Calcipotriol Abrogates Cancer-associated Fibroblast-derived IL-8-mediated Oxaliplatin Resistance in Gastric Cancer Cells Via Blocking PI3K/Akt Signaling

Overview

Journal Acta Pharmacol Sin

Specialty Pharmacology

Date 2022 Jun 8

PMID 35676532

Authors

Zhen-Xiong Zhao

Yan-Qiu Zhang

Hui Sun

Zi-Qi Chen

Jin-Jia Chang

Xin Wang

Xu Wang

Cong Tan

Shu-Juan Ni

Wei-Wei Weng

Meng Zhang

Lei Wang

Dan Huang

Yun Feng

Wei-Qi Sheng

Mi-Die Xu

Affiliations

Soon will be listed here.

Abstract

Activation of vitamin D receptor (VDR) in cancer-associated fibroblasts (CAFs) has been implicated in hesitating tumor progression and chemoresistance of several human malignancies. Yet, the role of VDR in CAF-induced chemotherapy resistance of gastric cancer (GC) cells remains elusive. In this study we first conducted immunohistochemistry analysis on tissue microarrays including 88 pairs of GC and normal mucosa samples, and provided clinical evidence that VDR was mainly expressed in gastric mucous cells but almost invisible in CAFs, and VDR expression was negatively correlated with malignant clinical phenotype and advanced stages, low VDR expression confers to poor overall survival rate of patients with GC. In a co-culture system of primary CAFs and cancer cells, we showed that treatment of HGC-27 and AGS GC cells with VDR ligand calcipotriol (Cal, 500 nM) significantly inhibited CAF-induced oxaliplatin resistance. By using RNA-sequencing and Human Cytokine Antibody Array, we demonstrated that IL-8 secretion from CAFs induced oxaliplatin resistance via activating the PI3K/AKT pathway in GC, whereas Cal treatment greatly attenuated the tumor-supportive effect of CAF-derived IL-8 on GC cells. Taken together, this study verifies the specific localization of VDR in GC tissues and demonstrates that activation of VDR abrogates CAF-derived IL-8-mediated oxaliplatin resistance in GC via blocking PI3K/Akt signaling, suggesting vitamin D supplementation as a potential strategy of enhancing the anti-tumor effect of chemotherapy in GC.

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