Plectin in cancer: From biomarker to therapeutic target

Abstract

The cytolinker and scaffolding protein, plectin, has emerged as a potent driver of malignant hallmarks in many human cancers due to its involvement in various cellular activities contrib-uting to tumorigenesis, including cancer cell proliferation, adhesion, migration, invasion, and signal transduction. Evidence shows that beyond plectin’s diverse protein interactome, its cancer‐specific mislocalization to the cell surface enables its function as a potent oncoprotein. As such, therapeutic targeting of plectin, its protein interactors, and, in particular, cancer‐specific plectin (CSP) presents an attractive opportunity to impede carcinogenesis directly. Here, we report on plectin’s differential gene and protein expression in cancer, explore its mutational profile, and discuss the current under-standing of plectin’s and CSP’s biological function in cancer. Moreover, we review the landscape of plectin as a prognostic marker, diagnostic biomarker, and target for imaging and therapeutic mo-dalities. We highlight how, beyond their respective biological importance, plectin’s common over-expression in cancer and CSP’s cancer‐specific bioavailability underscore their potential as high-value druggable targets. We discuss how recent evidence of the potent anti‐cancer effects of CSP therapeutic targeting opens the door for cell‐surface mislocalized proteins as novel therapeutic tar-gets.