Frontiers in Genetics (May 2021)

Transcriptome-Wide Identification of G-to-A RNA Editing in Chronic Social Defeat Stress Mouse Models

  • Ji Tao,
  • Ji Tao,
  • Ji Tao,
  • Chun-Yan Ren,
  • Chun-Yan Ren,
  • Chun-Yan Ren,
  • Chun-Yan Ren,
  • Zhi-Yuan Wei,
  • Zhi-Yuan Wei,
  • Zhi-Yuan Wei,
  • Fuquan Zhang,
  • Jinyu Xu,
  • Jian-Huan Chen,
  • Jian-Huan Chen,
  • Jian-Huan Chen

DOI
https://doi.org/10.3389/fgene.2021.680548
Journal volume & issue
Vol. 12

Abstract

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Emerging evidence suggests that RNA editing is associated with stress, neurological diseases, and psychiatric disorders. However, the role of G-to-A RNA editing in chronic social defeat stress (CSDS) remains unclear. We herein identified G-to-A RNA editing and its changes in the ventral tegmental area (VTA), a key region of the brain reward system, in CSDS mouse models under emotional stress (ES) and physiological stress (PS) conditions. Our results revealed 3812 high-confidence G-to-A editing events. Among them, 56 events were significantly downregulated while 23 significantly upregulated in CSDS compared to controls. Moreover, divergent editing patterns were observed between CSDS mice under ES and PS conditions, with 42 and 21 events significantly upregulated in PS and ES, respectively. Interestingly, differential RNA editing was enriched in genes with multiple editing events. Genes differentially edited in CSDS included those genetically associated with mental or neurodevelopmental disorders, especially mood disorders, such as FAT atypical cadherin 1 and solute carrier family 6 member 1. Notably, changes of G-to-A RNA editing were also implicated in ionotropic glutamate receptors, a group of well-known targets of adenosine-to-inosine RNA editing. Such results demonstrate dynamic G-to-A RNA editing changes in the brain of CSDS mouse models, underlining its role as a potential molecular mechanism of CSDS and stress-related diseases.

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