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Dive into the research topics where Yuzhe Ding is active.

Publication


Featured researches published by Yuzhe Ding.


Investigative Ophthalmology & Visual Science | 2011

Elastic Modulus Determination of Normal and Glaucomatous Human Trabecular Meshwork

Tingrui Pan; Yuzhe Ding; Christopher M. Reilly; Kate E. Keller; Ted S. Acott; Michael P. Fautsch; Christopher J. Murphy; Paul Russell

PURPOSE Elevated intraocular pressure (IOP) is a risk factor for glaucoma. The principal outflow pathway for aqueous humor in the human eye is through the trabecular meshwork (HTM) and Schlemms canal (SC). The junction between the HTM and SC is thought to have a significant role in the regulation of IOP. A possible mechanism for the increased resistance to flow in glaucomatous eyes is an increase in stiffness (increased elastic modulus) of the HTM. In this study, the stiffness of the HTM in normal and glaucomatous tissue was compared, and a mathematical model was developed to predict the impact of changes in stiffness of the juxtacanalicular layer of HTM on flow dynamics through this region. METHODS Atomic force microscopy (AFM) was used to measure the elastic modulus of normal and glaucomatous HTM. According to these results, a model was developed that simulated the juxtacanalicular layer of the HTM as a flexible membrane with embedded pores. RESULTS The mean elastic modulus increased substantially in the glaucomatous HTM (mean = 80.8 kPa) compared with that in the normal HTM (mean = 4.0 kPa). Regional variation was identified across the glaucomatous HTM, possibly corresponding to the disease state. Mathematical modeling suggested an increased flow resistance with increasing HTM modulus. CONCLUSIONS The data indicate that the stiffness of glaucomatous HTM is significantly increased compared with that of normal HTM. Modeling exercises support substantial impairment in outflow facility with increased HTM stiffness. Alterations in the biophysical attributes of the HTM may participate directly in the onset and progression of glaucoma.


Advanced Materials | 2011

UNIVERSAL NANOPATTERNABLE INTERFACIAL BONDING

Yuzhe Ding; Shaun P. Garland; Michael C. Howland; Alexander Revzin; Tingrui Pan

A nanopatternable polydimethylsiloxane (PDMS) oligomer layer is demonstrated as an interfacial adhesive for its intrinsic transferability and universal adhesiveness. Utilizing the well-established surface modification and bonding techniques of PDMS surfaces, irreversible bonding is formed (up to 400 kPa) between a wide range of substrate pairs, representing ones within and across different materials categories, including metals, ceramics, thermoset, and thermoplastic polymers.


Lab on a Chip | 2011

Capillary-driven automatic packaging.

Yuzhe Ding; Lingfei Hong; Baoqing Nie; Kit S. Lam; Tingrui Pan

Packaging continues to be one of the most challenging steps in micro-nanofabrication, as many emerging techniques (e.g., soft lithography) are incompatible with the standard high-precision alignment and bonding equipment. In this paper, we present a simple-to-operate, easy-to-adapt packaging strategy, referred to as Capillary-driven Automatic Packaging (CAP), to achieve automatic packaging process, including the desired features of spontaneous alignment and bonding, wide applicability to various materials, potential scalability, and direct incorporation in the layout. Specifically, self-alignment and self-engagement of the CAP process induced by the interfacial capillary interactions between a liquid capillary bridge and the top and bottom substrates have been experimentally characterized and theoretically analyzed with scalable implications. High-precision alignment (of less than 10 µm) and outstanding bonding performance (up to 300 kPa) has been reliably obtained. In addition, a 3D microfluidic network, aligned and bonded by the CAP technique, has been devised to demonstrate the applicability of this facile yet robust packaging technique for emerging microfluidic and bioengineering applications.


Lab on a Chip | 2013

Microfluidic impact printer with interchangeable cartridges for versatile non-contact multiplexed micropatterning

Yuzhe Ding; Eric C. Huang; Kit S. Lam; Tingrui Pan

Biopatterning has been increasingly used for well-defined cellular microenvironment, patterned surface topology, and guided biological cues; however, it meets challenges on biocompatibility, thermal and chemical sensitivity, as well as limited availability of reagents. In this paper, we aim at combining the desired features from non-contact inkjet printing and dot-matrix impact printing to establish a versatile multiplexed micropatterning platform, referred to as Microfluidic Impact Printer (MI-Printer), for emerging biomedical applications. Using this platform, we can achieve the distinct features of no cross-contamination, sub-microliter ink loading with a minimal dead volume, high-throughput printing, biocompatible non-contact processing, sequential patterning with self-alignment, wide adaptability for complex media (e.g., cell suspension or colloidal solutions), interchangeable/disposable cartridge design, and simple assembly and configuration, all highly desirable towards laboratory-based research and development. Specifically, the printing resolution of the MI-printer platform has been experimentally characterized and theoretically analysed. Optimal printing resolution of 80 μm has been repeatedly obtained. Furthermore, two useful functions of the MI-printer, multiplexed printing and combinatorial printing, have been experimentally demonstrated with less than 10 μm misalignment. Moreover, molecular and biological patterning, utilizing the multiplexed and combinatorial printing, has been implemented to illustrate the utility of this versatile printing technique for emerging biomedical applications.


Analytical Chemistry | 2015

Microfluidic-Enabled Print-to-Screen Platform for High-Throughput Screening of Combinatorial Chemotherapy

Yuzhe Ding; Jiannan Li; Wenwu Xiao; Kai Xiao; Joyce M. Lee; Urvashi Bhardwaj; Zijie Zhu; Philip Digiglio; Gaomai Yang; Kit S. Lam; Tingrui Pan

Since the 1960s, combination chemotherapy has been widely utilized as a standard method to treat cancer. However, because of the potentially enormous number of drug candidates and combinations, conventional identification methods of the effective drug combinations are usually associated with significantly high operational costs, low throughput screening, laborious and time-consuming procedures, and ethical concerns. In this paper, we present a low-cost, high-efficiency microfluidic print-to-screen (P2S) platform, which integrates combinatorial screening with biomolecular printing for high-throughput screening of anticancer drug combinations. This P2S platform provides several distinct advantages and features, including automatic combinatorial printing, high-throughput parallel drug screening, modular disposable cartridge, and biocompatibility, which can potentially speed up the entire discovery cycle of potent drug combinations. Microfluidic impact printing utilizing plug-and-play microfluidic cartridges is experimentally characterized with controllable droplet volume and accurate positioning. Furthermore, the combinatorial print-to-screen assay is demonstrated in a proof-of-concept biological experiment which can identify the positive hits among the entire drug combination library in a parallel and rapid manner. Overall, this microfluidic print-to-screen platform offers a simple, low-cost, high-efficiency solution for high-throughput large-scale combinatorial screening and can be applicable for various emerging applications in drug cocktail discovery.


international conference on solid state sensors actuators and microsystems | 2015

High-throughput print-to-screen (P2S) platform for combinatorial chemotherapy

Jiannan Li; Yuzhe Ding; Wenwu Xiao; Kai Xiao; J. Lee; Urvashi Bhardwaj; Zijie Zhu; Philip Digiglio; Kit S. Lam; Tingrui Pan

This paper reports a microfluidic enabled print-to-screen (P2S) platform, which can achieve low-cost, high-throughput, high-precision printing with plug-and-play disposable cartridge, as well as parallel screening with minimized crosstalk. The performance of the P2S platform is characterized and, using this platform, the cell-killing performance of 3-out-of-10 drug combinations towards ovarian cancer cell is, for the first time, studied and as a result, 15 out of 175 drug combinations are newly identified to exert potent cancer cell toxicity. This demonstrates the potent applicability of P2S platform for combinatorial chemotherapy, which can greatly speed up the entire cycle of drug cocktail discovery.


international conference on micro electro mechanical systems | 2012

Universal nano-adhesive of PDMS oligomers

Yuzhe Ding; Shaun P. Garland; Michael C. Howland; Alexander Revzin; Tingrui Pan

A nanopatternable oligomeric PDMS layer has been first reported as a nano-interfacial adhesive for its intrinsic transferability and universal adhesiveness. Utilizing well-established PDMS surface modification and bonding techniques, we have been able to form an irreversible bond between a wide range of substrate pairs, representing ones within and across different material categories, including metals, ceramics, thermoset, and thermoplastic polymers.


Annals of Biomedical Engineering | 2015

Design, Fabrication, and In Vitro Testing of an Anti-biofouling Glaucoma Micro-shunt

Ryan S. Harake; Yuzhe Ding; J. David Brown; Tingrui Pan


Archive | 2014

Non-contact bio-printing

Tingrui Pan; Yuzhe Ding; Eric J. Huang; Kit S. Lam


international conference on solid state sensors actuators and microsystems | 2013

Microfluidic impact printing (MI-printing) for biomedical applications

Yuzhe Ding; Eric C. Huang; Kit S. Lam; Tingrui Pan

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Tingrui Pan

University of California

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Kit S. Lam

University of California

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Eric C. Huang

University of California

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Jiannan Li

University of California

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Kai Xiao

University of California

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