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用于评估急性巨核细胞白血病微小/可测量残留病的免疫表型标志物。

Immunophenotypic markers for the evaluation of minimal/measurable residual disease in acute megakaryoblastic leukemia.

作者信息

Pinto Carina Maria, Bertolucci Camila Marques, Severino Alef Rafael, Dos Santos Tosi Juliana Fernanda, Ikoma-Colturato Maura R V

机构信息

Hospital Amaral Carvalho, Jau, São Paulo, Brazil.

Hospital Amaral Carvalho, Jau, São Paulo, Brazil; Sabin Medicina Diagnóstica, Brasilia, DF, Brazil.

出版信息

Hematol Transfus Cell Ther. 2024 Oct-Dec;46(4):542-548. doi: 10.1016/j.htct.2023.09.2364. Epub 2023 Nov 17.

DOI:10.1016/j.htct.2023.09.2364
PMID:38008596
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11451363/
Abstract

Acute megakaryoblastic leukemia is characterized by heterogeneous biology and clinical behavior. Immunophenotypic characteristics include the expression of megakaryocytic differentiation markers (e.g. CD41, CD42a, CD42b, CD61) associated with immaturity markers (CD34, CD117, HLA-DR) and myeloid markers (e.g. CD13, CD33) and even with lymphoid cross-lineage markers (e.g. CD7, CD56). Although the diagnostic immunophenotype has already been well described, given the rarity of the disease, its immunophenotypic heterogeneity and post-therapeutic instability, there is no consensus on the combination of monoclonal markers to detect minimal/measurable residual disease (MRD). Currently, MRD is an important tool for assessing treatment efficacy and prognostic risk. In this study, we evaluated the immunophenotypic profile of MRD in a retrospective cohort of patients diagnosed with acute megakaryoblastic leukemia, to identify which markers, positive or negative, were more stable after treatment and which could be useful for MRD evaluation. The expression profile of each marker was evaluated in sequential MRD samples. In conclusion, the markers evaluated in this study can be combined in an MRD immunophenotypic panel to investigate for megakaryoblastic leukemia. Although this study is retrospective and some data are missing, the information obtained may contribute to prospective studies to validate more specific strategies in the detection of MRD in acute megakaryoblastic leukemia.

摘要

急性巨核细胞白血病具有生物学特性和临床行为的异质性。免疫表型特征包括巨核细胞分化标志物(如CD41、CD42a、CD42b、CD61)的表达,这些标志物与不成熟标志物(CD34、CD117、HLA-DR)、髓系标志物(如CD13、CD33)甚至淋巴系跨谱系标志物(如CD7、CD56)相关。尽管诊断性免疫表型已得到充分描述,但鉴于该疾病的罕见性、其免疫表型的异质性以及治疗后的不稳定性,对于检测微小/可测量残留病(MRD)的单克隆标志物组合尚无共识。目前,MRD是评估治疗疗效和预后风险的重要工具。在本研究中,我们评估了一组诊断为急性巨核细胞白血病患者的回顾性队列中MRD的免疫表型特征,以确定哪些标志物(阳性或阴性)在治疗后更稳定,以及哪些标志物可用于MRD评估。在连续的MRD样本中评估每个标志物的表达谱。总之,本研究中评估的标志物可组合成一个MRD免疫表型 panel,用于调查巨核细胞白血病。尽管本研究是回顾性的且一些数据缺失,但所获得的信息可能有助于前瞻性研究,以验证在急性巨核细胞白血病中检测MRD的更具体策略。