Enhancing Anti-PD-1 Immunotherapy by Targeting MDSCs via Hepatic Arterial Infusion in Breast Cancer Liver Metastases.

IF 4.5 2区 医学 Q1 ONCOLOGY Cancers Pub Date : 2024-11-03 DOI:10.3390/cancers16213711
Minhyung Kim, Colin A Powers, Daniel T Fisher, Amy W Ku, Nickolay Neznanov, Alfiya F Safina, Jianmin Wang, Avishekh Gautam, Siddharth Balachandran, Anuradha Krishnamurthy, Katerina V Gurova, Sharon S Evans, Andrei V Gudkov, Joseph J Skitzki
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Abstract

Background: Surgery, chemotherapy, and radiation often have limited utility for advanced metastatic disease in the liver, and despite its promising activity in select cancers, PD-1 blockade therapy similarly has minimal benefit in this setting. Curaxin, CBL0137, is an experimental anti-cancer drug that disrupts the binding of DNA to histones, destabilizes chromatin, and induces Z-DNA formation which may stimulate anti-tumor immune responses.

Methods: Murine cell lines of colon (CT26) and breast (4T1) cancer were interrogated for survival and CBL0137-associated DNA changes in vitro. Immunocompetent models of liver metastases followed by CBL0137 hepatic arterial infusion (HAI) were used to examine in vivo tumor cell DNA alterations, treatment responses, and the immune contexture associated with CBL0137, both alone and in combination with anti-PD-1 therapy.

Results: CBL0137 induced immediate changes to favor tumor cell death in vitro and in vivo with an efficient tumor uptake via the HAI route. Toxicity to CBL0137 was minimal and anti-tumor treatment effects were more efficient with HAI compared to intravenous delivery. Immune effects were pronounced with CBL0137 HAI with concurrent depletion of a specific population of myeloid-derived suppressor cells and maintenance of effector T cell populations.

Conclusions: Combination of CBL0137 HAI with PD-1 blockade improved survival in 4T1 tumors but not in CT26 tumors, and therapeutic efficacy relies on the finding of simultaneous and targeted depletion of myeloid-derived suppressor cells and skewing of T cell populations to produce synergy with PD-1 blockade therapy.

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在乳腺癌肝转移中通过肝动脉灌注靶向 MDSCs 加强抗 PD-1 免疫疗法
背景:手术、化疗和放疗对肝脏晚期转移性疾病的作用往往有限,尽管PD-1阻断疗法在某些癌症中具有良好的活性,但在这种情况下也同样收效甚微。Curaxin(CBL0137)是一种实验性抗癌药物,它能破坏 DNA 与组蛋白的结合,破坏染色质的稳定性,并诱导 Z-DNA 的形成,从而刺激抗肿瘤免疫反应:方法:对结肠癌(CT26)和乳腺癌(4T1)的小鼠细胞系进行了体外生存和 CBL0137 相关 DNA 变化的检测。方法:研究结肠癌(CT26)和乳腺癌(4T1)小鼠细胞系在体外的存活率和与 CBL0137 相关的 DNA 变化,并使用免疫功能正常的肝转移模型进行 CBL0137 肝动脉灌注(HAI),以检测体内肿瘤细胞 DNA 变化、治疗反应以及与 CBL0137 相关的免疫环境,包括单独使用和与抗 PD-1 疗法联合使用:结果:CBL0137在体外和体内都能立即诱导肿瘤细胞死亡,并通过HAI途径被肿瘤有效吸收。与静脉给药相比,CBL0137 的毒性极小,而且通过 HAI 给药的抗肿瘤治疗效果更有效。CBL0137 HAI的免疫效果显著,同时消耗了特定的髓源性抑制细胞群,维持了效应T细胞群:CBL0137 HAI与PD-1阻断疗法联合使用可提高4T1肿瘤患者的生存率,但不能提高CT26肿瘤患者的生存率,疗效取决于是否能同时靶向消耗髓源性抑制细胞,并使T细胞群倾斜,从而与PD-1阻断疗法产生协同作用。
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来源期刊
Cancers
Cancers Medicine-Oncology
CiteScore
8.00
自引率
9.60%
发文量
5371
审稿时长
18.07 days
期刊介绍: Cancers (ISSN 2072-6694) is an international, peer-reviewed open access journal on oncology. It publishes reviews, regular research papers and short communications. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced.
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