Abstract 951

AML cells with CD34+CD38-CD123+ phenotype represent a subset enriched in leukemic stem cells. Moreover, this subpopulation has been described to be resistant to genotoxic agents as compared with leukemic bulk. However, the clinical impact of the amount of CD34+CD38-CD123+ remains poorly described. In this study we evaluated the prognostic impact of the amount of CD34+CD38-CD123+ cells detected at diagnosis in a series of AML patients treated by intensive chemotherapy according to trials from the French GOELAMS group.

Quantification of blast cells with the CD34+CD38-CD123+ phenotype was achieved by flow cytometry in 111 patients less than 66 years old with de novo AML treated by 3+7-like chemotherapy.

The characteristics of the patients are shown in table 1.

Age, WBC count, NPM1 mutation and FLT3-ITD had no impact on achievement of complete response (CR) whereas, CD34+CD38-CD123+ (>15%) and unfavourable karyotype were significantly correlated with lack of CR. By logistic regression, CD34+CD38-CD123+ (>15%) retains significance for CR achievement with an OR of 0.3 (0.11-0.84) (p=0.02). For the 91 complete responders, age, WBC count, karyotype, NPM1 mutation had no impact on disease-free survival (DFS).Interestingly, patients with <1%, 1–15%, >15% CD34+CD38-CD123+ had a median DFS of 57.6 (SE 6.6), 11.2 (SE 7.5) and 9.2 (SE 13.4) months, respectively (p<0.0001, figure 1). FTL3-ITD was also significantly associated with a shorter DFS. In multivariate analysis, CD34+CD38-CD123+<1% was significantly associated with a longer DFS (p=0.00025). Age, %CD34+CD38-CD123+, karyotype, NPM mutation and FLT3-ITD significantly influenced overall survival (OS) whereas WBC count had no impact. Median OS was particularly impressive for patients with CD34+CD38-CD123+<1%. Indeed, median OS was 78.2 (SE 10.7), and 15.3 (SE 5.8) months for CD34+CD38-CD123+<1% vs others, respectively (p<0.0001, figure 1). Multivariate analysis for OS retains two significant factors: adverse karyotype (95%CI, 1.19–4.02, p=0.012) and CD34+CD38-CD123+<1% (95%CI, 0.12–0.52, p=0.00018). Moreover, although the number of patients was low in favourable karyotype (CBF), CD34+CD38-CD123+<1% had a major impact on both DFS, median 57.6 vs 10.2 months for >1% (HR, 0.19, 0.06–0.59, p=0.0038) and OS, median not reached vs 18.5 months (p=0.0025).

This study emphasizes the prognosis impact of the CD34+CD38-CD123+ cell burden in AML patients, which is predictive for shorter OS and DFS when representing more than 1% of the leukemic cells, regardless of the usual prognosis categories. We provide here a new prognosis marker that may be easily translated to the clinical practice in AML although it remains to be validated on a large prospective cohort of patients. Moreover, new therapies targeting this subpopulation could help to improve outcome in AML patients.

Table

Characteristics of patients.

All patients N=111CD34+CD38-CD123+< 1 % N=40CD34+CD38-CD123+ 1-15% N=20CD34+CD38-CD123+> 15% N=20
Gender, M/F 50/62 19/21 24/27 6/14 
Age, median 48 (20–65) 47 (20–65) 51 (20–64) 50 (21–65) 
WBC,median (G/L) 33.2 (1–254) 13.8 (1–237.7) 41 (1.3–254) 32.9 (2.3–193.2) 
Favourable caryotype 23 11 
Intermediate caryotype 69 24 37 
Unfavourable caryotype 19 
NPM1 mutation 28/95 7/31 16/45 5/19 
FLT3-ITD 33/100 7/34 21/47 5/19 
Complete Response 91 (82%) 36 (90%) 42 (81.4%) 13 (65%) 
Relapse 53 (58.2%) 13 (36.1%) 30 (71.4%) 10 (76.9%) 
Allogeneic-SCT 33 (36.3%) 11 (30.6%) 15 (35.7%) 7 (53.8%) 
All patients N=111CD34+CD38-CD123+< 1 % N=40CD34+CD38-CD123+ 1-15% N=20CD34+CD38-CD123+> 15% N=20
Gender, M/F 50/62 19/21 24/27 6/14 
Age, median 48 (20–65) 47 (20–65) 51 (20–64) 50 (21–65) 
WBC,median (G/L) 33.2 (1–254) 13.8 (1–237.7) 41 (1.3–254) 32.9 (2.3–193.2) 
Favourable caryotype 23 11 
Intermediate caryotype 69 24 37 
Unfavourable caryotype 19 
NPM1 mutation 28/95 7/31 16/45 5/19 
FLT3-ITD 33/100 7/34 21/47 5/19 
Complete Response 91 (82%) 36 (90%) 42 (81.4%) 13 (65%) 
Relapse 53 (58.2%) 13 (36.1%) 30 (71.4%) 10 (76.9%) 
Allogeneic-SCT 33 (36.3%) 11 (30.6%) 15 (35.7%) 7 (53.8%) 
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Disclosures:

No relevant conflicts of interest to declare.

Figure 1:
Figure 1:. Impact of percentage of CD34+ CD38- CD123+ leukemic cells on outcome of patients with de novo AML. A, overall survival of 111 patients less than 66 years old treated by 3+7 like chemotherapy. B, disease-free survival of 91/111 complete responder patients.
View largeDownload slide

Impact of percentage of CD34+ CD38- CD123+ leukemic cells on outcome of patients with de novo AML. A, overall survival of 111 patients less than 66 years old treated by 3+7 like chemotherapy. B, disease-free survival of 91/111 complete responder patients.

Figure 1:
Figure 1:. Impact of percentage of CD34+ CD38- CD123+ leukemic cells on outcome of patients with de novo AML. A, overall survival of 111 patients less than 66 years old treated by 3+7 like chemotherapy. B, disease-free survival of 91/111 complete responder patients.
View largeDownload slide

Impact of percentage of CD34+ CD38- CD123+ leukemic cells on outcome of patients with de novo AML. A, overall survival of 111 patients less than 66 years old treated by 3+7 like chemotherapy. B, disease-free survival of 91/111 complete responder patients.

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Topics:
cd38, chemotherapy regimen, complete remission, flow cytometry, impedance threshold device, karyotype determination procedure, leukemia, myelocytic, acute, leukemic cells, leukemic hematopoietic stem cell, leukocyte count

Author notes

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Asterisk with author names denotes non-ASH members.

© 2010 by The American Society of Hematology
2010
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