Itaconate-mediated inhibition of succinate dehydrogenase regulates cytokine production in LPS-induced inflammation

Q4 Medicine

Medical Immunology (Russia) Pub Date : 2023-06-01 DOI:10.15789/1563-0625-imi-2841

D. E. Anisov, M. Drutskaya, M. A. Nosenko, S. Nedospasov

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Abstract

Itaconate is an immunoregulatory metabolite produced by myeloid cells and plays a key role in the regulation of the immune response. Itaconate, on the one hand, is able to suppress the activity of succinate dehydrogenase (SDH), thereby making a significant contribution to the metabolic reprogramming of the cell. On the other hand, itaconate can regulate the activity of a number of transcription factors and transcription regulators, thereby affecting gene expression. In most experimental studies, itaconate has been characterized predominantly as an anti-inflammatory agent. In particular, itaconate produced by activated macrophages inhibits the production of cytokines TNF, IL-1b, IL-6, IL-10. However, some evidence suggests a pro- inflammatory role for itaconate in a number of mouse disease models. Thus, the deletion of the Acod1 gene responsible for the production of itaconate leads to the suppression of the production of TNF and IL-6 in the mouse polymicrobial sepsis model, which means that in the context of inflammation in vivo, itaconate can act as an inducer of pro-inflammatory cytokines. The mechanism of itaconate regulation of cytokine production in systemic inflammation remains unexplored. In this work, we have shown that injection of itaconate and its derivative dimethyl itaconate into mice, followed by induction of inflammation by bacterial lipopolysaccharide (LPS), leads to changes in the content of cytokines in the blood. Interestingly, the systemic production of IL-6 and IL-10 in response to itaconate is increased, contrary to the results previously obtained in cell cultures. At the same time, IFNg production, on the contrary, is suppressed. Apparently, itaconate regulates the production of cytokines in vivo by suppressing the activity of SDH. Injection of the SDH inhibitor, dimethylmalonate, followed by induction of inflammation in mice, results in similar changes in blood cytokines observed in response to itaconate: increased production of IL-6, IL-10 and suppression of IFNg production. On the contrary, the addition of succinate, a SDH substrate, leads to the opposite effect on cytokine production. Thus, it can be assumed that the observed effects of itaconate on cytokine production in the model of LPS-induced inflammation are mediated by its ability to inhibit SDH. These results help to understand the controversial role of itaconate in inflammation and shed light on a previously undescribed relationship between SDH and cytokine production in inflammation in vivo.

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itaconate介导的琥珀酸脱氢酶抑制lps诱导炎症中细胞因子的产生

衣康酸是一种由骨髓细胞产生的免疫调节代谢物，在调节免疫应答中起关键作用。衣康酸一方面能够抑制琥珀酸脱氢酶(SDH)的活性，从而对细胞的代谢重编程做出重要贡献。另一方面，衣康酸可以调节多种转录因子和转录调节剂的活性，从而影响基因表达。在大多数实验研究中，衣康酸主要被认为是一种抗炎剂。特别是，活化的巨噬细胞产生衣康酸抑制细胞因子TNF, IL-1b, IL-6, IL-10的产生。然而，一些证据表明衣康酸在许多小鼠疾病模型中具有促炎作用。因此，在小鼠多微生物脓毒症模型中，衣康酸产生的Acod1基因缺失导致TNF和IL-6的产生受到抑制，这意味着在体内炎症的背景下，衣康酸可以作为促炎细胞因子的诱诱剂。衣康酸调节全身性炎症中细胞因子产生的机制尚不清楚。在这项工作中，我们已经证明，将衣康酸及其衍生物二甲基衣康酸注射到小鼠体内，然后通过细菌脂多糖(LPS)诱导炎症，导致血液中细胞因子含量的变化。有趣的是，与之前在细胞培养中获得的结果相反，衣康酸的全身IL-6和IL-10的产生增加了。与此同时，IFNg的生产反而受到抑制。显然，衣康酸通过抑制SDH活性来调节体内细胞因子的产生。注射SDH抑制剂二甲基丙二酸酯，然后在小鼠中诱导炎症，结果在对衣康酸的反应中观察到类似的血液细胞因子变化:IL-6、IL-10的产生增加，IFNg的产生受到抑制。相反，添加琥珀酸盐(SDH底物)会对细胞因子产生相反的影响。因此，我们可以假设，在lps诱导的炎症模型中，衣康酸对细胞因子产生的影响是通过其抑制SDH的能力介导的。这些结果有助于理解衣康酸在炎症中的有争议的作用，并阐明了先前描述的体内炎症中SDH和细胞因子产生之间的关系。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Medical Immunology (Russia) Medicine-Immunology and Allergy

CiteScore

0.70

自引率

0.00%

发文量

审稿时长

12 weeks

期刊介绍： The journal mission is to promote scientific achievements in fundamental and applied immunology to various medical fields, the publication of reviews, lectures, essays by leading domestic and foreign experts in the field of fundamental and experimental immunology, clinical immunology, allergology, immunodiagnostics and immunotherapy of infectious, allergy, autoimmune diseases and cancer.