Bugger Heiko, Boudina Sihem, Hu Xiao Xuan, Tuinei Joseph, Zaha Vlad G, Theobald Heather A, Yun Ui Jeong, McQueen Alfred P, Wayment Benjamin, Litwin Sheldon E, Abel E Dale
Division of Endocrinology, Metabolism, and Diabetes, Program in Human Molecular Biology and Genetics, University of Utah School of Medicine, Salt Lake City, Utah, USA.
Diabetes. 2008 Nov;57(11):2924-32. doi: 10.2337/db08-0079. Epub 2008 Aug 4.
Fatty acid-induced mitochondrial uncoupling and oxidative stress have been proposed to reduce cardiac efficiency and contribute to cardiac dysfunction in type 2 diabetes. We hypothesized that mitochondrial uncoupling may also contribute to reduced cardiac efficiency and contractile dysfunction in the type 1 diabetic Akita mouse model (Akita).
Cardiac function and substrate utilization were determined in isolated working hearts and in vivo function by echocardiography. Mitochondrial function and coupling were determined in saponin-permeabilized fibers, and proton leak kinetics was determined in isolated mitochondria. Hydrogen peroxide production and aconitase activity were measured in isolated mitochondria, and total reactive oxygen species (ROS) were measured in heart homogenates.
Resting cardiac function was normal in Akita mice, and myocardial insulin sensitivity was preserved. Although Akita hearts oxidized more fatty acids, myocardial O(2) consumption was not increased, and cardiac efficiency was not reduced. ADP-stimulated mitochondrial oxygen consumption and ATP synthesis were decreased, and mitochondria showed grossly abnormal morphology in Akita. There was no evidence of oxidative stress, and despite a twofold increase in uncoupling protein 3 (UCP3) content, ATP-to-O ratios and proton leak kinetics were unchanged, even after perfusion of Akita hearts with 1 mmol/l palmitate.
Insulin-deficient Akita hearts do not exhibit fatty acid-induced mitochondrial uncoupling, indicating important differences in the basis for mitochondrial dysfunction between insulin-responsive type 1 versus insulin-resistant type 2 diabetic hearts. Increased UCP3 levels do not automatically increase mitochondrial uncoupling in the heart, which supports the hypothesis that fatty acid-induced mitochondrial uncoupling as exists in type 2 diabetic hearts requires a concomitant increase in ROS generation.
脂肪酸诱导的线粒体解偶联和氧化应激被认为会降低心脏效率,并导致2型糖尿病患者出现心脏功能障碍。我们推测线粒体解偶联也可能导致1型糖尿病秋田小鼠模型(Akita)的心脏效率降低和收缩功能障碍。
通过超声心动图测定离体工作心脏的心脏功能和底物利用情况以及体内功能。在皂素通透化纤维中测定线粒体功能和解偶联情况,并在离体线粒体中测定质子泄漏动力学。在离体线粒体中测量过氧化氢生成量和乌头酸酶活性,在心脏匀浆中测量总活性氧(ROS)。
Akita小鼠静息时心脏功能正常,心肌胰岛素敏感性得以保留。尽管Akita小鼠心脏氧化更多脂肪酸,但心肌氧耗未增加,心脏效率也未降低。Akita小鼠中,ADP刺激的线粒体氧耗和ATP合成减少,线粒体形态明显异常。没有氧化应激的证据,尽管解偶联蛋白3(UCP3)含量增加了两倍,但即使在用1 mmol/l棕榈酸灌注Akita小鼠心脏后,ATP与氧的比值和质子泄漏动力学仍未改变。
胰岛素缺乏的Akita小鼠心脏未表现出脂肪酸诱导的线粒体解偶联,这表明胰岛素反应性1型糖尿病心脏与胰岛素抵抗性2型糖尿病心脏线粒体功能障碍的基础存在重要差异。UCP3水平升高不会自动增加心脏中的线粒体解偶联,这支持了以下假设:2型糖尿病心脏中存在的脂肪酸诱导的线粒体解偶联需要同时增加ROS生成。
Zotero 插件