胰岛素依赖型糖尿病的皮下胰岛素替代。药代动力学和药效学研究。

P O Olsson
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引用次数: 0

摘要

用聚乙二醇沉淀内源性胰岛素抗体后,用放射免疫法测定游离胰岛素和总胰岛素。研究了胰岛素依赖性糖尿病患者的胰岛素替代,包括不同方案的24小时游离胰岛素和葡萄糖谱,胰岛素制剂的混溶性,隔夜代谢控制以及不同剂量的输注泵。在游离胰岛素和总胰岛素测定中,用聚乙二醇沉淀免疫球蛋白几乎完全,回收率高。与在37℃下立即沉淀和测定的血浆样品相比,立即处理的血清(20℃)和在20℃下3小时后的血浆中游离胰岛素略有下降。在储存(-20℃)未沉淀的血浆样品中,游离胰岛素在4周后增加,在26周后的血清样品中也增加,而储存的peg上清则稳定。在健康对照中,发现基础胰岛素较低,餐后增加约10倍。没有发现早晨游离胰岛素或葡萄糖升高。在1或2个剂量方案中,24小时的游离胰岛素谱明显不符合生理性;有餐前和夜间高胰岛素血症,但没有与进餐相关的游离胰岛素峰值。早餐后血糖明显升高。强化方案与常规注射或输液泵,24小时自由胰岛素谱类似的生理。然而,餐峰延迟;白天使用输注泵时出现高胰岛素血症。在体外和体内实验中,与半合成的人lente胰岛素混合后,常规胰岛素立即丧失,但与生物合成的人NPH胰岛素混合后,常规胰岛素不会立即丧失。早晨血糖控制与睡前注射中等作用胰岛素或持续皮下胰岛素输注相似,但在恒定速率的输注泵下发现夜间高胰岛素血症较少。未见清晨血糖升高。剂量相关的游离胰岛素谱在注射泵给药后显示出来,尽管与餐后生理反应相比,它们是迟钝的。持续皮下注射胰岛素可加重餐后高胰岛素血症。血糖钳夹期间的葡萄糖消耗与游离胰岛素谱相对应,表明游离胰岛素代表生物活性激素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Subcutaneous insulin substitution in insulin-dependent diabetes mellitus. Pharmacokinetic and pharmacodynamic studies.

Determination of free and total insulin with radioimmunoassay, after precipitation of endogenous insulin antibodies with polyethylene glycol, was evaluated. Insulin substitution in insulin-dependent diabetic patients was investigated, embracing the 24 h free insulin and glucose profiles with different regimens, the miscibility of insulin preparations, the overnight metabolic control, and bolus doses of different size with infusion pumps. In the free and total insulin assay precipitation of immunoglobulins with polyethylene glycol was almost complete and the recovery was high. Compared to immediately precipitated and assayed plasma samples at 37 degrees C, free insulin slightly decreased in immediately processed serum (20 degrees C), and also in plasma after 3 h at 20 degrees C. In stored (-20 degrees C) unprecipitated plasma samples free insulin increased after 4 weeks and also in serum samples after 26 weeks, whereas stored PEG-supernates were stable. In healthy controls a low basal insulin was found, increasing about tenfold postprandially. No morning rise in free insulin or glucose was found. The 24 h free insulin profile was strikingly unphysiological with 1 or 2 dose regimens; there was preprandial and nocturnal hyperinsulinaemia but absence of meal-related free insulin peaks. A considerable glucose rise was found after breakfast. Intensive regimens with conventional injections or infusion pumps, gave 24 h free insulin profiles that were similar to the physiological. However, the prandial peaks were retarded; and hyperinsulinaemia was shown with infusion pumps during daytime. An immediate loss of regular insulin was demonstrated after mixture with semisynthetic human lente insulin in vitro and in vivo, but not after mixture with biosynthetic human NPH insulin. The morning glucose control was similar with a bedtime injection of intermediate-acting insulin or continuous subcutaneous insulin infusion, but less hyperinsulinaemia overnight was found with the infusion pump at a constant rate. No early morning glucose rise was demonstrated. Dose-related free insulin profiles were shown after bolus doses with an infusion pump, although they were retarded compared to the physiological postprandial response. The postprandial hyperinsulinaemia was aggravated by continuous subcutaneous insulin infusion. Glucose consumption during euglycaemic clamp corresponded to the free insulin profiles, indicating that free insulin represents the biologically active hormone.

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