The protein disulfide isomerase A3 and osteopontin axis promotes influenza-induced lung remodelling

IF 6.8 2区 医学 Q1 PHARMACOLOGY & PHARMACY British Journal of Pharmacology Pub Date : 2024-08-08 DOI:10.1111/bph.16511
Amit Kumar, Zoe F. Mark, Morgan P. Carbajal, Dhemerson Souza DeLima, Nicolas Chamberlain, Joseph Walzer, Mona Ruban, Ravishankar Chandrasekaran, Nirav Daphtary, Minara Aliyeva, Matthew E. Poynter, Yvonne M. W. Janssen-Heininger, Jason H. Bates, John F. Alcorn, Clemente J. Britto, Charles S. Dela Cruz, Anil G. Jegga, Vikas Anathy
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Abstract

Background and Purpose

Fibrotic lung remodelling after a respiratory viral infection represents a debilitating clinical sequela. Studying or managing viral–fibrotic sequela remains challenging, due to limited therapeutic options and lack of understanding of mechanisms. This study determined whether protein disulfide isomerase A3 (PDIA3) and secreted phosphoprotein 1 (SPP1), which are associated with pulmonary fibrosis, can promote influenza-induced lung fibrotic remodelling and whether inhibition of PDIA3 or SPP1 can resolve viral-mediated fibrotic remodelling.

Experimental Approach

A retrospective analysis of TriNetX data sets was conducted. Serum from healthy controls and influenza A virus (IAV)-infected patients was analysed. An inhibitor of PDIA3, punicalagin, and a neutralizing antibody for SPP1 were administered in mice. Macrophage cells treated with macrophage colony-stimulating factor (M-CSF) were used as a cell culture model.

Key Results

The TriNetX data set showed an increase in lung fibrosis and decline in lung function in flu-infected acute respiratory distress syndrome (ARDS) patients compared with non-ARDS patients. Serum samples revealed a significant increase in SPP1 and PDIA3 in influenza-infected patients. Lung PDIA3 and SPP1 expression increased following viral infection in mouse models. Punicalagin administration 2 weeks after IAV infection in mice caused a significant decrease in lung fibrosis and improved oxygen saturation. Administration of neutralizing SPP1 antibody decreased lung fibrosis. Inhibition of PDIA3 decreased SPP1secretion from macrophages, in association with diminished disulfide bonds in SPP1.

Conclusion and Implications

The PDIA3–SPP1 axis promotes post-influenza lung fibrosis in mice and that pharmacological inhibition of PDIA3 or SPP1 can treat virus-induced lung fibrotic sequela.

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蛋白二硫异构酶 A3 和骨化蛋白轴促进流感诱发的肺部重塑。
背景和目的:呼吸道病毒感染后的肺部纤维重塑是一种使人衰弱的临床后遗症。由于治疗方案有限且缺乏对机制的了解,研究或处理病毒性纤维化后遗症仍具有挑战性。本研究确定了与肺纤维化相关的蛋白二硫异构酶A3(PDIA3)和分泌型磷蛋白1(SPP1)能否促进流感诱导的肺纤维化重塑,以及抑制PDIA3或SPP1能否解决病毒介导的纤维化重塑:实验方法:对TriNetX数据集进行回顾性分析。对健康对照组和甲型流感病毒(IAV)感染患者的血清进行了分析。给小鼠注射 PDIA3 抑制剂 punicalagin 和 SPP1 中和抗体。用巨噬细胞集落刺激因子(M-CSF)处理的巨噬细胞作为细胞培养模型:TriNetX数据集显示,与非急性呼吸窘迫综合征(ARDS)患者相比,流感感染急性呼吸窘迫综合征(ARDS)患者的肺纤维化程度增加,肺功能下降。血清样本显示,流感感染患者的 SPP1 和 PDIA3 显著增加。病毒感染小鼠模型后,肺部 PDIA3 和 SPP1 的表达增加。在小鼠感染 IAV 2 周后服用 Punicalagin 可显著减少肺纤维化并改善血氧饱和度。施用中和 SPP1 抗体可减少肺纤维化。抑制 PDIA3 可减少巨噬细胞中 SPP1 的分泌,这与 SPP1 中二硫键的减少有关:PDIA3-SPP1轴促进了小鼠流感后的肺纤维化,药物抑制PDIA3或SPP1可治疗病毒诱发的肺纤维化后遗症。
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来源期刊
CiteScore
15.40
自引率
12.30%
发文量
270
审稿时长
2.0 months
期刊介绍: The British Journal of Pharmacology (BJP) is a biomedical science journal offering comprehensive international coverage of experimental and translational pharmacology. It publishes original research, authoritative reviews, mini reviews, systematic reviews, meta-analyses, databases, letters to the Editor, and commentaries. Review articles, databases, systematic reviews, and meta-analyses are typically commissioned, but unsolicited contributions are also considered, either as standalone papers or part of themed issues. In addition to basic science research, BJP features translational pharmacology research, including proof-of-concept and early mechanistic studies in humans. While it generally does not publish first-in-man phase I studies or phase IIb, III, or IV studies, exceptions may be made under certain circumstances, particularly if results are combined with preclinical studies.
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