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首页> 外文期刊>Diabetes care >The Effect of DPT-1 Intravenous Insulin Infusion and Daily Subcutaneous Insulin on Endogenous Insulin Secretion and Postprandial Glucose Tolerance
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The Effect of DPT-1 Intravenous Insulin Infusion and Daily Subcutaneous Insulin on Endogenous Insulin Secretion and Postprandial Glucose Tolerance

机译:DPT-1静脉内胰岛素输注和日皮下胰岛素对内源性胰岛素分泌和后葡萄糖耐量的影响

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摘要

OBJECTIVETo investigate the effect of parenteral insulin therapy on endogenous insulin secretion in the Diabetes Prevention Trial-Type 1 (DPT-1).RESEARCH DESIGN AND METHODSIn the parenteral insulin arm of DPT-1, subjects without diabetes at high risk of future type 1 diabetes randomized to active treatment received a yearly 4-day intravenous insulin infusion (IV-I) and daily subcutaneous insulin (SC-I). To examine the effects of these insulin therapies on endogenous insulin secretion, C-peptide and glucose levels were compared during oral glucose tolerance tests (OGTTs) performed on and off IV-I and SC-I. Forty-six paired OGTTs were performed in 30 subjects from DPT-1 to determine the effect of IV-I. Twenty paired OGTTs were performed in 15 subjects from DPT-1 to determine the effect of SC-I.RESULTSIV-I suppressed fasting and OGTT-stimulated C-peptide (62% and 40%, respectively), and it significantly lowered fasting glucose (67.4 4.5 mg/dL during IV-I vs. 90.9 +/- 1.8 mg/dL off insulin; P < 0.05). By contrast, post-OGTT glucose levels were significantly higher during IV-I: Glucose during IV-I versus off insulin at 120 min was 203.9 +/- 15.1 vs. 151.6 +/- 10.2 mg/dL, respectively (P < 0.05); 49% of OGTTs became transiently diabetic (>200 mg/dL at 120 min) when receiving IV-I. Fasting glucose was significantly lower when receiving SC-I versus when off insulin (85 +/- 3 vs. 94 +/- 2 mg/dL, respectively; P < 0.05), but SC-I did not significantly alter fasting or OGTT-stimulated C-peptide compared with being off insulin.CONCLUSIONSThese data demonstrate that the IV-I used in the DPT-1 markedly suppressed endogenous insulin secretion, which was frequently associated with postprandial glucose intolerance. SC-I, however, did not.
机译:目的探讨注射胰岛素治疗对内源性胰岛素分泌的作用的糖尿病预防试验-1型(DPT-1)。研究设计和方法在库DPT-1的肠外胰岛素手臂,受试者没有在未来的1型糖尿病的高危人群糖尿病随机分配到治疗活性接收每年4天的静脉内输注胰岛素(IV-I)和每日皮下胰岛素(SC-I)。为了检查内源胰岛素分泌的胰岛素这些疗法的效果,C肽和葡萄糖水平期间开启和关闭IV-I和SC-I进行口服葡萄糖耐量试验(OGTTs)进行了比较。四十六个成对OGTTs是在30名受试者从DPT-1执行以确定的IV-I的效果。二十配对OGTTs在15名受试者从DPT-1执行以确定的效果SC-I.RESULTSIV-I抑制空腹和OGTT刺激的C-肽(分别为62%和40%,),它显著降低空腹血糖( 67.4 4.5毫克/分升时IV-I相对于90.9±1.8毫克/分升离胰岛素; P <0.05)。相反,后OGTT葡萄糖水平期间IV-I均显著更高:在葡萄糖IV-I相对于断胰岛素在120分钟是203.9 +/- 15.1 151.6对比10.2 +/-毫克/分升,分别为(P <0.05) ; OGTTs 49%接受IV-I时成为瞬时糖尿病(> 200毫克/分升,在120分钟)。空腹血糖接收SC-I相对于当断开时胰岛素被显著降低(85 +/- 3与94 +/- 2毫克/升,分别; P <0.05),但SC-I没有显著ALTER空腹或OGTT-刺激的C-肽与被关闭insulin.CONCLUSIONSThese数据相比较表明,IV-I在DPT-1显着抑制内源性胰岛素分泌,这是经常与餐后葡萄糖耐受不良相关的使用。 SC-I,但是,没有。

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