Rapid leukocyte integrin activation by chemokines |
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Authors: | Carlo Laudanna Ji Yun Kim Gabriela Constantin Eugene C. Butcher |
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Affiliation: | Authors' addresses;Carlo Laudanna1, Ji Yun Kim2, Gabriela Constantin1, Eugene Butcher2, 1Section of General Pathology, Department of Pathology, Faculty of Medicine, University of Verona, 37138, Verona, Italy.2Department of Pathology, Stanford University School of Medicine, Stanford, California, 94305 and the Center for Molecular Biology and Medicine, the Veteran Affairs Health Care System, Palo Alto, California, 94304, CA, USA. |
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Abstract: | Summary: Chemokines control selective targeting of circulating leukocytes to the microvasculature by triggering inside-out signal transduction pathways leading to integrin-dependent adhesion. Integrin activation by chemokines is very rapid, is downmodulated within minutes and appears to involve both enhanced heterodimer lateral mobility on the plasma membrane, facilitating encounters with dispersed ligand, as well as induction of a high-affinity state. These two modalities of integrin activation by chemokines involve distinct signaling pathways in the cell, yet complement each other functionally, allowing binding of rolling cells under conditions of low as well as high ligand density. Recent data show that chemokines generate both pro- and anti-adhesive intracellular signaling events, whose equilibrium is likely to be relevant to the kinetics of adhesion and de-adhesion, and to cell movement during diapedesis and chemotaxis. Importantly, chemokines utilize different signaling mechanisms to modulate the activity of distinct integrin subtypes. These recent advances suggest that chemokines may regulate adhesive responses of immune cells based not only on patterns of chemokine receptor expression, but also on variable signaling pathways that can modulate the pro-adhesive responses of leukocytes as a function of their differentiated state, and of the local microenvironment. |
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