Oncogenic JAK2V617F causes PD-L1 expression, mediating immune escape in myeloproliferative neoplasms

被引:183
作者
Prestipino, Alessandro [1 ,2 ]
Emhardt, Alica J. [1 ]
Aumann, Konrad [3 ]
O'Sullivan, David [4 ]
Gorantla, Sivahari P. [1 ]
Duquesne, Sandra [1 ]
Melchinger, Wolfgang [1 ]
Braun, Lukas [1 ]
Vuckovic, Slavica [5 ,6 ]
Boerries, Melanie [7 ,8 ,9 ]
Busch, Hauke [7 ,10 ]
Halbach, Sebastian [7 ]
Pennisi, Sandra [1 ,2 ]
Poggio, Teresa [1 ,2 ]
Apostolova, Petya [1 ,11 ]
Veratti, Pia [1 ,8 ,9 ]
Hettich, Michael [12 ]
Niedermann, Gabriele [12 ]
Bartholomae, Mark [13 ]
Shoumariyeh, Khalid [1 ]
Jutzi, Jonas S. [1 ,14 ]
Wehrle, Julius [1 ,8 ,9 ,11 ]
Dierks, Christine [1 ]
Becker, Heiko [1 ]
Schmitt-Graeff, Annette [3 ]
Follo, Marie [1 ]
Pfeifer, Dietmar [1 ]
Rohr, Jan [15 ]
Fuchs, Sebastian [15 ]
Ehl, Stephan [15 ]
Hartl, Frederike A. [2 ,16 ]
Minguet, Susana [2 ,15 ,16 ]
Miething, Cornelius [1 ,8 ,9 ]
Heidel, Florian H. [17 ,18 ]
Kroeger, Nicolaus [19 ]
Triviai, Ioanna [19 ]
Brummer, Tilman [7 ,8 ,9 ,16 ]
Finke, Jurgen [1 ]
Illert, Anna L. [1 ]
Ruggiero, Eliana [20 ,21 ]
Bonini, Chiara [20 ,21 ]
Duyster, Justus [1 ,8 ,9 ]
Pahl, Heike L. [1 ]
Lane, Steven W. [5 ,22 ,23 ]
Hill, Geoffrey R. [5 ,22 ,23 ]
Blazar, Bruce R. [24 ]
von Bubnoff, Nikolas [1 ,8 ,9 ]
Pearce, Erika L. [4 ]
Zeiser, Robert [1 ,8 ,9 ,16 ]
机构
[1] Univ Freiburg, Fac Med, Med Ctr, Dept Hematol & Oncol, D-79106 Freiburg, Germany
[2] Albert Ludwigs Univ Freiburg, Fac Biol, D-79104 Freiburg, Germany
[3] Univ Freiburg, Fac Med, Inst Surg Pathol, D-79106 Freiburg, Germany
[4] Max Planck Inst Immunobiol & Epigenet, D-79108 Freiburg, Germany
[5] QIMR Berghofer Med Res Inst, Dept Immunol, Brisbane, Qld 4006, Australia
[6] Univ Queensland, Sch Med, Herston, Qld 4006, Australia
[7] Univ Freiburg, Fac Med, Inst Mol Med & Cell Res, D-79085 Freiburg, Germany
[8] German Canc Consortium DKTK, Partner Site Freiburg, Freiburg, Germany
[9] German Canc Res Ctr, D-69120 Heidelberg, Germany
[10] Univ Lubeck, Inst Cardiogenet, Inst Expt Dermatol, D-23562 Lubeck, Germany
[11] Univ Freiburg, Berta Ottenstein Programme, Fac Med, D-79106 Freiburg, Germany
[12] Univ Freiburg, Dept Radiat Oncol, Fac Med, D-79106 Freiburg, Germany
[13] Univ Freiburg, Dept Nucl Med, Fac Med, D-79106 Freiburg, Germany
[14] Univ Freiburg, Spemann Grad Sch Biol & Med, D-79085 Freiburg, Germany
[15] Univ Freiburg, Med Ctr, Ctr Chron Immunodeficiency, D-79106 Freiburg, Germany
[16] Univ Freiburg, BIOSS Ctr Biol Signalling Studies, D-79104 Freiburg, Germany
[17] Univ Hosp Jena, Dept Hematol & Oncol, Internal Med 2, D-07745 Jena, Germany
[18] Leibniz Inst Aging, Fritz Lipmann Inst, D-07745 Jena, Germany
[19] Univ Med Ctr Hamburg Eppendorf, Dept Stem Cell Transplant, D-20246 Hamburg, Germany
[20] Ist Sci San Raffaele, Unit Expt Hematol, I-20132 Milan, Italy
[21] Univ Vita Salute San Raffaele, I-20132 Milan, Italy
[22] Royal Brisbane & Womens Hosp, Brisbane, Qld, Australia
[23] Univ Queensland, Herston, Qld 4072, Australia
[24] Univ Minnesota, Dept Pediat, Div Blood & Marrow Transplantat, Minneapolis, MN 55455 USA
来源
SCIENCE TRANSLATIONAL MEDICINE | 2018年 / 10卷 / 429期
基金
欧洲研究理事会;
关键词
ACUTE MYELOID-LEUKEMIA; HODGKIN LYMPHOMA; CELLS; ACTIVATION; B7-H1; IDENTIFICATION; MYELOFIBROSIS; METABOLISM; PROGENITOR; MUTATIONS;
D O I
10.1126/scitranslmed.aam7729
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Recent evidence has revealed that oncogenic mutations may confer immune escape. A better understanding of how an oncogenic mutation affects immunosuppressive programmed death ligand 1 (PD-L1) expression may help in developing new therapeutic strategies. We show that oncogenic JAK2 (Janus kinase 2) activity caused STAT3 (signal transducer and activator of transcription 3) and STAT5 phosphorylation, which enhanced PD-L1 promoter activity and PD-L1 protein expression in JAK2(V617F)-mutant cells, whereas blockade of JAK2 reduced PD-L1 expression in myeloid JAK2(V617F)-mutant cells. PD-L1 expression was higher on primary cells isolated from patients with JAK2(V617F)-myeloproliferative neoplasms (MPNs) compared to healthy individuals and declined upon JAK2 inhibition. JAK2(V617F) mutational burden, pSTAT3, and PD-L1 expression were highest in primary MPN patient-derived monocytes, megakaryocytes, and platelets. PD-1 (programmed death receptor 1) inhibition prolonged survival in human MPN xenograft and primary murine MPN models. This effect was dependent on T cells. Mechanistically, PD-L1 surface expression in JAK2(V617F)-mutant cells affected metabolism and cell cycle progression of T cells. In summary, we report that in MPN, constitutive JAK2/STAT3/STAT5 activation, mainly in monocytes, megakaryocytes, and platelets, caused PD-L1-mediated immune escape by reducing T cell activation, metabolic activity, and cell cycle progression. The susceptibility of JAK2(V617F)-mutant MPN to PD-1 targeting paves the way for immunomodulatory approaches relying on PD-1 inhibition.
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页数:12
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