The putative tumour suppressor EXT1 alters the expression of cell- surface heparan sulfate

Craig McCormick; Yves Leduc; Diane Martindale; Kirsten Mattison; Lesley E. Esford; Angela P. Dyer; Frank Tufaro

doi:10.1038/514

The putative tumour suppressor EXT1 alters the expression of cell- surface heparan sulfate

Craig McCormick, Yves Leduc, Diane Martindale, Kirsten Mattison, Lesley E. Esford, Angela P. Dyer, Frank Tufaro

Research output: Contribution to journal › Article › peer-review

342 Citations (Scopus)

Abstract

Hereditary multiple exostoses (HME) is an autosomal dominant disorder characterized by the formation of cartilage-capped tumours (exostoses)that develop from the growth plate of endochondral bone. This condition can lead to skeletal abnormalities, short stature and malignant transformation of exostoses to chondrosarcomas or osteosarcomas. Linkage analyses have identified three different genes for HME, EXT1 on 8q24.1, EXT2 on 11p11-13 and EXT3 on 19p (refs 6-9). Most HME cases have been attributed to missense or frameshift mutations in these tumour-supressor genes, whose functions have remained obscure. Here, we show that EXT1 is an ER-resident type II transmembrane glycoprotein whose expression in cells results in the alteration of the synthesis and display of cell surface heparan sulfate glycosaminoglycans (GAGs). Two EXT1 variants containing aetiologic missense mutations failed to alter cell-surface glycosaminoglycans, despite retaining their ER-Iocalization.

Original language	English
Pages (from-to)	158-161
Number of pages	4
Journal	Nature Genetics
Volume	19
Issue number	2
DOIs	https://doi.org/10.1038/514
Publication status	Published - 1998
Externally published	Yes

ASJC Scopus Subject Areas

Genetics

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title = "The putative tumour suppressor EXT1 alters the expression of cell- surface heparan sulfate",

abstract = "Hereditary multiple exostoses (HME) is an autosomal dominant disorder characterized by the formation of cartilage-capped tumours (exostoses)that develop from the growth plate of endochondral bone. This condition can lead to skeletal abnormalities, short stature and malignant transformation of exostoses to chondrosarcomas or osteosarcomas. Linkage analyses have identified three different genes for HME, EXT1 on 8q24.1, EXT2 on 11p11-13 and EXT3 on 19p (refs 6-9). Most HME cases have been attributed to missense or frameshift mutations in these tumour-supressor genes, whose functions have remained obscure. Here, we show that EXT1 is an ER-resident type II transmembrane glycoprotein whose expression in cells results in the alteration of the synthesis and display of cell surface heparan sulfate glycosaminoglycans (GAGs). Two EXT1 variants containing aetiologic missense mutations failed to alter cell-surface glycosaminoglycans, despite retaining their ER-Iocalization.",

author = "Craig McCormick and Yves Leduc and Diane Martindale and Kirsten Mattison and Esford, {Lesley E.} and Dyer, {Angela P.} and Frank Tufaro",

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AU - McCormick, Craig

AU - Leduc, Yves

AU - Martindale, Diane

AU - Mattison, Kirsten

AU - Esford, Lesley E.

AU - Dyer, Angela P.

AU - Tufaro, Frank

PY - 1998

Y1 - 1998

N2 - Hereditary multiple exostoses (HME) is an autosomal dominant disorder characterized by the formation of cartilage-capped tumours (exostoses)that develop from the growth plate of endochondral bone. This condition can lead to skeletal abnormalities, short stature and malignant transformation of exostoses to chondrosarcomas or osteosarcomas. Linkage analyses have identified three different genes for HME, EXT1 on 8q24.1, EXT2 on 11p11-13 and EXT3 on 19p (refs 6-9). Most HME cases have been attributed to missense or frameshift mutations in these tumour-supressor genes, whose functions have remained obscure. Here, we show that EXT1 is an ER-resident type II transmembrane glycoprotein whose expression in cells results in the alteration of the synthesis and display of cell surface heparan sulfate glycosaminoglycans (GAGs). Two EXT1 variants containing aetiologic missense mutations failed to alter cell-surface glycosaminoglycans, despite retaining their ER-Iocalization.

AB - Hereditary multiple exostoses (HME) is an autosomal dominant disorder characterized by the formation of cartilage-capped tumours (exostoses)that develop from the growth plate of endochondral bone. This condition can lead to skeletal abnormalities, short stature and malignant transformation of exostoses to chondrosarcomas or osteosarcomas. Linkage analyses have identified three different genes for HME, EXT1 on 8q24.1, EXT2 on 11p11-13 and EXT3 on 19p (refs 6-9). Most HME cases have been attributed to missense or frameshift mutations in these tumour-supressor genes, whose functions have remained obscure. Here, we show that EXT1 is an ER-resident type II transmembrane glycoprotein whose expression in cells results in the alteration of the synthesis and display of cell surface heparan sulfate glycosaminoglycans (GAGs). Two EXT1 variants containing aetiologic missense mutations failed to alter cell-surface glycosaminoglycans, despite retaining their ER-Iocalization.

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The putative tumour suppressor EXT1 alters the expression of cell- surface heparan sulfate

Abstract

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