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Engineering synthetically modified insulin for glucose-responsive diabetes therapy

机译:工程合成修饰的胰岛素用于葡萄糖反应性糖尿病治疗

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摘要

Though a suite of different insulin variants have been used clinically to provide greater control over pharmacokinetics, no clinically used insulin can tune its potency and/or bioavailability in a glucose-dependent manner. In order to improve therapy for diabetic patients, a vision has been the development of autonomous closed-loop approaches. Toward this goal, insulin has been synthetically modified with glucose-sensing groups or groups that can compete with free glucose for binding to glucose-binding proteins and evaluated in pre-clinical models. Specifically, it was demonstrated that site-specific modification of insulin with phenylboronic acid can result in glucose-responsive activity, leading to faster recovery in diabetic mice following a glucose challenge but with less observed hypoglycemia in healthy mice. This strategy, along with several others being pursued, holds promise to improve the fidelity in glycemic control with routine insulin therapy.
机译:尽管临床上已经使用一套不同的胰岛素变体来提供对药代动力学的更大控制,但是没有临床上使用的胰岛素能够以葡萄糖依赖的方式调节其效能和/或生物利用度。为了改善对糖尿病患者的治疗,一种愿景是开发自主的闭环方法。为了达到这个目标,胰岛素已经被葡萄糖敏感基团或可以与游离葡萄糖竞争与葡萄糖结合蛋白结合的基团进行了合成修饰,并在临床前模型中进行了评估。具体而言,已证明用苯基硼酸对胰岛素进行位点特异性修饰可导致葡萄糖响应活性,从而导致糖尿病小鼠在葡萄糖激发后恢复更快,但在健康小鼠中观察到的低血糖较少。该策略以及其他一些正在追求的策略,有望提高常规胰岛素治疗的血糖控制保真度。

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