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阿卡波糖对早期2型糖尿病患者餐后单核血细胞反应的影响:AI(I)DA研究

Effect of acarbose on postmeal mononuclear blood cell response in patients with early type 2 diabetes: the AI(I)DA study.

作者信息

Hanefeld M, Schaper F, Koehler C, Bergmann S, Ugocsai P, Stelzer J, Schmitz G

机构信息

Center for Clinical Studies, GWT Dresden, Dresden, Germany.

出版信息

Horm Metab Res. 2009 Feb;41(2):132-6. doi: 10.1055/s-0028-1119407. Epub 2009 Feb 12.

Abstract

So far little is known about how the antidiabetic drugs acting at the level of gastrointestinal mucosa may affect immune and cellular response to food intake. The following study investigated the association between acarbose treatment and postprandial metabolism, immune- and inflammatory activity in patients with early type 2 diabetes: The Acarbose action on low grade Inflammation and Immune response in type 2 Diabetes on Atherosclerosis risk (AIIDA) study. Middle-aged patients (n=87) with early type 2 diabetes (2 h-plasma-glucose >or=11.1 mmol/l and/or HbA1c >or=6.5%) and sub-clinical inflammation (leucocytes >or=6.2 GPt/l and/or hsCRP >or=1.0 mg/l) underwent a mixed meal load (527 kcal). Metabolic parameters and markers of subclinical inflammation were measured at fasting (0'), 2 h-postprandial (2-hpp) and 4-hpp before and after 20 weeks of treatment with acarbose or placebo. Leukocytes and lymphocytes excursion after 20 weeks of treatment was significantly reduced with acarbose 4 h after testmeal [GPt/l] (7.5 vs. 7; p<0.05; and 2.29 vs. 2.14; p<0.05, respectively). Acarbose had only marginal effects on pp glucose, FFA, triglycerides, and insulin excursion. Biomarkers of inflammation (hsCRP, MBL, and PAI1) were not affected by acarbose. Multivariate analysis reveals only baseline leukocytes and of acarbose as independent determinant of 4-h leucocytes excursion. Postprandial metabolic and inflammatory parameters were strongly interrelated. These results suggest pleiotropic effects of acarbose, which may contribute to its vasoprotective potentials.

摘要

迄今为止,关于作用于胃肠道黏膜水平的抗糖尿病药物如何影响对食物摄入的免疫和细胞反应,人们了解甚少。以下研究调查了阿卡波糖治疗与2型糖尿病早期患者餐后代谢、免疫和炎症活动之间的关联:阿卡波糖对2型糖尿病动脉粥样硬化风险的低度炎症和免疫反应的作用(AIIDA)研究。患有2型糖尿病早期(2小时血浆葡萄糖≥11.1 mmol/l和/或糖化血红蛋白≥6.5%)和亚临床炎症(白细胞≥6.2 GPt/l和/或高敏C反应蛋白≥1.0 mg/l)的中年患者(n = 87)接受了混合餐负荷(527千卡)。在使用阿卡波糖或安慰剂治疗20周前后,分别在空腹(0')、餐后2小时(2-hpp)和餐后4小时(4-hpp)测量代谢参数和亚临床炎症标志物。餐后20周治疗后,试验餐后4小时,阿卡波糖使白细胞和淋巴细胞的波动显著降低[GPt/l](分别为7.5对7;p<0.05;以及2.29对2.14;p<0.05)。阿卡波糖对餐后血糖、游离脂肪酸、甘油三酯和胰岛素波动仅有轻微影响。炎症生物标志物(高敏C反应蛋白、甘露聚糖结合凝集素和纤溶酶原激活物抑制剂1)不受阿卡波糖影响。多变量分析显示,只有基线白细胞和阿卡波糖是餐后4小时白细胞波动的独立决定因素。餐后代谢和炎症参数密切相关。这些结果表明阿卡波糖具有多效性作用,这可能有助于其血管保护潜力。

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