Abstract

Proteins involved in the attachment of actin to cell membranes, particularly plasma membranes, will be investigated. Two types of actin-membrane association will be analyzed: (1) that which may involve a class of proteins found in many cell types that we and others have shown to be closely related to erythrocyte spectrin, and (2) that which occurs in specialized regions of membranes, such as in fibroblast adhesion plaques, where bundles of actin filaments terminate. A strategy of sequential analysis will be used to identify and characterize the components that link actin to the membrane in these different locations. During the investigation of non-erythrocyte spectrins we will attempt to identify proteins involved in linking spectrin itself to membranes. A variety of biochemical, immunological and electron microscopic approaches will be used to define the relationship between spectrin and cell surface and membrane components in non-erythroid cells. The role of spectrin in regulating the lateral mobility and distribution of cell surface components will be studied using fluorescence recovery after photobleaching and other techniques. We will try to dissociate spectrin from the plasma membrane by microinjecting live cells with antibodies against spectrin or against proteins to which it binds. Regarding the proteins involved in attachment of actin microfilament bundles to the plasma membrane, we will concentrate on the properties of vinculin and 215K, a new protein that we have recently identified infibroblast adhesion plaques. New proteins interacting with vinculin and 215K will be identified using affinity chromatography and chemical cross-linking reagents. In an attempt to develop a new model system for examining """"""""end-on"""""""" attachment of actin filaments to membranes, we will isolate thefascia adherens from cardiac muscle. This structrure is responsible for the membrane anchorage of actin in cardiac myofibrils. Again a strategy of sequential analysis will be used to define the components involved in attaching the actin filaments to this membrane.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM029860-05
Application #
3277562
Study Section
Cellular Biology and Physiology Subcommittee 1 (CBY)
Project Start
1981-04-01
Project End
1988-03-31
Budget Start
1985-04-01
Budget End
1986-03-31
Support Year
5
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Type
Schools of Medicine
DUNS #
078861598
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Thompson, William R; Yen, Sherwin S; Uzer, Gunes et al. (2018) LARG GEF and ARHGAP18 orchestrate RhoA activity to control mesenchymal stem cell lineage. Bone 107:172-180
Xu, Wenjing; Wittchen, Erika S; Hoopes, Samantha L et al. (2018) Small GTPase Rap1A/B Is Required for Lymphatic Development and Adrenomedullin-Induced Stabilization of Lymphatic Endothelial Junctions. Arterioscler Thromb Vasc Biol 38:2410-2422
Graham, David M; Andersen, Tomas; Sharek, Lisa et al. (2018) Enucleated cells reveal differential roles of the nucleus in cell migration, polarity, and mechanotransduction. J Cell Biol 217:895-914
Schaefer, Antje; van Duijn, Trynette J; Majolee, Jisca et al. (2017) Endothelial CD2AP Binds the Receptor ICAM-1 To Control Mechanosignaling, Leukocyte Adhesion, and the Route of Leukocyte Diapedesis In Vitro. J Immunol 198:4823-4836
Thompson, Peter M; Ramachandran, Srinivas; Case, Lindsay B et al. (2017) A Structural Model for Vinculin Insertion into PIP2-Containing Membranes and the Effect of Insertion on Vinculin Activation and Localization. Structure 25:264-275
Burridge, Keith (2017) Focal adhesions: a personal perspective on a half century of progress. FEBS J 284:3355-3361
Scott, David W; Tolbert, Caitlin E; Burridge, Keith (2016) Tension on JAM-A activates RhoA via GEF-H1 and p115 RhoGEF. Mol Biol Cell 27:1420-30
Lawson, Campbell D; Fan, Cheng; Mitin, Natalia et al. (2016) Rho GTPase Transcriptome Analysis Reveals Oncogenic Roles for Rho GTPase-Activating Proteins in Basal-like Breast Cancers. Cancer Res 76:3826-37
Burridge, Keith; Guilluy, Christophe (2016) Focal adhesions, stress fibers and mechanical tension. Exp Cell Res 343:14-20
Morillon 2nd, Y Maurice; Lessey-Morillon, Elizabeth Chase; Clark, Matthew et al. (2016) Antibody Binding to CD4 Induces Rac GTPase Activation and Alters T Cell Migration. J Immunol 197:3504-3511

Showing the most recent 10 out of 158 publications