Ruxolitinib mediated paradoxical JAK2 hyperphosphorylation is due to the protection of activation loop tyrosines from phosphatases

Myelofibrosis (MF) in 50% of cases is driven by an activating JAK2 mutation, mostly V617F. Ruxolinitib is approved for the treatment of MF. Responses to ruxolitinib in MF are of limited duration. Unexpectedly, treatment of JAK2-V617F expressing cells with ruxolitinib causes paradoxical hyperphosphor...

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Published inLeukemia Vol. 39; no. 7; pp. 1678 - 1691
Main Authors Gorantla, Sivahari P., Oelschläger, Lorenz, Prince, Gerin, Osius, Jasmin, Kolluri, Suresh Babu, Maluje, Yamil, Fähnrich, Anke, Ernst, Nancy, Barbosa Gulde, Alanis, Ludwig, Ralf Joachim, Gemoll, Timo, Fliedner, Stephanie, Walter, Wencke, Haferlach, Torsten, Gebauer, Niklas, Busch, Hauke, Duyster, Justus, von Bubnoff, Nikolas
Format Journal Article
LanguageEnglish
Published England Nature Publishing Group 01.07.2025
Nature Publishing Group UK
Subjects
Cloning
Competition
Conformation
Cytokines
Humans
Janus kinase 2
Janus Kinase 2 - chemistry
Janus Kinase 2 - genetics
Janus Kinase 2 - metabolism
Kinases
Mutation
Myelofibrosis
Nitriles
Phosphatase
Phosphorylation
Phosphorylation - drug effects
Primary Myelofibrosis - drug therapy
Primary Myelofibrosis - genetics
Primary Myelofibrosis - metabolism
Primary Myelofibrosis - pathology
Protein Tyrosine Phosphatases - metabolism
Pyrazoles - pharmacology
Pyrimidines
Stat5 protein
Tyrosine - metabolism
Germany
Online AccessGet full text
ISSN0887-6924
1476-5551
1476-5551
DOI10.1038/s41375-025-02594-7

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Summary:Myelofibrosis (MF) in 50% of cases is driven by an activating JAK2 mutation, mostly V617F. Ruxolinitib is approved for the treatment of MF. Responses to ruxolitinib in MF are of limited duration. Unexpectedly, treatment of JAK2-V617F expressing cells with ruxolitinib causes paradoxical hyperphosphorylation of JAK2 at activation loop Tyr1007/Tyr1008. The significance of ruxolitinib-induced JAK2 hyperphosphorylation is not well understood. We found that a ruxolitinib-resistant JAK2 variant (V617F + L983F) and a kinase dead mutant (JAK2-V617F + K882R) did not show paradoxical hyperphosphorylation after ruxolitinib treatment indicating that it is an intrinsic mechanism. Antibodies against pTyr1007/1008 failed to immunoprecipitate native JAK2-V617F in the presence of ruxolitinib, although JAK2-V617F was hyperphosphorylated at these sites, suggesting that in the presence of ruxolitinib the JAK2 activation loop is buried within the kinase domain. This stabilization of the activation loop conformation resulted in the protection of pTyr1007/1008 sites from phosphatases. Mutation of Arg975 and Lys999 to Ala reduced the phosphorylation at both Tyr1007/Tyr1008 residues, and notably, ruxolitinib treatment did not lead to JAK2 hyperphosphorylation. Importantly, hyperphosphorylated JAK2 after ruxolitinib dissociation displayed excess rebound activation of STAT5 target gene PIM kinase. Our results suggest a novel mode of kinase regulation by modulating kinase activity through conformational changes induced by ruxolitinib. Subject categories: JAK2-V617F, Ruxolitinib, JAK2 hyperphosphorylation, Phosphatases action, PIM kinases
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ISSN:0887-6924
1476-5551
1476-5551
DOI:10.1038/s41375-025-02594-7