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Non Selective Inhibition of COX Activity Reversed Inflammation and Reactive Oxygen Radicals Mediated Prostate Cancer Risk and Decreased Disease Progression in Preclinical Model

Non Selective Inhibition of COX Activity Reversed Inflammation and Reactive Oxygen Radicals Mediated Prostate Cancer Risk and Decreased Disease Progression in Preclinical Model

作     者:Maxwell Omabe Kenneth Nwobini Omabe Clement Ademola Famurewa Alberta Egwu Okorocha Grace Maxwell Omabe Maxwell Omabe;Kenneth Nwobini Omabe;Clement Ademola Famurewa;Alberta Egwu Okorocha;Grace Maxwell Omabe

作者机构:Tumor Immunology Group Division of Oncology Cancer Research Division Department of Pathology and Laboratory Medicine University of Saskatchewan Saskatoon Canada Molecular Pathology and Cancer Biology Research Group Chemical Pathology Division Department of Medical Laboratory Sciences Faculty of Health Science Ebonyi State University Ebonyi Nigeria Department of Biochemistry and Molecular Biology Faculty of Natural Sciences Federal University Ndufu Alike Ikwo Nigeria Department of Medical Biochemistry Faculty of Basic Medical Sciences Federal University Ndufu Alike Ikwo Nigeria Department of Physiology Faculty of Basic Medical Sciences Ebonyi State University Ebonyi Nigeria 

出 版 物:《Journal of Cancer Therapy》 (癌症治疗(英文))

年 卷 期:2016年第7卷第1期

页      面:41-49页

学科分类:1002[医学-临床医学] 100214[医学-肿瘤学] 10[医学] 

主  题:Inflammation Prostate Cancer Reactive Oxygen Species 

摘      要:Prostate cancer (PCa) represents the most frequent urologic diagnosis in elderly males. We have previously shown that exposure of prostate to lipopolysaccharide (LPS) promotes cancer risk. We investigated the effect of non-selective cyclooxygenase (COX) inhibition on prostate inflammation-mediated cancer risk in vivo. The prostates of male rats were inoculated with E. coli as sources of inflammatory molecules (LPS) and were treated with COX inhibitor, aspirin 2 mg/Kg orally for 14 days or PBS. Oxidative stress was induced with two 2 mls of hydrogen peroxide orally twice daily or PBS for 14 days;they were either treated with COX inhibitor or PBS for another 14 days. Blood was collected and analyzed for acid phosphatase and PSA. Data showed presences of LPS in the prostate of the rats resulted in gradual increase in PSA when compared to control (P 2O2 had 2.5 fold increase in acid phosphatase (ACP) compared control (P 0.0001), and by inhiting COX activity, a statistically significant reduction in ACP from 11.2 IU/L ± 0.67 to 5.7 IU/L ± 0.347 (P 0.0034) was observed. Thus since increased in PSA was associated to cancer risk, our data suggested that inflammation mediated prostate cancer risk was reversible by Inhibition of COX Activity in rats.

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