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Channelopathy-Related Scn10a Gene Variants Predict Cerebellar Dysfunction in Multiple Sclerosis Publisher Pubmed



Roostaei T1, 2, 6, 7 ; Sadaghiani S1, 2 ; Park MTM8, 9 ; Mashhadi R3 ; Nazeri A1 ; Noshad S1 ; Salehi MJ10 ; Naghibzadeh M1, 2 ; Moghadasi AN1, 4 ; Owji M1 ; Doosti R1 ; Taheri APH5 ; Rad AS5 ; Azimi A1, 11 Show All Authors
Authors
  1. Roostaei T1, 2, 6, 7
  2. Sadaghiani S1, 2
  3. Park MTM8, 9
  4. Mashhadi R3
  5. Nazeri A1
  6. Noshad S1
  7. Salehi MJ10
  8. Naghibzadeh M1, 2
  9. Moghadasi AN1, 4
  10. Owji M1
  11. Doosti R1
  12. Taheri APH5
  13. Rad AS5
  14. Azimi A1, 11
  15. Chakravarty MM8, 12
  16. Voineskos AN6, 7
  17. Nazeri A1
  18. Sahraian MA1, 4
Show Affiliations
Authors Affiliations
  1. 1. MS Research Center, Neuroscience Institute, Tehran University of Medical Sciences, Iran
  2. 2. Interdisciplinary Neuroscience Research Program, Tehran University of Medical Sciences, Iran
  3. 3. Urology Research Center, Tehran University of Medical Sciences, Iran
  4. 4. Department of Neurology, Tehran University of Medical Sciences, Iran
  5. 5. Department of Radiology, Tehran University of Medical Sciences, Iran
  6. 6. Kimel Family Translational Imaging-Genetics Laboratory, Research Imaging Centre, Campbell Family Mental Health Institute, Centre for Addiction and Mental Health, Toronto, Canada
  7. 7. Department of Psychiatry, University of Toronto, Canada
  8. 8. Cerebral Imaging Centre, Douglas Mental Health Institute, Verdun, France
  9. 9. Schulich School of Medicine and Dentistry, Western University, London, Canada
  10. 10. Department of Electrical Engineering, Sharif University of Technology, Tehran, Iran
  11. 11. Department of Neurology, Thomas Jefferson University, Philadelphia, PA, United States
  12. 12. Departments of Psychiatry and Biomedical Engineering, McGill University, Montreal, Canada

Source: Neurology Published:2016


Abstract

Objective: To determine the motor-behavioral and neural correlates of putative functional common variants in the sodium-channel NaV1.8 encoding gene (SCN10A) in vivo in patients with multiple sclerosis (MS). Methods: We recruited 161 patients with relapsing-onset MS and 94 demographically comparable healthy participants. All patients with MS underwent structural MRI and clinical examinations (Expanded Disability Status Scale [EDSS] and Multiple Sclerosis Functional Composite [MSFC]). Whole-brain voxel-wise and cerebellar volumetry were performed to assess differences in regional brain volumes between genotype groups. Resting-state fMRI was acquired from 62 patients with MS to evaluate differences in cerebellar functional connectivity. All participants were genotyped for 4 potentially functional SCN10A polymorphisms. Results: Two SCN10A polymorphisms in high linkage disequilibrium (r2 = 0.95) showed significant association with MSFC performance in patients with MS (rs6795970: p = 6.2 × 10-4; rs6801957: p = 0.0025). Patients with MS with rs6795970AA genotype performed significantly worse than rs6795970G carriers in MSFC (p = 1.8 × 10-4) and all of its subscores. This association was independent of EDSS and cerebellar atrophy. Although the genotype groups showed no difference in regional brain volumes, rs6795970AA carriers demonstrated significantly diminished cerebellar functional connectivity with the thalami and midbrain. No significant SCN10A-genotype effect was observed on MSFC performance in healthy participants. Conclusions: Our data suggest that SCN10A variation substantially influences functional status, including prominent effects on motor coordination in patients with MS. These findings were supported by the effects of this variant on a neural system important for motor coordination, namely cerebello-thalamic circuitry. Overall, our findings add to the emerging evidence that suggests that sodium channel NaV1.8 could serve as a target for future drug-based interventions to treat cerebellar dysfunction in MS. © 2016 American Academy of Neurology.
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