Abstract 3090

Several biologic markers have been identified which predict an unfavorable course in CLL. Reduced-intensity conditioning (RIC) allogeneic transplant may be able to overcome some of these. This retrospective analysis evaluates the effect of cytogenetics, including metaphase cytogenetics, on outcomes with RIC-allogeneic SCT.

From 2005–2011, 51 RIC-allogeneic SCTs were performed at The Ohio State University for CLL. There were 38 males (74.5%) and 13 females (25.5%) with a median age of 58 (range 37–73). The median interval between diagnosis and SCT was 48 months (range 9–270). Before SCT, a median 4 lines of chemotherapy were given (range 1–11). One patient was in CR at the time of SCT, 39 were in PR, and 11 had stable or progressive disease; the median CMI was 3 (range 0–7). Fifty-nine percent of patients had del17; 53% had 3 or more abnormalities on metaphase cytogenetics, and 37% had 5 or more abnormalities. The source was PBSC in 48 (94%), BM in 1 (2%) and CB in 2 (4%). Of the PB or BM SCTs, 19 donors (39.6%) were related and 29 (60.4%) were volunteer; 45 (92%) were matched and 4 (8%) had a 1 allele mismatch. There were 21 (41%) pairs with an ABO mismatch and 16 (31.4%) pairs with a gender mismatch. Conditioning was Flu/Bu +/− ATG in 42 patients (82.2%), FluCamTBI in 6 (11.8%), FluCy in 1 (2%), and FluCyTBI-based in 2 receiving CB (4%). Following transplant, 34 (66.6%) developed AGVHD (gr 1–2: 28, gr 3–4: 6) and 27 of 48 evaluable patients (56.3%) developed CGVHD (limited: 7, extensive: 20). With a median follow-up of 17.3 months (range 1–60), the estimated 3-year OS and PFS following transplant were 56.5% and 42.9% respectively. Table 1 lists variables which had a p-value of ≤0.1 on univariate analysis. The presence of del13 and ≥5 karyotype abnormalities remained significant on multivariate analysis for OS while ≥5 karyotype abnormalities and conditioning with an alemtuzumab-containing regimen were significant for PFS (Table 2). The estimated 3 year OS for patients with del13 was 32.2% and 23% for patients with ≥5 karyotype abnormalities, compared with 72.7% and 73.5% for those without, respectively. The estimated 3-year PFS was 21.5% for patients with ≥5 karyotype abnormalities and 0% for patients with an alemtuzumab-containing regimen and 53.9% and 49.3% for those without, respectively.

Table.

Variables included in multivariate analysis model.

Variablelogrank p-valuePFS
OS
Age ≥55 0.0072* … 
Del13 ≥4.7% 0.0039* 
Del17p ≥5.7% 0.0019* 0.0878 
Karyotype abnormalities ≥5 0.0002* 0.0138* 
Karyotype abnormalities ≥3 0.0186* 0.0623 
Largest node ≥4 cm 0.0277* … 
Marrow involvement ≥50% 0.0752 … 
Alemtuzumab conditioning … 0.0001* 
GVHD prophylaxis 0.0001* 0.0374* 
HLA mismatch <0.0001* … 
Variablelogrank p-valuePFS
OS
Age ≥55 0.0072* … 
Del13 ≥4.7% 0.0039* 
Del17p ≥5.7% 0.0019* 0.0878 
Karyotype abnormalities ≥5 0.0002* 0.0138* 
Karyotype abnormalities ≥3 0.0186* 0.0623 
Largest node ≥4 cm 0.0277* … 
Marrow involvement ≥50% 0.0752 … 
Alemtuzumab conditioning … 0.0001* 
GVHD prophylaxis 0.0001* 0.0374* 
HLA mismatch <0.0001* … 
*

statistically significant at p<0.05

Table 2.

Multivariate analysis of OS, PFS.

OS
VariableHR95% CIp-value
Del13q    
<4.7%   
≥4.7% 3.58 1.36 to 9.42 0.01 
Karyotype    
<4   
≥5 5.16 1.97 to 13.56 0.001 
PFS 
Variable HR 95% CI p-value 
Conditioning    
no alemtuzumab   
alemtuzumab 9.8 3.28 to 29.29 
Karyotype    
<4   
≥5 4.35 1.67 to 11.28 0.002 
OS
VariableHR95% CIp-value
Del13q    
<4.7%   
≥4.7% 3.58 1.36 to 9.42 0.01 
Karyotype    
<4   
≥5 5.16 1.97 to 13.56 0.001 
PFS 
Variable HR 95% CI p-value 
Conditioning    
no alemtuzumab   
alemtuzumab 9.8 3.28 to 29.29 
Karyotype    
<4   
≥5 4.35 1.67 to 11.28 0.002 

Due to small numbers, the alemtuzumab data should be interpreted with caution, but are consistent with previous reports. Increasing genomic complexity is known to predict for diminished chemosensitivity. Accordingly, the presence of 5 or more abnormalities on metaphase cytogenetics was demonstrated to be a poor prognostic indicator for both PFS and OS following SCT. There was substantial, but not universal, overlap among patients with del17, del13, and highly complex karyotype; this interplay merits further consideration. Better understanding of the evolution of genetic complexity will better define how to time transplant to allow for maximum benefit to those patients likely to evolve.
Figure 1.

OS and PFS by Karyotype

Disclosures:

No relevant conflicts of interest to declare.

Author notes

*

Asterisk with author names denotes non-ASH members.

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