Identification of the Her-2 Functional Site: Blockage of Receptor Heterodimerization

Abstract

Targeting HER2 is not as straightforward as it was originally predicted since many breast tumors express multiple HER receptors and co-express one or more HER ligands. This cross-talk network negatively impacts the response to the currently used HER2-targeted agents, highlighting the urgent need for a novel anti-HER2 molecule(s) presenting a combination strategy. Activation of the HER2 receptor is attained by several means: 1) receptor overexpression leads to homodimerization; 2) EGF induces EGFR-HER2 hetero-dimerization by binding to EGFR and inducing HER2 activation via crosstalk; and 3) Heregulin (HRG) induces HER3-HER2 hetero-dimerization by activating HER2 via its binding to the HER3 and HER4 receptors, in turn inducing receptor crosstalk and activation of a signaling cascade. In short, our preliminary study reveals that the specific disruption of an essential activating sequence existing on HER2 ECD domain III is capable of disabling the HER2 homo- and hetero-dimerization, thus blocking activation of HER2-driven oncogenic signaling and generating a dominant-negative Peptides or compounds with specificity for this functional site should add a previously unrecognized molecular approach to our therapeutic arsenal for the management of HER2-overexpressing carcinomas.

Document Details

Document Type

Technical Report

Publication Date

Sep 01, 2007

Accession Number

ADA478663

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