key: cord-0800221-x67ovc0q authors: Lukan, Norbert title: “Cytokine storm”, not only in COVID-19 patients. Mini-review date: 2020-09-29 journal: Immunol Lett DOI: 10.1016/j.imlet.2020.09.007 sha: 9fa7e71b1eefd195214cd845953092e8c81344ac doc_id: 800221 cord_uid: x67ovc0q Cytokine storm is a form of uncontrolled systemic inflammatory reaction activated by a variety of factors and leading to a harmful homeostatic process, even to patient´s death. Triggers that start the reaction are infection, systemic diseases and rarely anaphylaxis. Cytokine storm is frequently mentioned in connection to medical interventions such as transplantation or administration of drugs. Presented mini-review would like to show current possibilities how to fight or even stop such a life-threatening, immune-mediated process in order to save lives, not only in COVID-19 patients. Early identification of rising state and multilevel course of treatment is imperative. The most widely used molecule for systemic treatment remains tocilizumab. Except for anti-IL-6 treatment, contemporary research opens the possibilities for combination of pharmaceutical, non-pharmaceutical and adjunctive treatment in a successful fight with consequences of cytokine storm. Further work is needed to discover the exact signaling pathways that lead to cytokine storm and to determine how these effector molecules and/or combination of processes can help to resolve this frequently fatal episode of inflammation. It is a huge need for all scientists and clinicians to establish a physiological rational for new therapeutic targets that might lead to more personalized medicine approaches. Although to date, "cytokine storm" is mainly connected to COVID-19, many hypothesis concerning treatment modalities have been rising in the last fifteen years. It seems to be important to put together knowledge about known immunological mechanisms and the contemporary medicaments (except for antimicrobial drugs without immunomodulatory effect) which are potent to modulate immunologic answer even to fight against such a harmful process. A recent PubMed search for cytokine storm or cytokine release syndrome yielded 1102 and 1817 hits respectively; over 100 articles/year were within the past five years. Cytokine release syndrome (CRS) or "cytokine storm" is a form of uncontrolled systemic inflammatory reaction that can be triggered by a variety of factors. It starts fairly quickly in cases of severe (mainly respiratory) infections, in other types of massive immune activation such as severe courses of some systemic diseases (RA, SLE), rarely anaphylaxis. It can be frequently mentioned in connection to medical interventions such as transplantation [1] or administration of certain drugs (monoclonal antibodies, adoptive T-cell therapies) [2] . Subtle CRS may occur following immunization against rubella, human papillomavirus, or hepatitis B [3] . The term "cytokine release syndrome" appeared in the early '90s, when the anti-T-cell antibody muromonab-CD3 was introduced as an immunosuppressive treatment for solid organ transplantation [4] . Yet, Vegh et al. as early as in 1975 observed that by administering polyclonal antibodies the possibility of systemic anaphylactic reactions and other side effects may be present [5] . Presumably they supposed a cytokine-storm like reaction which has different phenotypes from the classical type-I or complement-mediated reaction. At that time such biomarkers as tryptase, IL-6, bradykinin etc. were not known or were on the early stages of immunological research [6] . Except for anti-thymocyte globulin [7, 8] , CRS has been described after administration of several antibody-based therapies such as rituximab [9] , alemtuzumab [10] , muromomab [4] , theralizumab [11] , nivolumab [12] , obinutuzumab [13] , brentuximab [14] . Anticancer non-protein-based treatment with oxaliplatin [15] and IMiDs (lenalidomide) [16] can activate cytokine storm as well. Furthermore, CRS was reported in stem cell transplantation and graft-versus-host disease. As mentioned above, cytokine storm is also a proposed pathomechanism of severe viral infections due to massive T cell stimulation. It is supposed to be combined with all influenza epidemics since Spanish flu in 1919 through dengue, Ebola to corona virus infection in 2020 [17] . CRS has been observed also in surgical patients with severe bacterial infections or in patients with inhalatory injury [18] . Such broad spectrum of etiological factors leading to clinical and laboratory manifestation of CRS like hypotension, hypoxia, fever, fatigue, myalgias, malaise, nausea, hypoxia, coagulopathy, capillary leakage, tachycardia, tachypnea, hemophagocytic lymphohistiocytosis/macrophage activation syndrome, organ toxicity, pulmonary edema, pneumonitis, and renal insufficiency support the basic scientific postulate: cytokine storm results from excessive pro-inflammatory stimuli, inadequate regulation of inflammation, immune cells or both [19] . Not only pro-inflammatory cytokines, but also anti-inflammatory cytokines appear in circulating blood, such as IL-10 and transforming growth factorbeta (TGF-beta). Cytokines work in counterbalance mode, as demonstrated on typical example: products of the Th2 immune response suppress the Th1 immune response and vice versa [20] . In a case of robust activation of immune balance, without the ability to resolve the inflammation, the collateral damage to surrounding cells can be catastrophic, resulting in septic shock, multiple organ dysfunction, immunosuppression and even death [21] . If the inflammatory response is properly regulated, regulatory mechanisms prevent the body from being damaged by systemic inflammation caused by sudden activation of cytokine release. Such inflammation can be resolved effectively, with little or no long-term damage to the host [22] . If CRS is primarily caused by environmental case, there is a strong request to allow restoration of homeostasis. Offending microbe, allergen, or cytotoxic agent when possible, should be eliminated. Antimicrobial treatment is indicated in any form of cytokine storm if contributing pathogen is suspected. Even though simultaneous antimicrobial treatment is not the topic of presented contribution, many of contemporary molecules have, except for their antimicrobial potency, also antiinflammatory and immunomodulatory effect. Canna and Behrens [19] propose a conceptual model of various cytokine release syndromes based on the nature of mechanisms of inflammation. Careful assessment of host and environmental factors strengthen the idea of rational therapeutic approach. In a case of host dependent mechanism of inflammation, they emphasize the use of cytotoxic agents while in a case of environmentally induced inflammation (infection) antimicrobials are predominately indicated. Data about cytokine storm in human anaphylaxis or other severe allergic (drug) reactions are scarce [23] . Even if all forms of cytokine release syndrome induced by environmental or host factors arrive at their final common pathway, the critical point is to understand and specify the exact mechanism directing more precise mode of treatment. The clinical picture of cytokine storm slightly varies in its several forms, but generally manifests as "overlap syndrome" laboratory manifesting in decreasing cell counts, decreasing ESR, increased ferritin level, NK dysfunction, and hemophagocytosis [19] . Although the primary cause of CRS is crucial to understand for restoring immunologic balance, the main focus in treatment should be directed towards final common pathway. At that level, influence on all pro-inflammatory and anti-inflammatory humoral and/or cellular compounds might have been considered. When activating intense inflammatory pathways through immune cells, endothelium, bone marrow, liver and kidney, a vicious circle of harmful processes can lead to death. Immunopathology could also be associated with extensive microthrombosis mostly in lungs, thus ischemic/reperfusion injury contributes to broadening of immune mediated inflammation [24] . Therefore, multilevel treatment opportunities should be a challenge ( Figure 1 ). Clinical picture of CRS or cytokine storm strikes suddenly and the main goal, after starting intensive care treatment and targeting the elimination environmental trigger (if possible), is to administer potential drugs capable of controlling cytokine production and its harmful effect. Excessive cytokine production by immunomodulatory drugs has its place on top of contemporary research. From web portal "ClinicalTrials.gov" 27 studies under key words cytokine release syndrome and 32 studies under cytokine storm were analyzed (last accessed 26 August 2020). Out of those trials, not all deal with immunomodulators. Studies involved in the text are summarized in Table 1 . Three studies are completed, two of them have already been published [25, 26] . Seven of these studies are focused on using haemoadsorbtion in CRS management caused by SARS-CoV-2 (NCT04324528, NCT04385771) in severe burns (NCT04195126), septic shock (NCT02288975), cardiac arrest (NCT03685383) and after CAR-T cell therapy (NCT04048434). Haemoadsorbtion can lead to a reduction of the circulating pro-and anti-inflammatory cytokines and thus improve the course of the disease and the outcome of patients. One of them (NCT03974386) recruits patients with sepsis to establish influence of environmentally induced inflammation caused by gram-negative bacterial endotoxin as the main trigger for systemic inflammatory reaction. Endotoxin binds to Toll-like receptor 4 (TLR4) and so induces a cytokine storm. The amount of endotoxin is associated with shock, insufficient intestinal perfusion, and poor prognosis. Therefore, haemoadsorbtion can antagonize the action of endotoxin reducing the cytokine storm and inflammatory response to improve the prognosis of sepsis. One study (NCT04327505) is focused on efficacy of hyperbaric oxygen which significantly reduces inflammatory cytokines. It is expected to be effective in the treatment of cytokine storm in viral J o u r n a l P r e -p r o o f infections (SARS-CoV-2). It is possible to suppose that a clinical effect of hyperbaric oxygen is caused by immunological factors. The effect on monocytes may be the basis for reduced levels of circulating proinflammatory cytokines under stress conditions [27] . Apparently, hyperbaric oxygen could influence inflammation following environmental triggers (injury, sepsis) [28] , but its effects on increased morbidity and mortality associated with aberrant inflammatory responses are largely unknown. Additional research is needed to estimate the effect of such treatment. Although immuno-modulatory therapy is not routinely recommended, majority of clinical trials on CRS are focused on direct influencing highly elevated pro-inflammatory cytokines (interleukin IL-1, IL-2, IL-6, IL-7, IL-10, IL-18, TNF-α, indirectly by modulation of INF-γ production or by interfering NF-κB through JAK inhibitors. If possible, it is critical to intervene prior to the initiation of CRS and severe respiratory distress mainly in patients at high risk of worsening. To increase the chances of survival of such patients, the compassionate use of available drugs is required, based on literature data and current experience of many clinicians. Patients with cytokine release syndrome secondary to viral etiology, show increased production of pro-inflammatory cytokines similar to that found in patients who develop CRS secondary to CAR-T cell therapy [29, 30] . The most common clinically used group of biological drugs are TNF-α blockers, but their role in treatment of cytokine storm remains unclear. Although TNF-α inhibiting agents have been reported to be effective in cytokine dysbalance, other report worsening during treatment with TNF-α inhibiting agents, the published results have been conflicting [31] . Tocilizumab remains the most commonly used therapy for systemic treatment of CRS. Multiple studies confirmed the correlation of peak IL-6 levels with the severity of CRS leading to the approval of tocilizumab for treatment of CRS concurrent with the approval of tisagenlecleucel, CAR T-cell therapy in non-Hodgkin lymphomas (DLBCL) [32] . Tocilizumab, IL-6 receptor-targeted monoclonal antibody has been effectively used to treat CRS in several scenarios. Since April 2020, newly opened clinical trial "Efficacy and safety of tocilizumab in the treatment of SARS-Cov-2 related pneumonia (TOSCA)" (NCT04332913) might show a rationale for those patients who develop CRS, blocking the complications caused by high levels of IL-6, and possibly preventing the development of a multi-organ failure. Two other studies recruit patients with the aim to influence CRS in hematopoietic stem cell transplantation (haplo-HSCT) (NCT03533101) and in CAR-T cell therapy pediatric patients with CD19 expressing relapsed and refractory B-cell acute lymphoblastic leukemia (NCT02906371). Other molecule which could manage CRS is siltuximab, a murine chimeric moAb which is an IL-6 antagonist. According to a survey published by special interest group of American Society for Blood and Marrow Transplantation Pharmacy, siltuximab should be considered for cases of tocilizumab-refractory CRS. The liable favour of siltuximab is its direct binding to IL-6 whereas tocilizumab binds to IL-6R which may result in increased IL-6 levels [33]. Perspective pathway in immunomodulatory approaches is to modulate levels of IL-1 by using anakinra or canakinumab. It is well established that an over-expression of interleukin-1 is one of the hallmarks in CRS, probably through activation of nuclear factor transcription and activator protein 1. Environmental trigger binds to TLRs which activate the formation of pro-IL-1 and activation of the inflammasome [34] . Inflammasome activation is important for the regulation of both the innate and adaptive immune mechanisms paving the way for specific immune responses. After the inflammasome activation, IL1-b is subsequently produced, which mediates the inflammation and thus contributes to cytokine storm. Shakoory et al. in 2016 [35] reported that IL-1R blockade with anakinra is associated with higher survival rate of septic patients presenting signs of cytokine storm. The safety and wide therapeutic margin of anakinra and the central role of IL-1 in the cytokine storm merit reconsideration of this therapeutic agent as a potential treatment option for CRS. This cytokine is not consistently elevated in patients with severe CRS [36] , so an aspect of personalized medicine approaches should be considered. Canakinumab is a monoclonal antibody directed against IL-1β [37] . Although canakinumab is an effective treatment in SJIA, it does not appear to have a significant effect on reducing the cytokine storm. IL-18 has a strong pro-inflammatory activity so inhibition of the pro-inflammatory cascade triggered by IL-18 can be a therapeutic target not only for the treatment of inflammatory diseases but also for cytokine storm. Gabay The Janus kinases (JAKs) transduce cytokine-induced signals from specific receptors that bind a broad array of cytokines, including those involved in almost all forms of CRS. Based on their essential roles in transmitting, the JAKs might become a target for pharmacologic manipulation not only in inflammatory diseases (rheumatoid arthritis, ulcerative colitis) and in myeloproliferative disorders (myelofibrosis, polycytaemia vera) but also in the management of cytokine storm. There are several antibody-based TH17 blockades (anti-IL-17, anti-IL-17R and anti-IL-12/23p40) available; however, the antibody-based treatment is expensive and has only a narrow spectrum of effects [39] . Therefore, treatment by JAK inhibitors is tested to restrict the pro-inflammatory function of existing TH17 cells. Treatment with the JAK1/2 inhibitor ruxolitinib significantly reduced the symptoms of disease and prolonged survival time in experimental murine model. Ruxolitinib diminished pro-inflammatory cytokine production, mitigating the cytokine-driven hyperinflammation that occurs in various cytokine release syndromes [40] . This experimental work supports the integration of JAK inhibitors such as ruxolitinib into clinical trials as a novel strategy to counteract pathological cytokine-driven tissue inflammation [41] . Since April 2020, three new, currently recruiting clinical trials are available on ClinicalTrial.gov (accessed 26 August 2020) focusing on treatment COVID-19 associated cytokine storm with ruxolitinib as monotherapy (NCT04362137, NCT04361903, NCT04334044 -see Table 1 ). Except for ruxolitinib, even baricitinib and fedratinib are potent and selective JAK inhibitors approved for indications in rheumatology and hematology. All three are powerful anti-inflammatory drugs that, as JAK-STAT signalling inhibitors, are likely to be effective against the consequences of the elevated levels of cytokines in various forms of CRS, not excluding viral etiology . Although the three candidates have similar JAK inhibitor potencies, Stebbing et al. [42] suggests, due to a high affinity for AAK1, baricitinib as the best of the group, especially given its once-daily oral dosing and acceptable side-effect profile. Two Italian studies (NCT04320277, NCT04358614) are registered for clinical testing of baricitinib and its effect on reduction of cytokine release. The second one is focused on reduction of ICU patient admission with COVID-19 associated moderate pneumonia. The last of three above mentioned JAK2 inhibitors which are used to restrict the proinflammatory function of existing TH17 cells is fedratinib. Fedratinib is approved in U.S. for myeloproliferative neoplasms. Wu and Yang [39] J o u r n a l P r e -p r o o f found that fedratinib treatment decreased in vitro the expression of IL-17 by murine TH-17 cells. He supposed fedratinib suppresses TH-17 associated cytokine pathways (including the effect of IL-6 on cells) and so could prevent the harmful effect of TH17 associated cytokine storm. A recent study has been published (phase I) for itacitinib, selective JAK-1 inhibitor in GVHD [43] . At that stage, no information concerning cytokine release syndrome has been obtained. Solitary trials registered on Clinical trial.gov are focused on adjunctive treatment. One study is being prepared for using immunonutrition (n3-fatty acids and antioxidant vitamins in extraordinary doses) on modulation of cytokine production. Such specific nutrients are capable to modulate the host immune response and ameliorate the cytokine storm (NCT01752348). Two others evaluate the effect of vitamin D on selected cytokines involved in cytokine storm in the Covid-19 (NCT04366908, NCT04476745). Reactive oxygen species may be involved in signal transduction pathways that stimulate production of pro-inflammatory cytokines through the activation of transcription factors (NF-kB). The decrease in oxidative stress by widely used antioxidants (N-acetylysteine and erdosteine) encourages us to use them in the treatment of cytokine storm. N-acetylcysteine (NAC) serves as a prodrug to L-cysteine and L-cysteine is a precursor to the naturally occurring antioxidant molecule -glutathione. NAC, a modified form of the amino acid cysteine inhibits the production of pro-inflammatory molecules (e.g., IL6, CCL5, CXCL8, and CXCL10) in H5N1-infected lung cells and reduces migration of monocyte in experimental model. With its anti-inflammatory effects, it may also be effective for the treatment of cytokine storm induced by severe influenza [44] . Similar encouraging results were observed in experimental model even with erdosteine [45, 46] . However, current clinical evidence indicates the administration of antioxidants has a limited effect on cytokine storm and further clinical studies would still be needed [47] . The study (NCT04458298) with OP-101 (dendrimer N-acetyl-cysteine) actually recruits severe COVID-19 patients with the aim to determine the effect of OP-101 in reducing proinflammatory cytokines. Not far from alleviating effect of previously mentioned antioxidants on CRS in animal models, similar protection on excessive release of pro-inflammatory cytokines by use of sodium cromoglycate was published by Han et al. [48] . Sodium cromoglycate or ketotifen generally used to treat allergic diseases, significantly inhibit degranulation and the acute release of histamine and inflammatory mediators from mast cells. Han observed that sodium cromoglycate protects mice effectively from death after viral infection by alleviating inflammatory injury via its function as an inhibitor of mast cell degranulation. Other experimental study evaluated mast cell degranulation after cromoglycate and ketotifen in rat liver histochemicaly resulting in decreased levels IL-6 and TNF-α [49] . Unclear results come from publications focusing on ameliorationg effect of (hydroxy)chloroquine over cytokine storm in COVID-19 patients [50] . Similar unexplicit results were published by He et al. in metaanalysis upon clinical evidence that even though ulinastatin, a serine protease inhibitor, suppresses proinflammatory cytokine elevation and upregulates the release of anti-inflammatory mediators. Because of the poor quality of the evaluated trials and the small cohorts, their findings should be interpreted cautiously [51] . Even macrolides have long been recognised to modulate immune-and anti-inflammatory actions. They suppress the "cytokine storm" in selected patients, yet the confirmation of their effect in larger series is still awaited [52] . Based on promising results in preclinical models by adjunctive immunomodulatory treatment, novel innovative approaches will emerge. Additional research is clearly needed to fully understand the mechanisms of intensive rise of cytokine storm and search for appropriate treatment options. Some J o u r n a l P r e -p r o o f preclinical studies are encouraging. Decreased production of proinflammatory cytokines Il-6 and Il-1 in cell cultures of human monocytes was observed after incubation with manomycin A, a polyketide antibiotic, with known potent anti-inflammatory and immunomodulatory effect [53] . Indeed, antimicrobials with immunomodulatory effect, such as manumycin A might have potential clinical importance and should be evaluated in further not only experimental studies. Other experimental studies show that PPAR-g agonist (pioglitazone) reduces proinflammatory cytokine production and increases the survival of influenza infected mice by 20-40% [54] . PPAR-g (pioglitazone, rosiglitazone) influence the transcription of the upstream inflammatory genes and so could prevent the cytokine storm in the cases of viral infections thus becoming an attractive target for immunomodulatory therapy [55] . Cytokine release syndrome is a sudden onset of almost life-threatening clinical symptomatology which can occur within diverse external or internal conditions. Early identification of rising state and multilevel course of treatment is imperative. Strictly immunologic approach is necessary mainly when considering immunomodulatory treatment. At present, the most widely used molecule for systemic treatment of CRS remains tocilizumab. Its FDA and EMA approval for the treatment of cytokine storm after CAR-T cell therapy gives us a promise for the future. The only exact knowledge about immunologic processes gives us possibilities for combination of pharmaceutical and nonpharmaceutical and adjunctive treatment in successful fight with consequences of CRS. Further work is needed to cut off the signaling pathways that lead to "cytokine storm" and to determine how these effector molecules can be most effectively targeted to help resolve this frequently fatal episode of inflammation. It is a huge need for all scientists and clinicians to establish a physiological rational for new therapeutic targets and understanding of exact genetics as well as epigenetic factors that might lead to more personalized medicine approaches. The author declares no commercial or financial conflict of interest. Yin and yang of cytokine regulation in solid organ graft rejection and tolerance Intensive Care in Hematological and Oncological Patients (iCHOP) Collaborative Group. 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