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The prevalence and associations of low testosterone levels and erectile dysfunction in a male diabetic urban populationKemp, Tanja January 2014 (has links)
Introduction: According to the literature, low serum testosterone levels are associated with diabetes mellitus. Minimal data exist for its prevalence or predictors in South Africa. Erectile dysfunction is a common condition in diabetic patients. The prevalence and predictors in our patient population is unknown.
Methods: An observational, cross-sectional study was performed in 150 consecutive male diabetic patients over the age of 50 years in the Diabetic clinic of Steve Biko Academic Hospital. These patients were evaluated for diabetes control and complications, the presence of erectile dysfunction and for hypogonadism symptoms. Morning serum testosterone levels were done. Subjects with low testosterone levels were compared to those with normal levels. Results: The mean age of the patients was 62 years (standard deviation (SD) 7.87), 91.3% had type 2 diabetes, and 84.7% were on insulin. The mean duration of diabetes was 15 years (SD 8.65). The mean body mass index was 30.7 (SD 5.37), the mean waist circumference was 112.4cm (SD 16.42), the median creatinine was 96μmol/L (interquartile range (IQR) 79-133) and the median HbA1C was 7.85% (IQR 6.80-9.30). Ischaemic heart disease was previously diagnosed in 40.7% of patients.
Some degree of erectile dysfunction was reported in 95.3% of the patients with 51.3% reporting serious dysfunction. The prevalence of androgen deficiency symptoms was 94.7%. Fifty percent of the men had low total testosterone levels; 40.7% had low modified calculated bioavailable testosterone levels, and in 27.3% both were low.
With multivariate logistic regression the significant factors associated with low total testosterone were waist circumference and known cardiovascular disease. For a low modified calculated bioavailable testosterone level significant variables were age, diabetes duration and body mass index and for an outcome defined as both the above the significant factors were diabetes duration, body mass index, and known cardiovascular disease. With multivariate logistic regression the significant factors associated with erectile dysfunction were age, body mass index, peripheral neuropathy score, and diuretic therapy.
The prevalence of symptoms of androgen deficiency was very high with 94.7% of all patients reporting a significant amount of symptoms on the Androgen Deficiency in Adult Males (ADAM) questionnaire. If only the total serum testosterone level was evaluated instead of the modified calculated bioavailable testosterone, the sensitivity was 69%, the specificity was 63%, with a poor positive predictive value of only 56%. The negative predictive value was better at 75%. Differences in quality of life scores were only seen for some erectile dysfunction subgroups but not for low testosterone levels.
Conclusion: This study confirms the high prevalence of low testosterone levels and of erectile dysfunction in diabetic male patients in a tertiary setting, and argues in favour of universal screening of this population group. Multiple predictors of low testosterone levels and of erectile dysfunction were identified. The ADAM questionnaire was not useful in identifying subjects with a low testosterone level. Total testosterone testing alone performed poorly in comparison with modified calculated bioavailable testosterone and is not the recommended test of choice. Erectile dysfunction negatively affected the quality of life. / Dissertation (MSc)--University of Pretoria, 2014. / gm2015 / Clinical Epidemiology / MSc / Unrestricted
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Efeitos da castração e da reposição hormonal com undecanoato de testosterona na bexiga urinária de ratos: análise estrutural, ultra-estrutural e bioquímica / Effects castration and hormonal replacement in the rat urinary bladder, structural, ultrastructural and biochemical analysisCarla Braga Mano Gallo 04 November 2009 (has links)
Evidências recentes em animais e humanos sugerem que níveis adequados de testosterona são necessários para as funções adequadas de diversos órgãos do sistema urogenital, incluindo a bexiga urinária. Estudos sobre os efeitos da testosterona na estrutura da parede da bexiga são raros. Portanto, o objetivo do presente trabalho é avaliar através de métodos qualitativos e quantitativos, as alterações estruturais da parede vesical de ratos submetidos à castração cirúrgica, bem como o papel da reposição hormonal na reversão das possíveis alterações estruturais. Foram usados 24 ratos machos Sprague-Dawley com aproximadamente 12 semanas de idade. Os animais foram divididos em 3 grupos compostos de 8 animais cada e tratados como a seguir. C = Grupo Castrado os animais foram submetidos a orquiectomia e sacrificados após 2 meses, S = Grupo Simulado os animais foram submetidos a operação simulada e sacrificados após 2 meses, T = Grupo Testosterona os animais foram submetidos a castração e após 1 mês foram submetidos a reposição hormonal com undecanoato de testosterona em dose única subcutânea de 100 mg/kg (T) e após 1 mês da reposição hormonal foram sacrificados. Foram realizadas análises quantitativa e qualitativa do colágeno (usando histoquímica, histomorfometria, bioquímica e microscopia eletrônica de varredura), e análise histomorfométrica do músculo liso e das fibras do sistema elástico na parede da bexiga em controles e em ratos submetidos apenas a castração, e em ratos submetidos a castração e reposição hormonal. A análise morfométrica da altura do urotélio não apresentou diferença entre os grupos. Não houve diferença significativa na análise quantitativa do colágeno, tanto por histomorfometria quanto por bioquímica. Entretanto, a análise qualitativa mostrou diferenças do colágeno no grupo castrado quando comparado aos controles e aos ratos com reposição hormonal. Existiu uma diminuição significativa nos valores absolutos das fibras do sistema elástico no grupo castrado. Por outro lado, o músculo liso apresentou um aumento significativo na massa muscular por densidade de área nos ratos castrados; entretanto, a contagem dos núcleos das células musculares não apresentou variação entre os grupos, demonstrando que o aumento foi devido a hipertrofia muscular e não por aumento do número de células. Interessantemente, a reposição hormonal com testosterona foi capaz de reverter todas as alterações observadas. Os resultados sugerem que a reposição hormonal, mesmo quando instituída em fase tardia, é efetiva na reversão das alterações da parede da bexiga produzidas por hipogonadismo secundário. / Recent evidences in animals and humans have suggested that adequate levels of testosterone are necessary to adequate functions of diverse organs of the urogenital system, including the urinary bladder. Studies on the effects of testosterone in the bladder wall structure are rare. Therefore, the objective of the present study is to evaluate, through qualitative and quantitative methods, the structural alterations in the bladder wall of rats submitted to surgical castration as well as the role of hormonal replacement in reversing the possible structural alterations. We used 24 male Sprague-Dawley rats that were approximately 12 weeks of age. The animals were divided into 3 groups composed of 8 animals each and treated as follows. Group C = group that underwent orchiectomy and were sacrificed after 2 months, Group S = sham group sacrificed after 2 months, and Group T = group that underwent orchiectomy, and after 1 month underwent testosterone replacement with a subcutaneous single dose of testosterone undecanoate at 100 mg/kg (T) and after 1 month of hormonal replacement, the animals were sacrificed. We performed a qualitative and quantitative analysis of collagen (by using histochemistry, histomorphometry, biochemistry, and scanning electron microscopy), and a histomorphometric analysis of smooth muscle and elastic system fibers in bladder wall of controls and rats submitted to orchiectomy alone and with hormonal replacement. The histomorphometric analysis on the epithelial height did not show differences among the groups. There was no statistically significant difference in the quantitative analysis for collagen, both by histomorphometry and biochemistry. Nevertheless, the qualitative analysis showed differences in collagen in the castrated group, when compared to controls and to rats with hormonal replacement. There was a significant decrease in the absolute values of elastic system fibers in the castrated group. On the other hand, the smooth muscle presented a significant increase in muscular mass by density of area in castrated rats; nevertheless, the counting of muscle cells nuclei did not present variation among the groups, demonstrating that this increase was due to cellular hypertrophy rather than by an increase in cells number. Interestingly, the hormonal replacement with testosterone was able to reverse all alterations observed. The results suggest that hormonal replacement, even when instituted at a late stage, is effective in reversing the bladder wall alterations produced by secondary hypogonadism.
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Efeitos da castração e da reposição hormonal com undecanoato de testosterona na bexiga urinária de ratos: análise estrutural, ultra-estrutural e bioquímica / Effects castration and hormonal replacement in the rat urinary bladder, structural, ultrastructural and biochemical analysisCarla Braga Mano Gallo 04 November 2009 (has links)
Evidências recentes em animais e humanos sugerem que níveis adequados de testosterona são necessários para as funções adequadas de diversos órgãos do sistema urogenital, incluindo a bexiga urinária. Estudos sobre os efeitos da testosterona na estrutura da parede da bexiga são raros. Portanto, o objetivo do presente trabalho é avaliar através de métodos qualitativos e quantitativos, as alterações estruturais da parede vesical de ratos submetidos à castração cirúrgica, bem como o papel da reposição hormonal na reversão das possíveis alterações estruturais. Foram usados 24 ratos machos Sprague-Dawley com aproximadamente 12 semanas de idade. Os animais foram divididos em 3 grupos compostos de 8 animais cada e tratados como a seguir. C = Grupo Castrado os animais foram submetidos a orquiectomia e sacrificados após 2 meses, S = Grupo Simulado os animais foram submetidos a operação simulada e sacrificados após 2 meses, T = Grupo Testosterona os animais foram submetidos a castração e após 1 mês foram submetidos a reposição hormonal com undecanoato de testosterona em dose única subcutânea de 100 mg/kg (T) e após 1 mês da reposição hormonal foram sacrificados. Foram realizadas análises quantitativa e qualitativa do colágeno (usando histoquímica, histomorfometria, bioquímica e microscopia eletrônica de varredura), e análise histomorfométrica do músculo liso e das fibras do sistema elástico na parede da bexiga em controles e em ratos submetidos apenas a castração, e em ratos submetidos a castração e reposição hormonal. A análise morfométrica da altura do urotélio não apresentou diferença entre os grupos. Não houve diferença significativa na análise quantitativa do colágeno, tanto por histomorfometria quanto por bioquímica. Entretanto, a análise qualitativa mostrou diferenças do colágeno no grupo castrado quando comparado aos controles e aos ratos com reposição hormonal. Existiu uma diminuição significativa nos valores absolutos das fibras do sistema elástico no grupo castrado. Por outro lado, o músculo liso apresentou um aumento significativo na massa muscular por densidade de área nos ratos castrados; entretanto, a contagem dos núcleos das células musculares não apresentou variação entre os grupos, demonstrando que o aumento foi devido a hipertrofia muscular e não por aumento do número de células. Interessantemente, a reposição hormonal com testosterona foi capaz de reverter todas as alterações observadas. Os resultados sugerem que a reposição hormonal, mesmo quando instituída em fase tardia, é efetiva na reversão das alterações da parede da bexiga produzidas por hipogonadismo secundário. / Recent evidences in animals and humans have suggested that adequate levels of testosterone are necessary to adequate functions of diverse organs of the urogenital system, including the urinary bladder. Studies on the effects of testosterone in the bladder wall structure are rare. Therefore, the objective of the present study is to evaluate, through qualitative and quantitative methods, the structural alterations in the bladder wall of rats submitted to surgical castration as well as the role of hormonal replacement in reversing the possible structural alterations. We used 24 male Sprague-Dawley rats that were approximately 12 weeks of age. The animals were divided into 3 groups composed of 8 animals each and treated as follows. Group C = group that underwent orchiectomy and were sacrificed after 2 months, Group S = sham group sacrificed after 2 months, and Group T = group that underwent orchiectomy, and after 1 month underwent testosterone replacement with a subcutaneous single dose of testosterone undecanoate at 100 mg/kg (T) and after 1 month of hormonal replacement, the animals were sacrificed. We performed a qualitative and quantitative analysis of collagen (by using histochemistry, histomorphometry, biochemistry, and scanning electron microscopy), and a histomorphometric analysis of smooth muscle and elastic system fibers in bladder wall of controls and rats submitted to orchiectomy alone and with hormonal replacement. The histomorphometric analysis on the epithelial height did not show differences among the groups. There was no statistically significant difference in the quantitative analysis for collagen, both by histomorphometry and biochemistry. Nevertheless, the qualitative analysis showed differences in collagen in the castrated group, when compared to controls and to rats with hormonal replacement. There was a significant decrease in the absolute values of elastic system fibers in the castrated group. On the other hand, the smooth muscle presented a significant increase in muscular mass by density of area in castrated rats; nevertheless, the counting of muscle cells nuclei did not present variation among the groups, demonstrating that this increase was due to cellular hypertrophy rather than by an increase in cells number. Interestingly, the hormonal replacement with testosterone was able to reverse all alterations observed. The results suggest that hormonal replacement, even when instituted at a late stage, is effective in reversing the bladder wall alterations produced by secondary hypogonadism.
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The potential relationships between hormone biomarkers and functional and health outcomes of ageingEendebak, Robert January 2017 (has links)
Although the female menopause has been extensively characterized as a well-defined symptomatic state of oestrogen deficiency, which responds relatively well to oestrogen replacement therapy, the symptomatic state of androgen deficiency in men is poorly defined and uncertainty exists whether it responds to testosterone replacement. It has been proposed that hypothalamic-pituitary-testicular (HPT)-axis function (responsible for the production of androgens) and regulation could be viewed as a âbarometerâ of health status in older men and that potential alterations in HPT-axis function and regulation reflect subclinical and clinical deficits in function and health, which may result in an aged phenotype of human health and disease in older men. The HPT-axis constitutes a well-defined, tractable, clinically-relevant, biological system, which may permit insight into the mechanisms underlying the expression of ageing-related phenotypes of human health and disease. By using a different lens â such as the genetic background; the compensatory responses within the HPT-axis; the syndromes of androgen deficiency; the ethnic background of an individual or the life course trajectory of function and health from conception into older age â to magnify potential dysregulation in the HPT-axis will it be possible to visualize and understand the phenotypic expression of human male ageing as a gradient of functional and health outcomes. This will allow for a better understanding of the physiological mechanics underlying symptomatic expression of dysregulation in the HPT-axis.
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