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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Role of additional chromosomal changes in the prognostic value of t(4;14) and del(17p) in multiple myeloma: the IFM experience
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Role of additional chromosomal changes in the prognostic value of t(4;14) and del(17p) in multiple myeloma: the IFM experience

机译:额外的染色体变化在多发性骨髓瘤中t(4; 14)和del(17p)的预后价值中的作用:IFM经验

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摘要

In multiple myeloma, cytogenetic changes are important predictors of patient outcome. In this setting, the most important changes are deletion 17p, del(17p), and translocation of chromosomes 4 and 14, t(4; 14), conferring a poor outcome. However, a certain degree of heterogeneity is observed in the survival of these high-risk patients. We hypothesized that other chromosomal changes may impact the outcome. We retrospectively analyzed a large series of 242 patients displaying either t(4; 14) (157 patients) or del(17p) (110 patients), 25 patients presenting both abnormalities, using single nucleotide polymorphism array. In patients with t(4; 14), del(1p32), del22q, and >30 chromosomal structural changes negatively impacted progression-free survival (PFS). For overall survival (OS), del(13q14), del(1p32), and the number of chromosomal structural changes worsened the prognosis of patients. For patients with del(17p), del6q worsened the prognosis of patients, whereas trisomy 15 and monosomy 14 were found to have a protective effect on PFS. For OS, del(1p32) worsened the prognosis of patients, whereas having >8 numerical changes was found to have a protective effect on survival. This study, which is the largest series of high-risk patients analyzed with the most modern genomic technique, identified 1 main factor negatively impacting survival: del(1p32).
机译:在多发性骨髓瘤中,细胞遗传学改变是患者预后的重要预测指标。在这种情况下,最重要的变化是删除17p,del(17p)以及染色体4和14,t(4; 14)的易位,从而导致不良结果。但是,在这些高危患者的生存中观察到一定程度的异质性。我们假设其他染色体变化可能会影响结果。我们使用单核苷酸多态性阵列回顾性分析了242例显示t(4; 14)(157例)或del(17p)(110例)的大系列患者,其中25例同时出现这两种异常。在t(4; 14)患者中,del(1p32),del22q和> 30的染色体结构变化会对无进展生存期(PFS)产生负面影响。对于总生存期(OS),del(13q14),del(1p32)和染色体结构变化的数量使患者的预后恶化。对于del(17p)患者,del6q恶化了患者的预后,而三体性15和单性性14对PFS具有保护作用。对于OS,del(1p32)使患者的预后恶化,而数值变化> 8则对生存率有保护作用。这项研究是使用最现代的基因组技术分析的最大系列的高危患者,发现了1个对存活率产生不利影响的主要因素:del(1p32)。

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