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Abstract

Background:

Multiple sclerosis (MS) treatment response varies significantly, hindering effective management and necessitating better predictive biomarkers. Pharmacogenomics offers a promising avenue to identify genetic markers that, combined with clinico-demographic predictors, could enhance personalized therapeutic decisions.

Objectives:

This multi-center study investigated genetic determinants of response to interferon-beta (IFN-β) and glatiramer acetate (GA) in European ancestry patients with relapsing–remitting MS (RRMS).

Methods:

After harmonization and quality control, we tested over 6 million genetic variants. We used negative binomial regression, meta-analysis, and gene-set enrichment to link variants, genes, and biological pathways to treatment response.

Results:

In 679 GA and 1614 IFN-β patients, the top GA variant was rs2053696A in MAP3 K1 (p = 3.97*10⁻⁹), involved in key signaling pathways. Another significant GA signal was in WWOX. For IFN-β, no genome-wide significant variants were found, but suggestive signals emerged near ZMIZ1, ZCCHC7, and other genes linked to immune function and interferon signaling. Gene-set analysis revealed IL-17 regulation for GA and ion channel pathways for IFN-β.

Conclusion:

This study identified novel genetic variants for GA response, implicating genes in crucial pathways. For IFN-β, suggestive signals point to immune and interferon-related genes. These findings enhance our understanding of genetic influences on RRMS treatment response, while highlighting pharmacogenomic research challenges.

Keywords

Multiple sclerosis pharmacogenomics interferons glatiramer acetate

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References

Compston

Coles

. Multiple sclerosis. Lancet 2008; 372(9648): 1502–1517.

International Multiple Sclerosis Genetics Consortium. Multiple sclerosis genomic map implicates peripheral immune cells and microglia in susceptibility. Science 2019; 365(6460): eaav7188.

Grossman

Knappertz

Laifenfeld

, et al. Pharmacogenomics strategies to optimize treatments for multiple sclerosis: Insights from clinical research. Prog Neurobiol 2017; 152: 114–130.

Huth

Gardin

Umehara

, et al. Prediction of the impact of cytochrome P450 2C9 genotypes on the drug-drug interaction potential of siponimod with physiologically-based pharmacokinetic modeling: A comprehensive approach for drug label recommendations. Clin Pharmacol Ther 2019; 106(5): 1113–1124.

Martinez-Forero

Pelaez

Villoslada

. Pharmacogenomics of multiple sclerosis: In search for a personalized therapy. Expert Opin Pharmacother 2008; 9(17): 3053–3067.

Ingwersen

Aktas

Hartung

. Advances in and algorithms for the treatment of relapsing-remitting multiple sclerosis. Neurotherapeutics 2016; 13(1): 47–57.

Johnson

Brooks

Cohen

, et al. Copolymer 1 reduces relapse rate and improves disability in relapsing-remitting multiple sclerosis: Results of a phase III multicenter, double-blind placebo-controlled trial. The Copolymer 1 Multiple Sclerosis Study Group. Neurology 1995; 45(7): 1268–1276.

Hočevar

Ristić

Peterlin

. Pharmacogenomics of multiple sclerosis: A systematic review. Front Neurol 2019; 10: 134.

Clarelli

Corona

Pääkkönen

, et al. Pharmacogenomics of clinical response to Natalizumab in multiple sclerosis: A genome-wide multi-centric association study. J Neurol 2024; 271(11): 7250–7263.

10.

International Multiple Sclerosis Genetics Consortium; MultipleMS Consortium. Locus for severity implicates CNS resilience in progression of multiple sclerosis. Nature 2023; 619(7969): 323–331.

11.

Clarelli

Liberatore

Sorosina

, et al. Pharmacogenetic study of long-term response to interferon-β treatment in multiple sclerosis. Pharmacogenomics J 2017; 17(1): 84–91.

12.

Aharoni

Eilam

Domev

, et al. The immunomodulator glatiramer acetate augments the expression of neurotrophic factors in brains of experimental autoimmune encephalomyelitis mice. Proc Natl Acad Sci U S A 2005; 102(52): 19045–19050.

13.

Melnikov

Sharanova

Sviridova

, et al. The influence of glatiramer acetate on Th17-immune response in multiple sclerosis. PLoS ONE 2020; 15(10): e0240305.

14.

Tumani

Kassubek

Hijazi

, et al. Patterns of TH1/TH2 cytokines predict clinical response in multiple sclerosis patients treated with glatiramer acetate. Eur Neurol 2011; 65(3): 164–169.

15.

Jensen

, et al. Quantitative assessment of iron accumulation in the deep gray matter of multiple sclerosis by magnetic field correlation imaging. AJNR Am J Neuroradiol 2007; 28(9): 1639–1644.

16.

Achiron

Gurevich

Snir

, et al. Zinc-ion binding and cytokine activity regulation pathways predicts outcome in relapsing-remitting multiple sclerosis. Clin Exp Immunol 2007; 149(2): 235–242.

17.

Kotelnikova

Kiani

Messinis

, et al. MAPK pathway and B cells overactivation in multiple sclerosis revealed by phosphoproteomics and genomic analysis. Proc Natl Acad Sci U S A 2019; 116(19): 9671–9676.

18.

Aldaz

Hussain

. WWOX loss of function in neurodevelopmental and neurodegenerative disorders. Int J Mol Sci 2020; 21(23): 8922.

19.

Liu

Wang

Zhao

, et al. Identification of novel drug targets for multiple sclerosis by integrating plasma genetics and proteomes. Exp Gerontol 2024; 194: 112505.

20.

Parnell

Schibeci

Fewings

, et al. The latitude-dependent autoimmune disease risk genes ZMIZ1 and IRF8 regulate mononuclear phagocytic cell differentiation in response to vitamin D. Hum Mol Genet 2019; 28(2): 269–278.

21.

Lozano-Ros

Martínez-Ginés

García-Domínguez

, et al. Changes in the expression of TGF-beta regulatory pathway genes induced by vitamin D in patients with relapsing-remitting multiple sclerosis. Int J Mol Sci 2023; 24(19): 14447.

22.

Javierre

Burren

Wilder

, et al. Lineage-specific genome architecture links enhancers and non-coding disease variants to target gene promoters. Cell 2016; 167(5): 1369–1384.e19.

23.

Ziętara

Wróblewska

Zajączkowska

, et al. The role of the JAK-STAT pathway in childhood B-cell acute lymphoblastic leukemia. Int J Mol Sci 2024; 25(13): 6844.

24.

Rizzo

Giacomini

Mechelli

, et al. Interferon-β therapy specifically reduces pathogenic memory B cells in multiple sclerosis patients by inducing a FAS-mediated apoptosis. Immunol Cell Biol 2016; 94(9): 886–894.

25.

Mayo

Trauger

Blain

, et al. Regulation of astrocyte activation by glycolipids drives chronic CNS inflammation. Nat Med 2014; 20(10): 1147–1156.

26.

Haas

Smith

Rocher-Ros

, et al. Lactate regulates metabolic and pro-inflammatory circuits in control of T cell migration and effector functions. PLoS Biol 2015; 13(7): e1002202.

27.

Esposito

Sorosina

Ottoboni

, et al. A pharmacogenetic study implicates SLC9a9 in multiple sclerosis disease activity. Ann Neurol 2015; 78(1): 115–127.

28.

Byun

Caillier

Montalban

, et al. Genome-wide pharmacogenomic analysis of the response to interferon beta therapy in multiple sclerosis. Arch Neurol 2008; 65(3): 337–344.

29.

Smith

. Sodium channels and multiple sclerosis: Roles in symptom production, damage and therapy. Brain Pathol 2007; 17(2): 230–242.

30.

Nicolae

Gamazon

Zhang

, et al. Trait-associated SNPs are more likely to be eQTLs: Annotation to enhance discovery from GWAS. PLoS Genet 2010; 6(4): e1000888.

Pharmacogenomics of response to interferon-beta and glatiramer acetate in Multiple Sclerosis: A multi-centric study