An APOE haplotype associated with decreased ε4 expression increases the risk of late onset Alzheimer's disease.

6533b871fe1ef96bd12d23c3

RESEARCH PRODUCT

An APOE haplotype associated with decreased ε4 expression increases the risk of late onset Alzheimer's disease.

Daniela Galimberti Francesco Lescai Francesco Lescai Carlo Gabelli Sandro Sorbi Roberta Ghidoni Aurelia Santoro Diego Albani Chiara Pirazzini Chiara Pirazzini Giuseppe D'agostino Federica Esposito Alessandra Codemo Filippo Martinelli Boneschi Gaetano Crepaldi Elio Scarpini Maurizio Cardelli Claudio Franceschi Fabrizio Tagliavini Giuliano Binetti Luisa Benussi Francesca Marchegiani Cristina Ruaro Gianluigi Forloni Fabiola Olivieri Andrea Maria Chiamenti Benedetta Nacmias

subject

Apolipoprotein E Male Linkage disequilibrium GENETICS Apolipoprotein E4 Late onset Genome-wide association study Biology Polymorphism Single Nucleotide Linkage Disequilibrium Alzheimer Disease Risk Factors medicine Humans Genetic Predisposition to Disease Longitudinal Studies Allele Genetics Chi-Square Distribution General Neuroscience Haplotype Age Factors General Medicine Single Nucleotide medicine.disease POLYMORPHISM Psychiatry and Mental health Clinical Psychology Haplotypes Italy Female Apolipoprotein E Geriatrics and Gerontology Alzheimer's disease Age of onset Genome-Wide Association Study

description

This paper addresses a tenet of the literature on APOE, i.e., the relationship between the effects of the e4, one of the established genetic risk factor for Alzheimer's disease (AD), and its expression levels as determined by APOE promoter polymorphisms. Five polymorphisms (-491 rs449647, -427 rs769446, -219 rs405509, and e rs429358-rs7412) were studied in 1308 AD patients and 1082 control individuals from the Central-Northern Italy. Major findings of the present study are the following: 1) the variants -219T and e4 increase the risk for late onset AD (LOAD) when they are both present in cis on the same chromosome (in phase); 2) the correlation between the haplotype (-219T/e4) and AD risk persists when the data are stratified by age; 3) this haplotype likely anticipates the age of onset of the disease. These data, while confirming the association between -219T and AD, highlight the importance of the phase of the alleles for the observed effects on AD risk, suggesting that this information has to be taken into account when assessing the AD genetic risk. Moreover, the data help to clarify the apparent discrepancy that emerges from the genetic analysis where an SNP characterizing the haplotype responsible for an increased risk for LOAD is coherently associated with a reduced expression of ApoE levels. Our data are compatible with the hypothesis of a complex role of ApoE in the AD pathogenesis, with positive and negative effects occurring concomitantly according to its expression levels and its protein-protein interactions largely unclarified.

year	journal	country	edition	language
2011-01-01	Journal of Alzheimer's disease : JAD

10.3233/jad-2011-101764 https://pubmed.ncbi.nlm.nih.gov/21206004