亚慢性鼻内脂多糖暴露诱导 NZBWF1 小鼠肺部自身免疫和肾小球肾炎。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
ACS Applied Electronic Materials Pub Date : 2024-12-01 Epub Date: 2024-07-08 DOI:10.1080/08916934.2024.2370536
Lauren K Heine, Lichchavi D Rajasinghe, James G Wagner, Ryan P Lewandowski, Quan-Zhen Li, Alexa L Richardson, Ashleigh N Tindle, Jenan J Shareef, Jack R Harkema, James J Pestka
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引用次数: 0

摘要

红斑狼疮是一种由基因-环境相互作用形成的全身性自身免疫性疾病,通常会发展为终末期肾衰竭。虽然亚慢性全身暴露于细菌脂多糖(LPS)会引发狼疮易感小鼠的自身免疫和肾小球肾炎,但吸入 LPS(在某些职业中很常见)是否会同样引发狼疮还不得而知。在这里,我们确定了亚慢性鼻内灌注 LPS 如何影响易患狼疮的 NZBWF1 雌性小鼠的自身免疫和肾小球肾炎的发展。简言之,对小鼠进行药物或大肠杆菌 LPS(0.8 μg/g)的鼻腔灌注,每周两次,持续 5 周,然后进行尸体解剖。为了进行系统性比较,使用相同的剂量/时间对其他组群的小鼠进行腹腔注射(IP)LPS。评估肺部的炎症和自身免疫反应,然后将其与全身自身免疫和肾小球肾炎联系起来。IN/LPS 暴露在肺部诱导:i)白细胞浸润;ii)细胞因子、趋化因子、IFN 调节基因和细胞死亡相关基因的 mRNA 标识;iii)异位淋巴组织形成;iv)多种 IgM 和 IgG 自身抗体(AAbs)。肺部效应与肿大的脾脏、升高的血浆 IgG AAbs 和发炎的含 IgG 肾小球相吻合。相比之下,IP/LPS 治疗会诱发全身自身免疫和肾小球肾炎,但没有肺部表现。综上所述,这些临床前研究结果表明,肺可能是易感基因个体通过呼吸性 LPS 触发自身免疫的关键节点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Subchronic intranasal lipopolysaccharide exposure induces pulmonary autoimmunity and glomerulonephritis in NZBWF1 mice.

Lupus, a systemic autoimmune disease shaped by gene-environment interplay, often progresses to endstage renal failure. While subchronic systemic exposure to bacterial lipopolysaccharide (LPS) triggers autoimmunity and glomerulonephritis in lupus-prone mice, it is unknown if inhaling LPS, which is common in certain occupations, can similarly trigger lupus. Here we determined how subchronic intranasal (IN) LPS instillation influences autoimmunity and glomerulonephritis development in lupusprone NZBWF1 female mice. Briefly, mice were IN-instilled with vehicle or E. coli LPS (0.8 μg/g) twice weekly for 5 wk, followed by necropsy. For systemic comparison, additional cohorts of mice were injected with LPS intraperitoneally (IP) using identical doses/timing. Lungs were assessed for inflammatory and autoimmune responses and then related to systemic autoimmunity and glomerulonephritis. IN/LPS exposure induced in the lung: i) leukocyte infiltration, ii)mRNA signatures for cytokines, chemokines, IFN-regulated, and cell death-related genes, iii) ectopic lymphoid tissue formation, and iv)diverse IgM and IgG autoantibodies (AAbs). Pulmonary effects coincided with enlarged spleens, elevated plasma IgG AAbs, and inflamed IgG-containing kidney glomeruli. In contrast, IP/LPS treatment induced systemic autoimmunity and glomerulonephritis without pulmonary manifestations. Taken together, these preclinical findings suggest the lung could serve as a critical nexus for triggering autoimmunity by respirable LPS in genetically predisposed individuals.

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CiteScore
7.20
自引率
4.30%
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567
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