Maintenance of chondroitin sulfation balance by chondroitin-4-sulfotransferase 1 is required for chondrocyte development and growth factor signaling during cartilage morphogenesis

doi:10.1242/dev.01948

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Development ePress online publication date 3 Aug 2005
doi: 10.1242/dev.01948

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Research article: Development and disease

Maintenance of chondroitin sulfation balance by chondroitin-4-sulfotransferase 1 is required for chondrocyte development and growth factor signaling during cartilage morphogenesis

Michael Klüppel, Thomas N. Wight, Christina Chan, Aleksander Hinek, and Jeffrey L. Wrana^*
^* Author for correspondence (e-mail: wrana{at}mshri.on.ca)

Glycosaminoglycans (GAGs) such as heparan sulfate and chondroitinsulfate are polysaccharide chains that are attached to coreproteins to form proteoglycans. The biosynthesis of GAGs isa multistep process that includes the attachment of sulfategroups to specific positions of the polysaccharide chains bysulfotransferases. Heparan-sulfate and heparan sulfate-sulfotransferasesplay important roles in growth factor signaling and animal development.However, the biological importance of chondroitin sulfationduring mammalian development and growth factor signaling ispoorly understood. We show that a gene trap mutation in theBMP-induced chondroitin-4-sulfotransferase 1 (C4st1) gene (alsocalled carbohydrate sulfotransferase 11 - Chst11), which encodesan enzyme specific for the transfer of sulfate groups to the4-O-position in chondroitin, causes severe chondrodysplasiacharacterized by a disorganized cartilage growth plate as wellas specific alterations in the orientation of chondrocyte columns.This phenotype is associated with a chondroitin sulfation imbalance,mislocalization of chondroitin sulfate in the growth plate andan imbalance of apoptotic signals. Analysis of several growthfactor signaling pathways that are important in cartilage growthplate development showed that the C4st1^gt/gt mutation led tostrong upregulation of TGF ${beta}$ signaling with concomitant downregulationof BMP signaling, while Indian hedgehog (Ihh) signaling wasunaffected. These results show that chondroitin 4-O-sulfationby C4st1 is required for proper chondroitin sulfate localization,modulation of distinct signaling pathways and cartilage growthplate morphogenesis. Our study demonstrates an important biologicalrole of differential chondroitin sulfation in mammalian development.

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