髓系肿瘤伴t(2;3)(p13-25;q25-29)的细胞遗传学特征:60例分析

Alexis V Dowiak, Carlos A Tirado
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引用次数: 0

摘要

涉及2号染色体短臂(p13-25)和3号染色体长臂远端(q25-29)的染色体易位是罕见的,迄今为止研究仍然很少。这些异常在髓系肿瘤中很常见,且预后较差。在相关条带范围内的染色体异常可能导致涉及EVI1基因的融合基因的异位表达或形成,但EVI1影响白血病发生的确切机制尚不清楚。在此,我们报告了60例来自Mitelman癌症染色体畸变和基因融合数据库的具有t(2;3)(p13-25;q25-29)的各种髓系恶性肿瘤患者的分析。在这些研究中,这种易位被报道为唯一的异常或在复杂核型的背景下。在进行分子细胞遗传学分析以评估EVI1(亲生态病毒整合位点1质子同源物)位点参与的分析中(n=19), 16(84%)证实其重排。在37%的研究中,t(2;3)被视为唯一的异常(n=22)。在11%的病例(n=4)中,t(2;3)是继发性的,在63%的病例中,t(2;3)有额外的染色体异常(n=38)。7号单体、5q臂缺失和易位(9;22)是最常见的异常,发生率分别为29% (n=11)、26% (n=10)和13% (n=5)。t(2;3)是一种没有其他分子特征的异常,这些在文献结果中的观察结果增加了对这种易位在髓系疾病,特别是急性髓系白血病(AML)中的近似发生率的讨论。这些数据突出了它的非随机性,并表明它是髓系疾病谱系的一部分。考虑到与这种易位相关的严重临床结果,该数据提供了关于细胞遗传学生物标志物的信息,以及对这组染色体异常在髓系疾病发展中的意义的理解。
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Cytogenetic Characterization of Myeloid Neoplasms with t(2;3)(p13-25;q25-29): An Analysis of 60 Cases.

Chromosomal translocations involving the short arm of chromosome 2 (p13-25) and the distal part of the long arm of chromosome 3 (q25-29) are rare and still poorly studied to date. These abnormalities are common in myeloid neoplasms and are associated with a poor prognosis. Chromosomal abnormalities within the involved range of bands may contribute to the ectopic expression or formation of fusion genes involving the EVI1 gene, but the exact mechanism by which EVI1 affects leukemogenesis remains unclear. Herein, we report an analysis of 60 patient cases presenting various myeloid malignancies with t(2;3)(p13-25;q25-29) compiled from the Mitelman Database of Chromosome Aberrations and Gene Fusions in Cancer. In these studies, this translocation has been reported as a sole abnormality or within the context of a complex karyotype. Among the analysis in which molecular cytogenetic analysis was performed in order to assess the involvement of the EVI1 (ecotropic virus integration site 1 proton homolog) locus (n=19), 16 (84%) confirmed its rearrangement. In 37% of studies, the t(2;3) was seen as a sole abnormality (n=22). The t(2;3) was secondary in 11% of cases (n=4), and in 63% of the cases the t(2;3) had additional chromosomal abnormalities (n=38). Monosomy 7, deletion of the 5q arm, and translocations involving (9;22) were most common abnormalities in order of prevalence, occurring in 29% (n=11), 26% (n=10), and 13% (n=5) of case studies, respectively. These observations in the results of the literature on t(2;3), an anomaly not otherwise molecularly characterized, adds to the discussion of this translocation's approximate incidence in myeloid disease, and specifically in acute myeloid leukemia (AML). The data highlights its nonrandom nature and suggests that it is a part of the myeloid spectrum of disorders. Considering the severe clinical outcome associated with this translocation, this data provides information about a cytogenetic biomarker as well as an understanding of the significance of this set of chromosomal anomalies in the development of myeloid disease.

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