USP17 is required for trafficking and oncogenic signaling of mutant EGFR in NSCLC cells

Aidan P. McCann,Peter Smyth,Francesco Cogo,William J. McDaid,Lai Jiang,Jia Lin,Emma Evergren,Roberta Burden,Sandra Van Schaeybroeck,Christopher J. Scott,James F. Burrows

USP17 is required for trafficking and oncogenic signaling of mutant EGFR in NSCLC cells

2018

Aidan P. McCann
Peter Smyth
Francesco Cogo
William J. McDaid
Lai Jiang
Jia Lin
Emma Evergren
Roberta Burden
Sandra Van Schaeybroeck
Christopher J. Scott
James F. Burrows

Background The deubiquitinase USP17 is overexpressed in NSCLC and has been shown to be required for the growth and motility of EGFR wild-type (WT) NSCLC cells. USP17 is also required for clathrin-mediated endocytosis of EGFR. Here, we examine the impact of USP17 depletion on the growth, as well as EGFR endocytosis and signaling, of EGFR mutant (MT) NSCLC cells. In particular, we examine NSCLC cells harboring an EGFR activating exon 19 deletion (HCC827), or both the L858R activating mutation and the T790M resistance gatekeeper mutation (H1975) which renders them resistant to EGFR tyrosine kinase inhibitors (TKIs).

Keywords:

Cell biology
Exon
T790M
Epidermal growth factor receptor
Endocytosis
Motility
Mutant
Biology
Mutation
Receptor

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