| Literature DB >> 34645618 |
Sofian Al Shboul1,2, Olimpia E Curran3,4, Javier A Alfaro5,6, Fiona Lickiss6, Erisa Nita5, Jacek Kowalski6, Faris Naji7, Rudolf Nenutil8, Kathryn L Ball5, Radovan Krejcir8, Borivoj Vojtesek8, Ted R Hupp5,6, Paul M Brennan9,10.
Abstract
Better understanding of GBM signalling networks in-vivo would help develop more physiologically relevant ex vivo models to support therapeutic discovery. A "functional proteomics" screen was undertaken to measure the specific activity of a set of protein kinases in a two-step cell-free biochemical assay to define dominant kinase activities to identify potentially novel drug targets that may have been overlooked in studies interrogating GBM-derived cell lines. A dominant kinase activity derived from the tumour tissue, but not patient-derived GBM stem-like cell lines, was Bruton tyrosine kinase (BTK). We demonstrate that BTK is expressed in more than one cell type within GBM tissue; SOX2-positive cells, CD163-positive cells, CD68-positive cells, and an unidentified cell population which is SOX2-negative CD163-negative and/or CD68-negative. The data provide a strategy to better mimic GBM tissue ex vivo by reconstituting more physiologically heterogeneous cell co-culture models including BTK-positive/negative cancer and immune cells. These data also have implications for the design and/or interpretation of emerging clinical trials using BTK inhibitors because BTK expression within GBM tissue was linked to longer patient survival.Entities:
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Year: 2021 PMID: 34645618 PMCID: PMC8548209 DOI: 10.26508/lsa.202101054
Source DB: PubMed Journal: Life Sci Alliance ISSN: 2575-1077