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非肥胖型2型糖尿病患者β细胞功能的进行性恶化。餐后血浆C肽水平是胰岛素依赖的一个指标。

Progressive deterioration of beta-cell function in nonobese type 2 diabetic subjects. Postprandial plasma C-peptide level is an indication of insulin dependency.

作者信息

Prando R, Odetti P, Melga P, Giusti R, Ciuchi E, Cheli V

机构信息

Department of Internal Medicine, University of Genoa, Italy.

出版信息

Diabetes Metab. 1996 Jun;22(3):185-91.

PMID:8697306
Abstract

The purpose of the present study was to characterize secondary failure (SF) to oral hypoglycaemic agents by assessment of threshold insulin-secretion values in relation to diabetes duration. One hundred and forty-seven nonobese diabetic patients, 35 to 80 years of age, with disease duration ranging from 1 to 36 years, were studied. Beta-cell function was assessed by meal-stimulated (delta CP) and glucagon-stimulated (delta aCP) C-peptide concentrations. The quality of glycaemic control was considered good if mean daily blood glucose was less than 8.5 mmol/l. One group with good (NOb-GC) and another with poor control (NOb-SF) were established. Mean daily glycaemia was negatively correlated with delta CP or delta aCP (r = -0.703 vs r = -0.696; p < 0.001) more than with basal C-peptide (r = -0.453; p < 0.001). A close positive correlation between meal-stimulated (delta CP) and glucagon-stimulated (delta aCP) C-peptide concentrations was observed (r = 0.869; p < 0.001). Residual beta-cell function (delta CP and delta aCP) was significantly correlated with known disease duration in both groups (GC: r = -0.693 and SF: r = -0.680; p < 0.001). Nonobese patients with SF showed early impaired secretion during the first years of disease, meal-stimulated delta CP being below 0.350 mmol/l. The most useful result in this study was the incremental value of C-peptide (delta CP), which showed minimal overlapping between the two groups. Basal, postprandial or postglucagon absolute values were less discriminating. The daily profile allowed measurement of both glycaemic control and insulin production after a regular meal. The validity of this measurement was confirmed by the strong correlation between meal-stimulated and glucagon-stimulated delta C-peptide concentrations. This parameter is a useful physiological marker of secondary failure.

摘要

本研究的目的是通过评估与糖尿病病程相关的胰岛素分泌阈值来描述口服降糖药的继发性失效(SF)。研究了147例年龄在35至80岁之间、病程为1至36年的非肥胖糖尿病患者。通过进餐刺激(ΔCP)和胰高血糖素刺激(ΔaCP)的C肽浓度评估β细胞功能。如果平均每日血糖低于8.5 mmol/L,则认为血糖控制质量良好。设立了一组血糖控制良好(NOb-GC)和另一组控制不佳(NOb-SF)的患者。平均每日血糖与ΔCP或ΔaCP呈负相关(r = -0.703 vs r = -0.696;p < 0.001),比与基础C肽的相关性(r = -0.453;p < 0.001)更强。观察到进餐刺激(ΔCP)和胰高血糖素刺激(ΔaCP)的C肽浓度之间存在密切的正相关(r = 0.869;p < 0.001)。两组患者的残余β细胞功能(ΔCP和ΔaCP)均与已知病程显著相关(GC组:r = -0.693,SF组:r = -0.680;p < 0.001)。患有SF的非肥胖患者在疾病的最初几年就出现早期分泌受损,进餐刺激的ΔCP低于0.350 mmol/L。本研究中最有用的结果是C肽的增加值(ΔCP),它显示两组之间的重叠最小。基础、餐后或胰高血糖素刺激后的绝对值鉴别能力较差。每日血糖曲线允许测量常规餐后的血糖控制和胰岛素分泌。进餐刺激和胰高血糖素刺激的ΔC肽浓度之间的强相关性证实了该测量方法的有效性。该参数是继发性失效的有用生理标志物。

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