Entry - %600209 - EXOSTOSES, MULTIPLE, TYPE III; EXT3 - OMIM

 
ICD+
% 600209

EXOSTOSES, MULTIPLE, TYPE III; EXT3


Cytogenetic location: 19p     Genomic coordinates (GRCh38): 19:1-26,200,001


Gene-Phenotype Relationships
Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key
19p Exostoses, multiple, type 3 600209 AD 2
Clinical Synopsis
 
Phenotypic Series
 

Skel
- Multiple exostoses
Inheritance
- Autosomal dominant (19p)
▲ Close
Exostoses, Multiple - PS133700 - 3 Entries
Location Phenotype Inheritance Phenotype
mapping key 		Phenotype
MIM number 		Gene/Locus Gene/Locus
MIM number
8q24.11 Exostoses, multiple, type 1 AD 3 133700 EXT1 608177
11p11.2 Exostoses, multiple, type 2 AD 3 133701 EXT2 608210
19p Exostoses, multiple, type 3 AD 2 600209 EXT3 600209
▲ Close

TEXT

For a phenotypic description and a discussion of genetic heterogeneity of multiple exostoses, see (133700).

Mapping

In a child with multiple exostoses with an interstitial deletion of chromosome 11, Le Merrer et al. (1994) excluded linkage to markers in the region 11p12-p11. However, the locus they termed 'EXT2' was mapped to 19p by linkage to a microsatellite DNA marker at the D19S221 locus. In studies of 21 families, they found a maximum location score of 7.22 with a proportion of families (35%) linked to chromosome 19 and a proportion of families (65%) linked to chromosome 8. Their data supported the location of EXT1 distal to D8S198 and the location of the other gene, designated EXT3, between D19S413 and D19S221.

Le Merrer et al. (1994) suggested that the close linkage of EXT3 to the JUNB (165161) and JUND (165162) protooncogenes on 19p makes these genes possible candidate genes, because malignancy is a complication of multiple exostoses and because transgenic mice defective for a functionally related gene (FOS; 164810) have been shown to develop multiple exostoses of long bones (Wang et al., 1991).

Francannet et al. (2001) reported a clinical and molecular study of 42 French families representing 217 affected individuals with multiple exostoses. They confirmed linkage to EXT1 in 29 of the families, EXT2 (133701) in 9, and EXT3 in 1. Francannet et al. (2001) concluded that there must be at least 1 additional locus for the multiple exostoses phenotype to account for the 3 unlinked families.


REFERENCES

  1. Francannet, C., Cohen-Tanugi, A., Le Merrer, M., Munnich, A., Bonaventure, J., Legeai-Mallet, L. Genotype-phenotype correlation in hereditary multiple exostoses. J. Med. Genet. 38: 430-434, 2001. [PubMed: 11432960, related citations] [Full Text]

  2. Le Merrer, M., Legeai-Mallet, L., Jeannin, P. M., Horsthemke, B., Schinzel, A., Plauchu, H., Toutain, A., Achard, F., Munnich, A., Maroteaux, P. A gene for hereditary multiple exostoses maps to chromosome 19p. Hum. Molec. Genet. 3: 717-722, 1994. [PubMed: 8081357, related citations] [Full Text]

  3. Wang, Z.-Q., Grigoriadis, A. E., Mohle-Steinlein, U., Wagner, E. F. A novel target cell for c-fos-induced oncogenesis: development of chondrogenic tumours in embryonic stem cell chimeras. EMBO J. 10: 2437-2450, 1991. [PubMed: 1714376, related citations] [Full Text]


Contributors:
Michael J. Wright - updated : 10/5/2001
Creation Date:
Victor A. McKusick : 11/30/1994
Edit History:
carol : 04/29/2019
joanna : 03/18/2004
ckniffin : 11/5/2003
carol : 10/30/2003
ckniffin : 10/29/2003
cwells : 10/9/2001
cwells : 10/5/2001
alopez : 7/10/1997
mimadm : 9/23/1995
carol : 11/30/1994

% 600209

EXOSTOSES, MULTIPLE, TYPE III; EXT3


ORPHA: 321;   DO: 206;  


Cytogenetic location: 19p     Genomic coordinates (GRCh38): 19:1-26,200,001


Gene-Phenotype Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key
19p Exostoses, multiple, type 3 600209 Autosomal dominant 2

TEXT

For a phenotypic description and a discussion of genetic heterogeneity of multiple exostoses, see (133700).

Mapping

In a child with multiple exostoses with an interstitial deletion of chromosome 11, Le Merrer et al. (1994) excluded linkage to markers in the region 11p12-p11. However, the locus they termed 'EXT2' was mapped to 19p by linkage to a microsatellite DNA marker at the D19S221 locus. In studies of 21 families, they found a maximum location score of 7.22 with a proportion of families (35%) linked to chromosome 19 and a proportion of families (65%) linked to chromosome 8. Their data supported the location of EXT1 distal to D8S198 and the location of the other gene, designated EXT3, between D19S413 and D19S221.

Le Merrer et al. (1994) suggested that the close linkage of EXT3 to the JUNB (165161) and JUND (165162) protooncogenes on 19p makes these genes possible candidate genes, because malignancy is a complication of multiple exostoses and because transgenic mice defective for a functionally related gene (FOS; 164810) have been shown to develop multiple exostoses of long bones (Wang et al., 1991).

Francannet et al. (2001) reported a clinical and molecular study of 42 French families representing 217 affected individuals with multiple exostoses. They confirmed linkage to EXT1 in 29 of the families, EXT2 (133701) in 9, and EXT3 in 1. Francannet et al. (2001) concluded that there must be at least 1 additional locus for the multiple exostoses phenotype to account for the 3 unlinked families.


REFERENCES

  1. Francannet, C., Cohen-Tanugi, A., Le Merrer, M., Munnich, A., Bonaventure, J., Legeai-Mallet, L. Genotype-phenotype correlation in hereditary multiple exostoses. J. Med. Genet. 38: 430-434, 2001. [PubMed: 11432960] [Full Text: https://doi.org/10.1136/jmg.38.7.430]

  2. Le Merrer, M., Legeai-Mallet, L., Jeannin, P. M., Horsthemke, B., Schinzel, A., Plauchu, H., Toutain, A., Achard, F., Munnich, A., Maroteaux, P. A gene for hereditary multiple exostoses maps to chromosome 19p. Hum. Molec. Genet. 3: 717-722, 1994. [PubMed: 8081357] [Full Text: https://doi.org/10.1093/hmg/3.5.717]

  3. Wang, Z.-Q., Grigoriadis, A. E., Mohle-Steinlein, U., Wagner, E. F. A novel target cell for c-fos-induced oncogenesis: development of chondrogenic tumours in embryonic stem cell chimeras. EMBO J. 10: 2437-2450, 1991. [PubMed: 1714376] [Full Text: https://doi.org/10.1002/j.1460-2075.1991.tb07783.x]


Contributors:
Michael J. Wright - updated : 10/5/2001

Creation Date:
Victor A. McKusick : 11/30/1994

Edit History:
carol : 04/29/2019
joanna : 03/18/2004
ckniffin : 11/5/2003
carol : 10/30/2003
ckniffin : 10/29/2003
cwells : 10/9/2001
cwells : 10/5/2001
alopez : 7/10/1997
mimadm : 9/23/1995
carol : 11/30/1994



NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2024 Johns Hopkins University.

NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2024 Johns Hopkins University.
Printed: May 3, 2024