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Malate initiates a proton-sensing pathway essential for pH regulation of inflammation

胞浆 生物化学 苹果酸脱氢酶 化学 信号转导 炎症 代谢物 体外 下调和上调 细胞生物学 生物 免疫学 基因
作者
Yujianan Chen,Ruihua Shi,Yan Xiang,Fan Li,Hong Tang,Gang He,Mei Zhou,Feng Xu,Jindong Tan,Pan Huang,Xiao Ye,Kun Zhao,Wen-yu Fu,Liuli Li,Xuting Bian,Huan Chen,Feng Wang,Teng Wang,Chenke Zhang,Binghua Zhou,Wan Chen,Taotao Liang,Jing-tong Lv,Xia Kang,Youxing Shi,E.-A. Kim,Yue Qin,Aubryanna Hettinghouse,Kaidi Wang,Xiangli Zhao,Mingyu Yang,Yunqing Tang,Hai‐long Piao,Lin Guo,Liu C,Hongming Miao,Kanglai Tang
出处
期刊:Signal Transduction and Targeted Therapy [Springer Nature]
卷期号:9 (1)
标识
DOI:10.1038/s41392-024-02076-9
摘要

Metabolites can double as a signaling modality that initiates physiological adaptations. Metabolism, a chemical language encoding biological information, has been recognized as a powerful principle directing inflammatory responses. Cytosolic pH is a regulator of inflammatory response in macrophages. Here, we found that L-malate exerts anti-inflammatory effect via BiP-IRF2BP2 signaling, which is a sensor of cytosolic pH in macrophages. First, L-malate, a TCA intermediate upregulated in pro-inflammatory macrophages, was identified as a potent anti-inflammatory metabolite through initial screening. Subsequent screening with DARTS and MS led to the isolation of L-malate-BiP binding. Further screening through protein‒protein interaction microarrays identified a L-malate-restrained coupling of BiP with IRF2BP2, a known anti-inflammatory protein. Interestingly, pH reduction, which promotes carboxyl protonation of L-malate, facilitates L-malate and carboxylate analogues such as succinate to bind BiP, and disrupt BiP-IRF2BP2 interaction in a carboxyl-dependent manner. Both L-malate and acidification inhibit BiP-IRF2BP2 interaction, and protect IRF2BP2 from BiP-driven degradation in macrophages. Furthermore, both in vitro and in vivo, BiP-IRF2BP2 signal is required for effects of both L-malate and pH on inflammatory responses. These findings reveal a previously unrecognized, proton/carboxylate dual sensing pathway wherein pH and L-malate regulate inflammatory responses, indicating the role of certain carboxylate metabolites as adaptors in the proton biosensing by interactions between macromolecules.
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