N1-乙酰基-5-甲氧基犬尿氨酸会随着海马体的衰老而减少,它能通过 CaMKII/CREB 磷酸化改善长期记忆

IF 8.3 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM Journal of Pineal Research Pub Date : 2024-01-12 DOI:10.1111/jpi.12934
Kazuki Watanabe, Yusuke Maruyama, Hikaru Iwashita, Haruyasu Kato, Jun Hirayama, Atsuhiko Hattori
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引用次数: 0

摘要

褪黑素是一种在自然界无处不在的分子,参与多种生理功能。在大脑中,褪黑激素会转化为 N1-乙酰基-N2-甲酰基-5-甲氧基喹氨酰胺(AFMK),然后转化为 N1-乙酰基-5-甲氧基喹氨酰胺(AMK),据报道,AMK 能强烈促进长期物体记忆的形成。然而,AMK在脑组织中的合成以及记忆形成的内在机制在很大程度上仍不为人所知。本研究采用了褪黑激素分泌品系 C3H/He 小鼠的年轻和年老个体。在松果体和血浆中,AMK的含量与夜间褪黑激素的含量相比非常低;相反,在海马中,AMK的含量高于褪黑激素。吲哚胺2,3-二加氧酶(Ido)mRNA在多种脑组织中表达,而色氨酸2,3-二加氧酶(Tdo)mRNA仅在海马中表达,其裂解物具有褪黑素向AFMK转化的活性,TDO抑制剂可阻断这种活性。AMK处理后,磷酸化cAMP反应元件结合蛋白(CREB)和PSD-95在整个海马组织中的表达水平显著增加。CREB磷酸化在整个组织中增加之前,在核部分中明显增强。在京都基因组百科全书(KEGG)通路分析中,我们发现老龄C3H/He小鼠海马中下调的基因更多地富集于长期延时(LTP)通路。基因组富集分析表明,LTP和神经活性受体相互作用基因组在老年小鼠海马中富集。此外,与年轻小鼠相比,老年小鼠海马中的Ido1和Tdo mRNA表达量明显下降,且Tdo mRNA的下降比Ido1更明显。此外,在老龄小鼠海马中,AMK水平的下降幅度高于褪黑激素水平的下降幅度,其下降幅度不到年轻小鼠的1/10。总之,我们首次证明了海马中与Tdo相关的褪黑激素到AMK的新陈代谢,并提出了AMK参与LTP和记忆形成的新机制。这些结果支持将 AMK 作为预防记忆衰退的潜在治疗药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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N1-Acetyl-5-methoxykynuramine, which decreases in the hippocampus with aging, improves long-term memory via CaMKII/CREB phosphorylation

Melatonin is a molecule ubiquitous in nature and involved in several physiological functions. In the brain, melatonin is converted to N1-acetyl-N2-formyl-5-methoxykynuramine (AFMK) and then to N1-acetyl-5-methoxykynuramine (AMK), which has been reported to strongly enhance long-term object memory formation. However, the synthesis of AMK in brain tissues and the underlying mechanisms regarding memory formation remain largely unknown. In the present study, young and old individuals from a melatonin-producing strain, C3H/He mice, were employed. The amount of AMK in the pineal gland and plasma was very low compared with those of melatonin at night; conversely, in the hippocampus, the amount of AMK was higher than that of melatonin. Indoleamine 2, 3-dioxygenase (Ido) mRNA was expressed in multiple brain tissues, whereas tryptophan 2,3-dioxygenase (Tdo) mRNA was expressed only in the hippocampus, and its lysate had melatonin to AFMK conversion activity, which was blocked by the TDO inhibitor. The expression levels of phosphorylated cAMP response element binding protein (CREB) and PSD-95 in whole hippocampal tissue were significantly increased with AMK treatment. Before increasing in the whole tissue, CREB phosphorylation was significantly enhanced in the nuclear fraction. In the Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway analysis, we found that downregulated genes in hippocampus of old C3H/He mice were more enriched for long-term potentiation (LTP) pathway. Gene set enrichment analysis showed that LTP and neuroactive receptor interaction gene sets were enriched in hippocampus of old mice. In addition, Ido1 and Tdo mRNA expression was significantly decreased in the hippocampus of old mice compared with young mice, and the decrease in Tdo mRNA was more pronounced than Ido1. Furthermore, there was a higher decrease in AMK levels, which was less than 1/10 that of young mice, than in melatonin levels in the hippocampus of old mice. In conclusion, we first demonstrated the Tdo-related melatonin to AMK metabolism in the hippocampus and suggest a novel mechanism of AMK involved in LTP and memory formation. These results support AMK as a potential therapeutic agent to prevent memory decline.

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来源期刊
Journal of Pineal Research
Journal of Pineal Research 医学-内分泌学与代谢
CiteScore
17.70
自引率
4.90%
发文量
66
审稿时长
1 months
期刊介绍: The Journal of Pineal Research welcomes original scientific research on the pineal gland and melatonin in vertebrates, as well as the biological functions of melatonin in non-vertebrates, plants, and microorganisms. Criteria for publication include scientific importance, novelty, timeliness, and clarity of presentation. The journal considers experimental data that challenge current thinking and welcomes case reports contributing to understanding the pineal gland and melatonin research. Its aim is to serve researchers in all disciplines related to the pineal gland and melatonin.
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