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Publication : Dynein drives nuclear rotation during forward progression of motile fibroblasts.

First Author  Levy JR Year  2008
Journal  J Cell Sci Volume  121
Issue  Pt 19 Pages  3187-95
PubMed ID  18782860 Mgi Jnum  J:139656
Mgi Id  MGI:3809336 Doi  10.1242/jcs.033878
Citation  Levy JR, et al. (2008) Dynein drives nuclear rotation during forward progression of motile fibroblasts. J Cell Sci 121(Pt 19):3187-95
abstractText  During directed cell migration, the movement of the nucleus is coupled to the forward progression of the cell. The microtubule motor cytoplasmic dynein is required for both cell polarization and cell motility. Here, we investigate the mechanism by which dynein contributes to directed migration. Knockdown of dynein slows protrusion of the leading edge and causes defects in nuclear movements. The velocity of nuclear migration was decreased in dynein knockdown cells, and nuclei were mislocalized to the rear of motile cells. In control cells, we observed that wounding the monolayer stimulated a dramatic induction of nuclear rotations at the wound edge, reaching velocities up to 8.5 degrees/minute. These nuclear rotations were significantly inhibited in dynein knockdown cells. Surprisingly, centrosomes do not rotate in concert with the nucleus; instead, the centrosome remains stably positioned between the nucleus and the leading edge. Together, these results suggest that dynein contributes to migration in two ways: (1) maintaining centrosome centrality by tethering microtubule plus ends at the cortex; and (2) maintaining nuclear centrality by asserting force directly on the nucleus.
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