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结直肠癌的代谢相关分子分类

Metabolism-Associated Molecular Classification of Colorectal Cancer.

作者信息

Zhang Meng, Wang Hai-Zhou, Peng Ru-Yi, Xu Fei, Wang Fan, Zhao Qiu

机构信息

Department of Gastroenterology, Zhongnan Hospital of Wuhan University, Wuhan, China.

Hubei Clinical Center & Key Lab of Intestinal & Colorectal Diseases, Wuhan University, Wuhan, China.

出版信息

Front Oncol. 2020 Dec 4;10:602498. doi: 10.3389/fonc.2020.602498. eCollection 2020.

Abstract

The high heterogeneity of colorectal cancer (CRC) is the main clinical challenge for individualized therapies. Molecular classification will contribute to drug discovery and personalized management optimizing. Here, we aimed to characterize the molecular features of CRC by a classification system based on metabolic gene expression profiles. 435 CRC samples from the Genomic Data Commons data portal were chosen as training set while 566 sample in GSE39582 were selected as testing set. Then, a non-negative matrix factorization clustering was performed, and three subclasses of CRC (C1, C2, and C3) were identified in both training set and testing set. Results showed that subclass C1 displayed high metabolic activity and good prognosis. Subclass C2 was associated with low metabolic activities and displayed high immune signatures as well as high expression of immune checkpoint genes. C2 had the worst prognosis among the three subtypes. Subclass C3 displayed intermediate metabolic activity, high gene mutation numbers and good prognosis. Finally, a 27-gene metabolism-related signature was identified for prognosis prediction. Our works deepened the understanding of metabolic hallmarks of CRC, and provided valuable information for "multi-molecular" based personalized therapies.

摘要

结直肠癌(CRC)的高度异质性是个体化治疗的主要临床挑战。分子分类将有助于药物发现和优化个性化管理。在此,我们旨在通过基于代谢基因表达谱的分类系统来表征CRC的分子特征。从基因组数据共享数据门户中选取435个CRC样本作为训练集,同时选择GSE39582中的566个样本作为测试集。然后,进行非负矩阵分解聚类,在训练集和测试集中均鉴定出CRC的三个亚类(C1、C2和C3)。结果显示,亚类C1表现出高代谢活性和良好的预后。亚类C2与低代谢活性相关,表现出高免疫特征以及免疫检查点基因的高表达。C2在三种亚型中预后最差。亚类C3表现出中等代谢活性、高基因突变数和良好的预后。最后,鉴定出一个27基因的代谢相关特征用于预后预测。我们的工作加深了对CRC代谢特征的理解,并为基于“多分子”的个性化治疗提供了有价值的信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/46f5/7746835/8c2e4bd2167b/fonc-10-602498-g001.jpg

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