A non-canonical immunometabolic function of BRD3 during sepsis

Nian Wang; Jiao Liu; Runliu Wu; Feng Chen; Chunhua Yu; Herbert Zeh; Xianzhong Xiao; Haichao Wang; Timothy R. Billiar; Ling Zeng; Jianxin Jiang; Daolin Tang; Rui Kang

doi:10.1016/j.devcel.2025.09.016

A non-canonical immunometabolic function of BRD3 during sepsis

Nian Wang, Jiao Liu, Runliu Wu, Feng Chen, Chunhua Yu, Herbert Zeh, Xianzhong Xiao, Haichao Wang, Timothy R. Billiar, Ling Zeng, Jianxin Jiang, Daolin Tang^*, Rui Kang^*

^*Corresponding author for this work

Surgery

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

Sepsis is a life-threatening condition characterized by a dysregulated host innate immune response to pathogen infection. Here, we identify a pathological role for bromodomain-containing 3 (BRD3) in driving septic shock by upregulating aconitate decarboxylase 1 (ACOD1) in monocytes and macrophages via a non-canonical pathway. Mechanistically, lipopolysaccharide triggers an interaction between BRD3 and tripartite motif containing 21 (TRIM21), which activates CREB binding lysine acetyltransferase (CREBBP) via its E3 ligase activity, facilitating CREBBP’s binding to and acetylation of cyclic adenosine monophophate (cAMP)-response-element-binding protein 1 (CREB1). BRD3 then recognizes and phosphorylates acetylated CREB1 at the transcription-activating site, thereby upregulating ACOD1 transcription. In four murine models of infection, myeloid-specific Brd3 deletion ( Brd3 ^Mye^−/− ) or pharmacological intervention using small-molecule inhibitor OTX015 confers significant protection, reducing systemic inflammation and organ injury, similar to the effects observed in Acod1 ^Mye−/− mice. In patients with sepsis, elevated BRD3 levels correlate with accelerated inflammation, increased disease severity, and a greater risk of in-hospital death. These findings establish BRD3 as a potential therapeutic target for managing infection-associated immune dysregulation.

Original language	English
Journal	Developmental Cell
DOIs	https://doi.org/10.1016/j.devcel.2025.09.016
State	Accepted/In press - 2025

Keywords

ACOD1
BRD3
immunometabolism
inflammation
itaconate
sepsis

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10.1016/j.devcel.2025.09.016

Cite this

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title = "A non-canonical immunometabolic function of BRD3 during sepsis",

abstract = "Sepsis is a life-threatening condition characterized by a dysregulated host innate immune response to pathogen infection. Here, we identify a pathological role for bromodomain-containing 3 (BRD3) in driving septic shock by upregulating aconitate decarboxylase 1 (ACOD1) in monocytes and macrophages via a non-canonical pathway. Mechanistically, lipopolysaccharide triggers an interaction between BRD3 and tripartite motif containing 21 (TRIM21), which activates CREB binding lysine acetyltransferase (CREBBP) via its E3 ligase activity, facilitating CREBBP{\textquoteright}s binding to and acetylation of cyclic adenosine monophophate (cAMP)-response-element-binding protein 1 (CREB1). BRD3 then recognizes and phosphorylates acetylated CREB1 at the transcription-activating site, thereby upregulating ACOD1 transcription. In four murine models of infection, myeloid-specific Brd3 deletion ( Brd3 Mye −/− ) or pharmacological intervention using small-molecule inhibitor OTX015 confers significant protection, reducing systemic inflammation and organ injury, similar to the effects observed in Acod1 Mye−/− mice. In patients with sepsis, elevated BRD3 levels correlate with accelerated inflammation, increased disease severity, and a greater risk of in-hospital death. These findings establish BRD3 as a potential therapeutic target for managing infection-associated immune dysregulation.",

keywords = "ACOD1, BRD3, immunometabolism, inflammation, itaconate, sepsis",

author = "Nian Wang and Jiao Liu and Runliu Wu and Feng Chen and Chunhua Yu and Herbert Zeh and Xianzhong Xiao and Haichao Wang and Billiar, {Timothy R.} and Ling Zeng and Jianxin Jiang and Daolin Tang and Rui Kang",

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year = "2025",

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AU - Wang, Nian

AU - Liu, Jiao

AU - Wu, Runliu

AU - Chen, Feng

AU - Yu, Chunhua

AU - Zeh, Herbert

AU - Xiao, Xianzhong

AU - Wang, Haichao

AU - Billiar, Timothy R.

AU - Zeng, Ling

AU - Jiang, Jianxin

AU - Tang, Daolin

AU - Kang, Rui

PY - 2025

Y1 - 2025

N2 - Sepsis is a life-threatening condition characterized by a dysregulated host innate immune response to pathogen infection. Here, we identify a pathological role for bromodomain-containing 3 (BRD3) in driving septic shock by upregulating aconitate decarboxylase 1 (ACOD1) in monocytes and macrophages via a non-canonical pathway. Mechanistically, lipopolysaccharide triggers an interaction between BRD3 and tripartite motif containing 21 (TRIM21), which activates CREB binding lysine acetyltransferase (CREBBP) via its E3 ligase activity, facilitating CREBBP’s binding to and acetylation of cyclic adenosine monophophate (cAMP)-response-element-binding protein 1 (CREB1). BRD3 then recognizes and phosphorylates acetylated CREB1 at the transcription-activating site, thereby upregulating ACOD1 transcription. In four murine models of infection, myeloid-specific Brd3 deletion ( Brd3 Mye −/− ) or pharmacological intervention using small-molecule inhibitor OTX015 confers significant protection, reducing systemic inflammation and organ injury, similar to the effects observed in Acod1 Mye−/− mice. In patients with sepsis, elevated BRD3 levels correlate with accelerated inflammation, increased disease severity, and a greater risk of in-hospital death. These findings establish BRD3 as a potential therapeutic target for managing infection-associated immune dysregulation.

AB - Sepsis is a life-threatening condition characterized by a dysregulated host innate immune response to pathogen infection. Here, we identify a pathological role for bromodomain-containing 3 (BRD3) in driving septic shock by upregulating aconitate decarboxylase 1 (ACOD1) in monocytes and macrophages via a non-canonical pathway. Mechanistically, lipopolysaccharide triggers an interaction between BRD3 and tripartite motif containing 21 (TRIM21), which activates CREB binding lysine acetyltransferase (CREBBP) via its E3 ligase activity, facilitating CREBBP’s binding to and acetylation of cyclic adenosine monophophate (cAMP)-response-element-binding protein 1 (CREB1). BRD3 then recognizes and phosphorylates acetylated CREB1 at the transcription-activating site, thereby upregulating ACOD1 transcription. In four murine models of infection, myeloid-specific Brd3 deletion ( Brd3 Mye −/− ) or pharmacological intervention using small-molecule inhibitor OTX015 confers significant protection, reducing systemic inflammation and organ injury, similar to the effects observed in Acod1 Mye−/− mice. In patients with sepsis, elevated BRD3 levels correlate with accelerated inflammation, increased disease severity, and a greater risk of in-hospital death. These findings establish BRD3 as a potential therapeutic target for managing infection-associated immune dysregulation.

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