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Biosynthetic Human Insulin and Insulin Analogs

机译:生物合成人胰岛素和胰岛素类似物

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Background: Biosynthetic human insulins and analogs have replaced animal insulins and permitted structural modifications to alter the rate of absorption, duration of action, improve reproducibility of effects, and modulate relative efficacy in various target tissues. Several forms of rapidly acting insulins nearly achieve rapid pharmacokinetics and pharmacodynamics similar to first-phase insulin release. There is need for even faster-acting analogs to mimic normal physiology and improve control of postprandial glycemic excursions. Two biosynthetic insulin analogs have sufficiently long duration of action for use as once-daily basal insulins; controversy persists regarding their respective risks of hypoglycemia and relative glycemic variability. Results: Basal-bolus therapy and insulin pump therapy, including closed-loop automated insulin delivery, require rapid-acting insulin analogs. The longer acting insulins can provide stable, reproducible basal insulin with reduced rates of hypoglycemia, particularly nocturnal hypoglycemia, greater efficacy in reducing mean glucose and glucose variability while increasing time in glucose target range. Inhalable human insulin provides very rapid action. Premixture of rapid-acting analogs with protamine has been useful for some patients with type 2 diabetes. An insulin analog with preferential efficacy at the liver has been developed and tested clinically but not marketed. Current research is aimed at developing even faster-acting insulin analogs. Long-acting basal insulins coformulated with GLP-1 receptor agonists or with a rapidly acting insulin analog have valuable clinical applications. Excipients, chaperones, local heating of the infusion site, and hyaluronidase have also been used to accelerate the absorption of insulin analogs. Conclusions: Biosynthetic human insulins have radically revolutionized management of both type 1 and type 2 diabetes worldwide. The ability to manipulate the structure and formulation of insulin provides for more physiologic pharmacokinetics and pharmacodynamics, enabling improved glycemic control, reduced risk of hypoglycemia, and reduced rates of long-term complications.
机译:背景:生物合成人胰岛素和类似物已取代动物胰岛素并允许的结构修饰改变吸收速度,作用持续时间,提高效果的再现性,并调节各种靶组织中的相对功效。几乎达到了类似于第一阶段胰岛素释放的快速药代动力学和药效学的几种形式的迅速作用的胰岛素。需要更快的模拟来模仿正常生理学,改善对餐后血糖缩放的控制。两种生物合成胰岛素类似物具有足够长的持续时间,用作次数 - 每日基础胰岛素;关于它们各自的低血糖和相对血糖变异性的各自风险的争议。结果:基底血管疗法和胰岛素泵治疗,包括闭环自动胰岛素递送,需要快速作用的胰岛素类似物。较长的作用胰岛素可以提供稳定的可重复的基础胰岛素,降低低血糖,特别是夜间低血糖,在降低平均葡萄糖和葡萄糖可变性时更高的功效,同时葡萄糖靶范围内的时间增加时间。可吸入的人胰岛素提供非常快速的行动。与protamine的快速作用类似物的预混物对某些患有2型糖尿病的患者有用。在肝脏上具有优先效力的胰岛素类似物,并在临床上进行了测试,但未销售。目前的研究旨在发展甚至更快的胰岛素类似物。用GLP-1受体激动剂或具有快速作用胰岛素类似物的长效基础胰岛素具有有价值的临床应用。还用于加速胰岛素类似物的赋形剂,伴侣,输液部位的局部加热和透明质酸酶。结论:生物合成人胰岛素在全球1型和2型糖尿病中具有根本性的革命性的管理。操纵胰岛素的结构和制剂的能力为更多的生理药代动力学和药效学提供了改善的血糖控制,降低低血糖风险,降低了长期并发症的率降低。

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