Abstract

Paxillin is a multi-domain, 68 KDa phosphoprotein that localizes to specialized actin-membrane-extracellular matrix attachment sites in cultured mammalian cells and in vivo. We will test the hypothesis that paxillin functions as a scaffold/adapter protein at the plasma membrane to coordinate the interplay between adhesion and growth factor-derived signals that result in reorganization of the actin cytoskeleton and control cell migration.
Aim 1 will examine the importance of the interaction between paxillin and the PKL-PIX-PAK (p21-activated kinase)-Nck complex, focusing on its role in effecting PAK function. The critical role of adhesion and growth factor regulated PKL tyrosine phosphorylation will also be determined.
Aim 2 will utilize paxillin null and PTP-PEST null fibroblasts to examine the essential role for paxillin-PTP-PEST interactions in controlling PTP-PEST-mediated effects on cell spreading, motility and p21-GTPase signaling.
Aim 3 will determine how the differential expression of two paxillin related proteins, Hic-5 and paxillin delta modulate integrin signaling to paxillin and associated proteins to effect cell migration and morphology during epithelial-mesenchymal transition. To accomplish these Aims cytoskeletal organization will be evaluated by immunofluorescence microscopy. Time-lapse video microscopy, Boyden and Dunn chamber assays will permit evaluation of dynamic cell shape and motility changes. Phosphorylation specific antibodies will be used to identify changes in the activity and location of focal adhesion and cytoskeletal proteins as well MAP kinase and other signaling intermediates. Rho-family GTPases activities will be assessed using GST-GTPase effector protein binding domains. It is anticipated that information gained from the proposed study will provide insight into the molecular mechanisms by which cells interact and communicate with their environment to regulate normal and neoplastic cell migration and will potentially identify protein-protein interactions/pathways that might in the future serve as targets for therapeutic intervention.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM047607-16
Application #
7099444
Study Section
Special Emphasis Panel (ZRG1-SSS-U (02))
Program Officer
Flicker, Paula F
Project Start
1991-08-05
Project End
2008-07-31
Budget Start
2006-08-01
Budget End
2007-07-31
Support Year
16
Fiscal Year
2006
Total Cost
$320,604
Indirect Cost

  Institution

Name
Upstate Medical University
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
058889106
City
Syracuse
State
NY
Country
United States
Zip Code
13210

  Publications

Gulvady, Anushree C; Dubois, Fatemeh; Deakin, Nicholas O et al. (2018) Hic-5 expression is a major indicator of cancer cell morphology, migration, and plasticity in three-dimensional matrices. Mol Biol Cell 29:1704-1717
Goreczny, Gregory J; Forsythe, Ian J; Turner, Christopher E (2018) Hic-5 regulates fibrillar adhesion formation to control tumor extracellular matrix remodeling through interaction with tensin1. Oncogene 37:1699-1713
Wang, Jing; Quach, Andy; Brasch, Megan E et al. (2017) On-command on/off switching of progenitor cell and cancer cell polarized motility and aligned morphology via a cytocompatible shape memory polymer scaffold. Biomaterials 140:150-161
Dubois, Fatemeh; Alpha, Kyle; Turner, Christopher E (2017) Paxillin regulates cell polarization and anterograde vesicle trafficking during cell migration. Mol Biol Cell 28:3815-3831
Rashid, Mamunur; Belmont, Judson; Carpenter, David et al. (2017) Neural-specific deletion of the focal adhesion adaptor protein paxillin slows migration speed and delays cortical layer formation. Development 144:4002-4014
Jacob, Andrew E; Amack, Jeffrey D; Turner, Christopher E (2017) Paxillin genes and actomyosin contractility regulate myotome morphogenesis in zebrafish. Dev Biol 425:70-84
Goreczny, G J; Ouderkirk-Pecone, J L; Olson, E C et al. (2017) Hic-5 remodeling of the stromal matrix promotes breast tumor progression. Oncogene 36:2693-2703
Jacob, Andrew E; Turner, Christopher E; Amack, Jeffrey D (2016) Evolution and Expression of Paxillin Genes in Teleost Fish. PLoS One 11:e0165266
Goreczny, Gregory J; Wormer, Duncan B; Turner, Christopher E (2015) A Simplified System for Evaluating Cell Mechanosensing and Durotaxis In Vitro. J Vis Exp :e52949
Deakin, Nicholas O; Turner, Christopher E (2014) Paxillin inhibits HDAC6 to regulate microtubule acetylation, Golgi structure, and polarized migration. J Cell Biol 206:395-413

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