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Imunossensor baseado em grafeno-polissulfona para detecção da artrite reumatoide: antipeptídeo citrulinadoSILVA JÚNIOR, Auvani Antunes da 09 March 2016 (has links)
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Previous issue date: 2016-03-09 / CAPEs / A artrite reumatóide (AR) é uma doença crônico-degenerativa, sistêmica, auto-imune. Atualmente, o anticorpo antipeptídeo citrulinado cíclico (Anti-PCC) é considerado o marcador mais importante para o diagnóstico preditivo e prognóstico da AR. Neste trabalho, desenvolveu-se um imunossensor eletroquímico para detecção do Anti-PCC, a partir da modificação da superfície de um eletrodo de carbono vítreo com nanocompósito de óxido de grafeno reduzido-polissulfona (Gor-PSF) o qual apresenta boas características de aumento da área eletrocatalítica e imobilização de moléculas biológicas. Foram realizados capturas de imagens micrográficas por microscopia eletrônica de varredura da superfície do eletrodo de trabalho antes e após sua modificação, pelas quais foi possível comprovar uma superfície lisa não modificada sem estruturas adsorvidas após limpeza física, e que a superfície modificada com Gor-PSF apresentou um recobrimento ideal de toda a superfície com a presença de uma estrutura esponjosa comprovando a modificação da área de trabalho. Para captura do Anti-PCC, antígenos citrulina (CCP-Ag) foram imobilizados sobre a superfície eletródica do nanocompósito por provável ligação covalente entre os grupos amino e carboxilícos presentes no CCP-Ag e no óxido de grafeno reduzido, respectivamente. A técnica de voltametria de onda quadrada (VOQ) foi empregada para detecção do Anti-PCC, produzindo um imunossensor livre de marcação. Observou-se que o GOR-PSF foi capaz de aumentar a corrente de pico anódico (Ipa) 2,2 vezes mais, comparado com o controle (sem GOR-PSF) demonstrando que o filme proporcionou melhor capacidade eletrocatalítica, sendo também estável (coeficiente de variação da corrente < 1 %) avaliado por submeter o eletrodo a 20 ciclos consecutivos de voltametria cíclica. O imunossensor proposto apresentou uma boa linearidade com r=0,983 (p<0.003; n = 5) e limite de detecção de 0,004 ng/mL de Anti-PCC. A plataforma sensora demonstrou propriedades desejáveis de estabilidade, sensibilidade e reprodutibilidade na detecção de Anti-PCC com perspectivas de desenvolvimento de dispositivos “point-of-care”. / Rheumatoid arthritis (RA) is a chronic degenerative disease, systemic, autoimmune. Currently, the cyclic citrullinated peptide (anti-CCP) is considered the most important predictive marker for the diagnosis and prognosis of RA. In this work, we developed an electrochemical immunosensor for the detection of anti-CCP, from the surface modification of a glassy carbon electrode with nanocomposite reduced-polysulfone graphene oxide (GOr-PSU) which has good rise characteristics of electrocatalytic area and immobilization of biological molecules. of micrographic images catches were performed by scanning electron microscopy of the surface of the working electrode before and after modification, by which it was possible to establish a smooth unmodified without adsorbed structures after physical cleaning, and that the modified surface with GOr-PSU presented an ideal coating the entire surface with the presence of a spongy structure confirming the modification of the work area. For capture of anti-CCP, citrulline antigens (Ag-CCP) were immobilized on the electrode surface of the nanocomposite probably due to covalent bond between the amino and carboxylic groups present in the CCP-Ag and the reduced graphene oxide, respectively. Square wave voltammetry technique (VOQ) was used for detection of anti-CCP producing a marking-free immunosensor. It was observed that the GOR-PSU was capable of increasing the anodic peak current (IPA) 2.2 times as compared with the control (without GOr-PSU) demonstrating that the electrocatalytic film provided better capacity also being stable (coefficient the variation of the current <1%) evaluated by subjecting the electrode 20 consecutive cycles of cyclic voltammetry. The proposed immunosensor exhibited good linearity with r = 0.983 (p <0.003; n = 5) and a detection limit of 0.004 ng / ml anti-CCP. The sensing platform demonstrated desirable properties of stability, sensitivity and reproducibility in the Anti-CCP detection with prospects of development of devices "point-of-care."
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Artrite reumatóide: avaliação de citocinas (IL-6e IL-10) da frequência da IgG do parvovírus B19 e desenvolvimento de um biossensor para antipeptídeo citrulinado cíclico (ACCP)MARIANO, Maria Helena Q. Araújo 26 May 2014 (has links)
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Previous issue date: 2014-05-26 / A artrite reumatóide (AR), é uma doença crônica inflamatória, em cuja etiologia estão
envolvidos fatores genéticos, ambientais e infecções. Dentre as infecções se
destacam as virais cujas proteínas modificam a função dos sinoviócitos como ocorre
com o Parvovírus B19 (PVB19). Estudos tem mostrado a participação das citocinas
IL-6 e L-10 na fisiopatogenia da AR. O diagnóstico da AR se baseia em critérios
clínicos, radiológicos e laboratoriais.Dentre os auto- anticorpos, o fator reumatóide
(FR) apresenta alta sensibilidade e baixa especificidade. Por lado, o anticorpo
antipeptídeo citrulinado cíclico (ACCP) é um importante marcador para o diagnóstico
e tem valor preditivo de um pior prognóstico. Sua detecção pelo ELISA, têm mostrado
excelente desempenho diagnóstico, embora seja oneroso e mais demorado. Visando
diagnósticos mais rápidos e práticos, os biossensores são ideais para testes tipo
“point-of-care” devido à sua portabilidade. Os objetivos desta tese foram: avaliar a
correlação dos niveis séricos de IL-10, IL-6 e a frequência do anti-IgG PVB19 com
atividade clínica da AR mediante os índices compostos de atividade de doença
(ICADs).em diferentes tratamentos e desenvolver um imunossensor eletroquímico
label free para ACCP.Foi desenvolvido um estudo transversal para estimar a
frequencia de anti-IgG PVB19 e determinar os níveis séricos da IL6 e IL10 pelo
método ELISA.O imunossensor constituído por eletrodos screen printed de ouro,foi
baseado no uso da SAM formada pela deposição do àcido tioglicólico.Oa antígenos
foram imobilizadosde modo orientado via grupos carboxílicos do TGA. Os resultados
mostraram uma frequencia de 73% (60/83) de IgG anti-PVB19 e uma correlação
significativa entre os níveis de IL-6 e as medidas de atividade de AR nos pacientes
com maior atividade inflamatória pelo EULAR. O maior contigente de pacientes IgG
anti-PVB19 positivos estava com moderada e alta atividade pelo EULAR.O
imunossensor eletroquímico apresentou uma resposta linear na curva de calibração,
bom coeficiente de correlação e limite de detecção menor do que o método ELISA. / Rheumatoid arthritis (RA) is a chronic inflammatory disease, whose etiology is influenced by
genetics, the environment, and infections. Among the various types of infections, the ones that
stand out are the viral infections whose proteins alter the function of synoviocytes as occurs
with Parvovirus B19 (PVB19). Studies have shown the involvement of the IL-6 and IL-10
cytokines in the physiopathogenesis of RA. Diagnosis of RA is based on clinical, radiological,
and laboratory criteria. In the autoantibodies, the rheumatoid factor (RF) has high sensitivity
and low specificity. The Anti-cyclic Citrullinated Peptide (anti-CCP) is an important marker for
the diagnosis and as a predictive value of a worst-case prognosis.Its detection by ELISA has
shown excellent diagnostic performance, but it is expensive and takes longer.Aiming for faster
and more practical diagnostics, biosensors are ideal for point-of-care testing, due to their
portability. The objectives of this thesis were to evaluate the correlation of the serum levels of
IL-10 and IL-6and the frequency of anti-IgG PVB19,with the clinical activity of RA, via
composite indices of disease activity, under different treatments, in order to develop a labelfree
electrochemical immunosensor for anti-CCP. A cross-sectional study was developed to
estimate the frequency of anti-IgGPVB19and to determine the serum levels of IL-6 and IL-10
by the ELISA method. The immunosensor consisting of screen-printed gold electrodes was
based on the use of the self-assembled monolayer (sam) formed by deposition of thioglycolic
acid. The antigens were immobilized, driven via carboxylic groups of the TGA. The results
showed a frequency of 73% (60/83) of IgG anti-PVB19 and a significant correlation between
the levels of IL-6 and the activity measures of AR in the patients with higher inflammatory
activity according to the EULAR. Most of the IgG anti-PVB19 positive patients had moderate
and high activity according to the EULAR. The electrochemical immunosensor showed a linear
response in the calibration curve, a good correlation coefficient, and a detection limit lower
than the ELISA method.
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Metabolic Regulation of T cell Responses by Antigen Presenting CellsCrowther, Rebecca 22 August 2022 (has links)
No description available.
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NUTRITIONAL AND CONTRACTILE REGULATION OF HUMAN MUSCLE PROTEIN SYNTHESIS: ROLE OF LEUCINE AND CITRULLINEChurchward-Venne, Tyler A. 04 1900 (has links)
<p>Amino acids are key nutritional stimuli that are both substrate for muscle protein synthesis (MPS), and signaling molecules that regulate the translational machinery. There is a dose-dependent relationship between protein intake and MPS that differs between young and elderly subjects. The current thesis contains results from three separate studies that were conducted to examine to potential to enhance smaller doses of protein, known to be suboptimal in their capacity to stimulate MPS, through supplementation with specific amino acids, namely leucine and citrulline.</p> <p>The first two studies examined the potential to enhance the muscle protein synthetic capacity of a smaller, suboptimal dose of whey protein with leucine. In study one, we concluded that leucine supplementation of a suboptimal dose of protein could render it as effective at enhancing rates of MPS as ~four times as much protein (25 g) under resting conditions, but not following resistance exercise. In study two, we examined the potential of leucine and branched-chain amino acids to enhance the MPS response of a suboptimal dose of protein within the context of mixed macronutrient ingestion. We concluded that supplementation with a relatively high dose of leucine could render it as effective at enhancing MPS rates as ~four times as much protein (25 g) under both resting and post-exercise conditions.</p> <p>In study three, we examined the potential of citrulline supplementation to enhance blood flow, microvascular circulation, and MPS in response to a suboptimal dose of whey protein in elderly subjects. We concluded that supplementation of a suboptimal dose of protein with citrulline did not augment bulk blood flow or muscle microvascular circulation. The major findings from the works presented in this thesis is that smaller doses of protein that normally elicit a suboptimal increase in MPS can be made more anabolic when supplemented with specific amino acids.</p> / Doctor of Philosophy (PhD)
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Intégrité de la muqueuse intestinale en présence d'obésité, de résistance à l'insuline et de dyslipidémieLalande, Catherine 02 February 2024 (has links)
Plusieurs études ont démontré des altérations de la muqueuse intestinale en contexte d’altérations métaboliques reliées à l’obésité chez des modèles animaux, et, plus récemment, des sujets humains. Toutefois, l’acquisition d’échantillons, effectuée par biopsies, est limitée par son caractère invasif. L’emploi de biomarqueurs sanguins de la fonctionnalité et de l’intégrité de l’intestin grêle permettrait d’augmenter le nombre de participants humains, mais également d’inclure des participants en santé ne présentant pas de pathologies intestinales. L’objectif de cette étude est d’évaluer le potentiel de la citrulline et de la protéine de liaison aux acides gras spécifique à l’intestin (I-FABP) à percevoir les changements fonctionnels et morphologiques de la muqueuse intestinale de participants présentant un large éventail d’adiposité et de sensibilité à l’insuline. Nous avons démontré que les taux plasmatiques de citrulline, marqueur de la masse et de la fonctionnalité entérocytaire, étaient diminués en présence d’obésité, de résistance à l’insuline (RI) et de diabète de type 2. L’I-FABP, marqueur de l’apoptose entérocytaire est, quant à elle, augmentée chez les diabétiques de type 2 (DT2), principalement ceux dont le diabète n’était pas contrôlé. Le ratio I-FABP/citrulline, marqueur du renouvellement cellulaire, était plus élevé à la fois chez les hommes RI et DT2. Nos résultats démontrent la présence de changements au niveau de la masse et de la fonctionnalité de la muqueuse intestinale en contexte d’altérations métaboliques associées à l’obésité, en particulier celles affectant l’homéostasie du glucose. L’utilisation de biopsies ou encore des méthodes d’imagerie par des études ultérieures serait bénéfique à la validation des changements morphologiques observés. Une meilleure connaissance de l’intestin grêle est essentielle afin de mieux comprendre son impact sur les maladies métaboliques ainsi que ses interactions avec le microbiote. / Several studies have shown small intestinal adaptations in obesity-related metabolic alterations in both animal and human models. However, access to sample is impeded by the invasive procedure it requires. Using plasma biomarkers to assess small intestinal integrity and functionality could improve the sample size of studies, and also to include healthy subjects without enteropathies. Our goal is to evaluate citrulline and intestinalspecific fatty-acid binding protein (I-FABP) ability to assess functional and morphological changes in the small mucosa of men with a wide range of adiposity and insulin sensitivity. In our study, citrulline, a marker of enterocyte mass and function, was lower in subjects with obesity, insulin resistance and type 2 diabetes. I-FABP, an apoptosis marker, was higher in type 2 diabetic (T2D) men, especially those with uncontrolled T2D. I-FABP/citrulline ratio, a marker of enterocyte turnover, was higher in both T2D and insulin resistant (IR) men. In conclusion, alterations in small intestinal mucosa mass and integrity were observed in obesity-related metabolic alterations, especially those related to glucose homeostasis. To assess morphological changes, biopsies or imagery should be included in future studies. A better understanding of the small intestine is crucial to understand its impacts on metabolic alteration and its interactions with the microbiota
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Impact de la citrulline sur le métabolisme du tissu adipeux / Citrulline effect on adipose tissue metabolismJoffin, Nolwenn 29 January 2015 (has links)
L’obésité s’accompagne de pathologies comme le diabète de type 2 et les maladies cardiovasculaires, liées à des dérégulations métaboliques et endocriniennes du tissu adipeux blanc (TAB). Au cours du vieillissement, la perte de masse musculaire peut être associée à l’obésité et définit le concept d’obésité sarcopénique. Les traitements mis en œuvre pour contrecarrer ces pathologies n’ont qu’un succès très partiel. Il est donc opportun de développer des stratégies alternatives originales qui pourraient aboutir à des thérapeutiques ciblées. Notre équipe étudie les régulations métaboliques du TAB, source majeure de stockage de l’énergie de l’organisme. Les triglycérides stockés sont libérés à jeun grâce à la lipolyse qui libère les acides gras non-estérifiés (AGNE) et le glycérol dans le sang, comme source d’énergie des autres tissus. En plus de la β-oxydation des AGNE, leur ré-estérification partielle intervient pour limiter leur libération lors de la lipolyse. La glycéronéogenèse est nécessaire à la ré-estérification en situation de jeûne. Des études préalables ont montré que l'administration de citrulline (CIT) pendant trois mois à des rats vieillissants induit une diminution d’environ 40% de la masse viscérale du TAB. Cet acide aminé non protéique est un complément alimentaire donné au cours du vieillissement ou à des sportifs pour augmenter la masse musculaire. Nous avons étudié les effets de la CIT sur des cultures d’explants de TAB de rats. Dans la première partie de ce travail, nous montrons que la CIT a un effet direct lipolytique et anti-glycéronéogénique sur les explants des rats qu’ils soient jeunes ou âgés. Cependant, la libération des AGNE du TAB des rats jeunes est limitée par une augmentation de la capacité oxydative du tissu. Avec l’âge, la masse du TAB augmente en parallèle à l’augmentation d’un état pro-inflammatoire. Afin de comprendre l’influence de ces deux paramètres indépendamment de l’âge, nous avons étudié dans la deuxième partie de ce travail, les effets de la CIT sur les explants de TAB de rats jeunes soumis à un régime contrôle (CD) ou hyperlipidique (HFD). Nous observons une augmentation, induite par la CIT, de la lipolyse et de la capacité ß-oxydative du TAB des rats quel que soit le régime, alors que la glycéronéogenèse est diminuée. Toutefois, les AGNE sont sélectivement libérés par le TAB de rats HFD, en relation avec une réduction drastique de leur ré-estérification. Le NO est un médiateur de ces effets. Dans une troisième partie, nous démontrons que la CIT agit directement sur le TAB de rats CD et HFD pour induire l'expression de la protéine découplante, UCP1, en lien avec le « brunissement » potentiel du TAB par cet acide aminé. Ces effets ne sont pas observés au sein du TAB des rats âgés. L’ensemble de nos résultats établit les bases pour de futures investigations visant à élucider les mécanismes par lesquels la CIT réduit la masse adipeuse et ouvre de nouvelles perspectives thérapeutiques pour lutter contre le surpoids et l’obésité sarcopénique. / Obesity is frequently associated with type 2 diabetes and cardiovascular diseases, related to metabolic and endocrine dysregulation of white adipose tissue (WAT). During aging, the loss of muscle mass may be associated with obesity and defines the concept of sarcopenic obesity. Treatments implemented to counteract these conditions showed a very partial success. It is therefore appropriate to develop original alternative strategies that could lead to targeted therapies. Our team studies the metabolic regulation of WAT, the major source of energy storage in the body. Non-esterified fatty acids (NEFA) and glycerol are released in the blood from stored triglycerides through lipolysis and used as a source of energy for other tissues. In addition to their β-oxidation, NEFA are re-esterified in part, a process that limits their release in the blood. Glyceroneogenesis is the pathway necessary to NEFA re-esterification in the fasting state. Previous studies showed that administration of citrulline (CIT) for three months to aging rats induced a decrease of approximately 40% of the visceral WAT mass. This non-protein amino acid is given as a dietary supplement during aging or sports to increase muscle mass. We studied the effects of CIT on explant cultures of rat WAT. In the first part of this work, we show that CIT exerts a direct lipolytic and anti-glyceroneogenic effect on explants from rats whether young or old. However, the release of NEFA from the explants of young rats is limited by an increase in the oxidative capacity of the tissue. During aging, WAT mass augments in parallel to the increase in a pro-inflammatory state. To understand the influence of these two parameters regardless of age, we studied in the second part of this work, the effects of CIT on WAT explants from young rats fed a control (CD) or high fat (HFD) diet. We show an CIT-induced increase in lipolysis and beta-oxidative capacity of WAT from rats whatever the diet, while glyceroneogenesis is reduced. However, NEFA are selectively released from WAT of HFD rats, in connection with a drastic reduction of their re-esterification. NO is a mediator of these effects. In the third part of this work, we show that CIT acts directly on WAT from CD and HFD rats to induce the expression of uncoupling protein, UCP1, in line with the potential "browning" of WAT by this amino acid. These effects were not observed in explants from old rats. Altogether our results establish the basis for future investigations aimed at elucidating the mechanisms by which CIT reduces body fat and open new therapeutic perspectives to fight overweight and sarcopenic obesity.
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Impact de la citrulline sur le métabolisme du tissu adipeux / Citrulline effect on adipose tissue metabolismJoffin, Nolwenn 29 January 2015 (has links)
L’obésité s’accompagne de pathologies comme le diabète de type 2 et les maladies cardiovasculaires, liées à des dérégulations métaboliques et endocriniennes du tissu adipeux blanc (TAB). Au cours du vieillissement, la perte de masse musculaire peut être associée à l’obésité et définit le concept d’obésité sarcopénique. Les traitements mis en œuvre pour contrecarrer ces pathologies n’ont qu’un succès très partiel. Il est donc opportun de développer des stratégies alternatives originales qui pourraient aboutir à des thérapeutiques ciblées. Notre équipe étudie les régulations métaboliques du TAB, source majeure de stockage de l’énergie de l’organisme. Les triglycérides stockés sont libérés à jeun grâce à la lipolyse qui libère les acides gras non-estérifiés (AGNE) et le glycérol dans le sang, comme source d’énergie des autres tissus. En plus de la β-oxydation des AGNE, leur ré-estérification partielle intervient pour limiter leur libération lors de la lipolyse. La glycéronéogenèse est nécessaire à la ré-estérification en situation de jeûne. Des études préalables ont montré que l'administration de citrulline (CIT) pendant trois mois à des rats vieillissants induit une diminution d’environ 40% de la masse viscérale du TAB. Cet acide aminé non protéique est un complément alimentaire donné au cours du vieillissement ou à des sportifs pour augmenter la masse musculaire. Nous avons étudié les effets de la CIT sur des cultures d’explants de TAB de rats. Dans la première partie de ce travail, nous montrons que la CIT a un effet direct lipolytique et anti-glycéronéogénique sur les explants des rats qu’ils soient jeunes ou âgés. Cependant, la libération des AGNE du TAB des rats jeunes est limitée par une augmentation de la capacité oxydative du tissu. Avec l’âge, la masse du TAB augmente en parallèle à l’augmentation d’un état pro-inflammatoire. Afin de comprendre l’influence de ces deux paramètres indépendamment de l’âge, nous avons étudié dans la deuxième partie de ce travail, les effets de la CIT sur les explants de TAB de rats jeunes soumis à un régime contrôle (CD) ou hyperlipidique (HFD). Nous observons une augmentation, induite par la CIT, de la lipolyse et de la capacité ß-oxydative du TAB des rats quel que soit le régime, alors que la glycéronéogenèse est diminuée. Toutefois, les AGNE sont sélectivement libérés par le TAB de rats HFD, en relation avec une réduction drastique de leur ré-estérification. Le NO est un médiateur de ces effets. Dans une troisième partie, nous démontrons que la CIT agit directement sur le TAB de rats CD et HFD pour induire l'expression de la protéine découplante, UCP1, en lien avec le « brunissement » potentiel du TAB par cet acide aminé. Ces effets ne sont pas observés au sein du TAB des rats âgés. L’ensemble de nos résultats établit les bases pour de futures investigations visant à élucider les mécanismes par lesquels la CIT réduit la masse adipeuse et ouvre de nouvelles perspectives thérapeutiques pour lutter contre le surpoids et l’obésité sarcopénique. / Obesity is frequently associated with type 2 diabetes and cardiovascular diseases, related to metabolic and endocrine dysregulation of white adipose tissue (WAT). During aging, the loss of muscle mass may be associated with obesity and defines the concept of sarcopenic obesity. Treatments implemented to counteract these conditions showed a very partial success. It is therefore appropriate to develop original alternative strategies that could lead to targeted therapies. Our team studies the metabolic regulation of WAT, the major source of energy storage in the body. Non-esterified fatty acids (NEFA) and glycerol are released in the blood from stored triglycerides through lipolysis and used as a source of energy for other tissues. In addition to their β-oxidation, NEFA are re-esterified in part, a process that limits their release in the blood. Glyceroneogenesis is the pathway necessary to NEFA re-esterification in the fasting state. Previous studies showed that administration of citrulline (CIT) for three months to aging rats induced a decrease of approximately 40% of the visceral WAT mass. This non-protein amino acid is given as a dietary supplement during aging or sports to increase muscle mass. We studied the effects of CIT on explant cultures of rat WAT. In the first part of this work, we show that CIT exerts a direct lipolytic and anti-glyceroneogenic effect on explants from rats whether young or old. However, the release of NEFA from the explants of young rats is limited by an increase in the oxidative capacity of the tissue. During aging, WAT mass augments in parallel to the increase in a pro-inflammatory state. To understand the influence of these two parameters regardless of age, we studied in the second part of this work, the effects of CIT on WAT explants from young rats fed a control (CD) or high fat (HFD) diet. We show an CIT-induced increase in lipolysis and beta-oxidative capacity of WAT from rats whatever the diet, while glyceroneogenesis is reduced. However, NEFA are selectively released from WAT of HFD rats, in connection with a drastic reduction of their re-esterification. NO is a mediator of these effects. In the third part of this work, we show that CIT acts directly on WAT from CD and HFD rats to induce the expression of uncoupling protein, UCP1, in line with the potential "browning" of WAT by this amino acid. These effects were not observed in explants from old rats. Altogether our results establish the basis for future investigations aimed at elucidating the mechanisms by which CIT reduces body fat and open new therapeutic perspectives to fight overweight and sarcopenic obesity.
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Impact de la citrulline sur le métabolisme du tissu adipeux / Citrulline effect on adipose tissue metabolismJoffin, Nolwenn 29 January 2015 (has links)
L’obésité s’accompagne de pathologies comme le diabète de type 2 et les maladies cardiovasculaires, liées à des dérégulations métaboliques et endocriniennes du tissu adipeux blanc (TAB). Au cours du vieillissement, la perte de masse musculaire peut être associée à l’obésité et définit le concept d’obésité sarcopénique. Les traitements mis en œuvre pour contrecarrer ces pathologies n’ont qu’un succès très partiel. Il est donc opportun de développer des stratégies alternatives originales qui pourraient aboutir à des thérapeutiques ciblées. Notre équipe étudie les régulations métaboliques du TAB, source majeure de stockage de l’énergie de l’organisme. Les triglycérides stockés sont libérés à jeun grâce à la lipolyse qui libère les acides gras non-estérifiés (AGNE) et le glycérol dans le sang, comme source d’énergie des autres tissus. En plus de la β-oxydation des AGNE, leur ré-estérification partielle intervient pour limiter leur libération lors de la lipolyse. La glycéronéogenèse est nécessaire à la ré-estérification en situation de jeûne. Des études préalables ont montré que l'administration de citrulline (CIT) pendant trois mois à des rats vieillissants induit une diminution d’environ 40% de la masse viscérale du TAB. Cet acide aminé non protéique est un complément alimentaire donné au cours du vieillissement ou à des sportifs pour augmenter la masse musculaire. Nous avons étudié les effets de la CIT sur des cultures d’explants de TAB de rats. Dans la première partie de ce travail, nous montrons que la CIT a un effet direct lipolytique et anti-glycéronéogénique sur les explants des rats qu’ils soient jeunes ou âgés. Cependant, la libération des AGNE du TAB des rats jeunes est limitée par une augmentation de la capacité oxydative du tissu. Avec l’âge, la masse du TAB augmente en parallèle à l’augmentation d’un état pro-inflammatoire. Afin de comprendre l’influence de ces deux paramètres indépendamment de l’âge, nous avons étudié dans la deuxième partie de ce travail, les effets de la CIT sur les explants de TAB de rats jeunes soumis à un régime contrôle (CD) ou hyperlipidique (HFD). Nous observons une augmentation, induite par la CIT, de la lipolyse et de la capacité ß-oxydative du TAB des rats quel que soit le régime, alors que la glycéronéogenèse est diminuée. Toutefois, les AGNE sont sélectivement libérés par le TAB de rats HFD, en relation avec une réduction drastique de leur ré-estérification. Le NO est un médiateur de ces effets. Dans une troisième partie, nous démontrons que la CIT agit directement sur le TAB de rats CD et HFD pour induire l'expression de la protéine découplante, UCP1, en lien avec le « brunissement » potentiel du TAB par cet acide aminé. Ces effets ne sont pas observés au sein du TAB des rats âgés. L’ensemble de nos résultats établit les bases pour de futures investigations visant à élucider les mécanismes par lesquels la CIT réduit la masse adipeuse et ouvre de nouvelles perspectives thérapeutiques pour lutter contre le surpoids et l’obésité sarcopénique. / Obesity is frequently associated with type 2 diabetes and cardiovascular diseases, related to metabolic and endocrine dysregulation of white adipose tissue (WAT). During aging, the loss of muscle mass may be associated with obesity and defines the concept of sarcopenic obesity. Treatments implemented to counteract these conditions showed a very partial success. It is therefore appropriate to develop original alternative strategies that could lead to targeted therapies. Our team studies the metabolic regulation of WAT, the major source of energy storage in the body. Non-esterified fatty acids (NEFA) and glycerol are released in the blood from stored triglycerides through lipolysis and used as a source of energy for other tissues. In addition to their β-oxidation, NEFA are re-esterified in part, a process that limits their release in the blood. Glyceroneogenesis is the pathway necessary to NEFA re-esterification in the fasting state. Previous studies showed that administration of citrulline (CIT) for three months to aging rats induced a decrease of approximately 40% of the visceral WAT mass. This non-protein amino acid is given as a dietary supplement during aging or sports to increase muscle mass. We studied the effects of CIT on explant cultures of rat WAT. In the first part of this work, we show that CIT exerts a direct lipolytic and anti-glyceroneogenic effect on explants from rats whether young or old. However, the release of NEFA from the explants of young rats is limited by an increase in the oxidative capacity of the tissue. During aging, WAT mass augments in parallel to the increase in a pro-inflammatory state. To understand the influence of these two parameters regardless of age, we studied in the second part of this work, the effects of CIT on WAT explants from young rats fed a control (CD) or high fat (HFD) diet. We show an CIT-induced increase in lipolysis and beta-oxidative capacity of WAT from rats whatever the diet, while glyceroneogenesis is reduced. However, NEFA are selectively released from WAT of HFD rats, in connection with a drastic reduction of their re-esterification. NO is a mediator of these effects. In the third part of this work, we show that CIT acts directly on WAT from CD and HFD rats to induce the expression of uncoupling protein, UCP1, in line with the potential "browning" of WAT by this amino acid. These effects were not observed in explants from old rats. Altogether our results establish the basis for future investigations aimed at elucidating the mechanisms by which CIT reduces body fat and open new therapeutic perspectives to fight overweight and sarcopenic obesity.
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Nitric oxide, arginine and acute pancreatitis /Sandström, Per A., January 2004 (has links) (PDF)
Diss. (sammanfattning) Linköping : Univ., 2004. / I publikationen felaktig serie: Linköping studies in health sciences. Härtill 4 uppsatser.
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Protein-bound citrulline and homocitrulline in rheumatoid arthritis:confounding features arising from structural homologyTurunen, S. (Sanna) 07 April 2014 (has links)
Abstract
Rheumatoid arthritis (RA) is an autoimmune disease causing inflammation of synovial joints, which may lead to permanent changes in cartilage and bone tissues. RA patients have antibodies binding to citrullinated and also to carbamylated proteins. Antibodies binding to citrulline are associated with more severe disease progression and may already appear years before clinical disease onset.
Citrulline and the lysine carbamylation product, homocitrulline, are similar in structure. Citrullinated proteins have been studied in RA and in neurological diseases, but researchers have been unaware of the effect of homocitrulline in citrulline detection methods. The purpose of the present study was to clarify the features of protein-bound citrulline and homocitrulline in relation to research done on citrullination and in immunological reactions related to rheumatoid arthritis.
In the first study of this thesis the confounding role of homocitrulline in citrulline detection was shown. In the first and second study the features of experimentally induced antibodies were assessed. The antibodies induced with citrulline- and homocitrulline-containing protein structures were shown to react both with the ureido groups and the protein structures. The antibodies were able to distinguish between citrulline and homocitrulline in the same sequence even though binding to both. In the third study the simultaneous presence of citrulline and homocitrulline in RA synovial tissue was shown.
In conclusion, considering the simultaneous presence of citrulline and homocitrulline and the binding features of the experimentally induced antibodies, homocitrulline could have a yet unsolved role in RA. Secondly, the existence of homocitrulline should be borne in mind in studies on citrullination. / Tiivistelmä
Nivelreuma on niveltulehduksen aiheuttava autoimmuunitauti, joka voi johtaa pysyviin muutoksiin nivelen rusto- ja luukudoksessa. Nivelreumaa sairastavilla esiintyy vasta-aineita sitrullinoituneita ja karbamyloituneita proteiineja vastaan. Sitrulliiniin sitoutuvia vasta-aineita voi esiintyä elimistössä jo vuosia ennen taudin puhkeamista, ja niiden esiintyminen on yhdistetty vaikeampaan taudinkuvaan.
Sitrulliini ja lysiinin karbamylaatiotuote homositrulliini ovat rakenteellisesti samankaltaisia. Proteiinien sitrullinaatiota on tutkittu nivelreumassa ja neurologisissa taudeissa, mutta homositrulliinin olemassaoloa tai sen vaikutusta tutkimusmenetelmiin ei ole huomioitu. Tämän tutkimuksen tarkoituksena oli selvittää proteiineihin sitoutuneiden sitrulliinin ja homositrulliinin ominaisuuksia aikaisempiin tutkimuksiin ja nivelreuman immunologisiin reaktioihin liittyen.
Tässä tutkimuksessa homositrulliinin osoitettiin häiritsevän sitrulliinin tunnistamista. Ensimmäisessä ja toisessa osatyössä aiheutettiin kokeellisesti vasta-aineita sitrulliinia ja homositrulliinia sisältävillä proteiinirakenteilla. Vasta-aineiden havaittiin reagoivan sekä ureidoryhmän että proteiinirakenteen kanssa. Vasta-aineet pystyivät erottamaan sitrulliinin ja homositrulliinin toisistaan samassa rakenteessa, vaikka sitoutuivat kumpaankin. Kolmannessa osatyössä osoitettiin, että sitrulliinia ja homositrulliinia esiintyy samanaikaisesti nivelreumapotilaan tulehtuneessa nivelkalvossa.
Tutkimus osoitti, että sitrulliinin ja homositrulliinin samanaikainen esiintyminen ja kokeellisesti aiheutettujen vasta-aineiden ominaisuudet huomioiden homositrulliinilla voi olla jokin toistaiseksi selvittämätön rooli nivelreumassa. Homositrulliinin olemassaolo on syytä huomioida sitrullinaatiota tutkittaessa.
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