PROFILE OF CD150 EXPRESSION IN BONE MARROW CELLS OF PATIENTS WITH ACUTE MYELOID LEUKEMIA.

Q3 Medicine

Experimental oncology Pub Date : 2022-11-01 DOI:10.32471/exp-oncology.2312-8852.vol-44-no-3.18307

L Shlapatska, I Gordiienko, A Polishchuk, D Gluzman

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引用次数: 1

Abstract

Background: Acute myeloid leukemia (AML) is a highly heterogeneous disease accompanied by the arrest of myeloid cell lineage differenti-ation due to accumulation of genetic abnormalities and clonal proliferation of myeloid blasts. Finding the differentially expressed molecules and studying their function within AML subgroups may help to improve diagnosis and prognosis with the aim of developing selected therapies for AML subsets. The aim of this study was to reveal the profile of CD150 cell surface expression on bone marrow (BM) cells of AML patients.

Materials and methods: The study was performed on samples of BM aspirates from 55 patients with primarily diagnosed AML. Flow cytometry analysis was applied for the evaluation of immunophenotype profile and CD150 cell surface expression on BM cells from AML patients.

Results: Four AML subtypes (M1, M2, M3 and M5) were identified. The CD150 expression was found in 14 (25.5%) cases predominantly of AML M3 subtype. CD150 expression was detected on 43.2-83.8% of leukemia cells in AML M3. The frequency of CD150 positive cases of non-M3 AML subtypes was low: all AML M1 cases were CD150-negative, while only 1 (10.0%) of 10 patients with AML M2 and 6 (19.4%) of 31 patients with AML M5 were CD150 positive. The median percentage of CD150 positive leukemia cells and the index of mean fluorescence intensity in AML M3 cases were significantly higher than in non-M3 AML cases (p < 0.05). The CD150 expression was significantly associated with CD11c, CD11b, CD14, CD34, CD36, CD56 and HLA-DR negative expression and CD33, CD38, CD117 positive expression among the examined cohort of patients with AML M3.

Conclusions: High level of CD150 expression is a unique feature of AML M3 subtype and may serve as additional phenotype marker for the identification of blast cells with impaired maturation at the promyelocyte stage and the development of AML M3. At the same time, the revealed negative association of CD150 expression with poor prognostic factor CD56 in AML M3 subtype also allows us to suggest potential prognostic value of CD150 examination in AML patients.

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cd150在急性髓性白血病患者骨髓细胞中的表达谱

背景:急性髓系白血病(AML)是一种高度异质性的疾病，由于遗传异常的积累和髓系细胞的克隆增殖，髓系细胞谱系分化受阻。发现AML亚群中的差异表达分子并研究其功能可能有助于改善诊断和预后，目的是开发针对AML亚群的选择性治疗方法。本研究的目的是揭示AML患者骨髓(BM)细胞上CD150细胞表面表达的谱。材料和方法:研究对象为55例初诊AML患者的骨髓抽吸样本。应用流式细胞术分析评价AML患者骨髓细胞的免疫表型谱和CD150细胞表面表达。结果:鉴定出4种AML亚型(M1、M2、M3和M5)。CD150在14例(25.5%)AML M3亚型中表达。在AML M3中，43.2-83.8%的白血病细胞中检测到CD150的表达。非m3型AML亚型CD150阳性的频率较低，所有M1型AML均为CD150阴性，而10例M2型AML中CD150阳性的仅有1例(10.0%)，31例M5型AML中CD150阳性的仅有6例(19.4%)。AML M3组CD150阳性白血病细胞中位数百分比和平均荧光强度指数均显著高于非M3组(p < 0.05)。在检查的AML M3患者队列中，CD150表达与CD11c、CD11b、CD14、CD34、CD36、CD56和HLA-DR阴性表达以及CD33、CD38、CD117阳性表达显著相关。结论:高水平的CD150表达是AML M3亚型的独特特征，可能作为鉴别早幼粒细胞阶段成熟受损的母细胞和AML M3发展的额外表型标记。同时，在AML M3亚型中CD150表达与不良预后因子CD56呈负相关，这也使我们提出CD150检测在AML患者中的潜在预后价值。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Experimental oncology Medicine-Oncology

CiteScore

1.40

自引率

0.00%

发文量

期刊介绍： The Experimental Oncology is an English-language journal that publishes review articles, original contributions, short communications, case reports and technical advances presenting new data in the field of experimental and fundamental oncology. Manuscripts should be written in English, contain original work, which has not been published or submitted for publication elsewhere. It also implies the transfer of the Copyright from the author to “Experimental Oncology”. No part of journal publications may be reproduced, stored in a retrieval system or transmitted in any form or by any means without the prior permission of the publisher.