Tumor microenvironment and epithelial mesenchymal transition as targets to overcome tumor multidrug resistance

Erin Nuray; Grahovac Jelena; Brozović Anamaria; Efferth Thomas

doi:10.1016/j.drup.2020.100715

Published June 25, 2020 | Version v.1

Journal article Open

Tumor microenvironment and epithelial mesenchymal transition as targets to overcome tumor multidrug resistance

1. Department of Pharmacology, School of Medicine, Antalya, Turkey
2. Laboratory for Experimental Pharmacology, Institute for Oncology and Radiology of Serbia, Belgrade, Serbia
3. Division of Molecular Biology, Ruđer Bošković Institute, Zagreb, Croatia
4. Department of Pharmaceutical Biology, Institute of Pharmaceutical and Biomedical Sciences, Johannes Gutenberg University, Mainz, Germany

It is well established that multifactorial drug resistance hinders successful cancer treatment. Tumor cell interactions with the tumor microenvironment (TME) are crucial in epithelial-mesenchymal transition (EMT) and multidrug resistance (MDR). TME-induced factors secreted by cancer cells and cancer-associated fibroblasts (CAFs) create an inflammatory microenvironment by recruiting immune cells. CD11b+/Gr-1+ myeloid-derived suppressor cells (MDSCs) and inflammatory tumor associated macrophages (TAMs) are main immune cell types which further enhance chronic inflammation. Chronic inflammation nurtures tumor-initiating/cancer stem-like cells (CSCs), induces both EMT and MDR leading to tumor relapses. Pro-thrombotic microenvironment created by inflammatory cytokines and chemokines from TAMs, MDSCs and CAFs is also involved in EMT and MDR. MDSCs are the most common mediators of immunosuppression and are also involved in resistance to targeted therapies, e.g. BRAF inhibitors and oncolytic viruses-based therapies. Expansion of both cancer and stroma cells causes hypoxia by hypoxia-inducible transcription factors (e.g. HIF-1α) resulting in drug resistance. TME factors induce the expression of transcriptional EMT factors, MDR and metabolic adaptation of cancer cells. Promoters of several ATP-binding cassette (ABC) transporter genes contain binding sites for canonical EMT transcription factors, e.g. ZEB, TWIST and SNAIL. Changes in glycolysis, oxidative phosphorylation and autophagy during EMT also promote MDR. Conclusively, EMT signaling simultaneously increases MDR. Owing to the multifactorial nature of MDR, targeting one mechanism seems to be non-sufficient to overcome resistance. Targeting inflammatory processes by immune modulatory compounds such as mTOR inhibitors, demethylating agents, low-dosed histone deacetylase inhibitors may decrease MDR. Targeting EMT and metabolic adaptation by small molecular inhibitors might also reverse MDR. In this review, we summarize evidence for TME components as causative factors of EMT and anticancer drug resistance.

Notes

This article is based upon work from COST Action 17104 STRATAGEM, supported by COST (European Cooperation in Science and Technology).Funding: NE is supported by grant no:118S378 from TUBITAK (The Scientific and Technological Research Council of Turkey);JG is supported by the grant III41026 from the Serbian Ministry of Education, Science and Technological Development. AB is supported by the Croatian Science Foundation (CSF, Project No. IP-2016-06-1036). TE is grateful for funding by the Germany Science Foundation (DFG), the German Cancer Aid, the Chinese Scholarship Council (CSC), and the German Academic Exchange Service (DAAD).

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