Division of Pulmonary and Critical Care Medicine, Department of Medicine, University of California, San Francisco, San Francisco, California.
Am J Respir Cell Mol Biol. 2022 Nov;67(5):520-527. doi: 10.1165/rcmb.2022-0107TR.
Coronavirus disease (COVID-19) begins with upper airway symptoms but proceeds in a significant proportion of patients to life-threatening infection of the lower respiratory tract, where an exuberant inflammatory response, edema, and adverse parenchymal remodeling impair gas exchange. Respiratory failure is caused initially by flooding of the airspaces with plasma exudate, sloughed epithelium, and inflammatory cells. For many patients with COVID-19, this acute phase has been observed to give way to a prolonged course of acute respiratory distress syndrome, and a significant proportion of patients go on to develop fibroproliferative remodeling of the lung parenchyma, which lengthens the duration of respiratory impairment and mechanical ventilation. Monocyte-derived macrophages have previously been implicated in the fibrotic phase of lung injury in multiple models. From several recent studies that used single-cell genomic techniques, a profile of the transcriptomic state of COVID-19 lung macrophages has emerged. Linkages have been made between these macrophages, which are monocyte-derived and CD163, and profibrotic macrophages found in other contexts, including animal models of fibrosis and idiopathic pulmonary fibrosis. Here, emerging concepts of macrophage profibrotic function in COVID-19 are highlighted with a focus on gaps in knowledge to be addressed by future research.
冠状病毒病(COVID-19)最初表现为上呼吸道症状,但在很大一部分患者中,会进展为危及生命的下呼吸道感染,此时过度活跃的炎症反应、水肿和不良的实质重塑会损害气体交换。呼吸衰竭最初是由于肺泡腔充满血浆渗出物、脱落的上皮细胞和炎症细胞引起的。对于许多 COVID-19 患者,这种急性期已经让位于急性呼吸窘迫综合征的长期病程,很大一部分患者继续发展为肺实质的纤维增殖性重塑,这延长了呼吸功能障碍和机械通气的持续时间。单核细胞衍生的巨噬细胞先前已被牵连到多种模型中的肺损伤纤维化阶段。从最近使用单细胞基因组技术的几项研究中,出现了 COVID-19 肺巨噬细胞转录组状态的特征。这些巨噬细胞与其他情况下(包括纤维化动物模型和特发性肺纤维化)发现的单核细胞衍生和 CD163 相关的促纤维化巨噬细胞之间建立了联系。本文重点介绍了 COVID-19 中巨噬细胞促纤维化功能的新观点,并强调了未来研究需要解决的知识空白。
