Étude du polymorphisme rs3846662 de l’HMGCR dans le cerveau et le système périphérique

Leduc, Valérie

05 1900

Dans cette thèse, l’impact du polymorphisme rs3846662 sur l’épissage alternatif de la 3-hydroxy-3-méthylglutaryl coenzyme A réductase (HMGCR) a été investigué in vivo, chez des patients atteints d’hypercholestérolémie familiale (HF) ou de maladie d’Alzheimer (MA). Le premier manuscrit adresse la problématique de la normalisation de la quantification relative des ARNm par PCR quantitative. Les découvertes présentées dans ce manuscrit nous ont permis de déterminer avec un haut niveau de confiance les gènes de référence à utiliser pour la quantification relative des niveaux d’ARNm de l’HMGCR dans des échantillons de sang (troisième manuscrit) et de tissus cérébraux post-mortem (quatrième manuscrit). Dans le deuxième manuscrit, nous démontrons grâce à l’emploi de trois cohortes de patients distinctes, soit la population canadienne française du Québec et les deux populations nord américaines « Alzheimer’s Disease Cooperative Study (ADCS) » et « Alzheimer’s Disease Neuroimaging Initiative (ADNI) », que le génotype AA au locus rs3846662 confère à ces porteurs une protection considérable contre la MA. Les femmes porteuses de ce génotype voient leur risque de MA diminuer de près de 50% et l’âge d’apparition de leurs premiers symptômes retarder de 3.6 ans. Les porteurs de l’allèle à risque APOE4 voient pour leur part leurs niveaux de plaques séniles et dégénérescences neurofibrillaires diminuer significativement en présence du génotype AA. Enfin, les individus atteints de déficit cognitif léger et porteurs à la fois de l’allèle APOE4 et du génotype protecteur AA voient leur risque de convertir vers la MA chuter de 76 à 27%. Dans le troisième manuscrit, nous constatons que les individus atteints d’HF et porteurs du génotype AA ont, contrairement au modèle établi chez les gens normaux, des niveaux plus élevés de cholestérol total et de LDL-C avant traitement comparativement aux porteurs de l’allèle G. Le fait que cette association n’est observée que chez les non porteurs de l’APOE4 et que les femmes porteuses du génotype AA présentent à la fois une augmentation des niveaux d’ARNm totaux et une résistance aux traitements par statines, nous indique que ce génotype influencerait non seulement l’épissage alternatif, mais également la transcription de l’HMGCR. Comme une revue exhaustive de la littérature ne révèle aucune étude abondant dans ce sens, nos résultats suggèrent l’existence de joueurs encore inconnus qui viennent influencer la relation entre le génotype AA, l’épissage alternatif et les niveaux d’ARNm de l’HMGCR. Dans le quatrième manuscrit, l’absence d’associations entre le génotype AA et les niveaux d’ARNm Δ13 ou de protéines HMGCR nous suggère fortement que ce polymorphisme est non fonctionnel dans le SNC affecté par la MA. Une étude approfondie de la littérature nous a permis d’étayer cette hypothèse puisque les niveaux de HNRNPA1, la ribonucléoprotéine influencée par l’allèle au locus rs3846662, sont considérablement réduits dans la MA et le vieillissement. Il est donc proposé que les effets protecteurs contre la MA associés au génotype AA soient le résultat d’une action indirecte sur le processus physiopathologique. / In this thesis, the impact of rs3846662 polymorphism on the alternative splicing of 3-hydroxy-3-methylglutaryl coenzyme A reductase (HMGCR) was investigated in vivo, in patients with familial hypercholesterolemia (FH) or Alzheimer disease (AD). The first manuscript addresses the issue of normalization in relative quantification of mRNA by quantitative PCR. The findings presented in this manuscript have allowed us to determine with a high level of certainty the appropriate reference genes to use for the relative quantification of HMGCR mRNA levels in blood samples (third manuscript) and postmortem brain tissues (fourth manuscript). In the second manuscript, we demonstrate through the use of three independent cohorts, namely the French Canadian population of Quebec and the two North American populations named "Alzheimer's Disease Cooperative Study (ADCS)" and "Alzheimer's Disease Neuroimaging Initiative (ADNI) ", that the AA genotype at locus rs3846662 confers significant protection against AD. Women carrying this genotype decrease their risk of AD by about 50%, and delay their age of onset of 3.6 years. For their part, individuals carrying both the APOE4 risk allele and the AA genotype have decreased levels of senile plaques and neurofibrillary tangles compared to individuals carrying both the APOE4 and HMGCR G alleles. Finally, individuals suffering from mild cognitive impairment and carrying both the APOE4 risk allele and the protective AA genotype see their risk of converting to AD drop from 76% to 27%. In the third manuscript, contrary to the model described in normal subjects, we discovered that individuals with FH carrying the AA genotype have higher levels of total cholesterol and LDL-C before treatment compared to the carriers of the G allele. This latter association is observed only in non-carriers of the APOE4 risk allele. Furthermore, women carrying the AA genotype have both an increase in total HMGCR mRNA levels and a decrease response to statin treatment. These results suggest the AA genotype has an impact not only on the alternative splicing, but also on the transcription of HMGCR. Since an exhaustive review of the literature has reveal no studies corroborating this hypothesis, our results suggest the existence of yet unknown players influencing the relationships between the AA genotype, alternative splicing and the mRNA levels of HMGCR. In the fourth manuscript, we uncovered no association between the AA genotype and Δ13 mRNA or HMGCR protein levels. This strongly suggests that the rs3846662 polymorphism is not functional in the CNS affected by AD. A thorough study of the literature enabled us to support this hypothesis since the levels of HNRNPA1, the ribonucleoprotein influenced by the allele status at rs3846662 locus, are significantly reduced in AD and aging. Accordingly, we propose that the protective effects of the AA genotype against AD may be mediated through indirect effects on the physiopathology of the disease.

rs3846662

épissage alternatif

ARNm

maladie d'Alzheimer

statine

hypercholestérolémie familiale

normalisation

quantification relative d'ARNm

rs3846662

alternative splicing

mRNA

Alzheimer's disease

statin

Familial hypercholesterolemia

normalization

relative quantification of mRNA

Cellules souches pluripotentes humaines et modélisation de maladies hépatiques : l'hypercholestérolémie familiale et les cholangiopathies / Human pluripotent stem cells and liver diseases modeling : Familial hypercholesterolemia and cholangiopathies

Dianat, Noushin

12 June 2014

La thérapie cellulaire pourrait représenter une alternative à la transplantation hépatique dans certaines pathologies comme les maladies métaboliques sévères. Toutefois, la pénurie de donneurs d’organes implique la nécessité de trouver de nouvelles sources de cellules hépatiques comme les cellules souches pluripotentes qui peuvent être amplifiées extensivement et différenciées en tout type cellulaire. Les cellules souches embryonnaires humaines (hESC) et les cellules souches pluripotentes induites humaines (hiPSC) générées à partir des cellules somatiques de patients puis différenciées en hépatocytes représentent une source potentielle d’hépatocytes. Ces cellules permettent en outre d’envisager la transplantation d’hépatocytes autologues génétiquement modifiés comme alternative à la transplantation hépatique pour le traitement de certaines maladies génétiques du foie. L’hypercholestérolémie familiale (HF) est une maladie autosomale dominante due à des mutations dans le gène codant le Récepteur aux Low Density Lipoproteins (RLDL) qui est à l’origine d’un taux élevé de cholestérol sanguin de patients HF. Les patients homozygotes doivent épurer leur sérum par LDL-aphérèse en moyenne deux fois par mois dès le plus jeune âge pour éviter les infarctus mortels survenant dès l’enfance. Les hépatocytes différenciées à partir des iPSC de patients et leur correction in vitro, permettent d'évaluer la faisabilité de la transplantation d'hépatocytes autologues génétiquement modifiés pour le traitement de l’hypercholestérolémie familiale.Au cours du développement du foie, des hépatocytes et des cholangiocytes, les deux types de cellules épithéliales hépatiques, dérivent de progéniteurs hépatiques bipotents (les hépatoblastes). Bien que les cholangiocytes formant les canaux biliaires intrahépatiques ne représentent qu'une petite fraction de la population cellulaire totale du foie (3%), ces cellules régulent activement la composition de la bile par réabsorption des acides biliaires, un processus qui est important dans des maladies choléstatiques du foie. Dans la première partie de cette étude nous avons mis au point une approche de différenciation des cellules souches pluripotentes (hESC et hiPSC) en cholangiocytes fonctionnels. Ces cellules serviront à la modélisation des maladies génétiques touchant les cholangiocytes formant des canaux biliaires. Dans la deuxième partie, nous avons généré des iPSC spécifiques de patients HF (HF-iPSC), différenciées en hépatocytes et corrigé le défaut phénotypique par transfert lentiviral de l’ADNc codant le LDLR dans les HF-iPSC. / Cell therapy can be an alternative to liver transplantation in some cases such as severe metabolic diseases. However, the shortage of organ donors implies the need to find new sources of liver cells such as hepatocytes derived from pluripotent stem cells that can be amplified and differentiated extensively into any cell type. Human embryonic stem cells (hESC) and human induced pluripotent stem cells (hiPSC) generated from somatic cells of patients and then differentiated into hepatocytes represent a potential source of transplantable hepatocytes. These cells now make it possible to consider the transplantation of genetically modified autologous hepatocytes as an alternative to liver transplantation for the treatment of genetic diseases of the liver.Familial hypercholesterolemia (FH) is an autosomal dominant disorder caused by mutations in the gene encoding the receptor for Low Density Lipoproteins (LDLR), which is the cause of high blood cholesterol in these patients. Homozygous patients should purify their serum LDL-apheresis on average twice a month starting at a young age to avoid fatal myocardial infarction occurring in childhood.Human hepatocytes differentiated from patient’s induced pluripotent stem cells (iPSCs) allow assessing the feasibility to transplant genetically modified autologous hepatocytes as treatment of familial hypercholesterolemia.During the liver development, hepatocytes and cholangiocytes, the two types of hepatic epithelial cells, derive from bipotent hepatic progenitors (hepatoblasts). Although cholangiocytes, forming intrahepatic bile ducts, represent a small fraction of the total liver cell population (3%), they actively regulate bile composition by secretion and reabsorption of bile acids, a process that is important in cholestatic liver diseases. In the first part of this study we developed an approach to differentiate pluripotent stem cells (hESC and hiPSC) into functional cholangiocytes. These cells could be used for the modeling of genetic biliary diseases. In the second part, we generated FH patient specific iPSCs (HF-iPSC), differentiated them into hepatocytes and tried to correct the disease phenotype by lentiviral introduction of LDLR cDNA cassette in HF-iPSC.

Cellules souches embryonnaires

Cellules souches pluripotentes induites

Humain

Différenciation

Foie

Développement

Thérapie génique

Thérapie cellulaire

Hépatocyte

Cholangiocyte

Hépatobalstes

Hypercholestérolémie familiale

Récepteur aux LDL

LDLR

Low density lipoprotein

Embryonic stem cells

Induced pluripotent stem cells

Differentiation

Human

Liver development

Gene therapy

Cell therapy

Hepatocyte

Cholangiocyte

Hepatoblast

Familial hypercholesterolemia

LDL receptor

LDLR

Low density lipoprotein

Low density lipoprotein receptor

Mécanismes impliqués dans la modulation de la néovascularisation post-ischémique : rôle de la rénine et des microARNs

Desjarlais, Michel

12 1900

No description available.

Néovascularisation

Angiogenèse

Cellule endothéliale (EC)

Cellule pro-Angiogénique (PAC)

Athérosclérose

Hypercholestérolémie

micro-ARN (miR)

Rénine

Inflammation

Stress oxydant

Ischémie

Neovascularization

Angiogenesis

Endothelial cell (EC)

Proangiogenic cell (PAC)

Atherosclerosis

Hypercholesterolemia

micro-RNA (miR)

Renin

Inflammation

Oxydative stress

Ischemia

Genetic Determinants of Rare Coding Variants on the Development of Early-Onset Coronary Artery Disease

Lali, Ricky

11 1900

Background: Coronary Artery Disease (CAD) represents the leading cause of mortality and morbidity worldwide despite declines in the prevalence of environmental risk factors. This trend has drawn attention to the risk conferred by genetic variation. Twin and linkage studies demonstrate a profound hereditary risk for CAD, especially in young individuals. Rare genetic variants conferring high risk for extreme disease phenotypes can provide invaluable insight into novel mechanisms underlying CAD development. Methods: Whole exome sequencing was performed to characterize rare protein-altering variants in 52 early-onset CAD (EOCAD) patients encompassing the DECODE study. The enrichment of Mendelian dyslipidemias in EOCAD was assessed through interrogation of pathogenic mutations among known lipid genes. The identification of novel genetic CAD associations was conducted through case-only and case-control approaches across all protein-coding genes using rare variant burden and variance component tests. Lastly, beta coefficients for significant risk genes from the European population in the Early-onset Myocardial Infarction (EOMI) cohort (N=552) were used to construct calibrated, single-sample rare variant gene scores (RVGS) in DECODE Europeans (N=39) and a local European CAD-free cohort (N=77). Results: A 20-fold enrichment of Familial hypercholesterolemia mutation carriers was detected in EOCAD cases compared to CAD-free controls (P=0.005). Association analysis using EOMI Europeans revealed exome-wide and nominal significance for two known CAD/MI genes: CELSR2 (P=1.1x10-17) and APOA5 (P=0.001). DECODE association revealed exome-wide and nominal significance for genes involved in endothelial integrity and immune cell activity. RVGS based upon beta coefficients of significant CAD/MI risk genes were significantly increased in DECODE (z-score=1.84; p=0.03) and insignificantly decreased among CAD-free individuals (z-score=-1.61; p=0.053). Conclusion: Rare variants play a pivotal role in the development early CAD through Mendelian and polygenic mechanisms. Construction of RVGS that are calibrated against population and technical biases can facilitate discovery of single-sample and cohort-based associations beyond what is detectable using standard methods. / Thesis / Master of Science (MSc)

Cost-effective delivery of managed nurse-based primary health care in a selected medical scheme

Seymore, Martha Magarieta

06 1900

The study was aimed at furthering the health objectives of the government's Reconstruction and Development Programme (ANC 1994b) in the area of primary health care. . The purpose of the study was to examine the possible reduction of medical scheme claims for cardiovascular disease by means of primary health care, so that medical scheme benefits do not become exhausted so rapidly. The overall outcome of the study showed that if cardiovascular disease could be diagnosed and treated early, the financial benefits could be substantial. This was illustrated by the comparison of primary, secondary and tertiary treatment of cardiovascular disease using case studies over a period of one year. Recommendations centered around nurse-based primary health care for cardiovascular disease and the cost-effective management of the medical scheme. It was concluded that as a result of nurse-based primary health care, costs could be contained so that medical scheme benefits would not become exhausted so rapidly. / Health Studies / M.A. (Nursing Science)

Cardiovascular diseases

Cholesterol

Cost escalation

Diabetes mellitus

Hypercholesterolemia,

Hypertension

Managed health care

Nurse-based primary health care,

Medical scheme

Primary health care

Risk factors

362.10425068

Medical policy -- South Africa

Medical care -- South Africa -- Finance

Nursing care plans -- South Africa

Health care reform -- South Africa.

Health insurance -- South Africa

Cost-effective delivery of managed nurse-based primary health care in a selected medical scheme

Seymore, Martha Magarieta

06 1900

The study was aimed at furthering the health objectives of the government's Reconstruction and Development Programme (ANC 1994b) in the area of primary health care. . The purpose of the study was to examine the possible reduction of medical scheme claims for cardiovascular disease by means of primary health care, so that medical scheme benefits do not become exhausted so rapidly. The overall outcome of the study showed that if cardiovascular disease could be diagnosed and treated early, the financial benefits could be substantial. This was illustrated by the comparison of primary, secondary and tertiary treatment of cardiovascular disease using case studies over a period of one year. Recommendations centered around nurse-based primary health care for cardiovascular disease and the cost-effective management of the medical scheme. It was concluded that as a result of nurse-based primary health care, costs could be contained so that medical scheme benefits would not become exhausted so rapidly. / Health Studies / M.A. (Nursing Science)

Cardiovascular diseases

Cholesterol

Cost escalation

Diabetes mellitus

Hypercholesterolemia,

Hypertension

Managed health care

Nurse-based primary health care,

Medical scheme

Primary health care

Risk factors

362.10425068

Medical policy -- South Africa

Medical care -- South Africa -- Finance

Nursing care plans -- South Africa

Health care reform -- South Africa.

Health insurance -- South Africa