Microenvironment-Induced Non-sporadic Expression of the AXL and cKIT Receptors Are Related to Epithelial Plasticity and Drug Resistance

Tiina A Jokela; Agnete S T Engelsen; Agata Rybicka; Fanny A Pelissier Vatter; James C Garbe; Masaru Miyano; Crina Tiron; Dan Ferariu; Lars A Akslen; Martha R Stampfer; James B Lorens; Mark A LaBarge

doi:10.3389/fcell.2018.00041

Microenvironment-Induced Non-sporadic Expression of the AXL and cKIT Receptors Are Related to Epithelial Plasticity and Drug Resistance

Front Cell Dev Biol. 2018 Apr 17:6:41. doi: 10.3389/fcell.2018.00041. eCollection 2018.

Authors

Tiina A Jokela^{1

2}, Agnete S T Engelsen^{1

3}, Agata Rybicka¹, Fanny A Pelissier Vatter¹, James C Garbe⁴, Masaru Miyano², Crina Tiron⁵, Dan Ferariu⁵, Lars A Akslen³, Martha R Stampfer⁴, James B Lorens^{1

3}, Mark A LaBarge^{2

3

4}

Affiliations

¹ Department of Biomedicine, University of Bergen, Bergen, Norway.
² Department of Population Sciences, Center for Cancer and Aging, City of Hope, Duarte, CA, United States.
³ Centre for Cancer Biomarkers, University of Bergen, Bergen, Norway.
⁴ Biological Systems and Engineering Division, Lawrence Berkeley National Laboratory, Berkeley, CA, United States.
⁵ Regional Institute of Oncology, Iasi, Romania.

Abstract

The existence of rare cancer cells that sporadically acquire drug-tolerance through epigenetic mechanisms is proposed as one mechanism that drives cancer therapy failure. Here we provide evidence that specific microenvironments impose non-sporadic expression of proteins related to epithelial plasticity and drug resistance. Microarrays of robotically printed combinatorial microenvironments of known composition were used to make cell-based functional associations between microenvironments, which were design-inspired by normal and tumor-burdened breast tissues, and cell phenotypes. We hypothesized that specific combinations of microenvironment constituents non-sporadically impose the induction of the AXL and cKIT receptor tyrosine kinase proteins, which are known to be involved in epithelial plasticity and drug-tolerance, in an isogenic human mammary epithelial cell (HMEC) malignant progression series. Dimension reduction analysis reveals type I collagen as a dominant feature, inducing expression of both markers in pre-stasis finite lifespan HMECs, and transformed non-malignant and malignant immortal cell lines. Basement membrane-associated matrix proteins, laminin-111 and type IV collagen, suppress AXL and cKIT expression in pre-stasis and non-malignant cells. However, AXL and cKIT are not suppressed by laminin-111 in malignant cells. General linear models identified key factors, osteopontin, IL-8, and type VIα3 collagen, which significantly upregulated AXL and cKIT, as well as a plasticity-related gene expression program that is often observed in stem cells and in epithelial-to-mesenchymal-transition. These factors are co-located with AXL-expressing cells in situ in normal and breast cancer tissues, and associated with resistance to paclitaxel. A greater diversity of microenvironments induced AXL and cKIT expression consistent with plasticity and drug-tolerant phenotypes in tumorigenic cells compared to normal or immortal cells, suggesting a reduced perception of microenvironment specificity in malignant cells. Microenvironment-imposed reprogramming could explain why resistant cells are seemingly persistent and rapidly adaptable to multiple classes of drugs. These results support the notion that specific microenvironments drive drug-tolerant cellular phenotypes and suggest a novel interventional avenue for preventing acquired therapy resistance.

Keywords: AXL; MEMA; breast cancer; cKIT; drug resistance; epithelial plasticity; microenvironment.

Abstract

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