ErbB Tyrosine Kinases and the Two Neuregulin Families Constitute a Ligand-Receptor Network

Author:

Pinkas-Kramarski Ronit1,Shelly Maya1,Guarino Bradley C.2,Wang Ling Mei3,Lyass Ljuba4,Alroy Iris1,Alamandi Mauricio3,Kuo Angera3,Moyer James D.2,Lavi Sara1,Eisenstein Miriam5,Ratzkin Barry J.6,Seger Rony7,Bacus Sarah S.4,Pierce Jacalyn H.3,Andrews Glenn C.2,Yarden Yosef1

Affiliation:

1. Departments of Molecular Cell Biology,1

2. Pfizer Central Research, Groton, Connecticut 063402;

3. The National Cancer Institute, Bethesda, Maryland 208923;

4. Advanced Cellular Diagnostics, Inc., Elmhurst Illinois 601264; and

5. Structural Biology,5 and

6. Amgen Center, Thousand Oaks, California 913206

7. Membrane Research and Recognition,7 The Weizmann Institute of Science, Rehovot 76100, Israel;

Abstract

ABSTRACT The recently isolated second family of neuregulins, NRG2, shares its primary receptors, ErbB-3 and ErbB-4, and induction of mammary cell differentiation with NRG1 isoforms, suggesting functional redundancy of the two growth factor families. To address this possibility, we analyzed receptor specificity of NRGs by using an engineered cellular system. The activity of isoform-specific but partly overlapping patterns of specificities that collectively activate all eight ligand-stimulatable ErbB dimers was revealed. Specifically, NRG2-β, like NRG1-α, emerges as a narrow-specificity ligand, whereas NRG2-α is a pan-ErbB ligand that binds with different affinities to all receptor combinations, including those containing ErbB-1, but excluding homodimers of ErbB-2. The latter protein, however, displayed cooperativity with the direct NRG receptors. Apparently, signaling by all NRGs is funneled through the mitogen-activated protein kinase (MAPK). However, the duration and potency of MAPK activation depend on the identity of the stimulatory ligand-receptor ternary complex. We conclude that the NRG-ErbB network represents a complex and nonredundant machinery developed for fine-tuning of signal transduction.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

Reference68 articles.

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5. A single autophosphorylation site confers oncogenicity to the Neu/ErbB-2 receptor and enables coupling to the MAP-kinase pathway;Ben-Levy R.;EMBO J.,1994

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