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普兰林肽对健康受试者低血糖症状、儿茶酚胺及胰高血糖素反应的影响。

Effect of pramlintide on symptom, catecholamine, and glucagon responses to hypoglycemia in healthy subjects.

作者信息

Heise Tim, Heinemann Lutz, Heller Simon, Weyer Christian, Wang Yan, Strobel Susan, Kolterman Orville, Maggs David

机构信息

Profil Institute for Metabolic Research, Neuss, Germany.

出版信息

Metabolism. 2004 Sep;53(9):1227-32. doi: 10.1016/j.metabol.2004.04.010.

Abstract

Pramlintide is an analog of the human glucoregulatory hormone amylin. Previous studies have shown no clear evidence that pramlintide modifies the response to insulin-induced hypoglycemia; however, a detailed assessment of responses at hypoglycemic thresholds has not been conducted. To further test the effect of pramlintide on symptom, catecholamine, and glucagon responses, a 3-step hypoglycemic clamp was investigated in healthy volunteers. In a randomized, double-blind, placebo-controlled, crossover study, 18 healthy subjects without diabetes received subcutaneous premeal injections of either placebo or 60 microg pramlintide 3 times daily for 5 consecutive days. On day 6, subjects received study drug with breakfast and, after a 7-hour fast, were connected to a Biostator for a 3-step, 3-hour clamp experiment (insulin infusion rate: 1.0 mU/kg/min; blood glucose targets: 70, 55, and 45 mg/dL). An intravenous (IV) infusion of pramlintide (16 microg/h) or placebo was initiated at t = 60 minutes. At the end of each 60-minute clamp step, autonomic (sweating, palpitations, hunger, etc) and neuroglycopenic (confusion, headache, odd behavior, etc) symptoms were assessed using a validated visual analog scale questionnaire. Blood samples were collected at 30-minute intervals for measurement of plasma glucose, insulin, pramlintide, catecholamine, and glucagon concentrations. Intraindividual and group mean responses showed that autonomic symptoms and plasma catecholamine and glucagon concentrations increased progressively during the clamp, with no discernible differences between pramlintide and placebo treatments. Group means for catecholamines at 60 minutes were: epinephrine 233 +/- 42, 892 +/- 85, 2,340 +/- 302 and 202 +/- 25, 774 +/- 114, 2,751 +/- 404 pg/mL and norepinephrine 1,138 +/- 86, 1,236 +/- 77, 1,721 +/- 158 and 1,278 +/- 108, 1,259 +/- 109, 1,580 +/-136 pg/mL (+/- SEM) for placebo- and pramlintide-treated groups at 70, 55, and 45 mg/dL glucose, respectively. Group means for glucagon were 72 +/- 6.3, 98 +/- 11.1, 130 +/- 14.7 and 63 +/- 3.6, 92 +/- 9.4, 120 +/- 16.0 pmol/L (+/- SEM) for placebo- and pramlintide-treated groups at 70, 55, and 45 mg/dL glucose, respectively. These results showed that pramlintide did not impair the symptom, catecholamine, and glucagon responses to insulin-induced hypoglycemia in healthy subjects.

摘要

普兰林肽是人体葡萄糖调节激素胰淀素的类似物。以往研究未发现明确证据表明普兰林肽会改变对胰岛素诱导的低血糖的反应;然而,尚未对低血糖阈值时的反应进行详细评估。为进一步测试普兰林肽对症状、儿茶酚胺和胰高血糖素反应的影响,在健康志愿者中开展了一项三步低血糖钳夹试验。在一项随机、双盲、安慰剂对照、交叉研究中,18名无糖尿病的健康受试者连续5天每天皮下餐前注射安慰剂或60微克普兰林肽3次。在第6天,受试者早餐时接受研究药物,禁食7小时后,连接到生物人工肾进行一项三步、3小时的钳夹试验(胰岛素输注速率:1.0 mU/kg/分钟;血糖目标:70、55和45 mg/dL)。在t = 60分钟时开始静脉输注普兰林肽(16微克/小时)或安慰剂。在每个60分钟的钳夹步骤结束时,使用经过验证的视觉模拟量表问卷评估自主神经症状(出汗、心悸、饥饿等)和神经低血糖症状(意识模糊、头痛、怪异行为等)。每隔30分钟采集血样,测量血浆葡萄糖、胰岛素、普兰林肽、儿茶酚胺和胰高血糖素浓度。个体内和组均值反应表明,钳夹期间自主神经症状以及血浆儿茶酚胺和胰高血糖素浓度逐渐升高,普兰林肽治疗组和安慰剂治疗组之间无明显差异。安慰剂治疗组和普兰林肽治疗组在血糖为70、55和45 mg/dL时,60分钟时儿茶酚胺的组均值分别为:肾上腺素233±42、892±85、2340±302和202±25、774±114、2751±404 pg/mL,去甲肾上腺素1138±86、1236±77、1721±158和1278±108、1259±109、1580±136 pg/mL(±标准误)。安慰剂治疗组和普兰林肽治疗组在血糖为70、55和45 mg/dL时,胰高血糖素的组均值分别为72±6.3、98±11.1、130±14.7和63±3.6、92±9.4、120±16.0 pmol/L(±标准误)。这些结果表明,普兰林肽不会损害健康受试者对胰岛素诱导的低血糖的症状、儿茶酚胺和胰高血糖素反应。

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