Ndisang Joseph Fomusi, Jadhav Ashok
Department of Physiology, University of Saskatchewan College of Medicine, 107 Wiggins Rd., Saskatoon, SK, Canada S7N 5E5.
Am J Physiol Endocrinol Metab. 2009 Apr;296(4):E829-41. doi: 10.1152/ajpendo.90783.2008. Epub 2009 Feb 3.
Hyperglycemia-induced oxidative stress is a common phenomenon in diabetes. Since oxidative stress depletes adiponectin and insulin levels, we investigated whether an upregulated heme oxygenase (HO) system would attenuate the oxidative destruction of adiponectin/insulin and improve insulin sensitivity and glucose metabolism in streptozotocin (STZ)-induced type 1 diabetes. HO was upregulated with hemin (15 mg/kg ip) or inhibited with chromium mesoporphyrin (CrMP, 4 micromol/kg ip). Administering hemin to STZ-diabetic rats reduced hyperglycemia and improved glucose metabolism, whereas the HO inhibitor CrMP annulled the antidiabetic effects and/or exacerbated fasting/postprandial hyperglycemia. Interestingly, the antidiabetic effects of hemin lasted for 2 mo after termination of therapy and were accompanied by enhanced HO-1 and HO activity of the soleus muscle, along with potentiation of plasma antioxidants like bilirubin, ferritin, and superoxide dismutase, with corresponding elevation of the total antioxidant capacity. Importantly, hemin abated c-Jun NH2-terminal kinase (JNK), a substance known to inhibit insulin biosynthesis, and suppressed markers/mediators of oxidative stress including 8-isoprostane, nuclear-factor (NF)-kappaB, activating protein (AP)-1, and AP-2 of the soleus muscle. Furthermore, hemin therapy significantly attenuated pancreatic histopathological lesions including acinar cell necrosis, interstitial edema, vacuolization, fibrosis, and mononuclear cell infiltration. Correspondingly, hemin increased plasma insulin and potentiated agents implicated in insulin sensitization and insulin signaling such as adiponectin, adenosine monophosphate-activated protein kinase (AMPK), cAMP, cGMP, and glucose transporter (GLUT)4, a protein required for glucose uptake. These were accompanied by improved glucose tolerance [intraperitoneal glucose tolerance text (IPGTT)], decreased insulin intolerance [intraperitoneal insulin tolerance test (IPITT)], and reduced insulin resistance [homeostasis model assessment of insulin resistance (HOMA-IR) index], whereas CrMP nullified the hemin-dependent antidiabetic and insulin-sensitizing effects. In conclusion, by concomitantly enhancing insulin and paradoxically potentiating insulin sensitivity, this study unveils a novel, unique, and long-lasting antidiabetic characteristic of upregulating HO with hemin that could be exploited against insulin-resistant and insulin-dependent diabetes.
高血糖诱导的氧化应激是糖尿病中的常见现象。由于氧化应激会消耗脂联素和胰岛素水平,我们研究了上调的血红素加氧酶(HO)系统是否会减弱脂联素/胰岛素的氧化破坏,并改善链脲佐菌素(STZ)诱导的1型糖尿病中的胰岛素敏感性和葡萄糖代谢。用氯高铁血红素(15 mg/kg腹腔注射)上调HO或用中卟啉铬(CrMP,4 μmol/kg腹腔注射)抑制HO。给STZ诱导的糖尿病大鼠注射氯高铁血红素可降低高血糖并改善葡萄糖代谢,而HO抑制剂CrMP则消除了抗糖尿病作用和/或加剧了空腹/餐后高血糖。有趣的是,氯高铁血红素的抗糖尿病作用在治疗终止后持续2个月,并伴有比目鱼肌HO-1和HO活性增强,以及血浆抗氧化剂如胆红素、铁蛋白和超氧化物歧化酶的增强,同时总抗氧化能力相应提高。重要的是,氯高铁血红素降低了已知会抑制胰岛素生物合成的c-Jun氨基末端激酶(JNK),并抑制了比目鱼肌氧化应激的标志物/介质,包括8-异前列腺素、核因子(NF)-κB、激活蛋白(AP)-1和AP-2。此外,氯高铁血红素治疗显著减轻了胰腺组织病理学病变,包括腺泡细胞坏死、间质水肿、空泡化、纤维化和单核细胞浸润。相应地,氯高铁血红素增加了血浆胰岛素,并增强了与胰岛素增敏和胰岛素信号传导相关的因子,如脂联素、腺苷单磷酸激活蛋白激酶(AMPK)、cAMP、cGMP和葡萄糖转运蛋白(GLUT)4,后者是葡萄糖摄取所需的蛋白质。这些伴随着葡萄糖耐量的改善[腹腔内葡萄糖耐量试验(IPGTT)]、胰岛素不耐受的降低[腹腔内胰岛素耐量试验(IPITT)]和胰岛素抵抗的降低[胰岛素抵抗稳态模型评估(HOMA-IR)指数],而CrMP则消除了氯高铁血红素依赖性的抗糖尿病和胰岛素增敏作用。总之,通过同时增强胰岛素并反常地增强胰岛素敏感性本研究揭示了用氯高铁血红素上调HO的一种新的、独特的和持久的抗糖尿病特性,可用于对抗胰岛素抵抗和胰岛素依赖型糖尿病。
