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Rac1 accumulates in the nucleus during the G2 phase of the cell cycle and promotes cell division.


ABSTRACT: Rac1 regulates a wide variety of cellular processes. The polybasic region of the Rac1 C terminus functions both as a plasma membrane-targeting motif and a nuclear localization sequence (NLS). We show that a triproline N-terminal to the polybasic region contributes to the NLS, which is cryptic in the sense that it is strongly inhibited by geranylgeranylation of the adjacent cysteine. Subcellular fractionation demonstrated endogenous Rac1 in the nucleus and Triton X-114 partition revealed that this pool is prenylated. Cell cycle-blocking agents, synchronization of cells stably expressing low levels of GFP-Rac1, and time-lapse microscopy of asynchronous cells revealed Rac1 accumulation in the nucleus in late G2 and exclusion in early G1. Although constitutively active Rac1 restricted to the cytoplasm inhibited cell division, activated Rac1 expressed constitutively in the nucleus increased the mitotic rate. These results show that Rac1 cycles in and out of the nucleus during the cell cycle and thereby plays a role in promoting cell division.

SUBMITTER: Michaelson D 

PROVIDER: S-EPMC2364699 | biostudies-literature | 2008 May

REPOSITORIES: biostudies-literature

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Rac1 accumulates in the nucleus during the G2 phase of the cell cycle and promotes cell division.

Michaelson David D   Abidi Wasif W   Guardavaccaro Daniele D   Zhou Mo M   Ahearn Ian I   Pagano Michele M   Philips Mark R MR  

The Journal of cell biology 20080428 3


Rac1 regulates a wide variety of cellular processes. The polybasic region of the Rac1 C terminus functions both as a plasma membrane-targeting motif and a nuclear localization sequence (NLS). We show that a triproline N-terminal to the polybasic region contributes to the NLS, which is cryptic in the sense that it is strongly inhibited by geranylgeranylation of the adjacent cysteine. Subcellular fractionation demonstrated endogenous Rac1 in the nucleus and Triton X-114 partition revealed that thi  ...[more]

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