孟鲁司特作用下诱导肺纤维化的组织病理学评价

Mohammed Rabah Mahdi, Wassan Abdul Kareem Abbas, Ghaith Ali Jasim
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摘要

肺纤维化(PF)是一种导致肺瘢痕形成的间质性肺疾病。肺纤维化有几种类型,如家族性肺纤维化、特发性肺纤维化和其他与非特异性间质性肺炎相关的肺纤维化。最常见的类型是特发性肺纤维化,原因不明。肺纤维化引起肺组织学改变,肺实质消失,取而代之的是炎症浸润,肺动脉轻度增厚。2011年肺纤维化的治疗包括硫唑嘌呤、皮质类固醇和n -乙酰半胱氨酸,但在2014年该指南被尼达尼布和吡非尼酮所取代。本研究使用吡非尼酮作为治疗肺纤维化的标准药物,孟鲁司特是Cysteinyl leukotrienes (CysLT)拮抗剂,与位于呼吸道平滑肌细胞上的受体(CysLTE4)结合,通过抑制炎症标志物tgf - β1产生抗炎作用。将60只雄性大鼠分为5组,每组12只,对照组灌胃蒸馏水,诱导组单次气管内给药博来霉素,吡非尼酮组50mg/kg,孟鲁司特组20mg/kg,联合组半剂量吡非尼酮和孟鲁司特。用孟鲁司特或吡非尼酮治疗28天后,处死大鼠,取各组脏器(肺)置于10%福尔马林缓冲液中进行组织病理学研究。博来霉素给药14天后,结果显示博来霉素各组肺实质大量消失,取而代之的是炎症浸润和肺动脉内侧增厚,而孟鲁司特和吡非尼酮组在治疗28天后肺实质和肺动脉正常。综上所述,除对照组外,博来霉素在14天后改变肺组织组织学,引起肺纤维化,而吡非尼酮、孟鲁司特和半剂量吡非尼酮与半剂量孟鲁司特联合用药28天后肺结构恢复正常。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Histopathological evaluation of induced pulmonary fibrosis under the effect of montelukast
Pulmonary fibrosis (PF) is an interstitial lung disease leading to scarring of the lung. There are several types of lung fibrosis as familial pulmonary fibrosis, idiopathic pulmonary fibrosis, and others associated with non-specific   interstitial pneumonia. The most common type is idiopathic pulmonary fibrosis which is an unknown cause. Lung fibrosis causes changes in the histology of the lung by the disappearance of the lung parenchyma, replaced by an inflammatory infiltrate, and mild thickening of the pulmonary artery. The management of pulmonary fibrosis included Azathioprine, corticosteroid, and N-acetyl cysteinyl in 2011 but in 2014 this guideline was removed and replaced by nintedanib and pirfenidone. This study used Pirfenidone, as standard therapy for the treatment of pulmonary fibrosis, and montelukast is Cysteinyl leukotrienes (CysLT) antagonist which binds to its receptor (CysLTE4) located on smooth muscle cells of the respiratory airway causing anti-inflammatory effect by inhibition of inflammatory markers as TGFβ1. Sixty male rats were divided into five groups,12 rats for each group where the control group received distilled water by gastric gavage, the induction group received bleomycin intratracheally as a single dose, the pirfenidone group received pirfenidone 50mg/kg, montelukast group received montelukast 20mg/kg and the combination group received a half dose of pirfenidone and montelukast. After twenty-eight days after the treatment with montelukast or pirfenidone sacrifice rats and collect the organ (lungs) from each group were then placed in buffer formalin 10% for histopathological study. After 14 days from bleomycin dose, results show that bleomycin cause massive disappearance of pulmonary parenchyma that was replaced by an inflammatory infiltrate and medial thickening of the pulmonary artery in all groups, but montelukast and pirfenidone show normal lung paranchyma and pulmonary artery after 28 days of treatment in pirfenidone, montelukast, and combination groups. In conclusion, that bleomycin changes the histology of the lung causing induction of lung fibrosis in all groups after 14 days except control group but pirfenidone, montelukast, and combination of half dose of pirfenidone with a half dose of montelukast return the lung to normal architecture after 28 days of treatment.
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