Knockdown of GnT-Va expression inhibits ligand-induced downregulation of the epidermal growth factor receptor and intracellular signaling by inhibiting receptor endocytosis

doi:10.1093/glycob/cwp023

Glycobiology Advance Access originally published online on February 18, 2009
Glycobiology 2009 19(5):547-559; doi:10.1093/glycob/cwp023

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Knockdown of GnT-Va expression inhibits ligand-induced downregulation of the epidermal growth factor receptor and intracellular signaling by inhibiting receptor endocytosis

Hua-Bei Guo², Heather Johnson², Matthew Randolph², Intaek Lee³ and Michael Pierce¹^,2

² Department of Biochemistry and Molecular Biology, Complex Carbohydrate Research Center, University of Georgia, Athens, GA, 30602
³ Department of Cell Biology, Yale University School of Medicine, New Haven, CT 06510 USA

¹ To whom correspondence should be addressed: Tel: +1-706-542-1701; Fax: +1-706-542-1759; e-mail: hawkeye{at}uga.edu

Received on December 20, 2008; revised on February 7, 2009; accepted on February 12, 2009

Changes in the expression of N-glycan branching glycosyltransferasescan alter cell surface receptor functions, involving their levelsof cell surface retention, rates of internalization into theendosomal compartment, and subsequent intracellular signaling.To study in detail the regulation of signaling of the EGF receptor(EGFR) by GlcNAcβ(1,6)Man branching, we utilized specificsiRNA to selectively knockdown GnT-Va expression in the highlyinvasive human breast carcinoma line MDA-MB231, which resultedin the attenuation of its invasiveness-related phenotypes. Comparedto control cells, ligand-induced downregulation of EGFR wassignificantly inhibited in GnT-Va-suppressed cells. This effectcould be reversed by re-expression of GnT-Va, indicating thatchanges in ligand-induced receptor downregulation were dependenton GnT-Va activity. Knockdown of GnT-Va had no significant effecton c-Cbl mediated receptor ubiquitination and degradation, butdid cause the inhibition of receptor internalization, showingthat altered signaling and delayed ligand-induced downregulationof EGFR expression resulted from decreased EGFR endocytosis.Similar results were obtained with HT1080 fibrosarcoma cellstreated with GnT-Va siRNA. Inhibited receptor internalizationcaused by the expression of GnT-Va siRNA appeared to be independentof galectin binding since decreased EGFR internalization inthe knockdown cells was not affected by the treatment of thecells with lactose, a galectin inhibitor. Our results show thatdecreased GnT-Va activity due to siRNA expression in human carcinomacells inhibits ligand-induced EGFR internalization, consequentlyresulting in delayed downstream signal transduction and inhibitionof the EGF-induced, invasiveness-related phenotypes.

Key words: EGFR / endocytosis / GnT-V / N-glycan

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