厄贝沙坦对胰岛素抵抗 JCR:LA-cp 大鼠肾脏和心脏损伤的减轻作用。
Irbesartan-mediated reduction of renal and cardiac damage in insulin resistant JCR : LA-cp rats.
机构信息
Alberta Institute for Human Nutrition, University of Alberta, Edmonton, Canada.
出版信息
Br J Pharmacol. 2009 Nov;158(6):1588-96. doi: 10.1111/j.1476-5381.2009.00417.x. Epub 2009 Oct 8.
BACKGROUND AND PURPOSE
Angiotensin II receptor antagonists (ARBs), originally developed for antihypertensive properties, have pleiotropic effects including direct vascular actions. We tested the hypothesis that the ARB irbesartan would be effective against micro- and macrovascular complications of the prediabetic metabolic syndrome using the obese, insulin-resistant JCR : LA-cp rat that exhibits micro- and macrovascular disease with ischaemic myocardial lesions and renal disease.
EXPERIMENTAL APPROACH
Obese male rats were treated with irbesartan (30 mg.kg(-1).day(-1), incorporated into chow) from 12 to 25 weeks of age.
KEY RESULTS
Irbesartan treatment caused no change in food intake or body weight. Fasting glycaemic control of the JCR : LA-cp rats was marginally improved, at the expense of increased plasma insulin levels ( approximately 50%). Fasting plasma triglycerides were marginally reduced ( approximately 25%), while cholesterol concentrations were unchanged. Elevated concentrations of adiponectin, monocyte chemotactic protein-1 and plasminogen activator inhibitor-1 were reduced along with severity of glomerular sclerosis. Macrovascular dysfunction (aortic hypercontractile response to noradrenergic stimulus and reduced endothelium-dependent relaxation) was improved and frequency of ischaemic myocardial lesions reduced (62%).
CONCLUSIONS AND IMPLICATIONS
Irbesartan reduces markers of inflammation and prothombotic status, improves macrovascular function and reduces glomerular sclerosis and myocardial lesions in a model of the metabolic syndrome. Unlike pharmaceutical agents targeted on metabolic dysfunction, irbesartan reduced end-stage disease without major reduction of plasma lipids or insulin. The protective effects appear to be secondary to unknown intracellular mechanisms, probably involving signal transduction pathways. Understanding these would offer novel pharmaceutical approaches to protection against cardiovascular disease.
背景与目的
血管紧张素Ⅱ受体拮抗剂(ARB)最初是为了降压特性而开发的,具有多种作用,包括直接的血管作用。我们使用肥胖、胰岛素抵抗的 JCR:LA-cp 大鼠来检验这样一个假说,即 ARB 厄贝沙坦对糖尿病前期代谢综合征的微血管和大血管并发症会有疗效,这种大鼠会发生微血管和大血管疾病,伴有缺血性心肌损伤和肾脏疾病。
实验方法
12 到 25 周龄的肥胖雄性大鼠给予厄贝沙坦(30 mg.kg(-1).day(-1),掺入饲料中)治疗。
主要结果
厄贝沙坦治疗没有改变食物摄入或体重。JCR:LA-cp 大鼠的空腹血糖控制略有改善,但代价是血浆胰岛素水平升高(约 50%)。空腹血浆甘油三酯略有降低(约 25%),而胆固醇浓度不变。高浓度的脂联素、单核细胞趋化蛋白-1 和纤溶酶原激活物抑制剂-1 随着肾小球硬化程度的加重而降低。大血管功能障碍(去甲肾上腺素刺激引起的主动脉高收缩反应和内皮依赖性舒张功能降低)得到改善,缺血性心肌损伤的发生率降低(62%)。
结论和意义
厄贝沙坦降低了炎症和促血栓形成状态的标志物,改善了大血管功能,减少了代谢综合征模型中的肾小球硬化和心肌损伤。与针对代谢功能障碍的药物不同,厄贝沙坦在没有明显降低血脂或胰岛素的情况下减少了终末期疾病。这些保护作用似乎是未知的细胞内机制的继发作用,可能涉及信号转导途径。了解这些机制将为预防心血管疾病提供新的药物治疗方法。
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