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α4β1-dependent adhesion strengthening under mechanical strain is regulated by paxillin association with the α4-cytoplasmic domain

Author: Alon Ronen
Benoit Martin
Feigelson Sara W.
Ginsberg Mark H.
Grabovsky Valentin
Ingber Donald E.
Manevich Eugenia
Matthews Benjamin D.
Overby Darryl R.
Rose David M.
Schmitz Julia
Shinder Vera
Sokolovsky-Eisenberg Maya
Winter Eitan
Publication venue: The Rockefeller University Press
Publication date: 19/12/2005
Field of study

The capacity of integrins to mediate adhesiveness is modulated by their cytoplasmic associations. In this study, we describe a novel mechanism by which α4-integrin adhesiveness is regulated by the cytoskeletal adaptor paxillin. A mutation of the α4 tail that disrupts paxillin binding, α4(Y991A), reduced talin association to the α4β1 heterodimer, impaired integrin anchorage to the cytoskeleton, and suppressed α4β1-dependent capture and adhesion strengthening of Jurkat T cells to VCAM-1 under shear stress. The mutant retained intrinsic avidity to soluble or bead-immobilized VCAM-1, supported normal cell spreading at short-lived contacts, had normal α4-microvillar distribution, and responded to inside-out signals. This is the first demonstration that cytoskeletal anchorage of an integrin enhances the mechanical stability of its adhesive bonds under strain and, thereby, promotes its ability to mediate leukocyte adhesion under physiological shear stress conditions

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PubMed Central

eScholarship - University of California

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Alpha4beta1-dependent adhesion strengthening under mechanical strain is regulated by paxillin association with the alpha4-cytoplasmic domain.

Author: Alon Ronen
Benoit Martin
Feigelson Sara W
Ginsberg Mark H
Grabovsky Valentin
Ingber Donald E
Manevich Eugenia
Matthews Benjamin D
Overby Darryl R
Rose David M
Schmitz Julia
Shinder Vera
Sokolovsky-Eisenberg Maya
Winter Eitan
Publication venue: eScholarship, University of California
Publication date: 01/12/2005
Field of study

The capacity of integrins to mediate adhesiveness is modulated by their cytoplasmic associations. In this study, we describe a novel mechanism by which alpha4-integrin adhesiveness is regulated by the cytoskeletal adaptor paxillin. A mutation of the alpha4 tail that disrupts paxillin binding, alpha4(Y991A), reduced talin association to the alpha4beta1 heterodimer, impaired integrin anchorage to the cytoskeleton, and suppressed alpha4beta1-dependent capture and adhesion strengthening of Jurkat T cells to VCAM-1 under shear stress. The mutant retained intrinsic avidity to soluble or bead-immobilized VCAM-1, supported normal cell spreading at short-lived contacts, had normal alpha4-microvillar distribution, and responded to inside-out signals. This is the first demonstration that cytoskeletal anchorage of an integrin enhances the mechanical stability of its adhesive bonds under strain and, thereby, promotes its ability to mediate leukocyte adhesion under physiological shear stress conditions

eScholarship - University of California