Abstract

Chemotaxis, or directed cell movement toward a small molecule ligand, plays a key role in many cellular and physiological responses, including metastasis of cancer cells, movement of neutrophils and macrophages in immune system reactions, migration of embryonic cells during development, and aggregation of Dictyostelium during development. In each of these varied cell types and processes, the responding cells are able to amplify a shallow extracellular chemoattractant gradient into a very steep intracellular gradient and thus translate the directional signal into directional cell movement. Fulfillment of this requirement occurs through an integrated circuit of signaling pathways that are highly conserved through evolution between Dictyostelium and man. Recent findings establish that the Ras and the related GTPase Rap1 are important for directional sensing, pseudopod formation, cell polarization, and cell attachment. Both Ras and Rap1 are preferentially activated at the leading edge of chemotaxing Dictyostelium cells and abrogation of their function impairs this process. This proposal focuses on the further examination of the roles of Ras and Rap1 of using Dictyostelium cells, which are amenable to biochemical, genetic, and cell biological approaches. We propose to identify the mechanisms by which the activations of Ras and Rap1 are regulated and spatially restricted to the leading edge of chemotaxing cells. This will be achieved through the analysis of a RasGEF complex and by examining defects in chemotaxis resulting from disruptions of specific GTPase activating proteins (GAPs) for Ras and for Rap1. Through the examination of the spatial and temporal regulation of activated Ras and Rap1 strains in which normal Ras and Rap1 activity is altered, we will elucidate the mechanisms by which cells orient themselves in a chemoattractant gradient. We propose to determine how Ras and Rap1 help mediate chemotaxis through the identification of downstream effectors. The function of these will be examined through the analysis of their null mutations with the aid of real-type fluorescent reporters and biochemical assays that reveal different components of directional sensing, pseudopod formation, and cell polarization. The work proposed in this application should provide new and important insights into mechanisms that control this highly evolutionarily conserved cell biological process, and thus provide the needed background to elucidate the cellular basis underlying a variety of human diseases, including those affecting innate immunity and metastasis of cancer cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM037830-25
Application #
8006445
Study Section
Cell Structure and Function (CSF)
Program Officer
Maas, Stefan
Project Start
1986-07-01
Project End
2012-04-30
Budget Start
2011-01-01
Budget End
2012-04-30
Support Year
25
Fiscal Year
2011
Total Cost
$609,441
Indirect Cost

  Institution

Name
University of California San Diego
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
804355790
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Liu, Youtao; Lacal, Jesus; Firtel, Richard A et al. (2018) Connecting G protein signaling to chemoattractant-mediated cell polarity and cytoskeletal reorganization. Small GTPases 9:360-364
Scavello, Margarethakay; Petlick, Alexandra R; Ramesh, Ramya et al. (2017) Protein kinase A regulates the Ras, Rap1 and TORC2 pathways in response to the chemoattractant cAMP in Dictyostelium. J Cell Sci 130:1545-1558
Liu, Youtao; Lacal, Jesus; Veltman, Douwe M et al. (2016) A G?-Stimulated RapGEF Is a Receptor-Proximal Regulator of Dictyostelium Chemotaxis. Dev Cell 37:458-72
Khanna, Ankita; Lotfi, Pouya; Chavan, Anita J et al. (2016) The small GTPases Ras and Rap1 bind to and control TORC2 activity. Sci Rep 6:25823
Bastounis, Effie; Álvarez-González, Begoña; del Álamo, Juan C et al. (2016) Cooperative cell motility during tandem locomotion of amoeboid cells. Mol Biol Cell 27:1262-71
Álvarez-González, Begoña; Meili, Ruedi; Bastounis, Effie et al. (2015) Three-dimensional balance of cortical tension and axial contractility enables fast amoeboid migration. Biophys J 108:821-832
Bastounis, Effie; Meili, Ruedi; Álvarez-González, Begoña et al. (2014) Both contractile axial and lateral traction force dynamics drive amoeboid cell motility. J Cell Biol 204:1045-61
Alvarez-González, Begoña; Meili, Ruedi; Firtel, Richard et al. (2014) Cytoskeletal Mechanics Regulating Amoeboid Cell Locomotion. Appl Mech Rev 66:
Kölsch, Verena; Shen, Zhouxin; Lee, Susan et al. (2013) Daydreamer, a Ras effector and GSK-3 substrate, is important for directional sensing and cell motility. Mol Biol Cell 24:100-14
del Álamo, Juan C; Meili, Ruedi; Álvarez-González, Begoña et al. (2013) Three-dimensional quantification of cellular traction forces and mechanosensing of thin substrata by fourier traction force microscopy. PLoS One 8:e69850

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