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地塞米松对变应性豚鼠抗原诱导的高分子量糖缀合物分泌的影响。

Effect of dexamethasone on antigen-induced high molecular weight glycoconjugate secretion in allergic guinea pigs.

作者信息

Savoie C, Plant M, Zwikker M, van Staden C J, Boulet L, Chan C C, Rodger I W, Pon D J

机构信息

Merck Frosst Centre for Therapeutic Research, Kirkland, Quebec, Canada.

出版信息

Am J Respir Cell Mol Biol. 1995 Aug;13(2):133-43. doi: 10.1165/ajrcmb.13.2.7626283.

Abstract

The ovalbumin-sensitized guinea pig is commonly used as a small animal model of allergic asthma. This animal model exhibits many of the hallmark characteristics observed in patients afflicted with asthma including nonspecific airway hyperreactivity, airway eosinophilia, early and late phase bronchoconstriction, and plasma extravasation into the airways. In addition, mucous hypersecretion in the airways of asthmatic patients is thought to be responsible for the plugging of distal airways and to contribute to the morbidity and mortality associated with the disease process. In this study we examined whether the allergic guinea pig model exhibits an increase in airway high molecular weight glycoconjugate (HMWG) secretion in response to an antigen challenge and whether dexamethasone exerts any modulatory effects upon the response. Ovalbumin (OVA) -sensitized guinea pigs were challenged with OVA 2 wk following the initial exposure. Trachobronchoalveolar lavages (TBAL) were performed, and the samples were assayed for total eosinophil cell number, eosinophil peroxidase activity (EPO), and both acidic and neutral HMWG content. Morphometric analysis of mucous-containing cells was also performed on tissue sections prepared from the trachea, mainstem bronchus, and three lobes of the left lung. Within 24 h of an antigen challenge, TBAL samples obtained from the allergic guinea pigs exhibited increases in eosinophil cell number, measured EPO enzyme activity, and acidic HMWG content compared to TBAL samples prepared from vehicle-exposed animals. These antigen-induced changes were dependent on the concentration of aerosolized OVA administered. Exposing the animals to 0.3% OVA provoked a 6.23-fold increase in airway eosinophils, 15-fold elevation in TBAL EPO enzyme activity, and 175% increase in TBAL acidic HMWG. No significant changes in TBAL neutral HMWG were measured. The changes in measured EPO activity correlated with the levels of acidic HMWG found in the TBAL samples (r = 0.73, P < or = 0.001). The measured increase in TBAL acidic HMWG was time dependent and was found to be maximal at 2 h post-antigen challenge. Morphometric analysis of Alcian blue (pH 2.5) -stained airway sections showed a decline in stored mucosubstances following the antigen exposure, supporting the notion that the allergic guinea pig model exhibits a mucosecretory component. Pretreating the animals with dexamethasone attenuated the antigen-induced release of HMWG and changes in measured EPO activity. In conclusion, these data indicate that the allergic guinea pig may be a useful model for examining the neural and cellular mechanisms underlying mucus hypersecretion in individuals afflicted with bronchial asthma.

摘要

卵清蛋白致敏的豚鼠通常被用作过敏性哮喘的小动物模型。该动物模型展现出了哮喘患者身上观察到的许多标志性特征,包括非特异性气道高反应性、气道嗜酸性粒细胞增多、早发性和迟发性支气管收缩,以及血浆渗入气道。此外,哮喘患者气道中的黏液分泌过多被认为是远端气道堵塞的原因,并导致了与疾病进程相关的发病率和死亡率。在本研究中,我们检测了过敏性豚鼠模型在抗原刺激后气道高分子量糖缀合物(HMWG)分泌是否增加,以及地塞米松对该反应是否有任何调节作用。在初次接触卵清蛋白(OVA)2周后,用OVA对致敏的豚鼠进行激发。进行气管支气管肺泡灌洗(TBAL),并对样本进行总嗜酸性粒细胞数、嗜酸性粒细胞过氧化物酶活性(EPO)以及酸性和中性HMWG含量的检测。还对从气管、主支气管和左肺的三个肺叶制备的组织切片进行了含黏液细胞的形态计量分析。在抗原激发后24小时内,与用赋形剂处理的动物制备的TBAL样本相比,从过敏性豚鼠获得的TBAL样本中嗜酸性粒细胞数增加、测得的EPO酶活性增加以及酸性HMWG含量增加。这些抗原诱导的变化取决于雾化OVA的给药浓度。将动物暴露于0.3%OVA可使气道嗜酸性粒细胞增加6.23倍、TBAL中EPO酶活性提高15倍以及TBAL酸性HMWG增加175%。未测得TBAL中性HMWG有显著变化。测得的EPO活性变化与TBAL样本中发现的酸性HMWG水平相关(r = 0.73,P≤0.001)。测得的TBAL酸性HMWG增加是时间依赖性的,并且在抗原激发后2小时达到最大值。对阿尔新蓝(pH 2.5)染色的气道切片进行形态计量分析显示,抗原暴露后储存的黏液物质减少,这支持了过敏性豚鼠模型具有黏液分泌成分的观点。用地塞米松预处理动物可减弱抗原诱导的HMWG释放和测得的EPO活性变化。总之,这些数据表明,过敏性豚鼠可能是一个有用的模型,用于研究支气管哮喘患者黏液分泌过多背后的神经和细胞机制。

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