Olaparib and Radiotherapy Induce Type I Interferon- and CD8+ T Cell-Dependent Sensitization to Immunotherapy in Pancreatic Cancer.

IF 5.3 2区 医学 Q1 ONCOLOGY
Victoria M Valvo, Qiang Zhang, Long Jiang, Erin A Holcomb, Ashley N Pearson, Anna G Edmunds, Hailey G Faulkner, Jadyn G James, Akshay Tate, Amanda K Huber, Zhuwen Wang, Yupei Guo, David Karnak, Leslie A Parsels, Joshua D Parsels, Yu L Lei, Alnawaz Rehemtulla, Heng Lin, Eileen S Carpenter, Daniel R Wahl, Vaibhav Sahai, Theodore S Lawrence, Michael D Green, Meredith A Morgan
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Abstract

PARP inhibitors sensitize pancreatic ductal adenocarcinoma (PDAC) to radiation by inducing DNA damage and replication stress. These mechanisms also have the potential to enhance radiation-induced type I interferon (T1IFN)-mediated antitumoral immune responses. We hypothesized that the PARP inhibitor olaparib would also potentiate radiation-induced T1IFN to promote antitumor immune responses and sensitization of otherwise resistant PDAC to immunotherapy. To test this hypothesis, we assessed the effects of olaparib and radiation on T1IFN production and sensitivity to αPD-L1 immunotherapy, as well as on the tumor microenvironment by single-cell RNA sequencing. We found that olaparib enhanced T1IFN production after radiation and had superior therapeutic efficacy in immunocompetent models. Olaparib and radiation treatment sensitized PDAC tumors to αPD-L1, resulting in decreased tumor burden and a 33% complete response rate. Combination treatment provided durable immune responses as shown by tumor rejection upon tumor rechallenge of previously cured mice. Furthermore, single-cell RNA sequencing analysis revealed that combination treatment induced an immunogenic tumor microenvironment characterized by interferon (IFN) responses in both PDAC and myeloid cell populations, macrophage polarization, and increased CD8+ terminal effector T-cell frequency and activity, findings which were confirmed by IHC and flow cytometry. Furthermore, CD8+ T cells and T1IFN signaling were required for therapeutic efficacy as host depletion of CD8+ T cells or the T1IFN receptor diminished treatment responses. Overall, our results indicate that olaparib enhances radiation-induced T1IFN-mediated immune signaling and subsequently an adaptive immune response, thus sensitizing pancreatic cancer to αPD-L1 therapy, supporting an ongoing clinical trial of this therapy in patients with PDAC.

PARP 抑制剂通过诱导 DNA 损伤和复制应激,使胰腺导管腺癌(PDAC)对辐射敏感。这些机制还有可能增强辐射诱导的 I 型干扰素(T1IFN)介导的抗肿瘤免疫反应。我们假设,PARP 抑制剂奥拉帕利也会增强辐射诱导的 T1IFN,从而促进抗肿瘤免疫反应,并使原本耐药的 PDAC 对免疫疗法敏感。为了验证这一假设,我们通过单细胞RNA测序评估了奥拉帕利和辐射对T1IFN产生和对αPD-L1免疫疗法敏感性的影响,以及对肿瘤微环境的影响。我们发现,奥拉帕利能增强放疗后T1IFN的产生,并在免疫功能正常的模型中具有更优越的疗效。奥拉帕利和放射治疗使PDAC肿瘤对αPD-L1敏感,从而减少了肿瘤负荷,完全应答率达到33%。联合治疗提供了持久的免疫反应,这体现在对先前治愈的小鼠进行肿瘤再挑战时出现的肿瘤排斥反应。此外,单细胞 RNA 测序分析表明,联合治疗诱导了一种免疫原性肿瘤微环境,其特征是 PDAC 和髓样细胞群中的干扰素(IFN)反应、巨噬细胞极化以及 CD8+ 末端效应 T 细胞频率和活性的增加,这些结果都得到了 IHC 和流式细胞术的证实。此外,CD8+ T细胞和T1IFN信号转导是疗效的必要条件,因为宿主CD8+ T细胞或T1IFN受体耗竭会降低治疗反应。总之,我们的研究结果表明,奥拉帕利能增强辐射诱导的 T1IFN 介导的免疫信号转导,进而增强适应性免疫反应,从而使胰腺癌对 αPD-L1 治疗敏感,支持正在进行的针对 PDAC 患者的临床试验。
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来源期刊
CiteScore
11.20
自引率
1.80%
发文量
331
审稿时长
3 months
期刊介绍: Molecular Cancer Therapeutics will focus on basic research that has implications for cancer therapeutics in the following areas: Experimental Cancer Therapeutics, Identification of Molecular Targets, Targets for Chemoprevention, New Models, Cancer Chemistry and Drug Discovery, Molecular and Cellular Pharmacology, Molecular Classification of Tumors, and Bioinformatics and Computational Molecular Biology. The journal provides a publication forum for these emerging disciplines that is focused specifically on cancer research. Papers are stringently reviewed and only those that report results of novel, timely, and significant research and meet high standards of scientific merit will be accepted for publication.
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