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Towards a vaccine for chronic obstructive pulmonary disease

机译:寻求一种用于慢性阻塞性肺疾病的疫苗

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This review discusses chronic obstructive pulmonary disease as an outcome of two pathogenic pathways: the first resulting from inhalation of toxins and the second a consequence of bacterial colonisation of damaged airways. Earlier assessment of the role played by bacteria in acute exacerbations was compromised by a deficiency of quality data and the use of parameters more relevant to invasive infection. Data are reviewed to support a hypothesis that states intrabronchial inflammation reflects an excessive and inappropriate host response (largely mediated by Th17 cells derived from gut-associated lymphoid tissues) to colonising bacteria acting as an 'antigen sump' (in essence, a hypersensitivity reaction). It is proposed that both viral and bacterial infections exacerbate inflammation through a common pathway that involves colonising bacteria. An oral vaccine containing inactivated non-typeable Haemophilus influenzae augments a protective loop that involves the aspiration of bronchus content into the gut and reduces the severity of acute exacerbations including the need for hospital admission by reducing the 'load' of bacteria comprising this final common path. The positive clinical results from trials using oral NTHi support both the concept that bacterial colonisation of damaged airways is a potent second pathogenic pathway and that oral immunotherapy provides a significant therapeutic advance in limiting damage in chronic obstructive pulmonary disease.
机译:这篇综述讨论了慢性阻塞性肺疾病是两种致病途径的结果:一种是吸入毒素导致的,另一种是细菌受损的气道细菌定殖的结果。缺乏质量数据和使用与侵袭性感染更相关的参数损害了对细菌在急性发作中所起作用的早期评估。审查数据以支持以下假设,即支气管内炎症反应了对定居细菌充当“抗原贮槽”(本质上是超敏反应)的过度和不适当的宿主反应(主要由源自肠道相关淋巴组织的Th17细胞介导) 。有人提出病毒和细菌感染都通过涉及细菌定植的共同途径加剧了炎症。含有灭活的不可分型流感嗜血杆菌的口服疫苗可增强保护环,将支气管内含物吸入肠道,并降低急性加重的严重性,包括通过减少构成这一最终共同途径的细菌的“负荷”来降低住院率。使用口服NTHi进行的试验获得的积极临床结果支持以下观点:受损气道的细菌定植是有效的第二致病途径,并且口服免疫疗法在限制慢性阻塞性肺疾病的损害方面提供了重要的治疗进展。

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