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contributor authorSmitha M. N. Rao
contributor authorVictor K. Lin
contributor authorUday Tata
contributor authorGanesh V. Raj
contributor authorKytai Nguyen
contributor authorJ.-C. Chiao
contributor authorJer-Tsong Hsieh
date accessioned2017-05-09T00:40:15Z
date available2017-05-09T00:40:15Z
date copyrightMay, 2010
date issued2010
identifier issn1949-2944
identifier otherJNEMAA-28035#021003_1.pdf
identifier urihttp://yetl.yabesh.ir/yetl/handle/yetl/144543
description abstractMigration of cancer cells from the primary organ site via the bloodstream to distant sites is critical to the development of malignant metastasis and is in part determined by soluble host factors in the serum. Conventional Boyden chamber assays to evaluate cell motility require high volumes of reagents and are impractical for high-throughput analysis. We have designed and evaluated a poly-dimethylsiloxane (PDMS) microfluidic device in order to systematically study cancer cell migration. Photolithography and soft lithography processes were used to fabricate the PDMS devices from a negative photoresist (SU-8) mold. The device provides two separate identical chambers that are interconnected by an array of identical narrow channels, 10 μm high, 25 μm wide, and 1000 μm long. One chamber is seeded with cancer cells whose migration characteristics are to be evaluated, while the other chamber contains media with chemoattractants toward which the cancer cells migrate. In this microfluidic chamber model, the migration of cancer cells within and across the microfluidic channels over a prescribed time was quantified using time-lapse photographs. The microfluidic chamber is a cost-effective platform that uses small volumes of reagents, can maintain stable chemokine gradients, allow real-time quantitative study of cancer cell migration, and provide information about cellular dynamics and biomechanical analysis. This work demonstrated the utility of the microfluidic device as a platform to study cancer cell migration as well as the potential applications in the identification of specific chemokine agents and development of drugs targeting cell migration.
publisherThe American Society of Mechanical Engineers (ASME)
titleDemonstration of Cancer Cell Migration Using a Novel Microfluidic Device
typeJournal Paper
journal volume1
journal issue2
journal titleJournal of Nanotechnology in Engineering and Medicine
identifier doi10.1115/1.4001280
journal fristpage21003
identifier eissn1949-2952
keywordsChannels (Hydraulic engineering)
keywordsPlasma desorption mass spectrometry
keywordsMicrofluidics
keywordsCancer AND Gradients
treeJournal of Nanotechnology in Engineering and Medicine:;2010:;volume( 001 ):;issue: 002
contenttypeFulltext


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