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A 4-lncRNA scoring system for prognostication of adult myelodysplastic syndromes

机译:用于成人骨髓增生异常综合症预后的4-lncRNA评分系统

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摘要

Long noncoding RNAs (lncRNAs) not only participate in normal hematopoiesis but also contribute to the pathogenesis of acute leukemia. However, their clinical and prognostic relevance in myelodysplastic syndromes (MDSs) remains unclear to date. In this study, we profiled lncRNA expressions in 176 adult patients with primary MDS, and identified 4 lncRNAs whose expression levels were significantly associated with overall survival (OS). We then constructed a risk-scoring system with the weighted sum of these 4 lncRNAs. Higher lncRNA scores were associated with higher marrow blast percentages, higher-risk subtypes of MDSs (based on both the Revised International Prognostic Scoring System [IPSS-R] and World Health Organization classification), complex cytogenetic changes, and mutations in RUNX1, ASXL1, TP53, SRSF2, and ZRSR2, whereas they were inversely correlated with SF3B1 mutation. Patients with higher lncRNA scores had a significantly shorter OS and a higher 5-year leukemic transformation rate compared with those with lower scores. The prognostic significance of our 4-lncRNA risk score could be validated in an independent MDS cohort. In multivariate analysis, higher lncRNA scores remained an independent unfavorable risk factor for OS (relative risk, 4.783; P < .001) irrespective of age, cytogenetics, IPSS-R, and gene mutations. To our knowledge, this is the first report to provide a lncRNA platform for risk stratification of MDS patients. In conclusion, our integrated 4-lncRNA risk-scoring system is correlated with distinctive clinical and biological features in MDS patients, and serves as an independent prognostic factor for survival and leukemic transformation. This concise yet powerful lncRNA-based scoring system holds the potential to improve the current risk stratification of MDS patients.
机译:长的非编码RNA(lncRNA)不仅参与正常的造血作用,而且还参与了急性白血病的发病机制。然而,迄今为止,它们在骨髓增生异常综合症(MDS)中的临床和预后相关性仍不清楚。在这项研究中,我们分析了176名成年MDS成人患者的lncRNA表达,并鉴定了4种lncRNA,其表达水平与总体生存率(OS)显着相关。然后,我们使用这4个lncRNA的加权总和构建了风险评分系统。较高的lncRNA分数与较高的骨髓胚细胞百分比,较高的MDS亚型(基于修订的国际预后评分系统[IPSS-R]和世界卫生组织的分类),复杂的细胞遗传学变化以及RUNX1,ASXL1, TP53,SRSF2和ZRSR2与SF3B1突变呈负相关。与分数较低的患者相比,lncRNA分数较高的患者的OS显着缩短,且5年白血病转化率较高。我们的4-lncRNA风险评分的预后意义可以在独立的MDS队列中进行验证。在多变量分析中,无论年龄,细胞遗传学,IPSS-R和基因突变如何,较高的lncRNA得分仍然是OS的独立不利因素(相对风险,4.783; P <.001)。据我们所知,这是第一个为MDS患者的风险分层提供lncRNA平台的报告。总之,我们集成的4-lncRNA风险评分系统与MDS患者独特的临床和生物学特征相关,可作为生存和白血病转化的独立预后因素。这种简洁而强大的基于lncRNA的评分系统具有改善MDS患者当前风险分层的潜力。

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