p300/CBP inhibitor A-485 alleviates acute liver injury by regulating macrophage activation and polarization

High morbidity and mortality are associated with acute liver injury (ALI) for which no effective targeted drugs or pharmacotherapies are available. Discovery of potential therapeutic targets as well as inhibitors that can alleviate ALI is imperative. As excessive inflammatory cytokines released by m...

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Autores principales: Peng, Jinjin, Li, Jiacheng, Huang, Jing, Xu, Pan, Huang, Heming, Liu, Yanjun, Yu, Liang, Yang, Yaxi, Zhou, Bing, Jiang, Hualiang, Chen, Kaixian, Dang, Yongjun, Zhang, Yuanyuan, Luo, Cheng, Li, Guangming
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2019
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6857059/
https://www.ncbi.nlm.nih.gov/pubmed/31754401
http://dx.doi.org/10.7150/thno.30707
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author Peng, Jinjin
Li, Jiacheng
Huang, Jing
Xu, Pan
Huang, Heming
Liu, Yanjun
Yu, Liang
Yang, Yaxi
Zhou, Bing
Jiang, Hualiang
Chen, Kaixian
Dang, Yongjun
Zhang, Yuanyuan
Luo, Cheng
Li, Guangming
author_facet Peng, Jinjin
Li, Jiacheng
Huang, Jing
Xu, Pan
Huang, Heming
Liu, Yanjun
Yu, Liang
Yang, Yaxi
Zhou, Bing
Jiang, Hualiang
Chen, Kaixian
Dang, Yongjun
Zhang, Yuanyuan
Luo, Cheng
Li, Guangming
author_sort Peng, Jinjin
collection PubMed
description High morbidity and mortality are associated with acute liver injury (ALI) for which no effective targeted drugs or pharmacotherapies are available. Discovery of potential therapeutic targets as well as inhibitors that can alleviate ALI is imperative. As excessive inflammatory cytokines released by macrophages are a critical cause of liver injury, we aimed to find novel compounds that could inhibit macrophage expression of inflammatory cytokines and alleviate liver injury. Methods: A high throughput assay was established to screen a small molecule inhibitor library of epigenetic targets. A highly selective catalytic p300/CBP inhibitor A-485 was identified as a potent hit in vitro and administrated to the lipopolysaccharide (LPS)/D-galactosamine (GalN)-induced mice in vivo. For in vitro analysis, RAW264.7 cells and primary BMDM cells exposed to LPS were co-incubated with A-485. A model of acute liver injury induced by LPS and GalN was used for evaluation of in vivo treatment efficacy. Results: A-485 inhibited LPS-induced inflammatory cytokine expression in a concentration-dependent manner in vitro. Significantly, A-485 administration alleviated histopathological abnormalities, lowered plasma aminotransferases, and improved the survival rate in the LPS/GalN-stimulated mice. Integrative ChIP-Seq and transcriptome analysis in the ALI animal model and macrophages revealed that A-485 preferentially blocked transcriptional activation of a broad set of pathologic genes enriched in inflammation-related signaling networks. Significant inhibition of H3K27ac/H3K18ac at promoter regions of these pivotal inflammatory genes was observed, in line with their suppressed transcription after A-485 treatment. Reduced expression of these pathological pro-inflammatory genes resulted in a decrease in inflammatory pathway activation, M1 polarization as well as reduced leukocyte infiltration in ALI mouse model, which accounted for the protective effects of A-485 on liver injury. Conclusion: Using a novel strategy targeting macrophage inflammatory activation and cytokine expression, we established a high-throughput screening assay to discover potential candidates for ALI treatment. We demonstrated that A-485, which targeted pathological inflammatory signaling networks at the level of chromatin, was pharmacologically effective in vivo and in vitro. Our study thus provided a novel target as well as a potential drug candidate for the treatment of liver injury and possibly for other acute inflammatory diseases.
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spelling pubmed-68570592019-11-21 p300/CBP inhibitor A-485 alleviates acute liver injury by regulating macrophage activation and polarization Peng, Jinjin Li, Jiacheng Huang, Jing Xu, Pan Huang, Heming Liu, Yanjun Yu, Liang Yang, Yaxi Zhou, Bing Jiang, Hualiang Chen, Kaixian Dang, Yongjun Zhang, Yuanyuan Luo, Cheng Li, Guangming Theranostics Research Paper High morbidity and mortality are associated with acute liver injury (ALI) for which no effective targeted drugs or pharmacotherapies are available. Discovery of potential therapeutic targets as well as inhibitors that can alleviate ALI is imperative. As excessive inflammatory cytokines released by macrophages are a critical cause of liver injury, we aimed to find novel compounds that could inhibit macrophage expression of inflammatory cytokines and alleviate liver injury. Methods: A high throughput assay was established to screen a small molecule inhibitor library of epigenetic targets. A highly selective catalytic p300/CBP inhibitor A-485 was identified as a potent hit in vitro and administrated to the lipopolysaccharide (LPS)/D-galactosamine (GalN)-induced mice in vivo. For in vitro analysis, RAW264.7 cells and primary BMDM cells exposed to LPS were co-incubated with A-485. A model of acute liver injury induced by LPS and GalN was used for evaluation of in vivo treatment efficacy. Results: A-485 inhibited LPS-induced inflammatory cytokine expression in a concentration-dependent manner in vitro. Significantly, A-485 administration alleviated histopathological abnormalities, lowered plasma aminotransferases, and improved the survival rate in the LPS/GalN-stimulated mice. Integrative ChIP-Seq and transcriptome analysis in the ALI animal model and macrophages revealed that A-485 preferentially blocked transcriptional activation of a broad set of pathologic genes enriched in inflammation-related signaling networks. Significant inhibition of H3K27ac/H3K18ac at promoter regions of these pivotal inflammatory genes was observed, in line with their suppressed transcription after A-485 treatment. Reduced expression of these pathological pro-inflammatory genes resulted in a decrease in inflammatory pathway activation, M1 polarization as well as reduced leukocyte infiltration in ALI mouse model, which accounted for the protective effects of A-485 on liver injury. Conclusion: Using a novel strategy targeting macrophage inflammatory activation and cytokine expression, we established a high-throughput screening assay to discover potential candidates for ALI treatment. We demonstrated that A-485, which targeted pathological inflammatory signaling networks at the level of chromatin, was pharmacologically effective in vivo and in vitro. Our study thus provided a novel target as well as a potential drug candidate for the treatment of liver injury and possibly for other acute inflammatory diseases. Ivyspring International Publisher 2019-10-22 /pmc/articles/PMC6857059/ /pubmed/31754401 http://dx.doi.org/10.7150/thno.30707 Text en © The author(s) This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Peng, Jinjin
Li, Jiacheng
Huang, Jing
Xu, Pan
Huang, Heming
Liu, Yanjun
Yu, Liang
Yang, Yaxi
Zhou, Bing
Jiang, Hualiang
Chen, Kaixian
Dang, Yongjun
Zhang, Yuanyuan
Luo, Cheng
Li, Guangming
p300/CBP inhibitor A-485 alleviates acute liver injury by regulating macrophage activation and polarization
title p300/CBP inhibitor A-485 alleviates acute liver injury by regulating macrophage activation and polarization
title_full p300/CBP inhibitor A-485 alleviates acute liver injury by regulating macrophage activation and polarization
title_fullStr p300/CBP inhibitor A-485 alleviates acute liver injury by regulating macrophage activation and polarization
title_full_unstemmed p300/CBP inhibitor A-485 alleviates acute liver injury by regulating macrophage activation and polarization
title_short p300/CBP inhibitor A-485 alleviates acute liver injury by regulating macrophage activation and polarization
title_sort p300/cbp inhibitor a-485 alleviates acute liver injury by regulating macrophage activation and polarization
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6857059/
https://www.ncbi.nlm.nih.gov/pubmed/31754401
http://dx.doi.org/10.7150/thno.30707
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