4.8 Article

Detection of Neanderthal Adaptively Introgressed Genetic Variants That Modulate Reporter Gene Expression in Human Immune Cells

Journal

MOLECULAR BIOLOGY AND EVOLUTION
Volume 39, Issue 1, Pages -

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/molbev/msab304

Keywords

neandertal; introgression; massively parallel reporter assay; positive selection; adaptation; immune

Funding

  1. National Science Foundation DDRIG [BCS-1847287]
  2. National Science Foundation [BCS-2020205]
  3. American School of Prehistoric Research, Harvard University
  4. National Institutes of Health [R35GM125055, R35GM128946]
  5. Alfred P. Sloan Research Fellowship
  6. Max Planck Society
  7. European Union through the European Regional Development Fund project [MOBEC008]
  8. European Union through Horizon 2020 research and innovation program [810645]
  9. [K99HG010669]
  10. [F32HG00922]

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This study utilized a Massively Parallel Reporter Assay (MPRA) to evaluate high-frequency introgressed variants from Neanderthals, identifying some variants that can modulate gene expression and are associated with immune function. The findings suggest that these variants may alter the binding motifs of important immune transcription factors, are linked to neutrophil and white blood cell count, and are associated with gene expression in innate immune pathways.
Although some variation introgressed from Neanderthals has undergone selective sweeps, little is known about its functional significance. We used a Massively Parallel Reporter Assay (MPRA) to assay 5,353 high-frequency introgressed variants for their ability to modulate the gene expression within 170 bp of endogenous sequence. We identified 2,548 variants in active putative cis-regulatory elements (CREs) and 292 expression-modulating variants (emVars). These emVars are predicted to alter the binding motifs of important immune transcription factors, are enriched for associations with neutrophil and white blood cell count, and are associated with the expression of genes that function in innate immune pathways including inflammatory response and antiviral defense. We combined the MPRA data with other data sets to identify strong candidates to be driver variants of positive selection including an emVar that may contribute to protection against severe COVID-19 response. We endogenously deleted two CREs containing expression-modulation variants linked to immune function, rs11624425 and rs80317430, identifying their primary genic targets as ELMSAN1, and PAN2 and STAT2, respectively, three genes differentially expressed during influenza infection. Overall, we present the first database of experimentally identified expression-modulating Neanderthal-introgressed alleles contributing to potential immune response in modern humans.

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