The Effect of Long-Term Tamsulosin Monotherapy and Tamsulosin - Dutasteride Combination Therapy on PKC-α Enzyme Expression in Prostate Stromal Tissue.

Besut Daryanto, Athaya Febriantyo Purnomo, Yulian Salis Patriawan, Basuki Bambang Purnomo
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Abstract

Background: The α-adrenergic receptor antagonist is the most effective medical therapy to reduce the dynamic component in patients with BPH. However, long-term administration of receptor antagonists can cause upregulation of mRNA receptor expression, resulting in tolerance of drug effectiveness. PKC-α is involved in the process of prostate smooth muscle contraction through activation of the voltage-gated Ca2+ conducted canal, influenced by androgen hormones, especially testosterone, and has an isoform with Twist1, a transcription factor that plays a role in up-regulation of androgen receptors.

Objective: The aim of the study was to compare the effect of long-term tamsulosin monotherapy and tamsulosin - dutasteride combination therapy in PKC-α enzyme expression in prostate stromal tissue of Rattus norvegicus rats of Wistar strain.

Methods: Out of 80 samples of Rattus norvegicus rats were divided into 8 groups with different interventions: negative control group, positive control group, tamsulosin monotherapy administration for 1 day, 3 day, and 6 day groups, and tamsulosin - dutasteride combination therapy for 1 day, 3 day, and 6 day groups. BPH was induced with 3 mg/kg of testosterone proprionate for 3 weeks, continued with drugs administration according to intervention grouping. Prostate stromal tissue was taken and prepared for PKC-α enzyme measurement with ELISA method.

Results: There was a significant difference (p<0.05) in the effect of tamsulosin monotherapy and tamsulosin-dutasteride combination therapy on the PKC-α expression. There was a strong positive relationship between the duration of tamsulosin-dutasteride combination therapy on the PKC-α expression, which means the longer the duration of the combination of tamsulosin-dutasteride combination the higher the PKC-α expression.

Conclusion: Administration of long-term tamsulosin - dutasteride combination therapy causes upregulation PKC-α expression more than tamsulosin only.

长期坦索罗辛单药治疗和坦索罗辛-度他雄胺联合治疗对前列腺基质组织中PKC-α酶表达的影响
背景:α-肾上腺素能受体拮抗剂是减少良性前列腺增生症患者动态成分的最有效药物疗法。然而,长期服用受体拮抗剂会引起 mRNA 受体表达上调,导致药物疗效耐受。PKC-α 通过激活电压门控 Ca2+ 传导管参与前列腺平滑肌收缩过程,受雄性激素(尤其是睾酮)的影响,并与在雄性激素受体上调过程中发挥作用的转录因子 Twist1 存在同工型:研究目的:比较长期坦索罗辛单药治疗和坦索罗辛-度他雄胺联合治疗对Wistar品系诺维格大鼠前列腺基质组织中PKC-α酶表达的影响:将80只大鼠分为8组,分别进行不同的干预:阴性对照组,阳性对照组,坦索罗辛单药治疗1天、3天和6天组,坦索罗辛-度他雄胺联合治疗1天、3天和6天组。用 3 mg/kg 丙酸睾酮诱导良性前列腺增生症,持续 3 周,然后按照干预组别继续用药。取前列腺基质组织,用 ELISA 法检测 PKC-α 酶:结果:PKC-α酶与前列腺基质组织中的PKC-α酶有明显差异(p长期服用坦索罗辛-度他雄胺联合疗法比仅服用坦索罗辛更能上调 PKC-α 的表达。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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