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Molecular and Cellular Biology, April 2001, p. 2847-2857, Vol. 21, No. 8
Department of Biochemistry and
Biophysics1 and Department of
Pharmacology,2 Lineberger Comprehensive Cancer
Center, University of North Carolina at Chapel Hill, Chapel Hill, North
Carolina 27599
Received 23 January 2001/Accepted 26 January 2001
The Rho family of Ras-related proteins, which includes Rac1, RhoA,
and Cdc42, is distinguished from other members of the Ras superfamily
of small GTPases in that its members possess additional sequences
positioned between
0270-7306/01/$04.00+0 DOI: 10.1128/MCB.21.8.2847-2857.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.
The Insert Region of Rac1 Is Essential for Membrane
Ruffling but Not Cellular Transformation
-strand 5 and
-helix 4, designated the insert
region. Previous studies have established the importance of an intact
insert region for the transforming, but not actin cytoskeletal
reorganization, activities of Cdc42 and RhoA. Similarly, the insert
region was determined to be essential for Rac1-mediated mitogenesis.
Additionally, an intact insert region was also determined to be
required for the antiapoptotic activity of Rac1 as well as for Rac1
activation of reactive oxygen species and the NF-
B transcription
factor. However, it has not been determined whether the insert region
is important for Rac1-mediated growth transformation. In this study, we
assessed the requirement for the insert region in Rac1 transformation
and signaling in NIH 3T3 cells. Unexpectedly, we found that a mutant of
constitutively activated Rac1 that lacked the insert region retained
potent transforming activity. The insert region of Rac1 was dispensable
for Rac1 stimulation of transcription from the cyclin D1 promoter and
for activation of the c-Jun, NF-
B, and E2F-1 transcription factors
but was essential for Rac1 induction of serum response factor activity.
While an intact insert region was dispensable for inducing reactive
oxygen species production in vivo, it was required for Rac1 induction
of lamellipodia. When taken together, these results show that the
insert region of Rac1 serves roles in regulating actin organization and
cell growth that are distinct from those of the analogous regions of
Cdc42 and RhoA and support its involvement in regulating specific
downstream effector interactions.
*
Corresponding author. Mailing address: Lineberger
Comprehensive Cancer Center, University of North Carolina at Chapel
Hill, Chapel Hill, NC 27599. Phone: (919) 966-5634. Fax: (919)
966-0162. E-mail: cjder{at}med.unc.edu.
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