| Literature DB >> 33409472 |
Paul V Murphy1, Antonio Romero2, Qi Xiao3,4, Anna-Kristin Ludwig5, Srinivas Jogula1, Nadezhda V Shilova6,7, Tanuja Singh8, Adele Gabba1, Bilal Javed4, Dapeng Zhang4, Francisco J Medrano2, Herbert Kaltner5, Jürgen Kopitz9, Nicolai V Bovin6, Albert M Wu8, Michael L Klein3, Virgil Percec4, Hans-Joachim Gabius5.
Abstract
The small 3-O-sulfated galactose head group of sulfatides, an abundant glycosphingolipid class, poses the (sphinx-like) riddle on involvement of glycan bridging by tissue lectins (sugar code). First, synthesis of head group derivatives for functionalization of amphiphilic dendrimers is performed. Aggregation of resulting (biomimetic) vesicles, alone or in combination with lactose, demonstrates bridging by a tissue lectin (galectin-4). Physiologically, this can stabilize glycolipid-rich microdomains (rafts) and associate sulfatide-rich regions with specific glycoproteins. Further testing documents importance of heterobivalency and linker length. Structurally, sulfatide recognition by galectin-8 is shown to involve sphingosine's OH group as substitute for the 3'-hydroxyl of glucose of lactose. These discoveries underscore functionality of this small determinant on biomembranes intracellularly and on the cell surface. Moreover, they provide a role model to examine counterreceptor capacity of more complex glycans of glycosphingolipids and to start their bottom-up glycotope surface programming.Entities:
Keywords: Biochemistry; Biophysics; Supramolecular Chemistry
Year: 2020 PMID: 33409472 PMCID: PMC7773886 DOI: 10.1016/j.isci.2020.101919
Source DB: PubMed Journal: iScience ISSN: 2589-0042