Structure and Machanism-Base Design of ErbB Receptor Inhibitors

Abstract

The work proposed for this award involved using the crystal structures of the extracellular domains of the EGF receptor (EGFR) and its homologs HER2/Neu/ErbB2, HER3/ErbB3, and HER4/ErbB4, which were recently determined in my lab and elsewhere, to design a new class of inhibitors of this family of receptors. These structures had shown that ligands bind to two separate surfaces in these receptors that are normally far apart in the absence of ligand. Binding ligand (e.g. EGF) requires a large conformational change in the receptor to bring these surfaces close together, and it is this conformational change that then leads to receptor dimerization and initiation of a signaling cascade through activation of a cytoplasmic tyrosine kinase. Our idea had been to create through mutagenesis a ligand that bound more tightly to one of the binding surfaces but not to the other. Theoretically, this ligand would bind to the receptor but not induce the conformational change needed to activate the receptor and thus serve an inhibitor of the receptor.

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Document Details

Document Type
Technical Report
Publication Date
Sep 01, 2005
Accession Number
ADA443243

Entities

People

  • Daniel J. Leahy

Organizations

  • Johns Hopkins University

Tags

DTIC Thesaurus Topics

  • Abstracts
  • Amino Acids
  • Biomedical Research
  • Breast Cancer
  • Cancer
  • Cell Line
  • Cells
  • Chemistry
  • Colon Cancer
  • Crystal Structure
  • Crystallization
  • Crystals
  • Growth Factors
  • Inhibitors
  • Neoplasms
  • Proteins
  • Small Molecules

Readers

  • Breast cancer cell signaling and growth regulation.