BCP-ALL中与IKZF1plus相关的细胞标记的特征。

IF 5 2区 医学 Q2 Medicine
Caroline Barbieri Blunck , Caroline Pires Poubel , Bruno A. Lopes , Thayana C. Barbosa , Ana Luiza Tardem Maciel , Elaine Sobral da Costa , Ariadne da Rocha Figueiredo , Marcelo G.P. Land , Márcia Trindade Schramm , Maura Rosane Valério Ikoma-Coltutato , Renan Garcia Gomes , Mecneide Mendes Lins , Thais Ferraz Aguiar , Marcela Braga Mansur , Mariana Emerenciano
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引用次数: 0

摘要

IKZF1缺失与B细胞前体急性淋巴细胞白血病(BCP-ALL)复发率升高有关。IKZF1del病例中有一个特殊的亚组,称为IKZF1plus(定义为同时出现IKZF1del和CDKN2A/B、PAX5或PAR1区域缺失,但无ERG缺失),该亚组也与预后较差有关,但最近的一些研究并未发现IKZF1del组和IKZF1plus组之间存在重大差异。因此,IKZF1plus 组仍需进一步了解,我们的研究旨在描述其分子异质性,并确定与 IKZF1plus 独家相关的分子标记物。我们对两个独立的病例系列(TARGET,n = 125;GenLAb,n = 60)进行了评估,将患者分为 3 组:IKZF1plus、IKZF1del 和 IKZF1wild。差异表达分析表明,与 IKZF1plus 组最相关的膜蛋白编码基因是KCNA5、GREB1、EPOR、SDK1 和 PTPRB。值得注意的是,KCNA5 和 GREB1 的差异表达水平在 GenLAb 验证系列中得到了验证。在拷贝数改变方面,我们在 IKZF1plus 组中观察到高频率的 VPREB1 基因缺失,以及 CD200 和 BTLA 基因的独家缺失。最近的研究表明,IKZF1plus 特征的重要性因基因亚组而异。在这种情况下,我们发现IKZF1plus与BCP-ALL中的某些基因存在关联,其中KCNA5和GREB1是最有希望预测IKZF1plus的生物标志物。深入了解这些遗传特征将有助于更好地进行风险评估,并为 BCP-ALL 的治疗策略提供准确的依据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Characterisation of cells markers associated with IKZF1plus in BCP-ALL
The presence of IKZF1 deletions has been associated with an increased relapse rate in B-cell precursor acute lymphoblastic leukaemia (BCP-ALL). There is a particular subset of IKZF1del cases called IKZF1plus (defined by the co-occurrence of IKZF1del and deletions in CDKN2A/B, PAX5, or the PAR1 region, in the absence of ERG deletions), which is also associated with worse prognosis, but some recent studies have not found major differences between the IKZF1del and IKZF1plus groups. Therefore, the IKZF1plus group still needs further comprehension and our study aims to characterise the molecular heterogeneity and identify molecular markers exclusively associated with IKZF1plus. Two independent series of cases (TARGET, n = 125 and GenLAb, n = 60) were evaluated by segregating patients into 3 groups: IKZF1plus, IKZF1del, and IKZF1wild. Differential expression analyses showed that the membrane protein-coding genes most associated with the IKZF1plus group were: KCNA5, GREB1, EPOR, SDK1, and PTPRB. Notably, KCNA5 and GREB1 differential expression levels were validated in the GenLAb validation series. Regarding copy number alterations, we observed a high frequency of VPREB1 deletions in the IKZF1plus group, as well as additional exclusive deletions in the CD200 and BTLA genes. Recent research suggests that the importance of the IKZF1plus profile varies depending on the genetic subgroup. In this scenario, we found associations between IKZF1plus and certain genes in BCP-ALL, being KCNA5 and GREB1 the most promising biomarkers for predicting IKZF1plus. A deeper understanding of these genetic profiles will allow a better risk assessment and offer precise rationale for therapeutic strategies in BCP-ALL.
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来源期刊
CiteScore
8.40
自引率
2.00%
发文量
314
审稿时长
54 days
期刊介绍: Translational Oncology publishes the results of novel research investigations which bridge the laboratory and clinical settings including risk assessment, cellular and molecular characterization, prevention, detection, diagnosis and treatment of human cancers with the overall goal of improving the clinical care of oncology patients. Translational Oncology will publish laboratory studies of novel therapeutic interventions as well as clinical trials which evaluate new treatment paradigms for cancer. Peer reviewed manuscript types include Original Reports, Reviews and Editorials.
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