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新型α-葡萄糖苷酶抑制剂米格列醇(Bay m1099)对餐后低血糖症状患者口服蔗糖负荷后血糖、胰岛素、C肽及胃抑肽反应的影响。

Effect of Miglitol (Bay m1099), a new alpha-glucosidase inhibitor, on glucose, insulin, C-peptide and GIP responses to an oral sucrose load in patients with post-prandial hypoglycaemic symptoms.

作者信息

Renard E, Parer-Richard C, Richard J L, Jureidini S, Orsetti A, Mirouze J

机构信息

Clinique des Maladies métaboliques et endocriniennes, Hôpital Lapeyronie, Montpellier, France.

出版信息

Diabete Metab. 1991 May-Jun;17(3):355-62.

PMID:1884880
Abstract

Sixteen patients suffering from symptoms suggestive of idiopathic reactive hypoglycaemia and reproducible during an oral glucose tolerance test when plasma glucose was less than or equal to 2.8 mM, were included in an acute, double-blind and cross-over study to test the efficacy of Miglitol (Bay m1099), a new alpha-glucosidase inhibitor versus placebo. Patients were randomized to ingest 100 mg Miglitol or placebo together with a sucrose solution (45 g/m2 body surface), one week apart. During four hours, plasma glucose levels were continuously monitored and plasma insulin and gastric inhibitory polypeptide (GIP) levels were measured at 30-minute intervals; serum C-peptide concentration was determined at 0, 30, 60 minutes and then every hour. The post-load rise in plasma glucose was significantly blunted by Miglitol, as shown by the reduced plasma glucose peak, the diminished early (0-120 min) area under the glycaemic curve and the decreased rate of plasma glucose rise. Thereafter, plasma glucose nadir was significantly raised and rate of plasma glucose fall was slowed by Miglitol with a concomitant improvement in the hypoglycaemic index. Insulin secretion was dampened as indicated by parallel reduction of plasma insulin and serum C-peptide peaks; morever, early area under the insulin curve and total (0-240 min) area under the C-peptide curve were significantly reduced. Decrease of plasma GIP peak and total area under the GIP curve were also significant. During sucrose tolerance test with Miglitol, hypoglycaemic symptoms were significantly alleviated but intestinal side-effects were common. Blunting the insulin response to glucose directly by delaying glucose absorption and indirectly through reducing GIP secretion, may be a valuable therapeutic approach in reactive hypoglycemia; nevertheless, long-term study with Miglitol are needed, due to the poor intestinal tolerance of this drug in the present acute study.

摘要

16例有特发性反应性低血糖症状且在口服葡萄糖耐量试验中当血浆葡萄糖小于或等于2.8 mM时症状可重现的患者,被纳入一项急性、双盲、交叉研究,以测试新型α-葡萄糖苷酶抑制剂米格列醇(Bay m1099)与安慰剂的疗效。患者被随机分组,间隔一周分别服用100 mg米格列醇或安慰剂以及蔗糖溶液(45 g/m²体表面积)。在4小时内,持续监测血浆葡萄糖水平,并每隔30分钟测量血浆胰岛素和胃抑肽(GIP)水平;在0、30、60分钟时测定血清C肽浓度,之后每小时测定一次。米格列醇显著抑制了负荷后血浆葡萄糖的升高,表现为血浆葡萄糖峰值降低、血糖曲线下早期(0 - 120分钟)面积减小以及血浆葡萄糖上升速率降低。此后,米格列醇使血浆葡萄糖最低点显著升高,血浆葡萄糖下降速率减慢,同时低血糖指数有所改善。血浆胰岛素和血清C肽峰值平行降低表明胰岛素分泌受到抑制;此外,胰岛素曲线下早期面积和C肽曲线下总(0 - 240分钟)面积显著减小。血浆GIP峰值降低以及GIP曲线下总面积减小也很显著。在使用米格列醇的蔗糖耐量试验期间,低血糖症状显著缓解,但肠道副作用常见。通过延迟葡萄糖吸收直接以及通过减少GIP分泌间接减弱胰岛素对葡萄糖的反应,可能是反应性低血糖的一种有价值的治疗方法;然而,由于在本急性研究中该药物肠道耐受性较差,因此需要对米格列醇进行长期研究。

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