A family with Ehlers -- Danlos syndrome type III/articular hypermobility syndrome has a glycine 637 to serine substitution in type III collagen

doi:10.1093/hmg/3.9.1617

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A family with Ehlers — Danlos syndrome type III/articular hypermobility syndrome has a glycine 637 to serine substitution in type III collagen

Paolo Narcisi, Allan J.Richards^*, Stanley D. Ferguson¹ and F.Michael Pope

Dermatology Research Group, Clinical Research Centre Watford Road, Harrow, Middlesex HA1 3UJ ¹Department of Paediatrics, Royal Gwent Hospital Newport, Gwent, UK

^*To whom correspondence should be addressed

Received May 10, 1994; Revised July 6, 1994; Accepted July 6, 1994

Ehlers — Danlos syndrome (EDS) is a heterogeneous groupof heritable disorders of connective tissue. The type III varietyis characterized by joint hypermobility and minor hyperextensibilityand softness of the skin. While collagen fibril structure hasbeen shown to be abnormal in such patients, the underlying moleculardefect(s) has not been determined. Here we characterize thefirst mutation found in a family with EDS III. Analysis of culturedfibroblasts from the affected family revealed intracellularretention of type III collagen. This is usually a biochemicalcharacteristic of EDS IV, caused by mutations of COL3A1. Analysisof the cDNA sequence in this EDS III family revealed a glycineto serine mutation at amino acid residue 637 of the type IIIcollagen molecule. This was confirmed by allele-specific oligonucleotidehybridization against amplified genomic DNA. Thus mutationsof type III collagen can cause either EDS IV or EDS III. Twoaffected family members had virtually normal skin and so moreclosely resembled the phenotype of articular hypermobility syndrome.

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A family with Ehlers — Danlos syndrome type III/articular hypermobility syndrome has a glycine 637 to serine substitution in type III collagen

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