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Publication : E2F1 has both oncogenic and tumor-suppressive properties in a transgenic model.

First Author  Pierce AM Year  1999
Journal  Mol Cell Biol Volume  19
Issue  9 Pages  6408-14
PubMed ID  10454586 Mgi Jnum  J:77880
Mgi Id  MGI:2182850 Doi  10.1128/mcb.19.9.6408
Citation  Pierce AM, et al. (1999) E2F1 has both oncogenic and tumor-suppressive properties in a transgenic model. Mol Cell Biol 19(9):6408-14
abstractText  Using a transgenic mouse model expressing the E2F1 gene under the control of a keratin 5 (K5) promoter, we previously demonstrated that increased E2F1 activity can promote tumorigenesis by cooperating with either a v-Ha-ras transgene to induce benign skin papillomas or p53 deficiency to induce spontaneous skin carcinomas. We now report that as K5 E2F1 transgenic mice age, they are predisposed to develop spontaneous tumors in a variety of K5-expressing tissues, including the skin, vagina, forestomach, and odontogenic epithelium. On the other hand, K5 E2F1 transgenic mice are found to be resistant to skin tumor development following a two-stage carcinogenesis protocol. Additional experiments suggest that this tumor-suppressive effect of E2F1 occurs at the promotion stage and may involve the induction of apoptosis. These findings demonstrate that increased E2F1 activity can either promote or inhibit tumorigenesis, dependent upon the experimental context.
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