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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Evidence of an epigenetic origin for high-risk 1q21 copy number aberrations in multiple myeloma
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Evidence of an epigenetic origin for high-risk 1q21 copy number aberrations in multiple myeloma

机译:多发性骨髓瘤中高风险1q21拷贝数异常的表观遗传起源的证据

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Multiple myeloma is a B-cell malignancy stratified in part by cytogenetic abnormalities, including the high-risk copy number aberrations (CNAs) of 11q21 and 17p(-). To investigate the relationship between 1q21 CNAs and DNA hypomethylation of the 1q12 pericentromeric heterochromatin, we treated in vitro peripheral blood cultures of 5 patients with balanced constitutional rearrangements of 1q12 and 5 controls with the hypomethylating agent 5-azacytidine. Using G-banding, fluorescence in situ hybridization, and spectral karyotyping, we identified structural aberrations and copy number gains of 1q21 in the treated cells similar to those found in patients with cytogenetically defined high-risk disease. Aberrations included 1q12 triradials, amplifications of regions juxtaposed to 1q12, and jumping translocations 1q12. Strikingly, all 5 patients with constitutional 1q12 rearrangements showed amplifications on the derivative chromosomes distal to the inverted or translocated 1q12 region, including MYCNin 1 case. At the same time, no amplification of the 1q21 region was found when the 1q12 region was inverted or absent. These findings provide evidence that the hypomethylation of the 1q12 region can potentially amplify any genomic region juxtaposed to it and mimic CNAs found in the bone marrow of patients with high-risk disease.
机译:多发性骨髓瘤是一种B细胞恶性肿瘤,部分由细胞遗传学异常分层,包括11q21和17p(-)的高风险拷贝数畸变(CNA)。为了研究1q21 CNA与1q12着丝粒异染色质的DNA甲基化不足之间的关系,我们用亚甲基化剂5-氮胞苷处理了5例平衡组成为1q12的患者和5例对照的体外血液培养。使用G带,荧光原位杂交和光谱核型分析,我们确定了与细胞遗传学定义的高危疾病患者相似的被处理细胞中1q21的结构畸变和拷贝数增加。像差包括1q12三向辐射,与1q12并置的区域的放大以及1q12的跳跃易位。引人注目的是,所有5名具有1q12结构重排的患者均显示了位于倒置或易位1q12区远端的衍生染色体上的扩增,包括MYCNin 1例。同时,当1q12区域倒置或不存在时,未发现1q21区域的扩增。这些发现提供了证据,即1q12区域的甲基化不足可能会放大与其并列的任何基因组区域,并模仿高危疾病患者的骨髓中发现的CNA。

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