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奥曲肽可逆转高胰岛素血症,并预防磺脲类药物过量引起的低血糖。

Octreotide reverses hyperinsulinemia and prevents hypoglycemia induced by sulfonylurea overdoses.

作者信息

Boyle P J, Justice K, Krentz A J, Nagy R J, Schade D S

机构信息

Department of Medicine, University of New Mexico School of Medicine, Albuquerque 87131-5271.

出版信息

J Clin Endocrinol Metab. 1993 Mar;76(3):752-6. doi: 10.1210/jcem.76.3.8445035.

Abstract

Emergency therapy of sulfonylurea overdoses with glucose is often unsatisfactory because glucose stimulates insulin release and initiates a need for escalating quantities of hypertonic glucose to maintain normoglycemia. We tested the hypothesis that octreotide, an analog of somatostatin, would reverse hyperinsulinemia induced by a sulfonylurea overdose. Eight normal subjects received glipizide (1.45 mg/kg) on three occasions. Within 3 h, all subjects became hypoglycemic (< 50 mg/dL) and were initially treated with 50% dextrose followed by 1) dextrose infusion, 2) octreotide (30 ng/kg.min, iv), or 3) diazoxide (300 mg, iv, every 4 h). Euglycemia (85 mg/dL) was maintained with supplementary dextrose in treatment limbs 2 and 3. Insulin concentrations were 4-5 times greater with dextrose alone or in combination with diazoxide than with octreotide (P < 0.01). Dextrose requirements during diazoxide or dextrose alone were not different, but were both greater than those during octreotide treatment (P < 0.0001). All therapies were stopped at 13 h. Glucose levels remained above 3.6 mmol/L (65 mg/dL) in six of eight subjects receiving octreotide for the remaining 4 h. Glucose fell to below 3.6 mmol/L within 1.5 h of stopping either dextrose or diazoxide in each subject. Overall, octreotide reduced and in four of eight subjects entirely eliminated the need for exogenous glucose after a large overdose of glipizide. We conclude that octreotide is safe and effective and should be strongly considered as a logical therapeutic alternative for this metabolic emergency.

摘要

使用葡萄糖对磺脲类药物过量进行急救治疗往往效果不佳,因为葡萄糖会刺激胰岛素释放,进而需要不断增加高渗葡萄糖的用量以维持正常血糖水平。我们检验了这样一个假设:生长抑素类似物奥曲肽能够逆转磺脲类药物过量所致的高胰岛素血症。八名正常受试者分三次接受了格列吡嗪(1.45毫克/千克)。在3小时内,所有受试者均出现低血糖(<50毫克/分升),最初均接受了50%葡萄糖治疗,随后分别接受:1)葡萄糖输注;2)奥曲肽(30纳克/千克·分钟,静脉注射);3)二氮嗪(300毫克,静脉注射,每4小时一次)。在治疗组2和治疗组3中,通过补充葡萄糖维持了血糖正常(85毫克/分升)。单独使用葡萄糖或与二氮嗪联合使用时的胰岛素浓度比使用奥曲肽时高4至5倍(P<0.01)。单独使用二氮嗪或葡萄糖时的葡萄糖需求量没有差异,但均高于奥曲肽治疗期间的需求量(P<0.0001)。所有治疗均在13小时时停止。在接受奥曲肽治疗的八名受试者中,有六名在剩余4小时内血糖水平保持在3.6毫摩尔/升(65毫克/分升)以上。在停止葡萄糖或二氮嗪治疗后,每个受试者的血糖在1.5小时内降至3.6毫摩尔/升以下。总体而言,在大剂量服用格列吡嗪后,奥曲肽减少了八名受试者中四名对额外葡萄糖的需求,并完全消除了另外四名受试者对额外葡萄糖的需求。我们得出结论,奥曲肽安全有效,应被视为这种代谢急症合理的治疗选择。

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