Global ETD Search

131	Síntese, caracterização e reatividade de antiradicais de dupla função / Synthesis , Characterization and Reactivity of Dual Function of Antioxidants Thiago Bueno Ruiz Papa 29 October 2015 (has links) A deterioração oxidativa de alimentos é o fator determinante na qualidade sensorial e nutricional do produto, podendo ocorrer em alimentos complexos tanto na fase contínua como na fase dispersa. Em geral, a formação de radicais e espécies reativas de oxigênio e nitrogênio é o evento primário que ocorre priori ao progresso da oxidação de componentes e estruturas sensíveis e está comumente associado a eventos na fase aquosa. A oxidação de lipídeos é frequentemente investigada em alimentos e em meio biológico separadamente dos eventos no meio aquoso e a proteção antioxidante somente avaliada na fase dispersa. Entretanto, a oxidação de proteínas e eventos na fase contínua vêm despertando considerável interesse e aparentemente antioxidantes eficientes na fase dispersa não protegem de forma eficaz as proteínas e os componentes na fase contínua. Um futuro progresso na proteção antioxidante de alimentos e sistemas biológicos origina de uma abordagem holística dos processos redox envolvidos em ambas as fases dispersa e contínua, bem como o uso combinado de espécies antioxidantes e antiredutoras para um superior efeito antiradical global. Neste sentido, foram preparados três novos compostos antiradicais de dupla função (antioxidante e antiredutor) com adequado balanço hidrofílico-lipofílico e aprimorada propriedade antiradical global. Os antiradicais diferulato de astaxantina, retinoato de quercetina e retinoato de epicatequina se mostraram melhores antioxidantes e antiredutores do que seus precursores isoladamente ou em misturas, apresentando superior eficiência na desativação do oxigênio singlete excitado, captação do radical 1-hidroxietila, menor efeito pró-oxidante em sistemas de oxidação catalisados por íons de ferro, e eficiência na redução do reativo estado triplete da safranina (E1/2 = 1,48 V vs. NHE). / The oxidative deterioration of foods is the determining factor in the sensory and nutritional quality of the product, which may occur in complex food both at the continuous and the dispersed phases. In general, the formation of radicals and reactive oxygen and nitrogen species is the primary event that occurs prior to the progress of oxidation of components and sensitive structures and is commonly associated with events in the aqueous phase. The oxidation of lipids is often investigated in food and biological media separately from the events in the aqueous phase and the measurement of the antioxidant protection is only evaluated in the dispersed phase. However, the oxidation of proteins and the events in the continuous phase have attracted considerable interest and apparently, efficient antioxidants in dispersed phase do not effectively protect proteins and components in the continuous phase. A further progress in the antioxidant protection of food and biological systems arise from a holistic approach of the redox processes involved in both the dispersed and continuous phases as well as the combined use of antioxidant and antireductant species for a superior overall antiradical effect. In this sense three new antiradical compounds with dual function (antioxidant and antireductant) were prepared with proper hydrophilic-lipophilic balance and global antiradical properties. The antiradicals astaxanthin diferulate, epicatechin retinoate, and quercetin retinoate are shown to be better antioxidant and antireductant than their precursors, isolated or in mixture, exhibiting enhanced singlet excited oxygen deactivation, 1-hydroxyethyl radical scavenging, lower pro-oxidative effect in the oxidative system catalysed by iron ions and an efficient reduction of the reactive triplet state of safranine (E1 / 2 = 1.48 V vs. NHE). ácido retinóico antioxidantes antirardicais antiredutores astaxantina epicatequina polifenóis quercetina antioxidante antiradicals antireductant astaxanthin epicatechin plant phenols quercetin retinoic acid
132	Functional and structural studies of proteins involved in the development and nerve signaling = FEZ1, SCOC and RARA = Estudos funcionais e estruturais de proteínas envolvidas no desenvolvimento e sinalização nervosa: FEZ1, SCOC e RARA / Estudos funcionais e estruturais de proteínas envolvidas no desenvolvimento e sinalização nervosa : FEZ1, SCOC e RARA Furlan, Ariane Silva, 1986- 05 October 2013 (has links) Orientador: Jörg Kobarg / Dissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Biologia / Made available in DSpace on 2018-08-23T08:43:43Z (GMT). No. of bitstreams: 1 Furlan_ArianeSilva_M.pdf: 17272017 bytes, checksum: cc7e8f01d7f236f37a6c9c63fcb9a8f9 (MD5) Previous issue date: 2013 / Resumo: O resumo poderá ser visualizado no texto completo da tese digital quando liberada / Abstract: The abstract is available with the full electronic document when available / Mestrado / Bioquimica / Mestra em Biologia Funcional e Molecular Proteína FEZ1 humana Proteína SCOC humana Receptor de ácido retinóico alfa FEZ1 protein, human SCOC protein, human Retinoic acid receptor alpha
133	Avaliação do efeito antitumoral in vitro de nanocápsulas de núcleo lipídico de tretinoína sobre células de adenocarcinoma de pulmão, linhagem A549 / In Vitro Antitumor Activity of Tretinoin-Loaded Lipid-Core Nanocapsules on human lung adenocarcinoma cell line (A549) Schultze, Eduarda 26 February 2013 (has links) Made available in DSpace on 2014-08-20T13:32:47Z (GMT). No. of bitstreams: 1 dissertacao_eduarda_schultze.pdf: 1903452 bytes, checksum: 1fd6d0e0478c9c31687ae8d7882532ea (MD5) Previous issue date: 2013-02-26 / Retinoid derivatives and analogs have been widely studied as antitumor agents due to their effects on cell proliferation and differentiation. Tretinoin (TT), also known as retinoic acid is a retinoid derivative that has been used as an adjuvant in the treatment of acute promyelocytic leukemia with excellent rates of remission. This compound has antiproliferative activity in various tumor types. However, non small cell lung cancer in general exhibit strong resistance to the effects of TT, which may be related to the deficiency in the cellular up-take of TT in that cell type. A strategy to enhance the antiproliferative activity of TT is to increase the cellular internalization of the compound through carriers such as liposomes or other vesicles or nanospheres or nanocapsules. Here we evaluated TT lipid-core nanocapsules (TT-LCNC) for their power to inhibit growth, induce apoptosis and interfere with the cell cycle of lung adenocarcinoma, A549 cell line, which is resistant to treatment with TT. The results showed that TT-LCNC was able to overcome the cellular resistance to treatment with TT, reducing cell viability and inducing apoptosis, upregulation of P21 and cell cycle arrest in G1 phase. / Derivados e análogos retinóides têm sido largamente estudados como agentes antitumorais devido a seus efeitos sobre a proliferação e diferenciação celular. Tretinoína (TT), também conhecida como ácido retinóico é um derivado retinóide que tem sido usado como adjuvante no tratamento de leucemia promielocítica aguda com excelentes índices de remissão da doença. Este composto exerce atividade antiproliferativa em diversos tipos de tumores. Entretanto, células de adenocarcinoma de pulmão humano em geral exibem uma forte resistência aos efeitos da tretinoína, a qual pode estar relacionada com a deficiência na internalização celular de tretinoína nesse tipo de célula. Uma estratégia para aumentar a atividade antiproliferativa de tretinoína é aumentar a captação celular do composto através de carreadores como lipossomas ou outras vesículas como nanocápsulas ou nanoesferas. Neste trabalho nanocápsulas de núcleo lipídico contendo tretinoína (TT-LCNC) foram avaliadas quanto ao seu potencial de inibir o crescimento, induzir a apoptose e interferir com o ciclo celular de células de adenocarcinoma de pulmão, linhagem A549, resistentes ao tratamento com TT livre. Os resultados demonstraram que TT-LCNC foi capaz de superar a resistência celular ao tratamento com TT, reduzindo a viabilidade celular e induzindo apoptose, superexpressão de P21 e parada do ciclo celular em G1. Tretinoin Retinoic acid Nanocapsules Lung cancer P21 Tretinoína Ácido retinóico Nanocápsulas Câncer de pulmão P21 CNPQ::CIENCIAS BIOLOGICAS::GENETICA
134	Evolution of the retinoic acid receptor / Evolution du récepteur de l'acide rétinoïque Gutierrez Mazariegos, Juliana 28 March 2014 (has links) L’acide rétinoïque (AR) est un morphogène dérivé de la vitamine A qui contrôle des processus clés au niveau cellulaire et pendant le développement embryonnaire des chordés. Chez les vertébrés les principaux acteurs de la voie de signalisation de l’AR sont les récepteurs de l’acide rétinoïque (RAR) et les récepteurs des x rétinoïdes (RXR). L’évolution de RAR est encore très mal connue cependant, des données récentes indiquent qu’il est également présent chez des animaux non-chordés. Suggérant ainsi, que l’origine évolutive de RAR et de la voie de signalisation de l’AR est plus ancienne qu’initialement prévu. Durant ma thèse j’ai pu retracer l’histoire évolutive de ce récepteur depuis son origine chez Urbilateria jusqu'à sa diversification, suite aux duplications génomiques chez les vertébrés. En caractérisant les RARs d’un annélide, un mollusque et un oursin j’ai démontré que chez l’annélide et l’oursin RAR est activé par l’AR, contrairement au RAR de mollusque qui n’est pas fonctionnel avec l’AR. De plus, des études menées chez l’annélide ont montré que les gènes régulés par l’AR chez cette espèce sont différents de ceux régulés chez les vertébrés. Ces données permettent donc de s’interroger sur la fonction ancestrale probable que ce récepteur avait chez Urbilateria. Finalement, la caractérisation moléculaire des RAR de cyclostomes nous a permis d’étudier l’impact des duplications génomiques sur l’évolution de la poche de liaison au ligand. Ainsi, les résultats obtenus pendant ma thèse permettent de mieux comprendre les relations entre le récepteur et son ligand ainsi que de découvrir de nouveaux aspects sur la fonction de RAR en présence de ligands non-classiques. / Retinoic acid (RA) is a fat-soluble morphogen derived from vitamin A that controls key cellular and developmental processes in chordates. In vertebrates, the major actors of the RA signaling pathway are the retinoic acid receptors (RARs) and the retinoid X receptors (RXRs). The evolution of RAR is still poorly understood, however, recently RARs have been identified in the genome of non-chordate species, suggesting that RAR and the RA pathway might have a more ancient evolutionary origin than previously thought. The work presented in this manuscript allowed us to retrace the evolutionary history of RAR from its origin in Urbilateria to its diversification following whole genome duplication events in vertebrates. We describe the characterization of the RARs from an annelid, a mollusk and a sea urchin. We showed that the receptors from the annelid and the sea urchin are functional RARs, however, the receptor from the mollusk is not functional with RA. Studies carried out in the annelid revealed that the signaling pathways regulated by RA in this species are different to the ones it regulates in vertebrates. These observations raise questions about the function of RA and RAR on the embryonic development of non-chordate species and their possible function in Urbilateria. Finally, the molecular characterization of cyclostome RARs allowed us to characterize the impact of whole genome duplications on the evolution of the ligand-binding pocket. Altogether, these data will allow us to better understand the relationship between the receptor and its ligand and to reveal novel insights on the function of RAR in response to non-classical ligands. Acide rétinoïque Évolution Récepteurs nucléaires Évolution des bilatériens Lophotrochozoaires Ambulacraires Retinoic acid Evolution Nuclear receptors Bilaterian evolution Lophotrochozoans Ambulacrarians 570
135	Analysis of cellular retinoic acid binding protein 2 expression in dermal fibroblasts; role in non-healing of chronic wounds Amjad, Arshi January 2017 (has links) Abstract Chronic, non-healing wounds constitute a massive financial burden on health care system. The healing processes of these wounds and their underlying pathology are only partly understood. In this study, important biological functions performed by Retinoic acid with its regulatory protein cellular retinoic acid binding protein 2 (CRABP2) were discussed. Possibly, these biological func-tions might be linked with chronic wound therapeutic by inducing antiproliferative activity of cells which leads to reduction in migration and growth rate of fibroblast during skin regeneration pro-cess in chronic wound healing. The aim of this study was to comparatively analyze the expression pattern of CRABP2 and P16 cyclic dependent kinase inhibitor in dermal fibroblasts at mRNA levels along with their morphological pattern, migration and growth rate. Fibroblasts were cultured and their morphology were observed by phase-contrast imaging. Difference in viability, migratory capacity was examined by Cell titer blue and scratch assay respectively and expression were meas-ured by polymerase chain reaction. Interestingly, the date revealed that morphology was altered and growth rate and migration velocity was significantly lower in chronic wound fibroblasts and senescent fibroblasts when compared with their control. Expression pattern revealed that CRABP2 was highly up-regulated only by senescent cells but not in chronic wound fibroblasts which point novel function for this protein in term of replicative senescence. However, P16 was not signifi-cantly altered among all fibroblasts which demands supplementary studies to conform the role of CRABP2 in fibroblast dysfunction and cellular senescence in chronic wounds. CRABP2 p16 chronic wound fibroblast senescent fibroblasts cellular senes-cence retinoic acid non-healing wounds. Medical and Health Sciences Medicin och hälsovetenskap
136	Repurposing 13-Cis-Retinoic Acid: A Potential Treatment for Aneurysms-Osteoarthritis Syndrome Putos, Samantha January 2015 (has links) Approximately 7000 rare disorders exist, affecting 2 percent of Canadians and millions of people worldwide. Given that for many rare diseases only one allele is mutated, we hypothesize inducing expression of the remaining wild-type allele may have a therapeutic effect. SMAD3 heterozygosity results in Aneurysms-Osteoarthritis Syndrome (AOS) – an aortic aneurysm disorder also known as Loeys-Dietz Syndrome Type 3. We conducted a screen of FDA-approved compounds and found that 13-cis-retinoic acid (13-CRA) induces SMAD3 in normal human fibroblast cultures. Treatment with therapeutic concentrations of 13-CRA increased SMAD3 mRNA in normal human fibroblasts, patient fibroblasts, wild-type murine vascular smooth muscle cells and Smad3+/- murine vascular smooth muscle cells. Increases in SMAD3 protein were also observed in normal human fibroblasts, patient fibroblasts, and wild-type murine vascular smooth muscle cells. Immunofluorescent imaging revealed the primary site of protein induction to be nuclear. We report here the in vitro induction of SMAD3 mRNA and protein by therapeutic levels of 13-CRA and suggest further investigation of this modality for the treatment of AOS. Loeys-Dietz Syndrome Type 3 Aneurysms-Osteoarthritis Syndrome SMAD3 13-cis-retinoic acid Isotretinoin Care for Rare TGF-beta
137	A sinalização pelo ácido retinóico e a origem evolutiva das câmaras cardíacas. / Retinoic acid signaling and the evolutionary origins of cardiac chambers. Marcos Sawada Simões Costa 17 April 2009 (has links) Nos últimos anos, nós propusemos um modelo de duas etapas para a padronização antero-posterior do coração. Ácido retinóico (AR) produzido pela enzima RALDH2 induz o destino sino atrial nos precursores cardíacos posteriores. Subsequentemente, estes precursores adquirem a capacidade de expressar RALDH2, formando uma onda caudo-rostral desta enzima. A nossa hipótese é que esta onda surgiu nos para padronizar as células precursoras da bomba circulatória ancestral em regiões de influxo e efluxo, resultando na origem das câmaras cardíacas. Para testar se a onda cauro-rostral é ancestral nos vertebrados, nós mapeamos a expressão de RALDH2 em relação ao campo cardíaco em anfíbios, vertebrados basais e no cordado invertebrado anfioxo. Nossos dados sugerem que o modelo de duas etapas está presente em anfíbios e peixes. Clonagem do gene RALDH em lampréias indica presença de AR no campo cardíaco. Em anfioxo, a caracterização do padrão de expressão do ortólogo da RALDH2 revela ausência da onda caudo-rostral. Nossos resultados sugerem que a onda caudo-rostral de RALDH2 foi cooptada nos vertebrados para padronizar o campo cardíaco no eixo AP, o que corrobora a hipotése de que este mecanismo foi importante na origem evolutiva das câmaras cardíacas. / In the last years, we have proposed a 2-step model for the establishment of cardiac chamber identities. Retinoic acid (RA) produced by its synthetic enzyme RALDH2, induces an atrial fate in posterior cardiac precursors of amniote embryos. Subsequently, a RALDH2 caudorostral wave engulfs posterior precursors. Our hypothesis is that this wave evolved in vertebrates to pattern an ancestral circulatory pump into AP fields, which were later fashioned into cardiac chambers. To test whether the wave is an ancestral or derived feature of amniotes, we mapped expression of RALDH2 in relation to the cardiac field in amphibians, basal vertebrates and the amphioxus. Our data suggests RA signaling patterns amphibian and piscine hearts. Cloning of RALDH in lampreys shows that RA synthesis takes place in the heart field. In the amphioxus, cloning of RALDH reveals a vertebrate-like expression pattern, although the RALDH2 wave is absent. Our results support the hypothesis that the caudorostral wave of RALDH2 was coopted to pattern the vertebrate cardiac field. This supports the hypothesis that the caudorostral wave of RALDH2 was an important player in the evolutionary origin of the cardiac chambers. Ácido retinóico Câmara cardíacas Coração Embriogênese Embriologia comparada Evolução Cardiac chambers Compartive embryology Embryogenesis Evolution Heart Retinoic acid
138	Antiproliferative effects of retinoic acid in breast cancer Rozendaal, Maria Johanna 04 1900 (has links) Les rétinoïdes sont utilisés dans le traitement d’une variété de tumeurs malignes et lésions précancéreuses. Leurs effets dans des lignées cellulaires dérivées de tumeurs solides tel que le cancer du sein ont été étudiés extensivement. Cependant, les bénéfices dans le cancer du sein restent à date peu clairs. Ceci est probablement du à l’hétérogénéité des tumeurs mammaires et la réponse très variable aux effets antiprolifératifs de l’acide rétinoïque. Dans les lignées cellulaires cancéreuses mammaires, la réponse l’AR est fortement corrélée au niveau d’expression du récepteur aux estrogènes alpha (ERα), qui régule l’expression du gène qui encode le récepteur à l’acide rétinoïque alpha, RARA. Malgré cela, certaines lignées cellulaires ER-négatives, comme la lignée HER2-positive SK-BR-3, ont été décrites comme étant sensibles à l’AR. Dans le Chapter 2: de cette thèse, nous avons étudié les mécanismes de la signalisation ER-dépendante et ER-indépendante dans les cellules cancéreuses mammaires. Nous avons utilisé des lignées ER-négatives et ER-positives pour démontrer qu’une partie de la réponse à l’AR est indépendante de la signalisation par ER. Nous avons identifié plusieurs gènes cibles primaires de l’AR qui ont des effets similaires à l’AR quand ils sont surexprimés dans des cellules mammaires cancéreuses. Cette étude apporte une meilleure compréhension des mécanismes complexes qui mènent à l’arrêt de croissance induit par l’AR dans les cellules cancéreuses mammaires. Dans le Chapitre 3, nous avons regardé plus en détails la signalisation ER-indépendante par l’AR dans des cellules ayant une amplification des gènes HER2 et RARA et nous avons identifié une synergie entre l’AR et le Herceptin dans ces cellules. Nous proposons que les gènes FOXO jouent une rôle dans cette synergie. Les cellules SK BR 3, ayant une coamplification HER2/RARA, pourraient représenter une classe de tumeurs qui pourraient bénéficier d’un traitement avec des rétinoïdes, en augmentent la réponse au Herceptin et potentiellement en réduisant la résistance au Herceptin. En conclusion, les données présentées dans cette thèse aident à mieux comprendre les mécanismes menant à l’arrêt de croissance induit par l’AR dans les cellules cancéreuses mammaires et fournissent une application potentielle pour l’utilisation de l’AR dans le traitement du cancer du sein. / Retinoids are being used in the treatment of several malignancies and precancerous lesions. Their effects on cell lines derived from solid tumors, such as breast cancer, have also been described extensively. Their benefit in breast cancer, however, remains unclear. This might be because of the high levels of heterogeneity of breast tumors and the very variable response to the antiproliferative effects of retinoic acid. In mammary tumor cell lines, the response to retinoic acid is highly correlated with the expression of the estrogen receptor alpha (ERα), which regulates the expression of the retinoic acid receptor alpha gene RARA. However, some ER-negative cell lines, such as the HER2 positive SK-BR-3 cell line, have been reported to be RA-sensitive. In Chapter 2: of this thesis we have investigated the mechanisms of ER-dependent and ER-independent RA signaling in breast cancer cells. Using ER-positive and ER-negative cell lines, we show that part of the response to RA is independent of ER signaling. Several direct retinoic acid targets were identified that could mimic antiproliferative effects of retinoic acid when overexpressed in breast cancer cells. This study has provided better insight in the complex mechanisms that lead to RA-induced growth arrest in breast cancer cells. In Chapter 3: we looked further into the ER-independent RA signaling in HER2/RARA-amplified cells and identified a synergy between RA and Herceptin in these cells. We propose a role for FOXOs in mediating this synergy. HER2/RARA coamplified breast tumors might represent a subclass of tumors that could benefit from retinoid treatment, both increase antitumor effects of Herceptin, as well as in potentially reducing Herceptin resistance. In conclusion, data presented in this thesis give better insight in the mechanisms of RA induced growth arrest in breast cancer cells and provide a potential application of retinoids in a subset of breast tumors. Cancer du sein Acide rétinoïque HER2 ERalpha Herceptin Breast cancer Retinoic acid
139	Rôle des rétinoïdes dans le contrôle du système dopaminergique et les maladies neurodégénératives associées / Role of retinoids in the control of the dopaminergic system and associated neurodegenerative disorders Ciancia, Marion 26 September 2018 (has links) Une perturbation de la signalisation dopaminergique dans le striatum est à l’origine de troubles moteurs tels que la maladie de Parkinson (MP) ou de Huntington (MH). Une diminution de la signalisation par l’AR a été observée chez les patients atteints de troubles de la voie nigro-striée et dans des modèles de MH et MP. Nos données indiquent que l’AR synthétisé par RALDH1 et se liant au récepteur RARβ dans le striatum est nécessaire au maintien du système nigro-strié. Une perturbation de cette signalisation entraîne une diminution de l’activité mitochondriale qui conduit à une augmentation du stress oxydatif puis à l’entrée en apoptose de la cellule. Il en résulte des troubles moteurs de type MH et MP. Le rétablissement du niveau striatal de l’AR et la stimulation de RARβ par un agoniste spécifique permettent de prévenir ces phénotypes. Nos travaux nous permettent de proposer RARβ comme une nouvelle cible thérapeutique potentielle dans le cadre des neurodégénérescences de type MH et MP. / A disturbed dopaminergic signaling in the striatum leads to motor disorders such as Huntington’s (HD) and Parkinson’s (PD) diseases. A decrease of the retinoic acid (RA) signaling is observed in patients presenting disorders of the nogro-striatal pathway as well as in HD and PD models. Our data indicate that RALDH1-synthesized RA that binds the receptor RARβ in the striatum is essential to maintain the nigro-striatal system. A disturbance in this RA signaling leads to a decreased mitochondrial respiration, an increased oxidative stress and an increased apoptosis in the dorso-lateral striatum. This cellular alterations lead to HD-like and PD-like motor disorders A rescue of the striatal RA level or the stimulation of RARβ by a specific agonist prevent this phenotypes. Our work allow us to point at RARβ as a new potential therapeutic target for neurodegenerescences like HD and PD. Striatum Dopamine Acide rétinoïque RARβ Mitochondries Neurodégénérescence. Striatum Dopamine Retinoic acid RARβ Mitochondria Neurodegenerative disorders 615.7 616.8
140	M1 to M2 Macrophage Induction Using Retinoic Acid and Mesenchymal Stem Cells Loaded on an Electrospun Pullulan/Gelatin Scaffold To Promote Healing of Chronic Wounds Assani, Kaivon 28 August 2018 (has links) No description available. Biomedical Engineering macrophage M1 to M2 macrophage induction chronic wounds tissue repair regenerative therapy retinoic acid mesenchymal stem cells

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