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一氧化氮金属供体 FOR811A [顺式-[Ru(bpy)2(2-MIM)(NO)] (PF6)3]对瑞士小鼠呼吸力学的平喘作用。

Anti-asthmatic effect of nitric oxide metallo-donor FOR811A [cis-[Ru(bpy)2(2-MIM)(NO)](PF6)3] in the respiratory mechanics of Swiss mice.

机构信息

Department of Veterinary Clinics, Faculty of Veterinary, Federal University of Pelotas, Pelotas, RS, Brazil.

Department of Physiology and Pharmacology, Faculty of Medicine, Federal University of Ceará, Fortaleza, CE, Brazil.

出版信息

PLoS One. 2021 Mar 12;16(3):e0248394. doi: 10.1371/journal.pone.0248394. eCollection 2021.

Abstract

We aimed at evaluating the anti-asthmatic effect of cis-Ru(bpy)2(2-MIM)(NO)3 (FOR811A), a nitrosyl-ruthenium compound, in a murine model of allergic asthma. The anti-asthmatic effects were analyzed by measuring the mechanical lung and morphometrical parameters in female Swiss mice allocated in the following groups: untreated control (Ctl+Sal) and control treated with FOR811A (Ctl+FOR), along asthmatic groups untreated (Ast+Sal) and treated with FOR811A (Ast+FOR). The drug-protein interaction was evaluated by in-silico assay using molecular docking. The results showed that the use of FOR811A in experimental asthma (Ast+FOR) decreased the pressure-volume curve, hysteresis, tissue elastance, tissue resistance, and airway resistance, similar to the control groups (Ctl+Sal; Ctl+FOR). However, it differed from the untreated asthmatic group (Ast+Sal, p<0.05), indicating that FOR811A corrected the lung parenchyma and relaxed the smooth muscles of the bronchi. Similar to control groups (Ctl+Sal; Ctl+FOR), FOR811A increased the inspiratory capacity and static compliance in asthmatic animals (Ast+Sal, p<0.05), showing that this metallodrug improved the capacity of inspiration during asthma. The morphometric parameters showed that FOR811A decreased the alveolar collapse and kept the bronchoconstriction during asthma. Beyond that, the molecular docking using FOR811A showed a strong interaction in the distal portion of the heme group of the soluble guanylate cyclase, particularly with cysteine residue (Cys141). In summary, FOR811A relaxed bronchial smooth muscles and improved respiratory mechanics during asthma, providing a protective effect and promising use for the development of an anti-asthmatic drug.

摘要

我们旨在评估顺式-[Ru(bpy)2(2-MIM)(NO)] (PF6)3 (FOR811A),一种亚硝酰基钌化合物,在过敏性哮喘小鼠模型中的抗哮喘作用。通过测量雌性瑞士小鼠的机械肺和形态计量学参数来分析抗哮喘作用,将这些小鼠分为以下几组:未治疗对照组(Ctl+Sal)和用 FOR811A 治疗的对照组(Ctl+FOR),以及未治疗哮喘组(Ast+Sal)和用 FOR811A 治疗的哮喘组(Ast+FOR)。通过分子对接的计算药物-蛋白相互作用评估。结果表明,在实验性哮喘(Ast+FOR)中使用 FOR811A 降低了压力-容积曲线、滞后、组织弹性、组织阻力和气道阻力,与对照组(Ctl+Sal;Ctl+FOR)相似。然而,它与未治疗的哮喘组(Ast+Sal)不同(p<0.05),表明 FOR811A 纠正了肺实质并放松了支气管平滑肌。与对照组(Ctl+Sal;Ctl+FOR)相似,FOR811A 增加了哮喘动物的吸气量和静态顺应性(Ast+Sal,p<0.05),表明该金属药物改善了哮喘期间的吸气能力。形态计量学参数表明,FOR811A 减少了哮喘期间的肺泡塌陷并保持了支气管收缩。除此之外,使用 FOR811A 的分子对接显示出与可溶性鸟苷酸环化酶血红素基团的远端部分具有很强的相互作用,特别是与半胱氨酸残基(Cys141)。总之,FOR811A 放松了支气管平滑肌并改善了哮喘期间的呼吸力学,提供了保护作用,并有望开发出一种抗哮喘药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9461/7954307/0597c627714e/pone.0248394.g001.jpg

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