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Citations to this article

BAM15 treats mouse sepsis and kidney injury, linking mortality, mitochondrial DNA, tubule damage, and neutrophils
Naoko Tsuji, … , Peter S.T. Yuen, Robert A. Star
Naoko Tsuji, … , Peter S.T. Yuen, Robert A. Star
Published February 9, 2023
Citation Information: J Clin Invest. 2023;133(7):e152401. https://doi.org/10.1172/JCI152401.
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Research Article Nephrology Article has an altmetric score of 5

BAM15 treats mouse sepsis and kidney injury, linking mortality, mitochondrial DNA, tubule damage, and neutrophils

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Abstract

Sepsis pathogenesis is complex and heterogeneous; hence, a precision-medicine strategy is needed. Acute kidney injury (AKI) following sepsis portends higher mortality. Overproduction of mitochondrial ROS (mtROS) is a potential mediator of sepsis and sepsis-induced AKI. BAM15, a chemical uncoupler, dissipates mitochondrial proton gradients without generating mtROS. We injected BAM15 into mice at 0, 6, or 12 hours after cecal ligation and puncture (CLP), and these mice were treated with fluids and antibiotics. BAM15 reduced mortality, even after 12 hours, when mice were ill, and BAM15 reduced kidney damage and splenic apoptosis. Serial plasma and urinary mitochondrial DNA (mtDNA) levels increased after CLP and decreased after BAM15 administration (at 0 or 6 hours). In vitro septic serum proportionately increased mtROS overproduction and mtDNA release from kidney tubule cells, which BAM15 prevented. BAM15 decreased neutrophil apoptosis and mtDNA release; neutrophil depletion counteracted BAM15 benefits. Further, mtDNA injection in vivo replicated inflammation and kidney injury, which was prevented by BAM15. A large dose of exogenous mtDNA reversed protection by BAM15. We conclude that BAM15 is an effective preventive and therapeutic candidate in experimental sepsis and that BAM15 and mtDNA, a potential drug-companion diagnostic/drug-efficacy pair for clinical sepsis, are mechanistically linked via mtROS.

Authors

Naoko Tsuji, Takayuki Tsuji, Tetsushi Yamashita, Naoki Hayase, Xuzhen Hu, Peter S.T. Yuen, Robert A. Star

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Total citations by year

Year: 2025 2024 2023 Total
Citations: 4 9 4 17
Citation information
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Citations to this article (17)

Title and authors Publication Year
Sepsis-induced cardiac dysfunction: mitochondria and energy metabolism
Yu X, Gao J, Zhang C
Intensive Care Medicine Experimental 2025
Combining RNA-seq, molecular docking and experimental verification to explore the mechanism of BAM15 as a potential drug for atherosclerosis
Ma M, Zhong J, Tai Y, Xu S, Pei Z, Wang X
Scientific Reports 2025
Targeting the immuno-inflammatory-microbial network: a key strategy for sepsis treatment
Xu Y, Wang J, Yuan R, Qin Z, Long K, Gao P
Frontiers in Immunology 2025
Piezo1 activation protects against sepsis-induced myocardial dysfunction in a pilot study
Gong A, Dai J, Zhao Y, Hu H, Guan C, Yu H, Wang K, Jin S, Wu Y, Xiao B
Scientific Reports 2025
STING contributes to lipopolysaccharide-induced tubular cell inflammation, pyroptosis and apoptosis by activating endoplasmic reticulum stress in acute kidney injury
Yun Cao, Xinghua Chen, Zijing Zhu, Zilv Luo, Yiqun Hao, Xueyan Yang, Jun Feng, Zongwei Zhang, Jijia Hu, Yonghong Jian, Jiefu Zhu, Wei Liang, Zhaowei Chen
Cell Death and Disease 2024
Identification of immune characteristic biomarkers and therapeutic targets in cuproptosis for sepsis by integrated bioinformatics analysis and single-cell RNA sequencing analysis
Wang T, Fang X, Sheng X, Li M, Mei Y, Mei Q, Pan A
Heliyon 2024
Comprehensive analysis of cuproptosis-related genes in immune infiltration and development of a novel diagnostic model for acute kidney injury
Li Y, Ding Y
Renal Failure 2024
Heparin-Binding Protein Promotes Acute Lung Injury in Sepsis Mice by Blocking the Aryl Hydrocarbon Receptor Signaling Pathway.
Ye K, Lin X, Chen TZ, Wang LH, Liu SX
Journal of inflammation research 2024
Immunotherapy in the context of sepsis-induced immunological dysregulation
Wu Y, Wang L, Li Y, Cao Y, Wang M, Deng Z, Kang H
Frontiers in immunology 2024
Lymphocytes and innate immune cells in acute kidney injury and repair.
Lee K, Jang HR, Rabb H
Nature reviews. Nephrology 2024
Copper-Based Nanoparticles for Effective Treatment Against Sepsis-Induced Lung Injury in Mice Model
Li JM, Zhang L, Pei SL, Guo L, Shen HL, He J, Guo YY, Zhang WQ, Lin F
International Journal of Nanomedicine 2024
The role of mitochondrial reactive oxygen species in initiating mitochondrial damage and inflammation in wasp-venom-induced acute kidney injury
Xia L, Yuan H, Gao Z, Lv Y, Xu L, Hu F
Journal of Toxicologic Pathology 2024
FGF8 Protects Against Polymicrobial Sepsis by Enhancing the Host's Anti-infective Immunity
Chen K, Ruan Y, Ma W, Yu X, Hu Y, Li Y, Tang H, Zhang X, Yin Y, Chen D, Song Z
The Journal of Infectious Diseases 2024
Preventing mitochondrial reverse electron transport as a strategy for cardioprotection.
Prag HA, Murphy MP, Krieg T
Basic Research in Cardiology 2023
BAM15 as a mitochondrial uncoupler: a promising therapeutic agent for diverse diseases.
Xiong G, Zhang K, Ma Y, Song Y, Zhang W, Qi T, Qiu H, Shi J, Kan C, Zhang J, Sun X
Frontiers in Endocrinology 2023
Polymeric Particle BAM15 Targeting Macrophages Attenuates the Severity of LPS-Induced Sepsis: A Proof of Concept for Specific Immune Cell-Targeted Therapy
Udompornpitak K, Bhunyakarnjanarat T, Saisorn W, Manipuntee C, Plengplang K, Sittichaitaweekul S, Jenphatanapong P, Udomkarnjananun S, Kaewduangduen W, Ariya-anandech K, Samaeng A, Insin N, Ritprajak P, Leelahavanichkul A
Pharmaceutics 2023
Regulatory networks of circRNA- centred ceRNAs in sepsis-induced acute kidney injury
Ma T, Wu J, Chen Z
Epigenetics : official journal of the DNA Methylation Society 2023

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