Delivery and actuation of aerosolized microbots.

Nano select : open access Pub Date : 2022-07-01 Epub Date: 2022-03-07 DOI:10.1002/nano.202100353
Coy J Zimmermann, Tyler Schraeder, Brandon Reynolds, Emily M DeBoer, Keith B Neeves, David W M Marr
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引用次数: 0

Abstract

For disease of the lung, the physical key to effective inhalation-based therapy is size; too large (10's of μm) and the particles or droplets do not remain suspended in air to reach deep within the lungs, too small (subμm) and they are simply exhaled without deposition. μBots within this ideal low-μm size range however are challenging to fabricate and would lead to devices that lack the speed and power necessary for performing work throughout the pulmonary network. To uncouple size from structure and function, here we demonstrate an approach where individual building blocks are aerosolized and subsequently assembled in situ into μbots capable of translation, drug delivery, and mechanical work deep within lung mimics. With this strategy, a variety of pulmonary diseases previously difficult to treat may now be receptive to μbot-based therapies.

雾化微珠的输送和驱动
对于肺部疾病而言,有效吸入疗法的物理关键在于尺寸;尺寸太大(10's μm),微粒或液滴就无法悬浮在空气中到达肺部深处;尺寸太小(亚微米),微粒或液滴就会被直接呼出而不会沉积。为了使尺寸与结构和功能脱钩,我们在此展示了一种方法,即先将单个构件气溶胶化,然后在原位组装成能够在肺模拟物深处进行翻译、药物输送和机械工作的微机器人。有了这种策略,以前难以治疗的各种肺部疾病现在都可能接受基于微机器人的疗法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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