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


ABSTRACT: 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.

SUBMITTER: Xu L 

PROVIDER: S-EPMC9630366 | biostudies-literature | 2022 Nov

REPOSITORIES: biostudies-literature

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

Xu Lian L   Chen Zhifeng Z   Li Xiaodi X   Xu Hui H   Zhang Yu Y   Yang Weiwei W   Chen Jing J   Zhang Shuqiang S   Xu Lingchi L   Zhou Songlin S   Li Guicai G   Yu Bin B   Gu Xiaosong X   Yang Jian J  

Scientific data 20221102 1


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  ...[more]

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