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Clusterization in acute myeloid leukemia based on prognostic alternative splicing signature to reveal the clinical characteristics in the bone marrow microenvironment

机译:基于预后替代剪接特征的急性髓性白血病聚类,揭示骨髓微环境中的临床特征

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Alternative splicing (AS), a crucial post-transcriptional regulatory mechanism in expanding the coding capacities of genomes and increasing the diversity of proteins, still faces various challenges in the splicing regulation mechanism of acute myeloid leukemia (AML) and microenvironmental changes. A total of 27,833 AS events were detected in 8337 genes in 178 AML patients, with exon skip being the predominant type. Approximately 11% of the AS events were significantly related to prognosis, and the prediction models based on various events demonstrated high classification efficiencies. Splicing factors correlation networks further altered the diversity of AS events through epigenetic regulation and clarified the potential mechanism of the splicing pathway. Unsupervised cluster analysis revealed significant correlations between AS and immune features, molecular mutations, immune checkpoints and clinical outcome. The results suggested that AS clusters could be used to identify patient subgroups with different survival outcomes in AML, among which C1 was both associated with good outcome in overall survival. Interestingly, C1 was associated with lower immune scores compared with C2 and C3, and favorable-risk cytogenetics was rarely distributed in C2, but much more common in C1. This study revealed a comprehensive landscape of AS events, and provides new insight into molecular targeted therapy and immunotherapy strategy for AML.
机译:替代剪接(AS),在扩大基因组的编码能力和增加蛋白质多样性的关键后调节调节机制,仍然面临着急性髓性白血病(AML)和微环境变化的剪接调控机制中的各种挑战。在178例AML患者的8337个基因中检测到总共27,833个作为事件,外显子跳过是主要类型。作为事件的约11%与预后显着相关,基于各种事件的预测模型表现出高分类效率。拼接因子相关网络通过表观遗传调节进一步改变了作为事件的多样性,并阐明了剪接途径的潜在机制。无监督的聚类分析揭示了免疫特征,分子突变,免疫检查点和临床结果之间的显着相关性。结果表明,由于簇可用于鉴定具有不同生存结果的患者亚组,其中C1均与整体存活的良好结果相关。有趣的是,与C2和C3相比,C1与降低的免疫分数相关,并且很少分布在C2中,但在C1中更常见。本研究揭示了作为事件的综合景观,并为AML的分子靶向治疗和免疫疗法策略提供了新的洞察力。

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