1%) patients. Among them, 3 patients refused treatment despite PSA progression. Five patients, who underwent RP as an intervention, all had organ-confined Gleason score smaller than = 6 disease. In 67 patients who underwent RP, 50 (74.6%) patients had insignificant prostate cancer and 8 (11.9%) patients showed unfavorable features. During follow-up,
click here biochemical recurrence occurred in 2 patients. Among 34 patients who received HT, 3 (8.8%) patients had PSA progression. Among 156 patients, 6 patients died due to other causes during follow-up. There were no patients who died due to prostate cancer. Conclusion: The clinical outcomes of incidental prostate cancer were satisfactory regardless of the initial treatment. However, according to recent researches and guidelines,
immediate definite therapy should be avoided without a careful assessment. We also believe that improved clinical staging is needed for these patients.”
“Background: A growing body of evidence shows that brain-derived neurotrophic factor (BDNF) plays a role in depressive disorder. Serum BDNF levels are lower in depressed patients and they increase after a long course of antidepressant treatment. Our study aims to test the effect of antidepressant treatment on serum BDNF levels in patients with a depressive Ro-3306 solubility dmso episode, after they have achieved remission in two studies in Macedonia and Bulgaria. Subjects and methods: In the Macedonian study 23 patients were included (11 female, 12 male) diagnosed with a first depressive episode p38 MAPK signaling pathway according to ICD-10, as well as 23 control subjects age- and sex-matched without a history of psychiatric disorder. In the Bulgarian study 10 female patients with depression and 10 control subjects were included. We have applied the Hamilton Depression Rating Scale (HDRS) to assess depression
severity. Blood samples were collected before antidepressive treatment and after remission was achieved (decrease to 7 points or less on HDRS). Results: In the Macedonian study, mean serum BDNF level at baseline was 13.15 +/- 6.75 ng/ml and the mean HDRS score was 28.52 +/- 4.02. Untreated depressed patients showed significantly lower serum BDNF levels compared to the control group (25.95 +/- 9.17 ng/ml). After remission was achieved, the mean serum BDNF level was 24.73 +/- 11.80 ng/ml whereas the mean HDRS score was 7.04 +/- 3.15. After 8 weeks of treatment there was no statistically significant difference in the serum BDNF levels between the two groups. In the Bulgarian study, baseline mean serum BDNF levels were 26.84 +/- 8.66 ng/ml, after 3 weeks treatment and remission was achieved mean serum BDNF levels were 30.33 +/- 9.25 ng/ml and in the control group mean serum BDNF levels were 25.04 +/- 2.88 ng/ml. Integrated results showed baseline mean serum BDNF levels of 17.30 +/- 9.66 ng/ml, after achieved remission 26.43 +/- 11.25 ng/ml and in the control group mean serum BDNF levels of 25.68 +/- 7.76 ng/ml.