PO.ET03.04 · 实验与分子治疗

OC201 and OC202e, an AI-driven drug combination, enhance the susceptibility of pancreatic cancer to FOLFIRINOX by modulating HIF-1alpha

海报缩略图:OC201 and OC202e, an AI-driven drug combination, enhance the susceptibility of pancreatic cancer to FOLFIRINOX by modulating HIF-1alpha
编号 3106 展板 6 时间 4/20 02:00–05:00 区域 Section 17 主讲 Sewon Kim
分会场 Overcoming Chemotherapy Resistance
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作者与单位

Yongjin Kim, Sewon Kim, Dong Sub Jung, So Jung Sung, Yenny Kim, Ki Sung Song, Hyemin Won, Yi Rang Kim, Jihoon Kang

Oncocross Co., Ltd, Seoul, Korea, Republic of

摘要 Abstract

Objective: Pancreatic cancer remains highly lethal, with a five-year survival rate of ~13%, largely due to late-stage diagnosis, aggressive progression, and resistance to standard therapies. Although FOLFIRINOX is the current first-line regimen, therapeutic resistance limits its durability. Our previous work showed that the AI-derived combination OC201 and OC202e suppresses EMT and metastasis. This study investigated whether OC201/OC202e enhances the response to FOLFIRINOX by modulating multidrug-resistance mechanisms. Methods: Panc-1 and MIA PaCa-2 cells were treated with OC201 and/or OC202e followed by FOLFIRINOX. Cell viability and clonogenic potential were assessed using MTT and colony-formation assays. Multidrug-resistance determinants-including hypoxia, extracellular matrix factors, dysregulated signaling, genetic alterations, stemness, and ABC transporters were analyzed by Western blotting and RT-qPCR. Stemness was further evaluated using sphere-formation assays. An in vivo hepatic metastasis model was established via intrasplenic injection of Panc-1 cells, followed by 10 weeks of treatment with OC201, OC202e, and/or FOLFIRINOX beginning two weeks post-injection. Metastatic burden was quantified histologically. Results: OC201/OC202e significantly enhanced FOLFIRINOX efficacy, as shown by reduced colony formation in both cell lines, while MTT assays indicated limited short-term synergy, suggesting a primarily long-term effect. In vivo, the combination further reduced hepatic metastatic lesions compared with FOLFIRINOX alone. Mechanistic analyses revealed decreased HIF-1alpha and stemness markers (CD44, Flotillin2) following combination treatment. HIF-1alpha expression correlated with stemness and FOLFIRINOX responsiveness, supporting its role in resistance. These findings align with the known EMT-stemness link and provide mechanistic insight into the observed synergy. Conclusion: The AI-derived OC201/OC202e combination enhances sensitivity to FOLFIRINOX and suppresses metastasis by targeting HIF-1alpha and the EMT-stemness axis. Reductions in clonogenicity and resistance-related markers highlight its potential as an adjuvant to standard chemotherapy and underscore the promise of AI-guided strategies for developing synergistic therapeutic combinations.
利益披露 Disclosure
Y. Kim, None.. S. Kim, None.. D. Jung, None.. S. Sung, None.. Y. Kim, None.. K. Song, None.. H. Won, None.. Y. Kim, None.. J. Kang, None.

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