Table 1.
Different aspects of the two phenotypes of COVID associated lung fibrosis.
| COVID-19 related ARDS (CARDS) | post-COVID pulmonary fibrosis (PCPF) | |
|---|---|---|
| Clinical features | 7–14 days after initial symptoms secondary pulmonary hypertension +++ |
4–6 to 12 weeks after initial infection secondary pulmonary hypertension + |
| Mortality 90 days | 30–50% | unknown |
| Risk factors | Mechanical ventilation, VILI, hyperoxia, prolonged hypoxia, increased BMI, elderly patients, possibly thromboembolism and hypercoagulability, possibly NETS | profound dyspnoea, higher respiratory rate, comorbid hypertension, ICU admission, hyperoxia, prolonged hypoxia, elderly patients, possibly thromboembolism and hypercoagulability, possibly NETS, higher CRP levels, lymphocytopenia, neutrophilia, eosinopenia lower baseline IFN-γ and MCP-3 |
| Biomarkers | Classic “cytokine storm” not observed IL-6 moderately increased persistent deactivation of key immune cells e.g. reduced surface expression of the mHLA-DR |
cytokine-driven: TGF-β and IL-1β longer telomere lengths appear to be protective, this genomic biomarker estimates balance of profibrotic and antifibrotic susceptibilities |
| Restrictive ventilatory defect | ++ | +++ (rib cage shrinkage) |
| Pneumothorax | +++ | ++ |
| Pathophysiology | Severe pulmonary infiltration/edema and endothelitis | inflammation leading to impaired alveolar homeostasis, alteration of pulmonary physiology resulting in pulmonary fibrosis |
ARDS = Acute Respiratory Distress Syndrome, CARDS = COVID-19 related ARDS, CRP = C-reactive protein, IFN-γ = interferon gamma, IL = interleukin, MCP-3 = monocyte chemoattractant protein 3, mHLA-DR = monocytic human leucocyte antigen-DR, NETS = neutrophil extracellular traps, PCPF = post-COVID pulmonary fibrosis, TGF = Tumour Growth Factor, VILI = mechanical ventilation-induced lung injury.