• Refine Query
  • Source
  • Publication year
  • to
  • Language
  • 2
  • 1
  • Tagged with
  • 4
  • 4
  • 4
  • 2
  • 2
  • 2
  • 2
  • 2
  • 2
  • 2
  • 2
  • 2
  • 2
  • 1
  • 1
  • 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

Function and regulation of myc-family bHLHZip transcription factors during the animal and plant cell cycle /

Su, Yingtao, January 2008 (has links) (PDF)
Diss. (sammanfattning) Uppsala : Sveriges lantbruksuniv., 2008. / Härtill 4 uppsatser.
2

Análise da expressão do fator de transcrição TCF21/POD-1 e de genes do ciclo celular em tumores adrenocorticais humanos. / Analysis of TCF21/POD-1 transcriptor factor and cycle cells genes expression in adult adrenocortical tumors.

Passaia, Barbara dos Santos 31 May 2016 (has links)
As massas adrenocorticais são majoritariamente (70-80%) adenomas adrenocorticais (ACA). Os carcinomas adrenocorticais (ACC) são mais raros e de prognóstico restrito, com incidência de 1-2 casos por milhão, com alta taxa de reincidência (70-80%). Apesar dos tumores adrenocorticais (ACT) serem raros, no Brasil a incidência desses tumores em crianças é cerca de 10 vezes superior ao do restante do mundo, devido a uma mutação do gene TP53. Atualmente, o diagnóstico de massas adrenocorticais é realizado através dos critérios de Weiss, que possuem limitações, e por isso é intensa a busca de novos marcadores moleculares que facilite o diagnóstico de ACTs. POD-1/ TCF21 é um fator de transcrição do tipo helix-loop-helix básica (bHLH) expresso nos sítios de interação mesênquima-epitélio durante o desenvolvimento embrionário. Em ACTs, POD-1 regula a expressão endógena de SF-1 através da ligação na sequencia E-box da região promotora de SF-1, e nesses tumores parece estar relacionado negativamente com genes reguladores do ciclo celular, como BUB1B. BUB1B é um gene que codifica uma quinase com funções importantes durante o checkpoint mitótico. A expressão de BUB1B é considerada fator de prognóstico em diferentes tipos de tumores, inclusive em ACTs humanos, nos quais a expressão combinada de BUB1B e PINK1 (ΔCtBUB1B - ΔCtPINK1) mostrou-se um bom marcador de sobrevida em pacientes com ACC. PINK1, quinase 1 induzida por PTEN, é regulada principalmente pela mitocôndria, e em ACTs sua expressão está reduzida em ACC mais agressivos. Temos como hipótese que a expressão de POD-1 pode ter valor diferencial no diagnóstico de massas adrenocorticais, e que a análise da expressão combinada de POD-1, BUB1B e PINK1 pode ter valor diferencial para prognóstico de pacientes com ACT. Nesse trabalho foram analisados, por reação de qPCR com sondas Taqman, o cDNA obtido de 130 amostras de tumores: 79 adultos (44 ACAs e 35 ACCs), 35 crianças com menos de 5 anos de idade (27 ACAs e 8 ACCs) e 16 crianças de 5 a 18 anos de idade (6 ACAs e 10 ACCs). Nossos resultados mostram que POD-1 e BUB1B tem valor diferencial em ACT adulto e que a expressão combinada de POD-1 e BUB1B pode ser um marcador de prognóstico em pacientes com carcinoma adulto. Enquanto que, a expressão combinada de POD-1 e SF-1 pode ter valor de diagnóstico em pacientes pediátricos com menos de 5 anos. Em resumo, concluímos que estudos experimentais devem ser realizados para comprovar a relação entre os genes estudados, para que os resultados sejam sólidos o suficiente para serem utilizados no diagnóstico e prognóstico dos tumores adrenocorticais. / The adrenocortical masses are mostly (70-80%) adrenocortical adenomas (ACA). Adrenocortical carcinomas (ACC) are scarce and have limited prognosis, with an incidence of 1-2 cases per million and high recurrence rate (70-80%). Despite adrenocortical tumors (ACT) are rare in Brazil the incidence of these tumors in children is about 10 times higher than the rest of the world, due to a mutation of the TP53 gene. Currently, the diagnosis of adrenocortical mass is carried through Weiss criteria that have limitations, so it is intensive the search for new molecular markers that facilitate the diagnostic of ACTs. TCF21/POD-1 is a transcription factor helix-loop-helix type expressed in mesenchymal-epithelial sites of interaction during embryonic development. In ACTs, POD-1 regulates the expression of endogenous SF-1 through binding the E-box sequence of SF-1 promoter region, and seems to be negatively relates with cell cycle regulatory genes such as BUB1B. BUB1B is a gene encoding a kinase-with important function during mitotic checkpoint. The expression of BUB1B is considered a prognostic factor in different types of tumors, including ACTs. Combined expression of BUB1B and PINK1 (ΔCtBUB1B - ΔCtPINK1) has been shown to be a good marker of survival in adults with ACC, whereas the PINK1 expression is reduced in the most aggressive ACC. We hypothesized that the POD-1 expression may have differential value in the diagnosis of adrenocortical masses, and that the analysis of the combined expression of POD-1, BUB1B and PINK1 may have differential value for the prognosis of patients with ACT. In this work were analyzed by PCRq Taqman probes the cDNA obtained from 130 tumor samples: 79 adults (44 ACAs and 35 ACCs), 35 children under 5 years old (27 ACAs and 8 ACCs) and 16 children 5-18 years of age (6 ACAs and 10 ACCs). Our results show that POD-1 and BUB1B has differential value in adult ACT, and the combined expression of POD-1 and BUB1B may have a prognostic value in patients with adult carcinoma. In addition, the combined expression of POD-1 and SF-1 might have diagnostic value in pediatric patients younger than 5 years. In summary, we conclude that experimental studies should be conducted to confirm the relationship between the genes studied, so that the results are solid enough to be used in the diagnosis and prognosis of adrenocortical tumors.
3

Análise da expressão do fator de transcrição TCF21/POD-1 e de genes do ciclo celular em tumores adrenocorticais humanos. / Analysis of TCF21/POD-1 transcriptor factor and cycle cells genes expression in adult adrenocortical tumors.

Barbara dos Santos Passaia 31 May 2016 (has links)
As massas adrenocorticais são majoritariamente (70-80%) adenomas adrenocorticais (ACA). Os carcinomas adrenocorticais (ACC) são mais raros e de prognóstico restrito, com incidência de 1-2 casos por milhão, com alta taxa de reincidência (70-80%). Apesar dos tumores adrenocorticais (ACT) serem raros, no Brasil a incidência desses tumores em crianças é cerca de 10 vezes superior ao do restante do mundo, devido a uma mutação do gene TP53. Atualmente, o diagnóstico de massas adrenocorticais é realizado através dos critérios de Weiss, que possuem limitações, e por isso é intensa a busca de novos marcadores moleculares que facilite o diagnóstico de ACTs. POD-1/ TCF21 é um fator de transcrição do tipo helix-loop-helix básica (bHLH) expresso nos sítios de interação mesênquima-epitélio durante o desenvolvimento embrionário. Em ACTs, POD-1 regula a expressão endógena de SF-1 através da ligação na sequencia E-box da região promotora de SF-1, e nesses tumores parece estar relacionado negativamente com genes reguladores do ciclo celular, como BUB1B. BUB1B é um gene que codifica uma quinase com funções importantes durante o checkpoint mitótico. A expressão de BUB1B é considerada fator de prognóstico em diferentes tipos de tumores, inclusive em ACTs humanos, nos quais a expressão combinada de BUB1B e PINK1 (ΔCtBUB1B - ΔCtPINK1) mostrou-se um bom marcador de sobrevida em pacientes com ACC. PINK1, quinase 1 induzida por PTEN, é regulada principalmente pela mitocôndria, e em ACTs sua expressão está reduzida em ACC mais agressivos. Temos como hipótese que a expressão de POD-1 pode ter valor diferencial no diagnóstico de massas adrenocorticais, e que a análise da expressão combinada de POD-1, BUB1B e PINK1 pode ter valor diferencial para prognóstico de pacientes com ACT. Nesse trabalho foram analisados, por reação de qPCR com sondas Taqman, o cDNA obtido de 130 amostras de tumores: 79 adultos (44 ACAs e 35 ACCs), 35 crianças com menos de 5 anos de idade (27 ACAs e 8 ACCs) e 16 crianças de 5 a 18 anos de idade (6 ACAs e 10 ACCs). Nossos resultados mostram que POD-1 e BUB1B tem valor diferencial em ACT adulto e que a expressão combinada de POD-1 e BUB1B pode ser um marcador de prognóstico em pacientes com carcinoma adulto. Enquanto que, a expressão combinada de POD-1 e SF-1 pode ter valor de diagnóstico em pacientes pediátricos com menos de 5 anos. Em resumo, concluímos que estudos experimentais devem ser realizados para comprovar a relação entre os genes estudados, para que os resultados sejam sólidos o suficiente para serem utilizados no diagnóstico e prognóstico dos tumores adrenocorticais. / The adrenocortical masses are mostly (70-80%) adrenocortical adenomas (ACA). Adrenocortical carcinomas (ACC) are scarce and have limited prognosis, with an incidence of 1-2 cases per million and high recurrence rate (70-80%). Despite adrenocortical tumors (ACT) are rare in Brazil the incidence of these tumors in children is about 10 times higher than the rest of the world, due to a mutation of the TP53 gene. Currently, the diagnosis of adrenocortical mass is carried through Weiss criteria that have limitations, so it is intensive the search for new molecular markers that facilitate the diagnostic of ACTs. TCF21/POD-1 is a transcription factor helix-loop-helix type expressed in mesenchymal-epithelial sites of interaction during embryonic development. In ACTs, POD-1 regulates the expression of endogenous SF-1 through binding the E-box sequence of SF-1 promoter region, and seems to be negatively relates with cell cycle regulatory genes such as BUB1B. BUB1B is a gene encoding a kinase-with important function during mitotic checkpoint. The expression of BUB1B is considered a prognostic factor in different types of tumors, including ACTs. Combined expression of BUB1B and PINK1 (ΔCtBUB1B - ΔCtPINK1) has been shown to be a good marker of survival in adults with ACC, whereas the PINK1 expression is reduced in the most aggressive ACC. We hypothesized that the POD-1 expression may have differential value in the diagnosis of adrenocortical masses, and that the analysis of the combined expression of POD-1, BUB1B and PINK1 may have differential value for the prognosis of patients with ACT. In this work were analyzed by PCRq Taqman probes the cDNA obtained from 130 tumor samples: 79 adults (44 ACAs and 35 ACCs), 35 children under 5 years old (27 ACAs and 8 ACCs) and 16 children 5-18 years of age (6 ACAs and 10 ACCs). Our results show that POD-1 and BUB1B has differential value in adult ACT, and the combined expression of POD-1 and BUB1B may have a prognostic value in patients with adult carcinoma. In addition, the combined expression of POD-1 and SF-1 might have diagnostic value in pediatric patients younger than 5 years. In summary, we conclude that experimental studies should be conducted to confirm the relationship between the genes studied, so that the results are solid enough to be used in the diagnosis and prognosis of adrenocortical tumors.
4

Novel Mechanisms and Approaches in the Study of Neurodegeneration and Neuroprotection. A Review

Kostrzewa, Richard M., Segura-Aguilar, Juan 01 December 2003 (has links)
Cellular mechanisms involved in neurodegeneration and neuroprotection are continuing to be explored, and this paper focuses on some novel discoveries that give further insight into these processes. Oligodendrocytes and activated astroglia are likely generators of the pro-inflammatory cytokines, such as the tumor necrosis factor family and interleukin family, and these glial support cells express adhesion receptors (e.g., VCAM) and release intercellular adhesion molecules (ICAM) that have a major role in neuronal apoptosis. Even brief exposure to some substances, in ontogeny and sometimes in adulthood, can have lasting effects on behaviors because of their prominent toxicity (e.g., NMDA receptor antagonists) or because they sensitize receptors (e.g., dopamine D2 agonists), possibly permanently, and thereby alter behavior for the lifespan. Cell cycle genes which may be derived from microglia, are the most-recent entry into the neuroprotection schema. Neuroprotection afforded by some common substances (e.g., melatonin) and uncommon substances [e.g., nicotine, green tea polyphenol (-)-epigallocatechin-3-gallate (EGCG), trolox], ordinarily thought to be simple radical scavengers, now are thought to invoke previously unsuspected cellular mechanisms in the process of neuroprotection. Although Alzheimer's disease (AD) has features of a continuous spectrum of neural and functional decline, in vivo PET imaging and and functional magnetic resonance imaging, indicate that AD can be staged into an early phase treatable by inhibitors of β and γ secretase; and a late phase which may be more amenable to treatment by drugs that prevent or reverse tau phosphorylation. Neural transplantation, thought to be the last hope for neurally injured patients (e.g., Parkinsonians), may be displaced by non-neural tissue transplants (e.g., human umbilical cord blood; Sertoli cells) which seem to provide similar neurotrophic support and improved behavior-without posing the major ethical dilemma of removing tissue from aborted fetuses. The objective of this paper is to invite added research into the newly discovered (or postulated) novel mechanisms; and to stimulate discovery of additional mechanisms attending neurodegeneration and neuroprotection.

Page generated in 0.0705 seconds