Validation fonctionnelle d'approches nutritionnelles à allégation "Bien veillir", capables de prévenir le vieillissement cérébral et les maladies neurodégénératives / Functional validation of nutritional approaches to allegation "well aging", able to prevent brain aging and neurodegenerative diseases

Allouche, Ahmad

13 December 2012

La maladie d'Alzheimer (MA) est une démence neurodégénérative caractérisée par des pertes de la mémoire et des troubles cognitifs. La toxicité des oligomères solubles du peptide [bêta]-amyloïde (A[bêta]Os) est centrale dans la phase précoce de la maladie. L'absence de traitements curatifs, l'aspect chronique des mécanismes pathogéniques et le partage de facteurs de risque communs avec les pathologies cardiovasculaires, notamment les paramètres alimentaires et le métabolisme lipidique, doivent inciter à considérer l'intérêt de méthodes préventives permettant d'empêcher l'apparition de la maladie. Dès lors, l'approche nutritionnelle apparaît comme une stratégie capable de limiter sa prévalence. Une souris modèle des stades précoces de MA nous a permit d'évaluer le potentiel préventif d'une alimentation enrichie en acide docosahexaénoïque (DHA, C22:6, n-3). Les résultats obtenus montrent qu'un apport alimentaire suffisant en DHA conduit à en enrichir les membranes dans les différentes structures cérébrales. En conséquence, les fonctions synaptiques sont préservées, même après exposition aigüe aux A[bêta]Os, ce qui maintient les capacités cognitives des souris exposées. Nous avons ensuite développé des stratégies nutritionnelles permettant d'évaluer les effets bénéfiques de DHA contre la dyslipidémie induite par l'alimentation et les déficits cognitifs associés au vieillissement normal ou pathologique. Les résultats obtenus à l'issue de notre étude révèlent qu'un apport alimentaire en DHA est capable de prévenir la dyslipidémie provoquée par un régime riche en lipides et de retarder le déclin cognitif lié au vieillissement cérébral normal ou pathologique / Alzheimer's disease is a neurodegenerative aging-related dementia that is characterized by loss of memory and cognitive disorders. Toxicity of soluble oligomers of [beta]-amyloid peptide (sOA[beta]) is a key element in early stages of the disease. Absence of curative therapies, chronic aspects of the pathogenic mechanisms implicated and influence of common risk factors shared with the cardiovascular diseases, including dietary parameters and lipid metabolism, should widely encourage considering the interest of preventive interventions allowing slowing the progression and delaying the clinical onset of Alzheimer's-related troubles. Therefore, nutritional approaches could appear as a strategy able to reduce the prevalence of this disease. Early Alzheimer's mouse model allowed us to assess the preventive potential of diets supplemented in docosahexaenoic acid (DHA, C22:6 n-3). Our results show that adequate dietary intake of DHA lead to increased levels in different brain structures. Consequently, hippocampal and cortical synaptic functions were preserved, even upon acute exposure to A[beta] oligomers, maintaining or improving the cognitive capacities of A[beta]-exposed mice. These improvements were positively correlated with DHA-enrichment associated in hippocampus and with preserved synaptic integrity. We also designed nutritional strategies in order to evaluate the beneficial effects of DHA on diet-induced dyslipidemia as well as on cognitive impairment and neurodegenerative processes associated with normal or pathologic aging. Our results show that dietary DHA can prevent high-fat diet-induced dyslipidemia and delay cognitive decline related with normal or pathological aging

Acides gras polyinsaturés n-3

Cognition

Dyslipidémie

Lipides

Maladie d'Alzheimer

Modèle souris

Nutrition

Oligomères A[bêta] solubles

Prévention

Vieillissement

Aging

Alzheimer's disease

Cognition

Dyslipidemia

Lipids

Mouse model

Nutrition

N-3 polyunsaturated fatty acids

Prevention

Soluble A[beta] oligomers

613.2

616.830 654

Associação entre consumo de ácidos graxos ômega 3 e transtorno de ansiedade: análise transversal do Estudo Longitudinal de Saúde do Adulto (ELSA-Brasil) / Omega 3 consumption and anxiety disorders: a cross-sectional analysis of the Brazilian Longitudinal Study of Adult Health (ELSA-Brasil)

Natacci, Lara Cristiane

01 August 2018

oucos estudos avaliaram a associação da ingestão de ácidos graxos ômega 3 e transtornos de ansiedade. O presente estudo utilizou dados transversais do exame de linha de base (2008-2010) do Estudo Longitudinal Brasileiro de Saúde do Adulto - ELSA-Brasil para avaliar essa associação. A exposição dietética foi medida por um questionário quantitativo de frequência alimentar validado para a população brasileira e adaptado para o estudo, e os diagnósticos mentais foram avaliados pelo Clinical Interview Schedule-Revised Version - CIS-R, diagnosticando transtornos mentais de acordo com a Classificação Internacional de Doenças - CID-10. Modelos de regressão logística foram construídos utilizando quintis do consumo de ácidos graxos ômega 3, ácidos graxos ômega 6, razão de consumo n-6/n-3, e ácidos graxos poli-insaturados, usando o primeiro quintil como referência. Dos 15.105 sujeitos participantes do ELSA-Brasil, foram excluídos aqueles que relataram ingestão de menos de 500 ou mais de 4000 kcal, aqueles que relataram ingestão de suplementos n-3 ou n-6 e aqueles que foram submetidos a cirurgia bariátrica. Após as exclusões, 12268 participantes permaneceram na análise, dos quais 1893 (15,4%) apresentaram transtornos de ansiedade. Os indivíduos com transtorno de ansiedade eram mais jovens, de sexo feminino, menor escolaridade e renda, referiram tabagismo atual e atividade física mais leve. Valores mais altos de IMC e de proteína C reativa de alta sensibilidade foram observados nos indivíduos com ansiedade. A ingestão diária média de ácido eicosapentaenoico (EPA), ácido docosapentanoico (DPA) e ácido docosaexaenoico (DHA) foi significativamente menor em participantes com ansiedade. Um maior consumo desses três ácidos graxos da família ômega-3 foi observado em indivíduos com mais idade, maior renda e escolaridade, com dislipidemia, consumo de álcool e tabagismo atuais, e prática de atividade física vigorosa. Após o ajuste para variáveis sociodemográficas (idade, sexo, etnia e educação) fatores de risco cardiovascular (hipertensão, diabetes, dislipidemia, tabagismo, ingestão de álcool e atividade física), calorias totais, qualidade da dieta e depressão, os participantes do quinto quintil de ingestão de EPA, DHA e DPA mostraram associação inversa com transtornos de ansiedade: OR 0,82 (IC 95%, 0,69-0,98), OR 0,83 (IC 95%, 0,69-0,98) e OR 0,82 (IC 95%, 0,69-0,98), respectivamente. Participantes no quinto quintil de razão ômega-6/ômega-3 tiveram associação positiva com transtornos de ansiedade. Nenhuma associação foi encontrada com a ingestão de PUFA, ou ômega-3 e ômega-6 isoladamente com ansiedade após os ajustes. Nesta análise, uma alta ingestão de ômega-3 EPA, DHA e DPA foi inversamente associada com a presença de transtornos de ansiedade, enquanto que a alta razão ômega-6/ômega-3 foi diretamente associada à presença desses transtornos, sugerindo um possível efeito protetor dos ácidos graxos omega-3 EPA, DPA e DHA contra a ansiedade / Few studies have evaluated the association of omega-3 fatty acids intake and anxiety disorders. The present study used cross-sectional data from the baseline (2008-2010) examination of the Brazilian Longitudinal Study of Adult Health - ELSA-Brazil to evaluate this association. The dietary exposure was measured by a quantitative food frequency questionnaire validated for the brazilian population and adapted for the study, and the mental diagnoses were assessed by the Clinical Interview Schedule-Revised Version (CIS-R), diagnosing mental disorders according to the International Classification of Diseases - ICD-10. Logistic regression models were built using quintiles of omega-3 fatty acids, omega-6 fatty acids, omega-6/omega-3 ratio, and polyunsaturated fatty acids consumption, using the first quintile as a reference. Of the 15,105 subjects participating in ELSA-Brazil, those who reported ingestion of less than 500 or more than 4000 kcal, those who reported ingestion of omega-3 or omega-6 supplements and those had undergone bariatric surgery were excluded. After exclusions, 12,268 participants remained in the analysis, of whom 1893 (15.4%) had anxiety disorders. Subjects with anxiety disorder were younger, female, had lower education and income, reported current smoking and mild physical activity. Higher values of BMI and high sensibility C reactive protein were observed in subjects with anxiety. The mean daily intakes of eicosapentaenoic acid (EPA), docosapentaenoic acid (DPA) and docosahexaenoic acid (DHA) were significantly lower in subjects with anxiety. A higher intake of these three omega-3 fatty acids was observed in older individuals with higher income and education, with current dyslipidemias, alcohol consumption and smoking, and vigorous physical activity. After adjustment for socio-demographic variables (age, sex, ethnicity and education), cardiovascular risk factors (hypertension, diabetes, dyslipidemia, smoking, alcohol intake and physical activity), total calories, diet quality and depression, EPA, DHA and DPA intakes showed an inverse association with anxiety disorders: OR 0.82 (95% CI, 0.69-0.98), OR 0.83 (95% CI, 0.69-0.98) and OR 0.82 (95% CI, 0.69-0.98), respectively. Participants in the fifth quintile of omega-6/omega-3 ratio had a positive association with anxiety disorders. No association was found with ingestion of PUFA, or omega-3 and omega-6 alone with anxiety after adjustments. In this analysis, a high intake of omega-3 EPA, DHA and DPA was inversely associated with the presence of anxiety disorders, while the higher omega-6 omega-3 ratio was directly associated with the presence of these disorders, suggesting a possible protector effect of omega-3 fatty acids EPA, DPA and DHA against anxiety

Ácidos graxos ômega-3

Ácidos graxos ômega-6

Ácidos graxos poli-insaturados

Anxiety disorders

Mental disorders

Ômega-3 fatty acids

Ômega-6 fatty acids

Omega6/omega3 ratio

Polyunsaturated fatty acids

Razão ômega6/ômega3

Transtornos de ansiedade

Transtornos mentais

Ações do óleo de peixe e triglicerídeos de cadeia média na esteatose hepática e estresse oxidativo induzidos pela dieta hiperlipídica em ratos / THE EFFECTS OF FISH OIL AND MEDIUM CHAIN TRIGLYCERIDES IN HEPATIC STEATOSIS AND OXIDATIVE STRESS INDUCED BY HIGH FAT DIET IN RATS

Almeida, Bianca Bellizzi de

14 October 2011

Introdução: A doença hepática gordurosa não alcoólica é caracterizada pelo acúmulo hepático de lipídeos, principalmente na forma de triglicerídeos. Devido à atividade inflamatória progressiva pode evoluir para uma forma mais grave, a esteatohepatite não alcoólica. Os ácidos graxos poli-insaturados ômega-3 são associados a efeitos metabólicos positivos para redução da esteatose hepática, no entanto, são mais susceptíveis a peroxidação lipídica. Os triglicerídeos de cadeia média (TCMs) promovem a prevenção do bloqueio da beta-oxidação de ácidos graxos e redução da peroxidação lipídica, no entanto os efeitos na redução da esteatose ainda são controversos. Objetivo: O objetivo do estudo foi avaliar as implicações da dieta hiperlipídica (HL+) com óleo de peixe ou com óleo de TCM no desenvolvimento da esteatose hepática, no perfil de ácidos graxos hepáticos e no estresse oxidativo em ratos. Metodologia: Cinquenta ratos machos da linhagem wistar foram divididos em 5 grupos. Os animais receberam água e comida a vontade durante 45 dias. A adaptação a dieta HL+ foi realizada nos primeiros 15 dias. A composição da dieta do grupo que recebeu somente a gordura animal (HL+GA) era de 50% de gordura animal, e a dieta dos grupos HL+OS, HL+TCM e HL+OP era composta por 35% de gordura animal e 15% de óleo de soja, óleo de TCM e óleo de peixe, respectivamente. Resultados: Todos os grupos que receberam as dietas hiperlipídicas apresentaram maior acúmulo de gordura total e de triglicerídes hepaticos e somente os grupos HL+GA e HL+TCM apresentaram maior acúmulo de colesterol total hepático em relação ao controle. O grupo HL+TCM apresentou maior acúmulo percentual de gordura e um exacerbado acúmulo de triglicerídeos hepáticos em relação aos grupos alimentados com as dietas HL+. A redução do colesterol total sérico foi observada nos grupos HL+TCM e HL+OP, comparados ao controle. A maior incorporação hepática dos ácidos graxos EPA e DHA no grupo HL+OP contribuiu para o aumento do Índice de Peroxibilidade dos ácidos graxos e das substâncias reativas ao ácido tiobarbitúrico livres e totais e para a depleção da vitamina E no fígado. A maior razão AGS/AGPI hepática observada no grupo HL+TCM contribuiu para a preservação dos antioxidantes hepáticos. A alanina aminotransferase, um marcador de dano hepático, apresentou-se aumentada em todos os grupos que receberam as dietas HL+. Conclusões: A dieta hiperlipídica foi eficiente na indução do acúmulo de gordura hepática. O uso do óleo de TCM foi associado a uma maior concentração de lipídeos e preservação dos antioxidantes hepáticos. A dieta hiperlipídica com óleo de peixe foi associada ao aumento significativo na peroxidação lipídica, apesar do menor acúmulo de colesterol e triglicerídeos hepaticos. / Introduction: The Non-alcoholic Fatty liver disease is characterized by hepatic accumulation of lipids, mainly in the form of triglycerides. The disease may progress to a more severe form, the Non-alcoholic steatohepatitis, due to progressive inflammatory activity. Many authors have shown positive metabolic effects associated with the use of polyunsaturated omega-3 fatty acids and reduction in hepatic steatosis. However, these fatty acids are more susceptible to lipid peroxidation. The medium chain triglycerides (MCTs) are able to block beta-oxidation of fatty acids and reduce lipid peroxidation, but the MCT effects in steatosis are still controversial. Objective: The aim of this study was to assess the implications of high-fat diet (HF+) with fish oil or with MCT oil in the development of hepatic steatosis, liver fatty acid profile and oxidative stress markers in rats. Methodology: Fifty wistar male rats were divided into 5 groups. The animals had free access to food and water for 45 days. The first 15 days was dedicated for adaptation to high-fat diet. The HF+AF group received high-fat diet with 50% of animal fat and the other high-fat diets were made with 35% of animal fat plus 15% of other types of fat: soybean oil (HF+SO), MCT oil (HF+MCT) and fish oil (HF+FO). Results: The high-fat groups had higher hepatic total fat and triglycerides accumulation and only the groups HF+AF and HF+MCT had higher accumulation of hepatic cholesterol compared to control. The HF+MCT group had the highest percentage of hepatic fat accumulation and an exacerbated triglyceride accumulation in the liver among HF+ groups. The serum total cholesterol decreased in groups HF+MCT and HF+FO compared with the control group. The highest incorporation of hepatic fatty acids EPA and DHA in the HF+FO group contributed to the increased fatty acids peroxidizability index and total and free hepatic TBARS and depletion of hepatic vitamin E. The biggest ratio SFA/PUFA of liver fatty acids observed in the HF+MCT group contributed to the preservation of hepatic antioxidants. The alanine aminotransferase is a liver damage marker and was increased in all high-fat groups. Conclusions: The high-fat diet was effective to increase the hepatic fat concentration. The consumption of MCT oil can increase the hepatic lipid concentration and hepatic antioxidants. There was a significant increase in hepatic lipid peroxidation in the HF+FO group, although hepatic cholesterol and triglycerides were decreased.

ácidos graxos poli-insaturados ômega-3

dieta hiperlipídica

esteatose hepática não alcoólica

high fat diet

medium-chain triglycerides

nonalcoholic fatty liver disease

polyunsaturated ômega-3 fatty acids

ratos

rats

triglicerídeos de cadeia média

Efeitos dos diferentes ácidos graxos no metabolismo lipídico e estresse oxidativo em camundongos C57/BL alimentados com dieta hiperlipídica e rica em frutose / Effects of different fatty acids on lipid metabolism and oxidative stress in C57/BL mice fed a high fat diet and rich in fructose

Manca, Camila Sanches

30 June 2017

A esteatose hepática não alcóolica está relacionada às causas crescentes de morbimortalidade de doenças hepáticas. Sua incidência está relacionada à obesidade e comorbidades vinculadas a esta, na qual tem despertado grande interesse na pesquisa. A modulação quantitativa da dieta pode promover ou retardar a patologia. Desta forma, terapias voltadas para retardar ou diminuir a esteatose hepática não alcóolica poderiam atenuar o dano hepático, melhorar a função hepática e reduzir sua progressão. Os objetivos do presente estudo foram: avaliar o consumo de óleos vegetais ricos em MUFAs e PUFAs usados comercialmente na prevenção ou redução da esteatose hepática analisando parâmetros do metabolismo lipídico hepático e sérico, estresse oxidativo e retardando a progressão de NAFLD. Material e Métodos: os animais foram divididos nos seguintes grupos: Controle (n=10) + HLF * (n=10); Grupo HLF * AZ (n=10); Grupo HLF* CN (n=10); Grupo HLF* S (n=10). Após 16 semanas de dieta e tratamento com os respectivos óleos, os animais foram anestesiados e o sangue retirado por punção cardíaca e os tecidos para as análises posteriores. Resultados: A oferta de uma dieta rica em gordura saturada (banha) + frutose ocasionou um aumento do peso no grupo HLF enquanto a administração dos respectivos óleos vegetais foi capaz de retardar o ganho de peso. O peso hepático e da soma dos tecidos adiposos epididimal e retroperitonial foi maior no HLF enquanto houve redução significativa no peso hepático HLF/S. O tecido retroperitonial foi menor no HLF/CN. De uma maneira geral o tratamento com os respectivos óleos vegetais diminui a esteatose em todos os grupos experimentais. A oferta de azeite extra virgem não refletiu no ganho de peso, porém o grupo teve um aumento significativo de TG e VLDL séricos, com diminuição do colesterol sérico. Avaliado histologicamente diminuiu o score de esteatose quando comparado ao HLF sendo classificado como esteatose macro e microvesicular de leve a moderada. O óleo de soja apresentou uma maior quantidade de PUFAs, sendo rico em n-6, refletiu na manutenção do peso dos animais, diminuiu a esteatose, sendo classificado como esteatatose leve, quando comparado ao HLF, porém aumentou o colesterol sérico. Apresentou um aumento de MDA e diminuição de GSH hepático. O óleo de canola devido a seu teor em ácidos graxos PUFAs (n-6 e n-3) teve maior incorporação do EPA e DHA que parecem ter evidenciado positivamente. Não apresentou alteração nos parâmetros bioquímicos e apresentou menor acúmulo de gordura hepática através da análise do percentual de gordura hepática e histopatologia, sendo caracterizado como esteatose leve. Pela peroxidação lipídica apresentou um maior acúmulo de MDA, porém um aumento de GSH. Contudo, a oferta dos respectivos óleos influenciou positivamente em diferentes mecanismos fisiológicos. / The Non-alcoholic fatty liver is related to the increasing causes of morbidity and mortality of liver diases. Its incidence is related to obesity and comorbidities linked to it, in which it has awaked great interest in the research. The disease is associated to genetic predisposition, lack of physical activity and high intake of saturated fats and fructose. Quantitative modulation of the diet may promote or retard the pathology. Thus, therapies aimed at delaying or decreasing non alcoholic hepatic steatosis could alleviate liver damage, improve liver function and reduce its progression. The objectives of the present study were: to evaluate the consumption of vegetable oils rich in commercially available MUFAs and PUFAs in the prevention or reduction of hepatic steatosis by analyzing parameters of hepatic and serum lipid metabolism, oxidative stress and delaying the progression of NAFLD. Material and Methods: animals were divided into the following groups: Control (n = 10) + HLF * (n = 10); Group HLF * AZ (n = 10); Group HLF * CN (n = 10); Group HLF * S (n = 10). After 16 weeks of diet and treatment with the respective oils, the animals were anesthetized and blood was withdrawn by cardiac puncture and tissues for further analysis. Results: The supply of a diet rich in saturated fat (lard) + fructose caused an increase in weight in the HLF group while the administration of the respective vegetable oils was able to delay the weight gain. Liver weight and sum of epididymal and retroperitoneal adipose tissues were higher in HLF while there was a significant reduction in HLF / S hepatic weight. Retroperitoneal tissue was lower in HLF / CN. In general, treatment with the respective vegetable oils decreases steatosis in all experimental groups. The supply of extra virgin olive oil did not reflect weight gain, but the group had a significant increase in serum TG and VLDL, with a decrease in serum cholesterol. Histologically it reduced the steatosis score when compared to the HLF being classified as mild to moderate macro and microvesicular steatosis. Soybean oil presented a higher amount of PUFAs, being rich in n-6, reflected in the maintenance of animal weight, decreased steatosis, being classified as mild steatosis when compared to HLF, but increased serum cholesterol. He presented an increase of MDA and decrease of hepatic GSH. Canola oil due to its content of PUFAs (n-6 and n-3) had greater incorporation of EPA and DHA than appear to have been positively evidenced. There was no alteration in the biochemical parameters and presented lower accumulation of liver fat through the analysis of the percentage of liver fat and histopathology, being characterized as mild steatosis. By the lipid peroxidation presented a greater accumulation of MDA, but an increase of GSH. However, the supply of the respective oils had a positive influence on different physiological mechanisms.

Ácidos graxos monoinsaturados

Ácidos graxos poli-insaturados

Ácidos graxos saturados

Camundongo C57/BL

Fructose

Frutose

Monounsaturated fatty acids (MUFAS)

Mouse C57/BL

Polyunsaturated fatty acids (PUFAS)

Saturated fatty acids (AGS)

L’oxydation modifie les effets métaboliques d'acides gras polyinsaturés de la série n-3 incorporés par différents vecteurs dans des régimes hyperlipidiques : contribution de l’absorption intestinale et de la réactivité cellulaire du 4-hydroxy-hexénal / The oxidation modifies the metabolic impacts of n-3 polyunsaturated fatty acids associated with different carriers in high-fat diets : contribuation of intestinal absorption and cellular reactivity of 4-hydroxy-hexenal

Awada, Manar

11 December 2012

Les aliments riches en acides gras polyinsaturés (AGPI) à longue chaîne (LC) de la série n-3 sont recommandés pour leurs effets bénéfiques sur la santé humaine et en particulier dans la prevention du développement des maladies métaboliques. Or, la biodisponibilité de ces AGPI et leur impact métabolique pourraient être modulés par la nature chimique des molécules qui les véhiculent dans les aliments (triacylglycérols, TG ou phospholipides, PL). De plus, ces AGPI sont sensibles à la peroxydation lipidique. S’ils ne sont pas protégés de l’oxydation, ils peuvent former des espèces réactives toxiques comme le 4-hydroxy-hexénal (4-HHE). Dans ce contexte, le but de notre étude a été d’évaluer l’impact de l’enrichissement de régimes hyperlipidiques en AGPI n-3 (i) portés par des TG ou des PL et (ii) sous forme non-oxydée ou oxydée, sur l’inflammation et le stress oxydant métaboliques et d’en comprendre certains mécanismes liés à l’absorption intestinale et la réactivité du 4-HHE. D’une part, notre étude a confirmé que la consommation d’AGPI-LC n-3 empêche l’induction du stress oxydant et de l’inflammation lors d’un régime hyperlipidique chez la souris. Cependant, par rapport aux TG, les PL vecteurs d’AGPI n-3 permettent de réduire la taille des adipocytes et de stimuler le système antioxydant. D’autre part, notre étude a montré que la consommation d’AGPI n-3 oxydés de manière modérée aboutit à une élévation des concentrations plasmatiques de 4-HHE et des marqueurs inflammatoires. De plus, une activation des voies inflammatoires ainsi que du stress du réticulum endoplasmique ont été détectées au niveau de l’intestin grêle. Nos résultats in vivo et in vitro sur cellules intestinales Caco-2/TC7 indiquent que cela peut être dû en partie à une absorption au niveau intestinal du 4-HHE, produit d’oxydations des AGPI n-3. Dans le contexte du développement des aliments contenant des AGPI-LC n-3, nos résultats contribuent à identifier les structures vectrices de ces acides gras les plus efficaces du point de vue métabolique. En santé publique et en pratique clinique, nos résultats constituent une nouvelle base de réflexion pour la mise en place de bonnes pratiques de production et de conservation des aliments et des compléments nutritionnels enrichis en AGPI-LC n-3 pour éviter leur oxydation et ses possibles effets délétères. / Dietary intake of n-3 long chain (LC) polyunsaturated fatty acids (PUFA) are recommended for their beneficial effects on human health, especially to prevent the development of metabolic diseases. However, the bioavailability of these PUFAs and their metabolic impact could be modulated by their chemical carriers (triacylglycerols, TG or phospholipids, PL). In addition, these PUFA are susceptible to lipid peroxidation. If they are not protected from oxidation, they can form toxic reactive species such as 4-hydroxy-hexenal (4-HHE). In this context, the aim of our study was to evaluate the impact of enriching high-fat diets with n-3 PUFA (i) bound to TG or PL and (ii) in unoxidized or oxidized form on the generation of inflammation and oxidative stress, and to understand some underlying mechanisms associated with intestinal absorption and reactivity of 4-HHE. On the one hand, our study confirmed in mice that the consumption of n-3 PUFA protects against oxidative stress and inflammation induced by high-fat diets. However, compared to TG, n-3 PUFA in the form of PL reduce the size of adipocytes and stimulate the antioxidant system. On the other hand, our study showed that the consumption of moderately oxidized n-3 PUFA results in increased plasma concentrations of 4-HHE and of inflammatory markers. In addition, activation of inflammatory pathways as well as endoplasmic reticulum stress were detected in the small intestine. Our results in vivo and in vitro, using intestinal Caco-2/TC7 cells, indicate that this can be partly due to the intestinal absorption of the end-product of n-3 PUFA oxidation, 4-HHE. In the context of the development of foods containing LC n-3 PUFA, our results contribute to identify the most effective PUFA carriers on a metabolic standpoint. Regarding public health and clinical practice, our results provide new basis for the set up of best practices regarding production and storage of food and supplements enriched with LC n-3 PUFA to avoid their lipid oxidation and its possible deleterious effects.

Biosciences

Acides gras polyinsaturés n-3

Triacylgylcerols

Phospholipide

Stress oxydant

4-hhe

Peroxydation lipidique

Biosciences

N-3 polyunsaturated fatty acids

Triacylglerols

Phospholipids

Oxidative stress

4-hhe

Lipid peroxidation

572.507 2

Assessing EPA + DHA requirements of Sparus aurata and Dicentrarchus labrax : impacts on growth, composition and lipid metabolism

Houston, Sam James Silver

January 2018

The gilthead seabream (Sparus aurata) and European seabass (Dicentrarchus labrax) require n-3 long-chain polyunsaturated fatty acids (LC-PUFA), eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA), for optimal growth and health. Due to the rapid growth of global aquaculture the quantity of marine oils used in aquafeeds has been limited, yet the overall quantity of oil in an aquafeed has increased by the addition of vegetable oil (VO) to supply dietary energy. For aquaculture to continue to grow more fish must be produced with less marine ingredients, yet EPA and DHA must be maintained at levels above fish requirements. This project set out to re-evaluate the requirement for EPA and DHA in gilthead seabream and European seabass. Two dose-response studies were designed and executed where juvenile seabream and seabass were fed one of six levels of EPA+DHA (0.2 – 3.2 % as fed). Biometric data were collected and analysed to determine new requirement estimates for EPA+DHA for fish of two weight ranges (24 – 80 g and 80 – 200 g). The effects of the dietary LC-PUFA gradient on lipid composition and metabolism were also considered.

Associação entre consumo de ácidos graxos ômega 3 e transtorno de ansiedade: análise transversal do Estudo Longitudinal de Saúde do Adulto (ELSA-Brasil) / Omega 3 consumption and anxiety disorders: a cross-sectional analysis of the Brazilian Longitudinal Study of Adult Health (ELSA-Brasil)

Lara Cristiane Natacci

01 August 2018

oucos estudos avaliaram a associação da ingestão de ácidos graxos ômega 3 e transtornos de ansiedade. O presente estudo utilizou dados transversais do exame de linha de base (2008-2010) do Estudo Longitudinal Brasileiro de Saúde do Adulto - ELSA-Brasil para avaliar essa associação. A exposição dietética foi medida por um questionário quantitativo de frequência alimentar validado para a população brasileira e adaptado para o estudo, e os diagnósticos mentais foram avaliados pelo Clinical Interview Schedule-Revised Version - CIS-R, diagnosticando transtornos mentais de acordo com a Classificação Internacional de Doenças - CID-10. Modelos de regressão logística foram construídos utilizando quintis do consumo de ácidos graxos ômega 3, ácidos graxos ômega 6, razão de consumo n-6/n-3, e ácidos graxos poli-insaturados, usando o primeiro quintil como referência. Dos 15.105 sujeitos participantes do ELSA-Brasil, foram excluídos aqueles que relataram ingestão de menos de 500 ou mais de 4000 kcal, aqueles que relataram ingestão de suplementos n-3 ou n-6 e aqueles que foram submetidos a cirurgia bariátrica. Após as exclusões, 12268 participantes permaneceram na análise, dos quais 1893 (15,4%) apresentaram transtornos de ansiedade. Os indivíduos com transtorno de ansiedade eram mais jovens, de sexo feminino, menor escolaridade e renda, referiram tabagismo atual e atividade física mais leve. Valores mais altos de IMC e de proteína C reativa de alta sensibilidade foram observados nos indivíduos com ansiedade. A ingestão diária média de ácido eicosapentaenoico (EPA), ácido docosapentanoico (DPA) e ácido docosaexaenoico (DHA) foi significativamente menor em participantes com ansiedade. Um maior consumo desses três ácidos graxos da família ômega-3 foi observado em indivíduos com mais idade, maior renda e escolaridade, com dislipidemia, consumo de álcool e tabagismo atuais, e prática de atividade física vigorosa. Após o ajuste para variáveis sociodemográficas (idade, sexo, etnia e educação) fatores de risco cardiovascular (hipertensão, diabetes, dislipidemia, tabagismo, ingestão de álcool e atividade física), calorias totais, qualidade da dieta e depressão, os participantes do quinto quintil de ingestão de EPA, DHA e DPA mostraram associação inversa com transtornos de ansiedade: OR 0,82 (IC 95%, 0,69-0,98), OR 0,83 (IC 95%, 0,69-0,98) e OR 0,82 (IC 95%, 0,69-0,98), respectivamente. Participantes no quinto quintil de razão ômega-6/ômega-3 tiveram associação positiva com transtornos de ansiedade. Nenhuma associação foi encontrada com a ingestão de PUFA, ou ômega-3 e ômega-6 isoladamente com ansiedade após os ajustes. Nesta análise, uma alta ingestão de ômega-3 EPA, DHA e DPA foi inversamente associada com a presença de transtornos de ansiedade, enquanto que a alta razão ômega-6/ômega-3 foi diretamente associada à presença desses transtornos, sugerindo um possível efeito protetor dos ácidos graxos omega-3 EPA, DPA e DHA contra a ansiedade / Few studies have evaluated the association of omega-3 fatty acids intake and anxiety disorders. The present study used cross-sectional data from the baseline (2008-2010) examination of the Brazilian Longitudinal Study of Adult Health - ELSA-Brazil to evaluate this association. The dietary exposure was measured by a quantitative food frequency questionnaire validated for the brazilian population and adapted for the study, and the mental diagnoses were assessed by the Clinical Interview Schedule-Revised Version (CIS-R), diagnosing mental disorders according to the International Classification of Diseases - ICD-10. Logistic regression models were built using quintiles of omega-3 fatty acids, omega-6 fatty acids, omega-6/omega-3 ratio, and polyunsaturated fatty acids consumption, using the first quintile as a reference. Of the 15,105 subjects participating in ELSA-Brazil, those who reported ingestion of less than 500 or more than 4000 kcal, those who reported ingestion of omega-3 or omega-6 supplements and those had undergone bariatric surgery were excluded. After exclusions, 12,268 participants remained in the analysis, of whom 1893 (15.4%) had anxiety disorders. Subjects with anxiety disorder were younger, female, had lower education and income, reported current smoking and mild physical activity. Higher values of BMI and high sensibility C reactive protein were observed in subjects with anxiety. The mean daily intakes of eicosapentaenoic acid (EPA), docosapentaenoic acid (DPA) and docosahexaenoic acid (DHA) were significantly lower in subjects with anxiety. A higher intake of these three omega-3 fatty acids was observed in older individuals with higher income and education, with current dyslipidemias, alcohol consumption and smoking, and vigorous physical activity. After adjustment for socio-demographic variables (age, sex, ethnicity and education), cardiovascular risk factors (hypertension, diabetes, dyslipidemia, smoking, alcohol intake and physical activity), total calories, diet quality and depression, EPA, DHA and DPA intakes showed an inverse association with anxiety disorders: OR 0.82 (95% CI, 0.69-0.98), OR 0.83 (95% CI, 0.69-0.98) and OR 0.82 (95% CI, 0.69-0.98), respectively. Participants in the fifth quintile of omega-6/omega-3 ratio had a positive association with anxiety disorders. No association was found with ingestion of PUFA, or omega-3 and omega-6 alone with anxiety after adjustments. In this analysis, a high intake of omega-3 EPA, DHA and DPA was inversely associated with the presence of anxiety disorders, while the higher omega-6 omega-3 ratio was directly associated with the presence of these disorders, suggesting a possible protector effect of omega-3 fatty acids EPA, DPA and DHA against anxiety

Ácidos graxos ômega-3

Ácidos graxos ômega-6

Ácidos graxos poli-insaturados

Razão ômega6/ômega3

Transtornos de ansiedade

Transtornos mentais

Anxiety disorders

Mental disorders

Ômega-3 fatty acids

Ômega-6 fatty acids

Omega6/omega3 ratio

Polyunsaturated fatty acids

Potential of omega-3 EPA/DHA 6/1 to ameliorate ageing-related endothelial dysfunction / Potentiel de la formulation omega-3 EPA/DHA 6/1 à améliorer la dysfonction endothéliale liée à l’âge

Farooq, Muhammad Akmal

17 October 2018

La présente étude évalue la capacité de la formulation d’oméga-3 EPA:DHA 6:1, une formulation capable d’induire la formation continue de monoxyde d’azote par la NO synthase endothéliale, à améliorer la dysfonction endothéliale liée à l’âge établie chez le rat. La dysfonction endothéliale liée à l’âge est caractérisée par une altération des composantes de la relaxation et une augmentation des réponses contractiles dépendantes de l’endothélium. L’âge augmente le stress oxydant vasculaire, l’expression de la NADPH oxydase, COX-2, eNOS, ACE, AT1R, et des marqueurs de senescence, alors que la COX-1 est sous-exprimé. La formulation EPA:DHA 6:1 améliore la composante NO, diminue l’EDCF et le stress oxydant vasculaire, et normalise l’expression des protéines cibles. En conclusion, la consommation chronique de EPA:DHA 6:1 améliore la dysfonction endothéliale liée à l’âge chez le rat, probablement en prévenant l’activation du système angiotensine locale et le stress oxydant en résultant. / EPA:DHA 6:1 omega-3 formulation has been shown to induce a sustained endothelial NO synthase-derived formation of nitric oxide. This study examined if the intake of EPA:DHA 6:1 improves an established ageing-related endothelial dysfunction. Ageing-related endothelial dysfunction was characterized by a blunted NO-mediated component of relaxation, abolished EDH-mediated component and increased COX-derived endothelium-dependent contractile responses. Ageing increased vascular oxidative stress, expression of NADPH oxidase subunits, COX-2, eNOS, ACE, AT1R, and senescence markers, whereas COX-1 was down-regulated. Chronic intake of EPA:DHA 6:1 improved the NO-mediated relaxations, reduced EDCFs, vascular oxidative stress and normalized the expression of protein markers. In conclusion, chronic intake of EPA:DHA 6:1 prevented the ageing-related endothelial dysfunction in old rats, most likely by preventing activation of the local angiotensin system and the subsequent vascular oxidative stress.

Vieillissement

Endothélium vasculaire

Monoxyde d’azote

Acides gras polyinsaturés oméga-3

Stress oxydant

Système angiotensine Local

Ageing

Vascular Endothelium

Nitric Oxide

Omega-3 polyunsaturated fatty acids

Oxidative stress

Local angiotensin system

615.7

616.13

Interações entre exposição a trauma no início da vida e deficiências de ácidos graxos poliinsaturados N-3 em marcadores biológicos de transtornos psiquiátricos / Interactions between early life trauma exposure and polyunsaturated fatty acid n-3 deficiency in biological markers of psychiatric disorders

Ferreira, Charles Francisco

January 2015

As exposições precoces às diferentes intervenções, como dietas e estresse, estão associadas a persistentes alterações sobre aspectos neuroquímicos e comportamentais, podendo este ser considerado um gatilho de transtornos psiquiátricos na vida adulta. O presente trabalho objetivou determinar se estas intervenções neonatais poderiam interagir com uma dieta deficiente em ácidos graxos poliinsaturados n-3 (n-3 PUFA), aplicados durante o desenvolvimento, com foco nos níveis centrais (hipocampo) e séricos do fator neurotrófico derivado do encéfalo (BDNF), bem como sobre a atividade enzimática e aspectos morfológicos (e.g. massa, potencial) mitocondriais do hipocampo de ratos machos adultos. Em nossa abordagem experimental animal, as ninhadas foram distribuídas aleatoriamente nos grupos intactos, manipulados neonatalmente [MN, separação mãe-filhote durante 10min/dia, entre o 1° e o 10° dia pós-natal (DPN)] e separado maternalmente [SM, separação mãe-filhote durante 3h/dia, entre o 1° e o 10° DPN]. No DPN 35, os filhotes machos foram agrupados em dieta n-3 PUFA adequada ou deficiente, por 17 semanas de tratamento. O peso e o consumo de ração foram aferidos semanalmente. Após este tratamento, soro e hipocampo foram coletados. Kits comerciais foram utilizados para a medição dos níveis hipocampais e séricos de BDNF (ELISA), bem como a atividade dos complexos da cadeia respiratória mitocondrial (método enzimático, análise espectrofotométrica), massa e potencial mitocondriais (MitoTracker, citometria de fluxo). A expressão gênica de BDNF no hipocampo também foi medido por RT-qPCR. Os testes estatísticos utilizados foram ANOVA de duas vias ou de medidas repetidas. Os níveis de significâncias foram fixados em p<0,05. A dieta deficiente em n-3 PUFA, associada aos estressores neonatais deste estudo (MN, SM) foram capazes de alterar o peso corporal e a ingestão de alimentos de um modo específico, uma vez que os níveis mais elevados destes parâmetros foram encontrados em animais submetidos a SM. Animais submetidos a MN alimentados com uma dieta n-3 PUFA deficiente exibiram uma maior atividade exploratória em resposta a um psicoestimulante (dietilpropiona). Embora os níveis proteicos séricos e hipocampais de BDNF permaneceram inalterados pelos tratamentos aplicados, fomos capazes de demonstrar a redução de sua expressão gênica em animais alimentados com uma dieta n-3 PUFA deficiente. Considerando os padrões mitocondriais e parâmetros de estresse oxidativo, as atividades das enzimas antioxidantes glutationa peroxidase (GPx) e catalase (CAT), bem como a produção de espécies reativas de oxigênio (EROs) se encontraram aumentadas no hipocampo de animais submetidos a uma deficiência crônica em n-3 PUFA. Esta deficiência mostrou interações com o fator estresse neonatal em alguns destes parâmetros (e.g. atividade da GPx, produção de EROs), indicando um possível sinergismo entre estressores neonatais e a deficiência em n-3 PUFA. Os níveis de tióis foram significativamente menores nos grupos estressados (MN, SM), sendo a dieta n-3 PUFA deficiente capaz de aumentar a quantidade de tiol no hipocampo. Por outro lado, animais estressados tratados cronicamente com uma dieta deficiente em n-3 PUFA apresentaram níveis mais elevados de tiol. Contudo, a MN per se foi capaz de diminuir o potencial mitocondrial hipocampal. Adicionalmente, um estudo com humanos teve como objetivo correlacionar os níveis de BDNF periféricos ao consumo de n-3 PUFA em adolescentes. Para este estudo, 137 adolescentes de uma amostra enriquecida para psicopatologias de ansiedade foram submetidos a um questionário de frequência alimentar (QFA), para uma análise quantitativa do consumo de macronutrientes e micronutrientes de n-3 PUFA. As correlações de Spearman foram realizadas para avaliar possíveis associações entre o consumo de n-3 PUFA e os níveis periféricos de BDNF. As amostras de sangue foram coletadas entre 7 a 10h após o período de 10-12h de jejum, sendo o soro armazenado para medir os níveis de BDNF. Todas as análises de BDNF foram realizadas no mesmo dia por ELISA, utilizando anticorpos monoclonais específicos para o BDNF, de acordo com as instruções do fabricante. Os efeitos de possíveis confundidores (e.g. consumo total de gordura, idade, sexo e medida de ansiedade) foram examinados por modelos de regressões lineares. Apesar de algumas limitações apresentadas (e.g. o tamanho reduzido da amostra, alta incidência de adolescentes ansiosos), o que poderia limitar a validade externa deste resultado, fomos capazes de detectar uma correlação entre o consumo de n-3 PUFA e os níveis séricos de BNDF em adolescentes. Como conclusão geral, esta tese demonstra que a manipulação neonatal e separação materna, associada com uma deficiência em n-3 PUFA, são capazes de alterar parâmetros comportamentais e neuroquímicos na idade adulta. Este sinergismo foi capaz de diminuir a expressão gênica de BDNF no hipocampo, embora não apresentando qualquer alteração deste parâmetro perifericamente. A correlação entre os níveis consumidos de n-3 PUFA, em uma população de adolescentes em idade escolar, com os níveis séricos de BDNF também foi encontrada. Ainda, as alterações nas atividades enzimáticas mitocondriais observadas no hipocampo destes animais reforçam a importância da participação desta estrutura, além de sua possível relação com o desenvolvimento de desordens psiquiátricas e de humor. Considerando-se a nossa abordagem metodológica em ratos, a mesma pode ser um protocolo útil para se estudarem as interações entre o ambiente precoce e a nutrição ao curso de vida em diferentes desfechos neuroquímicos. / Early exposure to different interventions, as diets and stress, are associated with persistent alterations in neurochemistry and behavior, and can be considered a trigger of psychiatric disorders in adulthood. This study investigated whether neonatal interventions interact with a diet deficient in n-3 polyunsaturated fatty acids (n-3 PUFA) applied during development, focusing on central (hippocampus) and serum brain-derived neurotrophic factor (BDNF), as well as mitochondrial enzymatic activity and morphology (e.g. mass, potential) in adult male rats. In our animal study, litters were randomized into non-handled (NH), handled [H, mother-offspring separation for 10min/day from 1st-10th postnatal day (PND)] and separated (S, separation for 3h/day from the 1st-10th PND) groups. On PND 35, male pups were randomized into adequate or deficient diet in n-3 PUFA for 17 weeks. The weight and food intake were measured weekly. Serum and hippocampi were collected after this n-3 PUFA treatment. Commercial kits were used for measuring hippocampal and serum BDNF (ELISA), as well as mitochondrial chain respirator complexes (enzymatic method, spectrophotometric analysis), mitochondrial mass and potential (MitoTracker, flow citometry). Hippocampal BDNF gene expression was also measure by RT-qPCR. Statistical testes used were Two-Way or repeated measures ANOVA. Significance levels were set at p<0.05. A n-3 PUFA deficient diet, in association with neonatal stressors used in this study (H, MS) were able to alter body weight and food intake in a specific way, since higher levels of these parameters were found in animals subjected to MS. Animals subjected to H fed an n-3 PUFA deficient diet displayed enhanced exploratory activity in response to a psychostimulant (diethylpropion). Although serum protein levels and hippocampus BDNF remained unchanged by the treatments applied, we were able to demonstrate its gene expression reduction in the hippocampus of animals fed an n-3 PUFA deficient diet. Considering mitochondrial and oxidative stress parameters, the activities of antioxidant enzymes glutathione peroxidase (GPx) and catalase (CAT) and the production of reactive oxygen species (ROS) were increased in the hippocampus of rats subjected to a deficiency n-3 PUFA. This deficiency displayed interactions with neonatal stress factor in some of these parameters (e.g. GPx activity, ROS), indicating a possible synergism between neonatal stressors and n-3 PUFA deficiency. Thiol levels were significantly decreased by neonatal stressors (H and MS), and the n-3 PUFA deficient diet was able to increase its total amount in hippocampus. On the other hand, chronically stressed animals treated with an n-3 PUFA deficient diet showed higher thiol levels. However, H per se was able to decrease mitochondrial potential in hippocampus. Additionally, a clinical study aimed to correlate peripheral BDNF levels and n-3 PUFA consumption in adolescents. For this study, 137 adolescents from a sample enriched for psychopathology of anxiety were subjected to a food frequency questionnaire (FFQ), in order for measuring the quantitative analysis of n-3 PUFA macronutrients and micronutrients consumption. Spearman correlations were performed to assess the association between n-3 PUFA consumption and serum BDNF levels. Blood samples were collected between 7 and 10h after fasting period of 10-12h, and serum was stored in order to measure BDNF levels. All BDNF measurements were performed in the same day by sandwich-ELISA using monoclonal antibodies specific for BDNF, according to the manufacturer’s instructions. Effects of potential confounders (e.g. total fat consumption, age, gender, anxiety) were examined using linear regression models. Although some limitations were presented (e.g. small sample size with high incidence of eager teenagers), which could limit the external validity of this result, we were able to detect a correlation between the consumption of n-3 PUFA and BDNF serum levels in adolescents. As a general conclusion, this thesis reports that neonatal handling and maternal separation, associated with a nutritional deficiency in n-3 PUFA, were able to change behavioral and neurochemical parameters in adulthood. This synergism was able to decrease BDNF gene expression in the hippocampus, while not presenting any change of this parameter peripherally. A correlation between the consumption levels of n-3 PUFA, in a population of schoolchildren with BDNF serum levels was also found. Still, changes in mitochondrial enzymatic activities observed in the hippocampus of these animals reinforce the importance of this structure participation and its relation to the development of psychiatric and mood disorders. Considering our rat methodological approach, it can be a useful tool for studying the interactions between early life environment and life-course nutrition on different neurochemical outcomes.

Manipulação neonatal

Ácidos graxos insaturados

Hipocampo

Mitocôndrias

Comportamento animal

Estresse

Transtornos mentais

Early stress

Neonatal handling

Maternal separation

N-3 polyunsaturated fatty acid

N-3 PUFA

Psychiatric disorders

Voies de signalisation impliquées dans la sensibilisation des tumeurs mammaires au docétaxel par les acides gras polyinsaturés n-3 / Signaling pathways involved in breast cancer cell chemosensitization to docetaxel by n-3 polyunsaturated fatty acids

Chauvin, Lucie

11 December 2015

La résistance des cellules tumorales à la chimiothérapie constitue une cause majeure d’échec des traitements anticancéreux. Des études précliniques montrent que les acides gras polyinsaturés oméga-3 à longues chaînes (AGPIn-3LC), apportés par l’alimentation, améliorent l’efficacité des chimiothérapies sans majorer les effets secondaires. Cette thèse a eu pour but d’identifier les mécanismes moléculaires impliqués dans l’augmentation de la sensibilité des cellules tumorales mammaires au docétaxel. Nous avons montré que le docétaxel induit un mécanisme de résistance via l’activation des voies de signalisation PKC/ERK et Akt impliquées dans la prolifération et la survie cellulaires. La modification de l’environnement lipidique membranaire par la supplémentation en AGPIn-3LC inhibe ces voies de signalisation et augmente l’efficacité du docétaxel dans des lignées tumorales mammaires et dans un modèle préclinique de tumeurs mammaires autochtones chez le rongeur. De plus, dans ce modèle in vivo, nous avons identifié une autre cible moléculaire régulée par les AGPIn-3LC : l’épiréguline, membre de la famille EGF. Les AGPIn-3LC bloquent l’induction de l’épiréguline par le VEGF dans les cellules endothéliales et induisent un remodelage de la vascularisation tumorale. Outre un effet direct des AGPIn-3LC sur les cellules tumorales, les AGPIn- 3LC agissent sur le microenvironnement tumoral. Ces travaux de thèse apportent des arguments supplémentaires pour l’utilisation des AGPIn-3LC comme molécules adjuvantes pour lutter contre la résistance des tumeurs mammaires aux agents anticancéreux. / Chemotherapy-resistant tumor cells are a major cause of cancer treatment failure. Preclinical studies show that polyunsaturated omega-3 long chain fatty acids (AGPIn-3LC), provided by food, improve the efficacy of chemotherapy without increasing side effects. AGPIn-3LCs are incorporated in cancer and stromal cells. This thesis aimed to identify molecular mechanisms involved in the increased sensitivity of mammary tumor cells to docetaxel. We have shown that docetaxel induces a resistance mechanism via activation of PKC/ERK and Akt pathways involved in cell proliferation and survival. Modification of the membrane lipid environment by AGPIn-3LCs supplementation inhibits these signaling pathways and increases the efficacy of docetaxel in mammary tumor cell lines and in a preclinical rodent model of native mammary tumors. Moreover, in this mammary tumor model we have found another molecular target regulated by AGPIn-3LCs: epiregulin, a member of the EGF family. AGPIn-3LCs inhibit epiregulin-VEGF induced in endothelial cells and induce a remodeling of tumor vasculature. Furthermore, AGPIn-3LCs act on the tumor microenvironment directly. This thesis work provides additional arguments for the use of AGPIn-3LCs as adjuvant molecules to reduce the resistance of breast tumors to anticancer agents.

Acide docosahéxanoïque

Cancer du sein

Chimiosensibilisation

Docétaxel

Voies de signalisation

Docosahexanoic acid

Breast cancer

Chemosensitization

Docetaxel

Signaling pathways