The yeast oligosaccharyltransferase complex can be replaced by STT3 from Leishmania major

doi:10.1093/glycob/cwn118

Glycobiology Advance Access originally published online on October 25, 2008
Glycobiology 2009 19(2):160-171; doi:10.1093/glycob/cwn118

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The yeast oligosaccharyltransferase complex can be replaced by STT3 from Leishmania major

Katrin Hese², Claudia Otto³, Françoise H Routier³ and Ludwig Lehle¹^,2

² Lehrstuhl für Zellbiologie und Pflanzenphysiologie, Universität Regensburg, Regensburg
³ Medizinische Hochschule Hannover, Zentrum Biochemie, Hannover, Germany

¹ To whom correspondence should be addressed: E-mail: ludwig.lehle{at}biologie.uni-regensburg.de

Received on September 25, 2008; revised on October 20, 2008; accepted on October 21, 2008

The key step of protein N-glycosylation is catalyzed by themultimeric oligosaccharyltransferase complex (OST). Biochemicaland genetic studies have revealed that OST from Saccharomycescerevisiae consists of nine subunits: Wbp1, Swp1, Stt3, Ost1,Ost2, Ost3, Ost4, Ost5, and Ost6. With the exception of Stt3,assumed to contain the catalytic site, little is known aboutthe function of other OST subunits. The existence of the OSTcomplex is suggested to allow substrate specificity and efficienttransfer, a close interaction with the translocon and the preventionof protein folding to ensure the efficient co-translationalmodification of proteins. However, in the recently completedgenome of the trypanosomatid parasite Leishmania major STT3(of which four paralogs exist, STT3-1, STT3-2, STT3-3, and STT3-4)is the only OST subunit that can be identified. Here we reportthat L.m.STT3 proteins, except STT3-3, are able to complementstt3 deficiency in yeast during vegetative growth, but onlypoorly during sporulation. By blue native electrophoresis wedemonstrate that the L.mSTT3 is active mainly as a free, monomericenzyme. In cell-free assays and also in vivo we find that L.mSTT3,expressed in yeast, has a broad specificity for nonglucosylatedlipid-linked mannose-oligosaccharides, typical for several protists.But when incorporated into the OST complex, L.mSTT3 transfersalso the common eukaryotic Glc₃Man₉GlcNAc₂-PP-Dol donor. Finally,three L.m.STT3 paralogs were shown to complement not only stt3but also ost1, ost2, wbp1, or swp1 mutants. Thus, STT3 fromLeishmania can substitute for the whole OST complex.

Key words: Leishmania / lipid-linked oligosaccharide / N-glycosylation / oligosaccharyltransferase / Saccharomyces

This paper is dedicated to Widmar Tanner on the occasion ofhis 70th birthday.

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