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Mechanotransduction through CytoskeletonThe goal of this project was to characterize the molecular mechanism by which cells recognize and respond to physical forces in their local environment. The project was based on the working hypothesis that cells sense mechanical stresses, such as those due to gravity, through their cell surface adhesion receptors (e.g., integrins) and that they respond as a result of structural arrangements with their internal cytoskeleton (CSK) which are orchestrated through use of tensegrity architecture. In this project, we carried out studies to define the architectural and molecular basis of cellular mechanotransduction. Our major goal was to define the molecular pathway that mediates mechanical force transfer between integrins and the CSK and to determine how mechanical deformation of integrin-CSK linkages is transduced into a biochemical response. Elucidation of the mechanism by which cells sense mechanical stresses through integrins and translate them into a biochemical response should help us to understand the molecular basis of the cellular response to gravity as well as many other forms of mechanosensation and tissue regulation. The specific aims of this proposal were: 1. To define the molecular basis of mechanical coupling between integrins, vinculin, and the actin CSK; 2. To develop a computer simulation of how mechanical stresses alter CSK structure and test this model in living cells; 3. To determine how mechanical deformation of integrin-CSK linkages is transduced into a biochemical response.
Document ID
20020071121
Acquisition Source
Goddard Space Flight Center
Document Type
Contractor or Grantee Report
Authors
Ingber, Donald
(Children's Hospital Boston, MA United States)
Date Acquired
September 7, 2013
Publication Date
January 1, 2002
Subject Category
Life Sciences (General)
Funding Number(s)
CONTRACT_GRANT: NAG5-4839
Distribution Limits
Public
Copyright
Work of the US Gov. Public Use Permitted.
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