Homeobox NKX2-3 promotes marginal-zone lymphomagenesis by activating B-cell receptor signalling and shaping lymphocyte dynamics

نویسندگان

  • Eloy F. Robles
  • Maria Mena-Varas
  • Laura Barrio
  • Sara V. Merino-Cortes
  • Péter Balogh
  • Ming-Qing Du
  • Takashi Akasaka
  • Anton Parker
  • Sergio Roa
  • Carlos Panizo
  • Idoia Martin-Guerrero
  • Reiner Siebert
  • Victor Segura
  • Xabier Agirre
  • Laura Macri-Pellizeri
  • Beatriz Aldaz
  • Amaia Vilas-Zornoza
  • Shaowei Zhang
  • Sarah Moody
  • Maria Jose Calasanz
  • Thomas Tousseyn
  • Cyril Broccardo
  • Pierre Brousset
  • Elena Campos-Sanchez
  • Cesar Cobaleda
  • Isidro Sanchez-Garcia
  • Jose Luis Fernandez-Luna
  • Ricardo Garcia-Muñoz
  • Esther Pena
  • Beatriz Bellosillo
  • Antonio Salar
  • Maria Joao Baptista
  • Jesús Maria Hernandez-Rivas
  • Marcos Gonzalez
  • Maria Jose Terol
  • Joan Climent
  • Antonio Ferrandez
  • Xavier Sagaert
  • Ari M. Melnick
  • Felipe Prosper
  • David G. Oscier
  • Yolanda R. Carrasco
  • Martin J. S. Dyer
  • Jose A. Martinez-Climent
چکیده

NKX2 homeobox family proteins have a role in cancer development. Here we show that NKX2-3 is overexpressed in tumour cells from a subset of patients with marginal-zone lymphomas, but not with other B-cell malignancies. While Nkx2-3-deficient mice exhibit the absence of marginal-zone B cells, transgenic mice with expression of NKX2-3 in B cells show marginal-zone expansion that leads to the development of tumours, faithfully recapitulating the principal clinical and biological features of human marginal-zone lymphomas. NKX2-3 induces B-cell receptor signalling by phosphorylating Lyn/Syk kinases, which in turn activate multiple integrins (LFA-1, VLA-4), adhesion molecules (ICAM-1, MadCAM-1) and the chemokine receptor CXCR4. These molecules enhance migration, polarization and homing of B cells to splenic and extranodal tissues, eventually driving malignant transformation through triggering NF-κB and PI3K-AKT pathways. This study implicates oncogenic NKX2-3 in lymphomagenesis, and provides a valid experimental mouse model for studying the biology and therapy of human marginal-zone B-cell lymphomas.

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عنوان ژورنال:

دوره 7  شماره 

صفحات  -

تاریخ انتشار 2016