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用于连续葡萄糖监测的经皮近红外荧光共振能量转移亲和传感器的体内性能评估

In vivo performance evaluation of a transdermal near- infrared fluorescence resonance energy transfer affinity sensor for continuous glucose monitoring.

作者信息

Ballerstadt Ralph, Evans Colton, Gowda Ashok, McNichols Roger

机构信息

BioTex, Inc., Houston, Texas 77054, USA.

出版信息

Diabetes Technol Ther. 2006 Jun;8(3):296-311. doi: 10.1089/dia.2006.8.296.

Abstract

The in vivo performance of a transdermal near-infrared fluorescence resonance energy transfer (FRET) affinity sensor was investigated in hairless rats, in order to validate its feasibility for glucose monitoring in humans. The sensor itself consists of a small hollow fiber implanted in dermal skin tissue, containing glucose-sensitive assay chemistry composed of agarose-immobilized Concanavalin A (ConA) and free dextran. The glucose-dependent fluorescence change is based on FRET between near-infrared-compatible donor and quencher dyes that are chemically linked to dextran and ConA, respectively. We conducted an acute in vivo evaluation of transdermal sensors with an optical fiber-coupled setup over 4 h, and a chronic in vivo evaluation of fully implanted sensors for up to 16 days. The fiber-coupled sensors followed trends of blood glucose concentrations very well with a delay of less than 5 min. The acute performance of the implanted sensors at the day of implantation was similar to that of the fiber-coupled sensors. After 2 weeks the implanted sensors remained functional, evidenced by an adequate correlation between sensor signal and changes in blood glucose excursions, but exhibited delays of approximately 10-15 min. Preliminary characterization of host response showed signs of mild inflammations around the implanted sensor, which were characterized by formation of a 10-20-microm-thick collagen band, typical for capsule formation. An acute study of systemic ConA biotoxicity was also conducted. A histological analysis of various organs and of clinical chemistry data showed no significant differences between rats receiving intradermal injections of ConA at 10 times the concentration in the sensor and rats in a control group (injection of saline solution). The absence of a toxicological or systemic response to ConA at a 10-fold larger amount than in the sensor should dispel concerns over the in vivo safety of ConA-based sensors. This study clearly demonstrates the feasibility of the proposed transdermal FRET-based sensor interrogation concept for glucose monitoring.

摘要

为验证其在人体葡萄糖监测中的可行性,在无毛大鼠体内研究了一种经皮近红外荧光共振能量转移(FRET)亲和传感器的性能。该传感器本身由植入真皮组织的一根小中空纤维组成,其中含有由琼脂糖固定的伴刀豆球蛋白A(ConA)和游离葡聚糖构成的葡萄糖敏感检测化学物质。葡萄糖依赖性荧光变化基于分别与葡聚糖和ConA化学连接的近红外兼容供体染料和猝灭染料之间的FRET。我们使用光纤耦合装置对经皮传感器进行了4小时的急性体内评估,并对完全植入的传感器进行了长达16天的慢性体内评估。光纤耦合传感器能很好地跟踪血糖浓度变化趋势,延迟时间不到5分钟。植入传感器在植入当天的急性性能与光纤耦合传感器相似。2周后,植入传感器仍保持功能,传感器信号与血糖波动变化之间有充分的相关性证明了这一点,但延迟时间约为10 - 15分钟。宿主反应的初步表征显示植入传感器周围有轻度炎症迹象,其特征是形成一条10 - 20微米厚的胶原带,这是典型的包膜形成。还进行了ConA全身生物毒性的急性研究。对各种器官的组织学分析和临床化学数据显示,接受皮内注射浓度为传感器中10倍的ConA的大鼠与对照组大鼠(注射盐溶液)之间没有显著差异。在比传感器中ConA含量大10倍的情况下没有出现对ConA的毒理学或全身反应,这应消除对基于ConA的传感器体内安全性的担忧。这项研究清楚地证明了所提出的基于经皮FRET传感器询问概念用于葡萄糖监测的可行性。

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