Mutation screening of spastin, atlastin, and REEP1 in hereditary spastic paraplegia

McCorquodale DS III, Ozomaro U, Huang J, Montenegro G, Kushman A, Citrigno L, Price J, Speziani F, Pericak‐Vance MA, Züchner S. Mutation screening of spastin, atlastin, and REEP1 in hereditary spastic paraplegia. Hereditary spastic paraplegia (HSP) comprises a group of clinically and genetically het...

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Published inClinical genetics Vol. 79; no. 6; pp. 523 - 530
Main Authors McCorquodale III, DS, Ozomaro, U, Huang, J, Montenegro, G, Kushman, A, Citrigno, L, Price, J, Speziani, F, Pericak-Vance, MA, Züchner, S
Format Journal Article
LanguageEnglish
Published Oxford, UK Blackwell Publishing Ltd 01.06.2011
Subjects
Adenosine Triphosphatases - genetics
Adolescent
Adult
ATL1
Child
Child, Preschool
Female
Genes, Dominant
Genes, Recessive
Genetic disorders
Genetic Markers
Genetic Testing
GTP Phosphohydrolases - genetics
GTP-Binding Proteins
Heat shock proteins
hereditary spastic paraplegia
Hereditary spastic parplegia
Humans
INDEL Mutation
Infant
Male
Medical screening
Membrane Proteins
Membrane Transport Proteins - genetics
Middle Aged
Motor neurons
Mutation
Mutation, Missense
Neurological disorders
REEP1
SPAST
Spastic Paraplegia, Hereditary - genetics
Spastin
X chromosome
Young Adult
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Summary:McCorquodale DS III, Ozomaro U, Huang J, Montenegro G, Kushman A, Citrigno L, Price J, Speziani F, Pericak‐Vance MA, Züchner S. Mutation screening of spastin, atlastin, and REEP1 in hereditary spastic paraplegia. Hereditary spastic paraplegia (HSP) comprises a group of clinically and genetically heterogeneous diseases that affect the upper motor neurons and their axonal projections. Over 40 chromosomal loci have been identified for autosomal dominant, recessive, and X‐linked HSP. Mutations in the genes atlastin, spastin and REEP1 are estimated to account for up to 50% of autosomal‐dominant HSP and currently guide the molecular diagnosis of HSP. Here, we report the mutation screening results of 120 HSP patients from North America for spastin, atlastin, and REEP1, with the latter one partially reported previously. We identified mutations in 36.7% of all tested HSP patients and describe 20 novel changes in spastin and atlastin. Our results add to a growing number of HSP disease‐associated variants and confirm the high prevalence of atlastin, spastin, and REEP1 mutations in the HSP patient population.
Bibliography:ArticleID:CGE1501
istex:D1EFC30DAA2D079015C8A34F3844E828FB4D559F
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These authors have contributed equally to this work.
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These authors contributed equally to this work.
ISSN:0009-9163
1399-0004
DOI:10.1111/j.1399-0004.2010.01501.x