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使用赖脯胰岛素的改良高胰岛素血症、正常血糖和低血糖钳夹技术用于胰岛素瘤诊断。

Modified hyperinsulinaemic, eu- and hypoglycaemic clamp technique using lispro-insulin for insulinoma diagnostic.

作者信息

Roudovitch N, Nauck M A, Schatz H, Pfeiffer A F

机构信息

Division of Endocrinology Department of Medicine, Clinic B. Franklin, Free University of Berlin, Germany.

出版信息

Exp Clin Endocrinol Diabetes. 2001;109(8):397-401. doi: 10.1055/s-2001-18992.

Abstract

Characterization of metabolically inadequate insulin secretion is essential for insulinoma diagnostics. Hyperinsulinaemic, eu- and hypoglycaemic clamp procedures have been used to suppress endogenous insulin secretion in healthy subjects. The use of exogenous insulin precluded the use of insulin as a parameter to be measured. We now suggest to use exogenous insulin lispro and an insulin-specific ELISA not cross reacting with insulin lispro. Thus, determination of insulin by ELISA in this experimental setting reflects endogenous insulin. A 39-year-old man with a surgically confirmed pancreatic insulinoma was studied under hyperinsulinaemic [lispro insulin 40 mU x m(-2) body surface x min(-1)] clamp conditions. Euglycaemia was achieved (3.8 +/- 0.5 mmol/L) for 1 h and hypoglycaemia (2.36 +/- 0.49 mmol/L) was achieved for another 30 min. Insulin was evaluated by ELISA (cross-reaction with lispro insulin < 0.006%, C-peptide < 0.01%, proinsulin < 0.001%) and by a nonselective RIA (cross-reaction with proinsulin 40%). In control subjects the euglycaemic hyperinsulinaemia suppressed C-peptide to 0.36 +/- 0.03 ng/ml and hypoglycaemic hyperinsulinaemia to 0.29 +/- 0.03 ng/ml. Endogenous insulin was suppressed to 2.8 +/- 0.03 mU/L under euglycaemia and to 2.6 +/- 0.03 mU/L under hypoglycaemia in control subjects. In the insulinoma patient apparently irregular but small changes in both C-peptide (1.43 +/- 0.1 ng/ml) and more pronounced changes in endogenous insulin concentrations 4.41 +/- 0.1 mU/l under euglycaemia and 5.35 +/- 0.3 mU/l under hypoglycaemic conditions, were observed. The basal level of insulin (ELISA insulin 4.6 mU/L) and C-peptide (1.7 ng/ml) were not markedly elevated. Determination of insulin allowed better characterization of irregular pulses because of the shorter half-life of insulin relative to C-peptide. The new modification of sequential eu- and hypoglycaemic clamp procedures should also be useful in pharmacological studies of insulinotropic substances. Direct measurement of peripheral insulin may be more sensitive than C-peptide to detect low levels of autonomous insulin secretion in small insulinomas.

摘要

代谢性胰岛素分泌不足的特征对于胰岛素瘤的诊断至关重要。高胰岛素血症、正常血糖和低血糖钳夹程序已被用于抑制健康受试者的内源性胰岛素分泌。外源性胰岛素的使用排除了将胰岛素作为测量参数的可能性。我们现在建议使用外源性赖脯胰岛素和一种与赖脯胰岛素无交叉反应的胰岛素特异性酶联免疫吸附测定法(ELISA)。因此,在这种实验环境中通过ELISA测定胰岛素反映的是内源性胰岛素。一名经手术确诊为胰腺胰岛素瘤的39岁男性在高胰岛素血症[赖脯胰岛素40 mU×m(-2)体表面积×min(-1)]钳夹条件下接受研究。实现正常血糖(3.8±0.5 mmol/L)1小时,然后实现低血糖(2.36±0.49 mmol/L)30分钟。通过ELISA(与赖脯胰岛素的交叉反应<0.006%,C肽<0.01%,胰岛素原<0.001%)和非选择性放射免疫分析法(RIA)(与胰岛素原的交叉反应40%)评估胰岛素。在对照受试者中,正常血糖高胰岛素血症将C肽抑制至0.36±0.03 ng/ml,低血糖高胰岛素血症将其抑制至0.29±0.03 ng/ml。在对照受试者中,正常血糖时内源性胰岛素被抑制至2.8±0.03 mU/L,低血糖时被抑制至2.6±0.03 mU/L。在胰岛素瘤患者中,观察到C肽(1.43±0.1 ng/ml)有明显不规则但较小的变化,内源性胰岛素浓度变化更明显,正常血糖时为4.41±0.1 mU/l,低血糖时为5.35±0.3 mU/l。胰岛素(ELISA胰岛素4.6 mU/L)和C肽(1.7 ng/ml)的基础水平没有明显升高。由于胰岛素的半衰期相对于C肽较短,胰岛素的测定能够更好地表征不规则脉冲。正常血糖和低血糖钳夹程序的新改进在促胰岛素物质的药理学研究中也应该是有用的。直接测量外周胰岛素在检测小胰岛素瘤中低水平的自主性胰岛素分泌方面可能比C肽更敏感。

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