Nicolas Hoertel1, Marina Sánchez-Rico2,3, Céline Cougoule4, Erich Gulbins5, Johannes Kornhuber6, Alexander Carpinteiro5,7, Katrin Anne Becker5, Angela M Reiersen8, Eric J Lenze8, David Seftel9, Cédric Lemogne10, Frédéric Limosin2. 1. DMU Psychiatrie et Addictologie, Département de Psychiatrie, Assistance Publique-Hôpitaux de Paris, Hôpital Corentin-Celton,INSERM, Institut de Psychiatrie et Neurosciences de Paris (IPNP), UMR_S1266, Université de Paris, Paris, France. nico.hoertel@yahoo.fr. 2. DMU Psychiatrie et Addictologie, Département de Psychiatrie, Assistance Publique-Hôpitaux de Paris, Hôpital Corentin-Celton,INSERM, Institut de Psychiatrie et Neurosciences de Paris (IPNP), UMR_S1266, Université de Paris, Paris, France. 3. Department of Psychobiology & Behavioural Sciences Methods, Faculty of Psychology, Universidad Complutense de Madrid, Campus de Somosaguas, Pozuelo de Alarcón, Madrid, Spain. 4. Institut de Pharmacologie et de Biologie Structurale, IPBS, Université de Toulouse, Toulouse, France. 5. Institute of Molecular Biology, University Medicine Essen, University of Duisburg-Essen, Essen, Germany. 6. Department of Psychiatry and Psychotherapy, University Hospital, Friedrich-Alexander University of Erlangen-Nuremberg, Erlangen, Germany. 7. Department of Hematology and Stem Cell Transplantation, University Hospital Essen, University of Duisburg-Essen, Essen, Germany. 8. Department of Psychiatry, Washington University in St. Louis School of Medicine, St. Louis, MO, USA. 9. Golden Gate Fields Medical Clinic, Berkeley, CA, USA. 10. Université de Paris, Assistance Publique-Hôpitaux de Paris, Hôpital Hôtel-Dieu, DMU Psychiatrie et Addictologie, Service de Psychiatrie de l'adulte, INSERM, Institut de Psychiatrie et Neurosciences de Paris (IPNP), UMR_S1266, Paris, France.
We read with great interest the correspondence letters of Salles et al. [1] and Stip et al. [2], following our multicenter observational retrospective study that showed a substantial association between antidepressant use and reduced risk of intubation or death in 7230 patients hospitalized for COVID-19 [3]. Salles et al. suggest that combining an antidepressant such as fluoxetine with rimonabant, an inverse agonist of CB1 cannabinoid receptor, may be useful against COVID-19, thanks to the antiviral and anti-inflammatory effects of the former and the potentially complementary anti-inflammatory properties of the later. Stip et al. significantly summarized the growing body of evidence of the potential benefit of different psychotropic medications in COVID-19 and their possible underlying mechanisms. They suggested further elucidation of ways that certain antidepressants may be acting in this indication. These two letters challenge us on the potential mechanisms that may underlie the potential positive effect of certain antidepressants on the course of COVID-19. This knowledge is crucial to help identify the more promising molecules for COVID-19 and help design trials evaluating these molecules.Since the initial release of our results in July, 2020 [4], several important studies have led to a substantially improved understanding of the mechanisms that may underlie the potential positive effect of certain antidepressants.First, molecules such as fluoxetine, fluvoxamine, paroxetine, escitalopram, or amitriptyline are antidepressants that belong to the group of functional inhibitors of acid sphingomyelinase (ASM), called FIASMA [5-7], that also comprises other medications commonly used in clinical practice, such as antihistamine medications (e.g., hydroxyzine, promethazine), calcium channel blockers (e.g., amlodipine, bepridil), and mucolytics (e.g., ambroxol [7]). These pharmacological compounds in vitro and in vivo inhibit ASM, an enzyme that catalyzes the hydrolysis of sphingomyelin into ceramide and phosphorylcholine [5-7]. Preclinical evidence indicates that SARS-CoV-2 activates the ASM/ceramide system, resulting in the formation of ceramide-enriched membrane domains that facilitate viral entry and infection by clustering ACE2, the cellular receptor of SARS-CoV-2 [6, 7]. The inhibition of the ASM/ceramide system by FIASMA antidepressants prevented infection of Vero E6 cells with SARS-CoV-2. Importantly, the reconstitution of ceramides in cells treated with these antidepressants restored the infection [6]. In healthy volunteers, oral administration of a low dose of the FIASMA antidepressant amitriptyline prevented infection of freshly isolated nasal epithelial cells with SARS-CoV-2 spike protein pseudotyped particles within 2 h, which was also restored after the reconstitution of ceramides in these cells [6]. These preclinical data were confirmed by another study that demonstrated an inhibition by fluoxetine of SARS-CoV-2 infection in cultured epithelial cells [8]. The potential benefit of FIASMA treatments among patients hospitalized for severe COVID-19 was recently explored in an observational multicenter retrospective study [9]. Therein, it was reported that taking a FIASMA medication upon hospital admission was associated with substantially reduced likelihood of intubation or death. This association was not specific to one FIASMA class (e.g., FIASMA antidepressants) or medication (e.g., fluoxetine) [9]. A similar significant association was found in another observational multicenter retrospective study conducted in patients with psychiatric disorders and hospitalized for severe COVID-19 [10]. A retrospective observational study also established a positive association between chronic administration of FIASMA and reduced mortality in COVID-19 hospitalized patients that was significant for the FIASMA amlodipine [11]. In a double-blind randomized clinical trial, outpatients treated with the FIASMA antidepressant fluvoxamine compared with placebo had a lower risk of clinical deterioration over 15 days of treatment [12]. The results of a prospective real-world evidence study also support this observation [13]. Finally, plasma markers of ceramide metabolism were found to be associated with respiratory severity and to correlate with inflammation in 49 patients hospitalized for COVID-19 [14]. Taken together, these results show the potentially crucial importance of the ASM/ceramide system as a treatment target in COVID-19, a mechanism likely to be shared by all variants [15]. They also support the continuation of FIASMA medications during SARS-CoV-2 infection [9].Second, anti-inflammatory properties of several antidepressants may have important value in regulating inflammation by inhibiting cytokine production in COVID-19. These anti-inflammatory effects might be explained (i) by the high affinity of certain antidepressants, such as fluvoxamine or fluoxetine, for Sigma-1 receptors [12, 16], which have been shown to restrict the endonuclease activity of an Endoplasmic Reticulum (ER) stress sensor called Inositol-Requiring Enzyme1 and to reduce cytokine expression without inhibiting classical inflammatory pathways, and/or (ii) by the inhibition of ASM in endothelial cells and the immune system [6, 7].Finally, other potential mechanisms include reduction in platelet aggregation, decreased mast cell degranulation, interference with endolysosomal viral trafficking and increased melatonin levels [16].These different but potentially interrelated mechanisms shared by several antidepressants such as fluvoxamine or fluoxetine, might collectively lead to anti-SARS-COV-2 effects while diminishing coagulopathy and cytokine storm consequences, which are known hallmarks of severe COVID-19.Following these preclinical, observational and clinical converging findings, and as stated by Salles et al. [1] and Stip et al. [2], large-scale double-blind placebo-controlled randomized clinical trials of FIASMA antidepressants for COVID-19 at different stages of the disease, either alone or combined with medications that have shown preliminary evidence of potential efficacy and good tolerability, are urgently needed. Fluoxetine and fluvoxamine, which display high in vitro inhibition effect on ASM, showed potential positive effects at usual antidepressant doses, and are easy to use, including high safety margins, good tolerability, widespread availability and low cost, should be considered compelling treatments to prioritize for phase 3 trials against COVID-19 [9].
Authors: Johannes Kornhuber; Philipp Tripal; Martin Reichel; Christiane Mühle; Cosima Rhein; Markus Muehlbacher; Teja W Groemer; Erich Gulbins Journal: Cell Physiol Biochem Date: 2010-05-18
Authors: Eric J Lenze; Caline Mattar; Charles F Zorumski; Angela Stevens; Julie Schweiger; Ginger E Nicol; J Philip Miller; Lei Yang; Michael Yingling; Michael S Avidan; Angela M Reiersen Journal: JAMA Date: 2020-12-08 Impact factor: 56.272
Authors: Alexander Carpinteiro; Michael J Edwards; Markus Hoffmann; Georg Kochs; Barbara Gripp; Sebastian Weigang; Constantin Adams; Elisa Carpinteiro; Anne Gulbins; Simone Keitsch; Carolin Sehl; Matthias Soddemann; Barbara Wilker; Markus Kamler; Thomas Bertsch; Karl S Lang; Sameer Patel; Gregory C Wilson; Silke Walter; Hartmut Hengel; Stefan Pöhlmann; Philipp A Lang; Johannes Kornhuber; Katrin Anne Becker; Syed A Ahmad; Klaus Fassbender; Erich Gulbins Journal: Cell Rep Med Date: 2020-10-29
Authors: Alexander Carpinteiro; Barbara Gripp; Markus Hoffmann; Stefan Pöhlmann; Nicolas Hoertel; Michael J Edwards; Markus Kamler; Johannes Kornhuber; Katrin Anne Becker; Erich Gulbins Journal: J Biol Chem Date: 2021-04-23 Impact factor: 5.157
Authors: Judith Marín-Corral; Jose Rodríguez-Morató; Alex Gomez-Gomez; Sergi Pascual-Guardia; Rosana Muñoz-Bermúdez; Anna Salazar-Degracia; Purificación Pérez-Terán; Marcos I Restrepo; Olha Khymenets; Noemí Haro; Joan Ramon Masclans; Oscar J Pozo Journal: Int J Mol Sci Date: 2021-04-30 Impact factor: 5.923
Authors: Senem Merve Fred; Suvi Kuivanen; Hasan Ugurlu; Plinio Cabrera Casarotto; Lev Levanov; Kalle Saksela; Olli Vapalahti; Eero Castrén Journal: Front Pharmacol Date: 2022-01-19 Impact factor: 5.810
Authors: Nicolas Hoertel; Marina Sánchez-Rico; Pedro de la Muela; Miriam Abellán; Carlos Blanco; Marion Leboyer; Céline Cougoule; Erich Gulbins; Johannes Kornhuber; Alexander Carpinteiro; Katrin Anne Becker; Raphaël Vernet; Nathanaël Beeker; Antoine Neuraz; Jesús M Alvarado; Juan José Herrera-Morueco; Guillaume Airagnes; Cédric Lemogne; Frédéric Limosin Journal: Biol Psychiatry Glob Open Sci Date: 2022-01-04
Authors: Marc De Hert; Victor Mazereel; Marc Stroobants; Livia De Picker; Kristof Van Assche; Johan Detraux Journal: Front Psychiatry Date: 2022-01-13 Impact factor: 4.157
Authors: Steven H Rauchman; Sherri G Mendelson; Courtney Rauchman; Lora J Kasselman; Aaron Pinkhasov; Allison B Reiss Journal: J Clin Med Date: 2021-12-24 Impact factor: 4.241
Authors: Nicolas Hoertel; Marina Sánchez-Rico; Erich Gulbins; Johannes Kornhuber; Alexander Carpinteiro; Miriam Abellán; Pedro de la Muela; Raphaël Vernet; Nathanaël Beeker; Antoine Neuraz; Aude Delcuze; Jesús M Alvarado; Céline Cougoule; Pierre Meneton; Frédéric Limosin Journal: Transl Psychiatry Date: 2022-03-03 Impact factor: 6.222
Authors: N Hoertel; M Sánchez-Rico; E Gulbins; J Kornhuber; R Vernet; N Beeker; A Neuraz; C Blanco; M Olfson; G Airagnes; C Lemogne; J M Alvarado; M Arnaout; C Cougoule; P Meneton; F Limosin Journal: Epidemiol Psychiatr Sci Date: 2022-03-30 Impact factor: 6.892
Authors: Marina Sánchez-Rico; Frédéric Limosin; Raphaël Vernet; Nathanaël Beeker; Antoine Neuraz; Carlos Blanco; Mark Olfson; Cédric Lemogne; Pierre Meneton; Christel Daniel; Nicolas Paris; Alexandre Gramfort; Guillaume Lemaitre; Pedro De La Muela; Elisa Salamanca; Mélodie Bernaux; Ali Bellamine; Anita Burgun; Nicolas Hoertel Journal: J Clin Med Date: 2021-12-15 Impact factor: 4.241