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来自不同启动子的基因表达可改善多发性骨髓瘤的预后分层。

Gene expression derived from alternative promoters improves prognostic stratification in multiple myeloma.

机构信息

Area de Oncología, Centro de Investigación Médica Aplicada (CIMA), Universidad de Navarra, IDISNA, Pamplona, Spain.

Tecnun School of Engineering, Universidad de Navarra, San Sebastian, Spain.

出版信息

Leukemia. 2021 Oct;35(10):3012-3016. doi: 10.1038/s41375-021-01263-9. Epub 2021 May 10.

Abstract

Clinical and genetic risk factors are currently used in multiple myeloma (MM) to stratify patients and to design specific therapies. However, these systems do not capture the heterogeneity of the disease supporting the development of new prognostic factors. In this study, we identified active promoters and alternative active promoters in 6 different B cell subpopulations, including bone-marrow plasma cells, and 32 MM patient samples, using RNA-seq data. We find that expression initiated at both regular and alternative promoters was specific of each B cell subpopulation or MM plasma cells, showing a remarkable level of consistency with chromatin-based promoter definition. Interestingly, using 595 MM patient samples from the CoMMpass dataset, we observed that the expression derived from some alternative promoters was associated with lower progression-free and overall survival in MM patients independently of genetic alterations. Altogether, our results define cancer-specific alternative active promoters as new transcriptomic features that can provide a new avenue for prognostic stratification possibilities in patients with MM.

摘要

目前,临床和遗传风险因素被用于多发性骨髓瘤(MM),以对患者进行分层并设计特定的治疗方法。然而,这些系统并不能捕捉到疾病的异质性,这支持了新的预后因素的发展。在这项研究中,我们使用 RNA-seq 数据在 6 种不同的 B 细胞亚群(包括骨髓浆细胞)和 32 个 MM 患者样本中鉴定了活性启动子和替代活性启动子。我们发现,在常规和替代启动子处起始的表达是每种 B 细胞亚群或 MM 浆细胞所特有的,与基于染色质的启动子定义具有显著的一致性。有趣的是,使用来自 CoMMpass 数据集的 595 个 MM 患者样本,我们观察到,一些替代启动子的表达与 MM 患者的无进展生存期和总生存期降低独立相关,而与遗传改变无关。总的来说,我们的结果将癌症特异性替代活性启动子定义为新的转录组特征,可为 MM 患者的预后分层提供新的途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cabe/8478642/3f634c9d3628/41375_2021_1263_Fig1_HTML.jpg

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