Modulating autophagy to boost the antitumor efficacy of TROP2-directed antibody-drug conjugate in pancreatic cancer.

Caili Xu, Xiting Huang, Qinchao Hu, Wenjing Xue, Kaicheng Zhou, Xingxiu Li, Yanyang Nan, Dianwen Ju, Ziyu Wang, Xuyao Zhang
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Abstract

Pancreatic cancer, characterized by a dismal prognosis and limited treatment options, persists as a formidable challenge in oncology. Trophoblast cell surface antigen 2 (TROP2)-directed antibody-drug conjugates have achieved great success in solid tumors such as breast cancer and uroepithelial carcinoma. However, their efficacy against pancreatic cancer was insufficient in clinical trials, necessitating an imperative exploration of underlying mechanisms and new therapeutic strategies. In this study, we indicated that αTROP2-MMAE, an antibody-drug conjugate targeting TROP2, induced apoptosis through the caspase-9/PARP pathway and exerted potent antitumor effects against TROP2-positive pancreatic cancer. Simultaneously, RNA sequencing suggested significant changes in autophagy after αTROP2-MMAE treatment. The formation of autophagosomes and activation of autophagic flux were markedly induced through mechanisms associated with suppressing the activation of the Akt/mTOR pathway. The addition of pharmacological inhibitors of autophagy enhanced the cytotoxicity and apoptosis caused by αTROP2-MMAE, revealing the cytoprotective role of autophagy in TROP2-positive pancreatic cancer. In the subcutaneous xenograft model using BxPC3 cells, the combined administration of αTROP2-MMAE and an autophagy inhibitor elevated the tumor inhibition rate of αTROP2-MMAE from 71.6 % to 99.0 %, resulting in the eradication of tumors in half of the mice. Collectively, our research demonstrated for the first time the cytoprotective role of autophagy in TROP2-targeted antibody-drug conjugate therapy for pancreatic cancer, providing new perspectives for mechanistic exploration and therapeutic strategies in the treatment of pancreatic cancer.

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调节自噬,提高 TROP2 引导的抗体-药物共轭物在胰腺癌中的抗肿瘤疗效。
胰腺癌预后不佳,治疗方案有限,一直是肿瘤学领域的巨大挑战。滋养层细胞表面抗原 2(TROP2)导向的抗体药物共轭物在乳腺癌和尿路上皮癌等实体瘤方面取得了巨大成功。然而,在临床试验中,它们对胰腺癌的疗效并不理想,因此有必要探索其潜在机制和新的治疗策略。本研究表明,靶向TROP2的抗体-药物共轭物αTROP2-MMAE可通过caspase-9/PARP途径诱导细胞凋亡,对TROP2阳性胰腺癌有较强的抗肿瘤作用。同时,RNA 测序表明,αTROP2-MMAE 治疗后自噬发生了显著变化。通过抑制 Akt/mTOR 通路活化的相关机制,自噬体的形成和自噬通量的激活被明显诱导。添加自噬药理抑制剂可增强αTROP2-MMAE的细胞毒性和凋亡,从而揭示自噬在TROP2阳性胰腺癌中的细胞保护作用。在使用 BxPC3 细胞的皮下异种移植模型中,αTROP2-MMAE 和自噬抑制剂的联合用药可使 αTROP2-MMAE 的肿瘤抑制率从 71.6% 提高到 99.0%,从而使半数小鼠的肿瘤被根除。总之,我们的研究首次证明了自噬在TROP2靶向抗体-药物共轭物治疗胰腺癌中的细胞保护作用,为胰腺癌的机理探索和治疗策略提供了新的视角。
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