Irreversible JNK1-JUN inhibition by JNK-IN-8 sensitizes pancreatic cancer to 5-FU/FOLFOX chemotherapy
Matthew B. Lipner, … , Gary L. Johnson, Jen Jen Yeh
Matthew B. Lipner, … , Gary L. Johnson, Jen Jen Yeh
Published March 26, 2020
Citation Information: JCI Insight. 2020;5(8):e129905. https://doi.org/10.1172/jci.insight.129905.
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Research Article Oncology Therapeutics

Irreversible JNK1-JUN inhibition by JNK-IN-8 sensitizes pancreatic cancer to 5-FU/FOLFOX chemotherapy

Abstract

Over 55,000 people in the United States are diagnosed with pancreatic ductal adenocarcinoma (PDAC) yearly, and fewer than 20% of these patients survive a year beyond diagnosis. Chemotherapies are considered or used in nearly every PDAC case, but there is limited understanding of the complex signaling responses underlying resistance to these common treatments. Here, we take an unbiased approach to study protein kinase network changes following chemotherapies in patient-derived xenograft (PDX) models of PDAC to facilitate design of rational drug combinations. Proteomics profiling following chemotherapy regimens reveals that activation of JNK-JUN signaling occurs after 5-fluorouracil plus leucovorin (5-FU + LEU) and FOLFOX (5-FU + LEU plus oxaliplatin [OX]), but not after OX alone or gemcitabine. Cell and tumor growth assays with the irreversible inhibitor JNK-IN-8 and genetic manipulations demonstrate that JNK and JUN each contribute to chemoresistance and cancer cell survival after FOLFOX. Active JNK1 and JUN are specifically implicated in these effects, and synergy with JNK-IN-8 is linked to FOLFOX-mediated JUN activation, cell cycle dysregulation, and DNA damage response. This study highlights the potential for JNK-IN-8 as a biological tool and potential combination therapy with FOLFOX in PDAC and reinforces the need to tailor treatment to functional characteristics of individual tumors.

Authors

Matthew B. Lipner, Xianlu L. Peng, Chong Jin, Yi Xu, Yanzhe Gao, Michael P. East, Naim U. Rashid, Richard A. Moffitt, Silvia G. Herrera Loeza, Ashley B. Morrison, Brian T. Golitz, Cyrus Vaziri, Lee M. Graves, Gary L. Johnson, Jen Jen Yeh

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Figure 4

JNK-IN-8 enhances growth inhibition by FOLFOX in PDX organoids and tumors corresponding to sustained p-JUN inhibition.

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JNK-IN-8 enhances growth inhibition by FOLFOX in PDX organoids and tumor...
(A) Organoid viability by bright-field microscopy at 1-μM doses of indicated treatments (left) and quantified across a broad range of doses by CellTiter-Glo 3D with normalization to DMSO vehicle (right) in 319-T1 organoids (n = 2). Scale bars: 500 μm. (B) In vivo 319-T1 PDX tumor growth displayed as box plots of log2(tumor volume fold change at 28d endpoint versus treatment initiation) and Kaplan-Meier survival plots with a tumor volume cutoff of 800 mm3. Log transformed ratio of p-JUN/ACTB protein levels by immunoblot from the same 319-T1 PDX tumors harvested before and after 28d treatments of respective drug regimens. Data normalized to pretreatment biopsy tumors. ACTB used as loading control. (C) In vivo 411-T1 PDX tumor growth data and p-JUN inhibition by immunoblot as above. Each group contained at least 5 mice. Significance determined by 1-way ANOVA with Tukey multiple comparisons tests. *P < 0.05; **P < 0.01, ***P < 0.001.