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    Genetic polymorphisms, their allele combinations and IFN-β treatment response in Irish multiple sclerosis patients

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    Date
    2009
    Author
    Ochs, Michael F.
    O'Doherty, Catherine
    Favorov, Alexander V.
    Heggarty, Shirley
    Graham, Colin
    Favorova, Olʹga Olegovna
    Hawkins, Stanley
    Hutchinson, Michael
    O'Rourke, Killian
    Vandenbroeck, Koen
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    Abstract
    Abstract
    IFN-β is widely used as first-line immunomodulatory treatment for multiple sclerosis. Response to treatment is variable (30–50% of patients are nonresponders) and requires a long treatment duration for accurate assessment to be possible. Information about genetic variations that predict responsiveness would allow appropriate treatment selection early after diagnosis, improve patient care, with time saving consequences and more efficient use of resources. Materials & methods: We analyzed 61 SNPs in 34 candidate genes as possible determinants of IFN-β response in Irish multiple sclerosis patients. Particular emphasis was placed on the exploration of combinations of allelic variants associated with response to therapy by means of a Markov chain Monte Carlo-based approach (APSampler). Results: The most significant allelic combinations, which differed in frequency between responders and nonresponders, included JAK2–IL10RB–GBP1–PIAS1 (permutation p-value was pperm = 0.0008), followed by JAK2–IL10–CASP3 (pperm = 0.001). Discussion: The genetic mechanism of response to IFN-β is complex and as yet poorly understood. Data mining algorithms may help in uncovering hidden allele combinations involved in drug response versus nonresponse.
    Citation:
    O’Doherty C, Favorov A, Heggarty S, Graham C, Favorova O, Ochs M, Hawkins S, Hutchinson M, O’Rourke K and Vandenbroeck K. Genetic polymorphisms, their allele combinations and interferon-β treatment response in Irish multiple sclerosis patients. Pharmacogenomics. 2009; 10: 1177-86.
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    URI
    https://dx.doi.org/10.2217/pgs.09.41
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