Three-dimensional chromatin mapping of sensory neurons reveals that promoter–enhancer looping is required for axonal regeneration

粘蛋白 染色质 增强子 再生(生物学) 生物 细胞生物学 神经科学 遗传学 基因表达 基因
作者
Ilaria Palmisano,Tong Liu,Wei Gao,Luming Zhou,Matthias Merkenschlager,Franziska Mueller,Jessica Chadwick,Rebecca Toscano Rivalta,Guiping Kong,James W. D. King,Ediem Al-Jibury,Yuyang Yan,Alessandro Carlino,Bryce Collison,Eleonora De Vitis,Sree Gongala,Francesco De Virgiliis,Zheng Wang,Simone Di Giovanni
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [Proceedings of the National Academy of Sciences]
卷期号:121 (38)
标识
DOI:10.1073/pnas.2402518121
摘要

The in vivo three-dimensional genomic architecture of adult mature neurons at homeostasis and after medically relevant perturbations such as axonal injury remains elusive. Here, we address this knowledge gap by mapping the three-dimensional chromatin architecture and gene expression program at homeostasis and after sciatic nerve injury in wild-type and cohesin-deficient mouse sensory dorsal root ganglia neurons via combinatorial Hi-C, promoter-capture Hi-C, CUT&Tag for H3K27ac and RNA-seq. We find that genes involved in axonal regeneration form long-range, complex chromatin loops, and that cohesin is required for the full induction of the regenerative transcriptional program. Importantly, loss of cohesin results in disruption of chromatin architecture and severely impaired nerve regeneration. Complex enhancer–promoter loops are also enriched in the human fetal cortical plate, where the axonal growth potential is highest, and are lost in mature adult neurons. Together, these data provide an original three-dimensional chromatin map of adult sensory neurons in vivo and demonstrate a role for cohesin-dependent long-range promoter interactions in nerve regeneration.
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