Phenotype of AD-HSP due to mutations in the SPAST gene: Comparison with AD-HSP without mutations

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Phenotype of AD-HSP due to mutations in the SPAST gene

Comparison with AD-HSP without mutations

P. McMonagle, MRCPI;, P.C. Byrne, PhD;, B. Fitzgerald, MB;, S. Webb, MD;, N.A. Parfrey, MD; and M. Hutchinson, FRCP

From the Department of Neurology (Drs. McMonagle, Webb, and Hutchinson), St. Vincent’s University Hospital and Department of Pathology (Drs. Byrne and Parfrey, B. Fitzgerald), University College Dublin and St. Vincent’s University Hospital, Dublin, Ireland.

Address correspondence and reprint requests to Dr. P. McMonagle, Department of Neurology, St. Vincent’s University Hospital, Elm Park, Dublin 4, Ireland; e-mail: p.mcmonagle{at}st-vincents.ie

BACKGROUND: "Pure" autosomal dominant hereditary spastic paraparesis(AD-HSP) is clinically and genetically heterogeneous. Thereare at least seven genetic loci with varying ages at onset anddisability. The SPAST gene at the SPG4 locus on chromosome 2pis the major disease gene for AD-HSP.

OBJECTIVES: To investigate whether there are distinct clinicalfeatures among families with AD-HSP due to SPAST mutations comparedwith families excluded from SPG4.

METHODS: Nineteen families with "pure" AD-HSP were identified,and the clinical features of family members were compared usinga standard protocol. With use of genetic studies, the familieswere divided into two groups for comparison: those with mutationsin SPAST, the "mutation-positive" group, and those excludedfrom SPG4 on the basis of linkage studies, the "SPG4-excluded"group.

RESULTS: Twenty-nine individuals from four families had mutationsin SPAST, whereas 22 individuals from three families comprisedthe SPG4-excluded group; in 11 families, the pattern of linkagewas unknown. In the one remaining family, no mutations werefound despite strong linkage to SPG4. Different mutations wereidentified in the four SPAST pedigrees, but the clinical picturewas similar in each. Comparison of the mutation-positive groupwith the SPG4-excluded group revealed an older age at onset(p = 0.03), more disability (p = 0.001), more rapidly progressiveparaparesis (p = 0.044), and more cognitive impairment (p =0.024) among affected individuals with SPAST mutations, notconfounded by disease duration. Conclusion: Despite differentmutations, SPAST families have a similar phenotype that canbe distinguished from other genetic groups.

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