The heparan sulfate proteoglycan Syndecan‑1 influences local bone cell communication via the RANKL/ OPG axis

The heparan sulfate proteoglycan Syndecan-1, a mediator of signals between the extracellular matrix and cells involved is able to interact with OPG, one of the major regulators of osteoclastogenesis. The potential of osteoblasts to induce osteoclastogenesis is characterized by a switch of OPG (low o...

Verfasser: Timmen, Melanie
Hidding, Heriburg
Götte, Martin
Khassawna, Thaqif
Kronenberg, Daniel
Stange, Richard
Dokumenttypen:Artikel
Medientypen:Text
Erscheinungsdatum:2020
Publikation in MIAMI:06.03.2023
Datum der letzten Änderung:06.03.2023
Angaben zur Ausgabe:[Electronic ed.]
Quelle:Scientific Reports 10 (2020) 20510, 1-12
Schlagwörter:Cell biology; Developmental biology; Endocrinology; Molecular biology; Physiology; Stem cells;
Fachgebiet (DDC):610: Medizin und Gesundheit
Lizenz:CC BY 4.0
Sprache:Englisch
Förderung:Finanziert über die DEAL-Vereinbarung mit Wiley 2019-2022.
Förderer: Deutsche Forschungsgemeinschaft / Projektnummer: 194347757
Format:PDF-Dokument
URN:urn:nbn:de:hbz:6-51009694711
Weitere Identifikatoren:DOI: 10.17879/51009713986
Permalink:https://nbn-resolving.de/urn:nbn:de:hbz:6-51009694711
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  • Onlinezugriff:10.1038_s41598-020-77510-3.pdf

    The heparan sulfate proteoglycan Syndecan-1, a mediator of signals between the extracellular matrix and cells involved is able to interact with OPG, one of the major regulators of osteoclastogenesis. The potential of osteoblasts to induce osteoclastogenesis is characterized by a switch of OPG (low osteoclastogenic potential) towards RANKL production (high osteoclastogenic potential). In the present study, we investigated the influence of endogenous Syndecan-1 on local bone-cell-communication via the RANKL/OPG-axis in murine osteoblasts and osteoclasts in wild type and Syndecan-1 lacking cells. Syndecan-1 expression and secretion was increased in osteoblasts with high osteoclastogenic potential. Syndecan-1 deficiency led to increased OPG release by osteoblasts that decreased the availability of RANKL. In co-cultures of Syndecan-1 deficient osteoblasts with osteoclast these increased OPG in supernatant caused decreased development of osteoclasts. Syndecan-1 and RANKL level were increased in serum of aged WT mice, whereas Syndecan-1 deficient mice showed high serum OPG concentration. However, bone structure of Syndecan-1 deficient mice was not different compared to wild type. In conclusion, Syndecan-1 could be regarded as a new modulator of bone-cell-communication via RANKL/OPG axis. This might be of high impact during bone regeneration or bone diseases like cancer where Syndecan-1 expression is known to be even more prevalent.