Abstract
An emerging paradigm holds that loss of negative signalling to receptor tyrosine kinases (RTKs) is permissive for their oncogenic activity. Herein, we have addressed tumor suppression by RALT/MIG-6, a transcriptionally controlled feedback inhibitor of ErbB RTKs, in breast cancer cells. Knockdown of RALT expression by RNAi enhanced the EGF-dependent proliferation of normal breast epithelial cells, indicating that loss of RALT signalling in breast epithelium may represent an advantageous condition during ErbB-driven tumorigenesis. Although mutational inactivation of the RALT gene was not detected in human breast carcinomas, RALT mRNA and protein expression was strongly and selectively reduced in ERBB2-amplified breast cancer cell lines. Reconstitution of RALT expression in ERBB2-amplified SKBr-3 and BT474 cells inhibited ErbB-2-dependent mitogenic signalling and counteracted the ability of ErbB ligands to promote resistance to the ErbB-2-targeting drug Herceptin. Thus, loss of RALT expression cooperates with ERBB2 gene amplification to drive full oncogenic signalling by the ErbB-2 receptor. Moreover, loss of RALT signalling may adversely affect tumor responses to ErbB-2-targeting agents.
| Original language | English |
|---|---|
| Pages (from-to) | 4540-4548 |
| Number of pages | 9 |
| Journal | Oncogene |
| Volume | 24 |
| Issue number | 28 |
| DOIs | |
| Publication status | Published - 30 Jun 2005 |
Bibliographical note
Funding Information: We thank M Fanciulli, S Giordano, N Hynes and G Piaggio for reagents, R Carsetti for cell sorting, S Alemà, D Birnbaum, PG Natali and S Soddu for discussion, R Fraioli for assistance. This work was supported by AIRC and FIRB grants to OS; G. Russo is supported by AIRC.Other keywords
- Breast cancer
- ErbB-2
- Herceptin
- MIG-6
- RALT
- Targeted therapies