Mapping the sclerostin–LRP4 binding interface identifies critical interaction hotspots in loops 1 and 3 of sclerostin

Abstract: The interaction of sclerostin (Scl) with the low‐density lipoprotein receptor‐related protein 4 (LRP4) leads to a marked reduction in bone formation by inhibiting the Wnt/β‐catenin pathway. To characterize the Scl–LRP4 binding interface, we sorted a combinatorial library of Scl variants and isolated variants with reduced affinity to LRP4. We identified Scl single‐mutation variants enriched during the sorting process and verified their reduction in affinity toward LRP4—a reduction that was not a result of chang… Show more