PO.ET03.08 · 实验与分子治疗

Prolonged KRAS-MAPK inhibition activates interferon signaling to promote cellular plasticity and uncover novel targets for combination therapy

海报缩略图:Prolonged KRAS-MAPK inhibition activates interferon signaling to promote cellular plasticity and uncover novel targets for combination therapy
编号 1874 展板 7 时间 4/20 09:00–12:00 区域 Section 19 主讲 Ashenafi Bulle, DVM;PhD
分会场 Targeting Drug Resistance 2: RAS Signaling
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作者与单位

Ashenafi Shiferaw Bulle1, Yali Chen1, Huaping Li1, Hung-Po Chen1, Iftikhar Ali Khawar1, Lin Li1, Yu Wang1, Peng Liu1, Vikas Kumar Somani1, Richard Kurupi1, Sapana Prakashrao Bansod1, Son Bang Le2, Marianna Ruzinova1, David D Tran2, Kian-Huat Lim1

1Washington University School of Medicine, Saint Louis, MO,2Keck School of Medicine of USC, Los Angeles, CA

摘要 Abstract

KRAS-MAPK cascade inhibition shows promise for treating PDAC. However, resistance arises through secondary mutations that restore MAPK signaling and trigger epithelial-to-mesenchymal transition (EMT), key mechanisms of acquired resistance. Here, we show that human PDAC specimens and cells treated long-term with an ERK inhibitor exhibit upregulation of EMT and interferon signaling, with similar pattern also seen following prolonged KRAS inhibition in PDAC cells. Using the GeneRep-nSCORE framework, we identified TRIM22, an interferon-inducible E3 ubiquitin ligase, as a key mediator of EMT and resistance by promoting proteasomal degradation of IκBalpha and activating NF-κB signaling. Searching for druggable targets, we found TACSTD2 (TROP2), an NF-κB target gene upregulated after EMT. Combining ulixertinib or the KRAS inhibitor MRTX1133 with the TROP2-directed antibody-drug conjugate sacituzumab govitecan effectively suppressed growth of PDAC patient-derived xenografts. This study highlights TRIM22's role in linking interferon signaling with EMT and identifies TROP2 as a therapeutic vulnerability to overcome acquired resistance.
利益披露 Disclosure
A. S. Bulle, None.. Y. Chen, None.. H. Li, None.. H. Chen, None.. I. Khawar, None.. L. Li, None.. Y. Wang, None.. P. Liu, None.. V. K. Somani, None.. R. Kurupi, None.. S. P. Bansod, None.. S. Le, None.. M. Ruzinova, None.. D. Tran, None.. K. Lim, None.

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