Schleimer Robert P
Northwestern University Feinberg School of Medicine, Division of Allergy-Immunology, 240 East Huron, Room 2318, Chicago, IL 60611.
Proc Am Thorac Soc. 2005;2(4):342-6; discussion 371-2. doi: 10.1513/pats.200504-030SR.
Innate immune responses appear to be partially responsible for maintaining inflammation and tissue destruction in chronic obstructive pulmonary disease. In the early stages of the disease in smokers, the airways are bombarded with large quantities of particulate material, and activation of phagocytic cells results in the release of many of the mediators believed to remodel the airways. Ironically, failure of the innate immune defense system, either by inherited deficiency or as a result of chronic smoke inhalation, is likely to result in increased susceptibility to infectious disease and exacerbations of chronic obstructive pulmonary disease. It is well known that deficiencies in the production of collectins, pentraxins, and complement can lead to increased infections, and several studies indicate that deficiency in one or another innate defense component is associated with increased exacerbations. Corticosteroids reduce exacerbations in part because of their ability to boost the production of innate host-defense molecules. Therapeutic approaches that stimulate the generation of antimicrobial molecules in the lungs might be able to reduce disease exacerbations.
先天性免疫反应似乎在慢性阻塞性肺疾病中炎症的维持和组织破坏方面起到了部分作用。在吸烟者疾病的早期阶段,气道会受到大量颗粒物的侵袭,吞噬细胞的激活会导致许多被认为会重塑气道的介质释放。具有讽刺意味的是,先天性免疫防御系统的失效,无论是由于遗传缺陷还是长期吸入烟雾,都可能导致对传染病的易感性增加以及慢性阻塞性肺疾病的加重。众所周知,凝集素、五聚素和补体产生不足会导致感染增加,多项研究表明,一种或另一种先天性防御成分的缺乏与病情加重有关。皮质类固醇能部分减少病情加重,这是因为它们有促进先天性宿主防御分子产生的能力。刺激肺部抗菌分子生成的治疗方法或许能够减少疾病的加重。