Blood Advances (Sep 2017)

Impact of genomic alterations on outcomes in myelofibrosis patients undergoing JAK1/2 inhibitor therapy

  • Jay Y. Spiegel,
  • Caroline McNamara,
  • James A. Kennedy,
  • Tony Panzarella,
  • Andrea Arruda,
  • Tracy Stockley,
  • Mahadeo Sukhai,
  • Mariam Thomas,
  • Justyna Bartoszko,
  • Jenny Ho,
  • Nancy Siddiq,
  • Dawn Maze,
  • Aaron Schimmer,
  • Andre Schuh,
  • Hassan Sibai,
  • Karen Yee,
  • Jamie Claudio,
  • Rebecca Devlin,
  • Mark D. Minden,
  • Suzanne Kamel-Reid,
  • Vikas Gupta

Journal volume & issue
Vol. 1, no. 20
pp. 1729 – 1738

Abstract

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Abstract: In myelofibrosis (MF), driver mutations in JAK2, MPL, or CALR impact survival and progression to blast phase, with the greatest risk conferred by triple-negative status. Subclonal mutations, including mutations in high–molecular risk (HMR) genes, such as ASXL1, EZH2, IDH1/2, and SRSF2 have also been associated with inferior prognosis. However, data evaluating the impact of next-generation sequencing in MF patients treated with JAK1/2 inhibitors are lacking. Using a 54-gene myeloid panel, we performed targeted sequencing on 100 MF patients treated with ruxolitinib (n = 77) or momelotinib (n = 23) and correlated mutational profiles with treatment outcomes. Ninety-nine patients had at least 1 mutation identified, 46 (46%) had 2 mutations, and 34 (34%) patients had ≥3 mutations. Seventy-nine patients carried a mutation in JAK2V617F, 14 patients had mutations in CALR, 6 patients had an MPL mutation, and 2 patients were triple negative. No mutation was significantly associated with spleen or anemia response. A high Dynamic International Prognostic Scoring System score and pretreatment transfusion dependence were associated with a shorter time to treatment failure (TTF), and this association retained significance on multivariable analysis. Patients with ASXL1 (hazard ratio [HR], 1.86; P = .03) and EZH2 mutations (HR, 2.94; P = .009) and an HMR profile (HR, 2.06; P = .01) had shorter TTF. On multivariate analysis, ASXL1 or EZH2 mutations were independently associated with shorter TTF and overall survival. These findings help identify patients unlikely to have a durable response with current JAK1/2 inhibitors and provide a framework for future studies.