Sage Journals: Discover world-class research

Abstract

Construction and supply of cell-based reagents for in vitro plate-based screens are often highlighted as a bottleneck within drug discovery. Recent years have seen the successful application of both cryopreservation and automation to increase the capacity and flexibility of cell provision. However, routine cell culture remains a fixed experimental process that requires cells to be prepared and used at specific times. We have investigated the potential of reduced temperature incubation to be used as a simple methodology for stopping and starting cell growth and introduce further flexibility into cell provision. Our results show that incubation of CHOK1, HEK293, and 1321N1 cells at 23 °C arrested growth while maintaining cell viability. Recovery of these paused cells at 37 °C resulted in resumption of normal cell growth and target protein function. Experiments demonstrated that paused cells, expressing either a recombinant G-protein-coupled receptor or an ion channel, performed comparably with the equivalent continuously cultured cells in a 384-well cell-based assay. This simple technique offers the potential to introduce flexibility into cell culture experiments and processes that were previously considered to be fixed. (Journal of Biomolecular Screening 2009:716-722)

Keywords

cell culture cell pausing cell-based assays reagent provision cell supply

References

Cawkill D. , Eaglestone S. : Evolution of cell-based reagent provision. Drug Discov Today 2007;12:820-825.

Zaman GJR , de Roos JADM , Blomenroehr M. , van Koppen CJ , Oosterrom J. : Cryopreserved cells facilitate cell-based drug discovery. Drug Discov Today 2007;12:521-526.

Wigglesworth MJ , Lawless KJ , Standing DJ , Mackenzie EK , Kitchen VR , Mckay F. , et al: Use of cryopreserved cells for enabling greater flexibility in compound profiling . J Biomol Screen 2008;13:354-362.

Hunt L. , Hacker DL , Grosjean F. , De Jesus M. , Uebersax L. , Jordan M. , et al: Low-temperature pausing of cultivated mammalian cells. Biotechnol Bioeng 2005;89:157-163.

Sonna LA , Fujita J. , Gaffin SL , Lilly CM : Effects of heat and cold stress on mammalian gene expression. J Appl Physiol 2002;92:1725-1742.

Fujita J. : Cold shock response in mammalian cells. J Mol Microbiol Biotechnol 1999;1:243-255.

Al-Fageeh MB , Marchant RJ , Carden MJ , Smales M. : The cold-shock response in cultured mammalian cells: harnessing the response for the improvement of recombinant protein production. Biotechnol Bioeng 2006;93:829-835.

Moore A. , Mercer J. , Dutina G. , Donahue CJ , Bauer KD , Mather JP , et al: Effects of temperature shift on cell cycle, apoptosis and nucleotide pools in CHO cell batch cultures. Cytotechnology 1997;23:47-54.

Zhang JH , Chung TD , Oldenburg KR : A simple statistical parameter for use in evaluation and validation of high-throughput screening assays J Biomol Screen 1999;4:67-73.

Use of Reduced Temperature Cell Pausing to Enhance Flexibility of Cell-Based Assays

Abstract

Keywords

References