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401	Confidence of Nursing Personnel in Their Understanding of the Psychosocial Impact of Prostate Cancer Williams, Sherry, Hemphill, Jean Croce, Knowles, Amy 01 January 2017 (has links) No description available. confidence nursing personnel psychosocial prostate cancer College of Nursing Nursing
402	Confidence of Nursing Personnel in their Understanding of the Psychosocial Impact of Prostate Cancer Williams, S., Hemphill, Jean Croce, Knowles, A. 01 October 2017 (has links) No description available. nursing personel confidence psychological impact prostate cancer College of Nursing Nursing
403	Moecular Profiling of Blood for Diagnostics and Discovery / AN EXHIBITION OF BLOOD MOLECULAR PROFILING FOR DIAGNOSTICS AND DISCOVERY Haas-Neill, Sandor January 2022 (has links) Molecular profiling of blood for several purposes, 1) To identify prostate cancer biomarkers, 2) to identify commonalities between asthma and mood disorders, and 3) to identify mRNAs that may be involved in psychobiotic changes to behaviour. / Every cell of the body has the opportunity to secrete molecules into the blood. These molecules: proteins, RNAs, and DNAs, can be secreted freely, or within extracellular vesicles (EV). The complement of specific molecules secreted by cells can vary in accordance with changes to their immediate environment, such as disease in a particular organ. Cells of the immune system which circulate in the blood may also change the rates at which they produce these molecules in response to a disease or unusual event occurring somewhere within the body. The full complement of proteins, RNAs, or DNAs from all sources within the blood can therefore be measured to garner information about disease states and communication between every tissue of the body. In this body of work, we leveraged this to address three separate challenges within medical science. First, we utilized blood as a source of biomarkers for disease and disease severity; isolating EVs from the blood of prostate cancer patients and healthy subjects and characterized their proteins with mass spectrometry to identify potential biomarkers for prostate cancer and its stages. Next, we explored the ability of blood to identify commonalities between distinct but often comorbid diseases; here we utilized publicly available datasets to identify transcripts or gene sets potentially facilitating the relationship between PTSD, MDD, and asthma. Finally, we utilized differential gene and gene sets expression to gain mechanistic insight into microbiota-gut-brain axis; investigating the hippocampus and blood of mice fed one of two psychobiotic bacteria: Lactobacillus rhamnosus JB1, Lactobacillus reuteri 6475. The analysis identified several mRNA expression differences potentially responsible for the mood-altering characteristics of these psychobiotic bacteria. This body of work illustrates the utility of blood omics data for addressing many problems within medical science, and highlights the large scale of information stored within the blood. / Thesis / Doctor of Philosophy (Medical Science) / Every cell of the body has the opportunity to secrete molecules into the blood. These molecules: proteins, ribonucleic acids (RNAs), and deoxyribonucleic acids (DNAs), can be secreted freely, or within small membrane compartments called extracellular vesicles (EV). Specific molecules are secreted more or less by cells depending on changes to their immediate environment, such as disease in a particular organ. We leveraged this to the benefit of medical science in three separate scenarios: 1) using the molecular contents of EVs to determine when someone has prostate cancer, and at what stage; 2) examining RNAs of the blood to determine why so many with asthma also have depression or PTSD; 3) measuring RNAs in the blood and hippocampus of mice to better understand how certain bacteria in the gut can alleviate depression. This work illustrates the utility of blood in tackling many challenging problems within medical science.
404	L'exposition aux anti-inflammatoires non stéroïdiens et aux antihypertenseurs et le risque de cancer de la prostate Perron, Linda 11 April 2018 (has links) Des études suggèrent que les anti-inflammatoires non stéroïdiens (AINS) et les antihypertenseurs préviendraient peut-être le développement du cancer de la prostate. La confirmation de ces observations pourrait conduire à l'élaboration de mesures de chimioprévention de ce cancer. Pour vérifier si l'usage de ces médicaments est associé au risque de développer un cancer de la prostate, nous avons réalisé une étude cas-témoins avec appariement sur l'âge. La population participante comportait 2221 cas et 11 105 témoins. La durée rétrospective d'observation s'étendait sur huit ans. Les renseignements sur la maladie et l'exposition médicamenteuse provenaient des banques de données informatisées de la Régie de l'assurance maladie du Québec et du Fichier des tumeurs du Québec. Nous avons observé que ceux recevant 80 mg ou plus d'acide acétylsalicylique (AAS) quotidiennement, depuis 8 ans, avaient 18 % moins de risque de développer un cancer de la prostate que les non-exposés (rapport de cotes (RC) = 0,82, intervalle de confiance à 95 % (IC) = 0,71-0,95). L'association entre l'AAS et le cancer de la prostate démontrait des gradients durée-réponse et dose-réponse consistants. Par ailleurs, nous avons observé que l'effet protecteur de l'AAS s'estompait rapidement lorsque cessait l'exposition. Ceci laisse croire que l'AAS pourrait retarder plutôt que prévenir le développement du cancer de la prostate. Le risque de néoplasie prostatique était indépendant de l'usage des AINS autres que l'AAS. Un biais de classification explique peut-être cette dernière constatation. Par ailleurs, par rapport aux non-exposés, le risque de cancer de la prostate chez les exposés aux antihypertenseurs était de 0,98 (IC, 0,88-1,08). Lorsque analysé par classe, seule l'exposition aux bêta-bloquants s'est avérée associée au risque de néoplasie prostatique (RC=0,86, IC=0,77-0,96). Par rapport aux non-exposés, le risque était de 0,89 (0,75-1,05), 0,91 (0,75-1,09), et 0,82 (0,69-0,96) chez ceux ayant cumulé moins d'un an, un à quatre ans et plus de quatre ans d'exposition aux bêta-bloquants, respectivement. De plus, les hommes exposés pendant au moins quatre ans à l'AAS et à un bêta-bloquant présentaient 31 % (RC=0,69, IC=0,50-0,97) moins de cancer de la prostate que les non-exposés. L'usage d'AAS de même que l'usage de bêta-bloquants serait donc, selon nos résultats, associé à une réduction du risque de survenue d'un cancer de la prostate. Prostate -- Cancer -- Chimioprévention Antiinflammatoires non stéroïdiens Hypotenseurs Aspirine Bêtabloquants
405	Special Issue “Diagnostic Biomarkers in Prostate Cancer 2020” Neuhaus, Jochen 04 May 2023 (has links) No description available. editorial, prostate cancer info:eu-repo/classification/ddc/610 ddc:610
406	Chromosomal aberrations in high grade prostatic intraepithelial neoplasia and prostate cancer in African American men Ramos, Kristina 11 October 2019 (has links) Recent advances in whole genome sequencing have led to many discoveries in the mechanisms involved in carcinogenesis. Genomic characterization of premalignant lesions in numerous cancers has led to new prevention strategies, early detection, and treatment options that have saved lives and improved the quality of life for the people suffering from these cancers. Prostate cancer (PCa) is the most common cancer in men in the United States (US) and the second leading cause of death in men from all cancers. However, in African American men (AAM) the mortality rate from PCa is 2.4 times higher than European American men (EAM). In addition, AAM are more likely to get PCa and have a higher PCa burden at diagnosis than their EAM counterparts. This may suggest that there are racial/ethnic differences in the mechanism of carcinogenesis in PCa. PCa and its premalignant lesion, high grade prostatic intraepithelial neoplasia (HGPIN), are one of the most heterogeneous and complex cancers for scientists to determine the mechanisms of carcinogenesis. Due to this complexity, research on HGPIN and PCa has been difficult to carry out and interpret. Projects have been undertaken and progress has been made in the discovery of some genes involved in PCa and potential drivers of initiation, progression and aggressiveness of PCa. However, these studies have mostly been conducted among EAM and have little ethnic diversity. Discovery of new prevention, early detection and treatment methods for PCa will not be possible without advances in the genetic characterization of the pathways of carcinogenesis of PCa among ethnically diverse study populations. To date there are no known genetic characterizations of HGPIN and PCa in AAM. This study aims to characterize chromosomal copy number aberrations (CNA) in paired HGPIN and PCa in AAM. By utilizing advanced microarray techniques, we will determine the degree to which HGPIN and PCa share CNA and identify CNA that may be involved in PCa progression. This study will lay the foundation for future research into CNA that may be used as potential biomarkers for early detection of neoplasms of high-risk for development into PCa in AAM. The discovery of biomarkers and the characterization of the mechanisms involved in PCa progression may lead to treatment options for the prevention of PCa and an overall better outcome for AAM suffering from PCa. Genetics African American Chromosome Genetics Intraepithelial neoplasia Neoplasia Prostate cancer
407	MicroRNA regulation of prostate cancer desensitization to androgen receptor antagonist drugs during androgen deprivation therapy Lorch, Robert A. 01 May 2011 (has links) The current standard treatment of prostate cancer by androgen deprivation therapy involves using drugs such as bicalutamide (Casodex) to antagonistically block androgen receptors that are normally present within prostate cells. Usually, the therapy is successful in the short run at limiting the growth of prostate cancer. However, in virtually all cases tumors begin to grow aggressively again after several months of treatment and new therapies must be started. The mechanism by which these prostate cells transform from androgen sensitive to androgen independent and anti-androgen resistant is unclear. In this study, we investigated the role of microRNAs, small 15 to 18 nucleotide regulatory RNAs, in regulating the desensitization of prostate cancer cells to the androgen receptor antagonist drug bicalutamide. In order to identify significant microRNAs, quantitative PCR was used to obtain genome-wide microRNA expression levels of 885 human microRNAs at different timepoints for androgen sensitive LNCaP cancer cells treated with bicalutamide and for untreated control cells in tissue culture. Analysis of microRNA expression by clustering analysis and by statistical comparisons of treatment groups resulted in identification of 28 microRNAs that have altered expression in the progression process. In silico target prediction analysis was performed with the microRNAs shown to have altered expression, and a group of genes predicted to be under microRNA regulatory control during cancer progression to resistance was identified. A microRNA expression profile can be useful in developing more effective prognostic and therapeutic tools for prostate cancer. Molecular Biology
408	Screening for Anticancer Agents to Inhibit Mitotic Kinases and Proliferation of Metastatic Prostate Cancer Cells Nguyen, Khoa 01 January 2016 (has links) Current treatments for prostate cancer (PCa) are marred with high relapse frequency and development of progressively aggressive cancers; developing new treatment options for PCa remains crucial. In this project, a series of synthetic compounds based on natural products will be screened to identify inhibitors for Aurora-A kinase (Aur-A). Aur-A facilitates centrosome separation and bipolar spindle formation during mitosis. Aur-A is overexpressed in metastatic PCa cells, and is a good candidate for targeted therapies. Compound libraries are designed using natural compounds that contain simple structural elements as starting points for developing drug like libraries. High-throughput screening of these libraries will be used to identify potent antimitotic agents that selectively affect cancer cells but not normal cells. A combination of in vitro protein assays – quantifying protein activity – cell-based assays – measuring cell growth and proliferation – and cell-reporter assays – to determine which metabolic pathway the compound affects – were used to identify potential inhibitors. Through these methods, we have identified several compounds, with special consideration to thiazole piperazine compounds, to successfully inhibit proliferation of metastatic PCa cells. Aurora-A Kinase Drug Screening Prostate Cancer Lipinski Metastatic Cancer Biology
409	A Novel Drug to Induce Apoptosis in Advanced Prostate Cancer Cells Sanghvi, Parshva A 01 January 2022 (has links) Prostate cancer is one of the leading causes of death for men in America as approximately 1 in 41 men will have prostate cancer. In this research, we focus on enzalutamide-resistant prostate cancer cells as cell resistance to enzalutamide is a prevalent obstacle in treating prostate cancer. We tested a novel compound library at different doses and observed each compound's efficacy in inducing apoptosis in enzalutamide-resistant cells. Furthermore, we analyzed the mechanism by which apoptosis was induced in compounds that showed a high efficacy at lower doses. Overall, we found that Darapladib shows promising results in treating cells that have acquired enzalutamide resistance. Advanced Prostate Cancer Novel Compounds Compound Screening Cancer Biology
410	Implications for XMRV Infections in Prostate Cancer Hong, Seunghee 23 January 2010 (has links) No description available. Molecular Biology Virology XMRV SEVI XPR1 prostate cancer IL-8

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