Ismael Francisco Aomar-Millán1, Juan Salvatierra2, José Luis Callejas-Rubio3, Enrique Raya-Álvarez2. 1. Servicio de Medicina Interna, Hospital Clínico Universitario San Cecilio, Granada, Spain. Electronic address: iaomarmillan@hotmail.com. 2. Servicio de Reumatología, Hospital Clínico Universitario San Cecilio, Granada, Spain. 3. Servicio de Medicina Interna, Hospital Clínico Universitario San Cecilio, Granada, Spain.
Dear Editor,We have read with interest the article by Figuero-Pérez et al. published in the last issue of your journal suggesting the usefulness of anakinra in severe respiratory SARS-CoV-2 infection refractory to tocilizumab and would like to make some observations.The clinical course of SARS-CoV-2 infection has three distinct clinical phases. In the initial phase there is viral replication with flu-like symptoms and then some patients progress, between day 6 and 13 of symptom onset, to a hyperinflammatory phase with the development of pneumonia that may progress to respiratory distress syndrome.The pathogenesis of severe SARS-CoV-2 infection involves dysregulation of the immune response with lymphopenia, increased pro-inflammatory cytokines (IL-1, IL-2, IL-6, IL-7 or TNF alpha) and a decrease in gamma-interferon. This leads to a systemic inflammatory syndrome with elevated acute phase reactants such as C-reactive protein and ferritin.Treatment of this inflammatory phase with drugs such as dexamethasone or tocilizumab has been shown to reduce mortality4, 5.Anakinra, an IL-1 receptor antagonist, has recently obtained EMA approval for treatment in adult patients with COVID-19 pneumonia and risk of progression to severe respiratory failure based on the SAVE MORE clinical trial which demonstrated a reduction in 28-day mortality and hospital stay in those treated early with anakinra.There is little evidence regarding rescue therapy in patients with poor clinical outcome despite corticosteroids and/or immunomodulators. In an article published by our group, we analysed 143 patients with moderate/severe SARS-CoV-2 pneumonia and hyperinflammation treated with various regimens based on the protocols of that date. We observed that in those who had not responded to corticosteroids with or without tocilizumab, treatment with anakinra could be a useful alternative. Our patients received 100 mg/12 h on day 1 if they weighed between 50 and 60 kg, 100 mg/8 h between 60 and 75 kg or 100 mg/6 h if they weighed >75 kg. Subsequently all received 100 mg/12 h from day 2 to day 6. After adjustment for age and clinical severity indices, anakinra administration was associated with a reduced risk of mortality (HR; .518, 95% CI .265–.910, p
= .0437).In the case published by Figuero-Pérez et al. we consider that it cannot be suggested that the patient's clinical improvement was due to anakinra when a single dose of 100 mg was administered. Given that the half-life of anakinra is 4−6 h and that of tocilizumab around 6 days, it is likely that the patient’s improvement was due to the effect of tocilizumab. There is currently no consensus on the optimal doses of anakinra in this clinical setting, but higher and longer doses have been used in the literature8, 9.
Authors: Juan Salvatierra; Úrsula Torres-Parejo; Francisco Anguita-Santos; Ismael Francisco Aomar-Millán; Naya Faro-Miguez; José Luis Callejas-Rubio; Ángel Ceballos-Torres; María Teresa Cruces-Moreno; Francisco Javier Gómez-Jiménez; José Hernández-Quero Journal: Intern Emerg Med Date: 2021-01-05 Impact factor: 3.397
Authors: Jesús Villar; Carlos Ferrando; Domingo Martínez; Alfonso Ambrós; Tomás Muñoz; Juan A Soler; Gerardo Aguilar; Francisco Alba; Elena González-Higueras; Luís A Conesa; Carmen Martín-Rodríguez; Francisco J Díaz-Domínguez; Pablo Serna-Grande; Rosana Rivas; José Ferreres; Javier Belda; Lucía Capilla; Alec Tallet; José M Añón; Rosa L Fernández; Jesús M González-Martín Journal: Lancet Respir Med Date: 2020-02-07 Impact factor: 30.700