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Enhanced pause correlates with airway neutrophils and airway-epithelial injury in asthmatic mice treated with dexamethasone

机译:增强的暂停与用地塞米松处理的哮喘小鼠的气道中性粒细胞和气道上皮损伤相关联

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摘要

Objective: To investigate the correlations among airway inflammation, airway epithelial injury and airway hyperresponsiveness (AHR) in asthmatic mice treated with dexamethasone. Methods: Female BALB/c mice were sensitized with intraperitoneal and hypodermic injections of ovalbumin (OVA) and aluminum on days 0, 7 and 14, challenged with OVA starting on day 21 for 10 days, and treated with dexamethasone via intraperitoneal injection starting on day 28 for 3 days. Female C57BL/6 mice were treated intranasally with house dust mite (HDM) on days 1 and 14, challenged intranasally with HDM on days 21, 23, 25, 27 and 29, and treated with sivelestat (a selective neutrophil elastase inhibitor) via intraperitoneal injection after each challenge. Following the final challenge, enhanced pause (Penh) and differential cell counts in the broncho-alveolar lavage fluid were measured and the correlations were analyzed. Results: Compared with OVA-challenged BALB/c mice, the counterpart mice treated with dexamethasone showed reduced Penh and shedding of airway epithelial cells. In addition, we found that Penh 50 (an indicator of AHR) had positive correlations with airway neutrophils and shedding of airway epithelial cells, but no correlation with eosinophils, lymphocytes or macrophages. Moreover, shedding of airway epithelial cells had positive correlations with airway neutrophils, but no correlation with eosinophils, lymphocytes or macrophages. Further, sivelestat decreased Penh 50 and shed airway-epithelial cells in HDM-challenged C57BL/6 mice. Conclusions: Collectively, our findings suggest that airway neutrophils and excessive shedding of airway epithelial cells, but not eosinophils, lymphocytes or macrophages, may be involved in AHR in asthmatic mice treated with dexamethasone.
机译:目的:探讨用地塞米松处理的哮喘小鼠的气道炎症,气道上皮损伤和气道高反应性(AHR)的相关性。方法:雌性BALB / C小鼠在0,7和14天的卵烧蛋白(OVA)和铝的腹膜内(OVA)和皮下注射致敏感,用OVA在第21天开始攻击10天,并在当天开始用腹膜内注射用地塞米松处理28天3天。雌性C57BL / 6小鼠在第1天和第14天鼻内与房屋粉尘(HDM)处理,在第21,21,23,25,27和29天,HDM攻击,并通过腹膜内用Sivelestat(选择性中性粒细胞弹性蛋白酶抑制剂)处理每次挑战后注射。在最终挑战之后,测量了支气管 - 肺泡灌洗液中的增强暂停(PENH)和差异细胞计数,并分析了相关性。结果:与OVA挑战的BALB / C小鼠相比,用地塞米松治疗的对手小鼠表现出低细的PENH和气道上皮细胞的脱落。此外,我们发现PENH 50(AHR的指标)与气道中性粒细胞和气道上皮细胞的脱落,但与嗜酸性粒细胞,淋巴细胞或巨噬细胞没有相关性。此外,气道上皮细胞的脱落与气道中性粒细胞呈正相关,但与嗜酸性粒细胞,淋巴细胞或巨噬细胞没有相关性。此外,Sivelestat在HDM攻击的C57BL / 6小鼠中减少了PENH 50和脱落气道上皮细胞。结论:集体,我们的研究结果表明,气道中性粒细胞和气道上皮细胞的过度脱落,而不是嗜酸性粒细胞,淋巴细胞或巨噬细胞,可参与用地塞米松处理的哮喘小鼠中的AHR。

著录项

  • 来源
    《The journal of asthma》 |2019年第1期|共10页
  • 作者单位

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Pediat Res Inst Childrens Hosp Chongqing Peoples R China;

    Chongqing Med Univ Pediat Res Inst Childrens Hosp Chongqing Peoples R China;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

    Chongqing Med Univ Ctr Clin Mol Med Chongqing Stem Cell Therapy Technol Res Ctr Childrens Hosp;

    Chongqing Med Univ Pediat Res Inst Childrens Hosp Chongqing Peoples R China;

    Chongqing Med Univ Dept Resp Med Key Lab Child Dev &

    Disorders Childrens Hosp Minist Educ;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 呼吸系及胸部疾病;
  • 关键词

    asthma; airway epithelium; dexamethasone; neutrophils; enhanced pause; airway hyperresponsiveness;

    机译:哮喘;呼吸道上皮;地塞米松;中性粒细胞;增强暂停;气道高反应性;

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