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1.
J Phys Chem Lett ; 11(12): 4655-4661, 2020 Jun 18.
Artículo en Inglés | MEDLINE | ID: mdl-32453583

RESUMEN

We reveal a unique mechanism by which pure water can be dissociated to form free radicals without requiring catalysts, electrolytes, or electrode contact by means of high-frequency nanometer-amplitude electromechanical surface vibrations in the form of surface acoustic waves (SAWs) generated on a piezoelectric substrate. The physical undulations associated with these mechanical waves, in concert with the evanescent electric field arising from the piezoelectric coupling, constitute half-wavelength "nanoelectrochemical cells" in which liquid is trapped within the SAW potential minima with vertical dimensions defined by the wave amplitude (∼10 nm), thereby forming highly confined polarized regions with intense electric field strengths that enable the breakdown of water. The ions and free radicals that are generated rapidly electromigrate under the high field intensity in addition to being convectively transported away from the cells by the bulk liquid recirculation generated by the acoustic excitation, thereby overcoming mass transport limitations that lead to ion recombination.

2.
Soft Matter ; 15(20): 4146-4152, 2019 May 22.
Artículo en Inglés | MEDLINE | ID: mdl-31050347

RESUMEN

Tactile haptic feedback is an important consideration in the design of advanced human-machine interfaces, particularly in an age of increasing reliance on automation and artificial intelligence. In this work, we show that the typical nanometer-order surface displacement amplitudes of piezoelectric transducers-which are too small to be detectable by the human touch, and constitute a significant constraint in their use for tactile haptic surface actuation-can be circumvented by coupling the vibration into a liquid to drive the deflection of a thermoplastic membrane. In particular, transmission of the sound energy from the standing wave vibration generated along a piezoelectric transducer into a microfluidic chamber atop which the membrane is attached is observed to amplify the mechanical vibration signalling through both the acoustic radiation pressure and the viscous normal stress acting on the membrane-the latter arising due to the acoustic streaming generated as the sound wave propagates through the liquid-to produce 100 µm-order static deflections of the membrane, upon which approximately 0.5 µm dynamic vibrations at frequencies around 1 kHz are superimposed; both these static and dynamic responses are within the perception range for human finger sensation. The large static deformation, the relatively fast response time, and the ability to incorporate a dynamic vibrotactile response together with the small size and potential for integration of the device into large scale arrays make this mechanism well suited for driving actuation in devices which require tactile haptic responses.

3.
Anal Chem ; 91(9): 5621-5628, 2019 05 07.
Artículo en Inglés | MEDLINE | ID: mdl-30915842

RESUMEN

We seek to demonstrate a robust, low-cost, and user-friendly acoustomicrofluidic platform that facilitates rapid, reproducible, and precise nanoliter sample dispensing. The solid-state chipscale platform exploits the unprecedented acceleration arising from high-frequency nanoelectromechanical vibrations, on the order of 10 million g, to jet the sample and hence generate a liquid bridge that spans across the substrate, on which the vibrations are generated and from which the sample originates, to a top target plate before rapidly pinching off to deposit the sample on the target with precise and reproducible volumes that can be tuned down to 0.22 µL with a standard error of 6.5% and coefficient of variation of 11.3%. The entire process occurs within approximately 10 ms. In addition to explicating the fundamental physical mechanism that underpins the technology, we demonstrate its use for serial dilution and concentration and, in particular, a cell-based drug toxicology assay. Moreover, we also show that multiple drop dispensing in an array, without requiring repositioning of the chip between dispensing steps, can be achieved through a simple but yet effective sequential directional jetting strategy, therefore allowing significant reduction in the total dispensing time in the case of massive-scale microarray operation. Given its low cost and compact size, the platform can easily be automated and parallelized, thus offering the prospect for introducing large-scale efficiencies in the laboratory workflow.

4.
Soft Matter ; 14(28): 5937-5938, 2018 Jul 18.
Artículo en Inglés | MEDLINE | ID: mdl-29926038

RESUMEN

Correction for 'Continuous tuneable droplet ejection via pulsed surface acoustic wave jetting' by Jasmine O. Castro et al., Soft Matter, 2018, DOI: 10.1039/c7sm02534c.

5.
Soft Matter ; 14(28): 5721-5727, 2018 Jul 18.
Artículo en Inglés | MEDLINE | ID: mdl-29845144

RESUMEN

We report a miniaturised platform for continuous production of single or multiple liquid droplets with diameters between 60 and 500 µm by interfacing a capillary-driven self-replenishing liquid feed with pulsed excitation of focussed surface acoustic waves (SAWs). The orifice-free operation circumvents the disadvantages of conventional jetting systems, which are often prone to clogging that eventuates in rapid degradation of the operational performance. Additionally, we show the possibility for flexibly tuning the ejected droplet size through the pulse width duration, thus avoiding the need for a separate device for every different droplet size required, as is the case for systems in which the droplet size is set by nozzles and orifices, as well as preceding ultrasonic jetting platforms where the droplet size is controlled by the operating frequency. Further, we demonstrate that cells can be jetted and hence printed onto substrates with control over the cell density within the droplets down to single cells. Given that the jetting does not lead to significant loss to the cell's viability or ability to proliferate, we envisage that this versatile jetting method can potentially be exploited with further development for cell encapsulation, dispensing and 3D bioprinting applications.

6.
ACS Appl Mater Interfaces ; 8(28): 17751-6, 2016 Jul 20.
Artículo en Inglés | MEDLINE | ID: mdl-27389811

RESUMEN

We report a simple method for on-demand continuous processing of composite liquid marbles with the aid of a 3D printed slide platform, which offers the potential for engineering novel functional surfaces for the production of combination drug therapies, particle-based barcode biomarkers and smart membranes, among other applications. Unlike other attempts at producing such liquid marbles, this novel technique not only facilitates controllable and reproducible production of the liquid marbles but also allows the selection of different morphologies such as banded, patchy, and Janus structures by controlling the coalescence conditions, with the possibility for tunable symmetric and asymmetric patterns, the latter by varying the particle species partitioning ratio.

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