Zimmer Kai, Kocher Florian, Untergasser Gerold, Kircher Brigitte, Amann Arno, Baca Yasmine, Xiu Joanne, Korn W Micheal, Berger Martin D, Lenz Heinz-Josef, Puccini Alberto, Fontana Elisa, Shields Anthony F, Marshall John L, Hall Michael, El-Deiry Wafik S, Hsiehchen David, Macarulla Teresa, Tabernero Josep, Pichler Renate, Khushman Moh'd, Manne Upender, Lou Emil, Wolf Dominik, Sokolova Viktorija, Schnaiter Simon, Zeimet Alain G, Gulhati Pat, Widmann Gerlig, Seeber Andreas
Department of Hematology and Oncology, Comprehensive Cancer Center Innsbruck (CCCI), Medical University Innsbruck (MUI), Innsbruck, Austria.
Tyrolean Cancer Research Institute, Innsbruck, Austria.
NPJ Precis Oncol. 2023 Jul 3;7(1):64. doi: 10.1038/s41698-023-00409-5.
Polybromo-1 (PBRM1) loss of function mutations are present in a fraction of biliary tract cancers (BTCs). PBRM1, a subunit of the PBAF chromatin-remodeling complex, is involved in DNA damage repair. Herein, we aimed to decipher the molecular landscape of PBRM1 mutated (mut) BTCs and to define potential translational aspects. Totally, 1848 BTC samples were analyzed using next-generation DNA-sequencing and immunohistochemistry (Caris Life Sciences, Phoenix, AZ). siRNA-mediated knockdown of PBRM1 was performed in the BTC cell line EGI1 to assess the therapeutic vulnerabilities of ATR and PARP inhibitors in vitro. PBRM1 mutations were identified in 8.1% (n = 150) of BTCs and were more prevalent in intrahepatic BTCs (9.9%) compared to gallbladder cancers (6.0%) or extrahepatic BTCs (4.5%). Higher rates of co-mutations in chromatin-remodeling genes (e.g., ARID1A 31% vs. 16%) and DNA damage repair genes (e.g., ATRX 4.4% vs. 0.3%) were detected in PBRM1-mutated (mut) vs. PBRM1-wildtype (wt) BTCs. No difference in real-world overall survival was observed between PBRM1-mut and PBRM1-wt patients (HR 1.043, 95% CI 0.821-1.325, p = 0.731). In vitro, experiments suggested that PARP ± ATR inhibitors induce synthetic lethality in the PBRM1 knockdown BTC model. Our findings served as the scientific rationale for PARP inhibition in a heavily pretreated PBRM1-mut BTC patient, which induced disease control. This study represents the largest and most extensive molecular profiling study of PBRM1-mut BTCs, which in vitro sensitizes to DNA damage repair inhibiting compounds. Our findings might serve as a rationale for future testing of PARP/ATR inhibitors in PBRM1-mut BTCs.
多溴-1(PBRM1)功能缺失突变存在于一部分胆管癌(BTC)中。PBRM1是PBAF染色质重塑复合物的一个亚基,参与DNA损伤修复。在此,我们旨在解析PBRM1突变(mut)BTC的分子格局,并确定潜在的转化方面。总共使用下一代DNA测序和免疫组织化学(Caris生命科学公司,亚利桑那州凤凰城)分析了1848份BTC样本。在BTC细胞系EGI1中进行了siRNA介导的PBRM1敲低,以评估体外ATR和PARP抑制剂的治疗易感性。在8.1%(n = 150)的BTC中鉴定出PBRM1突变,与胆囊癌(6.0%)或肝外BTC(4.5%)相比,在肝内BTC中更常见(9.9%)。在PBRM1突变(mut)与PBRM1野生型(wt)BTC中,检测到染色质重塑基因(如ARID1A,31%对16%)和DNA损伤修复基因(如ATRX,4.4%对0.3%)的共突变率更高。在PBRM1突变和PBRM1野生型患者之间未观察到实际总生存期的差异(HR 1.043,9可信区间0.821 - 1.325,p = 0.731)。在体外,实验表明PARP ± ATR抑制剂在PBRM1敲低的BTC模型中诱导合成致死性。我们的发现为在一名经过大量预处理的PBRM1突变BTC患者中使用PARP抑制提供了科学依据,该治疗诱导了疾病控制。本研究是对PBRM1突变BTC进行的最大规模和最广泛的分子谱分析研究,该研究表明其在体外对DNA损伤修复抑制化合物敏感。我们的发现可能为未来在PBRM1突变BTC中测试PARP/ATR抑制剂提供理论依据。
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