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Transcutaneous Implantation Methods for Improving the Long-Term Performance of Glucose Sensors in Rats

机译:改善大鼠葡萄糖传感器长期性能的经皮植入方法

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Translation of sensor design and function in animal models to human use is an ongoing challenge due to tissue anatomical and physiological differences between species, even at presumably analogous implant locations. Nevertheless, preclinical testing of sensors for long-term glucose monitoring in animals is required for evaluating sensor function in order to improve sensor design. Long-term glucose sensor testing in common laboratory animals (e.g., mice and rats) is especially difficult due to their small size, as well as limited site availability for sensor placement without disturbance or removal by the subject. However, improvements in sensor design and implantation methods to improve sensor survival in these animals could accelerate our understanding of the role of tissue reactions to sensor components, as well as allow reliable testing of biomaterials and various drug or growth factor delivery systems to potentially minimize or modulate tissue reactions. In this study, methods to secure a wire-type subcutaneous sensor in rats for a long period of time (ges28 d), utilizing new implantation techniques and devices were evaluated. Anchoring devices were incorporated into the sensor design and appropriate implantation methods were used to: (1) minimize potential membrane damage caused by animal motion; (2) prevent removal of the entire sensor or sensor wires by the animal; and (3) allow exterior access to wires for periodic sensor performance testing. The anchoring devices for securing sensors to the skin internally, which were sequentially investigated and improved (Protocol A to C), included a modified 22 gauge intravenous winged catheter (Protocol A), Silastic tubing (Protocol B) or silk suture loops held in place by Silastic tubing (Protocol C). The results show that after four weeks implantation, 60% (n = 10), 70% (n = 10), and 92% (n = 12) of the implanted devices survived (Protocols A, B, and C, respectively). Functional testing showed that 30% (n = 10), 40% (-n = 10), and 58% (n = 12) of the sensors still worked well four weeks after implantation (Protocols A, B, and C, respectively). No infections were visibly evident at the sites of sensor implantation at any time during the testing period for all protocols. Protocol C shows promise as a viable method for future sensor studies because of the anchoring device''s small size and because it was nearly impossible for rats to remove or damage the sensors.
机译:由于物种之间的组织解剖和生理差异,即使在大概相似的植入位置上,动物模型中传感器设计和功能向人类使用的转换也是一个持续的挑战。然而,需要对动物进行传感器的临床前测试,以便对动物进行长期葡萄糖监测,以评估传感器的功能,从而改善传感器的设计。由于它们的体积小,并且在放置传感器时不受受试者干扰或移除的局限性,在普通实验室动物(例如小鼠和大鼠)中进行长期葡萄糖传感器测试尤其困难。但是,对传感器设计和植入方法的改进以提高这些动物的传感器存活率可以加快我们对组织对传感器组件反应的作用的理解,并允许对生物材料和各种药物或生长因子输送系统进行可靠的测试,以尽可能地减少或减少调节组织反应。在这项研究中,评估了使用新的植入技术和设备在大鼠中长时间(ges28 d)固定线型皮下传感器的方法。锚定装置被并入传感器设计中,并采用适当的植入方法来:(1)尽量减少动物运动引起的潜在膜损伤; (2)防止动物移走整个传感器或传感器导线; (3)允许外部接触电线以进行定期的传感器性能测试。依次进行了研究和改进(协议A至C),用于将传感器内部固定在皮肤上的锚固设备包括改良的22号静脉有翼导管(协议A),硅橡胶管(协议B)或固定的丝线环通过Silastic管材(方案C)。结果表明,在植入四周后,分别有60%(n = 10),70%(n = 10)和92%(n = 12)的植入设备得以幸存(分别为协议A,B和C)。功能测试表明,植入后四周,仍有30%(n = 10),40%(-n = 10)和58%(n = 12)的传感器仍然工作良好(分别为协议A,B和C) 。在所有协议的测试期间中的任何时间,在传感器植入位置均未见明显感染。由于锚固装置的体积小,并且老鼠几乎不可能移除或损坏传感器,因此方案C有望成为未来传感器研究的可行方法。

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