Fernandes Darren J, Mitchell Richard W, Lakser Oren, Dowell Maria, Stewart Alastair G, Solway Julian
Section of Pulmonary and Critical Care Medicine, University of Chicago, Chicago, IL 60637, USA.
J Appl Physiol (1985). 2003 Aug;95(2):844-53. doi: 10.1152/japplphysiol.00192.2003.
It is now accepted that a host of cytokines, chemokines, growth factors, and other inflammatory mediators contributes to the development of nonspecific airway hyperresponsiveness in asthma. Yet, relatively little is known about how inflammatory mediators might promote airway structural remodeling or about the molecular mechanisms by which they might exaggerate smooth muscle shortening as observed in asthmatic airways. Taking a deep inspiration, which provides relief of bronchodilation in normal subjects, is less effective in asthmatic subjects, and some have speculated that this deficiency stems directly from an abnormality of airway smooth muscle and results in airway hyperresponsiveness to constrictor agonists. Here, we consider some of the mechanisms by which inflammatory mediators might acutely or chronically induce changes in the contractile apparatus that in turn might contribute to hyperresponsive airways in asthma.
现在人们已经认识到,多种细胞因子、趋化因子、生长因子和其他炎症介质促成了哮喘中非特异性气道高反应性的发展。然而,对于炎症介质如何促进气道结构重塑,或者它们可能通过何种分子机制像在哮喘气道中观察到的那样夸大平滑肌缩短,人们了解得相对较少。进行深呼吸在正常受试者中可缓解支气管扩张,但在哮喘患者中效果较差,一些人推测这种缺陷直接源于气道平滑肌异常,并导致气道对收缩激动剂的高反应性。在此,我们探讨炎症介质可能通过哪些机制急性或慢性地诱导收缩装置发生变化,进而可能导致哮喘患者气道高反应性。
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