Different Molecular Motors Mediate Platelet-derived Growth Factor and Lysophosphatidic Acid-stimulated Floating Collagen Matrix Contraction

Abe, Masatoshi; Ho, Cheryl; Kamm, Kristine E.; Grinnell, Frederick

doi:10.1074/jbc.m306228200

Cited by 49 publications

(55 citation statements)

References 48 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Human fibroblasts in collagen lack detectable Rho activation upon PDGF stimulation . Therefore, basal rather than agoniststimulated Rho kinase probably is required for cell migration and contraction, perhaps by maintaining basal levels of myosin light chain phosphorylation (Abe et al, 2003;Knock et al, 2008).…”

Section: Discussionmentioning

confidence: 99%

Collagen Fibril Flow and Tissue Translocation Coupled to Fibroblast Migration in 3D Collagen Matrices

Miron-Mendoza

Seemann

Grinnell

2008

MBoC

Self Cite

View full text Add to dashboard Cite

In nested collagen matrices, human fibroblasts migrate from cell-containing dermal equivalents into surrounding cell-free outer matrices. Time-lapse microscopy showed that in addition to cell migration, collagen fibril flow occurred in the outer matrix toward the interface with the dermal equivalent. Features of this flow suggested that it depends on the same cell motile machinery that normally results in cell migration. Collagen fibril flow was capable of producing large-scale tissue translocation as shown by closure of a ϳ1-mm gap between paired dermal equivalents in floating, nested collagen matrices. Our findings demonstrate that when fibroblasts interact with collagen matrices, tractional force exerted by the cells can couple to matrix translocation as well as to cell migration. INTRODUCTIONCell migration depends on the multistep process of cell extension, adhesion, exertion of backward tractional force, and tail retraction (Lauffenburger and Horwitz, 1996;Mitchison and Cramer, 1996;Galbraith and Sheetz, 1997;Beningo et al., 2001;Ridley et al., 2003). The extensive body of research underlying the multistep model is based on studies with tissue cells on extracellular matrix (ECM)-coated planar surfaces including rigid materials such as glass or plastic coverslips as well as flexible materials such as polyacrylamide. On ECM-coated planar surfaces, cells can modulate their cytoskeletal function and adhesion strength in response to surface mechanics (Balaban et al., 2001;Discher et al., 2005;Ingber, 2006;Vogel and Sheetz, 2006). However, adsorbed or covalently attached ECM molecules tend to be held in register with each other with little capacity to undergo cell-mediated mechanical and molecular reorganization.Type 1 collagen is the major protein component of fibrous connective tissues. These connective tissues provide mechanical support and frameworks throughout the body, and fibroblasts are the cell type primarily responsible for their biosynthesis and remodeling. Three-dimensional (3D) matrices prepared with type I collagen exhibit mechanical properties that resemble connective tissue (Barocas et al., 1995;Wakatsuki et al., 2000;Roeder et al., 2002;Silver et al., 2002;Ahlfors and Billiar, 2007). Unlike ECM-coated material surfaces, fibroblasts can mechanically remodel collagen matrices both locally and globally (Brown et al., 1998;Tomasek et al., 2002;Grinnell, 2003;Petroll, 2004; Tranquillo, 1999Such mechanical remodeling of connective tissue ECM is believed to be important for tissue homeostasis (Silver et al., 2002;Wiig et al., 2003;Goldsmith et al., 2004;Langevin et al., 2004), aging (Varani et al., 2004), repair (Tonnesen et al., 2000Tomasek et al., 2002;Grinnell, 2003), fibrosis (Eckes et al., 2000;Desmouliere et al., 2005), and tumorigenesis (Beacham and Cukierman, 2005;Gaggioli et al., 2007;Yamada and Cukierman, 2007).Cells interacting with 3D collagen matrices exhibit distinct patterns of cell signaling (Cukierman et al., 2002;Wozniak et al., 2003;Beningo et al., 2004;Rhee et al., 2007) and increa...

show abstract

Section: Discussionmentioning

confidence: 99%

Collagen Fibril Flow and Tissue Translocation Coupled to Fibroblast Migration in 3D Collagen Matrices

Miron-Mendoza

Seemann

Grinnell

2008

MBoC

Self Cite

View full text Add to dashboard Cite

show abstract

“…Based on pharmacological approaches, previous works suggested involvement of Rho GTPases in collagen gel contraction by fibroblasts (Abe et al, 2003;Parizi et al, 2000). Our recent studies show more directly that a tight regulation of RhoA activation controls collagen gel contraction and distribution of focal adhesions in fibroblasts .…”

Section: Journal Of Cell Science 119 (9)mentioning

confidence: 99%

Interactions of primary fibroblasts and keratinocytes with extracellular matrix proteins: contribution of α2β1 integrin

Zhang

Bothe

Hirche

et al. 2006

Journal of Cell Science

View full text Add to dashboard Cite

The α2β1 integrin is a collagen-binding protein with very high affinity for collagen I. It also binds several other collagens and laminins and it is expressed by many cells, including keratinocytes and fibroblasts in the skin. In the past, α2β1 integrin was suggested to be responsible for cell attachment, spreading and migration on monomeric collagen I and contraction of three-dimensional collagen lattices. In view of these functions, normal development and fertility in integrin α2-deficient mice, which we generated by targeting the integrin α2 gene, came as a surprise. This suggested the existence of compensatory mechanisms that we investigate here using primary fibroblasts and keratinocytes isolated from wild-type and α2-deficient mice, antibodies blocking integrin function and downregulation of integrin α2 expression. The results show that the α2β1 integrin is absolutely required for keratinocyte adhesion to collagens whereas for fibroblasts other collagen-binding integrins partially back-up the lack of α2β1 in simple adhesion to collagen monomers. A prominent requirement for α2β1 integrins became apparent when fibroblasts executed mechanical tasks of high complexity in three-dimensional surroundings, such as contracting free-floating collagen gels and developing isometric forces in tethered lattices. The deficits observed for α2-deficient fibroblasts appeared to be linked to alterations in the distribution of force-bearing focal adhesions and deregulation of Rho-GTPase activation.

show abstract

“…The involvement of myosin II also appeared to be supported by morphological/behavior responses of cells to the potent non-muscle myosin II inhibitor blebbistatin [8], including the inhibition of fibroblasts to remodel collagen fibers [9], invade the matrices [10] and contract floating matrices [11]. However these effects could *Corresponding Author: Yu-li Wang, University of Massachusetts Medical School, 377 Plantation, Suite 327, Worcester, MA 01605, Tel: 508-856-8782, Fax: 508-856-8774, e-mail: yuli.wang@umassmed.edu.…”

Section: Introductionmentioning

confidence: 99%

Traction forces of fibroblasts are regulated by the Rho-dependent kinase but not by the myosin light chain kinase

Beningo

Hamao

Dembo

et al. 2006

Archives of Biochemistry and Biophysics

115

View full text Add to dashboard Cite

Adhesive cells show complex mechanical interactions with the substrate, however the exact mechanism of such interactions, termed traction forces, is still unclear. To address this question we have measured traction forces of fibroblasts treated with agents that affect the myosin II-dependent contractile mechanism. Using the potent myosin II inhibitor blebbistatin, we demonstrate that traction forces are strongly dependent on a functional myosin II heavy chain. Since myosin II is regulated by both the myosin light chain kinase (MLCK) and, directly or indirectly, the Rho-associated kinase (ROCK), we examined the effects of inhibitors against these kinases. Interestingly, inhibition of the myosin light chain kinase had no detectable effect, while inhibition of the Rho-dependent kinase caused strong inhibition of traction forces. Our results indicate that ROCK and MLCK play nonredundant roles in regulating myosin II functions, and that a subset of myosin II, regulated by the Rho small GTPase, may be responsible for the regulation of traction forces in migrating fibroblasts.

show abstract

Different Molecular Motors Mediate Platelet-derived Growth Factor and Lysophosphatidic Acid-stimulated Floating Collagen Matrix Contraction

Cited by 49 publications

References 48 publications

Collagen Fibril Flow and Tissue Translocation Coupled to Fibroblast Migration in 3D Collagen Matrices

Collagen Fibril Flow and Tissue Translocation Coupled to Fibroblast Migration in 3D Collagen Matrices

Interactions of primary fibroblasts and keratinocytes with extracellular matrix proteins: contribution of α2β1 integrin

Traction forces of fibroblasts are regulated by the Rho-dependent kinase but not by the myosin light chain kinase

Contact Info

Product

Resources

About