Engineering of Specific Tissue Inhibitors to Block ADAM Type Metalloprotease-Mediated Mammary Neoplasia
Abstract
Communication between different signaling pathways enables cells to coordinate the responses to diverse environmental signals. Activation of the transmembrane growth factor precursor plays a critical role in this communication and often involves in metalloproteases-mediated proteolysis. Stimulation of G protein-coupled receptors (GPCR) transactivates the epidermal growth factor receptors (EGFR), which occurs via a metalloprotease-dependent cleavage of heparin-binding epidermal growth factor (HB-ECF). However, the metalloprotease mediating the transactivation remains elusive. We show that the integral membrane metalloprotease Kuzbanian (KUZ, ADAM10), which controls Notch signaling by cleaving Notch and its ligand Delta in Drosophila, stimulates GPCR transactivation of EGFR. Upon stimulation of the bombesin receptors, KUZ increases the docking and activation of adaptors SHC and Gabl on the EGFR, and activation of Ras and Erk. In contrast, transfection of a protease-domain deleted KUZ (K.MP) or blocking endogenous KUZ by morpholino antisense oligonucleotides suppresses the transactivation. The effect of KUZ on shedding of HB-EGF and consequent transactivation of the EGFR depends on its metalloprotease activity. GPCR activation enhances the association of KUZ and its substrate HB-EGF with tetraspanin CD9. Thus KUZ regulates the relay between GPCR and EGFR signaling pathways.
Document Details
- Document Type
- Technical Report
- Publication Date
- Jul 01, 2001
- Accession Number
- ADB281601
Entities
People
- Yibing Yan
- Zena Werb
Organizations
- University of California, San Francisco