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白藜芦醇对食管腺癌细胞信号通路的阻断揭示了分子和免疫调节特征。

Interception of Signaling Circuits of Esophageal Adenocarcinoma Cells by Resveratrol Reveals Molecular and Immunomodulatory Signatures.

作者信息

Dhir Hardika, Choudhury Monica, Patil Ketki, Cheung Candice, Bodlak Adriana, Pardo Danny, Adams Asana, Travaglino Stefano, Rojas Jose Araque, Pai S Balakrishna

机构信息

Wallace H. Coulter Department of Biomedical Engineering, Georgia Institute of Technology and Emory University, 313 Ferst Drive, Atlanta, GA 30332, USA.

出版信息

Cancers (Basel). 2021 Nov 19;13(22):5811. doi: 10.3390/cancers13225811.

Abstract

Deregulation of signaling pathways due to mutations sets the cell on a path to neoplasia. Therefore, recent reports of increased mutations observed in esophageal tissue reflects the enhanced risk of tumor formation. In fact, adenocarcinoma of the esophagus has been on the rise lately. Increase in mortality due to a paucity of efficacious drugs for this cancer prompted us to discover molecular signatures to combat this malady. To this end, we chose resveratrol-a polyphenol with anticancer property-and studied its impact on three esophageal adenocarcinoma cell lines (OE33, OE19 and FLO-1) by multilevel profiling. Here, we show the impact of resveratrol on the viability of the three adenocarcinoma esophageal cell systems studied, at the cellular level. Furthermore, an analysis at the molecular level revealed that the action was through the programmed cell death pathway, resulting in an increase in apoptotic and caspase-positive cells. The impact on reactive oxygen species (ROS) and a decrease in Bcl2 levels were also observed. Moreover, proteomic profiling highlighted pivotal differentially regulated signaling molecules. The phenotypic effect observed in resveratrol-treated esophageal cells could be due to the stoichiometry per se of the fold changes observed in entities of key signaling pathways. Notably, the downregulation of Ku80 and other pivotal entities by resveratrol could be harnessed for chemo-radiation therapy to prevent DNA break repair after radiation therapy. Additionally, multilevel profiling has shed light on molecular and immune-modulatory signatures with implications for discovering novel treatments, including chemo-immunotherapy, for esophageal adenocarcinomas which are known to be aggressive cancers.

摘要

由于突变导致的信号通路失调使细胞走上了肿瘤形成的道路。因此,最近在食管组织中观察到的突变增加的报告反映了肿瘤形成风险的增加。事实上,食管腺癌的发病率最近一直在上升。由于针对这种癌症的有效药物匮乏导致死亡率上升,促使我们去发现对抗这种疾病的分子特征。为此,我们选择了具有抗癌特性的多酚白藜芦醇,并通过多层次分析研究了它对三种食管腺癌细胞系(OE33、OE19和FLO-1)的影响。在这里,我们展示了白藜芦醇在细胞水平上对所研究的三种食管腺癌细胞系统活力的影响。此外,分子水平的分析表明,其作用是通过程序性细胞死亡途径,导致凋亡细胞和半胱天冬酶阳性细胞增加。还观察到了对活性氧(ROS)的影响以及Bcl2水平的降低。此外,蛋白质组学分析突出了关键的差异调节信号分子。在白藜芦醇处理的食管细胞中观察到的表型效应可能归因于关键信号通路实体中观察到的倍数变化的化学计量本身。值得注意 的是,白藜芦醇对Ku80和其他关键实体的下调可用于化学放射治疗,以防止放射治疗后DNA断裂修复。此外,多层次分析揭示了分子和免疫调节特征,这对于发现包括化学免疫疗法在内的针对已知具有侵袭性的食管腺癌的新治疗方法具有启示意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c4e/8616317/a6c97833a4c2/cancers-13-05811-g001.jpg

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