| کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
|---|---|---|---|---|
| 3353438 | 1216859 | 2011 | 13 صفحه PDF | دانلود رایگان |
SummaryPolarized segregation of proteins in T cells is thought to play a role in diverse cellular functions including signal transduction, migration, and directed secretion of cytokines. Persistence of this polarization can result in asymmetric segregation of fate-determining proteins during cell division, which may enable a T cell to generate diverse progeny. Here, we provide evidence that a lineage-determining transcription factor, T-bet, underwent asymmetric organization in activated T cells preparing to divide and that it was unequally partitioned into the two daughter cells. This unequal acquisition of T-bet appeared to result from its asymmetric destruction during mitosis by virtue of concomitant asymmetric segregation of the proteasome. These results suggest a mechanism by which a cell may unequally localize cellular activities during division, thereby imparting disparity in the abundance of cell fate regulators in the daughter cells.
► A dividing T cell unequally apportions T-bet to its daughter cells
► Localized destruction of T-bet occurs in the setting of proteasome asymmetry
► Phosphorylation of T-bet is critical for its degradation and asymmetry
► Inhibiting proteasome activity or asymmetry prevents unequal T-bet partitioning
Journal: - Volume 34, Issue 4, 22 April 2011, Pages 492–504