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与格列美脲治疗相关的严重低血糖期间的激素对抗调节及随后的格列美脲血清浓度

Hormonal counterregulation and consecutive glimepiride serum concentrations during severe hypoglycaemia associated with glimepiride therapy.

作者信息

Holstein A, Plaschke A, Hammer C, Ptak M, Kuhn J, Kratzsch C, Diekmann J, Kleesiek K, Maurer H H, Egberts E-H

机构信息

1st Department of Medicine, Klinikum Lippe, Röntgenstrasse 18, 32756, Detmold, Germany.

出版信息

Eur J Clin Pharmacol. 2003 Dec;59(10):747-54. doi: 10.1007/s00228-003-0697-9. Epub 2003 Nov 22.

Abstract

OBJECTIVE

To examine the release of counterregulatory hormones and consecutive glimepiride serum concentrations during severe hypoglycaemia (SH) associated with glimepiride therapy.

METHODS

In nine type-2 diabetic patients [age 81+/-9 (65-93) years; diabetes duration 9+/-4 (3-15) years; initial blood glucose 33+/-16 (10-54) mg/dl (1.8+/-0.9 mmol/l); HbA1c 7.2+/-1.1 (5.6-8.7)%; creatinine clearance 49+/-33 (15-107) ml/min] who experienced SH associated with glimepiride therapy with neuroglucopenic presentation, insulin, C-peptide, glucagon, epinephrine, norepinephrine, cortisol, adenocorticotrophic hormone (ACTH), human growth hormone (HGH) and pancreatic polypeptide (PP) were determined in blood samples taken at 4-h intervals prior to and during treatment with glucose i.v. Serum from the same samples was screened for sulphonylurea-type oral antidiabetics. Glimepiride concentrations were determined by a validated atmospheric pressure chemical ionization liquid chromatographic-mass spectrometry (APCI-LC-MS) assay.

RESULTS

Once treatment had begun, normoglycaemia was maintained; most glimepiride levels were below the limit of detection (LOD <0.01 mg/l) and further sulphonylureas could be excluded. The secretion of glucagon and epinephrine as counterregulatory hormonal responses was unaffected. In addition, protracted marked increases of cortisol and norepinephrine levels were demonstrated. Protracted stimulation of insulin and C-peptide occurred in a period of up to 24 h after SH. No significant protracted responses were observed for ACTH, HGH or PP.

CONCLUSION

In SH associated with glimepiride therapy, no correlation between glimepiride serum concentrations and the protracted stimulation of insulin and C-peptide was observed. The secretion of glucagon and epinephrine as counterregulatory hormonal responses was unaffected. Protracted increased release of cortisol might be a medium-term indicator of glimepiride-associated SH.

摘要

目的

研究与格列美脲治疗相关的严重低血糖(SH)期间,机体反调节激素的释放情况以及随后的格列美脲血清浓度变化。

方法

选取9例2型糖尿病患者[年龄81±9(65 - 93)岁;糖尿病病程9±4(3 - 15)年;初始血糖33±16(10 - 54)mg/dl(1.8±0.9 mmol/l);糖化血红蛋白7.2±1.1(5.6 - 8.7)%;肌酐清除率49±33(15 - 107)ml/min],这些患者在接受格列美脲治疗时出现了伴有神经低血糖症状的SH。在静脉输注葡萄糖治疗前及治疗期间,每隔4小时采集血样,测定其中胰岛素、C肽、胰高血糖素、肾上腺素、去甲肾上腺素、皮质醇、促肾上腺皮质激素(ACTH)、人生长激素(HGH)和胰多肽(PP)的含量。对同一样本的血清进行磺脲类口服降糖药筛查。采用经验证的大气压化学电离液相色谱 - 质谱联用(APCI - LC - MS)法测定格列美脲浓度。

结果

治疗开始后,血糖维持在正常水平;多数格列美脲水平低于检测限(LOD <0.01 mg/l),且可排除其他磺脲类药物。作为反调节激素反应的胰高血糖素和肾上腺素的分泌未受影响。此外,皮质醇和去甲肾上腺素水平出现持续显著升高。在SH发生后的长达24小时内,胰岛素和C肽受到持续显著刺激。未观察到ACTH、HGH或PP有明显的持续反应。

结论

在与格列美脲治疗相关的SH中,未观察到格列美脲血清浓度与胰岛素和C肽的持续刺激之间存在相关性。作为反调节激素反应的胰高血糖素和肾上腺素的分泌未受影响。皮质醇释放的持续增加可能是格列美脲相关SH的中期指标。

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