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. 2011 Oct 12;19(10):1433-42.
doi: 10.1016/j.str.2011.07.005. Epub 2011 Sep 22.

Wnt antagonists bind through a short peptide to the first β-propeller domain of LRP5/6

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Free article

Wnt antagonists bind through a short peptide to the first β-propeller domain of LRP5/6

Eric Bourhis et al. Structure. .
Free article

Abstract

The Wnt pathway inhibitors DKK1 and sclerostin (SOST) are important therapeutic targets in diseases involving bone loss or damage. It has been appreciated that Wnt coreceptors LRP5/6 are also important, as human missense mutations that result in bone overgrowth (bone mineral density, or BMD, mutations) cluster to the E1 propeller domain of LRP5. Here, we report a crystal structure of LRP6 E1 bound to an antibody, revealing that the E1 domain is a peptide recognition module. Remarkably, the consensus E1 binding sequence is a close match to a conserved tripeptide motif present in all Wnt inhibitors that bind LRP5/6. We show that this motif is important for DKK1 and SOST binding to LRP6 and for inhibitory function, providing a detailed structural explanation for the effect of the BMD mutations.

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