| Literature DB >> 36267971 |
Aoli Zhang1, Lipeng Liu1, Suyu Zong1, Xiaoyan Chen2, Chao Liu3, Lixian Chang1, Xiaojuan Chen1, Wenyu Yang1, Ye Guo1, Li Zhang1, Yao Zou1, Yumei Chen1, Yingchi Zhang1, Min Ruan1, Xiaofan Zhu1.
Abstract
Non-Down's syndrome acute megakaryocytic leukemia (non-DS-AMKL) is a subtype of childhood acute myeloid leukemia (AML), whose prognosis, prognostic factors and treatment recommendations have not yet to be defined in children. We conducted a retrospective study with 65 newly diagnosed non-DS-AMKL children from August 2003 to June 2020 to investigate the clinical impact of factors and clinical outcome. Among all 65 patients, 47 of them were treated at our center who received three different regimens due to time point of admission (CAMS-another, CAMS-2009 and CAMS-2016 protocol), and the efficacy were compared. Patients with newly diagnosed non-DS-AMKL accounted for 7.4% of pediatric AML cases. The median age of the patients was 18 months at diagnosis, and over 90% of them were under three-years-old. The overall survival (OS) rates were 33.3% ± 1.7%, 66.7% ± 24.4% and 74.2% ± 4.0% for three groups (CAMS-another, CAMS-2009 and CAMS-2016 regimen), respectively. In CAMS-2016 group, the complete remission (CR) rate after induction was 67.7% (21/31), while the total CR rate after all phases of chemotherapy was 80.6% (25/31). The 2-year survival probability did not significantly improve in patients underwent HSCT when compared with non-HSCT group (75.0% ± 4.7% vs. 73.9% ± 4.6%, p=0.680). Those who had a "dry tap" during BM aspiration at admission had significantly worse OS than those without "dry tap" (33.3% ± 8.6% vs. 84.0% ± 3.6%, p=0.006). Moreover, the results also revealed that patients with CD34+ had significantly lower OS (50.0% ± 6.7% vs. 89.5% ± 3.5%, p=0.021), whereas patients with CD36+ had significantly higher OS than those who were negative (85.0% ± 4.0% vs. 54.5% ± 6.6%, p=0.048). In conclusion, intensive chemotherapy resulted in improved prognosis of non-DS-AMKL children and subclassification may base on "dry tap" and immunophenotypic. Although some progress has been made, outcomes of non-DS-AMKL children remain unsatisfactory, especially in HSCT group, when compared with other AML types.Entities:
Keywords: non-DS-AMKL; outcomes; pediatric; prognostic factors; treatment
Year: 2022 PMID: 36267971 PMCID: PMC9577933 DOI: 10.3389/fonc.2022.940725
Source DB: PubMed Journal: Front Oncol ISSN: 2234-943X Impact factor: 5.738
Baseline characteristics of included non-DS-AMKL patients (n = 65).
| Characteristics | Patients |
|---|---|
| Gender ratio | 43M/22F |
| Median age at diagnosis, months(range) | 18 (5-89) |
| Median time from onset to diagnosis(range) | 2 (0.2-7) |
| Median WBC count, ×109/L (range) | 11.58 (2.44-55.35) |
| Median Hb count, g/L (range) | 82.4 (27-129) |
| Median PLT count, ×109/L (range) | 32 (6-222) |
| Hepatosplenomegaly, no. (%) | 24 (36.9%) |
| Median BM blasts, % (range) | 42.5 (4.0 -97.0) |
| Median PB blasts, % (range) | 16 (0 - 81.0) |
| “Dry tap”, no. (%) | 19/65(29.2%) |
|
| |
| PPO positive | 39 (83.0%) |
|
| |
| CD61 | 28 (48.3%) |
| CD41 | 36 (62.1%) |
| CD42b | 25 (43.1%) |
| CD34 | 19 (32.8%) |
| CD36 | 33 (56.9%) |
|
| |
| complex karyotypes | 21 (35.0%) |
| +21 | 18 (30.0%) |
| +19 | 19 (31.7%) |
| +8 | 20 (33.3%) |
| -7 | 2 (3.3%) |
| -13 | 3 (5.0%) |
| -15 | 4 (6.6%) |
M, male; F, female; Hb, hemoglobin; PLT, platelet; BM, bone marrow; PB, peripheral blood; PPO,platelet peroxidase.
Figure 1HE staining (A) and CD41 immunohistochemical staining (B) of the bone marrow from non-DS-AMKL children.
Figure 2A flowchart depicting newly diagnosed cases of non-DS-AML at our center from August 2003 to June 2020.
Figure 3Compared the OS (A) and EFS (B) in three distinct subgroups of pediatric non-DS-AMKL.
Figure 4The 2-year probabilities of OS (A) and EFS (B) comparing the outcomes in HSCT cohort with chemotherapy cohort. There is no significant difference in outcomes between the study groups. The 2-year probabilities of OS (C) and EFS (D) comparing the outcomes of patients with and without “dry tap”. The 2-year probabilities of OS (E) and EFS (F) comparing the outcomes of CD34+ and CD34- patients. “Dry tap” and CD34+ confer a poor outcome. The 2-year probabilities of OS (G) and EFS (H) comparing the outcomes of CD36+ and CD36- patients. CD36+ have a favorable outcome compared with CD36-.
Effects of potential factors on clinical outcomes in CAMS-2016 protocol (n=31).
| Cases | OS, % |
| EFS, % |
| ||
|---|---|---|---|---|---|---|
|
| ||||||
| male | 22 | 77.3% ± 4.4% | 0.426 | 72.7% ± 4.7% | 0.302 | |
| female | 9 | 66.7% ± 7.9% | 55.6% ± 8.0% | |||
|
| ||||||
| ≤12month | 8 | 87.5% ± 5.5% | 0.401 | 62.5% ± 7.5% | 0.699 | |
| >12month | 23 | 69.6% ± 4.7% | 69.6% ± 4.7% | |||
|
| ||||||
| Y | 6 | 33.3% ± 8.6% | 0.006 | 33.3% ± 8.8% | 0.030 | |
| N | 25 | 84.0% ± 3.6% | 76.0% ± 4.1% | |||
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|
| ||||||
| positive | 12 | 50.0% ± 6.7% | 0.021 | 41.7% ± 6.7% | 0.021 | |
| negative | 19 | 89.5% ± 3.5% | 84.2% ± 4.0% | |||
|
| ||||||
| positive | 20 | 85.0% ± 4.0% | 0.048 | 85.0% ± 3.9% | 0.007 | |
| negative | 11 | 54.5% ± 6.6% | 36.4% ± 6.2% | |||
|
| ||||||
| positive | 18 | 77.8% ± 4.6% | 0.779 | 77.8% ± 4.6% | 0.238 | |
| negative | 13 | 69.2% ± 5.9% | 53.8% ± 6.4% | |||
|
| ||||||
| positive | 15 | 80.0% ± 2.6% | 0.661 | 80.0% ± 2.6% | 0.215 | |
| negative | 16 | 68.8% ± 5.4% | 56.3% ± 5.9% | |||
|
| ||||||
| positive | 16 | 81.3% ± 4.7% | 0.529 | 81.3% ± 4.7% | 0.171 | |
| negative | 15 | 66.7% ± 5.6% | 53.3% ± 6.0% | |||
|
| ||||||
|
| ||||||
| Y | 11 | 63.6% ± 3.9% | 0.222 | 63.6% ± 3.7% | 0.599 | |
| N | 20 | 80.0% ± 4.4% | 70.0% ± 4.9% | |||
|
| ||||||
| Y | 14 | 57.1% ± 6.7% | 0.057 | 57.1% ± 6.8% | 0.233 | |
| N | 17 | 88.2% ± 3.9% | 76.5% ± 4.8% | |||
N, no; Y, yes.
Multivariable Cox Regression Analysis for OS and EFS in CAMS-2016 protocol n = 31.
| OS | EFS | |||||
|---|---|---|---|---|---|---|
| HR | 95% CI |
| HR | 95% CI |
| |
| Dry tap | 3.970 | (0.925,17.051) | 0.064 | 2.646 | (0.723,9.683) | 0.142 |
| CD34-positive | 4.038 | (0.781,20.865) | 0.096 | 3.006 | (0.741,12.194) | 0.124 |
| CD36-positive | 0.422 | (0.093,1.919) | 0.264 | 0.256 | (0.064,1.026) | 0.054 |