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Integrated microvalves for cortical drug-delivery at the cellular level.

机译:在细胞水平上用于皮质药物递送的集成微阀。

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摘要

Microelectrode arrays now allow the simultaneous electrical recording and stimulation of large numbers of neurons in the central nervous system, providing a basis for major advances in neuroscience and in prosthetic devices for disorders such as epilepsy, deafness, and Parkinson's disease. However, the neuronal system is chemical as well as electrical, and for many of these applications, the development of miniature drug-delivery systems for in-vivo use is essential. This research has developed microvalves that can be integrated into these arrays to provide control over the chemical environment at the cellular level.;Microchannels for drug delivery are formed in the body of a multi-electrode probe by undercutting a selectively-etched boron-doped silicon and/or dielectric masking structure. The mask openings are then sealed using deposited dielectrics. In order to control fluid flow in these channels, integrated microvalves have been developed that require only two extra masks beyond the normal probe process. The normally-open valve structure uses pressure to deflect a corrugated circular diaphragm against a seat, blocking the flow path as needed.;Using stress-compensated silicon dioxide and silicon nitride corrugated diaphragms 400mum in diameter and 1-2mum thick, two different on-probe pneumatically-actuated valve structures were demonstrated. Two sacrificial 5mum-thick polysilicon layers sandwiched between dielectric layers were used to form the two chambers of the microvalves. Both valve types provide an open flow rate greater than 500pL/sec at an applied input pressure of 10kPa and meet the design target of a leak rate less than 25pL/sec at an actuation pressure of 35kPa.;Prototype thermopneumatically-actuated microvalves were also designed and fabricated. Simulations show that using the phase-change of a low-boiling-point liquid (42°C, cyclopentane), less than 10mW is required to generate a drive pressure of 35kPa, closing the valve in less than 20msec. The temperature rise in the surrounding tissue should be less than 2°C, making the valve safe for use in-vivo. This is the first reported microvalve suitable for on-probe use in a cellular drug-delivery system, and as a low-voltage low-power structure capable of high actuation pressure and throw, it should have many other applications as well.
机译:现在,微电极阵列可以同时进行电记录和刺激中枢神经系统中的大量神经元,从而为神经科学和修复装置(如癫痫,耳聋和帕金森氏病)的重大进步提供了基础。但是,神经元系统既是化学系统也是电气系统,因此对于许多此类应用程序,开发用于体内使用的微型药物递送系统至关重要。这项研究已经开发出微阀,这些微阀可以集成到这些阵列中,从而在细胞水平上提供对化学环境的控制。通过对选择性腐蚀的掺硼硅进行底切,在多电极探针体内形成了用于药物输送的微通道。和/或电介质掩膜结构。然后使用沉积的电介质密封掩模开口。为了控制这些通道中的流体流动,已经开发出集成的微型阀,该微型阀仅需要两个额外的口罩即可,而不是常规的探测过程。常开阀结构利用压力使波纹状的圆形膜片偏向阀座,根据需要阻塞流路;使用应力补偿的二氧化硅和氮化硅波纹膜片,直径为400μm,厚度为1-2μm,两个不同演示了气动探针结构。夹在介电层之间的两个牺牲5mm厚多晶硅层用于形成微阀的两个腔室。两种类型的阀在施加的10kPa的输入压力下均可提供大于500pL / sec的打开流量,并能在35kPa的驱动压力下满足小于25pL / sec的泄漏率的设计目标;还设计了原型热气动微型阀和捏造。仿真表明,使用低沸点液体(42°C,环戊烷)的相变,要产生35kPa的驱动压力,需要不到10mW的功率,在不到20msec的时间内关闭阀门。周围组织的温度升高应低于2°C,以使瓣膜在体内安全使用。这是第一个报道的微阀,适用于在细胞药物输送系统中进行探头使用,并且作为一种能够实现高促动压力和喷射能力的低压低功率结构,它也应具有许多其他应用。

著录项

  • 作者

    Baek, Kyusuk.;

  • 作者单位

    University of Michigan.;

  • 授予单位 University of Michigan.;
  • 学科 Engineering Biomedical.;Engineering Electronics and Electrical.
  • 学位 Ph.D.
  • 年度 2009
  • 页码 113 p.
  • 总页数 113
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物医学工程;无线电电子学、电信技术;
  • 关键词

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