Literature DB >> 25186818

Two-dimensional motility of a macrophage cell line on microcontact-printed fibronectin.

Laurel E Hind1, Joanna L Mackay, Dianne Cox, Daniel A Hammer.   

Abstract

The ability of macrophages to migrate to sites of infection and inflammation is critical for their role in the innate immune response. Macrophage cell lines have made it possible to study the roles of individual proteins responsible for migration using molecular biology, but it has not been possible to reliably elicit the motility of macrophage cell lines in two dimensions. In the past, measurements of the motility of macrophage cell lines have been largely limited to transwell assays which provide limited quantitative information on motility and limited ability to visualize cell morphology. We used microcontact printing to create polydimethylsiloxane (PDMS) surfaces functionalized with fibronectin that otherwise support little macrophage adhesion. We used these surfaces to measure macrophage migration in two dimensions and found that these cells migrate efficiently in a uniform field of colony-stimulating factor-1, CSF-1. Knockdown of Cdc42 led to a nonstatistically significant reduction in motility, whereas chemical inhibition of PI3K activity led to a complete loss of motility. Inhibition of the RhoA kinase, ROCK, did not abolish the motility of these cells but caused a quantitative change in motility, reducing motility significantly on high concentrations of fibronectin but not on low concentrations. This study illustrates the importance of studying cell motility on well controlled materials to better understand the exact roles of specific proteins on cell migration.
© 2014 Wiley Periodicals, Inc. © 2014 Wiley Periodicals, Inc.

Entities:  

Keywords:  fibronectin; macrophage; microcontact printing; motility; podosome

Mesh:

Substances:

Year:  2014        PMID: 25186818      PMCID: PMC4266554          DOI: 10.1002/cm.21191

Source DB:  PubMed          Journal:  Cytoskeleton (Hoboken)        ISSN: 1949-3592


  34 in total

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Authors:  Michael T Yang; Jianping Fu; Yang-Kao Wang; Ravi A Desai; Christopher S Chen
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Authors:  W E Allen; G E Jones; J W Pollard; A J Ridley
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Authors:  D Cox; P Chang; Q Zhang; P G Reddy; G M Bokoch; S Greenberg
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8.  Subcellular optogenetic activation of Cdc42 controls local and distal signaling to drive immune cell migration.

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  8 in total

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