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Development of a novel histone deacetylase inhibitor unveils the role of HDAC11 in alleviating depression by inhibition of microglial activationoa mark
  • Baek, Soo Yeon ;
  • Lee, Jeehee ;
  • Kim, Taegwan ;
  • Lee, Hyelim ;
  • Choi, Hoon Seong ;
  • Park, Hahnbeom ;
  • Koh, Minseob ;
  • Kim, Eunha ;
  • Jung, Michael E. ;
  • Iliopoulos, Dimitrios ;
  • Lee, Jeong Yeon ;
  • Kim, Jonghoon ;
  • Lee, Sanghee

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Publication Year
2023-10-01
Publisher
Elsevier Masson s.r.l.
Citation
Biomedicine and Pharmacotherapy, Vol.166
Keyword
Depressive disorderHDAC inhibitorMicroglial activationNeuroinflammation
Mesh Keyword
AnimalsBrainDepressionHistone Deacetylase 2Histone Deacetylase InhibitorsHistone DeacetylasesMiceMicroglia
All Science Classification Codes (ASJC)
Pharmacology
Abstract
Histone deacetylases (HDACs) are key epigenetic regulators and classified into four subtypes. Despite the various roles of each HDAC isoform, the lack of selective HDAC inhibitors has limited the elucidation of their roles in biological systems. HDAC11, the sole class-IV HDAC, is highly expressed in the brain, however, the role of HDAC11 in microglia is not fully understood. Based on the modification of MC1568, we developed a novel HDAC inhibitor, 5. Interestingly, 5 suppresses lipopolysaccharide-induced microglial activation by the initiation of autophagy and subsequent inhibition of nitric oxide production. Furthermore, we demonstrated that 5 significantly alleviates depression-like behavior by inhibiting microglial activation in mouse brain. Our discovery reveals that specific pharmacological regulation of HDAC11 induces autophagy and reactive nitrogen species balance in microglia for the first time, which makes HDAC11 a new therapeutic target for depressive disorder.
Language
eng
URI
https://dspace.ajou.ac.kr/dev/handle/2018.oak/33579
DOI
https://doi.org/10.1016/j.biopha.2023.115312
Fulltext

Type
Article
Funding
This work was supported by the KIST Institutional Program under Grant (Nos. 2E32212, 2V09713 and 2E32164), a National Research Foundation of Korea (NRF) grant funded by the Korean government (NRF-2021R1C1C1005134, 2021R1A6A1A10044154 and RS-2023-00211336), and a research grant from Eli & Edythe Broad Foundation awarded to Prof. Dr. Dimitrios Iliopoulos. HMC3, BV-2, and HMO6 cell lines were kindly provided by Dr. H. Ryu and Dr. K. Park at the Korea Institute of Science and Technology (KIST) and by Prof. S. H. Paek at Seoul National University Hospital.This work was supported by the KIST Institutional Program under Grant (Nos. 2E32212, 2V09713 and 2E32164 ), a National Research Foundation of Korea ( NRF ) grant funded by the Korean government (NRF- 2021R1C1C1005134 , 2021R1A6A1A10044154 and RS-2023-00211336 ), and a research grant from Eli & Edythe Broad Foundation awarded to Prof. Dr. Dimitrios Iliopoulos. HMC3, BV-2, and HMO6 cell lines were kindly provided by Dr. H. Ryu and Dr. K. Park at the Korea Institute of Science and Technology (KIST) and by Prof. S. H. Paek at Seoul National University Hospital.
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