Altered fatty acid metabolism rewires cholangiocarcinoma stemness features

IF 9.5 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Giulia Lori , Mirella Pastore , Nadia Navari , Benedetta Piombanti , Richell Booijink , Elisabetta Rovida , Ignazia Tusa , Monika Lewinska , Jesper B. Andersen , Tiziano Lottini , Annarosa Arcangeli , Maria Letizia Taddei , Erica Pranzini , Caterina Mancini , Cecilia Anceschi , Stefania Madiai , Elena Sacco , Stefano Rota , Adriana Trapani , Gennaro Agrimi , Chiara Raggi
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引用次数: 0

Abstract

Background & Aims

Among the reprogrammed metabolic pathways described in cancer stem cells, aberrant lipid metabolism has recently drawn increasing attention. Our study explored the contribution of fatty acids (FA) in the regulation of stem-like features in intrahepatic cholangiocarcinoma (iCCA).

Methods

We previously identified a functional stem-like subset in human iCCA by using a three-dimensional sphere (SPH) model in comparison to parental cells grown as monolayers (MON). In this study, quantification of intracellular free FA and lipidomic analysis (triacylglycerol [TAG] composition, de novo synthesis products) was performed by Liquid chromatography–mass spectrometry (LC–MS); quadrupole time-of-flight liquid chromatography/mass spectrometry (Q-TOF LC/MS), respectively, in both SPH and MON cultures.

Results

Stem-like SPH showed a superior content of free FA (citric, palmitic, stearic, and oleic acids) and unsaturated TAG. Molecularly, SPH showed upregulation of key metabolic enzymes involved in de novo FA biosynthesis (AceCS1, ACLY, ACAC, FASN, ACSL1) and the mTOR signalling pathway. In patients with iCCA (n = 68), tissue expression of FASN, a key gene involved in FA synthesis, correlated with 5-year overall survival. Interference with FASN activity in SPH cells through both specific gene silencing (siRNA) or pharmacological inhibition (orlistat) decreased sphere-forming ability and expression of stem-like markers. In a murine xenograft model obtained by injection of iCCA-SPH cells, FASN inhibition by orlistat or injection of FASN-silenced cells significantly reduced tumour growth and expression of stem-like genes.

Conclusion

Altered FA metabolism contributes to the maintenance of a stem-like phenotype in iCCA. FASN inhibition may represent a new approach to interfere with the progression of this deadly disease.

Impact and implications

Recent evidence indicates that metabolic disorders correlate with an increased susceptibility to intrahepatic cholangiocarcinoma (iCCA). Our investigation emphasises the pivotal involvement of lipid metabolism in the tumour stem cell biology of iCCA, facilitated by the upregulation of crucial enzymes and the mTOR signalling pathway. From a clinical perspective, this underscores the dual role of FASN as both a prognostic indicator and a therapeutic target, suggesting that FASN inhibitors could enhance patient outcomes by diminishing stemness and tumour aggressiveness. These findings pave the way for novel therapeutic strategies for iCCA and shed light on its relationship with metabolic disorders such as diabetes, obesity, metabolic syndrome, and metabolic dysfunction-associated steatotic liver disease.

Abstract Image

脂肪酸代谢改变重塑了胆管癌干性特征
背景& 目的在癌症干细胞中描述的重编程代谢途径中,异常脂质代谢最近引起了越来越多的关注。我们的研究探讨了脂肪酸(FA)在调控肝内胆管癌(iCCA)干样特征中的贡献。方法我们先前通过使用三维球体(SPH)模型与单层生长的亲代细胞(MON)进行比较,确定了人类iCCA中的功能性干样亚群。在本研究中,采用液相色谱-质谱法(LC-MS)和四极杆飞行时间液相色谱/质谱法(Q-TOF LC/MS)分别对SPH和MON培养物进行了细胞内游离FA定量和脂质体分析(三酰甘油[TAG]组成、新合成产物)。结果类茎 SPH 显示出较高的游离脂肪酸(柠檬酸、棕榈酸、硬脂酸和油酸)和不饱和 TAG 含量。从分子角度看,SPH显示出参与新脂肪酸生物合成的关键代谢酶(AceCS1、ACLY、ACAC、FASN、ACSL1)和mTOR信号通路的上调。在 iCCA 患者(68 人)中,参与 FA 合成的关键基因 FASN 的组织表达与 5 年总生存率相关。通过特异性基因沉默(siRNA)或药物抑制(奥利司他)干扰SPH细胞中FASN的活性,可降低球形成能力和干样标志物的表达。在注射iCCA-SPH细胞获得的小鼠异种移植模型中,通过奥利司他抑制FASN或注射FASN沉默的细胞可显著减少肿瘤生长和干样基因的表达。影响和意义最近的证据表明,代谢紊乱与肝内胆管癌(iCCA)的易感性增加有关。我们的研究强调了脂质代谢在 iCCA 肿瘤干细胞生物学中的关键作用,关键酶和 mTOR 信号通路的上调促进了脂质代谢。从临床角度来看,这强调了FASN作为预后指标和治疗靶点的双重作用,表明FASN抑制剂可通过降低干细胞和肿瘤侵袭性来改善患者预后。这些发现为iCCA的新型治疗策略铺平了道路,并阐明了iCCA与糖尿病、肥胖症、代谢综合征和代谢功能障碍相关性脂肪肝等代谢性疾病的关系。
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来源期刊
JHEP Reports
JHEP Reports GASTROENTEROLOGY & HEPATOLOGY-
CiteScore
12.40
自引率
2.40%
发文量
161
审稿时长
36 days
期刊介绍: JHEP Reports is an open access journal that is affiliated with the European Association for the Study of the Liver (EASL). It serves as a companion journal to the highly respected Journal of Hepatology. The primary objective of JHEP Reports is to publish original papers and reviews that contribute to the advancement of knowledge in the field of liver diseases. The journal covers a wide range of topics, including basic, translational, and clinical research. It also focuses on global issues in hepatology, with particular emphasis on areas such as clinical trials, novel diagnostics, precision medicine and therapeutics, cancer research, cellular and molecular studies, artificial intelligence, microbiome research, epidemiology, and cutting-edge technologies. In summary, JHEP Reports is dedicated to promoting scientific discoveries and innovations in liver diseases through the publication of high-quality research papers and reviews covering various aspects of hepatology.
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