Cloning of the SCA7 gene reveals a highly unstable CAG repeat expansion

Gilles David,Nacer Abbas,Giovanni Stevanin,Alexandra Durr,Gaël Yvert,Géraldine Cancel,Chantal Weber,Georges Imbert,Frédéric Saudou,Eric Antoniou,Harry A. Drabkin,Robert M. Gemmill,Paola Giunti,Ali Benomar,Nicholas W. Wood,Merle Ruberg,Yves Agid,Jean-Louis Mandel,Alexis Brice

Cloning of the SCA7 gene reveals a highly unstable CAG repeat expansion

1997

Gilles David
Nacer Abbas
Giovanni Stevanin
Alexandra Durr
Gaël Yvert
Géraldine Cancel
Chantal Weber
Georges Imbert
Frédéric Saudou
Eric Antoniou
Harry A. Drabkin
Robert M. Gemmill
Paola Giunti
Ali Benomar
Nicholas W. Wood
Merle Ruberg
Yves Agid
Jean-Louis Mandel
Alexis Brice

The gene for spinocerebellar ataxia 7 (SCA7) has been mapped to chromosome 3p12–13. By positional cloning, we have identified a new gene of unknown function containing a CAG repeat that is expanded in SCA7 patients. On mutated alleles, CAG repeat size is highly variable, ranging from 38 to 130 repeats, whereas on normal alleles it ranges from 7 to 17 repeats. Gonadal instability in SCA7 is greater than that observed in any of the seven known neuro-degenerative diseases caused by translated CAG repeat expansions, and is markedly associated with paternal transmissions. SCA7 is the first such disorder in which the degenerative process also affects the retina.

Keywords:

Dentatorubral-pallidoluysian atrophy
Locus (genetics)
Genetics
Autosomal dominant cerebellar ataxia
Trinucleotide repeat expansion
Spinocerebellar ataxia
Molecular biology
Allele
Machado–Joseph disease
Gene mapping
Biology
positional cloning

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