Abstract
Introduction: Although day D14 BM after initiation of induction chemotherapy is accepted standard of care in AML patients (pts), it has poor predictive value and low accuracy for refractory disease. Currently there are no established clinical and laboratory factors which accurately predict which AML pts with positive D14 BM require immediate reduction chemotherapy for persistent disease and which pts achieve complete remission (CR)
Methods: We retrospectively analyzed pretreatment factors and post-induction response in AML pts to determine if clinical and laboratory characteristics can improve the predictive value of the D14 BM evaluation.
Results: Among 297 pts with D14 BM biopsies, 183 pts (61%) had positive D14 BM (either ≥ 5% myeloblasts or cellularity ≥ 20%). Of those with a positive D14 BM biopsy, no reinduction chemotherapy was given to 89 pts of which 57 (64%) pts had persistent disease at count recovery and 32 (36%) pts achieved CR. Persistent disease at count recovery after positive D14 BM was more likely associated with higher percentage of D14 myeloblasts, history of relapsed disease, and poor-risk disease category than pts with positive D14 BM who achieved CR. Age, D14 BM cellularity, and WBC at first day of induction chemotherapy had no significant influence on remission status in pts with a positive D14 BM (Table 1). We developed, and tested in a validation cohort, new prediction model using both D14 BM status and clinical/laboratory factors such as the percentage of blasts, history of relapsed disease, and poorer disease risk category. Then we compared results of this prediction model to that of D14 BM alone without the usage of clinical/laboratory prognostic factors. Our prediction model significantly improved the positive predictive value (84% vs.64% P=0.001) and the accuracy of prediction of recovery marrow status (0.88% vs. 80%, P=0.002) in AML pts with positive D14 BM (Table 2).
Conclusion: In this study we developed and validated a new prediction model for interpreting D14 BM biopsies in AML pts after induction chemotherapy. With the addition of readily available clinical and laboratory information, our multivariable model provides a more accurate prediction of recovery bone marrow status and identification of patients with positive D14 BM who may not benefit from early reduction chemotherapy.
. | Persistent AML at count recovery . | CR+CRi . | P value . |
---|---|---|---|
Number | 57 | 32 | |
Age, years Median (min, max) | 59 (19, 75) | 55.5 (20, 78) | 0.064* |
WBC Count at Induction, x 109/L Median (min, max) | 5.7 (0, 285) | 3 (0, 95) | 0.25* |
D14 Cellularity, % Median (min, max) | 10 (5, 40) | 10 (3, 60) | 0.079* |
D14 Blasts, % 0-10 10%-30 >30 | 13 20 24 | 15 13 4 | 0.0023* |
Disease Status Before Induction Therapy De novo Relapsed | 19 38 | 26 6 | <0.0001** |
Antecedent Hematologic Disorder Yes No | 25 32 | 6 26 | 0.021** |
Risk Favorable/Normal High | 13 44 | 19 13 | 0.0013*** |
. | Persistent AML at count recovery . | CR+CRi . | P value . |
---|---|---|---|
Number | 57 | 32 | |
Age, years Median (min, max) | 59 (19, 75) | 55.5 (20, 78) | 0.064* |
WBC Count at Induction, x 109/L Median (min, max) | 5.7 (0, 285) | 3 (0, 95) | 0.25* |
D14 Cellularity, % Median (min, max) | 10 (5, 40) | 10 (3, 60) | 0.079* |
D14 Blasts, % 0-10 10%-30 >30 | 13 20 24 | 15 13 4 | 0.0023* |
Disease Status Before Induction Therapy De novo Relapsed | 19 38 | 26 6 | <0.0001** |
Antecedent Hematologic Disorder Yes No | 25 32 | 6 26 | 0.021** |
Risk Favorable/Normal High | 13 44 | 19 13 | 0.0013*** |
AML, acute myeloid leukemia; CR, complete remission; CRi, complete remission with incomplete count recovery; D, day; WBC, white blood cell.
*Wilcoxon rank sum test. **Fisher's exact test. ***Chi-square test
. | Sensitivity . | Specificity . | PPV . | NPV . | Accuracy . | P value* . |
---|---|---|---|---|---|---|
Without prognostic factors | 0.88 | 0.77 | 0.64 | 0.93 | 0.80 | 0.002 |
With prognostic factors** | 0.78 | 0.93 | 0.84 | 0.90 | 0.88 |
. | Sensitivity . | Specificity . | PPV . | NPV . | Accuracy . | P value* . |
---|---|---|---|---|---|---|
Without prognostic factors | 0.88 | 0.77 | 0.64 | 0.93 | 0.80 | 0.002 |
With prognostic factors** | 0.78 | 0.93 | 0.84 | 0.90 | 0.88 |
*Comparison of accuracies by two-sample binomial test. **The percentage of myeloblasts in the D14 BM, disease status, and risk category were used as prognostic factors.NPV, negative predictive value; PPV, positive predictive variable.
No relevant conflicts of interest to declare.
Author notes
Asterisk with author names denotes non-ASH members.
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