SMN mRNA and protein levels in peripheral blood: biomarkers for SMA clinical trials

CJ Sumner, SJ Kolb, GG Harmison, NO Jeffries… - Neurology, 2006 - AAN Enterprises
CJ Sumner, SJ Kolb, GG Harmison, NO Jeffries, K Schadt, RS Finkel, G Dreyfuss
Neurology, 2006AAN Enterprises
Background: Clinical trials of drugs that increase SMN protein levels in vitro are currently
under way in patients with spinal muscular atrophy. Objective: To develop and validate
measures of SMN mRNA and protein in peripheral blood and to establish baseline SMN
levels in a cohort of controls, carriers, and patients of known genotype, which could be used
to follow response to treatment. Methods: SMN1 and SMN2 gene copy numbers were
determined in blood samples collected from 86 subjects. Quantitative reverse transcription …
Background: Clinical trials of drugs that increase SMN protein levels in vitro are currently under way in patients with spinal muscular atrophy.
Objective: To develop and validate measures of SMN mRNA and protein in peripheral blood and to establish baseline SMN levels in a cohort of controls, carriers, and patients of known genotype, which could be used to follow response to treatment.
Methods: SMN1 and SMN2 gene copy numbers were determined in blood samples collected from 86 subjects. Quantitative reverse transcription PCR was used to measure blood levels of SMN mRNA with and without exon 7. A cell immunoassay was used to measure blood levels of SMN protein.
Results: Blood levels of SMN mRNA and protein were measured with high reliability. There was little variation in SMN levels in individual subjects over a 5-week period. Levels of exon 7-containing SMN mRNA and SMN protein correlated with SMN1 and SMN2 gene copy number. With the exception of type I SMA, there was no correlation between SMN levels and disease severity.
Conclusion: SMN mRNA and protein levels can be reliably measured in the peripheral blood and used during clinical trials in spinal muscular atrophy, but these levels do not necessarily predict disease severity.
American Academy of Neurology