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Flow Cytometry Immunophenotyping Evaluation in Acute Lymphoblastic Leukemia: Correlation to Factors Affecting Clinic Outcome

机译:急性淋巴细胞白血病流式细胞仪免疫分型评估:与影响临床结果的因素的相关性。

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The authors conducted a flow cytometry immunophenotyping study in patients with acute lymphoblastic leukemia (ALL) from Natal, Rio Grande do Norte, Brazil. The patients (n = 126) were newly diagnosed using a panel of monoclonal antibodies: CD1a, CD2, CD3, CD4, CD7, CD8, CD10, CD13, CD33, CD14, CD19, CD22, CD79a, CD117, CD34, anti-IgM, anti-TdT, anti-HLA-Dr, and anti-human kappa and lambda light chains. Additional data, such as patients' age and gender, clinical and laboratory findings such as presence of tumor masses, lymphadenopathy, hepatomegaly, splenomegaly, leukemic infiltration in the central nervous system (CNS) were also investigated. Results showed that 56.7% of the cases were B-lineage ALL and 55% were T-cell ALL. Also, we found that males were more affected by the disease, regardless of immunological classification. The correlation between age and immunological subtypes showed that the B-lineage ALL occurred more frequently in patients aged under 15while the T-cell ALL subtype was more frequent in adults. Immunophenotypic profiles and morphological subtypes showed a direct correlation between L3 subtype and B-lineage ALL, while L1 and L2 subtypes correlated more often with B-cell lineage and T-cell ALL, respectively. Correlation analysis between immunophenotypic and clinical profiles showed that T-cell ALL was more associated with a higher incidence of lymphadenopathy, hepatomegaly, splenomegaly and CNS leukemic infiltration, also showing a greater blast cell count in peripheral blood than the other subgroups. The presented data suggest that immunophenotyping is an important method in the diagnosis, monitoring and prognostic assessment in determining the pathological mechanisms of evolution of ALL.
机译:作者对来自巴西里奥格兰德州纳塔尔市的急性淋巴细胞白血病(ALL)患者进行了流式细胞术免疫表型研究。使用一组单克隆抗体新诊断出患者(n = 126):CD1a,CD2,CD3,CD4,CD7,CD8,CD10,CD13,CD33,CD14,CD19,CD22,CD79a,CD117,CD34,抗IgM ,抗TdT,抗HLA-Dr以及抗人kappa和lambda轻链。还研究了其他数据,例如患者的年龄和性别,临床和实验室检查结果,例如是否存在肿瘤块,淋巴结病,肝肿大,脾肿大,中枢神经系统(CNS)白血病浸润。结果显示,B谱系ALL占56.7%,T细胞ALL占55%。此外,我们发现,无论免疫分类如何,男性都更容易受到该疾病的影响。年龄与免疫亚型之间的相关性表明,B谱系ALL在15岁以下患者中更常见,而T细胞ALL亚型在成人中更常见。免疫表型和形态亚型显示L3亚型与B谱系ALL直接相关,而L1和L2亚型与B细胞谱系和T细胞ALL相关性更高。免疫表型与临床特征之间的相关性分析显示,T细胞ALL与淋巴结病,肝肿大,脾肿大和CNS白血病浸润的发生率更高相关,并且与其他亚组相比,外周血中的原始细胞计数更高。提出的数据表明,免疫表型是确定ALL演变的病理机制的诊断,监测和预后评估的重要方法。

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