Sixty-four patients (pts) with chemotherapy-refractory CLL who were ineligible for ablative allogeneic HCT due to age and/or comorbidities were given nonablative-HCT from related (n=44) or unrelated donors (n=20) between 1997-2003 (Table). Median pt age was 56 (range 44–69) years, interval from diagnosis to HCT was 4.4 (3–25) years, and number of prior regimens was 4 (range 1–12). Sixty-one pts were refractory to at least 1 regimen, 56 to fludarabine (FLU), 19 to alkylating agents, 14 to rituxumab and 4 to CAMPATH, and 2 had failed autologous HCT. Twenty-three pts (36%) had disease responsive to last chemotherapy [28% partial (PR) and 8% complete remission (CR)] while 34 were nonresponsive and 7 had untested relapse. Conditioning for HCT consisted of 2 Gy TBI alone (n=11) or combined with FLU (n=53), 90 mg/m2. Postgrafting immunosuppression consisted of mycophenolate mofetil and cyclosporine. Pts received G-CSF mobilized peripheral blood mononuclear cells. After HCT, pts became neutropenic for a median of 11 days. Forty-four percent of pts had thrombocytopenia (<20,000 cells/ul). Three pts had graft rejection; 1 died with aplasia and 2 are alive with disease relapse. Incidences of grades II, III, and IV acute GVHD were 39%, 14%, and 2% respectively, and chronic GVHD was 50% at 2-years. With median follow up of 24 (range 2.8–62.8) months, the overall response rate was 67% (50% in CR). URD-pts had significantly higher CR rate than MRD-pts. All 11 responding patients tested had molecular eradication of their disease. Overall, 39 patients are alive; 25 in CR, 5 in PR, 2 with stable disease, and 7 with relapse/progression. Twenty-five pts died, 10 from progression, 10 from infections ± GVHD, 2 from cardiac causes, 1 from metastatic lung cancer, 1 from cerebral stroke and 1 from rejection and aplasia. Estimated 2-year rates of non-relapse mortality, disease free survival, and overall survival were 22%, 52%, and 60% respectively. In multivariate analysis, high pretransplant comorbidity scores predicted higher non-relapse mortality and worse survival while bulky lymphadenopathy predicted increased risk of progression. CLL appears susceptible to graft-versus-leukemia effects particularly after URD grafts and nonablative-HCT should be explored in phase II trials in pts with FLU-refractory CLL.

Table: Results

Related (n = 44)Unrelated (n = 20)P
Acute GVHD grade II, III, and IV 39%, 11%, and 2% 40%, 20%, and 0% 0.41 
2-year chronic extensive GVHD 44% 69% 0.56 
Median follow up (range) 31 (3–63) months 12 (3–39) months  
CR at 2-years 42% 78% 0.005 
Relapse/progression at 2 years 34% 5% 0.08 
Surviving pts 13 CR, 3 PR, 2 stable, 5 progression, 1 relapse 12 CR, 2 PR, 1 relapse  
2-year non-relapse mortality 22% 20% 0.75 
2-year disease free survival 44% 75% 0.15 
2-year overall survival 56% 74% 0.33 
Related (n = 44)Unrelated (n = 20)P
Acute GVHD grade II, III, and IV 39%, 11%, and 2% 40%, 20%, and 0% 0.41 
2-year chronic extensive GVHD 44% 69% 0.56 
Median follow up (range) 31 (3–63) months 12 (3–39) months  
CR at 2-years 42% 78% 0.005 
Relapse/progression at 2 years 34% 5% 0.08 
Surviving pts 13 CR, 3 PR, 2 stable, 5 progression, 1 relapse 12 CR, 2 PR, 1 relapse  
2-year non-relapse mortality 22% 20% 0.75 
2-year disease free survival 44% 75% 0.15 
2-year overall survival 56% 74% 0.33 
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Topics:
chemotherapy regimen, chronic b-cell leukemias, chronic lymphocytic leukemia, conditioning (psychology), donors, hematopoietic stem cell transplantation, human leukocyte antigens, brachial plexus neuritis, follow-up, graft-versus-host disease

Author notes

Corresponding author

2005, The American Society of Hematology
2004
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