瑞戈非尼可诱导DNA损伤并增强聚（ADP-核糖）聚合酶（PARP）抑制剂在胰腺导管癌中的疗效。

Regorafenib induces DNA damage and enhances PARP inhibitor efficacy in pancreatic ductal carcinoma.

作者信息

Pham Thao D, Becker Jeffrey H, Metropulos Anastasia E, Mubin Nida, Spaulding Christina, Bentrem David J, Munshi Hidayatullah G

机构信息

Department of Medicine, Feinberg School of Medicine, Northwestern University, Chicago, IL, USA.

The Robert H. Lurie Comprehensive Cancer Center, Chicago, IL, USA.

出版信息

BMC Cancer. 2024 Dec 20;24(1):1562. doi: 10.1186/s12885-024-13334-y.

DOI:10.1186/s12885-024-13334-y

PMID:39707244

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11662535/

Abstract

BACKGROUND

There is increasing interest in enhancing the response of the PARP inhibitor olaparib, which is currently approved for pancreatic ductal adenocarcinoma (PDAC) patients with defects in DNA damage repair associated with germline BRCA1/2 mutations. Moreover, agents that can mimic these defects in the absence of germline BRCA1/2 mutations are an area of active research in hopes of increasing the number of patients eligible for treatment with PARP inhibitors. The extent to which regorafenib, an FDA-approved tyrosine kinase inhibitor, can be used to enhance the efficacy of PARP inhibitors in PDAC cells without known BRCA1/2 mutations remains to be investigated.

METHODS

Comet assay, cell cycle analysis, western blotting, and immunofluorescent detection of H2AX were used to evaluate the extent to which regorafenib induces DNA damage in PDAC cell lines. The effects of regorafenib, either alone or in combination with PARPi inhibitors, on PDAC cell death were assessed by Annexin V/PI co-staining assay in cell lines and by immunohistochemistry staining for cleaved caspase-3 in mouse tumors and in ex vivo slice cultures of human PDAC tumors. Flow cytometry-based analysis was used to evaluate the ability of regorafenib to reprogram PDAC tumor microenvironment.

RESULTS

We now show that regorafenib, a tyrosine-kinase inhibitor with efficacy in several gastrointestinal malignancies, can enhance the response of olaparib in pancreatic cancer. While regorafenib induces DNA damage and limits the ability of PDAC cells to resolve the damage, regorafenib by itself does not induce apoptosis. However, regorafenib in combination with olaparib further induces DNA damage in vitro, in tumor-bearing mice, and in ex vivo slice cultures of human PDAC tumors, resulting in increased apoptosis compared to olaparib alone. Notably, we show that the efficacy of the combination treatment is not dependent on cytolytic T cells.

CONCLUSIONS

Together, these findings demonstrate that regorafenib can attenuate DNA damage response and potentiate the efficacy of PARP inhibitors in PDAC tumors.

摘要

背景

增强聚（ADP - 核糖）聚合酶（PARP）抑制剂奥拉帕利的反应受到越来越多的关注，奥拉帕利目前已被批准用于治疗患有与种系BRCA1/2突变相关的DNA损伤修复缺陷的胰腺导管腺癌（PDAC）患者。此外，在不存在种系BRCA1/2突变的情况下能够模拟这些缺陷的药物是一个活跃的研究领域，有望增加符合PARP抑制剂治疗条件的患者数量。美国食品药品监督管理局（FDA）批准的酪氨酸激酶抑制剂瑞戈非尼在无已知BRCA1/2突变的PDAC细胞中增强PARP抑制剂疗效的程度仍有待研究。

方法

采用彗星试验、细胞周期分析、蛋白质免疫印迹法以及H2AX免疫荧光检测来评估瑞戈非尼在PDAC细胞系中诱导DNA损伤的程度。通过细胞系中的膜联蛋白V/碘化丙啶（Annexin V/PI）共染色试验以及对小鼠肿瘤和人PDAC肿瘤的离体切片培养物中裂解的半胱天冬酶 - 3进行免疫组织化学染色，评估瑞戈非尼单独或与PARP抑制剂联合使用对PDAC细胞死亡的影响。基于流式细胞术的分析用于评估瑞戈非尼重编程PDAC肿瘤微环境的能力。

结果

我们现在表明，瑞戈非尼这种在多种胃肠道恶性肿瘤中有效的酪氨酸激酶抑制剂，可以增强奥拉帕利在胰腺癌中的反应。虽然瑞戈非尼诱导DNA损伤并限制PDAC细胞修复损伤的能力，但瑞戈非尼本身并不诱导细胞凋亡。然而，瑞戈非尼与奥拉帕利联合使用在体外、荷瘤小鼠以及人PDAC肿瘤的离体切片培养物中进一步诱导DNA损伤，与单独使用奥拉帕利相比，导致细胞凋亡增加。值得注意的是，我们表明联合治疗的疗效不依赖于细胞溶解性T细胞。