Garvey W T, Olefsky J M, Griffin J, Hamman R F, Kolterman O G
Diabetes. 1985 Mar;34(3):222-34. doi: 10.2337/diab.34.3.222.
We have studied the effects of 3 wk of continuous subcutaneous insulin infusion (CSII) on endogenous insulin secretion and action in a group of 14 type II diabetic subjects with a mean (+/-SEM) fasting glucose level of 286 +/- 17 mg/dl. Normal basal and postprandial glucose levels were achieved during insulin therapy at the expense of marked peripheral hyperinsulinemia. During the week of posttreatment evaluation, the subjects maintained a mean fasting glucose level of 155 +/- 11 mg/dl off insulin therapy, indicating a persistent improvement in carbohydrate homeostasis. Adipocyte insulin binding and in vivo insulin dose-response curves for glucose disposal using the euglycemic clamp technique were measured before and after therapy to assess the effect on receptor and postreceptor insulin action. Adipocyte insulin binding did not change. The insulin dose-response curve for overall glucose disposal remained right-shifted compared with age-matched controls, but the mean maximal glucose disposal rate increased by 74% from 160 +/- 14 to 278 +/- 18 mg/m2/min (P less than 0.0005). The effect of insulin treatment on basal hepatic glucose output was also assessed; the mean rate was initially elevated at 159 +/- 8 mg/m2/min but fell to 90 +/- 5 mg/m2/min in the posttreatment period (P less than 0.001), a value similar to that in control subjects. Endogenous insulin secretion was assessed in detail and found to be improved after exogenous insulin therapy. Mean 24-h integrated serum insulin and C-peptide concentrations were increased from 21,377 +/- 2766 to 35,584 +/- 4549 microU/ml/min (P less than 0.01) and from 1653 +/- 215 to 2112 +/- 188 pmol/ml/min (P less than 0.05), respectively, despite lower glycemia. Second-phase insulin response to an intravenous (i.v.) glucose challenge was enhanced from 170 +/- 53 to 1022 +/- 376 microU/ml/min (P less than 0.025), although first-phase response remained minimal. Finally, the mean insulin and C-peptide responses to an i.v. glucagon pulse were unchanged in the posttreatment period, but when glucose levels were increased by exogenous glucose infusion to approximate the levels observed before therapy and the glucagon pulse repeated, responses were markedly enhanced. Simple and multivariate correlation analysis showed that only measures of basal hepatic glucose output and the magnitude of the postbinding defect in the untreated state could be related to the respective fasting glucose levels in individual subjects.(ABSTRACT TRUNCATED AT 400 WORDS)
我们研究了连续3周皮下胰岛素输注(CSII)对14名II型糖尿病患者内源性胰岛素分泌及作用的影响,这些患者的平均(±标准误)空腹血糖水平为286±17mg/dl。胰岛素治疗期间实现了正常的基础和餐后血糖水平,但代价是显著的外周高胰岛素血症。在治疗后评估的一周内,受试者在未接受胰岛素治疗的情况下维持平均空腹血糖水平为155±11mg/dl,表明碳水化合物稳态持续改善。在治疗前后测量脂肪细胞胰岛素结合以及使用正常血糖钳夹技术测定葡萄糖处置的体内胰岛素剂量-反应曲线,以评估对受体及受体后胰岛素作用的影响。脂肪细胞胰岛素结合未发生变化。与年龄匹配的对照组相比,总体葡萄糖处置的胰岛素剂量-反应曲线仍向右偏移,但平均最大葡萄糖处置率从160±14增至278±18mg/m²/min,提高了74%(P<0.0005)。还评估了胰岛素治疗对基础肝葡萄糖输出的影响;平均速率最初升高至159±8mg/m²/min,但在治疗后期降至90±5mg/m²/min(P<0.001),该值与对照组相似。详细评估内源性胰岛素分泌,发现外源性胰岛素治疗后有所改善。尽管血糖较低,但平均24小时综合血清胰岛素和C肽浓度分别从21377±2766增至35584±4549μU/ml/min(P<0.01)和从1653±215增至2112±188pmol/ml/min(P<0.05)。静脉注射(i.v.)葡萄糖激发试验的第二相胰岛素反应从170±53增至1022±376μU/ml/min(P<0.025),尽管第一相反应仍很微小。最后,治疗后期静脉注射胰高血糖素脉冲后的平均胰岛素和C肽反应未改变,但当通过外源性葡萄糖输注使血糖水平升高至接近治疗前观察到的水平并重复胰高血糖素脉冲时,反应明显增强。简单和多变量相关分析表明,只有基础肝葡萄糖输出的测量值以及未治疗状态下结合后缺陷的程度与个体受试者各自的空腹血糖水平相关。(摘要截短至400字)
