5‐HT 2C R antagonist/5‐HT 2C R inverse agonist recovered the increased isolation‐induced aggressive behavior of BALB/c mice mediated by ADAR1 (p110) expression and Htr2c RNA editing

Weizhi Yu; Hong Xu; Ying Xue; Dong An; Huairui Li; Wei Chen; Deqin Yu; Yiping Sun; Jianmei Ma; Yiyuan Tang; Zhaoyang Xiao; Shengming Yin

首页> 外文期刊>Brain and Behavior >5‐HT 2C R antagonist/5‐HT 2C R inverse agonist recovered the increased isolation‐induced aggressive behavior of BALB/c mice mediated by ADAR1 (p110) expression and Htr2c RNA editing

【24h】

5‐HT 2C R antagonist/5‐HT 2C R inverse agonist recovered the increased isolation‐induced aggressive behavior of BALB/c mice mediated by ADAR1 (p110) expression and Htr2c RNA editing

机译：5‐HT 2C R拮抗剂/ 5‐HT 2C R反向激动剂恢复了由ADAR1（p110）表达和Htr2c RNA编辑介导的隔离诱导的BALB / c小鼠侵略行为

获取原文

获取外文期刊封面封底 >>

开具论文收录证明 >>

文献代查 >>

团队文献服务 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

Introduction Social isolation enhances the aggressive behavior of animals, but the detailed mechanism remains unclear. Epigenetic studies have suggested that Htr2c RNA editing is closely related to aggressive behavior. This study aims to obtain a fundamental understanding of how social isolation impacts adenosine deaminase acting on RNA 1 (ADAR1, RNA editing enzyme) and Htr2c RNA editing, leading to aggressive behavior, and explore the effective solutions for the recovery of this behavior. Methods We evaluated 21‐day‐old BALB/c mice with and without isolation for aggressive behavior using a resident‐intruder test. Immune‐reactivity and protein expression of ADAR1 (p110) were measured using immunohistochemistry and Western blotting. Htr2c RNA editing was evaluated using pyrosequencing. In addition, the 5‐HT 2C R antagonist SB243213/5‐HT 2C R inverse agonist SB206553 was used to treat the isolated mice, and the performance of both treatments on the behavior, ADAR1 (p110) expression, and Htr2c RNA editing in isolated mice was examined. Results Both the protein expression and immune‐reactivity of ADAR1 (p110) in the amygdala decreased, but the percentage of Htr2c RNA editing at A and B sites of amygdala only showed a moderate increase in isolated BALB/c mice with enhanced aggressive behavior compared to the age‐matched group‐housed BALB/c mice. Additionally, treatment with the 5‐HT 2C R antagonist SB243213/5‐HT 2C R inverse agonist SB206553 recovered the enhanced aggressive behavior of isolated mice and returned the protein expression and immune‐reactivity of ADAR1 (p110) back to the normal level. Moreover, compared to the age‐matched isolated mice treated with physiological saline, isolated mice treated with 5‐HT 2C R inverse agonist SB206553 showed a lower percentage of Htr2c RNA editing at both A and B sites, and the same result occurred in isolated mice treated with 5‐HT 2C R antagonist SB243213 at B site of Htr2c RNA editing. Conclusions The 5‐HT 2C R antagonist SB243213/5‐HT 2C R inverse agonist SB206553 recovered increased aggressive behavior of isolated BALB/c mice mediated by ADAR1 (p110) expression and Htr2c RNA editing.

机译：引言社会隔离增强了动物的攻击行为，但其详细机制仍不清楚。表观遗传学研究表明，Htr2c RNA编辑与攻击行为密切相关。这项研究旨在获得对社会隔离如何影响作用于RNA 1（ADAR1，RNA编辑酶）和Htr2c RNA编辑，导致攻击行为的腺苷脱氨酶的基本了解，并探索恢复这种行为的有效解决方案。方法我们使用常驻入侵者测试评估了21天大龄BALB / c小鼠（有或没有隔离）的攻击行为。使用免疫组织化学和蛋白质印迹法检测ADAR1（p110）的免疫反应性和蛋白质表达。使用焦磷酸测序评估Htr2c RNA编辑。此外，使用5‐HT 2C R拮抗剂SB243213 / 5‐HT 2C R反向激动剂SB206553治疗分离的小鼠，并在分离的小鼠中对行为，ADAR1（p110）表达和Htr2c RNA编辑进行两种治疗检查小鼠。结果杏仁核中ADAR1（p110）的蛋白表达和免疫反应性均下降，但杏仁核A和B位点的Htr2c RNA编辑百分比仅显示出与攻击性行为相比增强的孤立BALB / c小鼠适度增加与年龄匹配的成群饲养的BALB / c小鼠。此外，用5‐HT 2C R拮抗剂SB243213 / 5‐HT 2C R反向激动剂SB206553治疗可以恢复离体小鼠的增强攻击行为，并使ADAR1（p110）的蛋白表达和免疫反应性恢复正常水平。此外，与使用生理盐水处理的年龄匹配的分离小鼠相比，用5-HT 2C R反向激动剂SB206553处理的分离小鼠在A和B部位均显示出较低的Htr2c RNA编辑百分比，并且在分离的小鼠中发生了相同的结果在Htr2c RNA编辑的B位点用5-HT 2C R拮抗剂SB243213处理。结论5-HT 2C R拮抗剂SB243213 / 5‐HT 2C R反向激动剂SB206553可恢复由ADAR1（p110）表达和Htr2c RNA编辑介导的分离的BALB / c小鼠的侵略行为。

著录项

来源
《Brain and Behavior 》 |2018年第3期| 共13页
作者
Weizhi Yu; Hong Xu; Ying Xue; Dong An; Huairui Li; Wei Chen; Deqin Yu; Yiping Sun; Jianmei Ma; Yiyuan Tang; Zhaoyang Xiao; Shengming Yin;
展开▼
作者单位

展开▼
收录信息
原文格式 PDF
正文语种
中图分类临床医学 ;
关键词

相似文献

外文文献
中文文献
专利

1. The role of serotonin-2 (5-HT₂) and dopamine receptors in the behavioral actions of the 5-HT_2A/2C agonist, DOI, and putative 5-HT_2C inverse agonist, SR46349B [J] . Laura C. Scarlota, John A. Harvey, Vincent J. Aloyo Psychopharmacology . 2011 ,第2a3期

机译：血清素2（5-HT _{2 ）和多巴胺受体在5-HT _{2A / 2C 激动剂，DOI和推定的5-HT的行为中的作用_{2C 反向激动剂SR46349B}}}
2. Role of 5-HT2C receptors in the enhancement of c-Fos expression induced by a 5-HT2B/2C inverse agonist and 5-HT2 agonists in the rat basal ganglia [J] . NavaillesS., LagièreM., LeMoineC., Experimental Brain Research . 2013 ,第4期

机译：5-HT2C受体在大鼠基底神经节中由5-HT2B / 2C反向激动剂和5-HT2激动剂诱导的c-Fos表达增强中的作用
3. A novel Aminotetralin-Type Serotonin (5-HT)2C receptor-specific Agonist and 5-HT2A competitive Antagonist/5-HT2B inverse agonist with preclinical efficacy for Psychoses [J] . The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics . 2014 ,第2期

机译：新型氨基四氢叶酸型5-羟色胺（5-HT）2C受体特异性激动剂和5-HT 2A竞争性拮抗剂/ 5-HT 2B反向激动剂，对精神病具有临床前功效
4. 5‐HT2CR antagonist/5‐HT2CR inverse agonist recovered the increased isolation‐induced aggressive behavior of BALB/c mice mediated by ADAR1 (p110) expression and Htr2c RNA editing [O] . Weizhi Yu, Hong Xu, Ying Xue, 2018

机译：5‐HT2CR拮抗剂/ 5‐HT2CR反向激动剂恢复了由ADAR1（p110）表达和Htr2c RNA编辑介导的隔离诱导的BALB / c小鼠侵略行为
5. 5-HT2C R antagonist/5-HT2C R inverse agonist recovered the increased isolation-induced aggressive behavior of BALB/c mice mediated by ADAR1 (p110) expression and Htr2c RNA editing [O] . Weizhi Yu, Hong Xu, Ying Xue, 2018

机译：5-HT2C R拮抗剂/ 5-HT2C逆激动剂回收了ADAR1（P110）表达和HTR2C RNA编辑介导的BALB / C小鼠的增加的分离诱导的侵蚀行为

5‐HT 2C R antagonist/5‐HT 2C R inverse agonist recovered the increased isolation‐induced aggressive behavior of BALB/c mice mediated by ADAR1 (p110) expression and Htr2c RNA editing

摘要

著录项

相似文献

相关主题

期刊订阅