MATERNAL PRE-PREGNANCY BODY MASS INDEX, MACROSOMIA, AND MENTAL HEALTH IN CHILDREN AND ADOLESCENTS

Van, Lieshout J Ryan

10 1900

<p><strong>Objectives: </strong>To examine associations between macrosomia, maternal body mass index (BMI) during pregnancy, and psychopathology in youth, and to determine if these are due to prenatal environmental exposures or confounding variables.</p> <p><strong>Methods: </strong>Study 1 reviewed studies examining associations between macrosomia and mental health. Data from the Ontario Child Health Study (OCHS) were then used to explore these links in youth (Study 2). A second review summarized studies assessing associations between maternal pregnancy BMI and psychopathology in offspring (Study 3). Data from the Western Australia Pregnancy Cohort were then used to quantify associations between maternal pre-pregnancy BMI and child behaviour at age 1 and 2 (Study 4), and from 5-17 years of age (Study 5).</p> <p><strong>Results: </strong>Seven of the 15 studies that had examined associations between macrosomia and psychopathology supported a link. In the OCHS, youth born macrosomic had elevated externalizing scores compared those born at appropriate birth weights. Eight of 12 studies suggested that links exist between elevated maternal BMI during pregnancy and psychopathology in offspring. Maternal pre-pregnancy BMI was positively associated with offspring externalizing problems from age 2 to 17 and linked to less favourable trajectories of internalizing symptoms from 5-17. These findings persisted despite adjustment for confounders.</p> <p><strong>Conclusions: </strong>Youth born macrosomic have elevated levels of externalizing symptoms, though a more robust association was noted with maternal pre-pregnancy BMI. The data comprising this thesis suggest that associations between macrosomia/maternal BMI and externalizing and internalizing problems in youth may be due to intrauterine exposures rather than confounding variables.</p> / Doctor of Philosophy (PhD)

Maternal

Pre-Pregnancy

Body Mass Index

Macrosomia

Mental Disorders

Child

Epidemiology

Mental Disorders

Neurosciences

Psychiatric and Mental Health

Psychological Phenomena and Processes

Epidemiology

Neonatal morbidity among macrosomic infants in the James Bay Cree population of northern Quebec

Trevors, Tanya.

January 2001

No description available.

Cree Indians -- James Bay Region.

Fetal Macrosomia -- Quebec.

Birth weight -- James Bay Region.

Alterações Metabólicas 6-11 anos pós nascimento em filhos de mães com síndrome metabólica na gestação

Camargo, Lucas Pontes de

January 2019

Orientador: Carlos Antonio Negrato / Resumo: Objetivo: Avaliar a exposição à síndrome metabólica (SM) pré-gestacional e seus efeitos nos desfechos perinatais (crianças grandes para a idade gestacional, macrossomicos e nascimento pré-termo) e no risco a curto e longo prazo para o desenvolvimento de SM e repercussões metabólicas em filhos de população de baixa renda de mãe brasileira. Desenho do estudo: Esta análise não planejada e exploratória inclui uma coorte de pares de mães-filhos diagnosticados e tratados no Centro de Pesquisa em Diabetes Perinatal - Hospital Universitário da UNESP, Brasil, de 2004 a 2011. Este estudo avaliou mulheres com diabetes mellitus gestacional anterior e o risco de desenvolver diabetes tipo 2 após 6-11 anos após o parto e os dados foram coletados de fevereiro de 2016 a julho de 2018. Mães e bebês (n = 152) foram selecionados como pares e um estudo de acompanhamento foi conduzido como análise de dados secundários dos efeitos da síndrome metabólica pré-gravidez. Exames de acompanhamento, incluindo a materna e a prole, foram realizados entre 0 e 2 anos e entre 6 e 11 anos após o parto. Todas as análises foram realizadas usando o SAS para windows, v.9.4. Em todos os testes, foi utilizado o nível de significância de 5% ou o valor p correspondente. Resultados: A prevalência de SM pré-gravidez foi de 9,1%, contribuindo para a ocorrência de LGA, crinaças macrossômicos e prematuros ao nascer. Nossos resultados confirmaram que as mães com SM pré-gestacional apresentaram correlação (p <0,0001) entre a ... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Objective: To assess the pre-pregnancy metabolic syndrome (MetS) exposure and its effects on the perinatal outcomes (large-for-gestational age infants, macrosomic and preterm birth) and on short and long-term risk for the development of MetS and metabolic repercussions among offspring of low income population of Brazilian mother. Study design: This unplanned, exploratory analysis includes a cohort of pairs of mother-offspring diagnosed and treated in the Perinatal Diabetes Research Center-University Hospital-UNESP, Brazil from 2004-2011. This study evaluated women with previous gestational diabetes mellitus and the risk of developing type 2 diabetes after 6-11 years after delivery and the data was collected from February 2016 to July 2018. Mothers and infants (n=152) were selected as pairs and a follow up study was conducted as secondary data analysis of the effects of pre-pregnancy MetS. Follow-up examinations, including maternal and offspring were performed at 0-2 years and from 6-11 years after delivery. All analyzes were performed using SAS for windows, v.9.4. In all tests the significance level of 5% or the corresponding p-value was used. Results: The prevalence of pre-pregnancy MetS was 9.1%, a contributor for the occurrence LGA, macrosomic infants and preterm at birth. Our results confirmed that, the pre-pregnancy MetS mothers had correlation (p<0.0001) between the hip circumference, waist circumference and weight which were also directly leading to higher levels (p<0.... (Complete abstract click electronic access below) / Mestre

Síndrome metabólica.

resultados da gravidez

Grande para idade gestacional

Trabalho de parto prematuro.

Macrossomia

cardiovascular

Avaliação.

Obesidade.

Metabolic Syndrome

pregnancy outcomes

large for gestational age

preterm birth

macrosomia

Lançamento tributário.

obesity

Estimativa do peso do recem-nascido por meio de medidas ultrassonograficas bidimensionais e do volume da coxa fetal / Birth weight precition by two-dimensional ultrasound measurements and fetal thigh volume

Bennini Junior, João Renato, 1978-

27 November 2018

Orientadores: Cleisson Fabio Andrioli Peralta, Ricardo Barini / Dissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas / Made available in DSpace on 2018-11-27T11:44:05Z (GMT). No. of bitstreams: 1 BenniniJunior_JoaoRenato_M.pdf: 1809698 bytes, checksum: 399e6ab502353af527e35953428d5e09 (MD5) Previous issue date: 2009 / Resumo: Introdução: Alguns estudos demonstram que a predição do peso fetal usando a volumetria dos membros fetais é mais precisa do que quando se usam medidas bidimensionais (2D). Até hoje, somente o método multiplanar foi utilizado para a volumetria dos membros fetais. Desta forma, a utilidade do método rotacional (VOCAL®) para este fim nunca foi testada. Objetivos: Avaliar as variabilidades intra e interobservadores e a concordância entre as medidas do volume da coxa fetal realizadas com os métodos multiplanar e VOCAL®. Comparar as acurácias das fórmulas com medidas do volume da coxa fetal com as acurácias das fórmulas com medidas 2D. Comparar as acurácias das fórmulas deste estudo com as acurácias das fórmulas já publicadas. Métodos: 210 pacientes foram avaliadas, formando um grupo para gerar as fórmulas (n = 150) e um grupo para validá-las (n = 60). Os pacientes utilizados para gerar as fórmulas também foram utilizados para avaliar as variabilidades intra e interobservadores e a concordância entre as medidas realizadas pelos métodos multiplanar e VOCAL®. Foram utilizadas análises de regressão polinomial para criar uma equação com medidas 2D, uma com o volume da coxa fetal medido pelo método multiplanar (CoxaM) e uma com o volume da coxa fetal medido pelo método VOCAL® (CoxaV). Utilizaram-se testes t de Student pareados para comparar as acurácias das equações deste estudo com as acurácias das fórmulas já publicadas. Foram utilizadas análises proporcionais de Bland e Altman para avaliar as variabilidades intra e interobservadores e a concordância entre as medidas realizadas pelos métodos multiplanar e VOCAL®. Resultados: A diferença média percentual entre as medidas pelos métodos multiplanar e VOCAL® foi de -0,04 com limites de concordância de 95% de -8,17 e 8,09. A diferença média percentual e os limites de concordância de 95% entre as medidas na avaliação das variabilidades intra e interobservadores foram -1,10 (-7,67 to 5,47) e 0,61 (-7,68 to 8,91) para o método VOCAL® e 1,03 (-6,35 to 8,41) e -0,68 (-11,42 to 10,06) para o multiplanar. As melhores fórmulas para cálculo do peso fetal estimado (PFE) foram: PFE = -562.824 + 11.962 x CA x CF + 0,009 x DBP² x CA² (CA: circunferência abdominal; CF: comprimento femoral; DBP: diâmetro biparietal); PFE = 1033.286 + 12.733 x CoxaM; PFE = 1025.383 + 12.775 x CoxaV. Tanto no grupo que gerou as fórmulas como no grupo utilizado para validá-las não houve diferença significativa entre as acurácias das fórmulas com medidas 2D ou tridimensionais (3D). Quando aplicadas nas pacientes deste estudo, as acurácias das fórmulas 2D e 3D já publicadas foram significativamente piores dos que as das novas fórmulas. Conclusões: Os métodos VOCAL® e multiplanar são intercambiáveis para a volumetria da coxa fetal. Possivelmente as maiores fontes de discrepâncias na estimativa do peso fetal são as diferenças fenotípicas entre as pacientes utilizadas para criar as fórmulas. Os dados deste estudo reforçam a necessidade de fórmulas específicas para cada população, independentemente do uso de medidas 2D ou 3D. / Abstract: Introduction: Some authors have demonstrated that the prediction of birth weight using fetal limb volumetry is more precise than with two-dimensional ultrasound (2DUS). To date, only the multiplanar method has been used for fetal limb volumetry, so the usefulness of the rotational technique (VOCALTM - Virtual Organ Computer- aided AnaLysis) for this purpose has never been tested. Objectives: To evaluate the repeatability, reproducibility and agreement of measurements performed with multiplanar and VOCALTM techniques for total fetal thigh volumetry. To compare the accuracies of birth-weight-predicting models with total fetal thigh volumetry with models derived from 2DUS parameters. To compare the performances of our new formulas with those of previously published equations. Methods: 210 patients were prospectively evaluated to compose a formula-generating group (n = 150) and a prospective-validation group (n = 60). The patients of the formula-generating group were also used to evaluate the repeatability, reproducibility and the agreement of the measurements of multiplanar and VOCALTM techiniques for fetal thigh volumetry. Polynomial regression analysis was performed in the formula-generating group to generate one equation with 2DUS measurements, one with fetal thigh volume measured by the multiplanar technique (ThiM) and one with fetal thigh volume obtained by the VOCALTM method (ThiV). Paired samples t-tests were used to compare the accuracies of our equations with those of previously published 2D and three-dimensional (3D) equations. Proportionate Bland and Altman analyses were performed to determine the agreement between the two methods and to evaluate intra- and inter-observer variability. Results: The mean percentage difference between measurements performed with the VOCALTM and multiplanar techniques was -0.04 and the 95% limits of agreement were -8.17 and 8.09. The mean percentage difference and 95% limits of agreement between paired measurements in the assessment of intra- and inter-observer variability were -1.10 (-7.67 to 5.47) and 0.61 (-7.68 to 8.91) for the VOCALTM technique and 1.03 (-6.35 to 8.41) and -0.68 (-11.42 to 10.06) for the multiplanar method. The formulas with the best fit for the prediction of birth weight (EFW) were: EFW = -562.824 + 11.962 x AC x FL + 0.009 x BPD² x AC² (AC: abdominal circumference; FL: femur length; BPD: biparietal diameter); EFW = 1033.286 + 12.733 x ThiM; EFW = 1025.383 + 12.775 x ThiV. For both the formula-generating and the rospective-validation groups, there was no significant difference between the accuracies of the new 2DUS and 3DUS models. When applied to our population, the accuracies of previously published 2DUS and 3DUS formulas were significantly worse than our models. Conclusions: The VOCALTM and multiplanar techniques can be used interchangeably for total fetal thigh volumetry. We believe that the greatest sources of discrepancies in estimation of birth weight are the phenotypic differences among patients used to create each of the formulas mentioned in this study. Our data reinforce the need for customized birth weight prediction formulas, regardless of whether 2DUS or 3DUS measurements are employed. / Mestrado / Tocoginecologia / Mestre em Tocoginecologia

Peso fetal

Feto - Desenvolvimento

Macrossomia fetal

Retardo do crescimento fetal

Ultra-sonografia pré-natal

Quadril

Imagem tridimensional

Tamanho do orgão

Fetal weight

Fetal development

Fetal macrosomia

Fetal growth retardation

Ultrasonography, Prenatal

Thigh

Imaging, Three-Dimensional

Organ size

Η εγκυμοσύνη μετά τη χειρουργική αντιμετώπιση της παχυσαρκίας : Θρεπτική κατάσταση και έκβαση / Pregnancy following bariatric surgery : Nutritional status and outcome

Mead, Nancy

09 October 2014

Nutritional status during pregnancy and the effects of nutritional deficiencies on pregnancy outcomes following bariatric surgery is an important issue that warrants further study. Objective: To investigate pregnancy outcomes and nutritional indices following restrictive and malabsorptive procedures. Setting: University Hospital, Greece. Methods: We investigated pregnancy outcomes of 113 women who gave birth to 150 children following biliopancreatic diversion (BPD), Roux-en-Y gastric bypass (RYGB) and sleeve gastrectomy (SG) between June 1994 and December 2011. Biochemical indices and pregnancy outcomes were compared among the different types of surgery and to overall 20-year hospital data, as well as to 56 pre-surgery pregnancies in 36 women of the same group. Results: Anemia was observed in 24.2% and 15.6% of pregnancies following BPD and RYGB, respectively. Vitamin B12 levels decreased postoperatively in all groups, with no further decrease during pregnancy; however, low levels were observed not only after BPD (11.7%) and RYGB (15.6%), but also after SG (13.3%). Folic acid levels increased. Serum albumin levels decreased in all groups during pregnancy, but hypoproteinemia was seen only after BPD. Neonates after BPD had significantly lower average birth weight without a higher frequency of low birth weight defined as less than 2500gr. A comparison of neonatal data between babies born before surgery (BS) and siblings born after surgery (AS) showed that AS newborns had lower average birth weight with no significant differences in body length or head circumference and no cases of macrosomia. Conclusions: Our study showed reasonably good pregnancy outcomes in this sample population following all types of bariatric surgery provided nutritional supplement guidelines are followed. Closer monitoring is required in pregnancies following malabsorptive procedures especially regarding protein nutrition. / Η θρεπτική κατάσταση κατά τη διάρκεια της εγκυμοσύνης και οι συνέπειες διατροφικών ανεπαρκειών στην έκβαση της, που ακολουθεί μια χειρουργική επέμβαση για κλινική σοβαρή παχυσαρκία αποτελεί θέμα που χρήζει περαιτέρω έρευνας. Σκοπός της συγκεκριμένης μελέτης ήταν η διερεύνηση της θρεπτικής κατάστασης και της έκβασης της εγκυμοσύνης, τόσο στις μητέρες όσο και στα νεογνά, σε γυναίκες που είχαν υποβληθεί στο παρελθόν σε περιοριστικές και δυσαπορροφητικές επεμβάσεις για κλινικά σοβαρή παχυσαρκία. Μελετήθηκαν 113 γυναίκες που γέννησαν 150 παιδιά μετά από χολοπαγκρεατική εκτροπή (BPD), Roux-en-Y γαστρική παράκαμψη (RYGB) και επιμήκη γαστρεκτομή μεταξύ Ιουνίου 1994 και Δεκεμβρίου 2011. Συγκρίθηκαν τα αποτελέσματα των θρεπτικών δεικτών και της έκβασης της εγκυμοσύνης μεταξύ των επεμβάσεων καθώς και με τα 20ετή στοιχεία γεννήσεων του νοσοκομείου μας και τα αποτελέσματα από 56 προεγχειρητικές εγκυμοσύνες σε 36 από τις ίδιες γυναίκες. Αναιμία παρατηρήθηκε σε 24.2% και 15.6% των κυήσεων μετά από BPD και RYGB, αντίστοιχα. Τα επίπεδα της βιταμίνης B12 μειώθηκαν μετεγχειρητικά σε όλες τις ομάδες, χωρίς περαιτέρω μείωση κατά τη διάρκεια της εγκυμοσύνης• όμως, χαμηλά επίπεδα παρατηρήθηκαν σε κάποιες γυναίκες όχι μόνο μετά από BPD (11.7%) και RYGB (15.6%), αλλά και μετά από SG (13.3%). Τα επίπεδα του φυλλικού οξέος αυξήθηκαν μετεγχειρητικά και κατά τη διάρκεια της εγκυμοσύνης. Η τιμή της αλβουμίνης μειώθηκε σε όλες τις ομάδες κατά τη διάρκεια της εγκυμοσύνης, αλλά υποπρωτεϊναιμία παρατηρήθηκε μόνο μετά από BPD. Τα νεογνά μετά από BPD είχαν χαμηλότερο μέσο όρο βάρους γέννησης (p<0.05), χωρίς να υπάρχει μεγαλύτερη συχνότητα χαμηλού βάρους γέννησης (<2500gr). Η σύγκριση μεταξύ των νεογνών που γεννήθηκαν πριν και μετά το χειρουργείο έδειξε ότι τα νεογνά που γεννήθηκαν μετά είχαν χαμηλότερο βάρος (p<0.001) χωρίς σημαντικές διαφορές στη διάρκεια κύησης, στο μήκος ή στην περίμετρο της κεφαλής και καθόλου μακροσωμία. Συμπερασματικά, η δική μας μελέτη έδειξε σχετικά καλή θρεπτική κατάσταση και έκβαση στη εγκυμοσύνη μετά από όλους τους τύπους επεμβάσεων στη συγκεκριμένη πληθυσμιακή ομάδα εφόσον υπάρχει συστηματική παρακολούθηση και ακολουθούνται οι διατροφικές οδηγίες. Πιο στενή παρακολούθηση χρειάζεται μετά από δυσαπορροφητικές επεμβάσεις ιδιαίτερα ως προς το θέμα της πρωτεϊνικής θρέψης

Pregnancy

Bariatric surgery

Nutritional indices

Anemia

Vitamin B12

Folic acid

Protein malnutrition

Neonatal outcomes

Birth weight

Gestational age

Macrosomia

618.24

Εγκυμοσύνη

Θρεπτικές δείκτες

Αναιμία

Βιταμίνη Β12

Φυλλικό οξύ

Υποπρωτεΐναιμία

Έκβαση νεογνών

Βάρος γέννησης

Ηλικία κύησης

Μακροσωμία

Fatores clínicos, laboratoriais e expressão placentária de transportadores de glicose no diabetes melito gestacional: associação com a ocorrência de recém-nascido grande para idade gestacional / Clinical factors, laboratory and placental expression of glucose transporters in gestational diabetes mellitus: association with the occurrence of newborn large for gestational age

Tiago, Douglas Bernal

24 July 2013

O diabetes melito gestacional (DMG) está relacionado ao crescimento fetal exagerado. Entender a influência de fatores relacionados ao crescimento fetal auxilia na identificação dos fetos com maior risco de desvios da normalidade. Objetivo: comparar fatores clínicos, laboratoriais e a expressão placentária de transportadores de glicose segundo o crescimento fetal em pacientes com DMG. Método: Para análise dos fatores clínicos e laboratoriais foi realizado um estudo retrospectivo com 425 gestantes com DMG do Setor de Endocrinopatias da Divisão de Clínica Obstétrica do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo (HC FM-USP) no período de janeiro de 2003 a novembro de 2009. Para a análise da expressão placentária dos transportadores de glicose dos tipos 1 (GLUT1), 3 (GLUT3) e 4 (GLUT4) foram selecionados todos os casos de recém-nascidos grandes para idade gestacional (RNGIG) pareados com um caso controle de recém-nascido adequado para idade gestacional (RNAIG). Foram incluídas apenas gestações únicas e com DMG diagnosticado pelo teste de tolerância à glicose oral de 100 gramas, sem malformações fetais e com idade gestacional definida e confiável. Todas as gestantes realizaram dieta para diabetes, controle glicêmico diário e uso de insulina quando necessário. Os critérios de seguimento e tratamento seguiram rigorosamente as normas do Protocolo de Condutas do Setor de Endocrinopatias da Divisão de Clínica Obstétrica do HC-FMUSP. As gestantes foram divididas para análise dos dados em dois grupos: Fatores clínicos e laboratoriais com: 376 RNAIG e 49 RNGIG num total de 425 DMG. Expressão Placentária dos Transportadores de Glicose: 50 RNAIG e 44 RNGIG. Foram realizados testes de associação e médias das variáveis e relacionadas com os grupos de RNAIG e RNGIG. Resultados: Na análise univariada, dos fatores clínicos e laboratoriais, não houve diferenças entre os grupos quanto a: idade materna, antecedente familiar de diabetes, antecedente pessoal de hipertensão arterial, número de gestações, valores de glicemia de jejum e 1 hora no TTGO-100g, idade gestacional no parto, sexo do RN, tipo de parto e índice de Apgar no 1º e 5º minutos. Houve diferenças estatisticamente significativas entre os grupos quanto a: índice de massa corpórea pré-gestacional (p < 0,02); uso de insulina (p < 0,041); macrossomia anterior (p < 0,001); idade gestacional do diagnóstico do DMG (p < 0,001); glicemias de duas e três horas no TTGO-100g respectivamente com (p < 0,003) e (p < 0,026). Na análise de regressão logística foram considerados preditores independentes da ocorrência de RNGIG: o índice de massa corpórea pré - gestacional, a macrossomia anterior, aidade gestacional do diagnóstico do DMG e a glicemia de duas horas após sobrecarga de 100 gramas. Em relação a expressão dos transportadores de glicose não diferiram entre os grupos em relação a expressão de GLUT1 na decídua, GLUT3 na decídua e vilosidades e GLUT4 na decídua e vilosidades. Houve diferença entre os grupos quanto à: a expressão do GLUT1 nas vilosidades. Conclusões: O índice de massa corpórea pré - gestacional, a macrossomia anterior, a idade gestacional do diagnóstico do DMG e a glicemia de duas horas após sobrecarga de 100 gramas foram preditores da ocorrência de RNGIG. A expressão de GLUT1 nas vilosidades coriônicas teve relação com a ocorrência de RNGIG / Gestational diabetes mellitus (GDM) is related to excessive fetal growth. Knowing the influence of factors related to fetal growth assists in the identification of fetuses at high risk of deviations from normality. Objective: To compare clinical and laboratory tests and the placental expression of glucose transporters according to fetal growth in patients with GDM. Method: A retrospective study of clinical and laboratory factors related with large for gestational age newborns, included 425 pregnant women with GDM was carried out at Sector Endocrine Clinic of Obstetrics Hospital of the School of Medicine, University of São Paulo (HC-FMUSP), between January 2003 to November 2009. For the analysis of placental expression of glucose transporters types 1 (GLUT1), 3 (GLUT3) and 4 (GLUT4) were selected all cases of newborns large for gestational age (LGA) paired with a case control newly born appropriate for gestational age (AGA). We included only patients with singleton pregnancies and GDM diagnosed by OGTT-100g, with newborns without malformations and birth weight classified as adequate or large for gestational age. All pregnant women received diet for diabetes, daily glycemic control and insulin when necessary. The criteria for monitoring and treatment followed strictly the standards of Conduct Protocol Endocrine Obstetric Clinic of the Clinic Hospital, School of Medicine, University of São Paulo. The pregnancies were divided for analysis into two groups: 376 cases of newborns AGA and 49 cases of newborns LGA. Data were analyzed and considered the probability value p <0.05. Results: In the univariate analysis of clinical and laboratory factors, there were no differences between the groups regarding maternal age, family history of diabetes, personal history of hypertension, number of pregnancies, blood fasting glucose and 1 hour in- OGTT 100g, gestational age at delivery, gender of the newborn, type of delivery, Apgar score at 1st and 5th minutes. There were statistically significant differences between the groups regarding: body mass index before pregnancy (p <0.02), insulin (p <0.041), previous macrosomia (p <0.001), gestational age at diagnosis of GDM (p <0.001), blood glucose levels two and three hours at 100 g OGTT, respectively, with (p <0.003) (p <0.026). In logistic regression analysis were considered independent predictors of the occurrence of LGA: body mass index before pregnancy, previous macrosomia gestational age at diagnosis of GDM and two hours after glucose overload 100 grams. Regarding the expression of glucose transporters, the groups did not differ regarding the expression of GLUT1 in the decidua, GLUT3 in the decidua and villi and GLUT4 in the decidua and villi. There were differences between the groups regarding the expression of GLUT1 in the villi. Conclusions: The body mass index before pregnancy, previous macrosomia, gestational age of diagnosis of GDM and two hours after glucose overload 100 grams were predictors of the occurrence of LGA. The expression of GLUT1 in chorionic villi was related to the occurrence of LGA newborn

Body mass index

Case-control studies

Diabetes gestacional/diagnóstico

Diabetes gestational/diagnosis

Estudos de casos e controles

Fatores de risco

Fetal macrosomia/metabolism

Fetal weight/physiology

Índice de massa corporal

Infant newborn/growth & development

Macrossomia fetal/metabolismo

Peso fetal/fisiologia

Risk factors

Sodium-glucose transport proteins

Fatores clínicos, laboratoriais e expressão placentária de transportadores de glicose no diabetes melito gestacional: associação com a ocorrência de recém-nascido grande para idade gestacional / Clinical factors, laboratory and placental expression of glucose transporters in gestational diabetes mellitus: association with the occurrence of newborn large for gestational age

Douglas Bernal Tiago

24 July 2013

O diabetes melito gestacional (DMG) está relacionado ao crescimento fetal exagerado. Entender a influência de fatores relacionados ao crescimento fetal auxilia na identificação dos fetos com maior risco de desvios da normalidade. Objetivo: comparar fatores clínicos, laboratoriais e a expressão placentária de transportadores de glicose segundo o crescimento fetal em pacientes com DMG. Método: Para análise dos fatores clínicos e laboratoriais foi realizado um estudo retrospectivo com 425 gestantes com DMG do Setor de Endocrinopatias da Divisão de Clínica Obstétrica do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo (HC FM-USP) no período de janeiro de 2003 a novembro de 2009. Para a análise da expressão placentária dos transportadores de glicose dos tipos 1 (GLUT1), 3 (GLUT3) e 4 (GLUT4) foram selecionados todos os casos de recém-nascidos grandes para idade gestacional (RNGIG) pareados com um caso controle de recém-nascido adequado para idade gestacional (RNAIG). Foram incluídas apenas gestações únicas e com DMG diagnosticado pelo teste de tolerância à glicose oral de 100 gramas, sem malformações fetais e com idade gestacional definida e confiável. Todas as gestantes realizaram dieta para diabetes, controle glicêmico diário e uso de insulina quando necessário. Os critérios de seguimento e tratamento seguiram rigorosamente as normas do Protocolo de Condutas do Setor de Endocrinopatias da Divisão de Clínica Obstétrica do HC-FMUSP. As gestantes foram divididas para análise dos dados em dois grupos: Fatores clínicos e laboratoriais com: 376 RNAIG e 49 RNGIG num total de 425 DMG. Expressão Placentária dos Transportadores de Glicose: 50 RNAIG e 44 RNGIG. Foram realizados testes de associação e médias das variáveis e relacionadas com os grupos de RNAIG e RNGIG. Resultados: Na análise univariada, dos fatores clínicos e laboratoriais, não houve diferenças entre os grupos quanto a: idade materna, antecedente familiar de diabetes, antecedente pessoal de hipertensão arterial, número de gestações, valores de glicemia de jejum e 1 hora no TTGO-100g, idade gestacional no parto, sexo do RN, tipo de parto e índice de Apgar no 1º e 5º minutos. Houve diferenças estatisticamente significativas entre os grupos quanto a: índice de massa corpórea pré-gestacional (p < 0,02); uso de insulina (p < 0,041); macrossomia anterior (p < 0,001); idade gestacional do diagnóstico do DMG (p < 0,001); glicemias de duas e três horas no TTGO-100g respectivamente com (p < 0,003) e (p < 0,026). Na análise de regressão logística foram considerados preditores independentes da ocorrência de RNGIG: o índice de massa corpórea pré - gestacional, a macrossomia anterior, aidade gestacional do diagnóstico do DMG e a glicemia de duas horas após sobrecarga de 100 gramas. Em relação a expressão dos transportadores de glicose não diferiram entre os grupos em relação a expressão de GLUT1 na decídua, GLUT3 na decídua e vilosidades e GLUT4 na decídua e vilosidades. Houve diferença entre os grupos quanto à: a expressão do GLUT1 nas vilosidades. Conclusões: O índice de massa corpórea pré - gestacional, a macrossomia anterior, a idade gestacional do diagnóstico do DMG e a glicemia de duas horas após sobrecarga de 100 gramas foram preditores da ocorrência de RNGIG. A expressão de GLUT1 nas vilosidades coriônicas teve relação com a ocorrência de RNGIG / Gestational diabetes mellitus (GDM) is related to excessive fetal growth. Knowing the influence of factors related to fetal growth assists in the identification of fetuses at high risk of deviations from normality. Objective: To compare clinical and laboratory tests and the placental expression of glucose transporters according to fetal growth in patients with GDM. Method: A retrospective study of clinical and laboratory factors related with large for gestational age newborns, included 425 pregnant women with GDM was carried out at Sector Endocrine Clinic of Obstetrics Hospital of the School of Medicine, University of São Paulo (HC-FMUSP), between January 2003 to November 2009. For the analysis of placental expression of glucose transporters types 1 (GLUT1), 3 (GLUT3) and 4 (GLUT4) were selected all cases of newborns large for gestational age (LGA) paired with a case control newly born appropriate for gestational age (AGA). We included only patients with singleton pregnancies and GDM diagnosed by OGTT-100g, with newborns without malformations and birth weight classified as adequate or large for gestational age. All pregnant women received diet for diabetes, daily glycemic control and insulin when necessary. The criteria for monitoring and treatment followed strictly the standards of Conduct Protocol Endocrine Obstetric Clinic of the Clinic Hospital, School of Medicine, University of São Paulo. The pregnancies were divided for analysis into two groups: 376 cases of newborns AGA and 49 cases of newborns LGA. Data were analyzed and considered the probability value p <0.05. Results: In the univariate analysis of clinical and laboratory factors, there were no differences between the groups regarding maternal age, family history of diabetes, personal history of hypertension, number of pregnancies, blood fasting glucose and 1 hour in- OGTT 100g, gestational age at delivery, gender of the newborn, type of delivery, Apgar score at 1st and 5th minutes. There were statistically significant differences between the groups regarding: body mass index before pregnancy (p <0.02), insulin (p <0.041), previous macrosomia (p <0.001), gestational age at diagnosis of GDM (p <0.001), blood glucose levels two and three hours at 100 g OGTT, respectively, with (p <0.003) (p <0.026). In logistic regression analysis were considered independent predictors of the occurrence of LGA: body mass index before pregnancy, previous macrosomia gestational age at diagnosis of GDM and two hours after glucose overload 100 grams. Regarding the expression of glucose transporters, the groups did not differ regarding the expression of GLUT1 in the decidua, GLUT3 in the decidua and villi and GLUT4 in the decidua and villi. There were differences between the groups regarding the expression of GLUT1 in the villi. Conclusions: The body mass index before pregnancy, previous macrosomia, gestational age of diagnosis of GDM and two hours after glucose overload 100 grams were predictors of the occurrence of LGA. The expression of GLUT1 in chorionic villi was related to the occurrence of LGA newborn

Diabetes gestacional/diagnóstico

Estudos de casos e controles

Fatores de risco

Índice de massa corporal

Macrossomia fetal/metabolismo

Peso fetal/fisiologia

Body mass index

Case-control studies

Diabetes gestational/diagnosis

Fetal macrosomia/metabolism

Fetal weight/physiology

Infant newborn/growth & development

Risk factors

Sodium-glucose transport proteins

An Examination of Maternal Contributors and Potential Modifiers of Fetal Growth in Pregnancy

Ferraro, Zachary Michael

01 May 2012

A greater understanding of critical periods of body weight regulation, including pregnancy, may aid in efforts to optimize weight management strategies for the mother and her baby. The gestational period has been implicated to play, in the child, a vital role in the developmental origins of obesity and other cardiometabolic diseases later in life. Therefore, we initially examined existing literature on the role of maternal obesity and its link to pediatric obesity and documented the known underlying physiological mechanisms responsible for this relationship while suggesting potential intervention targets that may improve maternal-fetal outcomes. In a second paper, we aimed to quantify maternal predictors of large for gestational age (LGA) neonates in the Ottawa and Kingston (OaK) birth cohort with specific hypotheses verifying the independent contribution of maternal prepregnancy body mass index (BMI) and excessive gestational weight gain (GWG) to fetal overgrowth. This paper also highlights the clinical utility of the revised 2009 Institute of Medicine GWG guidelines and discusses the potential role of physiological factors underlying the observed associations between BMI, excessive GWG and LGA neonates. As a follow-up to our population-level analysis (i.e., OAK cohort), papers three and four highlight how the insulin-like growth factor (IGF) axis, a vital regulator of growth and development, may be compromised at the molecular level in cases of maternal obesity (paper 3) and excessive GWG (paper 4). In paper 3 we show that maternal obesity is associated with attenuated expression of IGF binding protein-4 (IGFBP4) in umbilical cord blood and discuss how this may preferentially promote fetal adipogenesis. The effects of excessive GWG on IGF axis protein expression are addressed in paper four where we show that excessive weight gain during pregnancy is associated with increased expression of IGFBP3 in maternal circulation in normoglycemic term pregnancies. In this paper we discuss the potential inhibitory role of IGFBP3 on adipogenesis and how it relates to glucose intolerance during pregnancy. Recognizing that both obesity and excessive GWG can alter physiological processes in mother and her baby, appropriate evidence-based interventions are warranted to best optimize outcomes. In paper five, we discuss the results of a study which sought to assess patient information channels and knowledge of nutrition and physical activity during pregnancy with the intent that these findings be applied to best design efficacious strategies that cater to the needs of our target group of pregnant women. In our analysis we show that the majority of pregnant women studied would be willing to participate in a lifestyle intervention for their own personal health and that of their child. Of great interest was the observation that most women were not informed of the importance of pregnancy-specific energy intake, or made aware of their own healthy GWG targets. Additionally, many of the respondents reported receiving no information pertaining to appropriate physical activity recommendations; despite the fact that the vast majority of participants consider this lifestyle modality to be safe during their pregnancy. Finally in paper six, we build on the results of our previous work and evaluate the risks and benefits of physical activity during pregnancy on maternal-fetal outcomes through a review of the literature and note that engaging in non-sedentary pursuits during gestation may aid in maternal weight regulation, protect against metabolic disorders and optimize neonatal birth weight and body composition. Overall, the collective nature of the papers presented in this dissertation provides qualitative and quantitative evidence to support not only the complexity of body weight regulation in the mother and her baby, but also highlights potential avenues for intervention that may improve maternal-fetal outcomes during this critical period.

Maternal obesity

Gestational weight gain

fetal

macrosomia

insulin-like growth factor

physical activity

exercise

developmental origins of disease

metabolism

insulin resistance

adiposity

pregnancy

lifestyle intervention

pediatric obesity

large for gestational age

fetal programming

nutrition

developmental programming

plasticity

An Examination of Maternal Contributors and Potential Modifiers of Fetal Growth in Pregnancy

Ferraro, Zachary Michael

01 May 2012

A greater understanding of critical periods of body weight regulation, including pregnancy, may aid in efforts to optimize weight management strategies for the mother and her baby. The gestational period has been implicated to play, in the child, a vital role in the developmental origins of obesity and other cardiometabolic diseases later in life. Therefore, we initially examined existing literature on the role of maternal obesity and its link to pediatric obesity and documented the known underlying physiological mechanisms responsible for this relationship while suggesting potential intervention targets that may improve maternal-fetal outcomes. In a second paper, we aimed to quantify maternal predictors of large for gestational age (LGA) neonates in the Ottawa and Kingston (OaK) birth cohort with specific hypotheses verifying the independent contribution of maternal prepregnancy body mass index (BMI) and excessive gestational weight gain (GWG) to fetal overgrowth. This paper also highlights the clinical utility of the revised 2009 Institute of Medicine GWG guidelines and discusses the potential role of physiological factors underlying the observed associations between BMI, excessive GWG and LGA neonates. As a follow-up to our population-level analysis (i.e., OAK cohort), papers three and four highlight how the insulin-like growth factor (IGF) axis, a vital regulator of growth and development, may be compromised at the molecular level in cases of maternal obesity (paper 3) and excessive GWG (paper 4). In paper 3 we show that maternal obesity is associated with attenuated expression of IGF binding protein-4 (IGFBP4) in umbilical cord blood and discuss how this may preferentially promote fetal adipogenesis. The effects of excessive GWG on IGF axis protein expression are addressed in paper four where we show that excessive weight gain during pregnancy is associated with increased expression of IGFBP3 in maternal circulation in normoglycemic term pregnancies. In this paper we discuss the potential inhibitory role of IGFBP3 on adipogenesis and how it relates to glucose intolerance during pregnancy. Recognizing that both obesity and excessive GWG can alter physiological processes in mother and her baby, appropriate evidence-based interventions are warranted to best optimize outcomes. In paper five, we discuss the results of a study which sought to assess patient information channels and knowledge of nutrition and physical activity during pregnancy with the intent that these findings be applied to best design efficacious strategies that cater to the needs of our target group of pregnant women. In our analysis we show that the majority of pregnant women studied would be willing to participate in a lifestyle intervention for their own personal health and that of their child. Of great interest was the observation that most women were not informed of the importance of pregnancy-specific energy intake, or made aware of their own healthy GWG targets. Additionally, many of the respondents reported receiving no information pertaining to appropriate physical activity recommendations; despite the fact that the vast majority of participants consider this lifestyle modality to be safe during their pregnancy. Finally in paper six, we build on the results of our previous work and evaluate the risks and benefits of physical activity during pregnancy on maternal-fetal outcomes through a review of the literature and note that engaging in non-sedentary pursuits during gestation may aid in maternal weight regulation, protect against metabolic disorders and optimize neonatal birth weight and body composition. Overall, the collective nature of the papers presented in this dissertation provides qualitative and quantitative evidence to support not only the complexity of body weight regulation in the mother and her baby, but also highlights potential avenues for intervention that may improve maternal-fetal outcomes during this critical period.

Maternal obesity

Gestational weight gain

fetal

macrosomia

insulin-like growth factor

physical activity

exercise

developmental origins of disease

metabolism

insulin resistance

adiposity

pregnancy

lifestyle intervention

pediatric obesity

large for gestational age

fetal programming

nutrition

developmental programming

plasticity

An Examination of Maternal Contributors and Potential Modifiers of Fetal Growth in Pregnancy

Ferraro, Zachary Michael

January 2012

A greater understanding of critical periods of body weight regulation, including pregnancy, may aid in efforts to optimize weight management strategies for the mother and her baby. The gestational period has been implicated to play, in the child, a vital role in the developmental origins of obesity and other cardiometabolic diseases later in life. Therefore, we initially examined existing literature on the role of maternal obesity and its link to pediatric obesity and documented the known underlying physiological mechanisms responsible for this relationship while suggesting potential intervention targets that may improve maternal-fetal outcomes. In a second paper, we aimed to quantify maternal predictors of large for gestational age (LGA) neonates in the Ottawa and Kingston (OaK) birth cohort with specific hypotheses verifying the independent contribution of maternal prepregnancy body mass index (BMI) and excessive gestational weight gain (GWG) to fetal overgrowth. This paper also highlights the clinical utility of the revised 2009 Institute of Medicine GWG guidelines and discusses the potential role of physiological factors underlying the observed associations between BMI, excessive GWG and LGA neonates. As a follow-up to our population-level analysis (i.e., OAK cohort), papers three and four highlight how the insulin-like growth factor (IGF) axis, a vital regulator of growth and development, may be compromised at the molecular level in cases of maternal obesity (paper 3) and excessive GWG (paper 4). In paper 3 we show that maternal obesity is associated with attenuated expression of IGF binding protein-4 (IGFBP4) in umbilical cord blood and discuss how this may preferentially promote fetal adipogenesis. The effects of excessive GWG on IGF axis protein expression are addressed in paper four where we show that excessive weight gain during pregnancy is associated with increased expression of IGFBP3 in maternal circulation in normoglycemic term pregnancies. In this paper we discuss the potential inhibitory role of IGFBP3 on adipogenesis and how it relates to glucose intolerance during pregnancy. Recognizing that both obesity and excessive GWG can alter physiological processes in mother and her baby, appropriate evidence-based interventions are warranted to best optimize outcomes. In paper five, we discuss the results of a study which sought to assess patient information channels and knowledge of nutrition and physical activity during pregnancy with the intent that these findings be applied to best design efficacious strategies that cater to the needs of our target group of pregnant women. In our analysis we show that the majority of pregnant women studied would be willing to participate in a lifestyle intervention for their own personal health and that of their child. Of great interest was the observation that most women were not informed of the importance of pregnancy-specific energy intake, or made aware of their own healthy GWG targets. Additionally, many of the respondents reported receiving no information pertaining to appropriate physical activity recommendations; despite the fact that the vast majority of participants consider this lifestyle modality to be safe during their pregnancy. Finally in paper six, we build on the results of our previous work and evaluate the risks and benefits of physical activity during pregnancy on maternal-fetal outcomes through a review of the literature and note that engaging in non-sedentary pursuits during gestation may aid in maternal weight regulation, protect against metabolic disorders and optimize neonatal birth weight and body composition. Overall, the collective nature of the papers presented in this dissertation provides qualitative and quantitative evidence to support not only the complexity of body weight regulation in the mother and her baby, but also highlights potential avenues for intervention that may improve maternal-fetal outcomes during this critical period.

Maternal obesity

Gestational weight gain

fetal

macrosomia

insulin-like growth factor

physical activity

exercise

developmental origins of disease

metabolism

insulin resistance

adiposity

pregnancy

lifestyle intervention

pediatric obesity

large for gestational age

fetal programming

nutrition

developmental programming

plasticity