实验性肺动脉高压模型中小鼠肺部炎症基因的表达:基于抗体的白细胞介素-9靶向递送的影响

IF 1.8 Q3 RESPIRATORY SYSTEM
Judith Heiss, K. Grün, I. Singerer, L. Tempel, M. Matasci, Christian Jung, Alexander Pfeil, P. C. Schulze, Dario Neri, Marcus Franz
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引用次数: 0

摘要

背景:肺动脉高压(PH)的发病机制是一个由炎症和肺血管重塑驱动的多因素过程。针对 PH 的这两个方面,我们最近测试了一种新型疗法:白细胞介素-9(IL9)与 F8(一种与纤连蛋白外域 A(EDA+ Fn)结合的抗体)融合。由于 EDA+ Fn 不存在于健康的成人组织中,但会在 PH 期间表达,因此 IL9 可被特异性地输送到受 PH 影响的组织中。我们发现,与假治疗小鼠相比,F8IL9 可减少肺血管重塑并减轻 PH。目的:为了评估 F8IL9 对 PH 相关炎症过程的可能影响,我们分析了参与肺免疫反应的基因的表达。方法我们在小鼠(n = 44)中应用单克洛汀(MCT)PH 模型。动物被分为五个实验组:无 PH 的假诱导动物(对照组,n = 4)、无处理的 MCT 诱导 PH(PH,n = 8)、双内皮素受体拮抗剂处理(双 ERA,n = 8)、F8IL9 处理(n = 12,2 种格式,每种格式 n = 6)或 KSFIL9 处理(KSFIL9,n = 12,2 种格式,每种格式 n = 6,KSF:具有无关抗原特异性的对照抗体)。28 天后,对肺部炎症反应(84 个基因)进行 RT-PCR 基因表达分析。结果显示与对照组相比,未经治疗的 PH 组有 19 个基因出现了相关的上调(+2.5 倍)。与未接受治疗的 PH 组相比,接受 F8IL9 治疗的肺组织中的基因表达水平有所降低。尤其是 CCL20、CXCL5、C 反应蛋白、五肽相关(CRPPR)和激肽原-1(KNG1)。结论根据上述假设,在 PH 动物模型中,F8IL9 治疗可减少与炎症相关的一些基因的上调。因此,我们假设基于 IL9 的免疫细胞因子治疗可能会调节各种炎症通路。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Expression of Inflammatory Genes in Murine Lungs in a Model of Experimental Pulmonary Hypertension: Effects of an Antibody-Based Targeted Delivery of Interleukin-9
Background: Pathogenesis of pulmonary hypertension (PH) is a multifactorial process driven by inflammation and pulmonary vascular remodeling. To target these two aspects of PH, we recently tested a novel treatment: Interleukin-9 (IL9) fused to F8, an antibody that binds to the extra-domain A of fibronectin (EDA+ Fn). As EDA+ Fn is not found in healthy adult tissue but is expressed during PH, IL9 is delivered specifically to the tissue affected by PH. We found that F8IL9 reduced pulmonary vascular remodeling and attenuated PH compared with sham-treated mice. Purpose: To evaluate possible F8IL9 effects on PH-associated inflammatory processes, we analysed the expression of genes involved in pulmonary immune responses. Methods: We applied the monocrotaline (MCT) model of PH in mice (n = 44). Animals were divided into five experimental groups: sham-induced animals without PH (control, n = 4), MCT-induced PH without treatment (PH, n = 8), dual endothelin receptor antagonist treatment (dual ERA, n = 8), F8IL9 treatment (n = 12, 2 formats with n = 6 each), or with KSFIL9 treatment (KSFIL9, n = 12, 2 formats with n = 6 each, KSF: control antibody with irrelevant antigen specificity). After 28 days, a RT-PCR gene expression analysis of inflammatory response (84 genes) was performed in the lung. Results: Compared with the controls, 19 genes exhibited relevant (+2.5-fold) upregulation in the PH group without treatment. Gene expression levels in F8IL9-treated lung tissue were reduced compared to the PH group without treatment. This was the case especially for CCL20, CXCL5, C-reactive protein, pentraxin related (CRPPR), and Kininogen-1 (KNG1). Conclusion: In accordance with the hypothesis stated above, F8IL9 treatment diminished the upregulation of some genes associated with inflammation in a PH animal model. Therefore, we hypothesize that IL9-based immunocytokine treatment will likely modulate various inflammatory pathways.
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来源期刊
Advances in respiratory medicine
Advances in respiratory medicine RESPIRATORY SYSTEM-
CiteScore
2.60
自引率
0.00%
发文量
90
期刊介绍: "Advances in Respiratory Medicine" is a new international title for "Pneumonologia i Alergologia Polska", edited bimonthly and addressed to respiratory professionals. The Journal contains peer-reviewed original research papers, short communications, case-reports, recommendations of the Polish Respiratory Society concerning the diagnosis and treatment of lung diseases, editorials, postgraduate education articles, letters and book reviews in the field of pneumonology, allergology, oncology, immunology and infectious diseases. "Advances in Respiratory Medicine" is an open access, official journal of Polish Society of Lung Diseases, Polish Society of Allergology and National Research Institute of Tuberculosis and Lung Diseases.
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