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Effect of oxygen supply on the size of implantable islet-containing encapsulation devices

机译:氧气供应对可植入的含胰岛包封装置尺寸的影响

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摘要

Beta-cell replacement therapy is a promising approach for the treatment of diabetes but is currently limited by the human islet availability and by the need for systemic immunosuppression. Tissue engineering approaches that will enable the utilization of islets or beta-cells from alternative sources (such as porcine islets or human stem cell derived beta cells) and minimize or eliminate the need for immunosuppression have the potential to address these critical limitations. However, tissue engineering approaches are critically hindered by the device size (similar to the size of a large flat screen television) required for efficacy in humans. The primary factor dictating the device size is the oxygen availability to islets to support their viability and function (glucose-stimulated insulin secretion [GSIS]). GSIS is affected (inhibited) at a much higher oxygen partial pressure [pO(2)] than that of viability (e.g. 10 mmHg as opposed to 0.1 mmHg). Enhanced oxygen supply (higher pO(2)) than what is available in vivo at transplant sites can have a profound effect on the required device size (potentially reduce it to the size of a postage stamp). This paper summarizes key information on the effect of oxygen on islet viability and function within immunoisolation devices and describes the potential impact of enhanced oxygen supply to devices in vivo on device size reduction.
机译:β细胞替代疗法是治疗糖尿病的一种有前途的方法,但是目前受到人类胰岛可用性和全身免疫抑制需求的限制。组织工程学方法将能够利用来自替代来源的胰岛或β细胞(例如猪胰岛或人干细胞衍生的β细胞),并最大限度地减少或消除对免疫抑制的需求,因此有可能解决这些关键局限性。但是,组织工程学方法受到人体功效所需的设备尺寸(类似于大型平板电视的尺寸)的严重阻碍。决定装置大小的主要因素是胰岛的氧气供应,以支持其生存能力和功能(葡萄糖刺激的胰岛素分泌[GSIS])。 GSIS的氧分压[pO(2)]比生存力(例如10 mmHg而不是0.1 mmHg)高得多(受影响)。比移植部位体内提供的氧气供应更高(更高的pO(2))可以对所需的设备尺寸产生深远的影响(有可能将其减小到邮票的尺寸)。本文总结了有关氧气对免疫隔离设备中胰岛活力和功能的影响的关键信息,并描述了体内向设备提供更多氧气对设备尺寸减小的潜在影响。

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