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Multiple Sclerosis

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What's Multiple Sclerosis (MS) First described by Charcot in 1868. ... In 1972, the association between multiple sclerosis and the HLA region of the ... – PowerPoint PPT presentation

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Title: Multiple Sclerosis


1
Multiple Sclerosis
  • CS295 Final Presentation
  • Yongxing Guo
  • Dec. 18, 2007

2
Outlines
  • Introduction to Multiple Sclerosis (MS)
  • Genomewide Association Study of MS
  • IL2RA IL7RA and MS risk
  • Comments

3
Whats Multiple Sclerosis (MS)
  • First described by Charcot in 1868.
  • A chronic inflammatory disease of the central
    nervous system (CNS), the brain and the spinal
    cord.
  • A malfunction of the immune system which leads to
    attacks against, and causes destruction of the
    myelin sheath.
  • Symptoms range from mild muscle weakness to
    partial or complete paralysis.
  • Widely considered an autoimmune disease

4
Epidemiology of Multiple Sclerosis
  • Monozygotic twins concordance rate is nearly 30
  • Siblings or dizygotic twins 2
  • Average Northern European population 0.1
  • Both genetic predisposition and largely unknown
    environmental factors are required to cause the
    disease

5
Association between MS and the HLA MHC Complex
  • In 1972, the association between multiple
    sclerosis and the HLA region of the genome was
    established.
  • HLA-DRB1 gene on chromosome 6p21 was identified.

The human leukocyte antigen system (HLA) is the
name of the human major histocompatibility
complex (MHC). This group of genes resides on
chromosome 6, and encodes cell-surface
antigen-presenting proteins and many other genes.
The major HLA antigens are essential elements in
immune function
6
Other Studies of MS
  • No other loci with a definitive association with
    the disease have been found.
  • Early efforts to screen the genome for linkage
    with the use of low-density maps of
    microsatellites were unsuccessful.
  • These results indicate that in multiple
    sclerosis, linkage studies lack the statistical
    power to detect susceptibility loci that may
    reside outside the HLA-MHC region.

7
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8
Overview
  • A genomewide association study
  • A transmission disequilibrium test of 334,923
    single-nucleotide polymorphisms (SNPs) was
    performed
  • A joint analysis of data from 12,360 subjects
    was performed
  • Alleles of IL2RA and IL7RA and those in the HLA
    locus are identified as heritable risk factors
    for multiple sclerosis

9
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10
Quality Control of Genotyping
MAF Minor Allele Frequency HW Hardy
Weinberg Equilibrium ME Mendelian Errors
11
Screening Analysis
WTCCC Wellcome Trust Case Control
Consortium NIMH National Institute of Mental
Health IMSGC International Multiple Sclerosis
Genetics Consortium
12
Replication Analysis
13
Overview of the Primary Genomewide Association
Scan Involving 931 Family Trios
P values (shown as log10 values) for results of
transmission disequilibrium testing are plotted
across the genome. The classic HLA-DR risk locus
on chromosome 6p21 stands out with strong
statistical significance (Plt110-81).
14
Observed and Expected Distributions for the
Results of Transmission Disequilibrium Testing
Red The expected null distribution Gray
P values for all 334,923 SNPs Black The
observed distribution after exclusion of the
SNPs across the extended HLA region
15
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16
Regional Plots for Associations in IL2RA
17
Regional Plots for Associations in IL7RA
18
Whats IL2RA IL7RA
  • Both are important in are important in T-cell
    mediated immunity
  • IL2RA
  • The interleukin-2 receptor (IL-2R) is
    heterotrimeric protein expressed on the surface
    of certain immune cells, such as lymphocytes,
    that binds and responds to a cytokine called
    interleukin 2.
  • Linked to two other autoimmune diseases type 1
    diabetes and autoimmune thyroid disease.
  • IL7RA
  • The protein encoded by this gene is a receptor
    for interleukine 7 (IL7)
  • Helps to control the activity of a class of
    immune cells called regulatory T cells.
  • IL7RA variant indicate an effect on gene
    expression with a change in the ratio of soluble
    to cell-bound interleukin-7 receptor

19
Comments
  • This is a hypothesis free association study.
  • The increased risk contributed by IL2RA and IL7RA
    is very low and that these two alleles explain
    only a very small proportion of the variance
    (0.2) in the risk of MS.
  • Complex disease association studies need a
    massive number of study samples and the
    collaboration of large consortia because of the
    small effect of common alleles.
  • No clues to new pathways emerged from among the
    top-scoring associations, in contrast to the
    results of some genomewide studies involving
    other complex diseases, such as type 2 diabetes.
  • The best-associated variants in the combined data
    analysis were actually not among the best hits in
    the initial screen
  • Genomewide association studies that rely on
    common SNPs monitor only common alleles
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