| Literature DB >> 30204432 |
Nikos K Karamanos1,2, Zoi Piperigkou1,2, Achilleas D Theocharis1, Hideto Watanabe3, Marco Franchi4, Stéphanie Baud5, Stéphane Brézillon6, Martin Götte7, Alberto Passi8, Davide Vigetti8, Sylvie Ricard-Blum9, Ralph D Sanderson10, Thomas Neill11, Renato V Iozzo11.
Abstract
The extracellular matrix (ECM) constitutes a highly dynamic three-dimensional structural network comprised of macromolecules, such as proteoglycans/glycosaminoglycans (PGs/GAGs), collagens, laminins, fibronectin, elastin, other glycoproteins and proteinases. In recent years, the field of PGs has expanded rapidly. Due to their high structural complexity and heterogeneity, PGs mediate several homeostatic and pathological processes. PGs consist of a protein core and one or more covalently attached GAG chains, which provide the protein cores with the ability to interact with several proteins. The GAG building blocks of PGs significantly influence the chemical and functional properties of PGs. The primary goal of this comprehensive review is to summarize major achievements and paradigm-shifting discoveries made on the PG/GAG chemistry-biology axis, focusing on structural variability, structure-function relationships, metabolic, molecular, and epigenetic mechanisms underlying their synthesis. Recent insights related to exosome biogenesis, degradation, and cell signaling, their status as diagnostic tools and potential pharmacological targets in diseases as well as current applications in nanotechnology and biotechnology are addressed. Moreover, issues related to docking studies, molecular modeling, GAG/PG interaction networks, and their integration are discussed.Entities:
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Year: 2018 PMID: 30204432 DOI: 10.1021/acs.chemrev.8b00354
Source DB: PubMed Journal: Chem Rev ISSN: 0009-2665 Impact factor: 60.622