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首页> 外文期刊>Respirology : >Resistin-like molecule-β is induced following bronchoconstriction of asthmatic airways.
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Resistin-like molecule-β is induced following bronchoconstriction of asthmatic airways.

机译:哮喘气道的支气管收缩后可诱导产生抵抗素样分子-β。

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摘要

Resistin-like molecule-β (RELM-β) is a necessary and sufficient stimulus for airway remodelling in animal models of asthma, but until recently, its role in human disease had not been investigated. The hypothesis that RELM-β expression would increase with increasing asthma severity and further increase following acute bronchoconstrictor challenges has been examined.Bronchial biopsies from healthy subjects and patients with mild and severe asthma were immunostained for RELM-β, as were airway biopsies obtained in mild asthmatics before and 4 days after repeated inhalation challenges with either allergen, methacholine or methacholine preceded by salbutamol as a control. Bronchial brushings were also evaluated for RELM-β mRNA.RELM-β immunoreactivity, which co-localized to airway epithelial cells, increased with disease severity; healthy volunteers, median per cent epithelial area 1.98%, mild asthma 3.49% and severe asthma 5.89% (P < 0.001 between groups). RELM-β immunoreactivity significantly and inversely correlated in asthma with forced expiratory volume in 1 s % predicted (P = 0.005). Acute changes in immunoexpression were evident after repeated inhalation challenge with allergen (2.15 % to 4.35 % (P = 0.01)) and methacholine (4.21 % to 6.16 % (P = 0.01)) but did not change in the salbutamol/methacholine challenge group. These changes correlated with change in basement membrane thickness (r = 0.38, P = 0.02). Epithelial RELM-β gene expression was not altered in asthma.RELM-β may play an important role not only in animal models of airway remodelling, but also in human airway pathology.
机译:抵抗素样分子-β(RELM-β)是哮喘动物模型中气道重塑的必要和充分刺激,但直到最近,其在人类疾病中的作用尚未得到研究。已经检验了以下假设:RELM-β表达会随着哮喘严重程度的增加而增加,并在急性支气管狭窄挑战后进一步增加。对健康受试者以及轻度和重度哮喘患者的支气管活检组织进行了RELM-β免疫染色,在轻度呼吸道活检组织中也进行了免疫染色哮喘患者在反复吸入刺激之前和之后4天,使用过敏原,乙酰甲胆碱或乙酰甲胆碱,然后以沙丁胺醇作为对照。还评估了支气管刷牙的RELM-βmRNA。共定位于气道上皮细胞的RELM-β免疫反应性随疾病的严重程度而增加。健康志愿者,上皮面积中位数百分比为1.98%,轻度哮喘为3.49%,重度哮喘为5.89%(组间P <0.001)。在哮喘中,RELM-β免疫反应性与预计的呼气量在1 s%的预测值之间呈显着负相关(P = 0.005)。在反复吸入变应原(2.15%至4.35%(P = 0.01))和甲胆碱(4.21%至6.16%(P = 0.01))后,免疫表达的急性变化明显,但在沙丁胺醇/美沙胆碱激发组中未改变。这些变化与基底膜厚度的变化相关(r = 0.38,P = 0.02)。哮喘中上皮RELM-β基因的表达没有改变。RELM-β不仅在气道重塑的动物模型中而且在人的气道病理学中都可能起重要作用。

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