Literature DB >> 12930840

The erythropoietin receptor transmembrane domain mediates complex formation with viral anemic and polycythemic gp55 proteins.

Stefan N Constantinescu1, Tzvia Keren, William P Russ, Iban Ubarretxena-Belandia, Yaniv Malka, Katharina F Kubatzky, Donald M Engelman, Harvey F Lodish, Yoav I Henis.   

Abstract

Erythropoietin receptor (EpoR) activation is crucial for mature red blood cell production. The murine EpoR can also be activated by the envelope protein of the polycythemic (P) spleen focus forming virus (SFFV), gp55-P. Due to differences in the TM sequence, gp55 of the anemic (A) strain SFFV, gp55-A, cannot efficiently activate the EpoR. Using antibody-mediated immunofluorescence co-patching, we show that the majority of EpoR forms hetero-oligomers at the cell surface with gp55-P and, surprisingly, with gp55-A. The EpoR TM domain is targeted by gp55-P and -A, as only chimeric receptors containing EpoR TM sequences oligomerized with gp55 proteins. Both gp55-P and gp55-A are homodimers on the cell surface, as shown by co-patching. However, when the homomeric interactions of the isolated TM domains were assayed by TOXCAT bacterial reporter system, only the TM sequence of gp55-P was dimerized. Thus, homo-oligomerization of gp55 proteins is insufficient for full EpoR activation, and a correct conformation of the dimer in the TM region is required. This is supported by the failure of gp55-A-->P, a mutant protein whose TM domain can homo-oligomerize, to fully activate EpoR. As unliganded EpoR forms TM-dependent but inactive homodimers, we propose that the EpoR can be activated to different extents by homodimeric gp55 proteins, depending on the conformation of the gp55 protein dimer in the TM region.

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Year:  2003        PMID: 12930840     DOI: 10.1074/jbc.M302974200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  12 in total

1.  Characterization of erythropoietin and hepcidin in the regulation of persistent injury-associated anemia.

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2.  Helix packing and orientation in the transmembrane dimer of gp55-P of the spleen focus forming virus.

Authors:  Wei Liu; Evan Crocker; Stefan N Constantinescu; Steven O Smith
Journal:  Biophys J       Date:  2005-05-13       Impact factor: 4.033

3.  Molecular determinants and thermodynamics of the amyloid precursor protein transmembrane domain implicated in Alzheimer's disease.

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4.  Topological control of cytokine receptor signaling induces differential effects in hematopoiesis.

Authors:  Kritika Mohan; George Ueda; Ah Ram Kim; Kevin M Jude; Jorge A Fallas; Yu Guo; Maximillian Hafer; Yi Miao; Robert A Saxton; Jacob Piehler; Vijay G Sankaran; David Baker; K Christopher Garcia
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5.  Friend spleen focus-forming virus transforms rodent fibroblasts in cooperation with a short form of the receptor tyrosine kinase Stk.

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6.  Activation of the N-terminally truncated form of the Stk receptor tyrosine kinase Sf-Stk by Friend virus-encoded gp55 is mediated by cysteine residues in the ecotropic domain of gp55 and the extracellular domain of Sf-Stk.

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8.  Ligand-independent homomeric and heteromeric complexes between interleukin-2 or -9 receptor subunits and the gamma chain.

Authors:  Yaniv Malka; Tekla Hornakova; Yohan Royer; Laurent Knoops; Jean-Christophe Renauld; Stefan N Constantinescu; Yoav I Henis
Journal:  J Biol Chem       Date:  2008-10-01       Impact factor: 5.157

9.  Screening for transmembrane association in divisome proteins using TOXGREEN, a high-throughput variant of the TOXCAT assay.

Authors:  Claire R Armstrong; Alessandro Senes
Journal:  Biochim Biophys Acta       Date:  2016-07-22

10.  Stat3 promotes the development of erythroleukemia by inducing Pu.1 expression and inhibiting erythroid differentiation.

Authors:  S Hegde; S Ni; S He; D Yoon; G S Feng; S S Watowich; R F Paulson; P A Hankey
Journal:  Oncogene       Date:  2009-07-06       Impact factor: 9.867

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