Osteogenesis Imperfecta

Overview

Journal Nat Rev Dis Primers

Specialty General Medicine

Date 2017 Aug 19

PMID 28820180

Citations 321

Authors

Joan C Marini

Antonella Forlino

Hans Peter Bachinger

Nick J Bishop

Peter H Byers

Anne De Paepe

Francois Fassier

Nadja Fratzl-Zelman

Kenneth M Kozloff

Deborah Krakow

Kathleen Montpetit

Oliver Semler

Affiliations

Soon will be listed here.

Abstract

Skeletal deformity and bone fragility are the hallmarks of the brittle bone dysplasia osteogenesis imperfecta. The diagnosis of osteogenesis imperfecta usually depends on family history and clinical presentation characterized by a fracture (or fractures) during the prenatal period, at birth or in early childhood; genetic tests can confirm diagnosis. Osteogenesis imperfecta is caused by dominant autosomal mutations in the type I collagen coding genes (COL1A1 and COL1A2) in about 85% of individuals, affecting collagen quantity or structure. In the past decade, (mostly) recessive, dominant and X-linked defects in a wide variety of genes encoding proteins involved in type I collagen synthesis, processing, secretion and post-translational modification, as well as in proteins that regulate the differentiation and activity of bone-forming cells have been shown to cause osteogenesis imperfecta. The large number of causative genes has complicated the classic classification of the disease, and although a new genetic classification system is widely used, it is still debated. Phenotypic manifestations in many organs, in addition to bone, are reported, such as abnormalities in the cardiovascular and pulmonary systems, skin fragility, muscle weakness, hearing loss and dentinogenesis imperfecta. Management involves surgical and medical treatment of skeletal abnormalities, and treatment of other complications. More innovative approaches based on gene and cell therapy, and signalling pathway alterations, are under investigation.

Citing Articles

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