Idiopathic pulmonary fibrosis (IPF) is a dreadful, chronic, and irreversibly progressive fibrosing disease leading to death in all patients affected, and IPF acute exacerbations constitute the most devastating complication during its clinical course. IPF exacerbations are subacute/acute, clinically significant deteriorations of unidentifiable cause that usually transform the slow and more or less steady disease decline to the unexpected appearance of acute lung injury/acute respiratory distress syndrome (ALI/ARDS) ending in death. The histological picture is that of diffuse alveolar damage (DAD), which is the tissue counterpart of ARDS, upon usual interstitial pneumonia, which is the tissue equivalent of IPF. ALI/ARDS and acute interstitial pneumonia share with IPF exacerbations the tissue damage pattern of DAD. 'Treatment' with high-dose corticosteroids with or without an immunosuppressant proved ineffective and represents the coup de grace for these patients. Provision of excellent supportive care and the search for and treatment of the 'underlying cause' remain the only options. IPF exacerbations require rapid decisions about when and whether to initiate mechanical support. Admission to an intensive care unit (ICU) is a particular clinical and ethical challenge because of the extremely poor outcome. Transplantation in the ICU setting often presents insurmountable difficulties.
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机译:特发性肺纤维化(IPF)是一种可怕的,慢性的,不可逆转的进行性纤维化疾病,导致所有受影响的患者死亡,并且IPF急性加重是其临床过程中最具有破坏力的并发症。 IPF恶化是亚急性/急性的,临床上无法查明原因的严重恶化,通常会导致疾病的缓慢和或多或少的稳定转变为急性肺损伤/急性呼吸窘迫综合征(ALI / ARDS)的意外出现,并最终死亡。组织学图片是弥漫性肺泡损伤(DAD),它是ARDS的组织对应物,是通常的间质性肺炎,它是IPF的组织等效物。 ALI / ARDS和急性间质性肺炎与IPF共同加重了DAD的组织损伤模式。大剂量皮质类固醇与或不与免疫抑制剂的“治疗”被证明是无效的,代表了这些患者的妙招。唯一的选择是提供优质的支持治疗以及寻找和治疗“根本原因”。 IPF恶化需要快速决定何时以及是否启动机械支撑。由于结局极差,因此入院重症监护病房(ICU)是一项特殊的临床和伦理挑战。在ICU环境中进行移植通常会遇到难以克服的困难。
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