AUTHOR=Sánchez-Juan Pascual , Moreno Sonia , de Rojas Itziar , Hernández Isabel , Valero Sergi , Alegret Montse , Montrreal Laura , García González Pablo , Lage Carmen , López-García Sara , Rodrííguez-Rodríguez Eloy , Orellana Adelina , Tárraga Lluís , Boada Mercè , Ruiz Agustín 

TITLE=The MAPT H1 Haplotype Is a Risk Factor for Alzheimer’s Disease in APOE ε4 Non-carriers

JOURNAL=Frontiers in Aging Neuroscience

VOLUME=11

YEAR=2019

URL=https://www.frontiersin.org/journals/aging-neuroscience/articles/10.3389/fnagi.2019.00327

DOI=10.3389/fnagi.2019.00327

ISSN=1663-4365

ABSTRACT=<p>An ancestral inversion of 900 kb on chromosome 17q21, which includes the microtubule-associated protein tau (<italic>MAPT</italic>) gene, defines two haplotype clades in Caucasians (H1 and H2). The H1 haplotype has been linked inconsistently with AD. In a previous study, we showed that an SNP tagging this haplotype (rs1800547) was associated with AD risk in a large population from the Dementia Genetics Spanish Consortium (DEGESCO) including 4435 cases and 6147 controls. The association was mainly driven by individuals that were non-carriers of the <italic>APOE</italic> ε4 allele. Our aim was to replicate our previous findings in an independent sample of 4124 AD cases and 3290 controls from Spain (GR@ACE project) and to analyze the effect of the H1 sub-haplotype structure on the risk of AD. The H1 haplotype was associated with AD risk (OR = 1.12; <italic>p</italic> = 0.0025). Stratification analysis showed that this association was mainly driven by the <italic>APOE</italic> ε4 non-carriers (OR = 1.15; <italic>p</italic> = 0.0022). Pooled analysis of both Spanish datasets (<italic>n</italic> = 17,996) showed that the highest AD risk related to the <italic>MAPT</italic> H1/H2 haplotype was in those individuals that were the oldest [third tertile (&gt;77 years)] and did not carry <italic>APOE</italic> ε4 allele (<italic>p</italic> = 0.001). We did not find a significant association between H1 sub-haplotypes and AD. H1c was nominally associated but lost statistical significance after adjusting by population sub-structure. Our results are consistent with the hypothesis that genetic variants linked to the <italic>MAPT</italic> H1/H2 are tracking a genuine risk allele for AD. The fact that this association is stronger in <italic>APOE</italic> ε4 non-carriers partially explains previous controversial results and might be related to a slower alternative causal pathway less dependent on brain amyloid load.</p>