Abstract

Life-threatening COVID-19 is associated with strong inflammation, where an IL-6-driven cytokine storm appears to be a cornerstone for enhanced pathology. Nonetheless, the specific inhibition of such pathway has shown mixed outcomes. This could be due to variations in the dose of tocilizumab used, the stage in which the drug is administered or the severity of disease presentation. Thus, we performed a retrospective multicentric study in 140 patients with moderate to critical COVID-19, 79 of which received tocilizumab in variable standard doses (< 400 mg, 400–800 mg or > 800 mg), either at the viral (1–7 days post-symptom onset), early inflammatory (8–15) or late inflammatory (16 or more) stages, and compared it with standard treated patients. Mortality, reduced respiratory support requirements and pathology markers were measured. Tocilizumab significantly reduced the respiratory support requirements (OR 2.71, CI 1.37–4.85 at 95%) and inflammatory markers (OR 4.82, CI 1.4–15.8) of all patients, but mortality was only reduced (4.1% vs 25.7%, p = 0.03) when the drug was administered at the early inflammatory stage and in doses ranging 400–800 mg in severely-ill patients. Despite the apparent inability of Tocilizumab to prevent the progression of COVID-19 into a critical presentation, severely-ill patients may be benefited by its use in the early inflammatory stage and moderate doses.

Highlights

  • Life-threatening COVID-19 is associated with strong inflammation, where an IL-6-driven cytokine storm appears to be a cornerstone for enhanced pathology

  • The records were screened for the following inclusion criteria: (i) patients with positive test results for SARS-CoV-2, (ii) hospitalized patients after a moderate to severe COVID-19, (iii) files that showed laboratory evaluations in at least 80% of the in-hospital days, (iv) patients receiving any kind of respiratory support, and (v) patients with signed informed consent for the study

  • After screening the databases of the aforementioned Hospitals in search for eligible clinical files, we identified 260 records. 201 matched our inclusion criteria, but only 140 of such could be included in the study after eliminating those that met any or all the exclusion criteria (Fig. 1)

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Summary

Introduction

Life-threatening COVID-19 is associated with strong inflammation, where an IL-6-driven cytokine storm appears to be a cornerstone for enhanced pathology. The specific inhibition of such pathway has shown mixed outcomes This could be due to variations in the dose of tocilizumab used, the stage in which the drug is administered or the severity of disease presentation. If inflammation progresses beyond 16 days to a late inflammatory stage (LIS), critical disease with acute respiratory distress syndrome, acute cardiac injury, multi-organ failure and death are most likely to ­occur[7,8] This line of thought leads to the hypothesis that the VS of the disease may be optimally treated with anti-viral agents, and without strong pleiotropic anti-inflammatory ­drugs[6]; whereas the inflammatory stage may be best controlled by the means of anti-inflammatory a­ gents[9,10], with little to no benefit from concomitant administration of anti-viral a­ gents[11]

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