Unexpected Basis for Impaired Glc3Man9GlcNAc2-P-P-Dolichol Biosynthesis by Elevated Expression of GlcNAc-1-P Transferase

doi:10.1093/glycob/cwm109

Glycobiology Advance Access originally published online on October 3, 2007
Glycobiology 2008 18(1):125-134; doi:10.1093/glycob/cwm109

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Unexpected Basis for Impaired Glc₃Man₉GlcNAc₂-P-P-Dolichol Biosynthesis by Elevated Expression of GlcNAc-1-P Transferase

Ningguo Gao², Jie Shang² and Mark A Lehrman¹^,2

² Department of Pharmacology, University of Texas Southwestern Medical Center, 6001 Forest Park Road, Dallas, TX 75390-9041, USA

¹ To whom correspondence should be addressed: Tel: +214-645-6172; Fax: +214-645-6173; e-mail: mark.lehrman{at}utsouthwestern.edu

Received on August 17, 2007; revised on September 29, 2007; accepted on September 30, 2007

GlcNAc-1-P transferase (GPT) transfers GlcNAc-1-P from UDP-GlcNActo dolichol-P (Dol-P), forming GlcNAc-P-P-Dol to initiate synthesisof the lipid-linked oligosaccharide Glc₃Man₉GlcNAc₂-P-P-dolichol(G₃M₉Gn₂-P-P-Dol). Elevated expression of GPT in CHO-K1 cellsis known to cause accumulation of the intermediate M₅Gn₂-P-P-Dol,presumably by excessively consuming Dol-P and thereby hinderingDol-P-dependent synthesis of Man-P-Dol (MPD) and Glc-P-Dol (GPD),which provide the residues for extending M₅Gn₂-P-P-Dol to G₃M₉Gn₂-P-P-Dol.If so, elevated GPT expression should increase oligosaccharide-P-P-Dolquantities and reduce monosaccharide-P-Dol quantities, whilerequiring GPT enzymatic activity. Here we report that elevatedGPT expression failed to appreciably alter the quantities ofthe two classes of dolichol-linked saccharide, and that neithera GPT inhibitor nor introduction of an inactivating mutationinto GPT prevented M₅Gn₂-P-P-Dol accumulation, arguing againstexcessive Dol-P consumption. Unexpectedly, we noticed similaritiesbetween the phenotypes of GPT overexpressers and of CHO-K1 cellslacking Lec35p (encoded by MPDU1, the congenital disorder ofglycosylation (CDG)-If locus), which is required for utilizationof MPD and GPD. By compensatory overexpression of Lec35p, G₃M₉Gn₂-P-P-Dolsynthesis in GPT overexpressers could be restored. However,GPT overexpression did not affect the levels of Lec35 mRNA orprotein. These results suggest that GPT may impair Lec35p function,and imply that upper as well as lower limits on GPT expressionexist in normal cells. Since the mammalian GPT gene can undergospontaneous amplification, the data also indicate a potentialbasis for forms of pseudo-CDG-If.

Key words: congenital disorder of glycosylation / dolichol / GPT / Lec35 / lipid-linked oligosaccharide

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