| Literature DB >> 25728669 |
Ignacio Moraga1, Gerlinde Wernig2, Stephan Wilmes3, Vitalina Gryshkova4, Christian P Richter3, Wan-Jen Hong5, Rahul Sinha6, Feng Guo1, Hyna Fabionar7, Tom S Wehrman8, Peter Krutzik8, Samuel Demharter9, Isabelle Plo10, Irving L Weissman6, Peter Minary9, Ravindra Majeti5, Stefan N Constantinescu4, Jacob Piehler3, K Christopher Garcia11.
Abstract
Most cell-surface receptors for cytokines and growth factors signal as dimers, but it is unclear whether remodeling receptor dimer topology is a viable strategy to "tune" signaling output. We utilized diabodies (DA) as surrogate ligands in a prototypical dimeric receptor-ligand system, the cytokine Erythropoietin (EPO) and its receptor (EpoR), to dimerize EpoR ectodomains in non-native architectures. Diabody-induced signaling amplitudes varied from full to minimal agonism, and structures of these DA/EpoR complexes differed in EpoR dimer orientation and proximity. Diabodies also elicited biased or differential activation of signaling pathways and gene expression profiles compared to EPO. Non-signaling diabodies inhibited proliferation of erythroid precursors from patients with a myeloproliferative neoplasm due to a constitutively active JAK2V617F mutation. Thus, intracellular oncogenic mutations causing ligand-independent receptor activation can be counteracted by extracellular ligands that re-orient receptors into inactive dimer topologies. This approach has broad applications for tuning signaling output for many dimeric receptor systems.Entities:
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Year: 2015 PMID: 25728669 PMCID: PMC4766813 DOI: 10.1016/j.cell.2015.02.011
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582