Integrative Omics Uncovers Low Tumorous Magnesium Content as A Driver Factor of Colorectal Cancer.

Rou Zhang, Meng Hu, Yu Liu, Wanmeng Li, Zhiqiang Xu, Siyu He, Ying Lu, Yanqiu Gong, Xiuxuan Wang, Shan Hai, Shuangqing Li, Shiqian Qi, Yuan Li, Yang Shu, Dan Du, Huiyuan Zhang, Heng Xu, Zongguang Zhou, Peng Lei, Hai-Ning Chen, Lunzhi Dai
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Abstract

Magnesium (Mg) deficiency is associated with increased risk and malignancy in colorectal cancer (CRC), yet the underlying mechanisms remain elusive. Here, we used genomic, proteomic, and phosphoproteomic data to elucidate the impact of Mg deficiency on CRC. Genomic analysis identified 160 genes with higher mutation frequencies in Low-Mg tumors, including key driver genes such as KMT2C and ERBB3. Unexpectedly, initiation driver genes of CRC, such as TP53 and APC, displayed higher mutation frequencies in High-Mg tumors. Additionally, proteomic and phosphoproteomic data indicated that low Mg content in tumors may activate epithelial-mesenchymal transition (EMT) by modulating inflammation or remodeling the phosphoproteome of cancer cells. Notably, we observed a negative correlation between the phosphorylation of DBN1 at S142 (DBN1S142p) and Mg content. A mutation in S142 to D (DBN1S142D) mimicking DBN1S142p up-regulated MMP2 and enhanced cell migration, while treatment with MgCl2 reduced DBN1S142p, thereby reversing this phenotype. Mechanistically, Mg2+ attenuated the DBN1-ACTN4 interaction by decreasing DBN1S142p, which in turn enhanced the binding of ACTN4 to F-actin and promoted F-actin polymerization, ultimately reducing MMP2 expression. These findings shed new light on the crucial role of Mg deficiency in CRC progression and suggest that Mg supplementation may be a promising preventive and therapeutic strategy for CRC.

整合分子生物学发现肿瘤镁含量低是结直肠癌的一个驱动因素
镁(Mg)缺乏与结直肠癌(CRC)的风险和恶性程度增加有关,但其潜在的机制仍然难以捉摸。在这里,我们利用基因组学、蛋白质组学和磷酸蛋白质组学数据来阐明镁缺乏对 CRC 的影响。基因组分析确定了低镁肿瘤中突变频率较高的160个基因,包括KMT2C和ERBB3等关键驱动基因。意想不到的是,TP53 和 APC 等 CRC 启动驱动基因在高镁肿瘤中的突变频率更高。此外,蛋白质组和磷酸化蛋白质组数据表明,肿瘤中的低镁含量可能会通过调节炎症或重塑癌细胞的磷酸化蛋白质组来激活上皮-间质转化(EMT)。值得注意的是,我们观察到 DBN1 在 S142 处的磷酸化(DBN1S142p)与镁含量呈负相关。模拟 DBN1S142p 的 S142 突变为 D(DBN1S142D)会上调 MMP2 并增强细胞迁移,而用 MgCl2 处理会降低 DBN1S142p,从而逆转这种表型。从机理上讲,Mg2+ 通过减少 DBN1S142p 减弱了 DBN1-ACTN4 的相互作用,这反过来又增强了 ACTN4 与 F-肌动蛋白的结合并促进了 F-肌动蛋白的聚合,最终减少了 MMP2 的表达。这些发现揭示了镁缺乏在 CRC 进展中的关键作用,并表明补充镁可能是一种很有前景的 CRC 预防和治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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