Real-time two- and three-dimensional imaging of monocyte motility and navigation on planar surfaces and in collagen matrices: roles of Rho

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作者
Robert Bzymek
Markus Horsthemke
Katrin Isfort
Simon Mohr
Kerstin Tjaden
Carsten Müller-Tidow
Marlies Thomann
Tanja Schwerdtle
Martin Bähler
Albrecht Schwab
Peter J. Hanley
机构
[1] Institut für Physiologie II,Analytical and Environmental Sciences Division
[2] Westfälische Wilhelms-Universität,undefined
[3] Institut für Molekulare Zellbiologie,undefined
[4] Westfälische Wilhelms-Universität,undefined
[5] Molekulare und Vaskuläre Kardiologie,undefined
[6] Universitätsklinikum Münster,undefined
[7] Hämatologie und Onkologie,undefined
[8] Universitätsklinikum Halle,undefined
[9] King’s College London,undefined
[10] Institut für Ernährungswissenschaft,undefined
[11] Universität Potsdam,undefined
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We recently found that macrophages from RhoA/RhoB double knockout mice had increased motility of the cell body, but severely impaired retraction of the tail and membrane extensions, whereas RhoA- or RhoB-deficient cells exhibited mild phenotypes. Here we extended this work and investigated the roles of Rho signaling in primary human blood monocytes migrating in chemotactic gradients and in various settings. Monocyte velocity, but not chemotactic navigation, was modestly dependent on Rho-ROCK-myosin II signaling on a 2D substrate or in a loose collagen type I matrix. Viewed by time-lapse epi-fluorescence microscopy, monocytes appeared to flutter rather than crawl, such that the 3D surface topology of individual cells was difficult to predict. Spinning disk confocal microscopy and 3D reconstruction revealed that cells move on planar surfaces and in a loose collagen matrix using prominent, curved planar protrusions, which are rapidly remodeled and reoriented, as well as resorbed. In a dense collagen type I matrix, there is insufficient space for this mode and cells adopt a highly Rho-dependent, lobular mode of motility. Thus, in addition to its role in tail retraction on 2D surfaces, Rho is critical for movement in confined spaces, but is largely redundant for motility and chemotaxis in loose matrices.
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