辛伐他汀与omega-3及其联合用药对肥胖雄性Wistar大鼠的抗肥胖作用

Rasha Aljuboury, N. Al-Shawi
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引用次数: 2

摘要

减少肥胖的战略已成为世界各地许多卫生机构和卫生工作人员的主要优先事项,因为肥胖的流行率在世界大部分地区上升并加剧,主要原因是现代生活方式往往更久坐不动,吃不健康的西式快餐越来越多。许多年前,降脂药物辛伐他汀;omega-3被认为是一种传统的降脂药物,有充分的证据证明它具有抗炎、保护心脏和降低甘油三酯的特性;两者合用可能在降低患者甘油三酯和总胆固醇治疗动脉粥样硬化方面具有互补作用。许多先前的研究已经发现辛伐他汀和omega-3的其他有益作用;因为辛伐他汀可以用于治疗阿尔茨海默病;预防前列腺癌;最近的研究表明,omega - 3除了可以预防肥胖之外还可以降低心脏性猝死的风险。但是,辛伐他汀单独或与omega-3联合作为潜在的抗肥胖治疗和/或预防肥胖的作用,尚不清楚它们对产热因素的影响。本研究采用实时荧光定量PCR技术评估辛伐他汀对包括UCP1在内的产热基因的影响,同时采用免疫组化方法检测iBAT和iWAT脂肪细胞中解偶联蛋白1 (UCP1)蛋白的表达。方法雄性Wistar大鼠120只(5 ~ 6周龄,体重100 ~ 150g),分为5组,分别给予辛伐他汀、omega-3和混合治疗两种不同剂量,高脂饮食组作为对照组。治疗时间为8周。每组每周取3只大鼠,沿60天采集肩胛间棕色脂肪组织(iBAT)和腹股沟白色脂肪组织(iWAT)。结果;辛伐他汀和omega-3对ucp1基因具有明显的激活作用,这反映了肥胖高脂饮食大鼠脂肪组织产热过程的增加,与单独服用辛伐他汀9mg/ kg /天相比,两者联合使用可协同增加产热机制。结论本研究为辛伐他汀单用或与omega-3联合应用抗肥胖提供了希望;通过增强白色和棕色脂肪组织的产热性,从而减轻体重。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Anti-obesity effect of simvastatin and omega-3 and its combination on obese model male Wistar rats
      Strategies to reduce obesity have become main priority for many health institution and health staff around the world, as the prevalence of obesity has risen and exacerbated in most of the world mainly because of the modern life style which tend to be more sedentary with an increase eating unhealthy fast western food. Many years ago, the lipid-lowering drug simvastatin; and omega-3 were considered as a traditional lipid-lowering drug that have been well-documented to possess anti-inflammatory, cardioprotective and triglyceride-lowering properties; and their co-administration may demonstrate a complementary effect in lowering patients' triglycerides and total cholesterol to treat atherosclerosis. Many previous studies have been found other beneficial effects for simvastatin, and omega-3; since, simvastatin can be used for the treatment of Alzheimer's disease; and for prevention of prostate cancer; while omega 3 can reduce the risk of sudden cardiac death in addition to preventing obesity that has been documented by recent studies. But, the effect of simvastatin alone or its combination with omega-3 as potential anti-obesity therapy and /or protection against obesity is not yet known through their effects on thermogenic factors. Aim of the study is to evaluate the effect of simvastatin on thermogenic genes including (UCP1) using quantitative real time PCR, while the expression of uncoupling protein 1 (UCP1) protein was detected in iBAT and iWAT adipocyte by immunohistochemistry. Method One hundred twenty (120) male Wistar rats (five-six week age and weighing 100-150g) were allocated into five groups: treated with two different doses of simvastatin, omega-3 and mixed treatment, in addition to high fat diet group which considered as a control group. Treatments were given for eight weeks. Three rats from each group were weekly-authenticated along the 60 days interscapular brown adipose tissue (iBAT) and inguinal white adipose tissues (iWAT) were obtained. Results; showed that simvastatin and omega-3 have an obvious activation of UCP1genes, this reflects an increase in thermogenic process in adipose tissue in obese high fat diet rats and their combination exert a synergistic increase in the thermogenic mechanism when compared to simvastatin 9mg/ kg /day alone. Conclusion this study gives a hope for the utilization of simvastatin either alone or in combination with omega-3 as anti-obesity therapy; through their enhancement of thermogenic in white and brown adipose tissues with a consequent weight loss.
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