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首页> 外文期刊>Endocrinology >Relaxin reverses airway remodeling and airway dysfunction in allergic airways disease.
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Relaxin reverses airway remodeling and airway dysfunction in allergic airways disease.

机译:在过敏性气道疾病中,松弛素逆转气道重塑和气道功能障碍。

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摘要

Mice deficient in the antifibrotic hormone relaxin develop structural changes in the airway that resemble airway remodeling, and demonstrate exaggerated remodeling changes in models of allergic airways disease (AAD). Relaxin expression in asthma has not been previously studied. We evaluated the efficacy of relaxin in the treatment of established airway remodeling in a mouse model of AAD. Relaxin expression in mouse AAD was also examined by immunohistochemistry and real-time PCR. BALB/c mice with established AAD were treated with relaxin or vehicle control (sc for 14 d), and effects on airway remodeling, airway inflammation, and airway hyperresponsiveness (AHR) were assessed. Relaxin expression was significantly reduced in the airways of mice with AAD compared with controls. Recombinant relaxin treatment in a mouse model of AAD reversed collagen deposition and epithelial thickening, and significantly improved AHR (all P < 0.05 vs. vehicle control), but did not influence airway inflammation or goblet cell hyperplasia. Relaxin treatment was associated with increased matrix metalloproteinase-2 levels, suggesting a possible mechanism for its antifibrotic effects. Endogenous relaxin expression is decreased in murine AAD, whereas exogenous relaxin represents a novel treatment capable of reversing established airway remodeling and AHR.
机译:缺乏抗纤维化激素松弛素的小鼠会在气道中形成类似于气道重塑的结构变化,并在过敏性气道疾病(AAD)模型中表现出夸大的重塑变化。先前尚未研究哮喘中松弛素的表达。我们评估了松弛素在AAD小鼠模型中建立的气道重塑中的疗效。还通过免疫组织化学和实时PCR检查了小鼠AAD中松弛素的表达。用松弛素或媒介物对照(sc治疗14 d)治疗已建立AAD的BALB / c小鼠,并评估其对气道重塑,气道炎症和气道高反应性(AHR)的影响。与对照组相比,在患有AAD的小鼠的气道中,松弛素的表达显着降低。 AAD小鼠模型中的重组松弛素治疗可逆转胶原蛋白沉积和上皮增厚,并显着改善AHR(与溶媒对照相比,所有P <0.05),但不影响气道炎症或杯状细胞增生。松弛素治疗与基质金属蛋白酶2水平升高有关,提示其抗纤维化作用的可能机制。内源性松弛素表达在鼠类AAD中降低,而外源性松弛素代表一种能够逆转已建立的气道重塑和AHR的新型治疗方法。

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