PLoS ONE (Jan 2017)

SOCS1 function in BCR-ABL mediated myeloproliferative disease is dependent on the cytokine environment.

  • Özlem Demirel,
  • Olivier Balló,
  • Pavankumar N G Reddy,
  • Olesya Vakhrusheva,
  • Jing Zhang,
  • Astrid Eichler,
  • Ramona Fernandes,
  • Susanne Badura,
  • Hubert Serve,
  • Christian Brandts

DOI
https://doi.org/10.1371/journal.pone.0180401
Journal volume & issue
Vol. 12, no. 7
p. e0180401

Abstract

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Treatment with tyrosine kinase inhibitors is the standard of care for Philadelphia chromosome positive leukemias. However the eradication of leukemia initiating cells remains a challenge. Circumstantial evidence suggests that the cytokine microenvironment may play a role in BCR-ABL mediated leukemogenesis and in imatinib resistance. Gene expression analyses of BCR-ABL positive ALL long-term cultured cells revealed strong reduction of SOCS mRNA expression after imatinib treatment, thereby demonstrating a strong inhibition of cytokine signaling. In this study we employed SOCS1-a strong inhibitor of cytokine signaling-as a tool to terminate external cytokine signals in BCR-ABL transformed cells in vitro and in vivo. In colony formation assays with primary bone marrow cells, expression of SOCS1 decreased colony numbers under pro-proliferative cytokines, while it conferred growth resistance to anti-proliferative cytokines. Importantly, co-expression of SOCS1 with BCR-ABL led to the development of a MPD phenotype with a prolonged disease latency compared to BCR-ABL alone in a murine bone marrow transplantation model. Interestingly, SOCS1 co-expression protected 20% of mice from MPD development. In summary, we conclude that under pro-proliferative cytokine stimulation at the onset of myeloproliferative diseases SOCS1 acts as a tumor suppressor, while under anti-proliferative conditions it exerts oncogenic function. Therefore SOCS1 can promote opposing functions depending on the cytokine environment.