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High-throughput microfluidic cell sorting platform (MICS)

Authors :
Barbara Mair
Randy Atwal
Peter M. Aldridge
Amy Hin Yan Tong
Sanna Masud
Edward H. Sargent
Stephane Angers
David Philpott
Shana O. Kelley
Meng Zhang
Jason Moffat
Publication Year :
2019
Publisher :
Research Square Platform LLC, 2019.

Abstract

Genome-scale functional genetic screens can be used to interrogate determinants of protein expression modulation of a target of interest. Such phenotypic screening approaches typically require sorting of large numbers of cells (>108). In conventional cell sorting techniques (i.e. fluorescence-activated cell sorting), sorting time, associated with high instrument and operating costs and loss of cell viability, are limiting to the scalability and throughput of these screens. We recently established a rapid and scalable high-throughput microfluidic cell sorting platform (MICS) using immunomagnetic nanoparticles to sort cells in parallel capable of sorting more than 108 HAP1 cells in under one hour while maintaining high levels of cell viability (Ref. 1). This protocol outlines how to set-up MICS for large-scale phenotypic screens in mammalian cells. We anticipate this platform being used for genome-wide functional genetic screens as well as other applications requiring the sorting of large numbers of cells based on protein expression.

Details

Database :
OpenAIRE
Accession number :
edsair.doi...........dbaca797411395082e96d681b8916aa0
Full Text :
https://doi.org/10.21203/rs.2.10282/v1