Genetic and immunophenotypic diversity of acute leukemias in children

IF 0.2 4区 医学 Q4 MEDICINE, RESEARCH & EXPERIMENTAL
Magdalena Pierzyna-Świtała, Ł. Sędek, B. Mazur
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引用次数: 3

Abstract

Abstract Acute leukemias are the most commonly diagnosed malignancies in children. Acute leukemias constitute a heterogeneous group of cancers resulting from clonal outgrowth and accumulation of immature precursor cells of different hematologic lineages. Cancerous transformation begins with disruption of cell maturation mechanisms triggered by particular environmental or endogenic factors, including innate and acquired immunodeficiencies as well as autoimmune diseases. Research in the field of acute leukemias has revealed many possible genetic abnormalities in leukemic cells, including both structural and numerical aberrations. The former can produce some particular fusion genes, yielding fusion protein products which can have an oncogenic potential in hematopoietic cells. Some of them, including translocations resulting in fusion product formation BCR-ABL1 and different fusion products involving the KMT2A gene, are markers of adverse prognosis, whereas numerical aberrations with high hyperdiploidy and chromosome number exceeding 51 are markers of favorable prognosis. Detection of these aberrations already has a well-grounded clinical significance in acute lymphoblastic leukemia and plays an important role in patient risk stratification. The appearance of particular genetic changes often correlates with the expression of certain markers on the surface of leukemic cells. Determination of expression or lack of specific antigens, that is, immunophenotyping, is possible with the use of the flow cytometry technique. Flow cytometry is currently considered as a fast and broadly available technique which can provide clinically useful information in a relatively short time after biological specimen collection. Flow cytometry also enables appropriate classification of acute leukemias.
儿童急性白血病的遗传和免疫表型多样性
急性白血病是儿童最常见的恶性肿瘤。急性白血病是由不同血液学谱系的未成熟前体细胞克隆生长和积累引起的异质组癌症。癌变始于由特定环境或内因因素(包括先天和获得性免疫缺陷以及自身免疫性疾病)引发的细胞成熟机制的破坏。在急性白血病领域的研究已经揭示了白血病细胞中许多可能的遗传异常,包括结构和数值畸变。前者可以产生一些特定的融合基因,产生在造血细胞中具有致癌潜力的融合蛋白产物。其中一些,包括导致融合产物形成BCR-ABL1和涉及KMT2A基因的不同融合产物的易位,是不良预后的标志,而高二倍体和染色体数目超过51的数值畸变是良好预后的标志。检测这些异常在急性淋巴细胞白血病中已经具有良好的临床意义,在患者风险分层中起着重要作用。特定基因变化的出现通常与白血病细胞表面某些标记物的表达有关。使用流式细胞术技术可以测定特异性抗原的表达或缺乏,即免疫表型。流式细胞术目前被认为是一种快速和广泛可用的技术,可以在生物标本采集后相对较短的时间内提供临床有用的信息。流式细胞术还可以对急性白血病进行适当的分类。
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来源期刊
Postȩpy higieny i medycyny doświadczalnej
Postȩpy higieny i medycyny doświadczalnej MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
0.60
自引率
0.00%
发文量
50
审稿时长
4-8 weeks
期刊介绍: Advances in Hygiene and Experimental Medicine (PHMD) is a scientific journal affiliated with the Institute of Immunology and Experimental Therapy by the Polish Academy of Sciences in Wrocław. The journal publishes articles from the field of experimental medicine and related sciences, with particular emphasis on immunology, oncology, cell biology, microbiology, and genetics. The journal publishes review and original works both in Polish and English. All journal publications are available via the Open Access formula in line with the principles of the Creative Commons licence.
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