Integrated analyses reveal evolutionarily conserved and specific injury response genes in dorsal root ganglion

Rodent dorsal root ganglion (DRG) is widely used for studying axonal injury. Extensive studies have explored genome-wide profiles on rodent DRGs under peripheral nerve insults. However, systematic integration and exploration of these data still be limited. Herein, we re-analyzed 21 RNA-seq datasets...

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Veröffentlicht in:Scientific data 2022-11, Vol.9 (1), p.666-16, Article 666
Hauptverfasser: Xu, Lian, Chen, Zhifeng, Li, Xiaodi, Xu, Hui, Zhang, Yu, Yang, Weiwei, Chen, Jing, Zhang, Shuqiang, Xu, Lingchi, Zhou, Songlin, Li, Guicai, Yu, Bin, Gu, Xiaosong, Yang, Jian
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Sprache:eng
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Zusammenfassung:Rodent dorsal root ganglion (DRG) is widely used for studying axonal injury. Extensive studies have explored genome-wide profiles on rodent DRGs under peripheral nerve insults. However, systematic integration and exploration of these data still be limited. Herein, we re-analyzed 21 RNA-seq datasets and presented a web-based resource (DRGProfile). We identified 53 evolutionarily conserved injury response genes, including well-known injury genes ( Atf3 , Npy and Gal ) and less-studied transcriptional factors ( Arid5a , Csrnp1 , Zfp367 ). Notably, we identified species-preference injury response candidates ( e.g. Gpr151 , Lipn , Anxa10 in mice; Crisp3 , Csrp3 , Vip , Hamp in rats). Temporal profile analysis reveals expression patterns of genes related to pre-regenerative and regenerating states. Finally, we found a large sex difference in response to sciatic nerve injury, and identified four male-specific markers ( Uty , Eif2s3y , Kdm5d , Ddx3y ) expressed in DRG. Our study provides a comprehensive integrated landscape for expression change in DRG upon injury which will greatly contribute to the neuroscience community.
ISSN:2052-4463
2052-4463
DOI:10.1038/s41597-022-01783-8