The overall unfavorable prognosis of CD10 negative (CD10) precursor B-cell acute lymphoblastic leukemia (BCP-ALL) is well known. We analyzed 4473 pediatric patients (pts) <18 years (y) with BCP-ALL and immunophenotyping of CD10 enrolled from 1986 to 2000 in three consecutive ALL-BFM trials to explore prognostic factors in the CD10 subset. CD10 negativity was defined by CD10 expression in <20% of blasts. 233 pts (5.2%) were CD10. In comparison to CD10 positive (CD10+) BCP-ALL pts, CD10 pts comprised more infants (age <1y 34% vs. 1%, p(X2)<0.001), more cases with hyperleukocytosis (WBC ≥100/nl 43% vs. 6%, p<0.001), more CNS involvement (CNS positive 10% vs. 2%; p<0.001) and an impaired treatment response (prednisone poor response (PPR) 22% vs. 5%, p<0.001; induction failure 6% vs. 1%, p<0.001). Estimated probability of 5 years event free survival (5y-pEFS) was significantly lower in pts with CD10 as compared to CD10+ BCP-ALL (49±3% vs 81±0.6%, p(log-rank)<0.001). Cox regression analysis including age, WBC, prednisone response (PR) and MLL/AF4 status as covariables revealed CD10 negativity as independent prognostic factor (RR 1.5, 95% confidence interval (CI) 1.1–2.1, p=0.01). Further analyses were performed within the CD10 group: 83% of infants and 60% of pts ≥1y were successfully analyzed for MLL/AF4. MLL/AF4 was detected in 55% of pts <1y and 27% of pts ≥1y. The well known risk factors for BCP-ALL (sex, age, WBC, CNS involvement, MLL/AF4 and PPR) also had prognostic impact within the CD10 group:

n*5y-pEFS* (%)SE (%)p (log-rank)
*5 pts w/o reinduction were excluded 
sex female 109 55 0.022 
 male 119 40  
age <1y 78 25 <0.001 
 ≥1y 150 62  
WBC <100/nl 128 62 <0.001 
 ≥100/nl 100 33  
CNS neg 181 54 0.011 
 pos 21 33 10  
MLL/AF4 neg 95 53 0.001 
 pos 61 29  
PR good 170 57 <0.001 
 poor 50 30  
n*5y-pEFS* (%)SE (%)p (log-rank)
*5 pts w/o reinduction were excluded 
sex female 109 55 0.022 
 male 119 40  
age <1y 78 25 <0.001 
 ≥1y 150 62  
WBC <100/nl 128 62 <0.001 
 ≥100/nl 100 33  
CNS neg 181 54 0.011 
 pos 21 33 10  
MLL/AF4 neg 95 53 0.001 
 pos 61 29  
PR good 170 57 <0.001 
 poor 50 30  
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Out of a number of immunophenotypic markers, analyzed at different expression cut-off points, CD24 at missing or weak expression of <40% and CD65 at high expression of ≥40% were significantly correlated with unfavorable clinical characteristics and worse outcome within the CD10 group. Significant correlation with PR could only be demonstrated for expression of CD24, which is presumed to act as negative regulator in B-cell development through mediation of apoptosis.

age<1y*WBC ≥100/nl*MLL/AF4 pos*PPR#pEFS§
n/total (%)n/total (%)n/total (%)n/total (%)% ±SE
* all p(X2)<0.01, #CD24 p=0.01, CD65 n.s., §all p(log-rank]<0.001 
CD24 <40% 37/77 (48) 52/77 (68) 33/56 (59) 24/73 (33) 32 ±5 
CD24 ≥40% 34/122 (28) 35/122 (29) 18/76 (24) 20/119 (17) 59 ±5 
CD65 <40% 56/180 (31) 67/180 (37) 39/120 (33) 39/175 (22) 30 ±7 
CD65 ≥40% 22/44 (50) 32/44 (73) 21/34 (62) 10/41 (24) 54 ±4 
age<1y*WBC ≥100/nl*MLL/AF4 pos*PPR#pEFS§
n/total (%)n/total (%)n/total (%)n/total (%)% ±SE
* all p(X2)<0.01, #CD24 p=0.01, CD65 n.s., §all p(log-rank]<0.001 
CD24 <40% 37/77 (48) 52/77 (68) 33/56 (59) 24/73 (33) 32 ±5 
CD24 ≥40% 34/122 (28) 35/122 (29) 18/76 (24) 20/119 (17) 59 ±5 
CD65 <40% 56/180 (31) 67/180 (37) 39/120 (33) 39/175 (22) 30 ±7 
CD65 ≥40% 22/44 (50) 32/44 (73) 21/34 (62) 10/41 (24) 54 ±4 
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Including age, WBC, PR and MLL/AF4 status as covariables, out of the analyzed markers only CD65 proved to be an independent prognostic factor in CD10 BCP-ALL (Cox regression analysis: RR 1.5, 95% CI 1.1–2.9, p=0.018). The identification of additional prognosis associated immunophenotypic markers may contribute to further refinement of treatment strategies for CD10 BCP-ALL pts.

Topics:
burkitt's lymphoma, leukemia, b-cell, acute, neprilysin, prognostic factors, child, brachial plexus neuritis, prednisone, immunophenotyping, leukocytosis, marked

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2005, The American Society of Hematology
2004
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