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- Title
Antitumour effects of PLC-?1-(SH2)<sub>2</sub>-TAT fusion proteins on EGFR/c-erbB-2-positive breast cancer cells.
- Authors
Katterle, Y.; Brandt, B.H.; Dowdy, S.F.; Niggemann, B.; Zänker, K.S.; Dittmar, T.
- Abstract
Due to its pivotal role in the growth factor-mediated tumour cell migration, the adaptor protein phospholipase C-?1 (PLC-?1) is an appropriate target to block ultimately the spreading of EGFR/c-erbB-2-positive tumour cells, thereby minimising metastasis formation. Here, we present an approach to block PLC-?1 activity by using protein-based PLC-?1 inhibitors consisting of PLC-?1 SH2 domains, which were fused to the TAT-transduction domain to ensure a high protein transduction efficiency. Two proteins were generated containing one PLC-?1-SH2-domain (PS1-TAT) or two PLC-?1-SH2 domains (PS2-TAT). PS2-TAT treatment of the EGFR/c-erbB-2-positive cell line MDA-HER2 resulted in a reduction of the EGF-mediated PLC-?1 tyrosine phosphorylation of about 30%, concomitant with a complete abrogation of the EGF-driven calcium influx. In addition to this, long-term PS2-TAT treatment both reduces the EGF-mediated migration of about 75% combined with a markedly decreased time locomotion of single MDA-HER2 cells as well as decreases the proliferation of MDA-HER2 cells by about 50%. Due to its antitumoral capacity on EGFR/c-erbB-2-positive breast cancer cells, we conclude from our results that the protein-based PLC-?1 inhibitor PS2-TAT may be a means for novel adjuvant antitumour strategies to minimise metastasis formation because of the blockade of cell migration and proliferation.British Journal of Cancer (2004) 90, 230-235. doi:10.1038/sj.bjc.6601506 www.bjcancer.com
- Subjects
PHOSPHOLIPASE C; EPIDERMAL growth factor; BREAST cancer; ANTINEOPLASTIC agents; CANCER cells; CANCER chemotherapy
- Publication
British Journal of Cancer, 2004, Vol 90, Issue 1, p230
- ISSN
0007-0920
- Publication type
Article
- DOI
10.1038/sj.bjc.6601506