Influence de l’alimentation hyperlipidique hypercholestérolémique sur l’expression génique embryonnaire et le développement de maladies à long terme : etudes sur le modèle lapin / Effect of hyperlipidic hypercholesterolemic diet on embryo genic expression and development of diseases at adult age : studies on rabbit model

Picone, Olivier

14 June 2011

Les problèmes de santé liés à l’alimentation hyperlipidique chez l’humain sont en constante progression. Or, une perturbation de l’environnement fœtal induit chez la descendance une susceptibilité plus grande à développer des maladies à l’âge adulte (DOHad : Developmental Origins of Health and Disease). L’objectif de ce travail de Thèse est d’évaluer, chez le lapin, les conséquences d’une alimentation hypercholestérolémique et hyperlipidique sur le développement embryonnaire, fœtal, et la survenue de troubles métaboliques à long terme.Nous avons nourri des lapines ad libitum avec un régime hypercholéstérolémique (0,2%) et hyperlipidique (8%) (HH) ou un régime témoin (C) à partir de l'âge de 10 (expérience 1) ou de 18 semaines (age de la mise à la reproduction, expérience 2). A la naissance, les portées ont été équilibrées et des croisements effectués pour différencier l'effet de l'alimentation de la mère pendant la gestation et pendant la lactation. Ainsi des lapereaux nés de mères HH ont été allaités par des mères C (groupe HH-C) ou HH (groupe HH-HH) et des lapereaux nés de mère C ont été allaités par des mères C (groupe C-C) ou HH (groupe C-HH). Au cours de l’expérience 1, un retard de croissance intra utérin (RCIU) significatif a été mis en évidence dès 9 jours de gestation par échographie dans le groupe HH (P<0,05). A la naissance, les laperaux étaient significativement plus légers (P<0,05). En raison d’un rattrapage pondéral rapide, il n’existait plus de différence significative au sevrage. Tous les lapins ont alors reçu un aliment témoin distribué ad libitum. A J176, il n’y avait pas de différence de poids entre les groupes HH-HH et HH-C, mais les animaux de ces deux groupes étaient significativement plus lourds que les groupes C-C and C-HH (P<0.05). De plus, la tension artérielle était plus élevée dans le groupe HH-HH par rapport à tous les autres groupes (P<0.05). Au cours de l’expérience 2, de tels effets physiologiques n’ont pas été observés. Les effets physiologiques n'ayant été observés que lorsque le régime avait été commencé avant la gestation, nous avons émis l'hypothèse que l'environnement maternel précoce avait été modifié, entrainant une perturbation du développement embryonnaire à l'origine des conséquences à long terme. l’expression des gènes au moment de la mise en route du génome embryonnaire a été étudié à l’aide d’une puce dédiée. L’analyse transcriptomique a permis de suggérer que certains transcrits étaient présents en quantités différentes. Nous avons montré par qRT-PCR que le régime HH induit une augmentation transitoire de la quantité de transcrit de l’adipophiline (présente à J2 mais pas à J5,5). L’analyse immunohistochimique montre une quantité plus importante de gouttelettes lipidiques localisées près du noyau dans les embryons issus de mères nourries par le régime HH à J5,5 comparé aux témoins. Ces résultats illustrent l’importance de la nutrition avant et pendant la gestation pour la determination de la croissance in utero et postnatale, ainsi que pour le développement de maladies métaboliques à long terme. La nutrition maternelle avant la gestation peut engendrer des modifications d’expression de gènes au moment de la transmission materno embryonnaire. / The prevalence of human health problems associated with high-fat diets continues to rise, as does the number of such problems known to be associated with this diet. Disruption of the fetal environment induces in progeny a greater susceptibility to developing diseases in adulthood (DOHad: Developmental Origins of Health and Disease). The objective of the work for this thesis was to assess in rabbits the consequences of a high-cholesterol and high-fat diet on embryonic and fetal development and on the onset of metabolic disorders in the long term.We fed rabbits ad libitum with a high-cholesterol (0.2%) and high-fat (8%) (HH) diet or a control (C) diet, starting at the age of 10 (experiment 1) or 18 weeks (age at which reproduction began, experiment 2).The litters were balanced at birth, and crossings were performed to differentiate the effect of the mother's food during gestation and during lactation. Accordingly, rabbits born to HH mothers were nursed by C (HH-C group) or HH (HH-HH) mothers and those born to C mothers were nursed either by C (C-C) or HH (C-HH) mothers. During experiment 1, ultrasound clearly showed significant intrauterine growth restriction (IUGR) beginning at 9 days of gestation in the HH group (P<0.05). At birth, these rabbits weighed significantly less than their C counterparts (P<0.05). Because of their rapid weight catch-up, the significant difference had disappeared at weaning. All the rabbits thereafter received control food distributed ad libitum. At D176, there was no difference in weight between the HH-HH and HH-C groups but the animals in both these groups were significantly heavier than those in the C-C and C-HH groups (P<0.05). Moreover, blood pressure was higher in the HH-HH group than in any of the other groups (P<0.05). These physiological effects were not observed during experiment 2. Because the physiological effects were observed only when the diet began before gestation, we hypothesized that the early maternal environment been modified, a change that resulted in disruption of embryo development with long-term consequences. We then used a specially designed chip to study gene expression at the maternal to embryonic transition. Transcriptomic analysis suggested that some transcripts were present in different quantities. We showed with qRT-PCR that the HH diet induced a transient augmentation in the quantity of adipophilin transcripts (present at D2 but not at D5.5). The immunohistochemical analysis on D5.5 showed a higher quantity of lipid droplets localized near the nucleus of embryos from mothers fed with the HH diet than in embryos of control mothers. These results illustrate the importance of nutrition before and during pregnancy in the determination of in utero and postnatal growth as well as in the development of metabolic diseases over the long term. Maternal nutrition before conception can engender modifications in gene expression at the moment of the maternal to embryonic transition.

Gestation

Echographie

PCR

Adipophiline

Embryon

Fœtus

Gestation

High-fat diet

Cholesterol

Embryo

Ultrasound,

PCR

Adipophilin

Effets sanitaires à long terme des stress de la Première Guerre mondiale / Long-term health effects of World War I stresses

Todd, Nicolas

10 October 2017

Cette thèse explore la Première Guerre mondiale comme modèle historique de stress psychologique subi dans l'enfance. L'Hypothèse d'Origine Développementale des Maladies (DOHaD) prévoit une susceptibilité accrue aux maladies chroniques à l'âge adulte des individus exposés à des événements traumatiques aux premiers stades du développement. Nous avons constitué une cohorte d'orphelins nés en 1914-1916, et ce grâce au statut de "pupilles de la Nation", créé par une loi de 1917 et accordé sur requête à tous les orphelins, quel que soit le statut socioéconomique de la famille. L'attribution du statut de pupille était inscrite en marge de l'acte de naissance. Les registres de naissance ont donc permis un recensement exhaustif de tous les pupilles nés dans les villes incluses ainsi qu'un suivi de la mortalité à l'âge adulte. Les actes de naissance de 7,250 pupilles ont été transcrits à ce jour. L'appel à la Base des Morts pour la France a fourni la date de décès du père, et donc sa position dans le calendrier de développement de l'enfant. Des matched non-orphans (MNOs) ont été sélectionnés dans les mêmes registres. Le critère d'intérêt était la longévité de ceux ayant atteint l'âge de 31 ans. Un écart orphelin - MNO de ~ 2.5 années a été trouvé en cas de perte prénatale du père, mais aucune différence n'a été mise en évidence dans le cas d'une perte postnatale. La conjonction de ces deux résultats suggère qu'un traumatisme in utero a un effet de programmation de la susceptibilité biologique à l'âge adulte assez fort pour altérer la longévité. / This thesis explores the First World War as a historical model in early life psychological stress. The Developmental Origins of Health and Disease (DOHaD) hypothesis predicts increased susceptibility to chronic diseases in adulthood for those exposed to an extreme psychological trauma in very early life. We collected vital information on French orphans born 1914-1916 thanks to the “pupille de la Nation” distinction, a legal status created in 1917 and granted upon request to all orphans. Notification of “adoption by the Nation” was by law inscribed on the birth certificate of a newly adopted child. Birth registers thus provided a census of all pupilles born in the included cities during the inclusion period as well as long-term mortality follow-up. The birth certificates of 7,250 pupilles have been digitized. Call to the Died for France Database enabled us to retrieve the paternal date of death. Matched non-orphans (MNOs) were drawn from the same birth registers. For each orphan, his MNO was therefore chosen born in the same district at the same time. The outcome of interest was longevity of those who survived to 31 y. An orphan-MNO difference in adult longevity of ~2.5 years was found for orphans who had lost their father before) birth (prenatal orphans), but no difference in adult longevity could be measured between postnatal orphans and their MNOs. These two results suggest early trauma in utero has programming effects on biological susceptibility in adulthood strong enough to alter longevity. The fact that no loss of lifespan was found in the case of a postnatal loss of father further suggests efficient buffers to early postnatal stress existed in French society.

Stress maternel

Première Guerre Mondiale

Cohorte historique

Pupilles de la Nation

Orphelins

Orphans

First World War

614.4

Risques épigénétiques de la procréation médicalement assistée : enjeux éthiques pour les parents, les futurs enfants et les professionnels de la santé

Roy, Marie-Christine

06 1900

La procréation médicalement assistée (PMA) permet à beaucoup d’individus infertiles de concevoir un enfant qui leur est génétiquement lié. Cependant, des données scientifiques émergentes suggèrent que la PMA pourrait entraîner des risques épigénétiques pour les futurs enfants. Conformément à l'hypothèse des origines développementales de la santé et des maladies, la PMA pourrait augmenter le risque de développer des maladies à apparition tardive par des mécanismes épigénétiques, car l’hyperovulation, les méthodes de fécondation et la culture embryonnaire pourraient nuire à la reprogrammation épigénétique de l'embryon. De tels risques épigénétiques soulèvent des enjeux éthiques pour toutes les parties prenantes: les futurs parents et enfants, les professionnels de la santé, et la société. Ce mémoire se concentre sur les questions éthiques soulevées par la prise en compte de ces risques lors de l'utilisation de la PMA. Pour mettre en lumière ces enjeux, nous utilisons l’approche principiste. Nous argüons qu'une tension éthique peut émerger entre le respect de l'autonomie procréative des parents d’intention et le devoir de minimiser les risques pour les enfants potentiels. Une seconde tension éthique peut émerger entre le droit des parents d’intention de faire un choix éclairé, et la réticence que peuvent avoir les professionnels de la santé de communiquer l’information sur les risques épigénétiques de la PMA, étant donné la validité incertaine de ces informations. Nous explorons aussi le risque de conflits d’intérêts pour les cliniciens des cliniques de PMA. Nous soutenons que les parents d’intention et les professionnels de la santé ont la responsabilité partagée de promouvoir les meilleurs intérêts du futur enfant. Nous plaidons pour que plus de recherche soit faite sur les effets de la PMA sur la santé des futurs enfants, pour que soient énoncées des lignes directrices priorisant le recours à des techniques moins risquées au niveau épigénétique, et pour que d’autres lignes directrices guident les professionnels de la santé dans la communication des risques épigénétiques associés à la PMA. Enfin, nous suggérons que cette communication se fasse dans le cadre d’une approche centrée sur le patient. Nous explorons aussi l’apport d’une approche narrative pour aborder les tensions éthiques soulevées par l’approche principiste. / The use of assisted reproductive technologies (ART) allows many coping with infertility to conceive. However, an emerging body of evidence suggests that ART could carry epigenetic risks for those conceived through the use of these technologies. In accordance with the Developmental Origins of Health and Disease (DOHaD) hypothesis, ART could increase the risk of developing late-onset diseases through epigenetic mechanisms, since superovulation, fertilization methods and embryo culture could impair the embryo’s epigenetic reprogramming. Such epigenetic risks raise ethical issues for all stakeholders: prospective parents and children, health professionals, and society. This thesis focuses on ethical issues raised by the consideration of these risks when using ART. To highlight these issues, we use the principlist approach. We argue that an ethical tension can emerge between respect for the reproductive autonomy of prospective parents and the duty to minimize the risks for potential children. A second ethical tension can emerge between the parents' right to make an informed choice about the use of ART, and the reluctance of health professionals to communicate epigenetic risk given its uncertain validity. We also explore the risks of conflicts of interests for health professionals in ART clinics. We argue that prospective parents and health professionals have a shared responsibility to promote the best interests of the future child. We also argue in favor of further research on the effects of ART on the health of future children, and in favor of clinical guidelines that prioritize the use of techniques that carry less epigenetic risk and that assist health professionals in communicating the epigenetic risks associated with ART. Finally, we suggest that this communication be done within the patient-centered approach. We also explore the contribution of a narrative approach to address the ethical tensions raised by the principlist approach.

Enjeux éthiques

Risques épigénétiques

Fécondation in vitro (FIV)

DOHaD

Assisted reproductive technologies (ART)

In vitro fertilization (IVF)

Epigenetic risks

Ethical issues

Le stress oxydatif d’origine nutritionnelle en période néonatale chez le cochon d’Inde et son impact à l’âge adulte sur l’homéostasie redox, le métabolisme énergétique et la méthylation génique

Teixeira Nascimento, Vitor

06 1900

Problématique : Durant la période fœtale, le métabolisme global du fœtus fonctionne en hypoxie, ce qui limite la phosphorylation oxydative dans la mitochondrie, et par conséquent la production d’adénosine triphosphate (ATP). Ces conditions sont nécessaires pour le développement intra-utérin. Lors de la naissance, l’augmentation des concentrations d’oxygène et un stress oxydatif permettent une transition métabolique. Une charge oxydative supplémentaire en période néonatale pourrait perturber cette transition métabolique et causer des complications. La nutrition parentérale (NP) administrée aux nouveau-nés prématurés apporte un triple fardeau oxydatif : une exposition à des peroxydes oxydants autogénérés par l’interaction des composants de la NP, une carence en vitamine C (instable en solution), et une déficience en glutathion, vu la charge oxydative élevée. Cette charge oxydative excessive affecte l’homéostasie redox au foie et aux poumons, ainsi que le métabolisme énergétique hépatique, et ce, par des effets immédiats et à long-terme. La méthylation de l’ADN est un possible mécanisme qui explique les effets à long terme. Le but de ce travail était de caractériser l’impact à court- et long-terme de la NP néonatale sur l’homéostasie redox, la méthylation de l’ADN, et le métabolisme des glucides et lipides, en isolant chacun des facteurs nutritionnels. Méthodes : Des cochons d’Inde ont été divisés dans les groupes suivants 1) NP : nutrition intraveineuse complète ; 2) NP+ glutathion disulfure (GSSG) (6 ou 12µM- substrat pour la synthèse intra-cellulaire de glutathion); 3) Diète complète : nutrition orale complète 4) Diète déficiente en Vitamine C; 5) Diète déficiente en Cystéine; 6) Diète double déficiente; ou. À 1 semaine de vie, la moitié des animaux était sacrifié et l’autre moitié a commencé à manger une diète complète jusqu’à l’âge adulte. Résultats et discussion : Les animaux ayant reçu une NP néonatale ont un métabolisme énergétique permettant la synthèse de nicotinamide adénine dinucléotide phosphate (NADPH) par l’augmentation de l’activité de la glucokinase (captation de glucose), et diminution de celles de la phosphofructokinase-1 (PFK-1) (glycolyse) et acétyl-CoA-carboxylase-1 (ACC)(lipogenèse). À l’âge adulte, les animaux ont une diminution des niveaux de GSSG, indiquant un débalancement de l’homéostasie redox vers le côté réducteur programmé par la NP néonatale. L’activité augmentée de l’ACC suggère une tendance à accumuler les lipides au foie à la suite d’une diète riche en glucides. L’ajout de glutathion à la NP ne prévient pas ces perturbations, car les déficiences en glutathion et vitamine C jouent un rôle sur la modulation des niveaux protéiques de l’ACC. Les diètes néonatales déficientes en vitamine C et cystéine augmentent l’activité de la PFK-1. Cette augmentation se maintient jusqu’à l’âge adulte chez les mâles, mais pas chez les femelles. Les niveaux protéiques de la glucokinase et ACC sont diminués à 1 semaine, et ceux de l’ACC sont élevés à 3 mois dans les groupes ayant reçu une des diètes déficientes. Ces effets sont similaires à ceux trouvés dans les animaux nourris avec la NP, suggérant que la déficience de la NP en ces nutriments et non les peroxydes cause ces effets. Dans tous les groupes, un stress oxydatif a été démontré à 1 semaine de vie, soit par l’augmentation des niveaux de GSSG, ou la diminution du GSH. Cet effet est vrai pour le foie et le poumon. Une réponse de Nrf2 est observée aussi au foie, ce qui caractérise un niveau bas de stress oxydatif. La baisse de GSH pulmonaire chez les animaux déficients est secondaire à l’inhibition oxydative de la voie de transméthylation au foie. Une diminution des niveaux d’ARNm de glutathion réductase et glutarédoxine sont observées, ce qui favorise encore le stress oxydatif pulmonaire. À long terme, les effets sont les opposés, soit débalancement de l’homéostasie redox vers le côté réducteur au foie et poumon. La méthylation de l’ADN était diminuée au foie des animaux nouveau-nés recevant les diètes déficientes, mais aucun changement n’a été observé aux poumons. Cette diminution est en accord avec les hauts niveaux d’ARNm des gènes de la protéine régulatrice de la glucokinase, et AMPK. À long-terme, l’effet inverse est observé pour la méthylation de l’ADN Conclusion : La NP modifie le flot d’énergie au foie à 1 semaine visant favoriser le métabolisme redox en détriment du métabolisme énergétique. Cet effet semble créer une déficience énergétique fonctionnelle, qui se développe en une lipogenèse accrue en âge adulte. Cela peut représenter un exemple de la plasticité développementale. Bien qu’un stress oxydatif en âge néonatal ne soit pas létal, il affecte le métabolisme énergétique et redox à long-terme, probablement par la méthylation de l’ADN. Les résultats de ce travail démontrent que ces animaux adultes ont une capacité accrue d’entreposer de l’énergie, soit par une lipogenèse plus élevée, soit par une accumulation d’énergie redox (glutathion). Aucune maladie métabolique n’était observée chez les animaux, mais il est attendu à ce que ces animaux développent ces maladies plus facilement suite à l’exposition à des insultes (habitudes de vie malsaines, tabagisme, etc.). / Problematic: During the fetal period, the general metabolism works under hypoxia, limiting oxidative phosphorylation in mitochondria and adenine triphosphate (ATP) synthesis. These conditions are necessary for intrauterine development. After birth, the increasing oxygen concentrations and the associated oxidative stress induce a metabolic transition. An excessive oxidative load during the neonatal period could perturb this transition. Parenteral nutrition (PN) administered to premature newborns comes with a triple oxidative burden: contaminating peroxides generated in solution, vitamin C deficiency (unstable in solution), and glutathione deficiency (caused by the high oxidative load). This oxidative load affects redox homoeostasis in the liver and lungs, as well as energy metabolism in the liver. These effects are not only immediate, but they are also delayed. DNA methylation is a candidate mechanism explaining the long-term effects. The objective of this work was to characterize the short- and long-term impacts of neonatal PN over redox homoeostasis, DNA methylation and carbohydrate and lipid metabolism by isolating each of these factors. Methods: Six groups of three-day-old guinea pigs received for 4 days either: 1) Total PN; 2) PN+glutathione disulfide (GSSG) (6 or 12µM-anti-peroxide);3) Vitamin C deficient; 4) Cysteine deficient; 5) Double deficient; or 6) Complete diets. At 1 week of life, half of the animals were sacrificed, and the other half started eating nutritionally complete diets until adulthood. Results and discussion: NP animals had energy metabolism shifted favouring nicotinamide adenine dinucleotide phosphate (NADPH) synthesis, as evidenced by the increase in glucokinase activity (glucose trapping in hepatocytes) and decrease in phosphfuctokinase-1 (PFK-1) (glycolysis) and acetyl-CoA-carboxyalase-1 (ACC) (lipogenesis) activities. Adding GSSG to parenteral nutrition prevents these changes. During adulthood, ACC activity is increased, suggesting a tendency to accumulate lipids after a diet rich in carbohydrates. Adding GSSG to PN does not prevent these changes as they seem to be caused by the nutritional deficiencies in vitamin C and cysteine. Neonatal diets deficient in vitamin C and cysteine increase PFK-1 activity. This increase is maintained until adulthood in males but not in females. Protein levels of glucokinase and ACC are decreased at 1 week of life and ACC levels are increased at adulthood in deficient groups. These effects are like the ones observed in PN animals. In all groups, oxidative stress is demonstrated in 1-week-old animals, either by an increase in GSSG levels, or a decrease in GSH. This is true for the liver and lungs. An Nrf2 response is also observed in the liver, suggesting a low level of oxidative stress. The decrease in lung GSH is secondary to the oxidative inhibition of the transmethylation pathway in the liver. Decreased levels of glutathione reductase and glutaredoxin mRNA levels are observed in lungs, favouring pulmonary oxidative stress. At adulthood, an imbalance in redox homeostasis towards a reducing state is observed in lungs and liver. DNA methylation was decreased in the liver of deficient animals at 1-week, but no changes were observed in lungs. This decrease is in accordance with the decrease in mRNA levels of glucokinase regulatory protein and AMPK. At adulthood, the opposite effect was observed for DNA methylation. Conclusion: Parenteral nutrition alters the energy flow in the liver of 1-week-old animals, favouring redox metabolism over energy metabolism. This effect seems to create a phenotype of functional energy deficiency which translates into an increased lipogenesis at adult age. This may be an example of developmental plasticity. Although neonatal oxidative stress is not lethal, it affects energy and redox metabolism at adulthood, probably through DNA methylation. The presented results demonstrate these animals have an increased capacity of storing energy, either through increased lipogenesis, or by an increase in redox energy accumulation (glutathione). No metabolic disease was observed. Although it would be expected that these animals would develop these diseases more easily after exposure to insults, such as unhealthy lifestyle habits, smoking, and others.

Glutathion

Vitamine C

Cystéine

Peroxydes

Nutrition parentérale

Prématurité

Glycolyse

Lipogenèse

Méthylation de l'ADN

Glutathione

Vitamin C

Cysteine

Peroxides

Parenteral nutrition

Glycolysis

Lipogenesis

DNA methylation

Nutrition / Nutrition (UMI : 0570)

BIRTHWEIGHT AND SUSCEPTIBILITY TO CHRONIC DISEASE

Issa Al Salmi

Unknown Date

The thesis examines the relationship of birthweight to risk factors and markers, such as proteinuria and glomerular filtration rate, for chronic disease in postnatal life. It made use of the Australian Diabetes, Obesity and Lifestyle Study (AusDiab). The AusDiab study is a cross sectional study where baseline data on 11,247 participants were collected in 1999-2000. Participants were recruited from a stratified sample of Australians aged ≥ 25 years, residing in 42 randomly selected urban and non-urban areas (Census Collector Districts) of the six states of Australia and the Northern Territory. The AusDiab study collected an enormous amount of clinical and laboratory data. During the 2004-05 follow-up AusDiab survey, questions about birthweight were included. Participants were asked to state their birthweight, the likely accuracy of the stated birthweight and the source of their stated birthweight. Four hundred and twelve chronic kidney disease (CKD) patients were approached, and 339 agreed to participate in the study. The patients completed the same questionnaire. Medical records were reviewed to check the diagnoses, causes of kidney trouble and SCr levels. Two control subjects, matched for gender and age, were selected for each CKD patient from participants in the AusDiab study who reported their birthweight. Among 7,157 AusDiab participants who responded to the questionnaire, 4,502 reported their birthweights, with a mean (standard deviation) of 3.4 (0.7) kg. The benefit and disadvantages of these data are discussed in chapter three. The data were analysed for the relationship between birthweight and adult body size and composition, disorders of glucose regulation, blood pressure, lipid abnormalities, cardiovascular diseases and glomerular filtration rate. Low birthweight was associated with smaller body build and lower lean mass and total body water in both females and males. In addition low birthweight was associated with central obesity and higher body fat percentage in females, even after taking into account current physical activity and socioeconomic status. Fasting plasma glucose, post load glucose and glycosylated haemoglobin were strongly and inversely correlated with birthweight. In those with low birthweight (< 2.5 kg), the risks for having impaired fasting glucose, impaired glucose tolerance, diabetes and all abnormalities combined were increased by 1.75, 2.22, 2.76 and 2.28 for females and by 1.40, 1.32, 1.98 and 1.49 for males compared to those with normal birthweight (≥ 2.5 kg), respectively. Low birthweight individuals were at higher risk for having high blood pressure ≥ 140/90 mmHg and ≥ 130/85 mmHg compared to those with normal birthweight. People with low birthweight showed a trend towards increased risk for high cholesterol (≥ 5.5 mmol/l) compared to those of normal birthweight. Females with low birthweight had increased risk for high low density lipoprotein cholesterol (≥ 3.5 mmol/l) and triglyceride levels (≥ 1.7 mmol/l) when compared to those with normal birthweight. Males with low birthweight exhibited increased risk for low levels of high density lipoprotein cholesterol (<0.9 mmol/l) than those with normal birthweight. Females with low birthweight were at least 1.39, 1.40, 2.30 and 1.47 times more likely to have angina, coronary artery disease, stroke and overall cardiovascular diseases respectively, compared to those ≥ 2.5 kg. Similarly, males with low birthweight were 1.76, 1.48, 3.34 and 1.70 times more likely to have angina, coronary artery disease, stroke and overall cardiovascular diseases compared to those ≥ 2.5 kg, respectively. The estimated glomerular filtration rate was strongly and positively associated with birthweight, with a predicted increase of 2.6 ml/min (CI 2.1, 3.2) and 3.8 (3.0, 4.5) for each kg of birthweight for females and males, respectively. The odd ratio (95% confidence interval) for low glomerular filtration rate (<61.0 ml/min for female and < 87.4 male) in people of low birthweight compared with those of normal birthweight was 2.04 (1.45, 2.88) for female and 3.4 (2.11, 5.36) for male. One hundred and eighty-nineCKD patients reported their birthweight; 106 were male. Their age was 60.3(15) years. Their birthweight was 3.27 (0.62) kg, vs 3.46 (0.6) kg for their AusDiab controls, p<0.001 and the proportions with birthweight<2.5 kg were 12.17% and 4.44%, p<0.001. Among CKD patients, 22.8%, 21.7%, 18% and 37.6% were in CKD stages 2, 3, 4 and 5 respectively. Birthweights by CKD stage and their AusDiab controls were as follows: 3.38 (0.52) vs 3.49 (0.52), p=0.251 for CKD2; 3.28 (0.54) vs 3.44 (0.54), p=0.121 for CKD3; 3.19 (0.72) vs 3.43 (0.56), p= 0.112 for CKD4 and 3.09 (0.65) vs 3.47 (0.67), p<0.001 for CKD5. The results demonstrate that in an affluent Western country with a good adult health profile, low birthweight people were predisposed to higher rates of glycaemic dysregulation, high blood pressure, dyslipidaemia, cardiovascular diseases and lower glomerular filtration rate in adult life. In all instances it would be prudent to adopt policies of intensified whole of life surveillance of lower birthweight people, anticipating this risk. The general public awareness of the effect of low birthweight on development of chronic diseases in later life is of vital importance. The general public, in addition to the awareness of people in medical practice of the role of low birthweight, will lead to a better management of this group of our population that is increasingly surviving into adulthood.

birth weight

birthweight

birth weight and renal volume

BIRTH WEIGHT QUESTIONNAIRE

chronic disease

Barker Hypothesis

Foetal development

DOHaD

gestational age

Anthropometric Characteristics

body composition

Height

weight

body mass index

Waist Circumference

hip circumference

Waist-hip Ratio

obesity

Central Obesity

Fatness

Lean Body Mass

Lean Mass

Fat Mass

body fat mass

Body Fat Percentage

body fatness

Body Surface Area

diabetes

Fasting Glucose

fasting insulin level

glucose tolerance

Impaired Fasting Glucose

Impaired Glucose Tolerance

Glycosylated Hemoglobin

HbA1c

IFG

glucose control

glycaemic control

Metabolic Syndrome

Syndrome X

blood pressure

Systolic Blood-pressure

Diastolic Blood-pressure

Systolic Hypertension

high blood pressure

Hypertension

Dyslipidaemia

Dyslipidemia

Total Cholesterol

Triglyceride

Low Density Lipoprotein Cholesterol

Ldl Cholesterol

High Density Lipoprotein

Hdl Cholesterol

Fibrinogen

angina

Angina-pectoris

Stroke

coronary artery disease

cardiovascular disease

Framingham

Framingham Heart Study

Framingham Score

coronary heart disease

Glomerular Filtration

glomerular filtration rate

Glomerular Hyperfiltration

Glomerular Injury

Glomerular Number

Nephrogenesis

Nephron Endowment

Nephron Number

NKF-K/DQQI Classification

Chronic Kidney Disease (ckd)

Chronic Kidney Failure

Kidney Failure

CKD STAGES

end-stage renal disease (ESRD)

end-stage renal failure

Cockcroft-gault

MDRD formula

Serum Creatinine

Urinary Creatinine

albuminuria

Albuminuria:creatinine Ratio

Kidney Development

Kidney dysfunction

low birth weight

low birth weight

Pre-term Birth

AusDiab Study

case control

longitudinal observational study

BIRTHWEIGHT AND SUSCEPTIBILITY TO CHRONIC DISEASE

Issa Al Salmi

Unknown Date

The thesis examines the relationship of birthweight to risk factors and markers, such as proteinuria and glomerular filtration rate, for chronic disease in postnatal life. It made use of the Australian Diabetes, Obesity and Lifestyle Study (AusDiab). The AusDiab study is a cross sectional study where baseline data on 11,247 participants were collected in 1999-2000. Participants were recruited from a stratified sample of Australians aged ≥ 25 years, residing in 42 randomly selected urban and non-urban areas (Census Collector Districts) of the six states of Australia and the Northern Territory. The AusDiab study collected an enormous amount of clinical and laboratory data. During the 2004-05 follow-up AusDiab survey, questions about birthweight were included. Participants were asked to state their birthweight, the likely accuracy of the stated birthweight and the source of their stated birthweight. Four hundred and twelve chronic kidney disease (CKD) patients were approached, and 339 agreed to participate in the study. The patients completed the same questionnaire. Medical records were reviewed to check the diagnoses, causes of kidney trouble and SCr levels. Two control subjects, matched for gender and age, were selected for each CKD patient from participants in the AusDiab study who reported their birthweight. Among 7,157 AusDiab participants who responded to the questionnaire, 4,502 reported their birthweights, with a mean (standard deviation) of 3.4 (0.7) kg. The benefit and disadvantages of these data are discussed in chapter three. The data were analysed for the relationship between birthweight and adult body size and composition, disorders of glucose regulation, blood pressure, lipid abnormalities, cardiovascular diseases and glomerular filtration rate. Low birthweight was associated with smaller body build and lower lean mass and total body water in both females and males. In addition low birthweight was associated with central obesity and higher body fat percentage in females, even after taking into account current physical activity and socioeconomic status. Fasting plasma glucose, post load glucose and glycosylated haemoglobin were strongly and inversely correlated with birthweight. In those with low birthweight (< 2.5 kg), the risks for having impaired fasting glucose, impaired glucose tolerance, diabetes and all abnormalities combined were increased by 1.75, 2.22, 2.76 and 2.28 for females and by 1.40, 1.32, 1.98 and 1.49 for males compared to those with normal birthweight (≥ 2.5 kg), respectively. Low birthweight individuals were at higher risk for having high blood pressure ≥ 140/90 mmHg and ≥ 130/85 mmHg compared to those with normal birthweight. People with low birthweight showed a trend towards increased risk for high cholesterol (≥ 5.5 mmol/l) compared to those of normal birthweight. Females with low birthweight had increased risk for high low density lipoprotein cholesterol (≥ 3.5 mmol/l) and triglyceride levels (≥ 1.7 mmol/l) when compared to those with normal birthweight. Males with low birthweight exhibited increased risk for low levels of high density lipoprotein cholesterol (<0.9 mmol/l) than those with normal birthweight. Females with low birthweight were at least 1.39, 1.40, 2.30 and 1.47 times more likely to have angina, coronary artery disease, stroke and overall cardiovascular diseases respectively, compared to those ≥ 2.5 kg. Similarly, males with low birthweight were 1.76, 1.48, 3.34 and 1.70 times more likely to have angina, coronary artery disease, stroke and overall cardiovascular diseases compared to those ≥ 2.5 kg, respectively. The estimated glomerular filtration rate was strongly and positively associated with birthweight, with a predicted increase of 2.6 ml/min (CI 2.1, 3.2) and 3.8 (3.0, 4.5) for each kg of birthweight for females and males, respectively. The odd ratio (95% confidence interval) for low glomerular filtration rate (<61.0 ml/min for female and < 87.4 male) in people of low birthweight compared with those of normal birthweight was 2.04 (1.45, 2.88) for female and 3.4 (2.11, 5.36) for male. One hundred and eighty-nineCKD patients reported their birthweight; 106 were male. Their age was 60.3(15) years. Their birthweight was 3.27 (0.62) kg, vs 3.46 (0.6) kg for their AusDiab controls, p<0.001 and the proportions with birthweight<2.5 kg were 12.17% and 4.44%, p<0.001. Among CKD patients, 22.8%, 21.7%, 18% and 37.6% were in CKD stages 2, 3, 4 and 5 respectively. Birthweights by CKD stage and their AusDiab controls were as follows: 3.38 (0.52) vs 3.49 (0.52), p=0.251 for CKD2; 3.28 (0.54) vs 3.44 (0.54), p=0.121 for CKD3; 3.19 (0.72) vs 3.43 (0.56), p= 0.112 for CKD4 and 3.09 (0.65) vs 3.47 (0.67), p<0.001 for CKD5. The results demonstrate that in an affluent Western country with a good adult health profile, low birthweight people were predisposed to higher rates of glycaemic dysregulation, high blood pressure, dyslipidaemia, cardiovascular diseases and lower glomerular filtration rate in adult life. In all instances it would be prudent to adopt policies of intensified whole of life surveillance of lower birthweight people, anticipating this risk. The general public awareness of the effect of low birthweight on development of chronic diseases in later life is of vital importance. The general public, in addition to the awareness of people in medical practice of the role of low birthweight, will lead to a better management of this group of our population that is increasingly surviving into adulthood.

birth weight

birthweight

birth weight and renal volume

BIRTH WEIGHT QUESTIONNAIRE

chronic disease

Barker Hypothesis

Foetal development

DOHaD

gestational age

Anthropometric Characteristics

body composition

Height

weight

body mass index

Waist Circumference

hip circumference

Waist-hip Ratio

obesity

Central Obesity

Fatness

Lean Body Mass

Lean Mass

Fat Mass

body fat mass

Body Fat Percentage

body fatness

Body Surface Area

diabetes

Fasting Glucose

fasting insulin level

glucose tolerance

Impaired Fasting Glucose

Impaired Glucose Tolerance

Glycosylated Hemoglobin

HbA1c

IFG

glucose control

glycaemic control

Metabolic Syndrome

Syndrome X

blood pressure

Systolic Blood-pressure

Diastolic Blood-pressure

Systolic Hypertension

high blood pressure

Hypertension

Dyslipidaemia

Dyslipidemia

Total Cholesterol

Triglyceride

Low Density Lipoprotein Cholesterol

Ldl Cholesterol

High Density Lipoprotein

Hdl Cholesterol

Fibrinogen

angina

Angina-pectoris

Stroke

coronary artery disease

cardiovascular disease

Framingham

Framingham Heart Study

Framingham Score

coronary heart disease

Glomerular Filtration

glomerular filtration rate

Glomerular Hyperfiltration

Glomerular Injury

Glomerular Number

Nephrogenesis

Nephron Endowment

Nephron Number

NKF-K/DQQI Classification

Chronic Kidney Disease (ckd)

Chronic Kidney Failure

Kidney Failure

CKD STAGES

end-stage renal disease (ESRD)

end-stage renal failure

Cockcroft-gault

MDRD formula

Serum Creatinine

Urinary Creatinine

albuminuria

Albuminuria:creatinine Ratio

Kidney Development

Kidney dysfunction

low birth weight

low birth weight

Pre-term Birth

AusDiab Study

case control

longitudinal observational study

BIRTHWEIGHT AND SUSCEPTIBILITY TO CHRONIC DISEASE

Issa Al Salmi

Unknown Date

The thesis examines the relationship of birthweight to risk factors and markers, such as proteinuria and glomerular filtration rate, for chronic disease in postnatal life. It made use of the Australian Diabetes, Obesity and Lifestyle Study (AusDiab). The AusDiab study is a cross sectional study where baseline data on 11,247 participants were collected in 1999-2000. Participants were recruited from a stratified sample of Australians aged ≥ 25 years, residing in 42 randomly selected urban and non-urban areas (Census Collector Districts) of the six states of Australia and the Northern Territory. The AusDiab study collected an enormous amount of clinical and laboratory data. During the 2004-05 follow-up AusDiab survey, questions about birthweight were included. Participants were asked to state their birthweight, the likely accuracy of the stated birthweight and the source of their stated birthweight. Four hundred and twelve chronic kidney disease (CKD) patients were approached, and 339 agreed to participate in the study. The patients completed the same questionnaire. Medical records were reviewed to check the diagnoses, causes of kidney trouble and SCr levels. Two control subjects, matched for gender and age, were selected for each CKD patient from participants in the AusDiab study who reported their birthweight. Among 7,157 AusDiab participants who responded to the questionnaire, 4,502 reported their birthweights, with a mean (standard deviation) of 3.4 (0.7) kg. The benefit and disadvantages of these data are discussed in chapter three. The data were analysed for the relationship between birthweight and adult body size and composition, disorders of glucose regulation, blood pressure, lipid abnormalities, cardiovascular diseases and glomerular filtration rate. Low birthweight was associated with smaller body build and lower lean mass and total body water in both females and males. In addition low birthweight was associated with central obesity and higher body fat percentage in females, even after taking into account current physical activity and socioeconomic status. Fasting plasma glucose, post load glucose and glycosylated haemoglobin were strongly and inversely correlated with birthweight. In those with low birthweight (< 2.5 kg), the risks for having impaired fasting glucose, impaired glucose tolerance, diabetes and all abnormalities combined were increased by 1.75, 2.22, 2.76 and 2.28 for females and by 1.40, 1.32, 1.98 and 1.49 for males compared to those with normal birthweight (≥ 2.5 kg), respectively. Low birthweight individuals were at higher risk for having high blood pressure ≥ 140/90 mmHg and ≥ 130/85 mmHg compared to those with normal birthweight. People with low birthweight showed a trend towards increased risk for high cholesterol (≥ 5.5 mmol/l) compared to those of normal birthweight. Females with low birthweight had increased risk for high low density lipoprotein cholesterol (≥ 3.5 mmol/l) and triglyceride levels (≥ 1.7 mmol/l) when compared to those with normal birthweight. Males with low birthweight exhibited increased risk for low levels of high density lipoprotein cholesterol (<0.9 mmol/l) than those with normal birthweight. Females with low birthweight were at least 1.39, 1.40, 2.30 and 1.47 times more likely to have angina, coronary artery disease, stroke and overall cardiovascular diseases respectively, compared to those ≥ 2.5 kg. Similarly, males with low birthweight were 1.76, 1.48, 3.34 and 1.70 times more likely to have angina, coronary artery disease, stroke and overall cardiovascular diseases compared to those ≥ 2.5 kg, respectively. The estimated glomerular filtration rate was strongly and positively associated with birthweight, with a predicted increase of 2.6 ml/min (CI 2.1, 3.2) and 3.8 (3.0, 4.5) for each kg of birthweight for females and males, respectively. The odd ratio (95% confidence interval) for low glomerular filtration rate (<61.0 ml/min for female and < 87.4 male) in people of low birthweight compared with those of normal birthweight was 2.04 (1.45, 2.88) for female and 3.4 (2.11, 5.36) for male. One hundred and eighty-nineCKD patients reported their birthweight; 106 were male. Their age was 60.3(15) years. Their birthweight was 3.27 (0.62) kg, vs 3.46 (0.6) kg for their AusDiab controls, p<0.001 and the proportions with birthweight<2.5 kg were 12.17% and 4.44%, p<0.001. Among CKD patients, 22.8%, 21.7%, 18% and 37.6% were in CKD stages 2, 3, 4 and 5 respectively. Birthweights by CKD stage and their AusDiab controls were as follows: 3.38 (0.52) vs 3.49 (0.52), p=0.251 for CKD2; 3.28 (0.54) vs 3.44 (0.54), p=0.121 for CKD3; 3.19 (0.72) vs 3.43 (0.56), p= 0.112 for CKD4 and 3.09 (0.65) vs 3.47 (0.67), p<0.001 for CKD5. The results demonstrate that in an affluent Western country with a good adult health profile, low birthweight people were predisposed to higher rates of glycaemic dysregulation, high blood pressure, dyslipidaemia, cardiovascular diseases and lower glomerular filtration rate in adult life. In all instances it would be prudent to adopt policies of intensified whole of life surveillance of lower birthweight people, anticipating this risk. The general public awareness of the effect of low birthweight on development of chronic diseases in later life is of vital importance. The general public, in addition to the awareness of people in medical practice of the role of low birthweight, will lead to a better management of this group of our population that is increasingly surviving into adulthood.

birth weight

birthweight

birth weight and renal volume

BIRTH WEIGHT QUESTIONNAIRE

chronic disease

Barker Hypothesis

Foetal development

DOHaD

gestational age

Anthropometric Characteristics

body composition

Height

weight

body mass index

Waist Circumference

hip circumference

Waist-hip Ratio

obesity

Central Obesity

Fatness

Lean Body Mass

Lean Mass

Fat Mass

body fat mass

Body Fat Percentage

body fatness

Body Surface Area

diabetes

Fasting Glucose

fasting insulin level

glucose tolerance

Impaired Fasting Glucose

Impaired Glucose Tolerance

Glycosylated Hemoglobin

HbA1c

IFG

glucose control

glycaemic control

Metabolic Syndrome

Syndrome X

blood pressure

Systolic Blood-pressure

Diastolic Blood-pressure

Systolic Hypertension

high blood pressure

Hypertension

Dyslipidaemia

Dyslipidemia

Total Cholesterol

Triglyceride

Low Density Lipoprotein Cholesterol

Ldl Cholesterol

High Density Lipoprotein

Hdl Cholesterol

Fibrinogen

angina

Angina-pectoris

Stroke

coronary artery disease

cardiovascular disease

Framingham

Framingham Heart Study

Framingham Score

coronary heart disease

Glomerular Filtration

glomerular filtration rate

Glomerular Hyperfiltration

Glomerular Injury

Glomerular Number

Nephrogenesis

Nephron Endowment

Nephron Number

NKF-K/DQQI Classification

Chronic Kidney Disease (ckd)

Chronic Kidney Failure

Kidney Failure

CKD STAGES

end-stage renal disease (ESRD)

end-stage renal failure

Cockcroft-gault

MDRD formula

Serum Creatinine

Urinary Creatinine

albuminuria

Albuminuria:creatinine Ratio

Kidney Development

Kidney dysfunction

low birth weight

low birth weight

Pre-term Birth

AusDiab Study

case control

longitudinal observational study