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151	Expressão de receptores androgenicos no lobulo ventral da prostata do gerbilo da Mongolia / Androgen receptors expression in the Mongolian gerbil ventral prostate Cordeiro, Renato Simões 30 July 2007 (has links) Orientador: Sebastião Roberto Taboga / Tese (doutorado) - Universidade Estadual de Campinas, Instituto de Biologia / Made available in DSpace on 2018-08-08T20:16:45Z (GMT). No. of bitstreams: 1 Cordeiro_RenatoSimoes_D.pdf: 4151474 bytes, checksum: 0ee256bf17ee9f60a582294e99e12f0c (MD5) Previous issue date: 2007 / Resumo: O crescimento normal, a diferenciação e a manutenção da integridade morfofuncional da glândula prostática são dependentes das interações de concentrações constantes de andrógenos com seus receptores. A necessidade de se estudar esta glândula em resposta aos hormônios e o efeito do bloqueio destes, deve-se ao fato da próstata humana ser o sítio de um grande número de doenças relacionadas à idade, sendo que as de maior importância clínica são o câncer prostático e a hiperplasia prostática benigna, as quais podem ser tratadas por estratégias de remoção de andrógenos. Este estudo teve por objetivo a análise imuno-histoquímica do grau de expressão do receptor androgênico (RA) no lóbulo ventral prostático do gerbilo após terapias de bloqueios androgênicos. Setenta e cinco gerbilos machos foram distribuídos, aleatoriamente, em 3 grupos de 25 animais, cada grupo representando uma fase do desenvolvimento pós-natal: jovem, adulto e senil. Em cada fase foi realizada uma análise morfológica e estereológica dos compartimentos prostáticos, bem como a análise imuno-histoquímica da expressão do RA. Além disso, estabeleceu-se a dosagem hormonal das concentrações séricas de testosterona, como método para verificar a relação da quantidade desse andrógeno com a expressão dos RA. Os resultados demonstraram haver um padrão heterogêneo de distribuição dos RA no lóbulo ventral ao longo do desenvolvimento pós-natal, em que quanto mais jovem for o animal maior a interação de andrógenos estimulando a expressão de RA nos compartimentos prostáticos. As terapias de bloqueios androgênicos diminuíram a expressão de RA no lóbulo ventral e a reposição androgênica após esses bloqueios não apresentou o mesmo grau de intensidade de expressão de RA próximo às condições fisiológicas normais. A regulação e a distribuição do RA nos tecidos prostáticos do gerbilo são mecanismos complexos e que, provavelmente, são geneticamente regulados por andrógenos antes do nascimento ou por outros fatores ainda desconhecidos. O gerbilo parece ser um modelo valioso na tentativa de melhorar o conhecimento do comportamento morfofisiológico e patológico dessa importante glândula em humanos ao longo do envelhecimento e da formulação de novas idéias de terapias de combate ao câncer de próstata / Abstract: The normal growth, differentiation and maintenance of the morphofunctional integrity of the prostate gland are dependent on the interaction of constant levels of androgens with their receptors. The need to study the responses to hormones under several conditions and the effect of their blockage is due to the fact that the human prostate is the site of a great number of age-related diseases, and the ones with a major medical importance are prostate cancer and benign prostatic hyperplasia, which can both be treated with androgen suppression. The aim of this study was to analyze immunohistochemical degree of expression of androgen receptor (AR) of the ventral lobe of the gerbil prostate during different phases of the postnatal development employing differents treatments for androgen blocking. Seventy-five male gerbils were distributed, randomly, into 3 groups of 25 animals each, where each group corresponded to one phase of postnatal development: young, adult and aged phase. In each phase, it was possible to morphologically and stereologically analyze the compartments of prostatic ventral lobe, as well as to immunohistochemically analyze the degree of expression of androgen receptor. In addition, it was possible to establish the hormonal dosage of serum testosterone concentrations given the comparative approach of the expression of androgen receptors. There is a heterogeneous pattern of AR distribution in the prostatic ventral lobe throughout postnatal development, in which the younger animal is the higher, the interaction of circulating androgens that stimulate the AR expression in the compartments prostatics. The androgen blockage therapies decreased AR expression in the ventral lobe, but the androgen reposition after these blockages was not showed the same the degree of expression of androgen receptor near normal physiological conditions. The regulation and distribution of AR along the gerbil prostatic tissues are complex mechanisms that are likely to be genetically regulated by androgens prenatally or by other factors that are still unknown. The gerbil seems to be a valuable model in the attempt to improve the understanding of the morphophysiological and pathological behavior of this important gland in humans throughout aging and to stimulate new therapeutic ideas to fight prostate cancer / Doutorado / Biologia Celular / Doutor em Biologia Celular e Estrutural Prostata Receptores de andrógenos Androgenos - Antagonistas Imuno-histoquímica Prostate Androgen receptors Antiandrogens Immunohistochemical
152	Analise molecular do gene do receptor de androgenos em pacientes 46, XY com ambiguidade genital e produção normal de testosterona / Molecular analysis of the androgen receptor gene in patient 46, XY presenting genital ambiguity and normal testosterone production Petroli, Reginaldo José, 1980- 15 August 2018 (has links) Orientador: Maricilda Palandi de Mello / Dissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Biologia / Made available in DSpace on 2018-08-15T17:10:17Z (GMT). No. of bitstreams: 1 Petroli_ReginaldoJose_M.pdf: 2303670 bytes, checksum: 1836c8a6df94a76ee177d830781dc293 (MD5) Previous issue date: 2010 / Resumo: Considera-se que insensibilidade androgênica seja a causa mais freqüente dos distúrbios da diferenciação do sexo em pacientes com cariótipo 46,XY. Trata-se de uma anomalia recessiva ligada ao cromossomo X, que pode se manifestar de forma branda, parcial ou completa, com um amplo espectro de variação fenotípica. O gene do receptor de andrógenos (AR) está localizado no cromossomo X, na região Xq11-12, sendo organizado em oito exons separados por introns de até 26 kb. Sua região codificante apresenta aproximadamente 2.757 pares de bases traduzindo uma proteína de 919 aminoácidos, cujo peso molecular é de aproximadamente 110 kDa. A proteína AR apresenta três domínios funcionais: domínio de regulação transcricional (amino-terminal), domínio de ligação ao DNA que contém dois dedos de zinco (zinc finger) e domínio de ligação ao esteróide (carboxi-terminal). O domínio amino-terminal possui repetições dos aminoácidos glutamina e glicina cujos números podem variar dentro da população normal. O domínio de ligação ao esteróide (carboxi-terminal), apresenta o maior número de mutações, cerca de 55% das descritas neste gene. Entre o domínio de ligação ao DNA e o domínio de ligação ao esteróide encontra-se a região hinge que contém um sinal responsável pela localização nuclear necessária para a translocação do complexo andrógeno/receptor do citoplasma para o núcleo da célula. Pacientes com cariótipo 46,XY e diagnóstico de insensibilidade androgênica geralmente apresentam fenótipo feminino ou ambigüidade genital, porém a produção de testosterona é normal. Nestes pacientes a investigação de mutações no gene do receptor de andrógeno é indicada para a identificação da alteração molecular relacionada à doença. Desta maneira, o presente estudo teve como objetivo a caracterização das alterações moleculares do gene AR, através da análise de seus oito exons e junções exons-introns por reação da cadeia da polimerase (PCR) seguida de sequenciamento dos fragmentos amplificados. Das 47 famílias que compõem a casuística deste trabalho, 14 apresentaram mutações no gene, sendo uma relacionada ao fenótipo brando da insensibilidade androgênica (p.P694S), sete relacionadas ao fenótipo parcial da insensibilidade androgênica (p.Q58L, p.A596T, p.S597R, p.M742V, p.Q798E, p.L830F e p.A896V) e seis relacionadas ao fenótipo completo da insensibilidade androgênica (p.R774H, p.P766S, p.C806F, p.R832Term, p.R855H e p.V866M). Uma paciente apresentou duas alterações, ambas no exon 6 deste gene. Quatro mutações estão sendo descritas pela primeira vez neste trabalho em pacientes com insensibilidade androgênica / Abstract: The androgen insensitivity syndrome (AIS) is considered the most frequent disorders of sex differentiation in patients with 46,XY karyotype. It is a recessive X linked disorder, which manifests as mild, partial or complete forms, with a broad spectrum of phenotypic variation. The androgen receptor gene (AR) is located on the X chromosome within Xq11-12 region. It is organized in eight exons separated by introns up to 26 kb in length. Its coding region comprises approximately 2,757 base pairs translating a protein of 919 amino acids, whose molecular weight is approximately 110 kDa. The AR protein has three functional domains: the transcriptional regulatory domain, the DNA binding domain which contains two zinc fingers and the steroid binding domain in the carboxy-terminal region. The amino-terminal domain presents repeats of glutamine and glycine whose numbers of residues vary within the normal population. The steroid-binding domain presents the highest number of mutations, around 55% of the mutations described in this gene are located in this region. Between the DNA-binding domain and the steroid-binding domain there is a hinge region that contains a signal responsible for nuclear localization required for translocation of the complex androgen/receptor from the cytoplasm to the cell nucleus. Patients with 46,XY karyotype and androgen insensitivity diagnosis usually have female or ambiguous genitalia, but normal testosterone production. In these patients the investigation of androgen receptor gene mutations is indicated to identify the molecular changes related with AIS. Therefore, the aim of this study was to characterize molecular alterations in the AR gene, by analysis of the eight exons and introns-exons junctions by polymerase chain reaction (PCR) followed by sequencing the amplified fragments. Fourteen out of 46 families comprised in this study had mutations identified. One mutation corresponded to the mild phenotype of androgen insensitivity (p.P694S), seven were related to the partial androgen insensitivity phenotype (p.Q58L, p.A596T, P. S597R, p.M742V, p.Q798E, p.L830F and p.A896V), and six were associated to the complete androgen insensitivity phenotype (p.R774H, p.P766S, p.C806F, p.R832Term, p.R855H and p.V866M). One patient presented two mutations, both located in exon 6 of the gene. Four mutations were described for the first time in this research in patients with androgen insensitivity / Mestrado / Genetica Animal e Evolução / Mestre em Genética e Biologia Molecular Gene AR Receptores de andrógenos Síndrome de resistência a andrógenos AR gene Androgens receptors Androgen-insensitivity syndrome
153	Imprinting estrogenico : efeito sobre a expressão do receptor de androgeno no hipotalamo de ratos Wistar / Effects of estrogenic imprinting on the androgen receptor expression in the hypothalamus of Wistar rats Oliveira, Elusa Cristina de 04 September 2008 (has links) Orientador: Hernandes Faustino de Carvalho / Dissertação (mestrado) - Universidade Estadual de Campinas, Instituto de Biologia / Made available in DSpace on 2018-08-11T07:07:28Z (GMT). No. of bitstreams: 1 Oliveira_ElusaCristinade_M.pdf: 10251411 bytes, checksum: b1a5d2634c9831ce84cdf0a70561fdc8 (MD5) Previous issue date: 2008 / Resumo: Em ratos machos, a completa função reprodutiva é criticamente dependente da adequada ação do estrógeno nos diferentes níveis do eixo hipotálamo-hipófise-gônadas. A administração de altas doses de estrógeno durante o período de diferenciação sexual resulta em diversas alterações no sistema reprodutor masculino. De forma geral, os estrógenos têm efeito anti-androgênico atuando no eixo hipotálamo-hipófise-testículos e, assim, reduzindo a produção de testosterona pelos testículos. A administração de estrógeno nos períodos. críticos do desenvolvimento promove um mecanismo conhecido como imprinting estrogênico. Este fenômeno é extremamente importante, pois pode ser acionado pela exposição do recém-nascido a várias substâncias com caráter estrogênico, e não somente ao estrógeno. Um dos efeitos do imprinting estrogênico causado por altas doses de estrógeno é a regulação negativa da expressão de receptores de andrógenos (ARs). na próstata e reduzida resposta a aplicações de andrógenos, o que parece alterar padrões de comportamento em machos. Diante disso, este trabalho investigou os aspectos relacionados aos mecanismos gerais envolvidos no imprinting estrogênico, com o propósito de analisar a participação do estrógeno e a sua influência sobre os ARs no hipotálamo de ratos Wistar. Para tanto, ratos machos foram tratados no período neonatal inicial com três doses de 15 mg/kg de 17p-estradiol (E2) e comparados com ratos controle (tratados apenas com óleo de milho) e com fêmeas que não receberam nenhum tratamento farmacológico, e os efeitos foram observados na idade adulta. Foram verificados os padrões de distribuição do AR por imunoistoquímica, o conteúdo total de AR por Western blotting e do correspondente RNAm por RT-PCR no hipotálamo dos animais submetidos à estrogenização neonatal. A estrogenização promoveu diminuição no conteúdo total de AR e na expressão do RNAm correspondente, e modificações no padrão de distribuição do AR nos núcleos ventromedial, pré-óptico medial anterior, paraventricular e área pré-óptica, aproximando-se do padrão apresentado por fêmeas. Portanto, esses dados indicam que o estrógeno é capaz de promover imprinting neonatal no hipotálamo e alterar a expressão do AR, o que possivelmente pode afetar o comportamento sexual desses animais / Abstract: In male rats, complete reproductive function is critically dependent on adequate estrogen action at different levels of the hypothalamic-pituitary-gonadal axis. The administration of high doses during the period of sexual differentiation results in irreversible alterati ns in the male reproductive system. In brief, the estrogens have anti-androgenic effects t. ey act in the hypothalamus-pituitary-testes axis, reducing the testosterone production by the testes. The administration of estrogen in critical periods of development promotes a mechanism known as estrogen imprinting. This phenomenon is extremely important, because it can be started by the exposure of the neonate to several estrogen-like substances with estrogen characteristics, and not only to estrogen. One of the estrogenic imprinting effects caused by high doses of estrogen is the negative regulation of the expression of androgen receptors (ARs) in the prostate and reduced responses to androgen exposure that seems to alter the male behavior. This study investigated the participation of estrogen and it influence on the ARs in the hypothalamus of Wistar rats afier estrogen imprinting. For this, male rats were treated in the early neonatal period with 17pestradiol (E2) three doses of 15mg/kg and compared with control rats (only treated with com oil) and with not treated females, and the effects were analyzed in the adulthood. The AR distribution pattem was analyzed by immunohistochemistry, the total content of the AR by Westem blotting and it's mRNA by RT-PCR in the hypothalamus oftreated animaIs. The neonatal estrogenization promoted decrease of expression oftne AR and its mRNA. Also revealed that the AR distribution, pattem at the ventromedial, anterior medial preoptic and paraventricular nuclei and preoptic area were altered and with a pattem close to not treated females. Therefore, our data indicate that estrogen is able to induce estrogen imprint in the hypothalamus and to alter the AR expression and possibly affecting the sexual behavior / Mestrado / Biologia Celular / Mestre em Biologia Celular e Estrutural Diferenciação do sexo Hipotálamo Imprinting estrogenico Receptores de andrógenos Sexual differentiation Hypothalamus Estrogen imprinting Androgen receptor
154	Bases moleculares da diminuição da capacidade funcional do receptor de androgênio mutado estudadas por simulações de dinâmica molecular / Molecular basis of functional impairment of androgen receptor mutants studied by molecular dynamics simulations da Silva, Julio Cesar Araujo, 1974- 21 August 2018 (has links) Orientador: Munir Salomão Skaf / Tese (doutorado) - Universidade Estadual de Campinas, Instituto de Química / Made available in DSpace on 2018-08-21T17:39:27Z (GMT). No. of bitstreams: 1 daSilva_JulioCesarAraujo_D.pdf: 43361733 bytes, checksum: 212cdef85174d1daf286133ff839cfb2 (MD5) Previous issue date: 2012 / Resumo: Receptores de androgênio (AR) são membros da superfamília de receptores nucleares que incluem os receptores de esteroides, entre outros. O AR liga os esteroides sexuais endógenos diidrotestosterona e testosterona. O desenvolvimento normal do fenótipo masculino e do sistema reprodutivo necessita de ações pré- e pósnatais promovidas pela interação do AR com esses hormônios. Mutações no gene do receptor de androgênio podem levar a várias doenças como o câncer de próstata e a síndrome de insensibilidade ao androgênio (AIS). Substituições diferentes no mesmo resíduo de aminoácido podem resultar em impactos variáveis na atividade do receptor levando a diferentes graus de AIS. Um grande número de mutações tem sido reportado para o AR envolvendo AIS e células tumorais de câncer de próstata e sua localização e função podem ajudar a entender como essas doenças devem ser tratadas. Entretanto, pouco se sabe sobre como as mutações mudam a estrutura e a dinâmica do AR, uma vez que apenas poucas estruturas cristalográficas de mutantes foram obtidas. Neste trabalho, apresentamos estudos de simulação de dinâmica molecular de algumas estruturas do AR humano com mutações localizadas no domínio de ligação do ligante (LBD) em comparação com a estrutura nativa complexadas com o ligante sintético metiltrienolona (R1881). Nosso objetivo é investigar as bases moleculares das mudanças sutis no receptor causadas pelas mutações que afetam sua afinidade pelo ligante R1881. Embora nenhum dos resíduos mutados deste estudo interajam diretamente com o ligante, os resultados das simulações indicaram que as mutações causam mudanças estruturais e dinâmicas no AR-LBD na região onde se localiza a mutação e na cavidade de ligação do ligante (LBP). A principal mudança observada foi o deslocamento do resíduo Arg752, facilitando a entrada de moléculas de água no LBP e o reposicionamento de cadeias laterais dos resíduos do domínio F, uma importante região que contribui para a estabilidade da estrutura do AR-LBD e da conformação ativa da hélice 12. Os resultados obtidos mostram que essas mutações, que ocorrem naturalmente, são exemplos de resíduos que não estão em contato direto com o ligante e não pertencem à região de recrutamento do coativador, mas que possuem um importante papel na ligação do ligante e na ativação do receptor por estabilizar a hélice 12 e o domínio F na conformação ativa / Abstract: Androgen receptors (AR) are members of the superfamily of nuclear receptors that includes the steroid receptors, among others. AR binds the male endogenous sex steroids, dihydrotestosterone and testosterone. Normal development of the male phenotype and reproductive system requires pre- and postnatal actions promoted by AR interaction with these hormones. Mutations in the androgen receptor gene may lead to several diseases like prostate cancer (PCa) and the androgen insensitivity syndrome (AIS). Different substitutions at the same amino acid residue may result in variable impact on the activity of the receptor leading to different degrees of AIS. A number of mutations have been reported for the AR in AIS and PCa tumor cells and their location and function may help us to understand how these diseases should be treated. Nevertheless, not much is known about how the mutations change the structure and dynamics of the AR since only a few crystallographic structures of mutants were obtained. In this work we present molecular dynamics simulation (MD) studies of some human AR mutations located in the ligand binding domain (LBD) in comparison with wild type (WT) structure in complex with the synthetic ligand methyltrienolone (R1881). Our goal is to investigate the molecular basis of subtle changes in the receptor caused by mutations in the AR-LBD/R1881 affinity. Although the mutated residues do not interact with the ligand, the simulations results indicated that the mutants cause structural and dynamical changes in the AR-LBD in the region in which the mutation is placed and in the binding pocket (LBP). The principal change observed was the displacement of residue Arg752, facilitating water penetration in LBP, and the repositioning of F-domain side chains, which makes important contributions to the stability of the AR-LBD structure and helix 12 active conformation. The results obtained show that these naturally occurring mutations are examples of residues that are not in contact with the ligand and do not belong to coactivator recruitment region, but which do have an important role in ligand binding and receptor activation by stabilizing the helix H12 and the F-domain in the active conformation / Doutorado / Físico-Química / Doutor em Ciências Receptor nuclear Receptor de androgênio Simulação de dinâmica molecular Nuclear receptor Androgen receptor Molecular dynamics simulations
155	Age-related androgen secretion in healthy women and in women with polycystic ovary syndrome Piltonen, T. (Terhi) 24 September 2004 (has links) Abstract The number of ovarian follicles declines with age resulting in a significant decrease of fertility by the age of 40. However, the age when follicle loss starts to affect ovarian endocrine function is not well recognized. The purpose of the present study was to investigate age-related ovarian/adrenal androgen secretion, which is crucial for estrogen biosynthesis in healthy women and in women with polycystic ovarian syndrome (PCOS). Another aim of the study was to compare the usefulness of different serum markers in assessing ovarian aging and in diagnosing polycystic ovaries (PCOs) and PCOS. The human chorionic gonadotropin (hCG) test was used to study the endocrine potential of ovaries/adrenals. The ovarian capacity to secrete and synthesize androgens was found to be decreased as early as at the age of 30 in regularly menstruating women. In women with PCOS, both basal and hCG-stimulated androgen levels were about 50% higher than in healthy women and they remained high until late reproductive age. Similarly to regularly menstruating women, the androgen secretion capacity in PCOS subjects decreased with age, and estradiol concentrations remained unchanged until the age of 44 years. Adrenal androgen synthesis was not changed during hCG-tests. Since serum antimüllerian hormone (AMH) and follicle stimulating hormone (FSH) levels were changed significantly after the age of 25 years in regularly menstruating women, they may be considered as useful serum markers reflecting the ovarian aging process. In women with PCOS, AMH levels were continuously 2- to 3-fold higher than in healthy women possibly reflecting high follicle number in these women. A decline in ovarian endocrine function before the age of 30 is one of the first signs of ovarian aging. However, in women with PCOS ovarian androgen secretion capacity is markedly increased and remain high throughout the reproductive years. The results of the present studies also indicate that LH/hCG does not play a role in adrenal androgen synthesis, since LH/hCG did not stimulate adrenal androgen synthesis. The measurement of AMH is a useful tool to estimate ovarian aging process as well as to diagnose PCOs/PCOS. androgen secretion antimüllerian hormone hCG-test ovarian aging polycystic ovary syndrome
156	Prostatic gene expression: probasin, human prostatic acid phosphatase and macrophage inhibitory cytokine-1 as model genes Patrikainen, L. (Lila) 16 February 2004 (has links) Abstract Gene products that are only expressed in one tissue or cell type are useful models for investigating the biochemical and molecular mechanisms of tissue/cell-specific gene regulation. The regulatory regions of such genes are also practical tools in gene therapy. In this work, prostate-specific and androgen-dependent gene regulation was investigated by using human prostatic acid phosphatase (hPAP) and rat probasin (rPB) as models. In DNase I footprinting, a protected 12 bp region was found in the PB gene between the nucleotides -251 and -240 only with nuclear extracts of prostatic origin. The sequence of this area was GAAAATATGATA. Weak interaction could be detected between the DNA-binding domain of AR and the prostatic transcription factor. The results also suggested that the prostatic regulatory protein makes AR binding to its response element more effective and concomitantly magnifies the effect of androgen. A hPAP construct containing the sequence between the nucleotides -734 and +467 in front of the CAT reporter gene was highly expressed in the prostate of transgenic mice. Five homologues (A-E) for our previously identified prostate-specific GAAAATATGATA DNA-binding site were found in the area where the sites C and E could bind the regulatory protein in EMSA. The prostatic transcription factor complex bound to the GAAAATATGATA site was purified and characterized from a suspension-adapted mass culture of PC-3 prostate cancer cells by using sequence-specific DNA affinity chromatography, mass spectrometry and supershifts. Several potential transcription factors were identified, but only USF2 was confirmed to be part of the transcription factor complex. Two PC-3 cell line variants (anchorage-dependent and suspension-adapted, anchorage-independent variants) were used as a model for advanced, androgen-independent prostate cancer. Genes that were overexpressed in a suspension-adapted PC-3 cell line were further investigated, since they can be considered as putative markers of metastatic activity. The macrophage inhibitory cytokine-1 (MIC-1) gene, which was overexpressed in the suspension-adapted PC-3 cell line, was further investigated in order to clarify the mechanism behind aggressive cell growth and androgen-independent gene regulation. In patient specimens, MIC-1 had no or low expression in benign prostatic hyperplasia and normal prostate but high in prostatic cancer and therefore it could be a useful marker for aggressive prostate cancer. Indomethacin increased the expression of MIC-1 in PC-3 cells, and apoptosis was also induced in this cell line but not in saPC-3 cell line suggesting a block in MIC-1 inducible apoptosis pathway. DNA-binding sites androgen receptor gene expression promoter prostate transcription factors
157	In vitro modulation of androgen and estrogen receptors in human prostate cells by essential fatty acids Prinsloo, Sophia Elizabeth 19 December 2005 (has links) Please read the abstract in the section 00front of this document / Dissertation (MSc (Reproductive Biology))--University of Pretoria, 2005. / Urology / unrestricted Essential fatty acids Imunocytochemistry Estrogen receptor Androgen receptors Prostate cancer Du-145 cells UCTD
158	A population-based analysis of the risk of hip fracture in men with prostate cancer exposed to radiation and androgen deprivation therapy Blood, Paul 11 1900 (has links) Prostate cancer is frequently diagnosed in elderly men and, despite the largely unproven survival benefits of treatment, the majority receive treatment. Treatment options include surgery, radiation, and/or androgen deprivation therapy (ADT). Risks associated with treatment include hip fracture. Current understanding suggests that hip fracture is a frequent cause of morbidity and mortality in the elderly, and both radiation treatment and ADT can increase the risk of hip fracture. It is important to understand these risks so they can be minimized and the morbidity of treatment reduced. The objectives of this study were to estimate the risk of hip fracture as a major adverse outcome of treatment for prostate cancer among elderly men. The specific objectives include estimating: 1) the risk of hip fracture and the dose-risk relationship among patients receiving curative radiation treatment, and 2) the risk of hip fracture associated with palliative ADT and relapsed ADT compared to curative ADT. The cancer diagnosis and treatment records of 32,673 men were linked to their hospital discharge abstracts. The risk of hip fracture was estimated using Cox regression and the estimates were adjusted for age, comorbidity, income, and year of diagnosis. The risk of hip fracture was 59% higher among men who received curative radiation when compared to men who received curative surgery. The risk of hip fracture fell by 6% with each one Gy increase in radiation dose between 55 and 81 Gy Biological Equivalent Dose to the hip-bone. The risk of hip fracture for subjects in the palliative ADT and relapsed ADT categories was 5.98 and 5.77 times the risk in comparison to men who received curative ADT treatment. Curative radiation treatment is associated with an increased risk of hip fracture when compared to curative surgery. The risk of hip fracture is greater with ADT for palliation and relapsed cancer than with curative treatment. Current treatments for prostate cancer contain significant risk of hip fracture for elderly men and these risks should be considered as part of the treatment decision. / Medicine, Faculty of / Population and Public Health (SPPH), School of / Graduate Prostate cancer Hip fracture Radiation Androgen deprivation therapy Radiotherapy Hormone therapy
159	Effect of Chronic Alcohol Abuse and Resistance Training on the Skeletal Muscle Androgen Receptor Concentration of Rats Vingren, Jakob L. 08 1900 (has links) The purpose was to examine the effect of chronic alcohol abuse on the androgen receptor content (AR) in skeletal muscle, and to determine if this effect was influenced by resistance training. Thirty-four male rats (456 ± 1 g; mean ± SE) were divided into 4 groups: Sham exercise-Ethanol, Sham exercise-Normal diet, Exercise-Ethanol, and Exercise-Normal diet. Both Exercise groups underwent a 6-week "squat" resistance training protocol and both Ethanol groups received an alcohol-rich diet throughout the 6-week period. Western blot analysis showed no effect of alcohol or resistance training on the AR of the extensor digitorum longus. For the rectus femoris, alcohol caused a decline in the AR (p=0.01). This reduction was not attenuated by resistance training. The AR of the soleus was not affected by chronic alcohol abuse alone; however, the resistance training induced increase in the AR was prevented by chronic alcohol abuse (p=0.03). Alcohol -- Physiological effect. Androgens -- Receptors. Rats -- Nervous system. ethanol androgen testosterone exercise weight training
160	Identificação e caracterização de transcritos humanos: novas famílias de pequenas GTPases e novos longos RNAs intrônicos não-codificantes / Identification and characterization of human transcripts: novel small GTPase gene families and novel Long Intronic non-coding RNAs Rodrigo Louro 27 November 2006 (has links) Terminado o sequenciamento do genoma humano, as atenções se voltaram para a determinação do conjunto completo de transcritos humanos. Diversos trabalhos sugerem que enquanto apenas uma pequena fração de mRNAs codificantes para proteína não é conhecida, existe um grande número de RNAs não-codificantes (ncRNAs) ainda não caracterizados. Nesse contexto, o presente trabalho visou explorar as informações de expressão gênica contidas em ESTs para identificar e caracterizar novos transcritos humanos. A busca genômica por membros de famílias gênicas relacionadas com câncer levou a identificação de novas pequenas GTPases, destacando uma subfamília que deve apresentar função supressora tumoral em próstata. Uma classe de ncRNAs longos, sem splicing, expressos antisenso a partir de regiões intrônicas foi descrita utilizando plataformas de microarrays, construídas pelo grupo, enriquecidas com seqüências sem anotação. O perfil de expressão de 23 ncRNAs intrônicos estava significativamente correlacionado com o grau de diferenciação de tumores de próstata (Gleason Score), e pode ser utilizado como candidato a marcador molecular de prognóstico. Um total de 39 ncRNAs intrônicos responderam à estimulação por andrógeno, apontando para um mecanismo regulatório da expressão intrônica por sinais fisiológicos hormonais. A biogênese da expressão intrônica parece ser complexa, pois uma fração não é transcrita pela RNA Polimerase II. A transcrição intrônica estava correlacionada com uso de exons em células tratadas com andrógeno. Assinaturas de expressão intrônica conservadas em tecidos humanos e de camundongos, e interações de transcritos intrônicos com proteínas regulatórias foram observadas. Este trabalho contribui com novas e originais evidências que dão apoio ao papel postulado para esses ncRNAs no controle fino do programa transcricional humano. / With the completion of the human genome sequence, attention has shifted towards determining the complete set of human transcripts. Multiple lines of evidence suggest that while only a small fraction of protein-coding mRNAs remains to be described, there is a huge amount of uncharacterized non-coding RNAs (ncRNAs). In this context, the present work sought to explore the gene expression information provided by ESTs to identify and characterize new human transcripts. A genomic-wide search for cancer related gene family members identified novel small GTPase genes, and highlighted an uncharacterized subfamily that may have a tumor suppressor role in prostate cancer. A class of long unspliced ncRNAs, expressed antisense from introns of protein-coding genes was described using custom-designed microarray platforms enriched with unannotated sequences. The expression profile of 23 intronic ncRNAs was significantly correlated to the degree of prostate tumor differentiation (Gleason Score), and could be used as a candidate prognostic molecular maker. A total of 39 intronic ncRNAs were responsive to androgen stimulation, poiting to a mechanism of intronic expression regulation by physiological hormone signals. Intronic ncRNA biogenesis seems to be complex, since a fraction of them is not transcribed by RNA Polymerase II. Intronic transcription was correlated to exon usage in androgen treated cells. Tissue expression signatures of intronic transcription were conserved in human and mouse, and intronic transcripts were found to interact with regulatory proteins. This work provides new and original contributions that support the postulated role of ncRNAs in the fine tunning of the human transcriptional program. Andrógeno Câncer de próstata Expressão gênica Introns RNAs Androgen Gene expression Introns Prostate cancer RNAs

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