Central obesity is associated with higher risk of developing a wide range of diseases independent of overall obesity. Genome-wide asso�ciation studies (GWASs) have identified more than 300 susceptibility loci associated with central obesity. However, the functional un�derstanding of these loci is limited by the fact that most loci are in non-coding regions. To address this issue, our study first prioritized
2,034 single-nucleotide polymorphisms (SNPs) based on fine-mapping and epigenomic annotation analysis. Subsequently, we em�ployed self-transcribing active regulatory region sequencing (STARR-seq) to systematically evaluate the enhancer activity of these prior�itized SNPs. The resulting data analysis identif... More
Central obesity is associated with higher risk of developing a wide range of diseases independent of overall obesity. Genome-wide asso�ciation studies (GWASs) have identified more than 300 susceptibility loci associated with central obesity. However, the functional un�derstanding of these loci is limited by the fact that most loci are in non-coding regions. To address this issue, our study first prioritized
2,034 single-nucleotide polymorphisms (SNPs) based on fine-mapping and epigenomic annotation analysis. Subsequently, we em�ployed self-transcribing active regulatory region sequencing (STARR-seq) to systematically evaluate the enhancer activity of these prior�itized SNPs. The resulting data analysis identified 141 SNPs with allelic enhancer activity. Further analysis of allelic transcription factor
(TF) binding prioritized 20 key TFs mediating the central-obesity-relevant genetic regulatory network. Finally, as an example, we illus�trate the molecular mechanisms of how rs8079062 acts as an allele-specific enhancer to regulate the expression of its targeted RNF157.
We also evaluated the role of RNF157 in the adipogenic differentiation process. In conclusion, our results provide an important resource
for understanding the genetic regulatory mechanisms underlying central obesity.
