组织中替代途径的失调导致持续的补体激活,并预测 COVID-19 疾病过程中的结局。
Alternative pathway dysregulation in tissues drives sustained complement activation and predicts outcome across the disease course in COVID-19.
机构信息
National Heart & Lung Institute, Imperial College London, London, UK.
Division of Infection and Immunity and UK Dementia Research Institute Cardiff, Cardiff University, Cardiff, UK.
出版信息
Immunology. 2023 Mar;168(3):473-492. doi: 10.1111/imm.13585. Epub 2022 Nov 28.
Complement, a critical defence against pathogens, has been implicated as a driver of pathology in COVID-19. Complement activation products are detected in plasma and tissues and complement blockade is considered for therapy. To delineate roles of complement in immunopathogenesis, we undertook the largest comprehensive study of complement in COVID-19 to date, comprehensive profiling of 16 complement biomarkers, including key components, regulators and activation products, in 966 plasma samples from 682 hospitalized COVID-19 patients collected across the hospitalization period as part of the UK ISARIC4C (International Acute Respiratory and Emerging Infection Consortium) study. Unsupervised clustering of complement biomarkers mapped to disease severity and supervised machine learning identified marker sets in early samples that predicted peak severity. Compared to healthy controls, complement proteins and activation products (Ba, iC3b, terminal complement complex) were significantly altered in COVID-19 admission samples in all severity groups. Elevated alternative pathway activation markers (Ba and iC3b) and decreased alternative pathway regulator (properdin) in admission samples were associated with more severe disease and risk of death. Levels of most complement biomarkers were reduced in severe disease, consistent with consumption and tissue deposition. Latent class mixed modelling and cumulative incidence analysis identified the trajectory of increase of Ba to be a strong predictor of peak COVID-19 disease severity and death. The data demonstrate that early-onset, uncontrolled activation of complement, driven by sustained and progressive amplification through the alternative pathway amplification loop is a ubiquitous feature of COVID-19, further exacerbated in severe disease. These findings provide novel insights into COVID-19 immunopathogenesis and inform strategies for therapeutic intervention.
补体作为对抗病原体的关键防御系统,被认为是 COVID-19 发病机制的驱动因素。在血浆和组织中检测到补体激活产物,并且考虑将补体阻断作为治疗方法。为了阐明补体在免疫发病机制中的作用,我们进行了迄今为止针对 COVID-19 的最大规模的补体综合研究,对来自 682 名住院 COVID-19 患者的 966 个血浆样本进行了 16 种补体生物标志物的综合分析,这些患者在住院期间的各个阶段均参与了英国 ISARIC4C(国际急性呼吸和新兴感染联盟)研究。未监督的补体生物标志物聚类与疾病严重程度相关,而监督机器学习则确定了早期样本中的标志物集,这些标志物集可预测疾病的严重程度峰值。与健康对照组相比,在所有严重程度组的 COVID-19 入院样本中,补体蛋白和激活产物(Ba、iC3b、末端补体复合物)均发生显著改变。入院样本中替代途径激活标志物(Ba 和 iC3b)升高和替代途径调节剂(备解素)降低与疾病更严重和死亡风险相关。大多数补体生物标志物在严重疾病中水平降低,这与消耗和组织沉积一致。潜在类别混合模型和累积发生率分析表明,Ba 的增加轨迹是预测 COVID-19 疾病严重程度和死亡高峰的有力指标。这些数据表明,早期、不受控制的补体激活是 COVID-19 的普遍特征,由替代途径放大环的持续和渐进放大驱动,在严重疾病中进一步加剧。这些发现为 COVID-19 的免疫发病机制提供了新的见解,并为治疗干预策略提供了信息。
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