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Literature DB >> 27998978

Three Tyrosine Residues in the Erythropoietin Receptor Are Essential for Janus Kinase 2 V617F Mutant-induced Tumorigenesis.

Fumihito Ueda¹, Kenji Tago², Hiroomi Tamura¹, Megumi Funakoshi-Tago³.

Abstract

The erythropoietin receptor (EpoR) regulates development of blood cells, and its full activation normally requires the cytokine erythropoietin (Epo). In the case of myeloproliferative neoplasms (MPN), Epo-independent signaling through EpoR can be caused by a point mutation, V617F, in the EpoR-interacting tyrosine kinase Janus kinase 2 (JAK2). In cells expressing the JAK2 V617F mutant, eight tyrosine residues in the intracellular domain of EpoR are phosphorylated, but the functional role of these phosphorylations in oncogenic signaling is incompletely understood. Here, to evaluate the functional consequences of the phosphorylation of these tyrosine residues, we constructed an EpoR-8YF mutant in which we substituted all eight tyrosine residues with phenylalanine. Co-expression of EpoR-8YF with the JAK2 V617F mutant failed to induce cytokine-independent cell proliferation and tumorigenesis, indicating that JAK2-mediated EpoR phosphorylation is the reason for JAK2 V617F mutant-induced oncogenic signaling. An exhaustive mutational analysis of the eight EpoR tyrosine residues indicated that three of these residues, Tyr-343, Tyr-460, and Tyr-464, are required for the JAK2 V617F mutant to exhibit its oncogenic activity. We also showed that phosphorylation at these three residues was necessary for full activation of the transcription factor STAT5, which is a critical downstream factor of JAK2 V617F-induced oncogenic signaling. In contrast, Epo stimulation could moderately stimulate the proliferation of cells expressing wild type JAK2 and EpoR-8YF, suggesting that the requirement of the phosphorylation of these three tyrosine residues seems to be specific for the oncogenic proliferation provoked by V617F mutation. Collectively, these results have revealed that phosphorylation of Tyr-343, Tyr-460, and Tyr-464 in EpoR underlies JAK2 V617F mutant-induced tumorigenesis. We propose that the targeted disruption of this pathway has therapeutic utility for managing MPN.

Entities: Chemical Disease Gene

Keywords: Janus kinase (JAK); Janus kinase 2 (JAK2); STAT transcription factor; V617F mutant; erythropoietin; erythropoietin receptor (EpoR); mutant; myeloproliferative neoplasms (MPN); signal transducer and activator of transcription 5 (STAT5); tumor

Mesh：

Substances：

Year: 2016 PMID： 27998978 PMCID： PMC5290956 DOI： 10.1074/jbc.M116.749465

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

47 in total

1. Stat5a serine 725 and 779 phosphorylation is a prerequisite for hematopoietic transformation.

Authors: Katrin Friedbichler; Marc A Kerenyi; Boris Kovacic; Geqiang Li; Andrea Hoelbl; Saliha Yahiaoui; Veronika Sexl; Ernst W Müllner; Sabine Fajmann; Sabine Cerny-Reiterer; Peter Valent; Hartmut Beug; Fabrice Gouilleux; Kevin D Bunting; Richard Moriggl
Journal: Blood Date: 2010-05-27 Impact factor: 22.113

2. Expression of a homodimeric type I cytokine receptor is required for JAK2V617F-mediated transformation.

Authors: Xiaohui Lu; Ross Levine; Wei Tong; Gerlinde Wernig; Yana Pikman; Sara Zarnegar; D Gary Gilliland; Harvey Lodish
Journal: Proc Natl Acad Sci U S A Date: 2005-12-19 Impact factor: 11.205

3. Activating mutation in the tyrosine kinase JAK2 in polycythemia vera, essential thrombocythemia, and myeloid metaplasia with myelofibrosis.

Authors: Ross L Levine; Martha Wadleigh; Jan Cools; Benjamin L Ebert; Gerlinde Wernig; Brian J P Huntly; Titus J Boggon; Iwona Wlodarska; Jennifer J Clark; Sandra Moore; Jennifer Adelsperger; Sumin Koo; Jeffrey C Lee; Stacey Gabriel; Thomas Mercher; Alan D'Andrea; Stefan Fröhling; Konstanze Döhner; Peter Marynen; Peter Vandenberghe; Ruben A Mesa; Ayalew Tefferi; James D Griffin; Michael J Eck; William R Sellers; Matthew Meyerson; Todd R Golub; Stephanie J Lee; D Gary Gilliland
Journal: Cancer Cell Date: 2005-04 Impact factor: 31.743

4. STAT5 activation is critical for the transformation mediated by myeloproliferative disorder-associated JAK2 V617F mutant.

Authors: Megumi Funakoshi-Tago; Kenji Tago; Miyuki Abe; Yoshiko Sonoda; Tadashi Kasahara
Journal: J Biol Chem Date: 2009-12-22 Impact factor: 5.157

5. Prediction of the structure of human Janus kinase 2 (JAK2) comprising JAK homology domains 1 through 7.

Authors: Fabrizio Giordanetto; Romano T Kroemer
Journal: Protein Eng Date: 2002-09

6. Critical Role of STAT5 transcription factor tetramerization for cytokine responses and normal immune function.

Authors: Jian-Xin Lin; Peng Li; Delong Liu; Hyun Tak Jin; Jianping He; Mohammed Ata Ur Rasheed; Yrina Rochman; Lu Wang; Kairong Cui; Chengyu Liu; Brian L Kelsall; Rafi Ahmed; Warren J Leonard
Journal: Immunity Date: 2012-04-20 Impact factor: 31.745

7. Interaction of STAT5 dimers on two low affinity binding sites mediates interleukin 2 (IL-2) stimulation of IL-2 receptor alpha gene transcription.

Authors: W K Meyer; P Reichenbach; U Schindler; E Soldaini; M Nabholz
Journal: J Biol Chem Date: 1997-12-12 Impact factor: 5.157

8. The cytokine-inducible Scr homology domain-containing protein negatively regulates signaling by promoting apoptosis in erythroid progenitor cells.

Authors: Robin Ketteler; Chetal S Moghraby; Jonathan G Hsiao; Olivier Sandra; Harvey F Lodish; Ursula Klingmüller
Journal: J Biol Chem Date: 2002-11-18 Impact factor: 5.157

9. JAK2 associates with the erythropoietin receptor and is tyrosine phosphorylated and activated following stimulation with erythropoietin.

Authors: B A Witthuhn; F W Quelle; O Silvennoinen; T Yi; B Tang; O Miura; J N Ihle
Journal: Cell Date: 1993-07-30 Impact factor: 41.582