Current Diagnostic Approach in Acute Myeloid Leukemia in the Republic of Macedonia: A Proposal for Minimal Screening-Based Clinical Stratification

Liljana Hadzi-Pecova, Sanja Trajkova, Aleksandar Stojanovik, Lidija Cevreska
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Abstract

Introduction

Acute myeloid leukemia (AML) represents a heterogeneous complex of disorders resulting from diverse mechanisms of leukemogenesis. Correct diagnosis of AML subtypes plays a central role for individual clinical risk stratification and therapeutic decisions. Motivated to improve and simplify the diagnosis and management of AML in the Republic of Macedonia, we conducted a prospective study at the University Clinic of Hematology.

Patients and Methods

A total of 76 adults (> 15 years of age; from an initial 77 tested) with acute leukemia who were consecutively admitted at the clinic were enrolled in the study. The aim of our study was to establish and standardize diagnostic approaches based on minimal screening tests that will facilitate risk-adapted therapy for each single AML patient. The diagnosis of acute leukemia was made by standard criteria of the French-American-British (FAB) Cooperative Study Group and confirmed by immunophenotyping bone marrow aspirates and/or peripheral blood samples following the criteria of the European Group for the Immunological Classification of Leukemia's (EGIL) and the British Committee for Standards in Hematology (BCSH).

Results

Our results showed that morphology and cytochemistry established lineage in 68 (89.4%) of patients. Immunophenotyping further revealed the exact lineage assignment of the blast cells in 11.8% of patients and also changed the lineage assignment in 3 patients and guided to implementation of specific molecular analyses for the further definition of some AML cases. Using an RQ-PCR assay we detected the presence of the fusion transcript PML/RARα in 5 patients and classified 10 more patients in the prognostic favorable genetic entity Core Binding Factor (CBF)-AML according to the presence of the abnormal fusion transcripts AML1—ETO, CBFβ—MYH11. Those results were essential for more appropriate single-patient therapeutic decisions.

Conclusion

Our multimodal diagnostic approach consisted of cytomorphology, cytochemistry, multiparameter flow cytometry, and molecular analyses improved the diagnosis and enabled individual clinical stratification in 38.2% of our AML patients.

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马其顿共和国急性髓系白血病的当前诊断方法:基于最小筛查的临床分层建议
急性髓性白血病(AML)是一种由不同的白血病发生机制引起的异质性复杂疾病。AML亚型的正确诊断对个体临床风险分层和治疗决策起着核心作用。为了改善和简化马其顿共和国AML的诊断和管理,我们在大学血液学诊所进行了一项前瞻性研究。患者与方法76例成人(>15岁;从最初的77名连续入院的急性白血病患者中,他们被纳入了这项研究。我们研究的目的是建立和标准化基于最小筛选试验的诊断方法,这将促进每个AML患者的风险适应治疗。急性白血病的诊断采用法、美、英(FAB)合作研究组的标准,并根据欧洲白血病免疫分类组(EGIL)和英国血液学标准委员会(BCSH)的标准,通过骨髓抽吸和/或外周血样本的免疫表型进行确认。结果68例(89.4%)患者经形态学和细胞化学鉴定为系。免疫表型分析进一步揭示了11.8%患者母细胞的确切谱系分配,并改变了3例患者的谱系分配,并指导实施特异性分子分析,以进一步定义一些AML病例。通过RQ-PCR检测,我们在5例患者中检测到了融合转录物PML/RARα的存在,并根据异常融合转录物am_1 - eto、CBFβ - myh11的存在,将另外10例患者分类为预后有利遗传实体核心结合因子(CBF)-AML。这些结果对于更合适的单患者治疗决策至关重要。结论:我们的多模式诊断方法包括细胞形态学、细胞化学、多参数流式细胞术和分子分析,提高了38.2% AML患者的诊断并实现了个体临床分层。
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