Association of early-onset Alzheimer's disease with an interleukin-1? gene polymorphism

Luigi Grimaldi(University of Milan), Valeria M. Casadei(University of Milan), Cinzia Ferri(University of Milan), Fabrizio Veglia, Federico Licastro(University of Bologna), Giorgio Annoni(University of Milan), Ida Biunno(Tecnologie Avanzate (Italy)), Gianluca De Bellis(Tecnologie Avanzate (Italy)), Sandro Sorbi(University of Florence), Claudio Mariani, Nicola Canal(University of Milan), W. Sue T. Griffin(University of Arkansas for Medical Sciences), M. Franceschi
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Abstract

Overexpression of the pluripotent cytokine interleukin-1 (IL-1) by microglial cells correlates with formation of neuritic beta-amyloid plaques in Alzheimer's disease (AD). We evaluated polymorphisms in the genes coding for the IL-1alpha, IL-1beta, and IL-1 receptor antagonist cytokines, and tested their association with the occurrence and age at onset of sporadic AD. We found a strong association between the IL-1A T/T genotype and AD onset before 65 years of age (odds ratio, 4.86), with carriers of this genotype showing an onset of disease 9 years earlier than IL-1A C/C carriers. A weaker association with the age at onset was also shown for the IL-1B and IL-1RN genes. These data suggest either a direct effect of the IL-1 gene family, mainly IL-1A, on the clinical onset of AD, or a linkage dysequilibrium with an unknown locus relevant to AD on chromosome 2.


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