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Role of sialylation of N-linked glycans in prion pathogenesis. | LitMetric

Role of sialylation of N-linked glycans in prion pathogenesis.

Cell Tissue Res

Center for Biomedical Engineering and Technology and Department of Anatomy and Neurobiology, University of Maryland School of Medicine, Baltimore, MD, 21201, USA.

Published: April 2023

AI Article Synopsis

Article Abstract

Mammalian prion or PrP is a proteinaceous infectious agent that consists of a misfolded, self-replicating state of the prion protein or PrP. PrP and PrP are posttranslationally modified with N-linked glycans, which are sialylated at the terminal positions. More than 30 years have passed since the first characterization of the composition and structural diversity of N-linked glycans associated with the prion protein, yet the role of carbohydrate groups that constitute N-glycans and, in particular, their terminal sialic acid residues in prion disease pathogenesis remains poorly understood. A number of recent studies shed a light on the role of sialylation in the biology of prion diseases. This review article discusses several mechanisms by which terminal sialylation dictates the spread of PrP across brain regions and the outcomes of prion infection in an organism. In particular, relationships between the sialylation status of PrP and important strain-specific features including lymphotropism, neurotropism, and neuroinflammation are discussed. Moreover, emerging evidence pointing out the roles of sialic acid residues in prion replication, cross-species transmission, strain competition, and strain adaptation are reviewed. A hypothesis according to which selective, strain-specified recruitment of PrP sialoglycoforms dictates unique strain-specific disease phenotypes is examined. Finally, the current article proposes that prion strains evolve as a result of a delicate balance between recruiting highly sialylated glycoforms to avoid an "eat-me" response by glia and limiting heavily sialylated glycoforms for enabling rapid prion replication.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9329487PMC
http://dx.doi.org/10.1007/s00441-022-03584-2DOI Listing

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