Marchetti Piero, Lupi Roberto, Federici Massimo, Marselli Lorella, Masini Matilde, Boggi Ugo, Del Guerra Silvia, Patanè Giovanni, Piro Salvatore, Anello Marcello, Bergamini Ettore, Purrello Francesco, Lauro Renato, Mosca Franco, Sesti Giorgio, Del Prato Stefano
Department of Endocrinology and Metabolism, Metabolic Unit, University of Pisa, Pisa, Italy.
Diabetes. 2002 May;51(5):1419-24. doi: 10.2337/diabetes.51.5.1419.
Type 2 (non-insulin-dependent) diabetes results from decreased insulin action in peripheral target tissues (insulin resistance) and impaired pancreatic beta-cell function. These defects reflect both genetic components and environmental risk factors. Recently, the common Gly(972)-->Arg amino acid polymorphism of insulin receptor substrate 1 (Arg(972) IRS-1) has been associated with human type 2 diabetes. In this study, we report on some functional and morphological properties of isolated human islets carrying the Arg(972) IRS-1 polymorphism. Insulin content was lower in variant than control islets (94 +/- 47 vs. 133 +/- 56 microU/islet; P < 0.05). Stepwise glucose increase (1.7 to 16.7 mmol/l) significantly potentiated insulin secretion from control islets, but not Arg(972) IRS-1 islets, with the latter also showing a relatively lower response to glyburide and a significantly higher response to arginine. Proinsulin release mirrored insulin secretion, and the insulin-to-proinsulin ratio in response to arginine was significantly lower from Arg(972) IRS-1 islets than from control islets. Glucose utilization and oxidation did not differ in variant and wild-type islets at both low and high glucose levels. Electron microscopy showed that Arg(972) IRS-1 beta-cells had a severalfold greater number of immature secretory granules and a lower number of mature granules than control beta-cells. In conclusion, Arg(972) IRS-1 islets have reduced insulin content, impaired insulin secretion, and a lower amount of mature secretory granules. These alterations may account for the increased predisposition to type 2 diabetes in individuals carrying the Gly(972)-->Arg amino acid polymorphism of IRS-1.
2型(非胰岛素依赖型)糖尿病是由外周靶组织中胰岛素作用降低(胰岛素抵抗)和胰腺β细胞功能受损所致。这些缺陷反映了遗传因素和环境危险因素。最近,胰岛素受体底物1的常见甘氨酸(972)→精氨酸氨基酸多态性(精氨酸(972)IRS-1)已与人类2型糖尿病相关联。在本研究中,我们报告了携带精氨酸(972)IRS-1多态性的分离人胰岛的一些功能和形态学特性。变异型胰岛的胰岛素含量低于对照胰岛(94±47对133±56微单位/胰岛;P<0.05)。葡萄糖逐步增加(1.7至16.7毫摩尔/升)显著增强了对照胰岛的胰岛素分泌,但对精氨酸(972)IRS-1胰岛无此作用,后者对格列本脲的反应相对较低,对精氨酸的反应则显著较高。胰岛素原释放反映了胰岛素分泌,精氨酸(972)IRS-1胰岛对精氨酸反应的胰岛素与胰岛素原比值显著低于对照胰岛。在低葡萄糖水平和高葡萄糖水平下,变异型和野生型胰岛的葡萄糖利用和氧化均无差异。电子显微镜显示,精氨酸(972)IRS-1β细胞的未成熟分泌颗粒数量比对照β细胞多几倍,成熟颗粒数量则较少。总之,精氨酸(972)IRS-1胰岛的胰岛素含量降低、胰岛素分泌受损且成熟分泌颗粒数量较少。这些改变可能解释了携带IRS-1甘氨酸(972)→精氨酸氨基酸多态性的个体患2型糖尿病易感性增加的原因。
