Wild type N-ras displays anti-malignant properties, in part by downregulating decorin.
Autores de IIS La Fe
Participantes ajenos a IIS La Fe
- Dulman RY
- Suzme R
- de Miera EV
- Vega ME
- Nguyen T
- Zavadil J
Grupos
Abstract
Previously, we have shown that wild type N-ras (wt N-ras) harbors an anti-malignant effect against mutated Ras and in tumors without Ras mutations. To investigate the molecular bases of this anti-malignant activity, we have studied the potency of this anti-malignant effect in a model system against SV40 large T antigen (SV40T). We show that wild-type N-ras (wt N-ras) counteracts the effects of SV40T in NIH3T3 cells as seen by a decrease in proliferation, anchorage independence and changes in migration. We also show that wt N-ras elicits the same anti-malignant effects in some human tumor cell lines (HT1080 and MDA-MB-231). Through mRNA and microRNA (miRNAs) expression profiling we have identified genes (decorin) and miRNAs (mir-29A, let-7b) modulated by wt N-ras potentially responsible for the anti-malignant effect. Wt N-ras appears to mediate its anti-malignant effect by downregulating some of the targets of the TGFß pathway and decorin, which are able to reverse the inhibition of migration induced by wt N-ras. Our experiments show that the molecules that mediate the anti-malignant effect by wt N-ras appear to be different from those modulated by transforming N-ras. The components of the pathways modulated by wt N-ras mediating its anti-malignant effects are potential targets for therapeutic intervention in cancer.
Datos de la publicación
- ISSN/ISSNe:
- 0021-9541, 1097-4652
- Tipo:
- Article
- Páginas:
- 2341-2351
- DOI:
- 10.1002/jcp.22969
- PubMed:
- 21809347
- Factor de Impacto:
- 1,978 SCImago ℠
- Cuartil:
- Q1 SCImago ℠
J CELL PHYSIOL John Wiley & Sons Inc.
Citas Recibidas en Web of Science: 9
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Filiaciones
Cita
BENET M,Dulman RY,Suzme R,de Miera EV,Vega ME,Nguyen T,Zavadil J,PELLICER A. Wild type N-ras displays anti-malignant properties, in part by downregulating decorin. J CELL PHYSIOL. 2012. 227. (6):p. 2341-2351. IF:4,218. (1).
Portal de investigación