"Azasteroid" from_date:2012

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                            1
                            2022PDQ Cancer Information
                            not be assessed from these studies and that persistent use of these agents increased sexual and erectile dysfunction. The review was based on MEDLINE and Cochrane Collaboration Library computerized searches through June 2010 using the Medical Subject Headings terms and text words finasteride, dutasteride, neoplasms, azasteroids, reductase inhibitors, and enzyme inhibitors to identify randomized trials. Eight
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                            3
                            2014Health Technology Assessment (HTA) Database.
                            Review Analysis
                            Appears Promising
                            ?
                            %20and%20Finasteride%20Final.pdfIndexing StatusSubject indexing assigned by CRDMeSH5-alpha Reductase Inhibitors; Azasteroids; Finasterides; Prostatic HyperplasiaLanguage PublishedEnglishCountry of organisationCanadaProvince or stateOntarioEnglish summaryAn English language summary is available.Address for correspondenceCanadian Agency for Drugs and Technologies in Health (CADTH), 865 Carling Avenue
                            4
                            2012NHS Economic Evaluation Database.
                            Review Analysis
                            Appears Promising
                            ?
                            . Indexing StatusSubject indexing assigned by NLMMeSH5-alpha Reductase Inhibitors /administration & Adrenergic alpha-1 Receptor Antagonists /administration & Aged; Azasteroids /administration & Cost-Benefit Analysis; Drug Therapy, Combination; Dutasteride; Humans; Male; Markov Chains; Middle Aged; Prostatic Hyperplasia /drug therapy /economics; Sulfonamides /administration & dosage /economics; dosage
                            5
                            2018FP Notebook
                            . Definition (NCI) A synthetic 4-azasteroid compound. Finasteride competitively binds to and inhibits steroid type II 5-alpha-reductase in the prostate gland, liver, and skin, thereby interfering with the enzymatic conversion of testosterone to 5-dihydrotestosterone (DHT) and reducing serum DHT levels. The reduction in serum DHT levels results in diminished stimulation of androgen receptors . Definition (PDQ) A synthetic 4-azasteroid compound. Finasteride competitively binds to and inhibits steroid type II 5-alpha-reductase in the prostate gland, liver, and skin, thereby interfering with the enzymatic conversion of testosterone to 5-dihydrotestosterone (DHT) and reducing serum DHT levels. The reduction in serum DHT levels results in diminished stimulation of androgen receptors
                            6
                            2015FP Notebook
                            . Definition (NCI) A synthetic 4-azasteroid compound. Finasteride competitively binds to and inhibits steroid type II 5-alpha-reductase in the prostate gland, liver, and skin, thereby interfering with the enzymatic conversion of testosterone to 5-dihydrotestosterone (DHT) and reducing serum DHT levels. The reduction in serum DHT levels results in diminished stimulation of androgen receptors . Definition (PDQ) A synthetic 4-azasteroid compound. Finasteride competitively binds to and inhibits steroid type II 5-alpha-reductase in the prostate gland, liver, and skin, thereby interfering with the enzymatic conversion of testosterone to 5-dihydrotestosterone (DHT) and reducing serum DHT levels. The reduction in serum DHT levels results in diminished stimulation of androgen receptors
                            7
                            2012Cancer cell international
                            in order to determine the impact on proliferation, on distribution during the different phases of the cell cycle, and on apoptosis/necrosis. In addition, lung cancer cell lines were treated with 4-azasteroids, which specifically inhibit SRD5A1 activity, and the effects on proliferation were measured. Statistical analyses using ANOVA and post-hoc Tamhane-T2-test were performed. In the case of non /necrosis assay. Treatment of lung cancer cell lines with 4-azasteroids did not significantly inhibit proliferation. In summary, the results suggest that SRD5A1 is not a crucial enzyme for the sustained proliferation of NSCLC cell lines.