Rac1 is required for cell proliferation and G2/M progression
KA Moore, R Sethi, AM Doanes, TM Johnson… - Biochemical …, 1997 - portlandpress.com
KA Moore, R Sethi, AM Doanes, TM Johnson, JB Pracyk, M Kirby, K Irani…
Biochemical journal, 1997•portlandpress.comWe have transiently expressed a dominant negative form of rac1 (N17rac1) using adenoviral-
mediated gene transfer. The level of N17rac1 expression is demonstrated to be proportional
to the multiplicity of infection. Expression of N17rac1 in Rat 2 fibroblasts results in cytostatic
growth arrest. Cell-cycle analysis demonstrates that cells expressing N17rac1 accumulate in
G2/M. These results suggest that rac1 is required for cell proliferation and provide the first
demonstration in mammalian cells of a role for small GTP-binding proteins in the G2/M …
mediated gene transfer. The level of N17rac1 expression is demonstrated to be proportional
to the multiplicity of infection. Expression of N17rac1 in Rat 2 fibroblasts results in cytostatic
growth arrest. Cell-cycle analysis demonstrates that cells expressing N17rac1 accumulate in
G2/M. These results suggest that rac1 is required for cell proliferation and provide the first
demonstration in mammalian cells of a role for small GTP-binding proteins in the G2/M …
We have transiently expressed a dominant negative form of rac1 (N17rac1) using adenoviral-mediated gene transfer. The level of N17rac1 expression is demonstrated to be proportional to the multiplicity of infection. Expression of N17rac1 in Rat 2 fibroblasts results in cytostatic growth arrest. Cell-cycle analysis demonstrates that cells expressing N17rac1 accumulate in G2/M. These results suggest that rac1 is required for cell proliferation and provide the first demonstration in mammalian cells of a role for small GTP-binding proteins in the G2/M transition.
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