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Treatment of Diabetic Rats With Insulin or a Synthetic Insulin Receptor Agonist Peptide Leads to Divergent Metabolic Responses

机译:用胰岛素或合成的胰岛素受体激动剂肽治疗糖尿病大鼠可引起不同的代谢反应

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摘要

In addition to lowering of blood glucose, treatment with insulin also induces lipid synthesis and storage. Patients with type 2 diabetes often suffer from lipid-related comorbidities including dyslipidemia, obesity, and fatty liver disease. We examined here in two separate studies changes in lipid dynamics in Zucker diabetic fatty (ZDF) rats, in response to 7 days of treatment with either insulin or the insulin receptor agonist peptide S597. In concert with blood glucose normalization, the treated rats displayed large increases in hepatic de novo lipid synthesis and deposition of newly synthesized lipids in adipose tissue depots, accompanied by weight gain and expansion of adipose depots. In both treatment groups, heavy water labeling revealed that after 2 h (study A), de novo lipogenesis was responsible for 80% of newly stored hepatic triglyceride (TG)-palmitate, and after 5 days (study B), ~60% of newly deposited TG-palmitate in adipose tissues originated from this pathway. Interestingly, in both studies, treatment with the insulin mimetic peptide resulted in significantly lower blood TG levels, plasma TG production rates, and hepatic de novo synthesized fatty acid in plasma TG compared with insulin. There were no differences in plasma TG turnover (clearance rate) in response to either treatment, consistent with differential actions on the liver. These results show that in ZDF rats, treatment with a synthetic insulin-receptor-activating peptide or with insulin to lower blood glucose is accompanied by different effects on hepatic lipid anabolism and blood TG profiles.
机译:除了降低血糖外,用胰岛素治疗还可以诱导脂质合成和储存。 2型糖尿病患者经常患有与脂质相关的合并症,包括血脂异常,肥胖和脂肪肝。我们在两项单独的研究中检查了Zucker糖尿病脂肪(ZDF)大鼠中脂质动力学的变化,这些变化是对使用胰岛素或胰岛素受体激动剂肽S597治疗7天的反应。与血糖正常化相一致,经治疗的大鼠在肝脏新生脂质的合成和新合成脂质在脂肪组织贮库中的沉积显着增加,伴随着体重增加和脂肪贮库的扩张。在两个治疗组中,重水标记均显示,在2小时后(研究A),新生脂肪形成占新储存的肝硬脂酸甘油三酯(TG)的80%,在5天后(研究B),约60%的脂肪形成。源自该途径的新沉积的TG-棕榈酸酯在脂肪组织中。有趣的是,在两项研究中,与胰岛素相比,用胰岛素模拟肽治疗可显着降低血浆TG中的血液TG水平,血浆TG生成速率和肝脏从头合成的脂肪酸。两种疗法对血浆TG的转化率(清除率)均无差异,这与对肝脏的不同作用相一致。这些结果表明,在ZDF大鼠中,用合成的胰岛素受体激活肽或胰岛素治疗以降低血糖,对肝脂质合成代谢和血液TG谱有不同的影响。

著录项

  • 来源
    《Diabetes》 |2015年第3期|1057-1066|共10页
  • 作者单位

    Department of Nutritional Sciences and Toxicology, University of California, Berkeley, Berkeley, CA,Department of Insulin Biology, Novo Nordisk, Maaloev, Denmark;

    Department of Insulin Biology, Novo Nordisk, Maaloev, Denmark;

    Department of Insulin Pharmacology, Novo Nordisk, Maaloev, Denmark;

    Department of Insulin Biology, Novo Nordisk, Maaloev, Denmark;

    Department of Insulin Pharmacology, Novo Nordisk, Maaloev, Denmark;

    Department of Nutritional Sciences and Toxicology, University of California, Berkeley, Berkeley, CA;

    Department of Nutritional Sciences and Toxicology, University of California, Berkeley, Berkeley, CA,KineMed, Inc., Emeryville, CA;

  • 收录信息 美国《科学引文索引》(SCI);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

  • 入库时间 2022-08-18 03:46:12

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