Kolterman O G, Gottlieb A, Moyses C, Colburn W
Amylin Pharmaceuticals, San Diego, California 92121, USA.
Diabetes Care. 1995 Aug;18(8):1179-82. doi: 10.2337/diacare.18.8.1179.
To demonstrate that intravenous administration of AC137 (25,28,29 tripro-human amylin), a human amylin analogue, modulates the rate of appearance of glucose derived from a standard oral meal in the peripheral circulation of patients with insulin-dependent diabetes mellitus (IDDM).
After the observation that a 2-h infusion of AC137 at a rate of 150 micrograms/h, in conjunction with the subjects' usual morning insulin dose, decreased postprandial hyperglycemia in 6 subjects with IDDM, a double-blind placebo-controlled two-period crossover design in an additional 18 IDDM patients was undertaken to confirm and extend the observation. Based on reasoning that an effect to modulate the appearance of orally administered glucose would have no impact on the disposition of an intravenous glucose load, nine patients were challenged with an intravenous glucose loads (300 mg/kg), while another nine patients were challenged with a standardized Sustacal meal (350 kcal) during a 5-h infusion of AC137 (50 micrograms/h). On each occasion, the subjects received their usual morning doses of insulin subcutaneously. The impact of the AC137 infusion on the plasma glucose responses to these different challenges was assessed.
Intravenous infusion of AC137 yielding steady state plasma concentrations of 225 +/- 15 pmol/l (mean +/- SE) reduced postprandial plasma glucose concentrations after the standardized Sustacal meal challenge. The mean area under the glucose curve, corrected for baseline, was reduced from -1,869 +/- 5,562 mg.dl-1.min during placebo infusion to -28,872 +/- 4,812 mg.dl-1.min during AC137 infusion, P = 0.0015. In contrast, an AC137 infusion producing steady-state concentrations of 234 +/- 16 pmol/l had no effect on the plasma glucose profile after administration of an intravenous glucose load.
AC137 administration, in these patients with IDDM, reduced postprandial hyperglycemia apparently by affecting the delivery rate of glucose from the gastrointestinal tract. AC137 may prove to be a clinically useful addition to insulin regimens to facilitate the achievement of glycemic control.
证明静脉注射人胰淀素类似物AC137(25,28,29-三脯氨酸人胰淀素)可调节胰岛素依赖型糖尿病(IDDM)患者外周循环中源自标准口服餐的葡萄糖出现率。
在观察到以150微克/小时的速率静脉输注AC137 2小时,并结合受试者通常的早晨胰岛素剂量,可降低6名IDDM患者的餐后高血糖后,对另外18名IDDM患者进行了双盲安慰剂对照两期交叉设计,以确认并扩展该观察结果。基于这样的推理,即调节口服葡萄糖出现的作用对静脉注射葡萄糖负荷的处置没有影响,9名患者接受静脉注射葡萄糖负荷(300毫克/千克)挑战,而另外9名患者在以50微克/小时的速率静脉输注AC137的5小时期间接受标准化的Sustacal餐(350千卡)挑战。每次,受试者均皮下注射其通常的早晨胰岛素剂量。评估了AC137输注对这些不同挑战的血浆葡萄糖反应的影响。
静脉输注AC137使稳态血浆浓度达到225±15皮摩尔/升(平均值±标准误),降低了标准化Sustacal餐挑战后的餐后血浆葡萄糖浓度。经基线校正后的葡萄糖曲线下平均面积,从安慰剂输注期间的-1,869±5,562毫克·分升-1·分钟降至AC137输注期间的-28,872±4,812毫克·分升-1·分钟,P = 0.0015。相比之下,产生稳态浓度为234±16皮摩尔/升的AC137输注对静脉注射葡萄糖负荷后的血浆葡萄糖曲线没有影响。
在这些IDDM患者中,给予AC137显然通过影响胃肠道葡萄糖的输送速率降低了餐后高血糖。AC137可能被证明是胰岛素治疗方案中有助于实现血糖控制的一种临床上有用的补充药物。
