Abstract

Adhesion of cells to one another and the extracellular matrix is a fundamental characteristic of all multicellular organisms. Recent work has shown that mechanical force applied to cell adhesion receptors, including the cadherins and integrins, can affect the activities of Rho family GTPases, thereby influencing the organization of the cytoskeleton and the stiffness of cells. This grant is aimed at understanding how signals from cadherins produce the cytoskeletal rearrangements necessary for cell stiffening, with an emphasis on understanding where the cell derives the energy required to support cell stiffening. In our preliminary studies, we discovered that application of force to E-cadherin stimulates glucose uptake and increases glucose transporters on the plasma membrane. Using molecular, biochemical and cell biological approaches, Aim 1 will define the molecular mechanism for how E-cadherin stimulates glucose uptake.
Aim 2 will determine how increased glucose uptake facilitates the cytoskeletal rearrangements required for stiffening. Here we aim to identify the RhoA activator and signaling pathways involved. Using magnetic tweezers and beads coated with the extracellular domain of E-cadherin we will determine how force-induced glucose uptake leads to the strengthening of cadherin-mediated adhesions.
The final aim will investigate how the force-induced glucose impacts the actin cytoskeleton and its regulation of cell growth and metastasis in vivo. Mouse models of breast cancer will be employed to explore the consequence that promoting E-cadherin mediated force transmission has on disease. When the work in this proposal is complete, we expect to establish a new paradigm for how glucose uptake is stimulated by force and facilitates cell stiffening. This paradigm can be applied to better understand force transmission by other proteins and will lay the groundwork for understanding if and how E- cadherin force transmission protects against the development of cancer.

Public Health Relevance

Despite significant advances in understanding its origins, biology, and treatment, breast cancer remains the second leading cause of cancer death in women. In this proposal, we seek to define how three newly identified proteins promote stiffening of breast cancer cells. Understanding the mechanisms by which these proteins act may lead to development of novel inhibitors and improved therapies to slow breast cancer and metastasis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM112805-01A1
Application #
8962257
Study Section
Intercellular Interactions (ICI)
Program Officer
Nie, Zhongzhen
Project Start
2015-08-15
Project End
2020-06-30
Budget Start
2015-08-15
Budget End
2016-06-30
Support Year
1
Fiscal Year
2015
Total Cost
$298,225
Indirect Cost
$100,725

  Institution

Name
University of Iowa
Department
Biochemistry
Type
Schools of Medicine
DUNS #
062761671
City
Iowa City
State
IA
Country
United States
Zip Code
52246

  Publications

Salvi, Alicia M; DeMali, Kris A (2018) Mechanisms linking mechanotransduction and cell metabolism. Curr Opin Cell Biol 54:114-120
Bays, Jennifer L; Campbell, Hannah K; Heidema, Christy et al. (2017) Linking E-cadherin mechanotransduction to cell metabolism through force-mediated activation of AMPK. Nat Cell Biol 19:724-731
Bays, Jennifer L; DeMali, Kris A (2017) It takes energy to resist force. Cell Cycle 16:1733-1734
Bays, Jennifer L; DeMali, Kris A (2017) Vinculin in cell-cell and cell-matrix adhesions. Cell Mol Life Sci 74:2999-3009
Campbell, Hannah K; Maiers, Jessica L; DeMali, Kris A (2017) Interplay between tight junctions & adherens junctions. Exp Cell Res 358:39-44