Translational aspects in targeting the stromal tumour microenvironment: from bench to bedside

New Horiz Transl Med. 2016 Jan;3(1):9-21. doi: 10.1016/j.nhtm.2016.03.001.

Abstract

Solid tumours comprise, not only malignant cells but also a variety of stromal cells and extracellular matrix proteins. These components interact via an array of signalling pathways to create an adaptable network that may act to promote or suppress cancer progression. To date, the majority of anti-tumour chemotherapeutic agents have principally sought to target the cancer cell. Consequently, resistance develops because of clonal evolution, as a result of selection pressure during tumour expansion. The concept of activating or inhibiting other cell types within the tumour microenvironment is relatively novel and has the advantage of targeting cells which are genetically stable and less likely to develop resistance. This review outlines key players in the stromal tumour microenvironment and discusses potential targeting strategies that may offer therapeutic benefit.

Keywords: T cell; cancer; fibroblast; microRNA; microenvironment; prognostic; stroma; therapeutic; tumour.