Dynamic changes and multiplication rate of white blood cell count may direct the timing of cytoreduction chemotherapy during induction treatment in newly diagnosed acute promyelocytic leukemia with low‑intermediate risk
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- Published online on: April 5, 2021 https://doi.org/10.3892/mco.2021.2274
- Article Number: 112
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Copyright: © Wen et al. This is an open access article distributed under the terms of Creative Commons Attribution License.
Abstract
Introduction
All-trans retinoic acid (ATRA) and arsenic trioxide (ATO) are two basic drugs for induction treatment for newly diagnosed acute promyelocytic leukemia (APL). Based on numerous clinical trials (1,2), the National Comprehensive Cancer Network (NCCN) guideline recommends ATRA combined with ATO as the standard induction treatment for de novo APL with low risk [white blood cell (WBC) count <10x109/l (3). Only if there are any contraindications to arsenic, ATRA combined with idarubicin could be considered (4-6). Chinese APL guideline also recommends ATRA combined with ATO as basic treatment for induction therapy for de novo APL (7). Anthracyclines or other cytoreduction chemotherapy could be chosen if WBC count is >10x109/l. After administration of ATRA and ATO, WBC count will typically rise and may lead to differentiation syndrome (DS). Cytoreduction chemotherapy may partially prevent or control the risks of DS. However, no guidelines give specific suggestions about when and how to initiate cytoreduction chemotherapy. Our previous research indicated that it was better to initiate cytoreduction chemotherapy when WBC count was between 4x109/l and 15x109/l during induction treatment for APL with low-intermediate risk (8). It is difficult for clinicians to decide to use chemotherapy when WBC count is not very high. However, the WBC count occasionally multiplies and exceeds 15x109/l very rapidly before clinicians can make a decision. To assess the appropriate time to initiate cytoreduction therapy during induction treatment, static WBC count may not be universally satisfactory. Hence, this study was designed to explore the relationship between the multiplication rate of WBC count and clinical effects during ATRA plus ATO-based induction treatment for patients with low-intermediate risk APL.
Patients and methods
Patients
Between January 2015 and December 2020, a total of 92 newly diagnosed patients were admitted to our hematology department. Of these, 60 patients were categorized into the low-intermediate risk group, and the remaining patients were categorized into the high risk group, based on Sanz's risk stratification model for survival prediction (9). All 58 patients (34 males and 24 females), with a median age of 34 years (range 17-71 years)] with low-intermediate risk, who had complete clinical data, were retrospectively enrolled in this study. Disease diagnosis was confirmed by bone marrow aspiration, chromosome karyotyping analysis, fluorescence in situ hybridization analysis and polymerase chain reaction. Informed consent prior to and regarding the treatment protocol was obtained from all patients analyzed in the present study.
Treatments
When a diagnosis of APL was suspected, ATRA (20 mg/m2/day) was administered at the earliest, until complete remission (CR) was achieved. All 58 patients received ATRA and ATO-based induction treatment. If the WBC count increased, cytotoxic agents-based chemotherapy was initiated based on the clinician's decision in order to reduce leukemia cells and prevent risks of DS. A total of 19 cases received idarubicin (8 mg/m2/day on days 1-3), 32 cases received daunorubicin (45 mg/m2/day on days 1-3), two cases received daunorubicin (45 mg/m2/day on days 1-3) combined with cytarabine (100 mg/m2/day on days 1-7), and five cases received only hydroxyurea (2.0-3.0 g/day, adjusted according to blood cells). Blood product support was applied to maintain platelet (PLT) level ≥30x109/l, hemoglobin level ≥70 g/l and plasma fibrinogen level ≥1.5 g/l. All adverse events related to treatments, including bone marrow depression, infection and bleeding, were graded according to the National Cancer Institute Common Terminology Criteria for Adverse Events version 4.03(10).
Definitions and groups
DS was diagnosed based on the incidence of at least two of the following clinical features: Unexplained fever, acute respiratory distress with interstitial pulmonary infiltrates, acute renal failure, weight gain >5 kg, unexplained hypotension, and pleuropericardial effusion (11). Prevention strategies included dexamethasone (10 mg q12h), and discontinuation of ATRA and ATO. All 58 patients were categorized according to Sanz's risk stratification score (9) as low risk (WBC count <10.0x109/l and PLT ≥40.0x109/l at diagnosis) and intermediate risk (WBC count <10x109/l and PLT <40.0x109/l). CR was defined as the presence of <5% blast cells in bone marrow aspirates, PLT >100x109/l and no juvenile cells in peripheral blood according to the criteria established by the US National Cancer Institute (12). Early mortality was defined as fatality during induction treatment from the first day of hospitalization. Eastern Cooperative Oncology Group (ECOG) performance status score (0-4 score) was applied to investigate the patient's physical status prior to chemotherapy (13). WBC count >4x109/l and WBC multiplication time <3 days was defined as rapid WBC multiplication. Table I presents a comparison of the baseline clinical and laboratory parameters of the groups with rapid WBC multiplication and without rapid WBC multiplication.
 | Table IBaseline demographic, clinical and laboratory characteristics of groups without (n=31) or with (n=27) rapid WBC multiplication. |
Statistical analysis
Statistical analysis was performed with SPSS v.22.0 software (SPSS Inc.). All data were collected in December 2020. Clinical features are presented as percentages (%) for categorical variables, and as mean values ± standard deviation for normally distributed continuous variables. The χ2 test was used to analyze the significance of differences in the distribution of categorical variables between the patient subsets, and the SNK method and Bonferroni's correction were used to compare the two groups. The unpaired Student's t-test or Mann-Whitney U test was used to analyze the significance of differences in the distributions of continuous parametric variables and ranked variables. Multivariate analysis was performed using a binary logistic regression model. WBC count at diagnosis, WBC count at chemotherapy initiation, peak WBC count, and with or without rapid WBC multiplication were considered in the multivariate analysis to evaluate their effects on DS, early mortality and grade 3-4 bleeding. P<0.05 was considered to indicate statistical significance.
Results
Comparisons of clinical effects between patients with and without rapid WBC multiplication
Comparison of the baseline features, clinical and laboratory parameters is shown in Table I. No significant differences were found in age, gender and ECOG score between the two groups. WBC count at diagnosis was slightly higher in the group with rapid WBC multiplication (2.14±1.66 x109/l vs. 3.82±2.98 x109/l, P=0.013). There was no difference between the two groups in Sanz's risk stratification (P=0.121). Biochemical tests showed no differences in uric acid, albumin and creatine levels in patients with or without rapid WBC multiplication. Coagulation functions including activated partial thromboplastin, prothrombin time, fibrinogen and D-dimer level were similar in the two groups.
As depicted in Table II, the incidence of DS was higher (48.1 vs. 6.5%, P=0.000), grade 3-4 bleeding was more frequent (34.8 vs. 6.5%, P=0.022), and peak WBC count was higher (30.4±20.0x109/l vs. 8.67±5.4x109/l, P=0.000) in the rapid WBC multiplication group. There were no differences in bone marrow depression, infection, CR rate, time to achieve CR and early mortality rate between the two groups.
| Table IIComparison of clinical effects in groups without (n=31) or with (n=27) rapid WBC multiplication. |
Multivariate associations
To further evaluate the effects of dynamic changes of WBC count during induction treatment on DS, early mortality and bleeding events, a binary logistic regression model was used. The results of multivariate analysis revealed that WBC count at chemotherapy initiation was an independent risk factor for the occurrence of DS [P=0.040, odds ratio (OR)=1.0216, 95% confidence interval (CI)=1.009-1.465]. Peak WBC count and rapid WBC multiplication were significantly related to grade 3-4 bleeding (P=0.019, OR=0.773, 95% CI=0.623-0.959; P=0.002, OR=99.567, 95% CI=5.738-1727.726). However, WBC count at diagnosis, WBC count at chemotherapy initiation, peak WBC count and rapid WBC multiplication were not independent risk factors for early mortality (Table III).
| Table IIIMultivariate analysis of WBC count at diagnosis and CT initiation, peak WBC count and rapid WBC multiplication. |
Discussion
European Leukemia Net updated the recommendations for management of APL in 2019(14). For non-high-risk APL patients (WBC ≤10x109/l), either ATRA plus ATO without chemotherapy or standard ATRA-idarubicin therapy were recommended as induction treatment, which was consistent with NCCN guidelines (3). In both guidelines, when and how to use cytoreduction therapy during ATRA plus ATO-based induction treatment was not discussed. However, the risks of DS may increase with the increase of WBC count, which may lead to other serious side effects. Hence, a randomized clinical trial was designed to compare the efficacy of ATRA-ATO vs. ATRA-ATO plus chemotherapy in all-risk patients with APL (15), but the results have not yet been published.
Our previous study found that WBC count can be conveniently used to direct cytoreduction chemotherapy during induction treatment for low-intermediate risk APL. When WBC count is between 4x109/l and 15x109/l, cytotoxic drugs could be initiated to control leukocytosis (8). However, for patients with different types of WBC count multiplication rate, single WBC count may be inadequate to decide on cytoreduction therapy. For slow type of WBC count multiplication, cytoreduction therapy may be optional, even if WBC count increases to >10x109/l. However, patients whose WBC count doubles rapidly, cytoreduction therapy should be considered even if WBC count is <10x109/l because of DS risk. Hence, this study attempted to establish the effects of WBC dynamic changes along with static WBC count on early adverse events including early death, DS, grade 3-4 infection and bleeding.
Since there were no similar studies to be referred, we defined rapid WBC multiplication as WBC count >4x109/l and multiplication time <3 days. It was a grouping method based on clinical experience. Comparison results indicated that patients with rapid WBC multiplication rate had higher possibility of DS and grade 3-4 bleeding, which was consistent with significantly higher peak WBC count in patients with rapid WBC multiplication. However, these adverse effects did not increase the incidence of early death. Multivariate analysis further proved that WBC count in chemotherapy was the most important factor for DS, and WBC multiplication rate was closely related to serious bleeding events.
The main limitation of this study was its retrospective design. In this study, baseline characteristics between the two groups were not statistically equal, especially WBC count at diagnosis. However, mean WBC count at diagnosis in both groups was less than normal level. Further multivariate analysis showed that the WBC count at diagnosis was not the most important factor for DS, early mortality and grade 3-4 bleeding, compared to other three factors. To some extent, multivariate analysis corrected the bias caused by differences in baseline characteristics. Different from previous research, this study collected patient's data from another hospital, and all patients were treated with ATRA plus ATO. However, we obtained similar result that WBC count at chemotherapy initiation was associated with DS.
Overall, WBC count at chemotherapy initiation along with WBC multiplication rate could direct the timing of cytoreduction chemotherapy during induction treatment in newly diagnosed acute promyelocytic leukemia with low-intermediate risk.
Acknowledgements
Not applicable.
Funding
The study was funded by a research project from Mianyang Health Commission (grant no. 201914).
Availability of data and materials
The datasets used and/or analyzed during the current study are available from the corresponding author on reasonable request.
Authors' contributions
FX conceived and designed the study, and provided administrative support. FX, JW and QZ designed the concept of the article and wrote the manuscript. FX and JW analyzed and interpreted the data, and confirmed the authenticity of the data. JW, QZ, HH, YL, JS, YZ, WQ and LS designed the concept of the article and collected the data. All authors contributed to the provision of study materials or patients. All authors read and approved the final manuscript.
Ethics approval and consent to participate
Ethics approval was obtained from the Ethics Committee of Mianyang Central Hospital (Mianyang, China; approval no. S-2019-099). Written informed consent prior to and regarding the treatment protocol was obtained from all patients analyzed in the present study.
Patient consent for publication
Not applicable.
Competing interests
The authors declare that they have no competing interests.
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