| Literature DB >> 31267558 |
Verena Paulitschke1,2,3, Ossia Eichhoff2, Christopher Gerner4, Philipp Paulitschke5, Andrea Bileck4, Thomas Mohr6, Phil F Cheng2, Alexander Leitner3, Emmanuella Guenova2, Ieva Saulite2, Sandra N Freiberger2, Anja Irmisch2, Bernhard Knapp7, Nina Zila1, Theodora-Pagona Chatziisaak2, Jürgen Stephan5, Joanna Mangana2, Rainer Kunstfeld1, Hubert Pehamberger1, Ruedi Aebersold3,8, Reinhard Dummer2, Mitchell P Levesque2.
Abstract
MAPK inhibitors (MAPKi) show outstanding clinical response rates in melanoma patients harbouring BRAF mutations, but resistance is common. The ability of melanoma cells to switch from melanocytic to mesenchymal phenotypes appears to be associated with therapeutic resistance. High-throughput, subcellular proteome analyses and RNAseq on two panels of primary melanoma cells that were either sensitive or resistant to MAPKi revealed that only 15 proteins were sufficient to distinguish between these phenotypes. The two proteins with the highest discriminatory power were PTRF and IGFBP7, which were both highly upregulated in the mesenchymal-resistant cells. Proteomic analysis of CRISPR/Cas-derived PTRF knockouts revealed targets involved in lysosomal activation, endocytosis, pH regulation, EMT, TGFβ signalling and cell migration and adhesion, as well as a significantly reduced invasive index and ability to form spheres in 3D culture. Overexpression of PTRF led to MAPKi resistance, increased cell adhesion and sphere formation. In addition, immunohistochemistry of patient samples showed that PTRF expression levels were a significant biomarker of poor progression-free survival, and IGFBP7 levels in patient sera were shown to be higher after relapse.Entities:
Keywords: zzm321990BRAFzzm321990; zzm321990PTRFzzm321990; mass spectrometry; melanoma; resistance
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Year: 2019 PMID: 31267558 PMCID: PMC6669927 DOI: 10.15252/embj.201695874
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598