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Carcinogênese prostática quimicamente induzida por N-metil N-nitrosuréia (MNU) em gerbilos da Mongólia = associação com promotores esteróides ou dieta hiperlipídica = Prostate carcinogenesis chemically induced by N-methyl-N Prostate carcinogenesis chemically induced by N-methyl-Nnitrosourea: association with steroids promoters or high-fat diet / Prostate carcinogenesis chemically induced by N-methyl-N nitrosourea (MNU) in Mongolian gerbils : association with steroids promoters or high-fat dietGonçalves, Bianca Facchim, 1986- 23 August 2018 (has links)
Orientadores: Sebastião Roberto Taboga, Silvana Gisele Pegorin de Campos / Tese (doutorado) - Universidade Estadual de Campinas, Instituto de Biologia / Made available in DSpace on 2018-08-23T14:53:15Z (GMT). No. of bitstreams: 1
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Previous issue date: 2013 / Resumo: Um dos principais desafios no campo de pesquisa do câncer prostático é a busca por sistemas modelo que permitam a investigação dos aspectos patológicos, bioquímicos e genéticos desta doença. O gerbilo Meriones unguiculatus tem possibilitado a avaliação de lesões prostáticas e sua evolução de estágio benigno para maligno (invasivo) após período relativamente curto de tratamento com o carcinógeno N-Metil-N-Nitrosuréia (MNU), um potente causador de metilação do DNA por ação direta. Assim, o presente trabalho teve por objetivos: 1) Determinar a incidência, multiplicidade e latência tumoral de lesões espontâneas e quimicamente induzidas nos lobos prostáticos ventral e dorsolateral do gerbilo; 2) Investigar se o estradiol exerce papel protetor e/ou promotor sobre neoplasias induzidas por MNU; 3) Avaliar o potencial promotor da dieta hiperlipídica sobre a carcinogênese induzida na próstata ventral; 4) Analisar a participação de produtos alterados de genes ras e do status global de metilação do DNA do epitélio prostático no processo tumoral mediado por MNU. Para tanto foram utilizados animais adultos submetidos à dose única intraperitoneal de MNU (50mg/Kg), exceto o grupo controle. Os grupos experimentais foram submetidos à exposição crônica de andrógeno, estradiol ou dieta hiperlipídica por 14 e 28 semanas. As metodologias aplicadas envolveram análises quantitativas e estatísticas de multiplicidade e incidência de lesões prostáticas, peso corporal, acúmulo de gordura corporal, peso prostático, dosagens hormonais, índice proliferativo, cariometria, frequência de células AR-positivas e basais, status global de metilação e determinação da expressão de proteínas. O modelo de indução tumoral prostática por MNU associado à testosterona no gerbilo se mostrou eficaz, pois reduziu a latência tumoral e permitiu o estudo de estágios avançados da carcinogênese após curto período. As neoplasias se manifestam inicialmente no lobo dorsolateral e requerem um tempo maior para se estabelecer no lobo ventral. No entanto, a progressão de lesões pré-malignas para malignas ocorre de maneira mais significativa no lobo ventral. Isso indica que a progressão tumoral ocorre de maneira distinta entre os lobos prostáticos e que vias alternativas estão possivelmente envolvidas nesse processo. A longa exposição a altas doses de estrógeno foi capaz de prevenir e reduzir a taxa de crescimento tumoral. Apesar dos efeitos terapêuticos contra a progressão neoplásica, a terapia estrogênica levou ao estabelecimento de um epitélio com características distintas da próstata normal, como: mudanças no padrão de metilação do DNA e aumento de células basais e AR positivas. Juntos, esses eventos contribuíram para criar um ambiente epitelial instável que pode provocar a recidiva das lesões em períodos subsequentes. A associação entre MNU e dieta hiperlipídica promoveu aumento na incidência de lesões estimuladas pelo carcinógeno isoladamente, as quais apresentaram maior número de células AR-positivas, ruptura da camada de músculo liso indicando microinvasão tumoral, e alta reatividade para metaloproteinase do tipo 2. A análise molecular indicou alta expressão das proteínas Ras em tecidos induzidos por MNU, sugerindo a participação dessa via na promoção e progressão de tumores prostáticos. Assim, conclui-se que a dieta hiperlipídica pode ser considerada um agente promotor da carcinogênese prostática, e o gerbilo representa um bom modelo para estudos histopatológicos / Abstract: One of the major challenges in the field of prostate cancer research is the search for model systems that allow the investigation of pathological, biochemical and genetic factors of this disease. The gerbil Meriones unguiculatus has enabled the evaluation of prostate lesions and evolution from benign to malignant (invasive) stage after a relatively short period of treatment with the carcinogen N-methyl-N-nitrosourea (MNU), a potent causative of DNA methylation by direct action. Thus, this study aimed to: 1) Determine the incidence, multiplicity, and tumor latency of spontaneous and chemically-induced lesions in ventral and dorsolateral gerbils' prostatic lobes; 2) Investigate whether estradiol exerts protective and/or promoter hole on neoplasms induced by MNU; 3) Evaluate the promotional potential of high-fat diet on induced-carcinogenesis in ventral prostate; 4) Analyze the involvement of altered ras gene products and the global DNA methylation status of prostate epithelium on MNU-mediated tumor process. Therefore, we used adult animals subjected to a single intraperitoneal dose (50mg/kg) of MNU, except the control group. The experimental groups were subjected to chronic exposure of androgen, estradiol or high-fat diet for 14 and 28 weeks. The methodologies involved quantitative and statistical analysis of multiplicity and incidence of prostatic lesions, body weight, body fat accumulation, prostate weight, hormonal measurements, proliferative index, karyometry, frequency of AR-positive and basal cells, global methylation status and determination of protein expression. The model of prostatic tumor induction by MNU associated with testosterone in the gerbil was effective because it reduced tumor latency and allows the study of advanced stages of carcinogenesis after short period. Neoplasms manifest initially in dorsolateral lobe and require a longer time to be established in ventral lobe. However, the progression from premalignant to malignant lesions occurs more significantly in the ventral lobe. This indicates that tumor progression occurs differently between prostatic lobes and alternative pathways maybe possibly involved in this process. Long exposure to high doses of estrogen was able to prevent and reduce the rate of tumor growth. Despite therapeutic effects against neoplastic progression, estrogen therapy led to the establishment of an epithelium with distinct characteristics from normal prostate, such as changes in the pattern of DNA methylation and increased amount of basal cell and ARpositive cells. Together, these events contributed to create an unstable epithelial compartment that can cause lesions recurrence in subsequent periods. The association between MNU and high-fat diet promoted an increase in incidence of lesions stimulated by carcinogen alone, which had a higher number of AR-positive cells, disruption of the smooth muscle layer indicating tumor microinvasion and high reactivity for metalloproteinase type 2. Molecular analysis indicated high expression of Ras proteins in tissues induced by MNU, suggesting the involvement of this pathway in the promotion and progression of prostate tumors. Thus, we conclude that the high-fat diet can be considered a promotional agent of prostate carcinogenesis and that gerbil is a good model for histopathological studies / Doutorado / Biologia Celular / Doutora em Biologia Celular e Estrutural
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Obesidade e resistência à ação da insulina: alterações moleculares, bioquímicas e estruturais. / Obesity and insulin resistance: molecular, biochemical and ultra-structural adaptations.Luciana Oquendo Pereira Lancha 25 November 2009 (has links)
O risco aumentado de mortalidade e morbidade associado à obesidade tem sido alvo de muitos estudos que tentam elucidar os aspectos da Síndrome Metabólica, caracterizada por algumas doenças metabólicas como resistência à insulina, hipertensão, dislipidemia. Apesar de muitos estudos tentarem elucidar as alterações metabólicas decorrentes da obesidade, poucos trabalhos têm analisado as conseqüências da dieta hiperlipídica sobre o metabolismo de aminoácidos. Assim, o objetivo deste estudo foi verificar os possíveis mecanismos responsáveis pelo desenvolvimento da intolerância à glicose após a ingestão de dieta hiperlipídica em ratas saudáveis. Os animais alimentados com dieta hiperlipídica por 60 dias, apresentaram redução na expressão gênica de Glut 4 do receptor de insulina, além de redução na atividade da hexoquinase e aumento na atividade de citrato sintase, aspartato aminotransferase e BCAA transaminase, indicando adaptação nas vias metabólicas, com aumento da atividade do ciclo de Krebs e maior utilização de aminoácidos em reações anapleróticas. / The possible causes of increased mortality and morbidity associated with obesity have been focused by many studies that attempt to understand the metabolic syndrome, characterized by various metabolic disorders such as insulin resistance, hypertension and dyslipidemia. Thus, the aim of this study was to verify the possible mechanisms responsible for developing glucose intolerance after a high fat diet intake in healthy female rats. Female Wistar rats were fed either with high fat diet or with the control diet for several weeks. The rats fed with a high fat diet for 60 days presented impaired Glut 4 and insulin receptor gene expression. High fat diet promoted a reduced activity of hexokinase and increased activity of citrate synthase, aspartate aminotransferase and BCAA transaminase, indicating an adaptation in the metabolic pathway, with increase activity of Krebs cycle and increased usage of amino acids in anaplerotic reactions.
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Charakterizace metabolických účinků omega-3 mastných kyselin u transgenních myší s expresí humánního PPARα / Characterization of metabolic effects of dietary omega-3 fatty acids in transgenic PPARα-humanized miceKalendová, Veronika January 2017 (has links)
Obesity is tightly connected with metabolic diseases including insulin resistance, type 2 diabetes or dyslipidemia. Peroxisome proliferator-activated receptor (PPAR)-α is a key transcription factor involved in the regulation of lipid metabolism, while its activity is stimulated by a variety of hypolipidemic drugs. n-3 polyunsaturated fatty acids (PUFA), including eicosapentaenoic (EPA) and docosahexaenoic (DHA) acid, are endogenous ligands of PPARα, and they are used in the form of fish oil as dietary supplements in order to lower blood lipid levels and to prevent cardiovascular disease. Wax esters represent a novel lipid form of EPA and DHA, and according to recent studies they could exert more potent effects than the classical fish oil (i.e. triacylglycerols). Mice of the 129S1/SvImJ inbred strain were used in the present experiment, and included wild-type (WT) mice, as well as transgenic mice either with the exclusive expression of the human form of PPARα (hPPARα) or mice completely lacking PPARα (PPARα-KO). Mice were fed for 8 weeks the following diets: (i) a control low-fat diet, (ii) obesogenic high-fat diet (cHF), and (iii) the cHF diet supplemented with the n-3 PUFA concentrate in the form of wax esters isolated from marine zooplankton Calanus finmarchicus (ω3Cal). Mice were subjected to...
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Aspects of the interrelation between hypertension and insulin resistanceOsuafor, Godswill Nwabuisi January 2009 (has links)
Magister Scientiae (Medical Bioscience) - MSc(MBS) / Conclusion of this study: These data suggest that 6 weeks of high-fat feeding induces hypertension but does not produce obesity, dyslipidemia and insulin resistance. However, this model may be useful in studying vascular reactivity in hypertension in the absence of insulin resistance. / South Africa
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Aspects of the interrelation between hypertension and insulin resistance: a preliminary studyNwabuisi, Osuafor Godswill January 2009 (has links)
Magister Scientiae (Medical Bioscience) - MSc(MBS) / Background: It is well known that some genetic factors and dietary factors, such as
excessive salt intake and excessive caloric intake (resulting in obesity) are risk factors for hypertension. Fifty percent of all hypertensive patients are also insulin resistant. Both hypertension and insulin resistance are again risk factors for other cardiovascular diseases such as atherosclerosis and heart failure. The nature of the association between hypertension and insulin resistance has not been clearly elucidated. Spontaneously hypertensive rats are the ideal models to study the aspects of the relationships between hypertension and insulin resistance. Models of high-fat feeding induce obesity,hypertension and insulin resistance and are thus used extensively to study hypertension because these models closely mimic some of the renal and cardiovascular changes found in human hypertensive patients. The present study was initiated to evaluate if insulin resistance will develop within 6 weeks in a model of high-fat diet induced hypertension and if so, to determine whether captopril will affect the presence of insulin resistance.This model should in future be used to study vascular reactivity to phenylephrine (PHE),acetylcholine (ACH) and sodium nitroprusside (SNP) in hypertensive animals in theabsence or presence of insulin resistance and in normotensive insulin resistant animals. Methods: In a series of experiments, rats were divided into four groups that received different treatments: (i) laboratory pellets, (ii) high-fat diet, (iii) high-fat diet plus captopril and (iv) high-fat diet plus vehicle. Body weight was measured weekly for 6 weeks. Systolic blood pressure (SBP) and diastolic blood pressure (DBP) were measured every week during the 6-weeks feeding period by the tail cuff method using a two channel computerized non-invasive system from Kent Scientific Corporation, USA.m Intraperitonealy glucose tolerance tests (IPGTTs) were performed at week 3 and week 6.After 6 weeks, and after an overnight fast, the plasma lipid profile was determined using a portable CardiochekTM blood test system. Fasting plasma insulin was determined using an immunoenzymatic assay for the in vitro quantitative measurement of rat insulin (INS) in serum and plasma. Insulin sensitivity was estimated by the quantitative insulin sensitivity check index (QUICKI) using the fasting plasma insulin and fasting glucose levels. After week 6 on the high-fat diet, thoracic aortae from the control and high-fat fed(HFD) animals were excised and vascular response to PHE, ACH and SNP were assessed in intact and denuded endothelium.Result: High-fat feeding did not cause a significant increase in body weight. High-fat feeding significantly increased systolic blood pressure from 125±2.1 mmHg in control animals to 155±5.9 mmHg in the HFD group (P < 0.05) and 158±5.6 mmHg in the HFDV group (P < 0.05). Diastolic blood pressure was increased from 86±2.8 mmHg in the control group to 117±2.5 mmHg in the HFD group (P < 0.05) and 113±3.4 mmHg in the HFDV group (P < 0.05). Visceral fat was increased from 0.8±0.1g in the control group to 3.1±0.6 g in the HFD group and 3.8±0.6 g in the HFDV group. IPGTTs performed at weeks 3 and 6 respectively did not differ significantly from the control group as evidenced from the AUC’s at weeks 3 and 6 respectively. High-fat feeding had no significant effects on blood cholesterol, triglyceride, high-density lipoprotein cholesterol (HDL-C), low-density lipoprotein cholesterol (LDL-C) values or and fasting plasma insulin levels. The KCl induced contraction in both aortic rings with intact and denuded endothelium did not differ significantly between the control and HFD groups (P= 0.4 and 0.8) respectively. The contraction mediated by KCl in aortic rings with intact
and denuded endothelium from the control or HFD groups also did not differ significantly(control: intact vs denuded, P = 0.2; HFD: intact vs denuded, P = 1). Dose responsecurves(1-10 μM) to PHE indicated slightly stronger contractions in the high-fat fed animals at submaximal doses tested. The maximum contraction achieved was however the same (94±19% and 99±2.6% relative to KCl induced contraction, in the control and HFD group respectively, P<0.05). Relaxation responses to ACH and SNP represent preliminary data.Conclusion: These data suggest that 6 weeks of high-fat feeding induces hypertension but does not produce obesity, dyslipidemia and insulin resistance. However, this model may be useful in studying vascular reactivity in hypertension in the absence of insulin
resistance.
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Influences génétique et environnementale de la génération de thrombineSanchez, Caroline 07 March 2011 (has links)
Dans ce travail nous nous sommes intéressés à caractériser les modulateurs génétiques et environnementaux de la génération de thrombine (ETP).Nous avons montré que le taux d’antithrombine (AT) peut être considéré comme un facteur continu de risque de thrombose. L’ETP, le plus élevé, est observé chez les porteurs d’un déficit quantitatif en AT. Les porteurs de la mutation AT Cambridge II présentent également une augmentation de l’ETP. Parallèlement à l’AT, nous avons confirmé l’effet positif de l’allèle PT 20210A sur la génération de thrombine d’autant plus qu’il existe des antécédents personnels de thrombose veineuse (TV). A côté de ces contributions, nous avons confirmé le rôle des taux plasmatiques de fibrinogène et de facteur II, du groupe sanguin et de la prise de contraceptifs oraux sur l’ETP.Nos résultats montrent également que chez le rat, un régime riche en graisses a un effet sur la génération de thrombine. Le régime gras maintient des taux élevés d’ETP après le sevrage, alors qu’une alimentation standard le diminue. Cet effet est partiellement expliqué par l’élévation des taux de facteur VII coagulant et ne suit pas l’évolution des modifications classiques du métabolisme glucidolipidique. Les niveaux élevés d’ETP observés pendant une alimentation riche en graisses se normalisent quatre semaines après le retour à une alimentation standard.En conclusion nos données suggèrent que l’ETP peut être considéré comme un indicateur de l’état prothrombotique des patients, mais son utilisation à l’échelle individuelle dans la prédiction du risque de thrombose veineuse reste à approfondir. La mesure de la génération de thrombine peut être un outil utile pour évaluer les conséquences des modifications du régime alimentaire ou des médicaments pour traiter l’obésité sur le potentiel procoagulant circulant / In this work, we studied genetic and environmental modulators of thrombin generation by endogenous thrombin potential (ETP).We showed that plasma levels of antithrombin (AT) can be considered as risk factors for thrombosis. ETP levels are higher in patients presenting a quantitative defect of AT. In addition, mutation AT Cambridge II is also associated with an increase of ETP. Besides the AT, we confirmed a positive effect of the prothrombin 20210A allele on thrombin generation, especially in presence of venous thrombosis antecedents. These contributions, we have confirmed the role of plasma fibrinogen and factor II, blood group and oral contraceptives on thrombin generation.In addition, our results also showed an effect of high fat diet on thrombin generation in rats. Conversely to the standard fat diet, high fat diet maintened high levels of ETP after weaning. High fat diet-induced effects persisted four weeks after switching to standard fat diet. This effect could be partially explained by higher rates of coagulation factors VII and did not follow classical changes in glucidolipidic metabolism.In conclusion our data suggest that ETP can be considered as an indicator of the prothrombotic state in patients, but require more explanation to predict a risk of venous thrombosis. The measurement of thrombin generation may be a useful tool for assessing the impact of changes in diet or medication to treat obesity on circulating procoagulant potential.
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Regulação anômala da autofagia em tecido adiposo na obesidade / Defective regulation of adipose tissue autophagy in obesityNuñez, Carla Evelyn Coimbra, 1979- 22 August 2018 (has links)
Orientadores: Eliana Pereira de Araújo, Lício Augusto Velloso / Tese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciências Médicas / Made available in DSpace on 2018-08-22T10:03:16Z (GMT). No. of bitstreams: 1
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Previous issue date: 2013 / Resumo: A obesidade e caracterizada pelo acumulo excessivo de gordura no organismo, podendo resultar em dano a saúde. Mudança socioeconômica, ocorrida nos últimos cinquenta anos tem contribuído para o aumento da prevalência da obesidade, a qual e hoje considerada um dos principais problemas de saúde publica no mundo. O acumulo progressivo de ácidos graxos no tecido adiposo, e eventualmente, em outros sítios anatômicos não especializados na estocagem de energia sob a forma de gordura como, por exemplo, o fígado e o músculo, e associado à ativação de uma resposta inflamatória subclinica que desempenha papel importante na indução da resistência a insulina. Esta, por sua vez, e considerada o mecanismo fisiopatogênico unificador de uma serie de doenças comumente associadas à obesidade, tais como o diabetes mellitus, a aterosclerose, a esteatohepatite nao-alcoolica, entre outros. A inflamação subclinica desempenha um papel central na indução da resistência a insulina em obesos. Atualmente o estresse de reticulo endoplasmático e a ativação da sinalização do TLR4 vêm sendo identificados como potenciais mecanismos ativadores da inflamação sub-clinica associada à obesidade. No ambiente intracelular a ativação dos sinais inflamatórios disparados por ambos, estresse de reticulo endoplasmático ou TLR4, podem associar-se, modulando ou sendo modulado por outros eventos. Um desses eventos e a autofagia que se caracteriza como um processo celular finamente regulado e desempenha um papel importante no controle de varias funções da célula, tais como, reciclagem de organelas, disponibilidade de nutrientes e diferenciação celular. Um estudo recente demonstrou a existência de aumento na atividade autofágica em tecido adiposo de pessoas obesas e propôs a associação causal entre autofagia e resistência a insulina. A redução da adiposidade e o mecanismo mais eficiente para reduzir à resistência a insulina em pessoas obesas. Entretanto, o impacto da redução de adiposidade sobre a regulação da autofagia no tecido adiposo não e conhecido. Neste estudo, a regulação da autofagia no tecido adiposo durante o emagrecimento foi observada em duas etapas distintas. Inicialmente, um modelo animal de obesidade induzida por dieta, submetido posteriormente, a restrição calórica de 40% durante quinze dias. Animais obesos alimentados ad libitum, apresentaram aumento dos marcadores de autofagia no tecido adiposo, o que foi revertido na restrição calórica. De forma diversa, a restrição ocasionou o aumento da autofagia nos animais magros. A reintrodução de alimentação ad libitum foi suficiente para reduzir a autofagia nos animais magros, mas não nos obesos, cuja supra-regulacao da autofagia foi mais uma vez observada. Na segunda parte do estudo, autofagia foi avaliada em fragmentos de tecido adiposo subcutâneo de pacientes obesos selecionados para cirurgia bariátrica colhidos no ato da cirurgia e apos um ano, aproximadamente. Foram incluídos no estudo nove pacientes obesos não-diabeticos e seis pacientes obesos diabéticos. Assim como no modelo animal, obesidade em humanos foi associada a um aumento dos marcadores de autofagia no tecido adiposo os quais foram reduzidos apos a perda de peso. Assim, na vigência da obesidade ocorre uma regulação anômala da autofagia, estando aumentada durante alimentação ad libitum e reduzindo-se com a restrição alimentar / Abstract: Obesity, defined as abnormal or excessive fat accumulation that may impair life quality, is one of the major public health problems in modern world. It results from an imbalance between food intake and energy expenditure leading to the progressive accumulation of fatty acids in the adipose tissue and in some tissues that are not specialized in energy storage, such as liver and muscle. Insulin resistance is one of the main outcomes of obesity and is regarded as the main mechanism connecting diseases that are commonly associated with obesity, such as, type 2 diabetes mellitus, atherosclerosis, and non-alcoholic steatohepatitis, among others. Subclinical inflammation plays a major role in the induction of insulin resistance in obesity. Recently, endoplasmic reticulum stress and the activation of TLR4 signaling have been identified as potential triggering mechanisms for obesity-associated subclinical inflammation. At the intracellular environment activation of inflammatory signaling triggered by either endoplasmic reticulum stress or TLR4 signaling can integrate and modulate or be modulated by other cellular events. One such event is autophagy which is a highly regulated process that plays an important role in the control of a wide range of cellular functions such as organelle recycling, nutrient availability and tissue differentiation. A recent study has shown an increased autophagic activity in the adipose tissue of obese subjects, and a role for autophagy in obesity associated insulin resistance was proposed. Body mass reduction is the most efficient approach to tackle insulin resistance in over-weight subjects; however, the impact of weight loss in adipose tissue autophagy is unknown. In this study we used a two-step approach to evaluate adipose tissue autophagy during body mass reduction. First, a mouse model of diet-induced obesity and diabetes was submitted to a fifteen-day, 40% caloric restriction. At base-line, markers of autophagy were increased in obese mice as compared to lean controls. Upon caloric restriction, autophagy increased in the lean mice, while decreasing in the obese mice. The reintroduction of ad libitum feeding was sufficient to rapidly reduce autophagy in the lean mice and increase autophagy in the obese mice. In the second part of the study, autophagy was evaluated in the subcutaneous adipose tissue of nine obese-non-diabetic and six obese-diabetic subjects undergoing bariatric surgery for body mass reduction. Specimens were collected during the surgery, and approximately one year later. As in the mouse model, human obesity was associated with increased autophagy and body mass reduction led to an attenuation of autophagy in the adipose tissue. Thus, while caloric restriction leads to increased autophagy in the adipose tissue in lean subjects, in obesity, autophagy is defectively regulated, being increased during ad libitum feeding and reduced upon caloric restriction / Doutorado / Clinica Medica / Doutora em Ciências
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Étude de la surexpression du récepteur activé par les proliférateurs de peroxysomes (PPAR) b/d spécifiquement dans les lymphocytes T : effet sur l’inflammation associée à l’obésité et à un choc septique / Study of T cell-specific overexpression of Peroxisome proliferator activated receptor (PPAR) b/d : effect on inflammation associated with obesity and septic shockLe Menn, Gwenaëlle 11 December 2018 (has links)
Le récepteur activé par les proliférateurs de peroxysomes (PPAR) b/d est un facteur de transcription impliqué dans l’activation de la voie d’oxydation des lipides qui possède également une fonction anti-inflammatoire. Étudié chez les macrophages, son rôle reste très peu connu dans d’autres cellules immunitaires comme les lymphocytes T. Nous avons généré un nouveau modèle murin où PPARb/d est surexprimé spécifiquement dans les lymphocytes T (souris Tg T-PPARb), afin d’étudier l’effet de sa surexpression sur le développement ainsi que la fonction des lymphocytes T grâce à deux types de challenges : métabolique et immunitaire. Nos résultats ont permis de mettre en évidence un rôle de PPARb/d dans le développement des lymphocytes T ab (blocage de leur développement) mais pas des lymphocytes T gd. On observe alors une diminution de 70% du nombre de lymphocytes T ab dans les organes lymphoïdes conduisant à une diminution du ratio de Lymphocytes T ab/gd. Les lymphocytes T ab qui arrivent tout de même à se développer ne surexpriment pas PPARb/d. Au cours d’un challenge métabolique (régime hyperlipidique), nous avons observé que les souris Tg T-PPARb sont partiellement protégées contre l’obésité. Elles présentent également une amélioration de leur phénotype métabolique (sensibilité à l’insuline et au glucose, stéatose hépatique) et inflammatoire (diminution de l’inflammation des dépôts de tissus adipeux). Au cours d’un challenge immunitaire (injection de LPS), nous observons une diminution du nombre de macrophages pro-inflammatoires M1 dans la cavité péritonéale des souris Tg T-PPARb dès 1h post-injection. Chez les souris contrôles, ce phénomène est visible à partir de 3h postinjection de LPS. Il semble ainsi que la réponse immunitaire des souris Tg T-PPARb soit plus précoce que celle des souris contrôles en réponse à un challenge immunitaire. En conclusion, la surexpression de PPARb spécifiquement dans les lymphocytes T semble provoquer une altération des populations de lymphocytes T ainsi qu’une potentielle modification de leur fonction qui pourraient expliquer que les souris Tg T-PPARb réagissent mieux que les souris contrôles lorsqu’elles sont soumises à différents types de challenges (immunitaire ou métabolique). / The Peroxisome Proliferator Activated Receptor (PPAR) b/d is a transcription factor involved in the activation of the lipid oxidation pathway that also has an anti-inflammatory function. While well-studied in macrophages, its role in other immune cells like in T cells remains largely unknown. We have generated a new mouse model in which PPARb/d is specifically overexpressed in T cells (Tg T-PPARb mice) and studied the effect of its overexpression on the development and the function of T cells through two types of challenge: metabolic and immune. Our results show a role of PPARb/d in the development of ab T cells (blocking their development) but not gd T cells. There is then a 70% decrease in the number of ab T cells in lymphoid organs leading to a decrease in the ab/gd T cell ratio. ab T cells that are still able to develop do not overexpress PPARb/d. During a metabolic challenge (high fat diet), we observed that Tg T-PPARb mice are partially protected against high fat diet inducedobesity. They also show an improvement in their metabolic (insulin and glucose sensitivity, hepatic steatosis) and inflammatory phenotype (decrease in inflammation in adipose tissue depots). During an immune challenge (LPS injection), we observed a decrease in pro-inflammatory M1 macrophage number in the peritoneal cavity of Tg TPPARb mice at 1h post-injection. In control mice, this phenomenon is seen at 3h post-injection of LPS. Thus, it appears that the immune response in Tg T-PPARb mice is faster than the one in control mice in response to an immune challenge. In conclusion, PPARb/d overexpression specifically in T cells appears to cause an alteration in T cell population as well as a potential change in their function which could explain that Tg T-PPARb mice respond better than control mice when they are subjected to different types of challenges (immune or metabolic).
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Účinky obezity a metabolického syndromu v průběhu infekce Trypanosoma Cruzi / Effects of obesity on the course of Trypanosoma cruzi infectionBrima, Wunnie January 2016 (has links)
Obesity is very widespread and detrimental to health. Obesity brings with it many changes including heightened immune function, and a higher prevalence of major cardiovascular disorders, cancer, diabetes, and Alzheimer disease. Obesity is also associated with shortened lifespan. The detrimental effects of obesity are linked to the "metabolic syndrome", a broad range of changes in metabolic processes and immune function. As a first approximation, we agree with this formulation but we will then proceed to document some of its weaknesses. (i) Crude mortality rates increase with increasing body mass index (BMI) but as the BMI approaches the normal range, mortality rates reverse (the now classic "J-shaped curve") so that individuals with reduced BMI have elevated mortality. (ii) A multiplicity of medical and surgical conditions have been reported where short term and medium term outcomes are better for overweight patients. These conditions are placed under the heading of "obesity paradox". (iii) The medical community has introduced a binary system for the metabolic syndrome ---- yes, patient has it or no, the patient does not have it, despite the fact that all of the changes that are considered components of the metabolic syndrome are continuous variables. Our work is focused on sharpening focus and improving...
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260 |
Účinky obezity a metabolického syndromu v průběhu infekce Trypanosoma Cruzi / Effects of obesity on the course of Trypanosoma cruzi infectionBrima, Wunnie January 2016 (has links)
Obesity is very widespread and detrimental to health. Obesity brings with it many changes including heightened immune function, and a higher prevalence of major cardiovascular disorders, cancer, diabetes, and Alzheimer disease. Obesity is also associated with shortened lifespan. The detrimental effects of obesity are linked to the "metabolic syndrome", a broad range of changes in metabolic processes and immune function. As a first approximation, we agree with this formulation but we will then proceed to document some of its weaknesses. (i) Crude mortality rates increase with increasing body mass index (BMI) but as the BMI approaches the normal range, mortality rates reverse (the now classic "J-shaped curve") so that individuals with reduced BMI have elevated mortality. (ii) A multiplicity of medical and surgical conditions have been reported where short term and medium term outcomes are better for overweight patients. These conditions are placed under the heading of "obesity paradox". (iii) The medical community has introduced a binary system for the metabolic syndrome ---- yes, patient has it or no, the patient does not have it, despite the fact that all of the changes that are considered components of the metabolic syndrome are continuous variables. Our work is focused on sharpening focus and improving...
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