Mutations in a newly identified GTPase gene cause autosomal dominant hereditary spastic paraplegia.

Journal: Nature Genetics
Published:
Abstract

The hereditary spastic paraplegias (HSPs; Strümpell-Lorrain syndrome, MIM number 18260) are a diverse class of disorders characterized by insidiously progressive lower-extremity spastic weakness (reviewed in refs. 1-3). Eight autosomal dominant HSP (ADHSP) loci have been identified, the most frequent of which is that linked to the SPG4 locus on chromosome 2p22 (found in approximately 42%), followed by that linked to the SPG3A locus on chromosome 14q11-q21 (in approximately 9%). Only SPG4 has been identified as a causative gene in ADHSP. Its protein (spastin) is predicted to participate in the assembly or function of nuclear protein complexes. Here we report the identification of mutations in a newly identified GTPase gene, SPG3A, in ADHSP affected individuals.

Authors
X Zhao, D Alvarado, S Rainier, R Lemons, P Hedera, C Weber, T Tukel, M Apak, T Heiman Patterson, L Ming, M Bui, J Fink

Similar Publications

Novel mutations in the Atlastin gene (SPG3A) in families with autosomal dominant hereditary spastic paraplegia and evidence for late onset forms of HSP linked to the SPG3A locus.
Novel mutations in the Atlastin gene (SPG3A) in families with autosomal dominant hereditary spastic paraplegia and evidence for late onset forms of HSP linked to the SPG3A locus.
Journal: Human mutation
Published: December 26, 2003
Hereditary spastic paraplegia: clinical genetic study of 15 families.
Hereditary spastic paraplegia: clinical genetic study of 15 families.
Journal: Archives of neurology
Published: June 24, 2004
Expansion of the phenotypic spectrum of SPG6 caused by mutation in NIPA1.
Expansion of the phenotypic spectrum of SPG6 caused by mutation in NIPA1.
Journal: Clinical neurology and neurosurgery
Published: April 17, 2010