Blood Advances (Nov 2017)

Constitutive Ras signaling and Ink4a/Arf inactivation cooperate during the development of B-ALL in mice

  • Tomasz Sewastianik,
  • Meng Jiang,
  • Kumar Sukhdeo,
  • Sanjay S. Patel,
  • Kathryn Roberts,
  • Yue Kang,
  • Ahmad Alduaij,
  • Peter S. Dennis,
  • Brian Lawney,
  • Ruiyang Liu,
  • Zeyuan Song,
  • Jessie Xiong,
  • Yunyu Zhang,
  • Madeleine E. Lemieux,
  • Geraldine S. Pinkus,
  • Jeremy N. Rich,
  • David M. Weinstock,
  • Charles G. Mullighan,
  • Norman E. Sharpless,
  • Ruben D. Carrasco

Journal volume & issue
Vol. 1, no. 25
pp. 2361 – 2374

Abstract

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Abstract: Despite recent advances in treatment, human precursor B-cell acute lymphoblastic leukemia (B-ALL) remains a challenging clinical entity. Recent genome-wide studies have uncovered frequent genetic alterations involving RAS pathway mutations and loss of the INK4A/ARF locus, suggesting their important role in the pathogenesis, relapse, and chemotherapy resistance of B-ALL. To better understand the oncogenic mechanisms by which these alterations might promote B-ALL and to develop an in vivo preclinical model of relapsed B-ALL, we engineered mouse strains with induced somatic KrasG12D pathway activation and/or loss of Ink4a/Arf during early stages of B-cell development. Although constitutive activation of KrasG12D in B cells induced prominent transcriptional changes that resulted in enhanced proliferation, it was not sufficient by itself to induce development of a high-grade leukemia/lymphoma. Instead, in 40% of mice, these engineered mutations promoted development of a clonal low-grade lymphoproliferative disorder resembling human extranodal marginal-zone lymphoma of mucosa-associated lymphoid tissue or lymphoplasmacytic lymphoma. Interestingly, loss of the Ink4a/Arf locus, apart from reducing the number of apoptotic B cells broadly attenuated KrasG12D-induced transcriptional signatures. However, combined Kras activation and Ink4a/Arf inactivation cooperated functionally to induce a fully penetrant, highly aggressive B-ALL phenotype resembling high-risk subtypes of human B-ALL such as BCR-ABL and CRFL2-rearranged. Ninety percent of examined murine B-ALL tumors showed loss of the wild-type Ink4a/Arf locus without acquisition of highly recurrent cooperating events, underscoring the role of Ink4a/Arf in restraining Kras-driven oncogenesis in the lymphoid compartment. These data highlight the importance of functional cooperation between mutated Kras and Ink4a/Arf loss on B-ALL.