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可植入葡萄糖传感器的小鼠模型:葡萄糖传感器开发的新模型。

Murine model of implantable glucose sensors: a novel model for glucose sensor development.

作者信息

Klueh Ulrike, Kreutzer Donald L

机构信息

Center for Molecular Tissue Engineering and Department of Surgery, University of Connecticut School of Medicine, Farmington, Connecticut 06030, USA.

出版信息

Diabetes Technol Ther. 2005 Oct;7(5):727-37; discussion 738-40. doi: 10.1089/dia.2005.7.727.

Abstract

Although implantable glucose sensors have existed for over 30 years, their function deteriorates in hours to days, in large part as a result of tissue responses to the implanted sensor (i.e., acute and chronic inflammation, fibrosis, and vessel regression). Little is known about the mediators and mechanisms that control these tissue responses to implantable glucose sensors. In the present study, we developed and validated a murine model for implantable glucose sensors, which suitably parallel sensor function in humans. Using special care in implantation and implant retaining techniques, we demonstrated that (1) sensor function deteriorates rapidly within days post-implantation and (2) loss of glucose sensor function correlated with tissue reactions at the sites of sensor implantation, especially in the vicinity of the glucose oxidase-based working electrode. These studies establish a murine model that can be used to evaluate implantable glucose sensors in vivo. This model should provide the foundation for future studies to understand the factors and mechanisms that control sensor function in vivo.

摘要

尽管可植入式葡萄糖传感器已经存在了30多年,但其功能在数小时至数天内就会恶化,这在很大程度上是由于组织对植入传感器的反应(即急性和慢性炎症、纤维化以及血管退化)所致。对于控制这些组织对可植入式葡萄糖传感器反应的介质和机制,我们知之甚少。在本研究中,我们开发并验证了一种用于可植入式葡萄糖传感器的小鼠模型,该模型与人类的传感器功能具有适当的相似性。通过在植入和固定植入物技术上格外小心,我们证明:(1)传感器功能在植入后数天内迅速恶化;(2)葡萄糖传感器功能的丧失与传感器植入部位的组织反应相关,特别是在基于葡萄糖氧化酶的工作电极附近。这些研究建立了一种可用于在体内评估可植入式葡萄糖传感器的小鼠模型。该模型应为未来研究理解控制体内传感器功能的因素和机制提供基础。

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