Recruitment of neutrophils in glomeruli in early mouse sepsis is associated with E-selectin expression and activation of endothelial NF-κB and MAPK pathways.

IF 3.6 3区医学 Q3 CELL BIOLOGY Journal of Leukocyte Biology Pub Date : 2024-07-02 DOI:10.1093/jleuko/qiae146

Zhendong Wang, Erna-Zulaikha Dayang, Peter J Zwiers, Martha L Hernandez Garcia, Matthijs Luxen, Matijs van Meurs, Jan A A M Kamps, Jill Moser, Grietje Molema

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Abstract

Sepsis is a dysregulated systemic inflammatory response to an infection, which can lead to multiple organ dysfunction syndrome that includes the kidney. Leukocyte recruitment is an important process of the host immune defense in response to sepsis. Endothelial cells (EC) actively regulate leukocyte recruitment by expressing adhesion molecules following the activation of dedicated intracellular signal transduction pathways. Previous studies reported that the expression of adhesion molecules was associated with the activation of endothelial NF-κB p65 and MAPK c-Jun pathways in vitro in response to conditions that mimic processes that occur in inflammation. This study aimed to investigate the spatiotemporal patterns of leukocyte recruitment, expression of adhesion molecules, and endothelial nuclear p65 and c-Jun localization in renal microvascular beds of septic mice. Here, we used a cecal ligation and puncture (CLP) sepsis mouse model and RT-qPCR and immunohistochemical staining. We showed that neutrophils, macrophages, and T lymphocytes were all present in the kidney, yet only neutrophils accumulated in a spatiotemporally discernible pattern, mainly in glomeruli at 4 hours after CLP-sepsis initiation. E-selectin, not VCAM-1, was expressed in glomeruli at the same time point. In a subset of mice at 72 hours after CLP-sepsis started, VCAM-1 expression was prominent in glomerular EC, which was not related to changes in mmu-microRNA(miR)-126a-3p levels, a short noncoding microRNA previously shown to inhibit the translation of VCAM-1 mRNA into protein. Nuclear localization of p65 and c-Jun occurred in EC of all microvascular segments at 4 and 7 hours after CLP-sepsis initiation. In summary, sepsis-induced recruitment of neutrophils, E-selectin expression, and NF-κB p65 and MAPK c-Jun pathway activation coincided in glomeruli at the early stage of the disease. In the other microvascular beds, sepsis led to NF-κB p65 and MAPK c-Jun pathway activation with limited expression of E-selectin and no association with VCAM-1 expression or leukocyte recruitment.

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小鼠败血症早期肾小球中中性粒细胞的募集与E-选择素的表达及内皮NF-κB和MAPK通路的激活有关。

败血症是一种对感染的全身性炎症反应失调，可导致包括肾脏在内的多器官功能障碍综合征。白细胞募集是应对败血症的宿主免疫防御的一个重要过程。内皮细胞（EC）在激活专用的细胞内信号转导通路后，通过表达粘附分子积极调节白细胞的募集。以前的研究报告称，在体外模拟炎症过程的条件下，粘附分子的表达与内皮 NF-κB p65 和 MAPK c-Jun 通路的激活有关。本研究旨在调查脓毒症小鼠肾微血管床中白细胞招募、粘附分子表达以及内皮细胞核 p65 和 c-Jun 定位的时空模式。在这里，我们使用了盲肠结扎和穿刺（CLP）脓毒症小鼠模型，并进行了 RT-qPCR 和免疫组化染色。我们发现中性粒细胞、巨噬细胞和T淋巴细胞都存在于肾脏中，但只有中性粒细胞在CLP败血症开始4小时后以时空可辨的模式聚集，主要在肾小球中。在同一时间点，肾小球中表达的是 E-选择素，而不是 VCAM-1。在 CLP-sepsis 开始 72 小时后的一组小鼠中，VCAM-1 在肾小球 EC 中的表达很突出，这与 mmu-microRNA(miR)-126a-3p（一种短的非编码 microRNA，以前曾被证明可抑制 VCAM-1 mRNA 翻译成蛋白质）水平的变化无关。在 CLP 败血症开始后 4 小时和 7 小时，p65 和 c-Jun 在所有微血管节段的 EC 中发生核定位。总之，脓毒症诱导的中性粒细胞招募、E-选择素表达、NF-κB p65 和 MAPK c-Jun 通路活化在疾病早期的肾小球中同时发生。在其他微血管床，脓毒症导致 NF-κB p65 和 MAPK c-Jun 通路活化，但 E-选择素的表达有限，与 VCAM-1 表达或白细胞募集没有关联。

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

Journal of Leukocyte Biology 医学-免疫学

CiteScore

11.50

自引率

0.00%

发文量

358

审稿时长

2 months

期刊介绍： JLB is a peer-reviewed, academic journal published by the Society for Leukocyte Biology for its members and the community of immunobiologists. The journal publishes papers devoted to the exploration of the cellular and molecular biology of granulocytes, mononuclear phagocytes, lymphocytes, NK cells, and other cells involved in host physiology and defense/resistance against disease. Since all cells in the body can directly or indirectly contribute to the maintenance of the integrity of the organism and restoration of homeostasis through repair, JLB also considers articles involving epithelial, endothelial, fibroblastic, neural, and other somatic cell types participating in host defense. Studies covering pathophysiology, cell development, differentiation and trafficking; fundamental, translational and clinical immunology, inflammation, extracellular mediators and effector molecules; receptors, signal transduction and genes are considered relevant. Research articles and reviews that provide a novel understanding in any of these fields are given priority as well as technical advances related to leukocyte research methods.