Variants in tubule epithelial regulatory elements mediate most heritable differences in human kidney function.
Gabriel B LoebPooja KathailRichard ShuaiRyan ChungReinier J GronaSailaja PeddadaVolkan SevimScot FedermanKarl MaderAudrey ChuJonathan DavitteJuan DuAlexander R GuptaChun Jimmie YeShawn ShaferLaralynne PrzybylaRadu RapiteanuNilah IoannidisJeremy F ReiterPublished in: bioRxiv : the preprint server for biology (2024)
Kidney disease is highly heritable; however, the causal genetic variants, the cell types in which these variants function, and the molecular mechanisms underlying kidney disease remain largely unknown. To identify genetic loci affecting kidney function, we performed a GWAS using multiple kidney function biomarkers and identified 462 loci. To begin to investigate how these loci affect kidney function, we generated single-cell chromatin accessibility (scATAC-seq) maps of the human kidney and identified candidate cis -regulatory elements (cCREs) for kidney podocytes, tubule epithelial cells, and kidney endothelial, stromal, and immune cells. Kidney tubule epithelial cCREs explained 58% of kidney function SNP-heritability and kidney podocyte cCREs explained an additional 6.5% of SNP-heritability. In contrast, little kidney function heritability was explained by kidney endothelial, stromal, or immune cell-specific cCREs. Through functionally informed fine-mapping, we identified putative causal kidney function variants and their corresponding cCREs. Using kidney scATAC-seq data, we created a deep learning model (which we named ChromKid) to predict kidney cell type-specific chromatin accessibility from sequence. ChromKid and allele specific kidney scATAC-seq revealed that many fine-mapped kidney function variants locally change chromatin accessibility in tubule epithelial cells. Enhancer assays confirmed that fine-mapped kidney function variants alter tubule epithelial regulatory element function. To map the genes which these regulatory elements control, we used CRISPR interference (CRISPRi) to target these regulatory elements in tubule epithelial cells and assessed changes in gene expression. CRISPRi of enhancers harboring kidney function variants regulated NDRG1 and RBPMS expression. Thus, inherited differences in tubule epithelial NDRG1 and RBPMS expression may predispose to kidney disease in humans. We conclude that genetic variants affecting tubule epithelial regulatory element function account for most SNP-heritability of human kidney function. This work provides an experimental approach to identify the variants, regulatory elements, and genes involved in polygenic disease.
Keyphrases
- genome wide
- copy number
- transcription factor
- dna methylation
- single cell
- gene expression
- endothelial cells
- rna seq
- deep learning
- bone marrow
- dna damage
- poor prognosis
- high density
- high throughput
- air pollution
- magnetic resonance imaging
- artificial intelligence
- stem cells
- pluripotent stem cells
- oxidative stress
- induced pluripotent stem cells
- genome wide association study
- high resolution
- computed tomography
- genome wide identification
- data analysis
- convolutional neural network
- mesenchymal stem cells
- diabetic nephropathy