KLF13 overexpression protects sepsis-induced myocardial injury and LPS-induced inflammation and apoptosis

IF 1.8 4区医学 Q3 PATHOLOGY

International Journal of Experimental Pathology Pub Date : 2022-12-30 DOI:10.1111/iep.12459

Ni Zeng, Zaijin Jian, Wenxin Zhu, Junmei Xu, Yongmei Fan, Feng Xiao

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引用次数: 1

Abstract

Sepsis remains a worldwide public health problem. This study aims to explore the role and mechanism of transcriptional factors (TFs) in sepsis-induced myocardial injury. Firstly, TF KLF13 was selected to explore its role in sepsis-induced myocardial injury. The caecal ligation and puncture (CLP) -induced sepsis mouse model was established and the septic mice were examined using standard histopathological methods. KLF13 expression was detected in the septic mouse heart and was also seen in a lipoploysaccharide (LPS) -induced cellular inflammation model. To explore this further both pro-apoptotic cleaved-caspase3/caspase3 and Bax levels and anti-apoptotic Bcl2 levels were examined, also in both models, In addition inflammatory cytokine (IL-1β, TNF-α, IL-8 and MCP-1) production and IκB-α protein level and p65 phosphorylation were examined in both septic mice and LPS-induced cells. Thus three parameters - cardiomyocyte apoptosis, inflammatory response and NF-κB pathway activation were evaluated under similar conditions. The septic mice showed significant oedema, disordered myofilament arrangement and degradation and necrosis to varying degrees in the myocardial cells. KLF13 was downregulated in both the septic mouse heart and the LPS-induced cellular inflammation model. Furthermore, both models showed abnormally increased cardiomyocyte apoptosis (increased cleaved-caspase3/caspase and Bax protein levels and decreased Bcl2 level), elevated inflammation (increased production of inflammatory cytokines) and the activated NF-κB pathway (increased p65 phosphorylation and decreased IκB-α protein level). KLF13 overexpression notably ameliorated sepsis-induced myocardial injury in vivo and in vitro. KLF13 overexpression protected against sepsis-induced myocardial injury and LPS-induced cellular inflammation and apoptosis via inhibiting the inflammatory pathways (especially NF-κB signalling) and cardiomyocyte apoptosis.

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KLF13过表达可保护脓毒症诱导的心肌损伤和lps诱导的炎症和细胞凋亡

脓毒症仍然是一个全球性的公共卫生问题。本研究旨在探讨转录因子(tf)在脓毒症心肌损伤中的作用及机制。首先选取TF KLF13，探讨其在脓毒症致心肌损伤中的作用。建立盲肠结扎穿刺(CLP)致脓毒症小鼠模型，采用标准组织病理学方法对脓毒症小鼠进行检查。在脓毒症小鼠心脏中检测到KLF13表达，在脂多糖(LPS)诱导的细胞炎症模型中也可见到KLF13表达。为了进一步探讨这一点，我们检测了两种模型中促凋亡的caspase3/caspase3和Bax水平以及抗凋亡的Bcl2水平，此外，我们检测了脓毒症小鼠和lps诱导的细胞中炎症因子(IL-1β、TNF-α、IL-8和MCP-1)的产生以及i- κ b -α蛋白水平和p65磷酸化。因此，在类似的条件下，心肌细胞凋亡、炎症反应和NF-κ b通路激活三个参数被评估。脓毒症小鼠心肌细胞明显水肿，肌丝排列紊乱，不同程度降解坏死。在脓毒症小鼠心脏和lps诱导的细胞炎症模型中，KLF13均下调。此外，两种模型均表现出心肌细胞凋亡异常增加(cleaved-caspase3/ caspasase和Bax蛋白水平增加，Bcl2蛋白水平降低)，炎症升高(炎症细胞因子产生增加)和NF-κB通路激活(p65磷酸化增加，i -κB -α蛋白水平降低)。KLF13过表达可显著改善脓毒症诱导的心肌损伤。KLF13过表达通过抑制炎症通路(尤其是NF-κB信号传导)和心肌细胞凋亡，对脓毒症诱导的心肌损伤和lps诱导的细胞炎症和凋亡具有保护作用。

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来源期刊

International Journal of Experimental Pathology 医学-病理学

CiteScore

4.50

自引率

3.30%

发文量

审稿时长

>12 weeks

期刊介绍： Experimental Pathology encompasses the use of multidisciplinary scientific techniques to investigate the pathogenesis and progression of pathologic processes. The International Journal of Experimental Pathology - IJEP - publishes papers which afford new and imaginative insights into the basic mechanisms underlying human disease, including in vitro work, animal models, and clinical research. Aiming to report on work that addresses the common theme of mechanism at a cellular and molecular level, IJEP publishes both original experimental investigations and review articles. Recent themes for review series have covered topics as diverse as "Viruses and Cancer", "Granulomatous Diseases", "Stem cells" and "Cardiovascular Pathology".