Journal
JOURNAL OF EXPERIMENTAL & CLINICAL CANCER RESEARCH
Volume 41, Issue 1, Pages -Publisher
BMC
DOI: 10.1186/s13046-022-02386-2
Keywords
Cholangiocarcinoma; Bile; Inflammation; Interleukin-6; KRAS; G9a histone methyl-transferase; Serine-glycine pathway; Metabolic reprogramming
Categories
Funding
- MCIN/AEI [PID2019-104878RB-I00]
- CIBERehd
- Instituto de Salud Carlos III (ISCIII) [PI15/01132, PI18/01075, PI16/01126, PI19/00819]
- Fondo Europeo de Desarrollo Regional (FEDER) Una manera de hacer Europa
- Fundacion Cientifica de la Asociacion Espanola Contra el Cancer (AECC Scientific Foundation
- Rare Cancers grant 2017)
- Gobierno de Navarra [58/17]
- IZKF
- START-Program of the Faculty of Medicine [691405]
- RWTH Aachen
- German Krebshilfe [70113000]
- Junta de Castilla y Leon [SA063P17]
- Gobierno Regional de Madrid [EXOHEP-CM S2017/BMD-3727, NanoLiver-CM Y2018/NMT-4949]
- Ministerio de Ciencia, Innovacion y Universidades MICINN-Agencia Estatal de Investigacion integrado en el Plan Estatal de Investigacion Cientifica y Tecnica y Innovacion [PID2019-104878RB-100, PID2020-117116RB-I00, SAF2014-54191-R, SAF2016-78711, SAF2017-87301-R, SAF2017-88933-R]
- MCIU/AEI/FEDER, UE [RTI2018-095134-B-100]
- Ayudas para apoyar a grupos de investigacion del sistema Universitario Vasco [IT971-16]
- Bio-Eusko Fundazioa (Eitb maratoia) [BIO15/CA/011, BIO15/CA/016/BD]
- Euskadi RIS3 [2019222054]
- HEPACARE Project from Fundacion La Caixa
- La Caixa Foundation
- European Foundation for Alcohol Research (ERAB) [EA 18/14]
- Union Iberoamericana de Universidades [UCM-25-2019]
- Fundacion Eugenio Rodriguez Pascual
- Fundacion Echebano
- Fundacio Marato TV3 [201916-31]
- Fundacion Mario Losantos
- Fundacion M Torres
- AMMF The Cholangiocarcinoma Charity [2018/117]
- Umbrella Ayudas 2018 BBVA Foundation Grants for Scientific Research Teams [LCF/PR/HP17/52190004]
- COST Action [CA181122]
- Spanish Carlos III Health Institute (ISCIII) [FIS PI18/01075, PI21/00922, CPII19/00008]
- Fondo Europeo de Desarrollo Regional (FEDER)
- CIBERehd (ISCIII)
- La Caixa Scientific Foundation [HR17-00601]
- AMMF-The Cholangiocarcinoma Charity [EU/2019/AMMFt/001]
- European Union's Horizon 2020 Research and Innovation Program [825510]
- AECC
- Ramon y Cajal Program contracts [RYC-2014-15242, RYC2018-024475-1]
- German Research Foundation [Tr 285/10-2, CRC1382, 403224013]
- cofinanciado con Fondos FEDER
- PSC Partners US [06119JB]
- [SFB TRR 57]
- [SFB 1382]
- [DFG TR285-10/1]
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By performing proteomic and metabolomic analyses, we identified new pro-tumorigenic mechanisms in intrahepatic cholangiocarcinoma (iCCA), including activation of EGFR signaling or KRAS mutation driving IL6 expression in tumor cells, as well as reprogramming of glucose metabolism and activation of the serine-glycine pathway. These findings provide potential therapeutic targets for iCCA.
Background Cholangiocarcinoma (CCA) is still a deadly tumour. Histological and molecular aspects of thioacetamide (TAA)-induced intrahepatic CCA (iCCA) in rats mimic those of human iCCA. Carcinogenic changes and therapeutic vulnerabilities in CCA may be captured by molecular investigations in bile, where we performed bile proteomic and metabolomic analyses that help discovery yet unknown pathways relevant to human iCCA. Methods Cholangiocarcinogenesis was induced in rats (TAA) and mice (Jnk(Delta hepa) + CCl4 + DEN model). We performed proteomic and metabolomic analyses in bile from control and CCA-bearing rats. Differential expression was validated in rat and human CCAs. Mechanisms were addressed in human CCA cells, including Huh28-KRAS(G12D) cells. Cell signaling, growth, gene regulation and [U-C-13]-D-glucose-serine fluxomics analyses were performed. In vivo studies were performed in the clinically-relevant iCCA mouse model. Results Pathways related to inflammation, oxidative stress and glucose metabolism were identified by proteomic analysis. Oxidative stress and high amounts of the oncogenesis-supporting amino acids serine and glycine were discovered by metabolomic studies. Most relevant hits were confirmed in rat and human CCAs (TCGA). Activation of interleukin-6 (IL6) and epidermal growth factor receptor (EGFR) pathways, and key genes in cancer-related glucose metabolic reprogramming, were validated in TAA-CCAs. In TAA-CCAs, G9a, an epigenetic pro-tumorigenic writer, was also increased. We show that EGFR signaling and mutant KRAS(G12D) can both activate IL6 production in CCA cells. Furthermore, phosphoglycerate dehydrogenase (PHGDH), the rate-limiting enzyme in serine-glycine pathway, was upregulated in human iCCA correlating with G9a expression. In a G9a activity-dependent manner, KRAS(G12D) promoted PHGDH expression, glucose flow towards serine synthesis, and increased CCA cell viability. KRAS(G12D) CAA cells were more sensitive to PHGDH and G9a inhibition than controls. In mouse iCCA, G9a pharmacological targeting reduced PHGDH expression. Conclusions In CCA, we identified new pro-tumorigenic mechanisms: Activation of EGFR signaling or KRAS mutation drives IL6 expression in tumour cells; Glucose metabolism reprogramming in iCCA includes activation of the serine-glycine pathway; Mutant KRAS drives PHGDH expression in a G9a-dependent manner; PHGDH and G9a emerge as therapeutic targets in iCCA.
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