How and why plants and human N-glycans are different: Insight from molecular dynamics into the "glycoblocks" architecture of complex carbohydrates

Beilstein J Org Chem. 2020 Aug 21:16:2046-2056. doi: 10.3762/bjoc.16.171. eCollection 2020.

Abstract

The N-glycosylation is one of the most abundant and diverse post-translational modifications of proteins, implicated in protein folding and structural stability, and mediating interactions with receptors and with the environment. All N-glycans share a common core from which linear or branched arms stem from, with functionalization specific to different species and to the cells' health and disease state. This diversity generates a rich collection of structures, all diversely able to trigger molecular cascades and to activate pathways, which also include adverse immunogenic responses. These events are inherently linked to the N-glycans' 3D architecture and dynamics, which remain for the large part unresolved and undetected because of their intrinsic structural disorder. In this work we use molecular dynamics (MD) simulations to provide insight into N-glycans' 3D structure by analysing the effects of a set of very specific modifications found in plants and invertebrate N-glycans, which are immunogenic in humans. We also compare these structural motifs and combine them with mammalian N-glycan motifs to devise strategies for the control of the N-glycan 3D structure through sequence. Our results suggest that the N-glycans' architecture can be described in terms of the local spatial environment of groups of monosaccharides. We define these "glycoblocks" as self-contained 3D units, uniquely identified by the nature of the residues they comprise, their linkages and structural/dynamic features. This alternative description of glycans' 3D architecture can potentially lead to an easier prediction of sequence-to-structure relationships in complex carbohydrates, with important implications in glycoengineering design.

Keywords: N-glycans; complex carbohydrates; fucose; glycoblocks; molecular dynamics; molecular recognition; xylose.

Grants and funding

The Irish Centre for High-End Computing (ICHEC) is gratefully acknowledged for generous allocation of computational resources. EF and CAF acknowledge the Irish Research Council (IRC) for funding through the Government of Ireland Postgraduate Scholarship Programme. EF and AMH acknowledge the John and Pat Hume Doctoral Scholarship Programme at Maynooth University for funding.