Co-inhibition of RAGE and TLR4 sensitizes pancreatic cancer to irreversible electroporation in mice by disrupting autophagy.

IF 6.9 1区医学 Q1 CHEMISTRY, MULTIDISCIPLINARY

Acta Pharmacologica Sinica Pub Date : 2025-06-01 Epub Date: 2025-02-14 DOI:10.1038/s41401-025-01487-w

Cui-Fang Ye, Jia-di Wu, Lin-Rong Li, Shu-Guo Sun, Yu-Gang Wang, Tian-An Jiang, Xin Long, Jun Zhao

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引用次数: 0

Abstract

Irreversible electroporation (IRE) is a local ablative treatment for patients with pancreatic cancer. During the IRE procedure, high-intensity electric pulses are released intratumorally to disrupt plasma membranes and induce cell death. Since the intensity of the pulsed electric field (PEF) can be decreased by the tumor microenvironment, some cancer cells are subjected to a sublethal PEF and may survive to cause tumor recurrence later. Autophagy activation induced by anticancer therapies is known to promote treatment resistance. In this study, we investigated whether autophagy is activated in residual cancer cells after IRE and assessed the roles it plays during tumor recurrence. Subcutaneous KPC-A548 or Panc02 murine pancreatic cancer cell line xenograft mouse models were established; once the tumors reached 7 mm in one dimension, the tumor-bearing mice were subjected to IRE. For in vitro sublethal PEF treatment, the pancreatic cancer cell suspension was in direct contact with the electrodes and pulsed at room temperature. We showed that autophagy was activated in surviving residual cells, as evidenced by increased expression of LC3 and p62. Suppression of autophagy with hydroxychloroquine (60 mg/kg, daily intraperitoneal injection) markedly increased the efficacy of IRE. We demonstrated that autophagy activation can be attributed to increased expression of high-mobility group box 1 (HMGB1); co-inhibition of two HMGB1 receptors, receptor for advanced glycosylation end products (RAGE) and Toll-like receptor 4 (TLR4), suppressed autophagy activation by upregulating the PI3K/AKT/p70 ribosomal S6 protein kinase (p70S6K) axis and sensitized pancreatic cancer cells to PEF. We prepared a polymeric micelle formulation (M-R/T) encapsulating inhibitors of both RAGE and TLR4. The combination of IRE and M-R/T (equivalent to RAGE inhibitor at 10.4 mg/kg and TLR4 inhibitor at 5.7 mg/kg, intravenous or intraperitoneal injection every other day) significantly promoted tumor apoptosis, suppressed cell cycle progression, and prolonged animal survival in pancreatic tumor models. This study suggests that disruption of HMGB1-mediated autophagy with nanomedicine is a promising strategy to enhance the response of pancreatic cancer to IRE.

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RAGE和TLR4的共同抑制通过破坏自噬使小鼠胰腺癌对不可逆电穿孔致敏。

不可逆电穿孔（IRE）是胰腺癌患者的一种局部消融治疗方法。在IRE过程中，肿瘤内释放高强度电脉冲以破坏质膜并诱导细胞死亡。由于脉冲电场（PEF）的强度可以被肿瘤微环境降低，一些癌细胞遭受亚致死的脉冲电场，并可能存活并引起肿瘤复发。已知抗癌治疗诱导的自噬激活可促进治疗耐药性。在本研究中，我们研究了IRE后残留癌细胞中自噬是否被激活，并评估了自噬在肿瘤复发中的作用。皮下建立KPC-A548或Panc02小鼠胰腺癌细胞系异种移植小鼠模型；当肿瘤在一维上达到7mm时，对荷瘤小鼠进行IRE。对于体外亚致死PEF治疗，胰腺癌细胞悬液与电极直接接触并在室温下脉冲。我们发现自噬在存活的残余细胞中被激活，LC3和p62的表达增加就是证据。羟氯喹（60 mg/kg，每日腹腔注射）抑制自噬可显著提高IRE的疗效。我们证明自噬激活可归因于高迁移率组框1 （HMGB1）的表达增加；共抑制两种HMGB1受体，晚期糖基化终产物受体（RAGE）和toll样受体4 (TLR4)，通过上调PI3K/AKT/p70核糖体S6蛋白激酶（p70S6K）轴抑制自噬激活，并使胰腺癌细胞对PEF敏感。我们制备了一种包封RAGE和TLR4抑制剂的聚合物胶束制剂（M-R/T）。在胰腺肿瘤模型中，IRE联合M-R/T（相当于RAGE抑制剂10.4 mg/kg和TLR4抑制剂5.7 mg/kg，每隔一天静脉或腹腔注射）显著促进肿瘤凋亡，抑制细胞周期进展，延长动物生存期。这项研究表明，纳米药物破坏hmgb1介导的自噬是增强胰腺癌对IRE反应的一种有希望的策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Acta Pharmacologica Sinica 医学-化学综合

CiteScore

15.10

自引率

2.40%

发文量

4365

审稿时长

2 months

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