AI Article Synopsis
- The study investigated mutations in the SOD1 gene among 66 sporadic and 4 familial ALS cases in Italy.
- A new nonsense mutation (K136X) and two known missense mutations (N65S, A95T) were identified in sporadic cases, showing varying disease severity.
- No links were found between intronic sequence variations and ALS, as the frequency of these variations in patients did not differ from that of 181 controls.
Article Abstract
Mutations in the SOD1 gene exons and exon/intron boundaries were searched in 66 sporadic and 4 familial Italian ALS cases consecutively referred to our centre from different Italian regions. A mutation was found in three sporadic cases (4.5%): a new nonsense mutation in exon 5 (K136X) in a patient with a rapid and severe disease course and two previously described missense nucleotide substitutions (N65S and A95T) in two patients with a mild disease course. Comparison of the clinical characteristics with previously reported patients carrying the same or similar mutations showed a remarkable genotype-phenotype correlation. No association was found with intronic sequence variations by comparing their frequency in the patients and in 181 matched controls.
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| http://dx.doi.org/10.1016/j.nmd.2006.07.004 | DOI Listing |
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