introduction Babies who are small at birth tend to develop high blood pressure as adults.[1-4] A recent study identified two groups of babies, born at term, who later had high [...]

Published
1993

41. Response to antenatal cholecalciferol supplementation is associated with common vitamin D related genetic variants

Author

Moon, R.J., Harvey, N.C., Cooper, C., D'Angelo, S., Curtis, E.M., Crozier, S.R., Barton, S.J., Robinson, S.M., Godfrey, K.M., Graham, N.J., Holloway, J.W., Bishop, N.J., Kennedy, S., Papageorghiou, A.T., Schoenmakers, I., Fraser, R., Gandhi, S.V., Prentice, A., Inskip, H.M., Javaid, M.K., and MAVIDOS Trial Group, MVT

Abstract

Context: Single nucleotide polymorphisms (SNP) in genes related to vitamin D metabolism have been associated with serum 25-hydroxyvitamin D [25(OH)D] concentration, but these relationships have not been examined following antenatal cholecalciferol supplementation. Objective: To determine whether SNPs in DHCR7, CYP2R1, CYP24A1 and GC are associated with the response to gestational cholecalciferol supplementation. Design: Within-randomization-group analysis of the MAVIDOS trial of antenatal cholecalciferol supplementation. Setting: Hospital antenatal clinics. Participants: 682 women of White ethnicity (351 placebo, 331 cholecalciferol) were included. SNPs at rs12785878 (DHCR7), rs10741657 (CYP2R1), rs6013897 (CYP24A1) and rs2282679 (GC) were genotyped. Interventions: 1000 IU/day cholecalciferol from 14 weeks gestation until delivery. Main Outcome Measure: 25(OH)D at randomisation and 34 weeks gestation were measured in a single batch (Diasorin Liaison). Associations between 25(OH)D and the SNPs were assessed by linear regression using an additive model (beta represents the change in 25(OH)D per additional common allele). Results: Only rs12785878 (DHCR7) was associated with baseline 25(OH)D [β=3.1nmol/l (95% CI 1.0, 5.2), p

Published
2017

43. Determinants of the maternal 25-hydroxyvitamin D response to vitamin D supplementation during pregnancy

Author

Moon, R.J., Harvey, N.C., Cooper, C., D'Angelo, S., Crozier, S.R., Inskip, H.M., Schoenmakers, I., Prentice, A., Arden, N.K., Bishop, N.J., Carr, A., Dennison, E.M., Eastell, R., Fraser, R., Gandhi, S.V., Godfrey, K.M., Kennedy, S., Mughal, M.Z., Papageorghiou, A.T., Reid, D.M., Robinson, S.M., and Javaid, M.K.

Subjects
Adult, Vitamins, Original Articles, Weight Gain, Young Adult, Double-Blind Method, Pregnancy, Outcome Assessment, Health Care, Humans, Female, Pregnancy Trimesters, Seasons, Vitamin D, Cholecalciferol
Abstract

Context: Current approaches to antenatal vitamin D supplementation do not account for interindividual differences in 25-hydroxyvitamin D (25(OH)D) response. Objective: We assessed which maternal and environmental characteristics were associated with 25(OH)D after supplementation with cholecalciferol. Design: Within-randomization-group analysis of participants in the Maternal Vitamin D Osteoporosis Study trial of vitamin D supplementation in pregnancy. Setting: Hospital antenatal clinics. Participants: A total of 829 pregnant women (422 placebo, 407 cholecalciferol). At 14 and 34 weeks of gestation, maternal anthropometry, health, and lifestyle were assessed and 25(OH)D measured. Compliance was determined using pill counts at 19 and 34 weeks. Interventions: 1000 IU/d of cholecalciferol or matched placebo from 14 weeks of gestation until delivery. Main Outcome Measure: 25(OH)D at 34 weeks, measured in a single batch (Diasorin Liaison). Results: 25(OH)D at 34 weeks of gestation was higher in the women randomized to vitamin D (mean [SD], 67.7 [21.3] nmol/L) compared with placebo (43.1 [22.5] nmol/L; P < .001). In women randomized to cholecalciferol, higher pregnancy weight gain from 14 to 34 weeks of gestation (kg) (β = −0.81 [95% confidence interval −1.39, −0.22]), lower compliance with study medication (%) (β = −0.28 [−0.072, −0.48]), lower early pregnancy 25(OH)D (nmol/L) (β = 0.28 [0.16, 0.40]), and delivery in the winter vs the summer (β = −10.5 [−6.4, −14.6]) were independently associated with lower 25(OH)D at 34 weeks of gestation. Conclusions: Women who gained more weight during pregnancy had lower 25(OH)D in early pregnancy and delivered in winter achieved a lower 25(OH)D in late pregnancy when supplemented with 1000 IU/d cholecalciferol. Future studies should aim to determine appropriate doses to enable consistent repletion of 25(OH)D during pregnancy., Within the treatment arm of the MAVIDOS RCT, poorer 25(OH)D response to 1000IU/d cholecalciferol was associated with lower initial 25(OH)D, greater pregnancy weight gain and delivery in winter.

Published
2017

45. Relation of birth weight and childhood respiratory infection to adult lung function and death from chronic obstructive airways disease

Author

Barker, D.J.P., Godfrey, K.M., Fall, C., Osmond, C., Winter, P.D., and Shaheen, S.O.

Subjects
Birth weight, Low -- Health aspects -- Measurement, Lung diseases, Obstructive -- Risk factors, Forced expiratory volume -- Measurement -- Health aspects, Health, Measurement, Risk factors, Health aspects
Abstract

Introduction Evidence from several sources suggests that infection of the lower respiratory tract in early childhood may impair lung function in adult life and lead to respiratory symptoms. Follow up [...]

Published
1991

46. The effect of maternal anaemia and iron deficiency on the ratio of fetal weight to placental weight

Author

Godfrey, K.M., Redman, C.W.G., Barker, D.J.P., and Osmond, C.

Subjects
Prenatal influences -- Physiological aspects, Anemia in pregnancy -- Physiological aspects, Birth weight, Low -- Physiological aspects, Hypertension -- Risk factors, Placenta -- Measurement, Health
Abstract

Studies have shown that low birth weight is associated with the development of hypertension, or high blood pressure, in adult life. In one study, patients with the highest blood pressures were found to have birth weights lower than expected in relation to weights of the placenta, the tissue that provides nutrition to the fetus during pregnancy. The prenatal influences, or conditions during pregnancy, that contribute to a disproportion between the weights of the fetus and the placenta are not known, but may include nutrition and smoking. This study assessed the maternal factors that contribute to a large placental weight and high ratio of placental weight to birth weight, and influence the development of hypertension in adulthood. The study involved 8,684 pregnant women who gave birth between January 1987 and January 1989. The conditions associated with large placental weight and/or high ratios of placental weight to birth weight included low levels of maternal hemoglobin, the oxygen-carrying pigment of red blood cells; large declines in mean cell volume, a measure of the volume, or size, of individual blood cells; anemia, a decrease in red blood cells; and increased weight of the mother, indicated by the body mass index. Smoking was associated with low placental weight, but not with increased placental weight to birth weight ratios. These findings show that anemia and iron deficiency may contribute to the development of increased placental weight and increased ratios of placental weight to birth weight. In addition, the results suggest that nutritional factors influence the disproportion between placental weight and fetal growth. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

47. How long should catheter-acquired urinary tract infection in women be treated? A randomized controlled study

Author

Harding, Godfrey K.M., Nicolle, Lindsay E., Ronald, Allan R., Preiksaitis, Jutta K., Forward, Kevin R., Low, Donald E., and Cheang, Mary

Subjects
Women -- Diseases, Urinary tract infections -- Drug therapy, Urinary catheterization -- Complications, Antibiotics -- Evaluation, Health
Abstract

The most common infections acquired by hospitalized patients are urinary tract infections, and 80 percent of these are associated with the use of bladder catheters to collect urine. These catheters are inserted and maintained in as sterile a fashion as possible, but they predispose patients to infection. Little useful data exist on how to treat these catheter-associated infections, if at all. A group of 119 women with asymptomatic, catheter-associated urinary tract infections were randomly assigned to receive either no treatment, one dose of the antibiotic trimethoprim-sulfamethoxazole, or 10 days of that same antibiotic, and all were followed with a series of urine cultures to assess the efficacy of the various regimens. In addition, a group of 32 women with infections and symptoms that suggested that the infections were limited to the lower urinary tract (the bladder) were assigned to receive either one dose or 10 days of trimethoprim-sulfamethoxazole, and 10 patients whose infections probably involved the upper urinary tract (the kidneys) received 10 days of the antibiotic. The results of these studies suggested that 36 percent of those without symptoms who received no treatment had resolution of their infections spontaneously, while a smaller group of them developed symptoms without therapy. Among the asymptomatic patients who were treated with the antibiotic, there was no significant difference in the cure rate between those who had received a single dose and those who were treated for 10 days. Similarly, those with symptomatic lower tract infection responded equally to either one dose or 10 days of trimethoprim-sulfamethoxazole. When the patients were divided into those who were under and those over 65 years old, a clear difference in efficacy of the various regimens was observed. Older women had far less spontaneous clearance of bacteria without treatment, and did not respond as well to single-dose therapy as to 10 day courses. Even those older women treated with 10 days of antibiotic had less frequent cures than those who were under 65 (61 percent versus 88 percent) who received only a single dose. The conclusions of the study are that urinary tract infections resulting from the presence of indwelling bladder catheters should be treated, with single-dose therapy performing as well as 10-day regimens in those under 65. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

48. Asymptomatic bacteriuria: which patients should be treated?

Author

Zhanel, George C., Harding, Godfrey K.M., and Guay, David R.P.

Subjects
Bacteria in the urine -- Care and treatment, Bacteria in the urine -- Drug therapy, Health
Abstract

Asymptomatic bacteriuria is the presence of bacteria in the urine without accompanying symptoms of illness. Although it is common in both community nursing homes and hospitals, there is limited knowledge about the complications of asymptomatic bacteriuria for various patient groups and medical disorders. After a review of the literature, it is recommended that newborns, preschool children, pregnant women, and men less than 60 years of age receive antibiotic therapy for asymptomatic bacteriuria. In addition, antimicrobial agents are recommended for patients with abnormal urinary tracts, and for patients undergoing procedures involving the insertion of instruments into the genitourinary tract. Treatment with antibacterial agents is not recommended for school-age children, nonpregnant or young women, elderly persons with normal urinary tracts, or patients with long-term indwelling catheters, such as cancer patients receiving chemotherapy. It is not clear whether antimicrobial agents should be given to patients with short-term indwelling catheters or ileal conduits, a surgical connection between the small intestine and an opening in the abdominal wall. Because little is known about the outcome of asymptomatic bacteriuria in various patient populations, antimicrobial treatment of this infection is controversial. Hence these recommendations should not necessarily be accepted as standards of practice. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1990

50. Associations of Maternal Vitamin B12 Concentration in Pregnancy With the Risks of Preterm Birth and Low Birth Weight: A Systematic Review and Meta-Analysis of Individual Participant Data

Author

Rogne, T., Tielemans, M.J., Chong, M.F., Yajnik, C.S., Krishnaveni, G.V., Poston, L., Jaddoe, V.W., Steegers, E.A., Joshi, S., Chong, Y.S., Godfrey, K.M., Yap, F., Yahyaoui, R., Thomas, T., Hay, G., Hogeveen, M., Demir, A., Saravanan, P., Skovlund, E., Martinussen, M.P., Jacobsen, G.W., Franco, O.H., Bracken, M.B., Risnes, K.R., Rogne, T., Tielemans, M.J., Chong, M.F., Yajnik, C.S., Krishnaveni, G.V., Poston, L., Jaddoe, V.W., Steegers, E.A., Joshi, S., Chong, Y.S., Godfrey, K.M., Yap, F., Yahyaoui, R., Thomas, T., Hay, G., Hogeveen, M., Demir, A., Saravanan, P., Skovlund, E., Martinussen, M.P., Jacobsen, G.W., Franco, O.H., Bracken, M.B., and Risnes, K.R.

Abstract

Item does not contain fulltext, Vitamin B12 (hereafter referred to as B12) deficiency in pregnancy is prevalent and has been associated with both lower birth weight (birth weight <2,500 g) and preterm birth (length of gestation <37 weeks). Nevertheless, current evidence is contradictory. We performed a systematic review and a meta-analysis of individual participant data to evaluate the associations of maternal serum or plasma B12 concentrations in pregnancy with offspring birth weight and length of gestation. Twenty-two eligible studies were identified (11,993 observations). Eighteen studies were included in the meta-analysis (11,216 observations). No linear association was observed between maternal B12 levels in pregnancy and birth weight, but B12 deficiency (<148 pmol/L) was associated with a higher risk of low birth weight in newborns (adjusted risk ratio = 1.15, 95% confidence interval (CI): 1.01, 1.31). There was a linear association between maternal levels of B12 and preterm birth (per each 1-standard-deviation increase in B12, adjusted risk ratio = 0.89, 95% CI: 0.82, 0.97). Accordingly, B12 deficiency was associated with a higher risk of preterm birth (adjusted risk ratio = 1.21, 95% CI: 0.99, 1.49). This finding supports the need for randomized controlled trials of vitamin B12 supplementation in pregnancy.

Published
2017

Catalog

Books, media, physical & digital resources
See catalog results