Loading-induced Bone Formation is Mediated by Wnt1 Induction in Osteoblast-lineage Cells

Overview

Journal FASEB J

Specialties Biology
Physiology

Date 2022 Aug 15

PMID 35969160

Authors

Lisa Y Lawson

Nicole Migotsky

Christopher J Chermside-Scabbo

John T Shuster

Kyu Sang Joeng

Roberto Civitelli

Brendan Lee

Matthew J Silva

Affiliations

Soon will be listed here.

Abstract

Mechanical loading on the skeleton stimulates bone formation. Although the exact mechanism underlying this process remains unknown, a growing body of evidence indicates that the Wnt signaling pathway is necessary for the skeletal response to loading. Recently, we showed that Wnts produced by osteoblast lineage cells mediate the osteo-anabolic response to tibial loading in adult mice. Here, we report that Wnt1 specifically plays a crucial role in mediating the mechano-adaptive response to loading. Independent of loading, short-term loss of Wnt1 in the Osx-lineage resulted in a decreased cortical bone area in the tibias of 5-month-old mice. In females, strain-matched loading enhanced periosteal bone formation in Wnt1F/F controls, but not in Wnt1F/F; OsxCreERT2 knockouts. In males, strain-matched loading increased periosteal bone formation in both control and knockout mice; however, the periosteal relative bone formation rate was 65% lower in Wnt1 knockouts versus controls. Together, these findings show that Wnt1 supports adult bone homeostasis and mediates the bone anabolic response to mechanical loading.

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