Agritrop
Accueil

Involvement of Notch1 in the development of mouse mammary tumors

Dievart Anne, Beaulieu Normand, Jolicoeur Paul. 1999. Involvement of Notch1 in the development of mouse mammary tumors. Oncogene : 5973-5981.

https://doi.org/10.1038/sj.onc.1202991

Article de revue ; Article de revue à facteur d'impact
[img] Version publiée - Anglais
Accès réservé aux personnels Cirad jusqu'au 31 Décembre 2999.
Utilisation soumise à autorisation de l'auteur ou du Cirad.
ID577261 .pdf
Télécharger (393kB) | Demander une copie

Résumé : The MMTV/neu transgenic (Tg) mice spontaneously develop mammary tumors stochastically after a long latent period, suggesting that the c-neu/erbB2 oncogene is not sufficient for tumor formation. To identify putative collaborator(s) of the c-neu/erbB2, we used the provirus insertional mutagenesis approach with mammary tumors arising in MMTV/neu Tg mice infected with the mouse mammary tumor virus (MMTV). The Notch1 gene was identified as a novel target for MMTV provirus insertional activation. In Notch1-rearranged tumors, the Notch1 gene was interrupted by the MMTV provirus insertion upstream of the exons coding for the TM domain. These insertions led to overexpression of novel 5' truncated vary with 7 kb RNA coding for 280 kDa mutant protein harboring only the Notch1 ectodomain, N(EC)mut. These may be involved in tumor formation. Another consequence of these insertions was the expression of truncated 3' Notch1 transcripts (3.5 - 4.5 kb) and proteins (86 - 110 kDa) deleted of most of the extracellular sequences (Notch1intra). We found that 3' truncated Notch1intra can transform HC11 mouse mammary epithelial cells in vitro. Deletion analysis revealed that the ankyrin-repeats and the domain 1 (aa 1751 - 1821) are required, while a signal peptide, the two conserved cysteines (C1652 and C1685) and the OPA and PEST sequences are dispensable for transformation. These results indicate that the N-terminally truncated Notch1intra protein behaves as an oncogene in this system.

Classification Agris : L53 - Physiologie animale - Reproduction
L73 - Maladies des animaux
S50 - Santé humaine

Auteurs et affiliations

  • Dievart Anne, Clinical Research Institute of Montréal (CAN) ORCID: 0000-0001-9460-4638
  • Beaulieu Normand, Clinical Research Institute of Montréal (CAN)
  • Jolicoeur Paul, Université de Montréal (CAN)

Source : Cirad-Agritrop (https://agritrop.cirad.fr/577261/)

Voir la notice (accès réservé à Agritrop) Voir la notice (accès réservé à Agritrop)

[ Page générée et mise en cache le 2024-08-16 ]

EnglishLangue par défaut du navigateur

Copyright CIRAD - A propos du Cirad - Mentions légales - Contact