Variant-to-function mapping of late-onset Alzheimer's disease GWAS signals in human microglial cell models implicates RTFDC1 at the CASS4 locus.
Elizabeth A BurtonMariana ArgenzianoKieona CookMolly RidlerSumei LuChun SuElisabetta ManduchiSheridan H LittletonMichelle E LeonardKenyaita M HodgeLi-San WangGerard D SchellenbergMatthew E JohnsonMatthew C PahlJames A PippinAndrew D WellsStewart A AndersonChristopher D BrownStruan F A GrantAlessandra ChesiPublished in: bioRxiv : the preprint server for biology (2024)
Late-onset Alzheimer's disease (LOAD) research has principally focused on neurons over the years due to their known role in the production of amyloid beta plaques and neurofibrillary tangles. In contrast, recent genomic studies of LOAD have implicated microglia as culprits of the prolonged inflammation exacerbating the neurodegeneration observed in patient brains. Indeed, recent LOAD genome-wide association studies (GWAS) have reported multiple loci near genes related to microglial function, including TREM2 , ABI3 , and CR1 . However, GWAS alone cannot pinpoint underlying causal variants or effector genes at such loci, as most signals reside in non-coding regions of the genome and could presumably confer their influence frequently via long-range regulatory interactions. We elected to carry out a combination of ATAC-seq and high-resolution promoter-focused Capture-C in two human microglial cell models (iPSC-derived microglia and HMC3) in order to physically map interactions between LOAD GWAS-implicated candidate causal variants and their corresponding putative effector genes. Notably, we observed consistent evidence that rs6024870 at the GWAS CASS4 locus contacted the promoter of nearby gene, RTFDC1 . We subsequently observed a directionallly consistent decrease in RTFDC1 expression with the the protective minor A allele of rs6024870 via both luciferase assays in HMC3 cells and expression studies in primary human microglia. Through CRISPR-Cas9-mediated deletion of the putative regulatory region harboring rs6024870 in HMC3 cells, we observed increased pro-inflammatory cytokine secretion and decreased DNA double strand break repair related, at least in part, to RTFDC1 expression levels. Our variant-to-function approach therefore reveals that the rs6024870-harboring regulatory element at the LOAD ' CASS4' GWAS locus influences both microglial inflammatory capacity and DNA damage resolution, along with cumulative evidence implicating RTFDC1 as a novel candidate effector gene.
Keyphrases
- genome wide
- late onset
- genome wide association study
- inflammatory response
- copy number
- dna methylation
- neuropathic pain
- endothelial cells
- transcription factor
- high resolution
- poor prognosis
- early onset
- dna damage
- genome wide identification
- induced apoptosis
- induced pluripotent stem cells
- oxidative stress
- genome wide association
- crispr cas
- lipopolysaccharide induced
- regulatory t cells
- single cell
- lps induced
- spinal cord
- genome wide analysis
- gene expression
- cell cycle arrest
- dendritic cells
- cognitive decline
- spinal cord injury
- cell therapy
- magnetic resonance
- pluripotent stem cells
- high throughput
- long non coding rna
- magnetic resonance imaging
- signaling pathway
- stem cells
- genome editing
- mesenchymal stem cells
- bioinformatics analysis
- cell death
- cell proliferation
- mild cognitive impairment
- type iii
- pi k akt
- cell free
- computed tomography
- endoplasmic reticulum stress
- tandem mass spectrometry