Project description:Nematopogon swammerdamellus (large long-horn)

Project description:Acrobasis suavella (thicket knot-horn), genomic and transcriptomic data

Project description:Ochlodes sylvanus (large skipper), genomic and transcriptomic data

Project description:Pieris brassicae (large white), genomic and transcriptomic data

Project description:Nymphalis polychloros (large tortoiseshell), genomic and transcriptomic data

Project description:Cheilosia vulpina (large burdock Cheilosia), genomic and transcriptomic data

Project description:Noctua pronuba (large yellow underwing), genomic and transcriptomic data

Project description:Andrena hattorfiana (large scabious mining bee), genomic and transcriptomic data

Project description:Nysson spinosus (large spurred digger wasp), genomic and transcriptomic data

Project description:The dorsal horn of the spinal cord transforms incoming somatosensory information and transmits it supraspinally to generate sensory perception, including pain and itch. Recent research using mouse Cre-driver lines has implicated specific populations of dorsal horn neurons in the transmission of different types of pain. In parallel, human genome-wide association studies (GWAS) have identified dozens of loci confidently associated with the genetic predisposition to chronic pain. The ability to connect controlled experiments in rodent models with human genetic studies could provide a platform for translational research, but the cell type heterogeneity of the dorsal horn and the complex genetic architecture of chronic pain have created challenges in bridging that gap. Here, we apply a variety of single cell genomic technologies and a comparative genomic analysis to identify conserved dorsal horn neuron subtypes whose open chromatin regions show enrichment for genetic variants associated with human chronic pain phenotypes. To achieve this, we first use single nucleus RNA-Seq and fluorescence in situ hybridization in Rhesus macaque to create a more detailed map of primate dorsal horn neuron subtypes. These were integrated with publicly available human and mouse single nucleus RNA-Seq datasets to create a multi-modal cross species atlas. Then, for the mouse dorsal horn, we combined single nucleus RNA-Seq, spatial transcriptomics, and single nucleus ATAC-Seq to infer spatial and epigenomic profiles of conserved dorsal horn neuron subtypes. Finally, we compared our conserved cell-type open chromatin resource to chronic pain GWAS and found that open chromatin regions of specific dorsal horn neuron subtypes showed enrichment for a variety of human chronic pain phenotypes. Our results provide a foundation to further explore how conserved dorsal horn neuron subtypes influence the transmission of pain signals.