PARP-1 可选择性地影响肝内胆管癌中 KRAS 驱动的表型和分子特征。

IF 23 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Gut Pub Date : 2024-09-09 DOI:10.1136/gutjnl-2023-331237
Friederike L Keggenhoff, Darko Castven, Diana Becker, Stojan Stojkovic, Jovana Castven, Carolin Zimpel, Beate K Straub, Tiemo Gerber, Harald Langer, Patricia Hähnel, Thomas Kindler, Jörg Fahrer, Colm J O'Rourke, Ursula Ehmer, Anna Saborowski, Lichun Ma, Xin Wei Wang, Timo Gaiser, Matthias S Matter, Christian Sina, Stefanie Derer, Ju-Seog Lee, Stephanie Roessler, Bernd Kaina, Jesper B Andersen, Peter R Galle, Jens U Marquardt
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引用次数: 0

摘要

目的:肝内胆管癌(iCCA)是第二大最常见的原发性肝癌,但治疗方案有限。KRAS 突变是 iCCA 中最常见的基因改变之一,与不良的临床预后和治疗反应有关。最近的研究结果表明,聚(ADP-核糖)聚合酶1(PARP-1)与KRAS驱动的癌症有关,但其在胆管癌发生中的确切作用仍未确定:设计:利用RNAi、CRISPR/Cas9和药物抑制KRAS突变和非突变细胞,在患者衍生细胞和已建立的iCCA细胞中进行PARP-1抑制。此外,还通过水动力尾静脉注射将 Parp-1 基因敲除小鼠与 iCCA 诱导相结合,以评估对 Kras 驱动型和 Kras 野生型 iCCA 表型和分子特征的影响。在真实的人类 iCCA 中证实了其临床意义:结果:PARP-1在KRAS突变的人类iCCA中明显增强。基于PARP-1的干预措施优先损害了人KRAS突变细胞系的细胞活力和致瘤性。同样,在Kras/Tp53诱导的iCCA和Akt/Nicd诱导的iCCA中,Parp-1的缺失会引起不同的表型,并会抑制Kras依赖性胆管癌的发生。转录组分析证实,CHK1介导的DNA损伤应答途径和复制应激反应优先受损。同样,抑制 CHK1 能有效逆转 PARP-1 介导的效应。最后,Parp-1消耗诱导了KRAS突变iCCA的分子转换,再现了预后良好的人类iCCA患者:我们的研究结果确定了 PARP-1 在激活致癌 KRAS 信号的 iCCA 患者中的新型预后和治疗作用。
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PARP-1 selectively impairs KRAS-driven phenotypic and molecular features in intrahepatic cholangiocarcinoma.

Objective: Intrahepatic cholangiocarcinoma (iCCA) is the second most common primary liver cancer with limited therapeutic options. KRAS mutations are among the most abundant genetic alterations in iCCA associated with poor clinical outcome and treatment response. Recent findings indicate that Poly(ADP-ribose)polymerase1 (PARP-1) is implicated in KRAS-driven cancers, but its exact role in cholangiocarcinogenesis remains undefined.

Design: PARP-1 inhibition was performed in patient-derived and established iCCA cells using RNAi, CRISPR/Cas9 and pharmacological inhibition in KRAS-mutant, non-mutant cells. In addition, Parp-1 knockout mice were combined with iCCA induction by hydrodynamic tail vein injection to evaluate an impact on phenotypic and molecular features of Kras-driven and Kras-wildtype iCCA. Clinical implications were confirmed in authentic human iCCA.

Results: PARP-1 was significantly enhanced in KRAS-mutant human iCCA. PARP-1-based interventions preferentially impaired cell viability and tumourigenicity in human KRAS-mutant cell lines. Consistently, loss of Parp-1 provoked distinct phenotype in Kras/Tp53-induced versus Akt/Nicd-induced iCCA and abolished Kras-dependent cholangiocarcinogenesis. Transcriptome analyses confirmed preferential impairment of DNA damage response pathways and replicative stress response mediated by CHK1. Consistently, inhibition of CHK1 effectively reversed PARP-1 mediated effects. Finally, Parp-1 depletion induced molecular switch of KRAS-mutant iCCA recapitulating good prognostic human iCCA patients.

Conclusion: Our findings identify the novel prognostic and therapeutic role of PARP-1 in iCCA patients with activation of oncogenic KRAS signalling.

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来源期刊
Gut
Gut 医学-胃肠肝病学
CiteScore
45.70
自引率
2.40%
发文量
284
审稿时长
1.5 months
期刊介绍: Gut is a renowned international journal specializing in gastroenterology and hepatology, known for its high-quality clinical research covering the alimentary tract, liver, biliary tree, and pancreas. It offers authoritative and current coverage across all aspects of gastroenterology and hepatology, featuring articles on emerging disease mechanisms and innovative diagnostic and therapeutic approaches authored by leading experts. As the flagship journal of BMJ's gastroenterology portfolio, Gut is accompanied by two companion journals: Frontline Gastroenterology, focusing on education and practice-oriented papers, and BMJ Open Gastroenterology for open access original research.
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