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Vol. 13, Issue 5, 1722-1734, May 2002
Department of Physiology, School of Medicine, University of
Pennsylvania, Philadelphia, Pennsylvania 19104-6085
We screened for polypeptides that interact specifically with dynein
and identified a novel 24-kDa protein (PLAC-24) that binds directly to
dynein intermediate chain (DIC). PLAC-24 is not a dynactin
subunit, and the binding of PLAC-24 to the dynein intermediate chain is
independent of the association between dynein and dynactin. Immunocytochemistry using PLAC-24-specific polyclonal antibodies revealed a punctate perinuclear distribution of the polypeptide in
fibroblasts and isolated epithelial cells. However, as epithelial cells
in culture make contact with adjacent cells, PLAC-24 is specifically
recruited to the cortex at sites of contact, where the protein
colocalizes with components of the adherens junction. Disruption of the
cellular cytoskeleton with latrunculin or nocodazole indicates that the
localization of PLAC-24 to the cortex is dependent on intact actin
filaments but not on microtubules. Overexpression of
-catenin also
leads to a loss of PLAC-24 from sites of cell-cell contact. On the
basis of these data and the recent observation that cytoplasmic dynein
is also localized to sites of cell-cell contact in epithelial cells, we
propose that PLAC-24 is part of a multiprotein complex localized to
sites of intercellular contact that may function to tether microtubule
plus ends to the actin-rich cellular cortex.
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