Molecular heterogeneity in the mild autosomal dominant forms of osteogenesis imperfecta. Academic Article

abstract

• Mild osteogenesis imperfecta (OI type I and OI type IV) is characterized by postnatal onset of fractures, absence of skeletal deformity, presenile hearing loss with or without blue sclerae, and dentinogenesis imperfecta. Using one common DNA polymorphism associated with the pro alpha 2(I) human collagen gene, we found genetic heterogeneity in this disorder. In three families, the OI phenotype segregated independently of the DNA polymorphism, whereas in one family, the OI phenotype cosegregated with a DNA polymorphism in a manner suggesting linkage. Use of DNA polymorphisms associated with both type I procollagen genes should provide a tool to unravel the molecular heterogeneity of various heritable disorders of the connective tissue.

authors

• Prockop, Darwin

published proceedings

• Am J Hum Genet

author list (cited authors)

• Tsipouras, P., Brresen, A. L., Dickson, L. A., Berg, K., Prockop, D. J., & Ramirez, F.

citation count

• 50

complete list of authors

• Tsipouras, P||Børresen, AL||Dickson, LA||Berg, K||Prockop, DJ||Ramirez, F

publication date

• November 1984

published in

• American Journal of Human Genetics  Journal

keywords

• DNA Restriction Enzymes
• Genes, Dominant
• Genotype
• Heterozygote
• Humans
• Osteogenesis Imperfecta
• Pedigree
• Phenotype
• Polymorphism, Genetic
• Procollagen

PubMed Central ID

• 6097110

start page

• 1172

end page

• 1179

volume

• 36

issue

• 6