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. 2017 Mar 28;5(2):13. doi: 10.3390/biomedicines5020013

Table 1.

Patient, disease, and treatment characteristics.

Variable N (%)
Cohort Size, Overall 775
Transplant Indication
Myeloid malignancies 520 (67.1)
AML/MDS 408
Myeloproliferative and MDS/MPN overlap neoplasia 112
Lymphoid malignancies 228 (29.4)
ALL, including lymphoblastic lymphoma 110
Lymphoma, including CLL 77
Myeloma 41
Non-malignant disorders 27 (3.5)
Disease Stage at Transplant
Early/low-risk 288 (37.2)
Intermediate or advanced/high-risk 487 (62.8)
Conditioning Regimen
Myeloablative (including reduced toxicity myeloablative) * 527 (68.0)
Reduced intensity or non-myeloablative ** 248 (32.0)
Donor Type
Sibling 393 (50.7)
HLA matched 388
1 Ag mismatched 5
Unrelated 382 (49.3)
HLA matched (10/10 or 12/12 including DRB3-5) 246
HLA mismatched 136
Graft Source
Bone marrow 143 (18.5)
Peripheral blood (G-CSF mobilized) 632 (81.5)
Incorporation of ATG
No 425 (54.8)
Yes 350 (45.2)
ATG-Fresenius (Grafalon, Neovii) 256
Lower dose *** 160
Higher dose *** 96
Thymoglobuline 87
Lower dose *** 71
Higher dose *** 16
Alemtuzumab *** 7 (0.9)
Post-grafting Immunosuppression
MTX-based (mainly CsA/MTX) 340 (43.9)
MTX-free (mainly CsA/MMF) 435 (56.1)
HLA-C KIR-L Status
C1/1 291 (37.5)
C1/2 363 (46.9)
C2/2 121 (15.6)

* Myeloablative conditioning (MAC) regimens included full intensity MAC (total body irradiation (TBI) 10–13.2 Gy plus high-dose cyclophosphamide ± etoposide, or busulfan 12.8 mg/kg i.v. (or equivalent oral dose) plus high-dose cyclophosphamide ± etoposide), or reduced toxicity myeloablative conditioning (RTC, fludarabine plus i.v. busulfan 9.6–12.8 mg/kg ± thiotepa, or fludarabine plus 8.25–10 Gy TBI). ** Reduced intensity conditioning (RIC) included fludarabine plus either 4 Gy TBI or i.v. busulfan 6.4 mg/kg ± thiotepa. Non-myeloablative (NMA) regimen included fludarabine ± cyclophosphamide ± a maximum dose of either 2 Gy TBI or i.v. busulfan 3.2 mg/kg. In patients with refractory acute leukemia, the preparative regimen was intensified either by the addition of etoposide or thiotepa, or by application of a sequential protocol consisting of a 4-day FLAC (fludarabine, cytarabine) or FLAMSA (fludarabine, cytarabine ± amsacrine) induction phase followed after a 3-day rest by a TBI- or busulfan-based RIC or RTC. *** For anti-thymocyte globulin (ATG)-F, a lower dose was defined as ≤30 mg/kg total, and higher doses were those ≥35 mg/kg total. For Thymoglobuline, a lower dose was defined as ≤5 mg/kg total, and higher doses were those ≥7.5 mg/kg total. Alemtuzumab was dosed 40–100 mg flat (independent of bodyweight), with a median dose of 50 mg. All alemtuzumab doses were assigned to the higher-dose serotherapy group. HLA: human leukocyte antigen; AML, acute myeloid leukemia; MDS, myelodysplastic syndromes; ALL, acute lymphoblastic leukemia; CLL, chronic lymphocytic leukemia; MTX, methotrexate