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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
1

Mechanistic Analysis of Differential Signal Transduction Mediated by the Insulin Receptor Substrate Proteins IRS-1 and IRS-2: A Dissertation

Landis, Justine M. 11 August 2014 (has links)
The Insulin Receptor Substrate (IRS) proteins IRS-1 and IRS-2 are cytoplasmic adaptor proteins that organize and propagate intracellular signaling downstream of specific growth factor receptors, including the Insulin and Insulin-Like Growth Factor-1 Receptors (IR and IGF-1R, respectively). Despite sharing a high level of homology and the ability to stimulate Phosphotidylinositol-3-Kinase (PI3K) and Mitogen-Activated Protein Kinase (MAPK) signaling, IRS-1 and IRS-2 play distinct roles in mammary tumor progression. Specifically, IRS-1 promotes growth and proliferation, whereas IRS- 2 promotes motility, invasion, survival, aerobic glycolyis, and metastasis. To further understand the differences between IRS-1 and IRS-2, I investigated the mechanistic basis of IRS-2-mediated PI3K activation. I identified tyrosines in IRS-2 that mediate its recruitment and activation of PI3K in response to insulin and IGF-1 stimulation. Using a PI3K-binding deficient IRS-2 mutant, I demonstrated that IRS-2-dependent PI3K signaling promotes aerobic glycolysis through its ability to selectively regulate the phosphorylation of the Akt effector Glycogen Synthase Kinase-3β (Gsk-3β). I also performed a rigorous comparison of IRS-1 and IRS-2 signal transduction and their ability to regulate functions associated with tumor progression. These studies required the generation of a novel model system where IRS-1 and IRS-2 function could be compared in a genetically identical background. Using this model, I confirmed a role for IRS-1 in growth regulation and IRS-2 in tumor cell invasion, as well as expanded the understanding of differential IRS protein function by showing that IRS-2 more vi effectively promotes Akt activation. The model system I have established can be used for further characterization of IRS-1 and IRS-2-specific functions.
2

Nck1 is required for ER stress-induced insulin resistance and regulation of IRS1-dependent insulin signalling

Laberge, Marie-Kristine. January 2008 (has links)
Activation of the Unfolded Protein Response (UPR) following stress in the Endoplasmic Reticulum (ER) is an important mechanism by which obesity results in insulin resistance and type II diabetes. We uncovered a role for the adaptor protein Nck in modulating the UPR. In this study, we report that obese Nck1-/- mice, which show lower levels of UPR in liver and adipose tissue, present improved insulin signalling in these tissues. We established that the effect of Nck1 is cell autonomous by showing that HepG2 cells treated with Nck1 siRNA have reduced ER stress-induced UPR and Insulin Receptor Substrate-1 (IRS-1) serine phosphorylation. In these cells, we observed that the IRS-1 levels and activation of signalling components downstream of the insulin receptor were increased. This correlates with enhanced cell survival to stress and insulin stimulated glycogen synthesis. Overall, we demonstrated that Nck1 participates in ER-stress-induced insulin resistance and regulation of IRS-1-dependent signalling.
3

Nck1 is required for ER stress-induced insulin resistance and regulation of IRS1-dependent insulin signalling

Laberge, Marie-Kristine. January 2008 (has links)
No description available.
4

Avaliação da etapa inicial do sinal insulínico em tecido muscular e hepático de ratos tratados cronicamente com NaF

Chiba, Fernando Yamamoto [UNESP] 05 February 2010 (has links) (PDF)
Made available in DSpace on 2014-06-11T19:27:45Z (GMT). No. of bitstreams: 0 Previous issue date: 2010-02-05Bitstream added on 2014-06-13T20:17:06Z : No. of bitstreams: 1 chiba_fy_me_araca.pdf: 754628 bytes, checksum: 34bc263d9874acda6daffee82f61b8b5 (MD5) / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) / Nos últimos anos, tem havido uma redução acentuada nos índices de cárie dentária em diversas regiões do mundo, fato que tem sido atribuído à exposição às substâncias fluoretadas, principalmente na forma de água de abastecimento público e dentifrício. Simultaneamente, nota-se a ocorrência do aumento da prevalência de fluorose dentária. Estudo realizado em 25 pacientes (15 a 30 anos de idade) com fluorose endêmica mostrou que 40% destes tinham a tolerância à glicose prejudicada, porém esta anomalia foi revertida com a remoção do excesso do flúor na água consumida. O NaF ocasiona inibição da glicólise, diminuição da secreção de insulina e hiperglicemia. Muitas destas respostas sugerem que o NaF pode ocasionar resistência à insulina. Se isto for confirmado, é recomendável diminuir a concentração de fluoreto nos dentifrícios utilizados principalmente por crianças diabéticas, pois a ingestão de pasta dental contendo flúor pode levar à piora na situação de saúde destas crianças. Sabendo-se que o fluoreto pode alterar o metabolismo de carboidratos, tornou-se fundamental caracterizar o efeito do NaF sobre: 1) a sensibilidade à insulina; 2) o grau de fosforilação em tirosina do substrato do receptor de insulina - pp185 (IRS-1/IRS-2); 3) a fluoremia, glicemia e insulinemia. Para tanto, foram utilizados ratos Wistar machos (1 mês de idade) castrados. Após 30 dias da castração, os animais foram divididos aleatoriamente em dois grupos: 1) grupo controle (CN), o qual foi submetido ao tratamento sem NaF, mas com uma solução de NaCl (9,54 mg/kg p.c.) que contém a mesma quantidade de sódio em relação à do grupo fluoreto de sódio; 2) grupo NaF (FN) que será submetido ao tratamento com NaF (4,0 mg de flúor/kg p.c.) na água de beber e na ração durante 42... / Over the last years, there has been a significant reduction in the incidence of dental caries in several regions of the world. This has been attributed to ingestion of fluoridated products, especially in the form of public water supplies and toothpaste. Simultaneously, there has been an increase in the prevalence of dental fluorosis. A study conducted in 25 patients (15 to 30 years of age) with endemic fluorosis showed that 40% of these had to impaired glucose tolerance, but this anomaly was reversed by removing the excess of fluoride from drinking water. NaF causes glycolysis inhibition, decrease on insulin secretion and hyperglycemia. These responses suggest that NaF can cause insulin resistance. If this is confirmed, the use of dentifrices with lower fluoride content is recommended, especially for diabetic children, for whom excessive F consumption may lead to worsening the condition of these children’s health. Knowing that F can interfere with carbohydrate metabolism, we felt it was important and fundamental to undertake a study to examine the chronic effect of NaF on: 1) insulin sensitivity; 2) pp185 (IRS-1/IRS-2) tyrosine phosphorylation in gastrocnemius muscle and liver of rats; 3) fluoremia, glycemia and insulinemia. For this study, castrated Wistar male rats (1 month of age) were used. Thirty days after castration, the animals were randomly divided in two groups: 1) control group (CN) which was subjected to treatment without NaF, but with a solution of NaCl (9.54 mg / kg bw) which contains the same amount of sodium in relation to the group NaF; 2) group NaF (FN) that was submitted to treatment with NaF administered in the drinking water and F contained in food pellets (F total inferred: 4.0 mg F / Kg bw / day in the form of NaF) during 42 days. After 6 weeks, the following experiments were conducted: 1) assessment... (Complete abstract, click electronic address below)
5

Avaliação da etapa inicial do sinal insulínico em tecido muscular e hepático de ratos tratados cronicamente com NaF /

Chiba, Fernando Yamamoto. January 2010 (has links)
Orientador: Doris Hissako Sumida / Banca: Cléa Adas Saliba Garbin / Banca: Marília Afonso Rabelo Buzalaf / Resumo: Nos últimos anos, tem havido uma redução acentuada nos índices de cárie dentária em diversas regiões do mundo, fato que tem sido atribuído à exposição às substâncias fluoretadas, principalmente na forma de água de abastecimento público e dentifrício. Simultaneamente, nota-se a ocorrência do aumento da prevalência de fluorose dentária. Estudo realizado em 25 pacientes (15 a 30 anos de idade) com fluorose endêmica mostrou que 40% destes tinham a tolerância à glicose prejudicada, porém esta anomalia foi revertida com a remoção do excesso do flúor na água consumida. O NaF ocasiona inibição da glicólise, diminuição da secreção de insulina e hiperglicemia. Muitas destas respostas sugerem que o NaF pode ocasionar resistência à insulina. Se isto for confirmado, é recomendável diminuir a concentração de fluoreto nos dentifrícios utilizados principalmente por crianças diabéticas, pois a ingestão de pasta dental contendo flúor pode levar à piora na situação de saúde destas crianças. Sabendo-se que o fluoreto pode alterar o metabolismo de carboidratos, tornou-se fundamental caracterizar o efeito do NaF sobre: 1) a sensibilidade à insulina; 2) o grau de fosforilação em tirosina do substrato do receptor de insulina - pp185 (IRS-1/IRS-2); 3) a fluoremia, glicemia e insulinemia. Para tanto, foram utilizados ratos Wistar machos (1 mês de idade) castrados. Após 30 dias da castração, os animais foram divididos aleatoriamente em dois grupos: 1) grupo controle (CN), o qual foi submetido ao tratamento sem NaF, mas com uma solução de NaCl (9,54 mg/kg p.c.) que contém a mesma quantidade de sódio em relação à do grupo fluoreto de sódio; 2) grupo NaF (FN) que será submetido ao tratamento com NaF (4,0 mg de flúor/kg p.c.) na água de beber e na ração durante 42... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Over the last years, there has been a significant reduction in the incidence of dental caries in several regions of the world. This has been attributed to ingestion of fluoridated products, especially in the form of public water supplies and toothpaste. Simultaneously, there has been an increase in the prevalence of dental fluorosis. A study conducted in 25 patients (15 to 30 years of age) with endemic fluorosis showed that 40% of these had to impaired glucose tolerance, but this anomaly was reversed by removing the excess of fluoride from drinking water. NaF causes glycolysis inhibition, decrease on insulin secretion and hyperglycemia. These responses suggest that NaF can cause insulin resistance. If this is confirmed, the use of dentifrices with lower fluoride content is recommended, especially for diabetic children, for whom excessive F consumption may lead to worsening the condition of these children's health. Knowing that F can interfere with carbohydrate metabolism, we felt it was important and fundamental to undertake a study to examine the chronic effect of NaF on: 1) insulin sensitivity; 2) pp185 (IRS-1/IRS-2) tyrosine phosphorylation in gastrocnemius muscle and liver of rats; 3) fluoremia, glycemia and insulinemia. For this study, castrated Wistar male rats (1 month of age) were used. Thirty days after castration, the animals were randomly divided in two groups: 1) control group (CN) which was subjected to treatment without NaF, but with a solution of NaCl (9.54 mg / kg bw) which contains the same amount of sodium in relation to the group NaF; 2) group NaF (FN) that was submitted to treatment with NaF administered in the drinking water and F contained in food pellets (F total inferred: 4.0 mg F / Kg bw / day in the form of NaF) during 42 days. After 6 weeks, the following experiments were conducted: 1) assessment... (Complete abstract, click electronic address below) / Mestre
6

Localization of Insulin Receptor Substrate-2 in Breast Cancer: A Dissertation

Clark, Jennifer L. 29 March 2012 (has links)
The insulin-like growth factor-1 receptor (IGF-1R) and many of its downstream signaling components have long been implicated in tumor progression and resistance to therapy. The insulin receptor substrate-1 (IRS-1) and IRS-2 adaptor proteins are two of the major downstream signaling intermediates of the IGF-1R. Despite their considerable homology, previous work in our lab and others has shown that IRS-1 and IRS-2 play divergent roles in breast cancer cells. Signaling through IRS-1 promotes cell proliferation, whereas signaling through IRS-2 promotes cell motility and invasion, as well as glycolysis. Moreover, using a mouse model of mammary tumorigenesis, our lab demonstrated that IRS-2 acts as a positive regulator of metastasis, while IRS-1 cannot compensate for this function. The focus of my thesis research is to understand how IRS-2, but not IRS-1, promotes breast carcinoma cell invasion and metabolism to support metastasis. In preliminary studies, I have found that IRS-1 and IRS-2 exhibit different expression patterns in both cell lines and human tumors with correlations to patient survival, which provides a potential mechanism for their distinct functions. The localization of IRS-1 and IRS-2 within separate intracellular compartments would determine their access to downstream effectors and substrates, and this would result in unique cellular outcomes. Specifically, I have observed that IRS-2, but not IRS-1, co-localizes with microtubules in breast carcinoma cell lines with implications for signaling through AKT and mTORC2. The goal of this research is to determine how the localization of IRS-2 contributes to its regulation of breast cancer progression and response to therapy and how this information could be used to better predict patient outcomes.
7

Insulin Receptor Substrate-2 (IRS-2): A Novel Hypoxia-Responsive Gene in Breast Cancer: A Dissertation

Mardilovich, Katerina 11 May 2011 (has links)
Breast cancer is the most common malignancy among women in the U.S. While many successful treatments exist for primary breast cancer, very few are available for patients with metastatic disease. The purpose of this study was to understand the role of Insulin Receptor Subtrate-2 (IRS-2) in breast cancer metastasis. IRS-2 belongs to the IRS family of cytoplasmic adaptor proteins that mediate signaling from cell surface receptors, many of which have been implicated in cancer. Although the IRS proteins are highly homologous in structure and have some complementary functions, growing evidence supports that the IRS proteins have unique roles in cancer. IRS-1 has been shown to promote tumor cell proliferation, while IRS-2 has been positively associated with cancer cell invasion, glycolysis and tumor metastasis. In the current work, we identified IRS-2 as a novel hypoxia-responsive gene in breast carcinoma cells. In contrast, IRS-1 expression does not increase in response to hypoxia, supporting the notion of their non-overlapping functions. Hypoxia promotes the adaptation and resistance of cancer cells to chemo- and radiation therapy, and also promotes tumor cell survival, invasion and metastasis by selecting for aggressive tumor cells that can survive under stressful low oxygen conditions. We have shown that IRS-2 upregulation in response to hypoxia promotes Akt signaling and tumor cell viability and invasion. We identified a cell context-dependent role for Hypoxia Inducible Factor (HIF) in the regulation of IRS-2 expression in hypoxia, with HIF-2 playing a more dominant role than HIF-1. We also demonstrate that binding of Snail, a regulator of the EMT, to the IRS-2 promoter keeps the chromatin in an open conformation that is permissive for HIF-dependent transcription of IRS-2 in hypoxia. IRS-2 is not upregulated by hypoxia in well-differentiated epithelial-like carcinoma cells that do not express Snail, implicating IRS-2 gene expression as part of the EMT programming. In summary, we have identified an endogenous mechanism by which cancer cells can shift the balance of IRS-1 and IRS-2 to favor IRS-2 expression and function, which promotes survival, invasion, and ultimately metastasis. Understanding the mechanism of IRS-2 regulation by hypoxia may reveal new therapeutic targets for metastatic breast cancer.

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