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Publication : α-Dystroglycan hypoglycosylation affects cell migration by influencing β-dystroglycan membrane clustering and filopodia length: A multiscale confocal microscopy analysis.

First Author  Palmieri V Year  2017
Journal  Biochim Biophys Acta Volume  1863
Issue  9 Pages  2182-2191
PubMed ID  28572004 Mgi Jnum  J:255628
Mgi Id  MGI:6104979 Doi  10.1016/j.bbadis.2017.05.025
Citation  Palmieri V, et al. (2017) alpha-Dystroglycan hypoglycosylation affects cell migration by influencing beta-dystroglycan membrane clustering and filopodia length: A multiscale confocal microscopy analysis. Biochim Biophys Acta 1863(9):2182-2191
abstractText  Dystroglycan (DG) serves as an adhesion complex linking the actin cytoskeleton to the extracellular matrix. DG is encoded by a single gene as a precursor, which is constitutively cleaved to form the alpha- and beta-DG subunits. alpha-DG is a peripheral protein characterized by an extensive glycosylation that is essential to bind laminin and other extracellular matrix proteins, while beta-DG binds the cytoskeleton proteins. The functional properties of DG depend on the correct glycosylation of alpha-DG and on the cross-talk between the two subunits. A reduction of alpha-DG glycosylation has been observed in muscular dystrophy and cancer while the inhibition of the interaction between alpha- and beta-DG is associated to aberrant post-translational processing of the complex. Here we used confocal microscopy based techniques to get insights into the influence of alpha-DG glycosylation on the functional properties of the beta-DG, and its effects on cell migration. We used epithelial cells transfected with wild-type and with a mutated DG harboring the mutation T190M that has been recently associated to dystroglycanopathy. We found that alpha-DG hypoglycosylation, together with an increased protein instability, reduces the membrane dynamics of the beta-subunit and its clustering within the actin-rich domains, influencing cell migration and spontaneous cell movement. These results contribute to give novel insights into the involvement of aberrant glycosylation of DG in the developing of muscular dystrophy and tumor metastasis.
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