酮症倾向2型糖尿病：高血糖对β细胞功能和骨骼肌胰岛素信号传导的影响

Ketosis-prone type 2 diabetes: effect of hyperglycemia on beta-cell function and skeletal muscle insulin signaling.

作者信息

Umpierrez Guillermo E, Smiley Dawn, Gosmanov Aidar, Thomason Donald

机构信息

Department of Medicine, Emory University School of Medicine, Atlanta, Georgia.

出版信息

Endocr Pract. 2007 May-Jun;13(3):283-90. doi: 10.4158/EP.13.3.283.

DOI:10.4158/EP.13.3.283

PMID:17599861

Abstract

OBJECTIVE

To determine the underlying mechanism for the severe and transient beta-cell dysfunction and impaired insulin action in obese African American patients with ketosis-prone diabetes.

METHODS

The effect of sustained hyperglycemia (glucotoxicity) and increased free fatty acids (lipotoxicity) on beta-cell function was assessed by changes in insulin secretion during a 20-hour glucose (200 mg/m2 per minute) and a 48-hour Intralipid (40 mL/h) infusion, respectively. Insulin-activated signaling pathways and pattern of Akt-1 and Akt-2 expression and insulin-stimulated phosphorylation were analyzed in skeletal muscle biopsy specimens. Studies were performed in an obese African American woman within 48 hours after resolution of diabetic ketoacidosis and 1 week after discontinuation of insulin treatment.

RESULTS

Dextrose infusion rapidly increased C-peptide levels from a baseline of 3.2 ng/mL to a mean of 7.1 +/- 0.5 ng/mL during the first 8 hours of infusion; thereafter, C-peptide levels progressively declined. Lipid infusion was not associated with any deleterious effect on insulin and C-peptide secretion. Initial in vitro stimulation of muscle tissue with insulin resulted in a substantial and selectively decreased Akt-2 expression and insulin-stimulated phosphorylation on the serine residue. Improved metabolic control resulted in 70% greater Akt expression at near-normoglycemic remission in comparison with the period of hyperglycemia.

CONCLUSION

Hyperglycemia, but not increased free fatty acid levels, led to progressive beta-cell dysfunction and impaired insulin secretion. Hyperglycemia was also associated with diminished skeletal muscle Akt expression and phosphorylation in an African American woman with ketosis-prone diabetes, and this defect improved notably with aggressive insulin therapy. These results indicate the importance of glucose toxicity in the pathogenesis of ketosis-prone diabetes in obese African American patients.

摘要

目的

确定易发生酮症的肥胖非裔美国糖尿病患者出现严重且短暂的β细胞功能障碍及胰岛素作用受损的潜在机制。

方法

分别通过20小时葡萄糖（每分钟200 mg/m²）输注和48小时脂肪乳（40 mL/h）输注期间胰岛素分泌的变化，评估持续性高血糖（糖毒性）和游离脂肪酸增加（脂毒性）对β细胞功能的影响。在骨骼肌活检标本中分析胰岛素激活的信号通路以及Akt-1和Akt-2的表达模式和胰岛素刺激的磷酸化情况。研究在一名肥胖非裔美国女性患者身上进行，该患者在糖尿病酮症酸中毒缓解后48小时内且胰岛素治疗中断1周后接受检查。

结果

葡萄糖输注在输注的前8小时内迅速将C肽水平从基线的3.2 ng/mL提高到平均7.1±0.5 ng/mL；此后，C肽水平逐渐下降。脂肪乳输注未对胰岛素和C肽分泌产生任何有害影响。最初用胰岛素对肌肉组织进行体外刺激导致Akt-2表达大幅且选择性降低，以及丝氨酸残基上胰岛素刺激的磷酸化减少。与高血糖期相比，改善代谢控制使接近正常血糖缓解时的Akt表达增加了70%。