AI Article Synopsis
- Dyggve-Melchior-Clausen syndrome (DMC) and Smith-McCort dysplasia (SMC) are rare genetic disorders affecting bone development, linked to mutations in the DYM gene on chromosome 18.
- DMC typically results from loss-of-function mutations leading to more severe skeletal issues, while SMC is associated with milder missense mutations that may retain some DYM activity.
- A study of three consanguineous families revealed specific mutations in DMC, but no mutations were found in one SMC family, indicating potential genetic differences within these disorders.
Article Abstract
Dyggve-Melchior-Clausen syndrome (DMC) (MIM 223800) and Smith-McCort dysplasia (SMC) (MIM 607326) are rare allelic autosomal recessive spondylo-epi-metaphyseal dysplasias (SEMDs) characterized by similar skeletal manifestations. Both phenotypes have been mapped to chromosome 18q21.1 and mutations in the DYM (dymeclin) gene were identified in 13 families with DMC and in two families with SMC. Most mutations identified in DMC predict a loss of function, while those identified in SMC are mainly missense mutations, presumably associated with residual DYM activity and a less severe phenotype. We studied three consanguineous families from Turkey, Lebanon, and Georgia, one with SMC and two with DMC and identified different homozygous DYM mutations (IVS3 194-1G > A, 938_942delTGTCT) in the DMC families. No mutation was identified in the SMC family, possibly suggesting genetic heterogeneity of this disorder.
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| http://dx.doi.org/10.1002/ajmg.a.31090 | DOI Listing |
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