Cognitively healthy centenarians are characterized by lower frequencies of six disease-associatedHLAalleles

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Abstract

Background

Human leukocyte antigen (HLA) genes are key regulators of immune function and have been implicated in susceptibility to various diseases. However, their role in healthy longevity remains unclear. Here, we investigate the relationship between disease-associatedHLAalleles and the likelihood of becoming a cognitively healthy centenarian (CHC).

Methods

We imputedHLAgenotypes using genetic data from 3,634 individuals, including 354 CHCs from the Dutch 100-plus Study and 3,269 middle-aged healthy individuals from multiple Dutch cohorts. We examined associations between 59HLAalleles previously linked to 12 diseases—including Alzheimer’s disease (AD), ten autoimmune disorders, and SARS- CoV-2—and the likelihood of becoming a CHC. Logistic regression models were used to estimate odds ratios (ORs), adjusting for population structure. We then calculated centenarian effect ratios (CERs) to compare the effect sizes ofHLAalleles on the chance of becoming a CHC relative to their known effects on disease susceptibility, assessing the directions of potential pleiotropic effects.

Results

While the genomes of CHCs were not enriched with any specificHLAalleles, six alleles reduced the likelihood of becoming a CHC (ORs=0.59–0.74, FDR<0.1). These alleles clustered into three haplotypes based on linkage disequilibrium: a class II haplotype (HLA- DRB1*01:01,HLA-DQA1*01:01,HLA-DQB1*05:01), a class I haplotype (HLA-C*03:04,HLA-B*40:01), and an independent class I allele (HLA-A*02:01). We identified both synergistic and antagonistic pleiotropic relationships between autoimmune disease-associatedHLAalleles and becoming a CHC, with similar magnitudes of effect sizes.HLAalleles associated with increased risk of AD consistently exhibited synergistic pleiotropies, with a 5- to 10-fold larger effect on decreased likelihood of healthy longevity.

Conclusions

Our findings highlight a complex interplay betweenHLAalleles associated with autoimmune disease susceptibility and healthy longevity. The strongly increased effect sizes and synergistic pleiotropic relationships between the likelihood of becoming a cognitively healthy centenarian andHLAalleles previously associated with AD, highlight the involvement of immune-related mechanisms in longevity and neurodegeneration. Further studies, employing Next-Generation-Sequencing and Long-Read-Sequencing, preferably in diverse populations, are needed to map our findings to the full genetic resolution of theHLAregion.

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