Chia Chee W, Carlson Olga D, Kim Wook, Shin Yu-Kyong, Charles Cornelia P, Kim Hee Seung, Melvin Denise L, Egan Josephine M
National Institute on Aging, Intramural Research Program, National Institutes of Health, Baltimore, Maryland, USA.
Diabetes. 2009 Jun;58(6):1342-9. doi: 10.2337/db08-0958. Epub 2009 Mar 10.
Glucose-dependent insulinotropic polypeptide (GIP), unlike glucagon-like peptide (GLP)-1, lacks glucose-lowering properties in patients with type 2 diabetes. We designed this study to elucidate the underlying pathophysiology.
Twenty-two insulin-naïve subjects with type 2 diabetes were given either synthetic human GIP (20 ng x kg(-1) x min(-1)) or placebo (normal saline) over 180 min, starting with the first bite of a mixed meal (plus 1 g of acetaminophen) on two separate occasions. Frequent blood samples were obtained over 6 h to determine plasma GIP, GLP-1, glucose, insulin, glucagon, resistin, and acetaminophen levels.
Compared with placebo, GIP induced an early postprandial increase in insulin levels. Intriguingly, GIP also induced an early postprandial augmentation in glucagon, a significant elevation in late postprandial glucose, and a decrease in late postprandial GLP-1 levels. Resistin and acetaminophen levels were comparable in both interventions. By immunocytochemistry, GIP receptors were present on human and mouse alpha-cells. In alphaTC1 cell line, GIP induced an increase in intracellular cAMP and glucagon secretion. CONCLUSIONS; GIP, given to achieve supraphysiological plasma levels, still had an early, short-lived insulinotropic effect in type 2 diabetes. However, with a concomitant increase in glucagon, the glucose-lowering effect was lost. GIP infusion further worsened hyperglycemia postprandially, most likely through its suppressive effect on GLP-1. These findings make it unlikely that GIP or GIP receptor agonists will be useful in treating the hyperglycemia of patients with type 2 diabetes.
与胰高血糖素样肽(GLP)-1不同,葡萄糖依赖性促胰岛素多肽(GIP)在2型糖尿病患者中缺乏降血糖特性。我们设计本研究以阐明其潜在的病理生理学机制。
22名未经胰岛素治疗的2型糖尿病受试者在两个不同的时间段,从第一口混合餐(加1克对乙酰氨基酚)开始,在180分钟内接受合成人GIP(20 ng·kg⁻¹·min⁻¹)或安慰剂(生理盐水)。在6小时内频繁采集血样以测定血浆GIP、GLP-1、葡萄糖、胰岛素、胰高血糖素、抵抗素和对乙酰氨基酚水平。
与安慰剂相比,GIP诱导餐后早期胰岛素水平升高。有趣的是,GIP还诱导餐后早期胰高血糖素升高、餐后晚期血糖显著升高以及餐后晚期GLP-1水平降低。两种干预措施下抵抗素和对乙酰氨基酚水平相当。通过免疫细胞化学检测,人和小鼠的α细胞上存在GIP受体。在αTC1细胞系中,GIP诱导细胞内cAMP增加和胰高血糖素分泌增加。结论:给予GIP以达到超生理血浆水平时,在2型糖尿病中仍具有早期、短暂的促胰岛素作用。然而,伴随着胰高血糖素的增加,降血糖作用丧失。GIP输注进一步使餐后高血糖恶化,最可能是通过其对GLP-1的抑制作用。这些发现表明GIP或GIP受体激动剂不太可能用于治疗2型糖尿病患者的高血糖。
Zotero 插件