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Reconstruction of pathway modification induced by nicotinamide using multi-omic network analyses in triple negative breast cancer

机译:应用多组网分析技术重建烟酰胺诱导的途径修饰在三阴性乳腺癌中的应用

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摘要

Triple negative breast cancer (TNBC) is characterized by an aggressive biological behavior in the absence of a specific target agent. Nicotinamide has recently been proven to be a novel therapeutic agent for skin tumors in an ONTRAC trial. We performed combinatory transcriptomic and in-depth proteomic analyses to characterize the network of molecular interactions in TNBC cells treated with nicotinamide. The multi-omic profiles revealed that nicotinamide drives significant functional alterations related to major cellular pathways, including the cell cycle, DNA replication, apoptosis and DNA damage repair. We further elaborated the global interaction networks of molecular events via nicotinamide-inducible expression changes at the mRNA and functional protein levels. This approach indicated that nicotinamide treatment rewires interaction networks toward dysfunction in DNA damage repair and away from a pro-growth state in TNBC. To our knowledge, the high-resolution network interactions identified in the present study provide the first evidence to comprehensively support the hypothesis of nicotinamide as a novel therapeutic agent in TNBC.
机译:三阴性乳腺癌(TNBC)的特征是在没有特定目标药物的情况下具有侵略性的生物学行为。最近,在ONTRAC试验中,烟酰胺已被证明是一种针对皮肤肿瘤的新型治疗剂。我们进行了组合转录组和深度蛋白质组学分析,以表征烟酰胺处理的TNBC细胞中分子相互作用的网络。多组学概况表明,烟酰胺驱动与主要细胞途径有关的重大功能改变,包括细胞周期,DNA复制,细胞凋亡和DNA损伤修复。我们通过在mRNA和功能蛋白水平上通过烟酰胺诱导的表达变化进一步阐述了分子事件的全球相互作用网络。这种方法表明烟酰胺治疗使相互作用网络重新导向DNA损伤修复中的功能障碍,并远离TNBC中的促生长状态。据我们所知,本研究中确定的高分辨率网络相互作用为全面支持烟酰胺作为TNBC中新型治疗剂的假设提供了第一个证据。

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