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. Author manuscript; available in PMC: 2017 Nov 1.
Published in final edited form as: Br J Haematol. 2016 Jul 19;175(3):496–504. doi: 10.1111/bjh.14260

Table I.

Patient Characteristics, including the entire cohort, as well as the subset of controls (n=43) included in the day +68 landmark analysis.

Sorafenib Patients (n=26) All Control Patients (n=55) P-value vs. Sorafenib Day +68 Landmark Controls (n=43) P-value vs. Sorafenib

Age, years; median (range) 55 (20–74) 56 (25–73) 0.75 56 (25–73) 0.78

Sex, male 12 (46%) 19 (35%) 0.34 13 (30%) 0.21

Race, white 24 (92%) 48 (87%) 0.99 37 (86%) 0.99

Antecedent Disease 0.62 0.64
   De novo 22 (85%) 43 (78%) 34 (79%)
   tAML 3 (12%) 6 (11%) 4 (9%)
   Prior MDS or MPN 1 (4%) 6 (11%) 5 (12%)

Cytogenetic Risk 0.99 0.84
   Favourable 1 (4%) 2 (4%) 2 (5%)
   Intermediate 23 (88%) 47 (87%) 38 (90%)
   Adverse 2 (8%) 4 (8%) 2 (5%)

NPM1 mutation 14 (56%) 21 (76%) 0.17 21 (78%) 0.14

Induction Treatment 0.71 0.67
  7+3 based induction 23 (88%) 50 (91%) 40 (93%)
  ADE 0 3 1
  Cytarabine/Mitoxantrone 3 0 0
  IA 0 2 2

Consolidation Therapy 0.0045 0.016
 None 10 10 8
  High/Int Cytarabine – 1 cycle 14 19 15
  High/Int Cytarabine – 2+ cycles 1 13 6
  Cytarabine + Anthracycline 0 10 9
  Sorafenib based 1 3 2

TKI prior to HCT 7 (27%) 15 (27%) 0.99 11 (26%) 0.99
  Midostaurin vs. Placebo 0 8 6
  Sorafenib 7 7 5

ECOG PS at HCT 0.76 0.79
   0 6 (25%) 17 (31%) 12 (28%)
   1 14 (58%) 27 (49%) 21 (49%)
   2 4 (17%) 11 (20%) 10 (23%)

Induction Intensity prior to HCT 0.81 0.99
   Myeloablative 14 (54%) 27 (49%) 22 (51%)
   Reduced intensity 12 (46%) 28 (51%) 21 (49%)

Donor Type 0.99 0.74
   Matched 21 (81%) 45 (82%) 37 (86%)
   Mismatched 5 (19%) 10 (18%) 6 (14%)

aGVHD prophylaxis 0.23 0.46
   CNI and Methotrexate 17 (65%) 27 (49%) 24 (56%)

All values given as n (%) unless otherwise indicated

ADE: cytarabine, daunorubicin; aGVHD: acute graft-versus-host disease; CNI: calcineurin inhibitor; ECOG PS: Eastern Cooperative Oncology Group performance score; HCT: haematopoietic cell transplantation; IA: idarubicin, cytarabine; MDS: myelodysplastic syndrome; MPN: myeloproliferative neoplasm; tAML: therapy-related acute myeloid leukaemia; TKI: tyrosine kinase inhibitor.