Entry - #226900 - EPIPHYSEAL DYSPLASIA, MULTIPLE, 4; EDM4 - OMIM

 
ICD+
# 226900

EPIPHYSEAL DYSPLASIA, MULTIPLE, 4; EDM4


Alternative titles; symbols

MULTIPLE EPIPHYSEAL DYSPLASIA, AUTOSOMAL RECESSIVE
MULTIPLE EPIPHYSEAL DYSPLASIA WITH CLUBFOOT
MULTIPLE EPIPHYSEAL DYSPLASIA WITH BILAYERED PATELLAE


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
5q32 Epiphyseal dysplasia, multiple, 4 226900 AR 3 SLC26A2 606718
Clinical Synopsis
 
Phenotypic Series
 

INHERITANCE
- Autosomal recessive
GROWTH
Height
- Short stature (3rd-90th centile, infrequent finding)
SKELETAL
- Multiple epiphyseal dysplasia
Spine
- Scoliosis
Pelvis
- Hip dysplasia
- Small femoral heads
- Flattened proximal femoral epiphyses
Limbs
- Limited elbow flexion
- Double layered patella
- Arthralgia
- Small humeral, distal radii, and ulnae epiphyses
- Mildly shortened ulna
- Flat proximal femoral epiphyses
Hands
- Brachydactyly
- Mild shortened metacarpals
Feet
- Clubfoot
MISCELLANEOUS
- Genetic heterogeneity, see EDM1 (132400), EDM2 (600204), EDM3 (600969), and EDM5 (607078)
- Allelic to diastrophic dysplasia (222600), atelosteogenesis, type II (256050), and achondrogenesis, type IB (600972)
MOLECULAR BASIS
- Caused by mutation in the solute carrier family 26 (sulfate transporter), member 2 gene (SLC26A2, 606718.0002)
▲ Close

TEXT

A number sign (#) is used with this entry because of evidence that autosomal recessive multiple epiphyseal dysplasia-4 (EDM4) is caused by homozygous or compound heterozygous mutation in the DTDST gene (SLC26A2; 606718) on chromosome 5q32.

Clinical Features

Juberg and Holt (1968) described 3 sisters and a brother with multiple epiphyseal dysplasia (MED). The parents were normal and not related. This family and some previously published families, including some with instances of parental consanguinity, led them to support recessive inheritance for one form of multiple epiphyseal dysplasia. MED with apparent recessive inheritance was also reported by Ribbing (1937), Waugh (1952), Hunt et al. (1967), and Gamboa and Lisker (1974). In some of these families, the differentiation from recessive pseudoachondroplastic spondyloepiphyseal dysplasia (177170) may not be clear. In that disorder, spinal changes may be evident mainly in radiographs taken before puberty. Maroteaux et al. (1975) suggested that the recessive form of MED may differ from the dominant in the presence of flat femoral head and lack of metaphyseal irregularities in the metacarpals and phalanges. Chondrocytes contain inclusions, probably of lysosomal origin, with granular or filamentous material.

Sheffield (1998) reviewed literature on double-layered patella, its relationship to multiple epiphyseal dysplasia, radiographic findings, and clinical implications.

Deere et al. (1995) found linkage of a dominant form of MED, which they classified as the Fairbank type, to 19q (EDM1; 132400), but failed to find linkage to chromosome 19 in a family with unaffected parents in which 3 of 7 sibs were affected. The 2 adult sibs in the latter family were examined radiographically and there appeared to be no phenotypic differences between them.

Superti-Furga et al. (1999) reported a 36-year-old man of tall-normal stature who had requested genetic counseling for a presumed dominant form of multiple epiphyseal dysplasia. Bilateral clubfoot had been surgically corrected in childhood. Lateral knee x-rays at 8 years of age showed bilateral double-layered patellae. Cleft palate, swelling of the ear pinnae, and 'hitch-hiker thumb' were absent. A homozygous mutation in the DTDST gene (R279W; 606718.0002) was found. The authors classified this phenotype as autosomal recessive multiple epiphyseal dysplasia.

Huber et al. (2001) reported 2 unrelated sibships initially thought to have isolated clubfoot. In the first sibship, dizygotic twins had respectively unilateral metatarsus varus and bilateral clubfeet. Subsequently mild epiphyseal dysplasia of the upper femurs was noted. In the second sibship, the 2 children were originally thought to have isolated clubfoot but subsequent examination of x-rays demonstrated delayed ossification of the hip epiphyses and mild flaring of the metaphyses in 1 case and brachymesophalangy and hip subluxation in the second case. A homozygous R279W mutation in the DTDST gene (606718.0002) was found in each case. Huber et al. (2001) noted the absence of double-layered patellae in these cases. The authors suggested that their patients, taken together with the patient of Superti-Furga et al. (1999), added to the view that the clinical spectrum of abnormalities caused by DTDST mutations is broader than originally believed and includes apparently isolated clubfoot.

Makitie et al. (2003) reported 3 patients from 2 families who were born to nonconsanguineous parents and developed signs of hip dysplasia in early childhood. Two had episodes of recurrent patella dislocations. Stature and the feet, ears, and palate were normal. X-rays showed dysplasia of femoral heads, mild generalized epiphyseal dysplasia, abnormal patella ossification, and normal hands and feet. A homozygous mutation in the DTDST gene (C653S; 606718.0011) was detected in each case.

Barreda-Bonis et al. (2018) reported a 14-year-old girl and her maternal grandfather with EDM4. When initially evaluated at the age of 16 months for disproportionate short stature, the girl had bilateral clubfoot, rhizomelic shortening of the extremities, and micrognathia with a high-arched palate. Her height was -3.09 SD and her arm span was severely reduced. Bone age was consistent with chronological age until puberty when it accelerated. At her most recent evaluation at age 14.8 years, her height was -1.9 SD with an advanced bone age of 16 years. Her BMI was 27. Skeletal survey at 20 months showed short, broad femoral necks with delayed ossification centers. Radii and ulna were bowed. She had deformities of both forearms and generalized flattening of the epiphyses. Acromicria was observed, with synostoses between the second and third metatarsals of both feet. She also had a double-layered patella. Her grandfather had short stature (143 cm, -5.33 SD) with shortening of his upper limbs and early joint problems, including bilateral hip pain in his twenties and a hip replacement in his forties, with a subsequent revision on the right hip at age 60. At age 70, surgical intervention of his shoulder joint for osteoarthritis was planned. His radiographic findings were similar to those seen in his granddaughter.


Inheritance

The transmission pattern of EDM4 in the family reported by Superti-Furga et al. (1999) was consistent with autosomal recessive inheritance.


Molecular Genetics

Superti-Furga et al. (1999) reported a homozygous DTDST mutation (R279W; 606718.0002) in a 36-year-old man of tall-normal stature with multiple epiphyseal dysplasia.

Huber et al. (2001) reported homozygous R279W mutations (606718.0002) in the DTDST gene in 2 unrelated sibships initially thought to have isolated clubfoot.

Czarny-Ratajczak et al. (2001) identified the homozygous R279W mutation in 2 probands with multiple epiphyseal dysplasia and multipartite patella.

Of 21 patients from 15 families with recessive multiple epiphyseal dysplasia, Ballhausen et al. (2003) identified homozygosity for the R279W mutation in 18 patients from 12 families. Three of the families were consanguineous. The main clinical findings included foot and hand deformities, joint complaints, and slightly reduced stature on average. The main radiographic findings were flat proximal femoral epiphyses, mild brachydactyly, and double layered patellae.

Makitie et al. (2003) identified a homozygous DTDST mutation (C653S; 606718.0011) in 2 unrelated sibships with early childhood-onset hip dysplasia, recurrent patella dislocation, and normal stature. Abnormal patella ossification was characteristic.

Using a targeted next-generation sequencing skeletal dysplasia panel, Barreda-Bonis et al. (2018) identified mutations in the SLC26A2 gene in a 14-year-old-girl and her maternal grandfather with EDM4. The girl was compound heterozygous for the common R279W mutation (606718.0002), inherited from her mother, and a S522F mutation (606718.0015), inherited from her father. Her grandfather was homozygous for the R279W mutation. The girl's mother was short (-3.53 SD), but was only a carrier of the R279W mutation.


REFERENCES

  1. Ballhausen, D., Bonafe, L., Terhal, P., Unger, S. L., Bellus, G., Classen, M., Hamel, B. C., Spranger, J., Zabel, B., Cohn, D. H., Cole, W. G., Hecht, J. T., Superti-Furga, A. Recessive multiple epiphyseal dysplasia (rMED): phenotype delineation in eighteen homozygotes for DTDST mutation R279W (Letter) J. Med. Genet. 40: 65-71, 2003. [PubMed: 12525546, related citations] [Full Text]

  2. Barreda-Bonis, A. C., Barraza-Garcia, J., Parron, M., Pastor, I., Heath, K. E., Gonzalez-Casado, I. Multiple SLC26A2 mutations occurring in a three-generational family. Europ. J. Med. Genet. 61: 24-28, 2018. [PubMed: 29024831, related citations] [Full Text]

  3. Czarny-Ratajczak, M., Lohiniva, J., Rogala, P., Kozlowski, K., Perala, M., Carter, L., Spector, T. D., Kolodziej, L., Seppanen, U., Glazar, R., Krolewski, J., Latos-Bielenska, A., Ala-Kokko, L. A mutation in COL9A1 causes multiple epiphyseal dysplasia: further evidence for locus heterogeneity. Am. J. Hum. Genet. 69: 969-980, 2001. [PubMed: 11565064, images, related citations] [Full Text]

  4. Deere, M., Blanton, S. H., Scott, C. I., Langer, L. O., Pauli, R. M., Hecht, J. T. Genetic heterogeneity in multiple epiphyseal dysplasia. Am. J. Hum. Genet. 56: 698-704, 1995. [PubMed: 7887425, related citations]

  5. Gamboa, I., Lisker, R. Multiple epiphyseal dysplasia tarda: a family with autosomal recessive inheritance. Clin. Genet. 6: 15-19, 1974. [PubMed: 4426126, related citations]

  6. Huber, C., Odent, S., Rumeur, S., Padovani, P., Penet, C., Cormier-Daire, V., Munnich, A., Le Merrer, M. Sulphate transporter gene mutations in apparently isolated club foot. (Letter) J. Med. Genet. 38: 191-192, 2001. [PubMed: 11303514, related citations] [Full Text]

  7. Hunt, D. D., Ponseti, I. V., Pedrini-Mille, A., Pedrini, V. Multiple epiphyseal dysplasia in two siblings. J. Bone Joint Surg. Am. 49: 1611-1627, 1967. [PubMed: 4229795, related citations]

  8. Juberg, R. C., Holt, J. F. Inheritance of multiple epiphyseal dysplasia, tarda. Am. J. Hum. Genet. 20: 549-563, 1968. [PubMed: 5703690, related citations]

  9. Makitie, O., Savarirayan, R., Bonafe, L., Robertson, S., Susic, M., Superti-Furga, A., Cole, W. G. Autosomal recessive multiple epiphyseal dysplasia with homozygosity for C653S in the DTDST gene: double-layer patella as a reliable sign. Am. J. Med. Genet. 122A: 187-192, 2003. [PubMed: 12966518, related citations] [Full Text]

  10. Maroteaux, P., Stanescu, R., Cohen-Solal, D. Dysplasie poly-epiphysaire probablement recessive autosomique: apport de l'etude ultra-structurale dans l'isolement de cette forme autonome. Nouv. Presse Med. 4: 2169-2172, 1975. [PubMed: 170585, related citations]

  11. Ribbing, S. Studien ueber hereditaere multiple Epiphysenstoerungen. Acta Radiol. Suppl. 34: 7-107, 1937.

  12. Sheffield, E. G. Double-layered patella in multiple epiphyseal dysplasia: a valuable clue in the diagnosis. J. Pediat. Orthop. 18: 123-128, 1998. [PubMed: 9449113, related citations]

  13. Superti-Furga, A., Neumann, L., Riebel, T., Eich, G., Steinmann, B., Spranger, J., Kunze, J. Recessively inherited multiple epiphyseal dysplasia with normal stature, club foot, and double layered patella caused by a DTDST mutation. J. Med. Genet. 36: 621-624, 1999. [PubMed: 10465113, related citations]

  14. Watt, J. K. Multiple epiphyseal dysplasia: a report of four cases. Brit. J. Surg. 39: 533-535, 1952. [PubMed: 14935176, related citations] [Full Text]

  15. Waugh, W. Dysplasia epiphysialis multiplex in three sisters. J. Bone Joint Surg. Br. 34: 82-87, 1952. [PubMed: 12999879, related citations] [Full Text]

  16. Weaver, D. D., Otter, M., Colyer, R. A., Jackson, C. E. Juberg-Holt type recessive multiple epiphyseal dysplasia tarda in an Amish family. (Abstract) Am. J. Hum. Genet. 30: 71A only, 1978.


Contributors:
Sonja A. Rasmussen - updated : 03/22/2019
Cassandra L. Kniffin - updated : 12/9/2003
Felicity Collins - updated : 12/5/2003
Michael J. Wright - updated : 6/28/2002
Michael J. Wright - updated : 11/8/1999
Creation Date:
Victor A. McKusick : 6/3/1986
Edit History:
alopez : 11/19/2024
alopez : 11/30/2023
carol : 03/25/2019
carol : 03/22/2019
carol : 05/24/2016
carol : 5/23/2016
terry : 1/13/2011
carol : 10/25/2006
carol : 10/25/2006
carol : 12/12/2003
ckniffin : 12/9/2003
carol : 12/8/2003
carol : 12/5/2003
alopez : 6/28/2002
terry : 6/28/2002
alopez : 6/28/2002
alopez : 6/28/2002
carol : 2/27/2002
alopez : 7/19/2001
alopez : 7/19/2001
joanna : 7/16/2001
alopez : 11/8/1999
alopez : 11/8/1999
carol : 12/16/1998
mark : 3/29/1995
mimadm : 2/19/1994
carol : 5/21/1993
carol : 2/18/1993
carol : 3/30/1992
supermim : 3/16/1992

# 226900

EPIPHYSEAL DYSPLASIA, MULTIPLE, 4; EDM4


Alternative titles; symbols

MULTIPLE EPIPHYSEAL DYSPLASIA, AUTOSOMAL RECESSIVE
MULTIPLE EPIPHYSEAL DYSPLASIA WITH CLUBFOOT
MULTIPLE EPIPHYSEAL DYSPLASIA WITH BILAYERED PATELLAE


SNOMEDCT: 715672007;   ORPHA: 93307;   DO: 0070300;  


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
5q32 Epiphyseal dysplasia, multiple, 4 226900 Autosomal recessive 3 SLC26A2 606718

TEXT

A number sign (#) is used with this entry because of evidence that autosomal recessive multiple epiphyseal dysplasia-4 (EDM4) is caused by homozygous or compound heterozygous mutation in the DTDST gene (SLC26A2; 606718) on chromosome 5q32.

Clinical Features

Juberg and Holt (1968) described 3 sisters and a brother with multiple epiphyseal dysplasia (MED). The parents were normal and not related. This family and some previously published families, including some with instances of parental consanguinity, led them to support recessive inheritance for one form of multiple epiphyseal dysplasia. MED with apparent recessive inheritance was also reported by Ribbing (1937), Waugh (1952), Hunt et al. (1967), and Gamboa and Lisker (1974). In some of these families, the differentiation from recessive pseudoachondroplastic spondyloepiphyseal dysplasia (177170) may not be clear. In that disorder, spinal changes may be evident mainly in radiographs taken before puberty. Maroteaux et al. (1975) suggested that the recessive form of MED may differ from the dominant in the presence of flat femoral head and lack of metaphyseal irregularities in the metacarpals and phalanges. Chondrocytes contain inclusions, probably of lysosomal origin, with granular or filamentous material.

Sheffield (1998) reviewed literature on double-layered patella, its relationship to multiple epiphyseal dysplasia, radiographic findings, and clinical implications.

Deere et al. (1995) found linkage of a dominant form of MED, which they classified as the Fairbank type, to 19q (EDM1; 132400), but failed to find linkage to chromosome 19 in a family with unaffected parents in which 3 of 7 sibs were affected. The 2 adult sibs in the latter family were examined radiographically and there appeared to be no phenotypic differences between them.

Superti-Furga et al. (1999) reported a 36-year-old man of tall-normal stature who had requested genetic counseling for a presumed dominant form of multiple epiphyseal dysplasia. Bilateral clubfoot had been surgically corrected in childhood. Lateral knee x-rays at 8 years of age showed bilateral double-layered patellae. Cleft palate, swelling of the ear pinnae, and 'hitch-hiker thumb' were absent. A homozygous mutation in the DTDST gene (R279W; 606718.0002) was found. The authors classified this phenotype as autosomal recessive multiple epiphyseal dysplasia.

Huber et al. (2001) reported 2 unrelated sibships initially thought to have isolated clubfoot. In the first sibship, dizygotic twins had respectively unilateral metatarsus varus and bilateral clubfeet. Subsequently mild epiphyseal dysplasia of the upper femurs was noted. In the second sibship, the 2 children were originally thought to have isolated clubfoot but subsequent examination of x-rays demonstrated delayed ossification of the hip epiphyses and mild flaring of the metaphyses in 1 case and brachymesophalangy and hip subluxation in the second case. A homozygous R279W mutation in the DTDST gene (606718.0002) was found in each case. Huber et al. (2001) noted the absence of double-layered patellae in these cases. The authors suggested that their patients, taken together with the patient of Superti-Furga et al. (1999), added to the view that the clinical spectrum of abnormalities caused by DTDST mutations is broader than originally believed and includes apparently isolated clubfoot.

Makitie et al. (2003) reported 3 patients from 2 families who were born to nonconsanguineous parents and developed signs of hip dysplasia in early childhood. Two had episodes of recurrent patella dislocations. Stature and the feet, ears, and palate were normal. X-rays showed dysplasia of femoral heads, mild generalized epiphyseal dysplasia, abnormal patella ossification, and normal hands and feet. A homozygous mutation in the DTDST gene (C653S; 606718.0011) was detected in each case.

Barreda-Bonis et al. (2018) reported a 14-year-old girl and her maternal grandfather with EDM4. When initially evaluated at the age of 16 months for disproportionate short stature, the girl had bilateral clubfoot, rhizomelic shortening of the extremities, and micrognathia with a high-arched palate. Her height was -3.09 SD and her arm span was severely reduced. Bone age was consistent with chronological age until puberty when it accelerated. At her most recent evaluation at age 14.8 years, her height was -1.9 SD with an advanced bone age of 16 years. Her BMI was 27. Skeletal survey at 20 months showed short, broad femoral necks with delayed ossification centers. Radii and ulna were bowed. She had deformities of both forearms and generalized flattening of the epiphyses. Acromicria was observed, with synostoses between the second and third metatarsals of both feet. She also had a double-layered patella. Her grandfather had short stature (143 cm, -5.33 SD) with shortening of his upper limbs and early joint problems, including bilateral hip pain in his twenties and a hip replacement in his forties, with a subsequent revision on the right hip at age 60. At age 70, surgical intervention of his shoulder joint for osteoarthritis was planned. His radiographic findings were similar to those seen in his granddaughter.


Inheritance

The transmission pattern of EDM4 in the family reported by Superti-Furga et al. (1999) was consistent with autosomal recessive inheritance.


Molecular Genetics

Superti-Furga et al. (1999) reported a homozygous DTDST mutation (R279W; 606718.0002) in a 36-year-old man of tall-normal stature with multiple epiphyseal dysplasia.

Huber et al. (2001) reported homozygous R279W mutations (606718.0002) in the DTDST gene in 2 unrelated sibships initially thought to have isolated clubfoot.

Czarny-Ratajczak et al. (2001) identified the homozygous R279W mutation in 2 probands with multiple epiphyseal dysplasia and multipartite patella.

Of 21 patients from 15 families with recessive multiple epiphyseal dysplasia, Ballhausen et al. (2003) identified homozygosity for the R279W mutation in 18 patients from 12 families. Three of the families were consanguineous. The main clinical findings included foot and hand deformities, joint complaints, and slightly reduced stature on average. The main radiographic findings were flat proximal femoral epiphyses, mild brachydactyly, and double layered patellae.

Makitie et al. (2003) identified a homozygous DTDST mutation (C653S; 606718.0011) in 2 unrelated sibships with early childhood-onset hip dysplasia, recurrent patella dislocation, and normal stature. Abnormal patella ossification was characteristic.

Using a targeted next-generation sequencing skeletal dysplasia panel, Barreda-Bonis et al. (2018) identified mutations in the SLC26A2 gene in a 14-year-old-girl and her maternal grandfather with EDM4. The girl was compound heterozygous for the common R279W mutation (606718.0002), inherited from her mother, and a S522F mutation (606718.0015), inherited from her father. Her grandfather was homozygous for the R279W mutation. The girl's mother was short (-3.53 SD), but was only a carrier of the R279W mutation.


See Also:

Watt (1952); Weaver et al. (1978)

REFERENCES

  1. Ballhausen, D., Bonafe, L., Terhal, P., Unger, S. L., Bellus, G., Classen, M., Hamel, B. C., Spranger, J., Zabel, B., Cohn, D. H., Cole, W. G., Hecht, J. T., Superti-Furga, A. Recessive multiple epiphyseal dysplasia (rMED): phenotype delineation in eighteen homozygotes for DTDST mutation R279W (Letter) J. Med. Genet. 40: 65-71, 2003. [PubMed: 12525546] [Full Text: https://doi.org/10.1136/jmg.40.1.65]

  2. Barreda-Bonis, A. C., Barraza-Garcia, J., Parron, M., Pastor, I., Heath, K. E., Gonzalez-Casado, I. Multiple SLC26A2 mutations occurring in a three-generational family. Europ. J. Med. Genet. 61: 24-28, 2018. [PubMed: 29024831] [Full Text: https://doi.org/10.1016/j.ejmg.2017.10.007]

  3. Czarny-Ratajczak, M., Lohiniva, J., Rogala, P., Kozlowski, K., Perala, M., Carter, L., Spector, T. D., Kolodziej, L., Seppanen, U., Glazar, R., Krolewski, J., Latos-Bielenska, A., Ala-Kokko, L. A mutation in COL9A1 causes multiple epiphyseal dysplasia: further evidence for locus heterogeneity. Am. J. Hum. Genet. 69: 969-980, 2001. [PubMed: 11565064] [Full Text: https://doi.org/10.1086/324023]

  4. Deere, M., Blanton, S. H., Scott, C. I., Langer, L. O., Pauli, R. M., Hecht, J. T. Genetic heterogeneity in multiple epiphyseal dysplasia. Am. J. Hum. Genet. 56: 698-704, 1995. [PubMed: 7887425]

  5. Gamboa, I., Lisker, R. Multiple epiphyseal dysplasia tarda: a family with autosomal recessive inheritance. Clin. Genet. 6: 15-19, 1974. [PubMed: 4426126]

  6. Huber, C., Odent, S., Rumeur, S., Padovani, P., Penet, C., Cormier-Daire, V., Munnich, A., Le Merrer, M. Sulphate transporter gene mutations in apparently isolated club foot. (Letter) J. Med. Genet. 38: 191-192, 2001. [PubMed: 11303514] [Full Text: https://doi.org/10.1136/jmg.38.3.191]

  7. Hunt, D. D., Ponseti, I. V., Pedrini-Mille, A., Pedrini, V. Multiple epiphyseal dysplasia in two siblings. J. Bone Joint Surg. Am. 49: 1611-1627, 1967. [PubMed: 4229795]

  8. Juberg, R. C., Holt, J. F. Inheritance of multiple epiphyseal dysplasia, tarda. Am. J. Hum. Genet. 20: 549-563, 1968. [PubMed: 5703690]

  9. Makitie, O., Savarirayan, R., Bonafe, L., Robertson, S., Susic, M., Superti-Furga, A., Cole, W. G. Autosomal recessive multiple epiphyseal dysplasia with homozygosity for C653S in the DTDST gene: double-layer patella as a reliable sign. Am. J. Med. Genet. 122A: 187-192, 2003. [PubMed: 12966518] [Full Text: https://doi.org/10.1002/ajmg.a.20282]

  10. Maroteaux, P., Stanescu, R., Cohen-Solal, D. Dysplasie poly-epiphysaire probablement recessive autosomique: apport de l'etude ultra-structurale dans l'isolement de cette forme autonome. Nouv. Presse Med. 4: 2169-2172, 1975. [PubMed: 170585]

  11. Ribbing, S. Studien ueber hereditaere multiple Epiphysenstoerungen. Acta Radiol. Suppl. 34: 7-107, 1937.

  12. Sheffield, E. G. Double-layered patella in multiple epiphyseal dysplasia: a valuable clue in the diagnosis. J. Pediat. Orthop. 18: 123-128, 1998. [PubMed: 9449113]

  13. Superti-Furga, A., Neumann, L., Riebel, T., Eich, G., Steinmann, B., Spranger, J., Kunze, J. Recessively inherited multiple epiphyseal dysplasia with normal stature, club foot, and double layered patella caused by a DTDST mutation. J. Med. Genet. 36: 621-624, 1999. [PubMed: 10465113]

  14. Watt, J. K. Multiple epiphyseal dysplasia: a report of four cases. Brit. J. Surg. 39: 533-535, 1952. [PubMed: 14935176] [Full Text: https://doi.org/10.1002/bjs.18003915815]

  15. Waugh, W. Dysplasia epiphysialis multiplex in three sisters. J. Bone Joint Surg. Br. 34: 82-87, 1952. [PubMed: 12999879] [Full Text: https://doi.org/10.1302/0301-620X.34B1.82]

  16. Weaver, D. D., Otter, M., Colyer, R. A., Jackson, C. E. Juberg-Holt type recessive multiple epiphyseal dysplasia tarda in an Amish family. (Abstract) Am. J. Hum. Genet. 30: 71A only, 1978.


Contributors:
Sonja A. Rasmussen - updated : 03/22/2019
Cassandra L. Kniffin - updated : 12/9/2003
Felicity Collins - updated : 12/5/2003
Michael J. Wright - updated : 6/28/2002
Michael J. Wright - updated : 11/8/1999

Creation Date:
Victor A. McKusick : 6/3/1986

Edit History:
alopez : 11/19/2024
alopez : 11/30/2023
carol : 03/25/2019
carol : 03/22/2019
carol : 05/24/2016
carol : 5/23/2016
terry : 1/13/2011
carol : 10/25/2006
carol : 10/25/2006
carol : 12/12/2003
ckniffin : 12/9/2003
carol : 12/8/2003
carol : 12/5/2003
alopez : 6/28/2002
terry : 6/28/2002
alopez : 6/28/2002
alopez : 6/28/2002
carol : 2/27/2002
alopez : 7/19/2001
alopez : 7/19/2001
joanna : 7/16/2001
alopez : 11/8/1999
alopez : 11/8/1999
carol : 12/16/1998
mark : 3/29/1995
mimadm : 2/19/1994
carol : 5/21/1993
carol : 2/18/1993
carol : 3/30/1992
supermim : 3/16/1992



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® 1966-2025 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® 1966-2025 Johns Hopkins University.
Printed: March 5, 2025