Department of Surgical Oncology, UMC Utrecht Cancer Centre, Utrecht, the Netherlands.
Oncode Institute, Hubrecht Institute - Royal Academy of Arts and Sciences and University Medical Centre Utrecht, Utrecht, the Netherlands.
Br J Surg. 2019 Sep;106(10):1404-1414. doi: 10.1002/bjs.11206. Epub 2019 Jun 14.
Patients with peritoneal metastases from colorectal cancer have a poor prognosis. If the intraperitoneal tumour load is limited, patients may be eligible for cytoreductive surgery followed by hyperthermic intraperitoneal chemotherapy (HIPEC). This treatment has improved overall survival, but recurrence rates are high. The aim of this study was to create a preclinical platform for the development of more effective intraperitoneal chemotherapy strategies.
Using organoid technology, five tumour cultures were generated from malignant ascites and resected peritoneal metastases. These were used in an in vitro HIPEC model to assess sensitivity to mitomycin C (MMC) and oxaliplatin, the drugs used most commonly in HIPEC. The model was also used to test a rational combination treatment involving MMC and inhibitors of the checkpoint kinase ATR.
MMC was more effective in eliminating peritoneal metastasis-derived organoids than oxaliplatin at clinically relevant concentrations. However, the drug concentrations required to eliminate 50 per cent of the tumour cells (IC50) were higher than the median clinical dose in two of five organoid lines for MMC, and all five lines for oxaliplatin, indicating a general resistance to monotherapy. ATR inhibition increased the sensitivity of all peritoneal metastasis-derived organoids to MMC, as the IC50 decreased 2·6-12·4-fold to well below concentrations commonly attained in clinical practice. Live-cell imaging and flow cytometric analysis showed that ATR inhibition did not release cells from MMC-induced cell cycle arrest, but caused increased replication stress and accelerated cell death.
Peritoneal metastasis-derived organoids can be used to evaluate existing HIPEC regimens on an individual-patient level and for development of more effective treatment strategies. Surgical relevance Cytoreductive surgery followed by hyperthermic intraperitoneal chemotherapy (HIPEC) has improved prognosis of patients with peritoneal metastases from colorectal cancer, but disease recurrence is common. More effective and personalized HIPEC is urgently needed. Organoid technology is frequently used for drug screens, as patient-derived organoids can accurately predict clinical therapeutic response in vitro. A panel of organoids was established from peritoneal metastases from colorectal cancer and used to develop a model for testing HIPEC regimens in vitro. Patient-derived organoids differed in sensitivity to commonly used chemotherapeutics, in line with variable clinical outcomes following cytoreductive surgery-HIPEC. Combining MMC with an ATR inhibitor improved the efficacy of MMC. Peritoneal metastasis-derived organoids can be used as a platform to test novel (combination) strategies that increase HIPEC efficacy. In the future, organoids could be used to select patent-tailored HIPEC regimens.
结直肠癌腹膜转移患者预后较差。如果腹腔内肿瘤负荷有限,患者可能有资格接受细胞减灭术联合腹腔热灌注化疗(HIPEC)。这种治疗方法提高了总生存率,但复发率很高。本研究旨在为开发更有效的腹腔化疗策略创建一个临床前平台。
使用类器官技术,从恶性腹水和切除的腹膜转移灶中生成了 5 个肿瘤培养物。这些培养物用于体外 HIPEC 模型,以评估丝裂霉素 C(MMC)和奥沙利铂的敏感性,这两种药物是 HIPEC 中最常用的药物。该模型还用于测试涉及 MMC 和检查点激酶 ATR 抑制剂的合理联合治疗。
在临床相关浓度下,MMC 比奥沙利铂更有效地消除腹膜转移源性类器官。然而,消除 50%肿瘤细胞所需的药物浓度(IC50)在 5 个类器官系中的 2 个对 MMC 和所有 5 个对奥沙利铂的浓度均高于中位数临床剂量,表明普遍存在单药耐药性。ATR 抑制增加了所有腹膜转移源性类器官对 MMC 的敏感性,IC50 降低了 2.6-12.4 倍,降至远低于临床实践中常达到的浓度。活细胞成像和流式细胞分析表明,ATR 抑制不会使细胞从 MMC 诱导的细胞周期阻滞中释放,但会导致复制应激增加和细胞死亡加速。
腹膜转移源性类器官可用于在个体患者水平评估现有的 HIPEC 方案,并开发更有效的治疗策略。手术相关性细胞减灭术联合腹腔热灌注化疗(HIPEC)改善了结直肠癌腹膜转移患者的预后,但疾病复发很常见。迫切需要更有效和个性化的 HIPEC。类器官技术常用于药物筛选,因为患者来源的类器官可以在体外准确预测临床治疗反应。从结直肠癌腹膜转移灶中建立了一组类器官,并用于建立体外测试 HIPEC 方案的模型。患者来源的类器官对常用化疗药物的敏感性不同,与细胞减灭术-HIPEC 后的临床转归变化一致。MMC 与 ATR 抑制剂联合使用可提高 MMC 的疗效。腹膜转移源性类器官可作为平台,用于测试增加 HIPEC 疗效的新型(联合)策略。在未来,类器官可用于选择适合患者的 HIPEC 方案。
Zotero 插件
