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治疗1型糖尿病:从胰岛素给药策略到双激素控制

Treating type 1 diabetes: from strategies for insulin delivery to dual hormonal control.

作者信息

McCall A L, Farhy L S

机构信息

Department of Medicine and Center for Diabetes Technology, University of Virginia, Charlottesville, VA 22908, USA.

出版信息

Minerva Endocrinol. 2013 Jun;38(2):145-63.

Abstract

Type 1 diabetes is a disorder where slow destruction of pancreatic β-cells occurs through autoimmune mechanisms. The result is a progressive and ultimately complete lack of endogenous insulin. Due to β-cell lack, secondary abnormalities in glucagon and likely in incretins occur. These multiple hormonal abnormalities cause metabolic instability and extreme glycemic variability, which is the primary phenotype. As the disease progresses patients often develop hypoglycemia unawareness and defects in their counterregulatory defenses. Intensive insulin therapy may thus lead to 3-fold excess of severe hypoglycemia and severely hinder the effective and safe control of hyperglycemia. The main goal of the therapy for type 1 diabetes has long been physiological mimicry of normal insulin secretion based on monitoring which requires considerable effort and understanding of the underlying physiology. Attainment of this goal is challenged by the nature of the disease and our current lack of means to fully repair the abnormal endocrine pancreas interactive functions. As a result, various insulin preparations have been developed to partially compensate for the inability to deliver timely exogenous insulin directly to the portal/intrapancreatic circulation. It remains an ongoing task to identify the ideal routes and regimens of their delivery and potentially that of other hormones to restore the deficient and disordered hormonal environment of the pancreas to achieve a near normal metabolic state. Several recent technological advances help addressing these goals, including the rapid progress in insulin pumps, continuous glucose sensors, and ultimately the artificial pancreas closed-loop technology and the recent start of dual-hormone therapies.

摘要

1型糖尿病是一种通过自身免疫机制导致胰腺β细胞缓慢破坏的疾病。其结果是内源性胰岛素逐渐并最终完全缺乏。由于β细胞缺乏,胰高血糖素以及可能的肠促胰岛素会出现继发性异常。这些多种激素异常会导致代谢不稳定和血糖极度波动,这是主要表型。随着疾病进展,患者常常会出现低血糖无知觉以及反调节防御功能缺陷。强化胰岛素治疗可能因此导致严重低血糖的发生率增加三倍,并严重阻碍高血糖的有效和安全控制。长期以来,1型糖尿病治疗的主要目标一直是基于监测对正常胰岛素分泌进行生理模拟,这需要付出相当大的努力并理解潜在的生理学知识。实现这一目标受到疾病性质以及我们目前缺乏完全修复异常内分泌胰腺相互作用功能手段的挑战。因此,已经开发出各种胰岛素制剂,以部分弥补无法将及时的外源性胰岛素直接输送到门静脉/胰腺内循环的能力。确定其理想的给药途径和方案以及可能的其他激素的给药途径和方案,以恢复胰腺缺乏和紊乱的激素环境,从而实现接近正常的代谢状态,仍然是一项持续的任务。最近的几项技术进步有助于实现这些目标,包括胰岛素泵、连续血糖传感器的快速发展,最终还有人工胰腺闭环技术以及最近开始的双激素疗法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b3a9/4220674/cd51b2edb3dd/nihms568405f1.jpg

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