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Research ArticleBRAIN

Genetic Correlations of Brain Lesion Distribution in Multiple Sclerosis: An Exploratory Study

M.H. Sombekke, M.M. Vellinga, B.M.J. Uitdehaag, F. Barkhof, C.H. Polman, D. Arteta, D. Tejedor, A. Martinez, J.B.A. Crusius, A.S. Peña, J.J.G. Geurts and H. Vrenken
American Journal of Neuroradiology March 2011, DOI: https://doi.org/10.3174/ajnr.A2352
M.H. Sombekke
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M.M. Vellinga
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B.M.J. Uitdehaag
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F. Barkhof
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C.H. Polman
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D. Arteta
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D. Tejedor
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A. Martinez
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J.B.A. Crusius
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A.S. Peña
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J.J.G. Geurts
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H. Vrenken
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Abstract

BACKGROUND AND PURPOSE: In MS, the total brain lesion volume and spatial distribution of lesions across the brain vary widely among individual patients. We hypothesized that spatial distribution may be partially driven by genetic predisposition, and we aimed to explore relations among candidate genes and the spatial distribution of white matter brain lesions in MS.

MATERIAL AND METHODS: Genotypes of 69 SNPs in 208 patients with MS were related to the spatial distribution of T2 brain lesions. Lesions were manually outlined on MR images, and binary lesion masks were produced and registered to a common space. With Randomise software, the lesion masks were related to genotype by using a voxelwise nonparametric GLM approach, followed by clusterwise analysis. We used a DNA chip with SNPs selected from the literature on MS susceptibility, severity, and phenotypes.

RESULTS: For 11 of these SNPs, 1 of the genotypes expressed significant clusters of increased or decreased lesion probability in varying, predominantly periventricular, brain regions. When we statistically controlled the voxelwise analyses for effects of total brain lesion volume, only 1 SNP remained significant: rs2227139, located within the MHC class II region. This SNP retained its periventricular cluster of significantly increased lesion probability for the heterozygote genotype.

CONCLUSIONS: Heterozygosity of rs2227139 (MHC class II region) is associated with increased right frontal periventricular lesion probability (P < .01). Ten other SNPs showed associations between genotype and spatial lesion distribution that are partly explained by total lesion volume.

Footnotes

  • BTNL2
    butyrophilin-like 2
    CCL5
    chemokine (C-C motif) ligand 5
    CCR5
    chemokine (C-C motif) receptor 5
    CNS
    central nervous system
    CRYAB
    α B crystallin
    EAE
    experimental autoimmune encephalomyelitis
    EDSS
    Expanded Disability Status Scale
    FAS
    tumor necrosis factor receptor superfamily, member 6
    FLIRT
    FMRIB Nonlinear Image Registration Tool
    FSL
    FMRIB Software Library
    FMRIB
    Functional MR Imaging of the Brain
    GLM
    general linear model
    HLA
    human leucocyte antigen
    HLA-DRB1
    major histocompatibility complex, class II, DRB1 (Homo sapiens)
    IFNGR2
    interferon gamma receptor 2 (interferon γ transducer 1)
    IQR
    interquartile range
    LPM
    lesion probability mapping
    MAF
    minor allele frequency
    MHC
    major histocompatibility complex
    MS
    multiple sclerosis
    NADH
    nicotinamide adenine dinucleotide
    NDUFS7
    NADH dehydrogenase (ubiquinone) Fe-S protein 7
    PNMT
    phenylethanolamine N-methyltransferase
    PPMS
    primary-progressive MS
    RRMS
    relapsing-remitting MS
    rs-nr
    RefSNP accession ID
    SNP
    single nucleotide polymorphism
    SPMS
    secondary-progressive MS
    UCP2
    uncoupling protein 2

  • © 2011 American Society of Neuroradiology
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Cite this article
M.H. Sombekke, M.M. Vellinga, B.M.J. Uitdehaag, F. Barkhof, C.H. Polman, D. Arteta, D. Tejedor, A. Martinez, J.B.A. Crusius, A.S. Peña, J.J.G. Geurts, H. Vrenken
Genetic Correlations of Brain Lesion Distribution in Multiple Sclerosis: An Exploratory Study
American Journal of Neuroradiology Mar 2011, DOI: 10.3174/ajnr.A2352

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Genetic Correlations of Brain Lesion Distribution in Multiple Sclerosis: An Exploratory Study
M.H. Sombekke, M.M. Vellinga, B.M.J. Uitdehaag, F. Barkhof, C.H. Polman, D. Arteta, D. Tejedor, A. Martinez, J.B.A. Crusius, A.S. Peña, J.J.G. Geurts, H. Vrenken
American Journal of Neuroradiology Mar 2011, DOI: 10.3174/ajnr.A2352
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