Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.

Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.

The cystine-knot containing protein Sclerostin is an important negative regulator of bone growth and therefore represents a promising therapeutic target. It exerts its biological task by inhibiting the Wnt (wingless and int1) signaling pathway, which participates in bone formation by promoting the d...

Full description

Bibliographic Details
Main Authors: Verena Boschert, Maarten van Dinther, Stella Weidauer, Katharina van Pee, Eva-Maria Muth, Peter Ten Dijke, Thomas D Mueller
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3843708?pdf=render
id doaj-a228ee4bb24a4ece9007e486537ddd70
record_format Article
spelling doaj-a228ee4bb24a4ece9007e486537ddd702020-11-25T01:09:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-01811e8171010.1371/journal.pone.0081710Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.Verena BoschertMaarten van DintherStella WeidauerKatharina van PeeEva-Maria MuthPeter Ten DijkeThomas D MuellerThe cystine-knot containing protein Sclerostin is an important negative regulator of bone growth and therefore represents a promising therapeutic target. It exerts its biological task by inhibiting the Wnt (wingless and int1) signaling pathway, which participates in bone formation by promoting the differentiation of mesenchymal stem cells to osteoblasts. The core structure of Sclerostin consists of three loops with the first and third loop (Finger 1 and Finger 2) forming a structured β-sheet and the second loop being unstructured and highly flexible. Biochemical data showed that the flexible loop is important for binding of Sclerostin to Wnt co-receptors of the low-density lipoprotein related-protein family (LRP), by interacting with the Wnt co-receptors LRP5 or -6 it inhibits Wnt signaling. To further examine the structural requirements for Wnt inhibition, we performed an extensive mutational study within all three loops of the Sclerostin core domain involving single and multiple mutations as well as truncation of important regions. By this approach we could confirm the importance of the second loop and especially of amino acids Asn92 and Ile94 for binding to LRP6. Based on a Sclerostin variant found in a Turkish family suffering from Sclerosteosis we generated a Sclerostin mutant with cysteines 84 and 142 exchanged thereby removing the third disulfide bond of the cystine-knot. This mutant binds to LRP6 with reduced binding affinity and also exhibits a strongly reduced inhibitory activity against Wnt1 thereby showing that also elements outside the flexible loop are important for inhibition of Wnt by Sclerostin. Additionally, we examined the effect of the mutations on the inhibition of two different Wnt proteins, Wnt3a and Wnt1. We could detect clear differences in the inhibition of these proteins, suggesting that the mechanism by which Sclerostin antagonizes Wnt1 and Wnt3a is fundamentally different.http://europepmc.org/articles/PMC3843708?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Verena Boschert
Maarten van Dinther
Stella Weidauer
Katharina van Pee
Eva-Maria Muth
Peter Ten Dijke
Thomas D Mueller
spellingShingle Verena Boschert
Maarten van Dinther
Stella Weidauer
Katharina van Pee
Eva-Maria Muth
Peter Ten Dijke
Thomas D Mueller
Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.
PLoS ONE
author_facet Verena Boschert
Maarten van Dinther
Stella Weidauer
Katharina van Pee
Eva-Maria Muth
Peter Ten Dijke
Thomas D Mueller
author_sort Verena Boschert
title Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.
title_short Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.
title_full Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.
title_fullStr Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.
title_full_unstemmed Mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for Wnt-signaling inhibition.
title_sort mutational analysis of sclerostin shows importance of the flexible loop and the cystine-knot for wnt-signaling inhibition.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description The cystine-knot containing protein Sclerostin is an important negative regulator of bone growth and therefore represents a promising therapeutic target. It exerts its biological task by inhibiting the Wnt (wingless and int1) signaling pathway, which participates in bone formation by promoting the differentiation of mesenchymal stem cells to osteoblasts. The core structure of Sclerostin consists of three loops with the first and third loop (Finger 1 and Finger 2) forming a structured β-sheet and the second loop being unstructured and highly flexible. Biochemical data showed that the flexible loop is important for binding of Sclerostin to Wnt co-receptors of the low-density lipoprotein related-protein family (LRP), by interacting with the Wnt co-receptors LRP5 or -6 it inhibits Wnt signaling. To further examine the structural requirements for Wnt inhibition, we performed an extensive mutational study within all three loops of the Sclerostin core domain involving single and multiple mutations as well as truncation of important regions. By this approach we could confirm the importance of the second loop and especially of amino acids Asn92 and Ile94 for binding to LRP6. Based on a Sclerostin variant found in a Turkish family suffering from Sclerosteosis we generated a Sclerostin mutant with cysteines 84 and 142 exchanged thereby removing the third disulfide bond of the cystine-knot. This mutant binds to LRP6 with reduced binding affinity and also exhibits a strongly reduced inhibitory activity against Wnt1 thereby showing that also elements outside the flexible loop are important for inhibition of Wnt by Sclerostin. Additionally, we examined the effect of the mutations on the inhibition of two different Wnt proteins, Wnt3a and Wnt1. We could detect clear differences in the inhibition of these proteins, suggesting that the mechanism by which Sclerostin antagonizes Wnt1 and Wnt3a is fundamentally different.
url http://europepmc.org/articles/PMC3843708?pdf=render
work_keys_str_mv AT verenaboschert mutationalanalysisofsclerostinshowsimportanceoftheflexibleloopandthecystineknotforwntsignalinginhibition
AT maartenvandinther mutationalanalysisofsclerostinshowsimportanceoftheflexibleloopandthecystineknotforwntsignalinginhibition
AT stellaweidauer mutationalanalysisofsclerostinshowsimportanceoftheflexibleloopandthecystineknotforwntsignalinginhibition
AT katharinavanpee mutationalanalysisofsclerostinshowsimportanceoftheflexibleloopandthecystineknotforwntsignalinginhibition
AT evamariamuth mutationalanalysisofsclerostinshowsimportanceoftheflexibleloopandthecystineknotforwntsignalinginhibition
AT petertendijke mutationalanalysisofsclerostinshowsimportanceoftheflexibleloopandthecystineknotforwntsignalinginhibition
AT thomasdmueller mutationalanalysisofsclerostinshowsimportanceoftheflexibleloopandthecystineknotforwntsignalinginhibition
_version_ 1725178529888337920

Similar Items