Detarya Marutpong, Lert-Itthiporn Worachart, Mahalapbutr Panupong, Klaewkla Methus, Sorin Supannika, Sawanyawisuth Kanlayanee, Silsirivanit Atit, Seubwai Wunchana, Wongkham Chaisiri, Araki Norie, Wongkham Sopit
Department of Biochemistry, Faculty of Medicine, and Center for Translational Medicine, Khon Kaen University Khon Kaen 40002, Thailand.
Future Health Innovation Technology Co., Ltd. Bangkok 10170, Thailand.
Am J Cancer Res. 2022 Sep 15;12(9):4140-4159. eCollection 2022.
Cholangiocarcinoma (CCA) is a lethal cancer in that the incidence is now increasing worldwide. N-acetylgalactosaminyltransferase 5 (GALNT5), an enzyme that initiates the first step of mucin type-O glycosylation, has been reported to promote aggressiveness of CCA cells via the epithelial to the mesenchymal transition (EMT) process, and Akt/Erk activation. In this study, the clinical and biological relevance of GALNT5 and the molecular mechanisms by which GALNT5 modulated EGFR in promoting CCA progression were examined. Using publicly available datasets, upregulation of GALNT5 in patient CCA tissues and its correlation with EGFR expression was noted. High levels of GALNT5 were significantly associated with the short survival of patients, suggesting a prognostic marker of GALNT5 for CCA. GALNT5 modulated EGFR expression as shown in CCA cell lines. Upregulation of GALNT5 significantly increased EGFR mRNA and protein in GALNT5 overexpressing cells, whereas suppression of GALNT5 expression gave the opposite results. The molecular dynamics simulations and MM/PB(GB)SA-based free energy calculations showed that O-glycosylation on the EGFR extracellular domain enhanced the structural stability, compactness, and H-bond formation of the EGF/GalNAc-EGFR complex compared with those of EGF/EGFR. This stabilized the growth factor binding site and fostered stronger interactions between EGF and EGFR. Using the EGF-induced EGFR activation model, GALNT5 was shown to mediate EGFR stability via a decreased rate of EGFR degradation and enhanced EGFR activity by increasing the binding affinity of EGF/EGFR that consequently increasing the activation of EGFR and its downstream effectors Akt and Erk. In summary, GALNT5 was upregulated in CCA tissues and associated with a worse prognosis. The study identified for the first time the impacts of GALNT5 on EGFR activity by increasing: 1) EGFR expression via a transcriptional-dependent mechanism, 2) EGFR stability by reducing EGFR degradation, and 3) EGFR activation through an increased binding affinity of EGF/EGFR which all together fostered the activation of EGFR. These results expanded the understanding of the molecular mechanism of how GALNT5 impacted CCA progression and suggested GALNT5 as a new target for therapeutic intervention against metastatic CCA.
胆管癌(CCA)是一种致命性癌症,其全球发病率目前正在上升。N-乙酰半乳糖胺基转移酶5(GALNT5)是一种启动粘蛋白O型糖基化第一步的酶,据报道它通过上皮-间质转化(EMT)过程以及Akt/Erk激活来促进CCA细胞的侵袭性。在本研究中,研究了GALNT5的临床和生物学相关性以及GALNT5在促进CCA进展过程中调节表皮生长因子受体(EGFR)的分子机制。利用公开可用的数据集,发现患者CCA组织中GALNT5上调及其与EGFR表达的相关性。GALNT5水平高与患者生存期短显著相关,提示GALNT5可作为CCA的预后标志物。如在CCA细胞系中所示,GALNT5调节EGFR表达。GALNT5过表达细胞中GALNT5上调显著增加EGFR mRNA和蛋白,而抑制GALNT5表达则产生相反结果。分子动力学模拟和基于MM/PB(GB)SA的自由能计算表明,与EGF/EGFR相比,EGFR胞外域上的O-糖基化增强了EGF/GalNAc-EGFR复合物的结构稳定性、紧凑性和氢键形成。这稳定了生长因子结合位点并促进了EGF与EGFR之间更强的相互作用。使用EGF诱导的EGFR激活模型,结果显示GALNT5通过降低EGFR降解速率来介导EGFR稳定性,并通过增加EGF/EGFR的结合亲和力来增强EGFR活性,从而增加EGFR及其下游效应物Akt和Erk的激活。总之,GALNT5在CCA组织中上调且与较差的预后相关。该研究首次确定了GALNT5对EGFR活性的影响,具体方式为:1)通过转录依赖性机制增加EGFR表达;2)通过减少EGFR降解来提高EGFR稳定性;3)通过增加EGF/EGFR的结合亲和力来激活EGFR,所有这些共同促进了EGFR的激活。这些结果扩展了对GALNT5影响CCA进展分子机制的理解,并提示GALNT5可作为转移性CCA治疗干预的新靶点。
