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Laminin-332 and α3β1 integrin-supported migration of bronchial epithelial cells is modulated by fibronectin. | LitMetric

Laminin-332 and α3β1 integrin-supported migration of bronchial epithelial cells is modulated by fibronectin.

Am J Respir Cell Mol Biol

1 Department of Cell and Molecular Biology and Department of Medicine, Division of Pulmonary and Critical Care Medicine, Northwestern University Feinberg School of Medicine, Chicago, Illinois.

Published: November 2013

AI Article Synopsis

  • The bronchiolar epithelium repair after damage involves cell migration over an extracellular matrix made up of molecules like fibronectin and laminin, which support movement and adhesion.
  • BEP2D and NHBE cells were studied to understand how laminin and fibronectin affect their adhesion and migration, revealing that these cells move faster on a matrix rich in laminin α3β3γ2 (LM332) compared to fibronectin.
  • Fibronectin was found to enhance the adhesion of these cells to LM332 surfaces, indicating it plays a key adhesive role in supporting migration during airway epithelial wound healing.

Article Abstract

The repair of the bronchiolar epithelium damaged by cell-mediated, physical, or chemical insult requires epithelial cell migration over a provisional matrix composed of complexes of extracellular matrix molecules, including fibronectin and laminin. These matrix molecules support migration and enhance cell adhesion. When cells adhere too tightly to their matrix they fail to move; but if they adhere too little, they are unable to develop the traction force necessary for motility. Thus, we investigated the relative contributions of laminin and fibronectin to bronchiolar cell adhesion and migration using the immortalized bronchial lung epithelial cell line (BEP2D) and normal human bronchial epithelial (NHBE) cells, both of which assemble a laminin α3β3γ2 (LM332)/fibronectin-rich matrix. Intriguingly, BEP2D and NHBE cells migrate significantly faster on an LM332-rich matrix than on fibronectin. Moreover, addition of fibronectin to LM332 matrix suppresses motility of both cell types. Finally, fibronectin enhances the adhesion of both BEP2D and NHBE cells to LM332-coated surfaces. These results suggest that fibronectin fine tunes LM332-mediated migration by boosting bronchiolar cell adhesion to substrate. We suggest that, during epithelial wound healing of the injured airway, fibronectin plays an important adhesive role for laminin-driven epithelial cell motility by promoting a stable cellular interaction with the provisional matrix.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3931100PMC
http://dx.doi.org/10.1165/rcmb.2012-0509OCDOI Listing

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