STAT-6 信号通路而非白细胞介素-1 介导多壁碳纳米管诱导的小鼠肺纤维化：来自不良结局途径框架的见解。

Stat-6 signaling pathway and not Interleukin-1 mediates multi-walled carbon nanotube-induced lung fibrosis in mice: insights from an adverse outcome pathway framework.

机构信息

Environmental Health Science and Research Bureau, Health Canada, Ottawa, ON, K1A 0K9, Canada.

Department of Biological and Chemical Work Environment, National Institute of Occupational Health, Oslo, Norway.

出版信息

Part Fibre Toxicol. 2017 Sep 13;14(1):37. doi: 10.1186/s12989-017-0218-0.

DOI:10.1186/s12989-017-0218-0

PMID:28903780

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5598059/

Abstract

BACKGROUND

The accumulation of MWCNTs in the lung environment leads to inflammation and the development of disease similar to pulmonary fibrosis in rodents. Adverse Outcome Pathways (AOPs) are a framework for defining and organizing the key events that comprise the biological changes leading to undesirable events. A putative AOP has been developed describing MWCNT-induced pulmonary fibrosis; inflammation and the subsequent healing response induced by inflammatory mechanisms have been implicated in disease progression. The objective of the present study was to address a key data gap in this AOP: empirical data supporting the essentiality of pulmonary inflammation as a key event prior to fibrosis. Specifically, Interleukin-1 Receptor1 (IL-1R1) and Signal Transducer and Activator of Transcription 6 (STAT6) knock-out (KO) mice were employed to target inflammation and the subsequent healing response using MWCNTs as a model pro-fibrotic stressor to determine whether this altered the development of fibrosis.

RESULTS

Wild type (WT) C57BL/6, IL-1R1 (KO) or STAT6 KO mice were exposed to a high dose of Mitsui-7 MWCNT by intratracheal administration. Inflammation was assessed 24 h and 28 days post MWCNT administration, and fibrotic lesion development was assessed 28 days post MWCNT administration. MWCNT-induced acute inflammation was suppressed in IL-1R1 KO mice at the 24 h time point relative to WT mice, but this suppression was not observed 28 days post exposure, and IL-1R1 KO did not alter fibrotic disease development. In contrast, STAT6 KO mice exhibited suppressed acute inflammation and attenuated fibrotic disease in response to MWCNT administration compared to STAT6 WT mice. Whole genome analysis of all post-exposure time points identified a subset of differentially expressed genes associated with fibrosis in both KO mice compared to WT mice.

CONCLUSION

The findings support the essentiality of STAT6-mediated signaling in the development of MWCNT-induced fibrotic disease. The IL-1R1 KO results also highlight the nature of the inflammatory response associated with MWCNT exposure, and indicate a system with multiple redundancies. These data add to the evidence supporting an existing AOP, and will be useful in designing screening strategies that could be used by regulatory agencies to distinguish between MWCNTs of varying toxicity.

摘要

背景

MWCNTs 在肺部环境中的积累会导致炎症，并在啮齿动物中引发类似于肺纤维化的疾病。不良结局途径（AOP）是一种定义和组织构成导致不良事件的生物学变化的关键事件的框架。已经开发出一种描述 MWCNT 诱导的肺纤维化的假定 AOP；炎症和随后由炎症机制引起的愈合反应被牵连在疾病进展中。本研究的目的是解决该 AOP 中的一个关键数据空白：支持肺炎症作为纤维化前关键事件的实证数据。具体来说，使用白细胞介素 1 受体 1 (IL-1R1) 和信号转导和转录激活因子 6 (STAT6) 敲除 (KO) 小鼠作为模型促纤维化应激物靶向炎症和随后的愈合反应，以确定这是否改变纤维化的发展。

结果

野生型 (WT) C57BL/6、IL-1R1 (KO) 或 STAT6 KO 小鼠通过气管内给药暴露于 Mitsui-7 MWCNT 的高剂量下。在 MWCNT 给药后 24 小时和 28 天评估炎症，并在 MWCNT 给药后 28 天评估纤维性病变发展。与 WT 小鼠相比，MWCNT 诱导的急性炎症在 24 小时时间点在 IL-1R1 KO 小鼠中受到抑制，但这种抑制在暴露后 28 天未观察到，并且 IL-1R1 KO 并未改变纤维化疾病的发展。相比之下，与 STAT6 WT 小鼠相比，STAT6 KO 小鼠在接受 MWCNT 给药后表现出抑制的急性炎症和减轻的纤维化疾病。所有暴露后时间点的全基因组分析确定了 KO 小鼠与 WT 小鼠相比与纤维化相关的一组差异表达基因。

结论

这些发现支持 STAT6 介导的信号在 MWCNT 诱导的纤维化疾病发展中的必要性。 IL-1R1 KO 的结果还突出了与 MWCNT 暴露相关的炎症反应的性质，并表明存在具有多种冗余的系统。这些数据增加了支持现有 AOP 的证据，并将有助于设计筛选策略，监管机构可以使用这些策略来区分具有不同毒性的 MWCNTs。