• Salbach-Hirsch, Juliane
• Schnabelrauch, Matthias
• Rademann, Jörg
• Rother, Sandra
• Balamurugan, Kanagasabai
• Pählig, Sophie
• Köhler, Linda
• Dürig, Jan Niklas
• Hofbauer, Christine
• Guillem-Gloria, Pedro M.
• Ruiz-Gómez, Gloria
• Pisabarro, María Teresa
• Furesi, Giulia
• Hintze, Vera
• Hofbauer, Lorenz C.
• Moeller, Stephanie
• Heidig, Sophie Luise

Abstract

<p>The WNT signaling pathway is a central regulator of bone development and regeneration. Functional alterations of WNT ligands and inhibitors are associated with a variety of bone diseases that affect bone fragility and result in a high medical and socioeconomic burden. Hence, this cellular pathway has emerged as a novel target for bone-protective therapies, e.g. in osteoporosis. Here, we investigated glycosaminoglycan (GAG) recognition by Dickkopf-1 (DKK1), a potent endogenous WNT inhibitor, and the underlying functional implications in order to develop WNT signaling regulators. In a multidisciplinary approach we applied in silico structure-based de novo design strategies and molecular dynamics simulations combined with synthetic chemistry and surface plasmon resonance spectroscopy to Rationally Engineer oligomeric Glycosaminoglycan derivatives (_REGAG) with improved neutralizing properties for DKK1. In vitro and in vivo assays show that the GAG modification to obtain _REGAG translated into increased WNT pathway activity and improved bone regeneration in a mouse calvaria defect model with critical size bone lesions. Importantly, the developed _REGAG outperformed polymeric high-sulfated hyaluronan (sHA3) in enhancing bone healing up to 50% due to their improved DKK1 binding properties. Thus, rationally engineered GAG variants may represent an innovative strategy to develop novel therapeutic approaches for regenerative medicine.</p>

Topics

• impedance spectroscopy
• surface
• simulation
• molecular dynamics
• defect
• surface plasmon resonance spectroscopy