3D chromatin-based variant-to-gene maps across 57 human cell types reveal the cellular and genetic architecture of autoimmune disease susceptibility

  1. Khanh B. Trang
  2. Prabhat Sharma
  3. Laura Cook
  4. Zachary Mount
  5. Rajan M. Thomas
  6. Nikhil N. Kulkarni
  7. Matthew C. Pahl
  8. James A. Pippin
  9. Chun Su
  10. Klaus H. Kaestner
  11. Joan M. O’Brien
  12. Yadav Wagley
  13. Kurt D. Hankenson
  14. Ashley Jermusyk
  15. Jason W. Hoskins
  16. Laufey T. Amundadottir
  17. Mai Xu
  18. Kevin M. Brown
  19. Stewart A. Anderson
  20. Wenli Yang
  21. Paul M. Titchenell
  22. Patrick Seale
  23. Babette S. Zemel
  24. Alessandra Chesi
  25. Neil Romberg
  26. Megan K. Levings
  27. Struan F.A. Grant
  28. Andrew D. Wells
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Abstract

A portion of the genetic basis for many common autoimmune disorders has been uncovered by genome-wide association studies (GWAS), but GWAS do not reveal causal variants, effector genes, or the cell types impacted by disease-associated variation. We have generated 3D genomic datasets consisting of promoter-focused Capture-C, Hi-C, ATAC-seq, and RNA-seq and integrated these data with GWAS of 16 autoimmune traits to physically map disease-associated variants to the effector genes they likely regulate in 57 human cell types. These 3D maps of gene cis -regulatory architecture are highly powered to identify the cell types most likely impacted by disease-associated genetic variation compared to 1D genomic features, and tend to implicate different effector genes than eQTL approaches in the same cell types. Most of the variants implicated by these cis -regulatory architectures are highly trait-specific, but nearly half of the target genes connected to these variants are shared across multiple autoimmune disorders in multiple cell types, suggesting a high level of genetic diversity and complexity among autoimmune diseases that nonetheless converge at the level of target gene and cell type. Substantial effector gene sharing led to the common enrichment of similar biological networks across disease and cell types. However, trait-specific pathways representing potential areas for disease-specific intervention were identified. To test this, we pharmacologically validated squalene synthase, a cholesterol biosynthetic enzyme encoded by the FDFT1 gene implicated by our approach in MS and SLE, as a novel immunomodulatory drug target controlling inflammatory cytokine production by human T cells. These data represent a comprehensive resource for basic discovery of gene cis -regulatory mechanisms, and the analyses reported reveal mechanisms by which autoimmune-associated variants act to regulate gene expression, function, and pathology across multiple, distinct tissues and cell types.

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  1. Version published to 10.1101/2024.08.12.24311676v1 on medRxiv