- Yu, Miao;
- Zemke, Nathan R;
- Chen, Ziyin;
- Juric, Ivan;
- Hu, Rong;
- Raviram, Ramya;
- Abnousi, Armen;
- Fang, Rongxin;
- Zhang, Yanxiao;
- Gorkin, David U;
- Li, Yang;
- Zhao, Yuan;
- Lee, Lindsay;
- Schmitt, Anthony D;
- Qiu, Yunjiang;
- Dickel, Diane E;
- Visel, Axel;
- Pennacchio, Len A;
- Hu, Ming;
- Ren, Bing
While a rich set of putative cis -regulatory sequences involved in mouse fetal development has been annotated recently based on chromatin accessibility and histone modification patterns, delineating their role in developmentally regulated gene expression continues to be challenging. To fill this gap, we mapped chromatin contacts between gene promoters and distal sequences genome-wide in seven mouse fetal tissues, and for one of them, across six developmental stages. We identified 248,620 long-range chromatin interactions centered at 14,138 protein-coding genes and characterized their tissue-to-tissue variations as well as developmental dynamics. Integrative analysis of the interactome with previous epigenome and transcriptome datasets from the same tissues revealed a strong correlation between the chromatin contacts and chromatin state at distal enhancers, as well as gene expression patterns at predicted target genes. We predicted target genes of 15,098 candidate enhancers, and used them to annotate target genes of homologous candidate enhancers in the human genome that harbor risk variants of human diseases. We present evidence that schizophrenia and other adult disease risk variants are frequently found in fetal enhancers, providing support for the hypothesis of fetal origins of adult diseases.