Tissue Proteomic Analysis Identifies Mechanisms and Stages of Immunopathology in Fatal COVID-19.
Clark D RussellAsta ValanciuteNaomi N GachanjaJillian StephenRebekah Penrice-RandalStuart D ArmstrongSara ClohiseyBo WangWael Al QsousWilliam A WallaceGabriel C OniscuJo StevensDavid J HarrisonKevin DhaliwalJulian A HiscoxJohn Kenneth BaillieAhsan R AkramDavid A DorwardChristopher D LucasPublished in: American journal of respiratory cell and molecular biology (2021)
Immunopathology occurs in the lung and spleen in fatal COVID-19, involving monocytes/macrophages and plasma cells. Anti-inflammatory therapy reduces mortality but additional therapeutic targets are required. We aimed to gain mechanistic insight into COVID-19 immunopathology by targeted proteomic analysis of pulmonary and splenic tissues. Lung parenchymal and splenic tissue was obtained from 13 post-mortem examinations of patients with fatal COVID-19. Control tissue was obtained from cancer resection samples (lung) and deceased organ donors (spleen). Protein was extracted from tissue by phenol extraction. Olink® multiplex immunoassay panels were used for protein detection and quantification. Proteins with increased abundance in the lung included MCP-3, antiviral TRIM21 and pro-thrombotic TYMP. OSM and EN-RAGE/S100A12 abundance was correlated, and associated with inflammation severity. Unsupervised clustering identified 'early viral' and 'late inflammatory' clusters with distinct protein abundance profiles, and differences in illness duration prior to death and presence of viral RNA. In the spleen, lymphocyte chemotactic factors and CD8A were decreased in abundance, and pro-apoptotic factors were increased. B-cell receptor signalling pathway components and macrophage colony stimulating factor (CSF-1) were also increased. Additional evidence for a sub-set of host factors (including DDX58, OSM, TYMP, IL-18, MCP-3 and CSF-1) was provided by overlap between (i) differential abundance in spleen and lung tissue, (ii) meta-analysis of existing datasets, and (iii) plasma proteomic data. This proteomic analysis of lung parenchymal and splenic tissue from fatal COVID-19 provides mechanistic insight into tissue anti-viral responses, inflammation and disease stages, macrophage involvement, pulmonary thrombosis, splenic B-cell activation and lymphocyte depletion. This article is open access and distributed under the terms of the Creative Commons Attribution 4.0 International License (https://creativecommons.org/licenses/by/4.0/).
Keyphrases
- sars cov
- coronavirus disease
- anti inflammatory
- oxidative stress
- antibiotic resistance genes
- machine learning
- pulmonary hypertension
- gene expression
- minimally invasive
- cell death
- squamous cell carcinoma
- pulmonary embolism
- bone marrow
- young adults
- induced apoptosis
- endoplasmic reticulum stress
- cancer therapy
- cell proliferation
- cardiovascular disease
- amino acid
- genome wide
- electronic health record
- cell therapy
- data analysis
- cerebrospinal fluid
- mesenchymal stem cells
- high throughput
- pi k akt
- anaerobic digestion