Abstract
The Dbl oncogene is a putative exchange factor for the small GTPases RhoA and Cdc42, which are involved in actin polymerization into stress fibers and filopodia, respectively. We report here that, upon adhesion to fibronectin, Dbl-transformed NIH3T3 cells display a contracted, polygonal shape with a high number of short stress fibers. In contrast, untransformed NIH3T3 cells acquire the characteristic fibroblast morphology and organize a regular mesh of long stress fibers. We show that in Dbl-transformed and in untransformed NIH3T3 cells the different shape and actin cytoskeleton organization observed in the early steps of adhesion involves activation of distinct GTPases. Upon adhesion to fibronectin, cell morphology of Dbl-transformed NIH3T3 cells depends on activation of RhoA and not of Cdc42. In contrast Cdc42 activation is necessary to untransfected NIH3T3 cells to acquire their fibroblast shape. In both Dbl-transformed and in untransformed NIH3T3 cells a basal Rac activation is necessary to support stress fiber organization, while constitutive Rac activation promotes ruffles and lamellipodia formation. As a consequence of RhoA activation, Dbl-transformed cells show high activity of ROCK-α and CRIK kinases, two known RhoA effectors. In addition Dbl-transformed and NIH3T3 cells expressing the constitutive active form of RhoA are less motile on fibronectin than cells expressing constitutive active Cdc42. We conclude that in NIH3T3 cells in response to fibronectin the expression of the Dbl oncogene leads to a predominant activation of RhoA which both supports the peculiar cell shape and actin cytoskeleton organization in stress fibers and regulates cell motility.
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References
Aspenstrom P . 1999 Curr Opin Cell Biol 11: 95–102
Avraham H and Weinberg RA . 1989 Mol Cell Biol 9: 2058–2066
Bagrodia S, Taylor SJ, Jordon KA, Van Aelst L and Cerione RA . 1998 J Biol Chem 273: 23633–23636
Barry ST, Flinn HM, Humphries MJ, Critchley DR and Ridley AJ . 1997 Cell Adhes Commun 4: 387–398
Cepko CL, Roberts BE and Mulligan RC . 1984 Cell 37: 1053–1062
Chardin P, Boquet P, Madaule P, Popoff MR, Rubin EJ and Gill DM . 1989 EMBO J 8: 1087–1092
Clark EA, King WG, Brugge JS, Symons M and Hynes RO . 1998 J Cell Biol 142: 573–586
Coso OA, Chiariello M, Yu JC, Teramoto H, Crespo P, Xu N, Miki T and Gutkind JS . 1995 Cell 81: 1137–1146
Dartsch PC, Ritter M, Haussinger D and Lang F . 1994 Eur J Cell Biol 63: 316–325
Defilippi P, Olivo C, Tarone G, Mancini P, Torrisi MR and Eva A . 1997 Oncogene 14: 1933–1943
Defilippi P, Olivo C, Venturino M, Dolce L, Silengo L and Tarone G . 1999 Micr Res Tech 47: 67–78
Di Cunto F, Calautti E, Hsiao J, Ong L, Topley G, Turco E and Dotto GP . 1998 J Biol Chem 273: 29706–29711
Dillon ST and Feig LA . 1995 Methods Enzymol 256: 174–184
Felice GR, Eason P, Nermut MV and Kellie S . 1990 Eur J Cell Biol 52: 47–59
Flatau G, Lemichez E, Gauthier M, Chardin P, Paris S, Fiorentini C and Boquet P . 1997 Nature 387: 729–733
Hall A . 1998 Science 279: 509–514
Hart MJ, Eva A, Evans T, Aaronson SA and Cerione RA . 1991 Nature 354: 311–314
Hart MJ, Eva A, Zangrilli D, Aaronson SA, Evans T, Cerione RA and Zheng Y . 1994 J Biol Chem 269: 62–65
Hill CS, Winne J and Treisman R . 1995 Cell 81: 1159–1170
Ishizaki T, Naito M, Fujisawa K, Maekawa M, Watanabe N, Saito Y and Narumiya S . 1997 FEBS Lett 404: 118–124
Keely PJ, Westwick JK, Whitehead IP, Der CJ and Parise LV . 1997 Nature 390: 632–636
Lin R, Bagrodia S, Cerione R and Manor D . 1997 Curr Biol 7: 794–797
Michiels F, Habets GG, Stam JC, van der Kammen RA and Collard JG . 1995 Nature 375: 338–340
Minden A, Lin A, Claret FX, Abo A and Karin M . 1995 Cell 81: 1147–1157
Miranti CK, Leng L, Maschberger P, Brugge JS and Shattil SJ . 1998 Curr Biol 8: 1289–1299
Montaner S, Perona R, Saniger L and Lacal JC . 1998 J Biol Chem 273: 12779–12785
Nobes CD and Hall A . 1995 Cell 81: 53–62
Okada CY and Reichsteiner M . 1982 Cell 29: 33–41
Price LS, Leng J, Schwartz MA and Bokoch GM . 1998 Mol Biol Cell 9: 1863–1871
Qiu RG, Abo A, McCormick F and Symons M . 1997 Mol Cell Biol 17: 3449–3458
Qiu RG, Chen J, Kirn D, McCormick F and Symons M . 1995a Nature 374: 457–459
Qiu RG, Chen J, McCormick F and Symons M . 1995b Proc Natl Acad Sci 92: 11781–11785
Ren XD, Kiosses WB and Schwartz MA . 1999 EMBO J 18: 578–585
Ron D, Graziani G, Aaronson SA and Eva A . 1989 Oncogene 4: 1067–1072
Ron D, Zannini M, Lewis M, Wickner RB, Hunt LT, Graziani G, Tronick SR, Aaronson SA and Eva A . 1991 New Biol 3: 372–379
Sander EE, van Delft S, ten Klooster JP, Reid T, van der Kammen RA, Michiels F and Collard JG . 1998 J Cell Biol 143: 1385–1398
Tarone G, Cirillo D, Giancotti FG, Comoglio PM and Marchisio PC . 1985 Exp Cell Res 159: 141–157
Tarone G, Galetto G, Prat M and Comoglio PM . 1982 J Cell Biol 94: 179–186
Van Aelst L and D'Souza-Schorey C . 1997 Genes Dev 11: 2295–2322
Westwick JK, Lambert QT, Clark GJ, Symons M, Van Aelst L, Pestell RG and Der CJ . 1997 Mol Cell Biol 17: 1324–1335
Whitehead IP, Campbell S, Rossman KL and Der CJ . 1997 Biochim Biophys Acta 1332: F1–F23
Wu WJ, Lin R, Cerione RA and Manor D . 1998 J Biol Chem 273: 16655–16658
Yron I, Deckert M, Reff ME, Munshi A, Schwartz MA and Altmen A . 1999 Cell Adhes Commun 7: 1–11
Zangrilli D and Eva A . 1995 Methods Enzymol 256: 347–358
Zhang S, Han J, Sells MA, Chernoff J, Knaus UG, Ulevitch RJ and Bokoch GM . 1995 J Biol Chem 270: 23934–23936
Zhou K, Wang Y, Gorski JL, Nomura N, Collard J and Bokoch GM . 1998 J Biol Chem 273: 16782–16786
Acknowledgements
We are indebted to Drs P Boquet, R Cerione, S Gutkind, A Hall, L Lim, and S Narumiya for providing reagents. We also thank Dr F Di Cunto for helpful discussion. C Olivo was supported by a short term fellowship by National Research Council to visit Dr P Boquet laboratory. This work was supported by grants of the Italian Association for Cancer Research (AIRC), MURST ‘Cofinanziamento Programmi di Ricerca', Istituto Superiore di Sanita', Progetto ‘Sostituzioni funzionali, organi artificiali e trapianti di organi' and from Ministero della Sanità, Progetto finalizzato N. ICSO70.2/RF95.221.
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Olivo, C., Vanni, C., Mancini, P. et al. Distinct involvement of Cdc42 and RhoA GTPases in actin organization and cell shape in untransformed and Dbl oncogene transformed NIH3T3 cells. Oncogene 19, 1428–1436 (2000). https://doi.org/10.1038/sj.onc.1203440
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DOI: https://doi.org/10.1038/sj.onc.1203440
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