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FGF signalling regulates bone growth through autophagy

Authors :
Sandro Montefusco
Elena Polishchuk
Roman S. Polishchuk
Alison Forrester
Rosa Bartolomeo
Maria Svelto
Maria Antonietta De Matteis
Carmine Settembre
Diego L. Medina
Laura Cinque
Antonio Rossi
Rossella Venditti
Edoardo Nusco
Cinque, Laura
Forrester, Alison
Bartolomeo, Rosa
Svelto, Maria
Venditti, Rossella
Montefusco, Sandro
Polishchuk, Elena
Nusco, Edoardo
Rossi, Antonio
Medina Sanabria, Diego Lui
Polishchuk, Roman
De Matteis, Maria Antonietta
Settembre, Carmine
Source :
Nature. 528(7581)
Publication Year :
2014

Abstract

Skeletal growth relies on both biosynthetic and catabolic processes. While the role of the former is clearly established, how the latter contributes to growth-promoting pathways is less understood. Macroautophagy, hereafter referred to as autophagy, is a catabolic process that plays a fundamental part in tissue homeostasis. We investigated the role of autophagy during bone growth, which is mediated by chondrocyte rate of proliferation, hypertrophic differentiation and extracellular matrix (ECM) deposition in growth plates. Here we show that autophagy is induced in growth-plate chondrocytes during post-natal development and regulates the secretion of type II collagen (Col2), the major component of cartilage ECM. Mice lacking the autophagy related gene 7 (Atg7) in chondrocytes experience endoplasmic reticulum storage of type II procollagen (PC2) and defective formation of the Col2 fibrillary network in the ECM. Surprisingly, post-natal induction of chondrocyte autophagy is mediated by the growth factor FGF18 through FGFR4 and JNK-dependent activation of the autophagy initiation complex VPS34-beclin-1. Autophagy is completely suppressed in growth plates from Fgf18(-/-) embryos, while Fgf18(+/-) heterozygous and Fgfr4(-/-) mice fail to induce autophagy during post-natal development and show decreased Col2 levels in the growth plate. Strikingly, the Fgf18(+/-) and Fgfr4(-/-) phenotypes can be rescued in vivo by pharmacological activation of autophagy, pointing to autophagy as a novel effector of FGF signalling in bone. These data demonstrate that autophagy is a developmentally regulated process necessary for bone growth, and identify FGF signalling as a crucial regulator of autophagy in chondrocytes.

Details

ISSN :
14764687
Volume :
528
Issue :
7581
Database :
OpenAIRE
Journal :
Nature
Accession number :
edsair.doi.dedup.....018a3f80233b397a71380d2390914142