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Faculté de Médecine, Faculté des Sciences Université Paris XII, Institut National de la Santé et de la Recherche Médicale, Unité 492 de Physiopathologie et Thérapeutique Respiratoire, 94010 Créteil; Faculté de Médecine, Laboratoire d'Enzymologie et de Chimie des Protéines, 37032 Tours Cedex; and Département des Sciences du Vivant, Service de Neurovirologie, Commissariat à l'Énergie Atomique, 92265 Fontenay aux Roses, France
Epidemiological and experimental
studies suggest that diesel exhaust particles (DEPs) may be associated
with increased respiratory mortality and morbidity. Several recent
studies have also shown that DEPs increase the production of
inflammatory cytokines by human bronchial epithelium (HBE) cells in
vitro. The present study investigates the effects of DEPs on the
interaction of l-HBE cells (16HBE14o-) with the cell and matrix
microenvironment based on evaluation of integrin-type cell/matrix
ligand expression, cytoskeleton (CSK) stiffness, and matrix remodeling
via matrix metalloproteinase (MMP)-1, MMP-2, and MMP-9 expression. The
results showed that DEP exposure induced: 1) a net
dose-dependent decrease in CSK stiffness through actin fibers,
2) a concomitant specific reduction of both
3- and
1-integrin subunits extensively
expressed on the HBE cell surface, 3) a decrease in the
level of CD44, which is a major HBE cell-cell and HBE cell-matrix
adhesion molecule; and 4) an isolated decrease in MMP-1
expression without any change in tissue inhibitor of matrix
metalloproteinase (TIMP)-1 or TIMP-2 tissue inhibitors. Restrictive
modulation of cell-matrix interaction, cell-cell connection, CSK
stiffness, and fibrillary collagen remodeling results in a decreased
wound closure capacity and an increased deadhesion capacity. In
conclusion, on the basis of these results, we can propose that, in
addition to their ability to increase the production of inflammatory
cytokines, DEPs could also alter the links between actin CSK and the
extracellular matrix, suggesting that they might facilitate HBE cell
detachment in vivo.
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