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首页> 外文期刊>Haematologica >Long non-coding RNA expression profile in cytogenetically normal acute myeloid leukemia identifies a distinct signature and a new biomarker in NPM1-mutated patients
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Long non-coding RNA expression profile in cytogenetically normal acute myeloid leukemia identifies a distinct signature and a new biomarker in NPM1-mutated patients

机译:在细胞遗传学上正常的急性髓性白血病中长的非编码RNA表达谱在NPM1突变的患者中发现了独特的特征和新的生物标志物

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Long non-coding RNAs are defined as transcripts larger than 200 nucleotides but without protein-coding potential. There is growing evidence of the important role of long non-coding RNAs in cancer initiation, development and progression. In this study, we sought to evaluate the long non-coding RNA expression profile of patients with cytogenetically normal acute myeloid leukemia (AML). RNA-sequencing of 40 cytogenetically normal AML patients allowed us to quantify 11,036 long non-coding RNAs. Among these, more than 8000 were previously undescribed long non-coding RNAs. Using unsupervised analysis, we observed a specific long non-coding RNA expression profile dependent on the mutational status of the NPM1 gene. Statistical analysis allowed us to identify a minimal set of 12 long non-coding RNAs capable of discriminating NPM1 -mutated from NPM1 -wild-type patients. These results were validated by qRT-PCR on an independent cohort composed of 134 cytogenetically normal AML patients. Furthermore, we have identified one putative biomarker, the long non-coding RNA XLOC_109948 whose expression pattern predicts clinical outcome. Interestingly, low XLOC_109948 expression indicates a good prognosis especially for NPM1 -mutated patients. Transient transfection of GapmeR against XLOC_109948 in NPM1 -mutated OCI-AML3 cell line treated with Ara-C or ATRA enhances apoptosis suggesting XLOC_109948 plays a role in drug sensitivity. This study improves our knowledge of the long non-coding RNA transcriptome in cytogenetically normal AML patients. We observed a distinct long non-coding RNA expression profile in patients with the NPM1 mutation. The newly identified XLOC_109948 long non-coding RNA emerged as a strong prognostic factor able to better stratify NPM1-mutated patients.
机译:长的非编码RNA被定义为大于200个核苷酸但没有蛋白编码潜能的转录物。越来越多的证据表明,长的非编码RNA在癌症的发生,发展和进展中起着重要的作用。在这项研究中,我们试图评估细胞遗传学正常的急性髓细胞性白血病(AML)患者的长期非编码RNA表达谱。 40位细胞遗传学正常的AML患者的RNA测序使我们能够量化11,036个长的非编码RNA。其中,超过8000个先前未描述的长非编码RNA。使用无监督分析,我们观察到了特定的长非编码RNA表达谱,这取决于NPM1基因的突变状态。统计分析使我们能够鉴定最少12组能够区分NPM1-突变型和NPM1-野生型患者的长非编码RNA。这些结果通过qRT-PCR在由134个细胞遗传学正常AML患者组成的独立队列中得到验证。此外,我们已经鉴定出一种推定的生物标记物,即长的非编码RNA XLOC_109948,其表达模式可预测临床结果。有趣的是,低XLOC_109948表达表明预后良好,尤其是对于NPM1突变的患者。在Ara-C或ATRA处理的NPM1突变的OCI-AML3细胞系中,针对XLOC_109948的GapmeR瞬时转染可增强细胞凋亡,提示XLOC_109948在药物敏感性中起作用。这项研究提高了我们对细胞遗传学正常AML患者中较长的非编码RNA转录组的了解。我们观察到具有NPM1突变的患者中独特的长非编码RNA表达谱。新近鉴定出的XLOC_109948长非编码RNA作为能够更好地对NPM1突变患者进行分层的强大预后因素而出现。

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