Recessive multiple epiphyseal dysplasia (rMED): phenotype delineation in eighteen homozygotes for DTDST mutation R279W

Ballhausen, Diana; Bonafé, Luisa; Terhal, Paulien A; Unger, Sheila; Bellus, Gary A.; Claßen, Martin; Hamel, B.C.J.; Spranger, Jürgen W.; Zabel, Bernard; Cohn, Daniel H.; Cole, William G.; Hecht, Jacqueline; Superti‐Furga, Andrea

doi:10.1136/jmg.40.1.65

Cited by 66 publications

(102 citation statements)

References 20 publications

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“…The p.R279W is a common SLC26A2 mutation. Compound heterozygotes or homozygotes of this mutation usually manifest severe skeletal dysplasia, although patients with milder phenotypes have been reported 31 .…”

Section: Discussionmentioning

confidence: 99%

Analysis of 589,306 genomes identifies individuals resilient to severe Mendelian childhood diseases

Chen¹,

Shi²,

Hakenberg³

et al. 2016

Nat Biotechnol

275

252

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Section: Discussionmentioning

confidence: 99%

Analysis of 589,306 genomes identifies individuals resilient to severe Mendelian childhood diseases

Chen¹,

Shi²,

Hakenberg³

et al. 2016

Nat Biotechnol

275

252

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“…The central role of Slc26a2 in supplying the bulk of cellular SO 4 2Ϫ is evident from the lethality of deletion of the SLC26A2 gene in humans and mice (20,22), mainly due to under-sulfation of proteoglycans leading to aberrant development (23). Indeed, measurement of SO 4 2Ϫ uptake in fibroblast from patients with a severe form of the disease showed reduced or lack of SO 4 2Ϫ uptake (20,24).…”

Section: Slc26a2 Is a Ubiquitously Expressed Somentioning

confidence: 99%

Solute Carrier Family 26 Member a2 (Slc26a2) Protein Functions as an Electroneutral SO42−/OH−/Cl− Exchanger Regulated by Extracellular Cl−

Ohana

Shcheynikov

Park

et al. 2012

Journal of Biological Chemistry

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“…Detailed clinical and mutation data have been reported previously for four of these patients. Three of these patients with clinical findings consistent with rMED had homozygous DTDST mutations; 14,15 one had radiographic findings typical of EDM1 and was found to have a COMP mutation. 18 Of the remaining 26 patients, 25 consented to participate in the study.…”

Section: Patientsmentioning

confidence: 99%

“…Taking together with the previously reported mutations, 10,14,15,18,19 Figure 5 Patient 16 was diagnosed with MED in early childhood. At 10 years he was asymptomatic but had genua vara, increased lumbar lordosis, short stature (o3%) and generalized joint laxity.…”

Section: New Phenotypic Entities Two Distinctive New Phenotypic Entitmentioning

confidence: 99%

Mutations in the known genes are not the major cause of MED; distinctive phenotypic entities among patients with no identified mutations

et al. 2004

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Multiple epiphyseal dysplasia (MED) is a clinically and genetically heterogeneous chondrodysplasia. Mutations in six genes (COMP, COL9A1, COL9A2, COL9A3, MATN3 and DTDST) have been reported, but the genotype -phenotype correlations and the proportions of cases due to mutations in these genes are still not well characterized. We performed a clinical, radiological and molecular analysis of known MED genes on 29 consecutive MED patients. The mutation analysis resulted in identification of the DTDST mutation in four patients (14%), the COMP mutation in three (10%) and the MATN3 mutation in three (10%). Thus, a disease-causing mutation was identified in 10 patients altogether (34%). The phenotypic features observed in the patients with mutations were in accordance with previously described phenotypes, but two new distinct phenotypic entities were identified in patients in whom no mutation was found. One of them was characterized by severe, early-onset dysplasia of the proximal femurs with almost complete absence of the secondary ossification centres and abnormal development of the femoral necks. The other phenotype was characterized by 'mini-epiphyses', resulting in severe dysplasia of the proximal femoral heads. The findings suggest that mutations in the known genes are not the major cause of MED and are responsible for less than half of the cases. The existence of additional MED loci is supported by the exclusion of known loci by mutation analysis and finding of specific subgroups among these patients.

show abstract

Recessive multiple epiphyseal dysplasia (rMED): phenotype delineation in eighteen homozygotes for DTDST mutation R279W

Cited by 66 publications

References 20 publications

Analysis of 589,306 genomes identifies individuals resilient to severe Mendelian childhood diseases

Analysis of 589,306 genomes identifies individuals resilient to severe Mendelian childhood diseases

Solute Carrier Family 26 Member a2 (Slc26a2) Protein Functions as an Electroneutral SO42−/OH−/Cl− Exchanger Regulated by Extracellular Cl−

Mutations in the known genes are not the major cause of MED; distinctive phenotypic entities among patients with no identified mutations

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