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输注生长抑素增加葡萄糖清除率的胰腺外效应。

Extrapancreatic effect of somatostatin infusion to increase glucose clearance.

作者信息

Bergman R N, Ader M, Finegood D T, Pacini G

出版信息

Am J Physiol. 1984 Sep;247(3 Pt 1):E370-9. doi: 10.1152/ajpendo.1984.247.3.E370.

Abstract

Constant intraportal insulin, coupled with variable intraportal glucagon, was used in the attempt to reestablish basal metabolic conditions in dogs during somatostatin (SRIF) infusion (0.8 micrograms X min-1 X kg-1). SRIF alone lowered glucose (G), insulin (I), and glucagon (GN) (G: 90 +/- 5 to 69 +/- 1 mg/dl; I: 18 +/- 4 to 4 +/- 1 microU/ml; GN: 257 +/- 52 to 168 +/- 40 pg/ml; P less than 0.05 or better). Hormone replacement. Hypoglycemia persisted (G at steady state, SS, 60-150 min): 12 +/- 3 mg/dl below basal; P = 0.006) despite intraportal insulin replacement (200 microU X min-1 X kg-1; insulin at basal: 14 +/- 1; at SS: 14 +/- 2 microU/ml; P greater than 0.9) and glucagon overreplacement (basal: 341 +/- 42; SS: 486 +/- 80 pg/ml; P less than 0.05). Glucose clearance was increased 65% above basal (P less than 0.0001). Insulin underreplacement. With a lower intraportal insulin infusion rate (50 microU X min-1 X kg-1), insulin fell from basal (10 +/- 2 microU/ml) to 4 +/- 1 microU/ml during steady state (P = 0.03). Glucose and glucose clearance were normalized to basal values (G: 85 +/- 3 mg/dl, P = 0.3; clearance: 5.7 +/- 0.5 ml X min-1 X kg-1; P = 0.2) with full glucagon replacement (basal: 281 +/- 120; SS: 264 +/- 80 pg/ml; P greater than 0.9). Thus, during constant SRIF infusion, normoglycemia was reattained when insulin was underreplaced via the portal vein. The failure to reattain euglycemia with normoinsulinemia was due to a SRIF-induced increase in extrahepatic glucose clearance. Insulin replacement and growth hormone (GH) infusion. GH (15 ng X min-1 X kg-1) partially reversed the hypoglycemia during SRIF, with full insulin replacement. The SRIF-induced increase in glucose clearance may be partially mediated by a decrease in GH.

摘要

在生长抑素(SRIF)输注(0.8微克×分钟⁻¹×千克⁻¹)期间,通过持续门静脉输注胰岛素并结合门静脉内可变剂量的胰高血糖素,试图在犬中重建基础代谢状态。单独使用SRIF可降低血糖(G)、胰岛素(I)和胰高血糖素(GN)水平(G:从90±5降至69±1毫克/分升;I:从18±4降至4±1微单位/毫升;GN:从257±52降至168±40皮克/毫升;P<0.05或更佳)。激素替代。尽管进行了门静脉内胰岛素替代(200微单位×分钟⁻¹×千克⁻¹;基础胰岛素水平:14±1;稳态时:14±2微单位/毫升;P>0.9)和胰高血糖素过量替代(基础值:341±42;稳态时:486±80皮克/毫升;P<0.05),低血糖仍持续存在(稳态时,60 - 150分钟的血糖水平:比基础值低12±3毫克/分升;P = 0.006)。葡萄糖清除率比基础值增加了65%(P<0.0001)。胰岛素替代不足。当门静脉内胰岛素输注速率较低(50微单位×分钟⁻¹×千克⁻¹)时,胰岛素在稳态期间从基础水平(10±2微单位/毫升)降至4±1微单位/毫升(P = 0.03)。在完全胰高血糖素替代(基础值:281±120;稳态时:264±80皮克/毫升;P>0.9)的情况下,葡萄糖和葡萄糖清除率恢复到基础值(G:85±3毫克/分升,P = 0.3;清除率:5.7±0.5毫升×分钟⁻¹×千克⁻¹;P = 0.2)。因此,在持续SRIF输注期间,如果通过门静脉进行胰岛素替代不足,可重新实现血糖正常。在正常胰岛素水平下未能恢复正常血糖是由于SRIF诱导的肝外葡萄糖清除率增加。胰岛素替代与生长激素(GH)输注。在完全胰岛素替代的情况下,GH(15纳克×分钟⁻¹×千克⁻¹)可部分逆转SRIF期间的低血糖。SRIF诱导的葡萄糖清除率增加可能部分由GH减少介导。

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