Literature DB >> 27246700

Identification of Novel N-Glycosylation Sites at Noncanonical Protein Consensus Motifs.

Mark S Lowenthal1, Kiersta S Davis1, Trina Formolo1, Lisa E Kilpatrick1, Karen W Phinney1.   

Abstract

N-glycosylation of proteins is well known to occur at n class="Chemical">asparagine residues that fall within the canonical consensus sequence N-X-S/T but has also been identified at a small number of asparagine residues within N-X-C motifs, including the N491 residue of human serotransferrin. Here we report novel glycosylation sites within noncanonical consensus motifs, in the conformation N-X-C, based on mass spectrometry analysis of partially deglycosylated glycopeptide targets. Alpha-1-acid glycoprotein (A1AG) and serotransferrin (Tf) were observed for the first time to be N-glycosylated on asparagine residues within a total of six unique noncanonical motifs. N-glycosylation was initially predicted in silico based on the evolutionary conservation of the N-X-C motif among related mammalian species and demonstrated experimentally in A1AG from porcine, canine, and feline sources and in human serotransferrin. High-resolution liquid chromatography-tandem mass spectrometry was employed to collect fragmentation data of predicted GlcNAcylated peptides and to assign modification sites within N-X-C motifs. A combination of targeted analytical techniques that includes complementary mass spectrometry platforms, enzymatic digestions, and partial-deglycosylation procedures was developed to confirm the novel observations. Additionally, we found that A1AG in porcine and canine sources is highly N-glycosylated at a noncanonical motif (N-Q-C) based on semiquantitative multiple reaction monitoring analysis-the first report of an N-X-C motif exhibiting substantial N-glycosylation. Although reports of N-X-C motif N-glycosylation are relatively uncommon in the literature, this work adds to a growing list of glycoproteins reported with glycosylation at various forms of noncanonical motifs.

Entities:  

Keywords:  A1AG; LC−MS/MS; N-X-C; N-glycosylation; consensus motif; evolutionary conservation; mass spectrometry; noncanonical glycosylation; transferrin

Mesh:

Substances:

Year:  2016        PMID: 27246700      PMCID: PMC5100817          DOI: 10.1021/acs.jproteome.5b00733

Source DB:  PubMed          Journal:  J Proteome Res        ISSN: 1535-3893            Impact factor:   4.466


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