key: cord-0871076-g9bqzm19
authors: Pal, Amit; Squitti, Rosanna; Picozza, Mario; Pawar, Anil; Rongioletti, Mauro; Dutta, Atanu Kumar; Sahoo, Sibasish; Goswami, Kalyan; Sharma, Praveen; Prasad, Rajendra
title: Zinc and COVID-19: Basis of Current Clinical Trials
date: 2020-10-22
journal: Biol Trace Elem Res
DOI: 10.1007/s12011-020-02437-9
sha: 58ad37ccd528e682a9ae77d3889d1016a7e9e66f
doc_id: 871076
cord_uid: g9bqzm19

Coronavirus disease-2019 (COVID-19) pandemic continues to threaten patients, societies, and economic and healthcare systems around the world. Like many other diseases, the host immune system determines the progress of COVID-19 and fatality. Modulation of inflammatory response and cytokine production using immunonutrition is a novel concept that has been applied to other diseases as well. Zinc, one of the anti-inflammatory and antioxidant micronutrient found in food with well-established role in immunity, is currently being used in some clinical trials against COVID-19. This review integrates the contemporary studies of role of zinc in antiviral immunity along with discussing its potential role against COVID-19, and ongoing COVID-19 clinical trials using zinc.

As the whole world is grappling with coronavirus disease-2019 (COVID-19) pandemic caused by the severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2), there is a frantic race for finding treatment regimens based on current knowledge until effective vaccine and ad hoc drugs are developed. Indeed, therapeutic approaches against COVID-19, mostly centered on the management of its immunopathology and/or tailored to directly control viral replication, are for now based on off-label prescription. Several human trials are currently in progress to assess the therapeutic indexes of drugs already approved for other diseases (i.e., drug repurposing), and in combination with dietary supplements like vitamin C, vitamin D, vitamin B 12 , probiotics, and zinc (Zn). Zn is a common theme in both prophylactic and curative COVID-19 clinical studies using nutritional supplements.

Zn, the second most abundant trace metal in the human body after iron, is essential for multiple cellular functions including maintenance of immune health. Notably, "Zn proteome" is estimated to encompass around 3000 proteins [1] including ∼ 750 Zn finger transcription factors, a number of which are deeply implicated in homeostasis and inflammation. Ever since Zn deficiency was demonstrated as a human disease more than 56 years ago, it has been implicated in immune dysfunction, growth retardation, hypogonadism, and cognitive impairment [2, 3] . Importantly, Zn also plays a critical role in antiviral immunity [4, 5] . Readers are referred to specialized reviews on essential role of Zn in human health (including Zn homeostasis and transporters) and other nonviral/viral diseases [5] [6] [7] [8] [9] [10] [11] [12] [13] [14] [15] [16] .

With so many clinical trials going on against the COVID-19 pandemic, there is scientific curiosity about the nature and basis of these trials [17] . In this review, we will discuss the basis of clinical trials using adjunct Zn therapy for COVID-19 through the prism of its indispensable role in antiviral immunity along with briefly discussing immunopathology of COVID-19.

As already shown for SARS and Middle East respiratory syndrome (MERS), the host immune response plays a central role also in the pathology associated to SARS-CoV-2 infection, as the fatalities occurring among COVID-19 patients are often preceded by the so-called cytokine storm, a massive systemic release of proinflammatory cytokines such as interleukin (IL)-1b, IL-6, and tumor necrosis factor-α (TNF-α). These events ultimately contribute to acute respiratory distress syndrome (ARDS) and lead to vascular hyperpermeability, diffuse coagulopathy, multi-organ failure, and eventually death [18, 19] . These cytokines are mainly secreted by innate immune cells such as monocytes, macrophages, and dendritic cells (DC), which are supposed to act mainly in the early phases of infections. However, cytokine storm occurs at late stages of SARS-CoV-2 infection, when the adaptive, instead of the innate immune response, is known to become prominent.

A series of timely coordinated actions are required for an effective immune response against viral infections, and the agenda in which these actions move may be outlined by opposing early/innate versus late/adaptive immune response waves. Firstly, innate immune and infected tissue cells initiate primitive and unspecific reactions in an attempt to restrain viral replication by producing type-I interferons (IFN), IFN-α and IFN-β, and to attract blood cells to the site of infection by producing chemokine and TNF-α, which activates endothelial cells enhancing vascular adhesion and diapedesis of leukocytes, and by secreting other proinflammatory cytokines to activate leukocytes. It is peculiar that, while SARS-CoV-2 replication in permissive cells may be effectively inhibited by exogenously added type-I IFN, endogenous production of IFN-α and IFN-β upon infection is inhibited by proteins encoded by SARS-CoV-related viruses, whereas chemokines and inflammatory cytokines are highly produced contributing to an unbalanced response [20, 21] .

During this first phase of the immune response, DC migrate to lymph nodes and initiate a complex and slower intercellular cascade, ultimately culminating in the expansion and maturation of adaptive, virus-specific T and B lymphocytes. Seroconversion-i.e., the appearance in the blood of antibodies against immunogenic viral proteins-and probably the clonal expansion of virus-specific T cells, occurs in most COVID-19 patients 10 days after symptom onset [22] and severe disease and cytokine storm are associated in time and magnitude with the immunoglobulin response in SARS-CoV-1 [23] and SARS-CoV-2 infection [24, 25] .

Strikingly, a similar cytokine storm is also the most notable side effect of chimeric antigen receptor T (CAR-T) cell therapy, and its severity is forecasted by the extent of tumor burden [26] , leading to the hypothesis that a high antigen (i.e., viral) load at the time of the (late) adaptive immune cell activity against SARS-CoV-2, when antibodies and virus-specific T cells arise, may favor a massive second wave of cytokine release by innate cells in a positive feedback loop. Much effort is now trying to decipher, in the immunotherapy setting, the exact mechanisms pushing this positive feedback from adaptive to innate cells, which may deserve our attention to anticipate plausible pathways to interfere with COVID-19 immunopathology. One line of evidence points to cytokines produced by T cells upon antigenic stimulation, namely to TNF-α [27] and granulocyte-macrophage colony-stimulating factor (GM-CSF) [28] , as triggers of the secondary systemic toxic cytokine release by innate cells. Importantly, these two cytokines are unnecessary (both) or detrimental (GM-CSF) for on-target effects of CAR-T cells [28] , which suggests that they may be dispensable also for the antiviral response to SARS-CoV-2.

There is a clear sex-and age-dependent bias in COVID-19related mortality. Better outcomes in women, for instance, may be the result of a more pronounced IFN-α production by plasmacytoid DC [29] during initial phases of infection. The more effective viral containment operated by such a response could be assumed to lower the antigen load at the onset of the adaptive wave and prevent the cytokine storm. In studies from patients during the 2003 SARS-CoV-1 outbreak, treatment with synthetic type-I IFN in conjunction with steroids has proven useful to ameliorate pneumonia course [30] , and early, in contrast to delayed, type-I IFN treatment rescued mice from death after SARS-CoV-1 infection [31] . On the other hand, aging of the immune system, which is associated to chronic low-level activation of innate cells, also entails a delayed and inflated response upon pathogen encountering [32] . Lastly, with age, adaptive cells become slow in mounting antigen-specific responses to novel pathogens secondary to the loss of the naive B and T cell repertoire due to thymic involution [33] .

Data gleaned from seminal animal model studies have added considerable knowledge about the principal roles of Zn in the immune system. Zn is an essential micronutrient, which plays an important role in the physiology of the immune system by acting as signaling molecule. Zn not only acts as an antiinflammatory agent but also functions as an antioxidant stabilizing membrane [34] . Zn deficiency impinges on survival of immune cells and adversely affects important functions such as phagocytosis, target cell killing, and cytokine production ( Fig. 1) . It is clearly evident from studies on preclinical models that Zn deficiency plays a role in thymus and lymphoid tissue atrophy [35] and declines in the mechanisms of activation of both helper T cell [36] and cytotoxic CD8 + T cell responses [37] . Specifically, Zn deficiency leads to compromised immune system, as evidenced by degeneration of thymus, lymphopenia, and defective lymphocyte responses [3, 5, 34] . Zn deficiency causes immunodeficiency with severe lymphopenia that is characterized in part by a considerable decrease in developing B cell compartments in the bone marrow [3, 38] . Moreover, Zn potentiates IFN-α effect by an order of magnitude [39] which can be used to counteract IFN antagonism by SARS-CoV-2 proteins.

A marked neutrophilia is observed in severe COVID-19 patients [40] . Zn gluconate supplementation is able to reduce airway neutrophil infiltration and TNF-α release by inhibiting NF-kB-dependent transcription of inflammatory genes [41] . The Zn finger CCHC-type containing 3 (ZCCHC3) potentiates TLR3 signaling induced by double-strand RNA [42] , which is produced during intracellular replication of coronaviruses.

In vitro, Zn deficiency induced enhanced IL-6 and IL-1β production, as well as higher expression of intercellular adhesion molecule 1 (ICAM-1), important for leukocytes' extravasation, of CD86, a co-stimulatory molecule involved in T cell activation, and of HLA-DR, a MHC-II molecule, in cultured human monocytic cells [43] . Moreover, aged mice have lower plasma Zn concentration, and this was associated to higher IL-6 and ICAM-1 gene expression in splenocytes [43] . Thus, Zn supplementation may be instrumental to reduce inflammatory cytokines, particularly IL-6 and IL-1β, and at the same time to enhance the protective, though inhibited, type-I IFN response in SARS-CoV-2 infection. Zn deficiency indicates towards the decreased interferon-γ (IFN-γ) production, a major component of Th1 cytokine panel [44] . Since Th1 and Th2 responses are mutually inhibited by the effect of their respective signature cytokines IFN-γ and IL-4, such imbalance between Th1 and Th2 might lead to dysfunctions in cellmediated immune response [34] .

There can be a whole lot of factors for the development of Zn deficiency, whether geographic, socioeconomic, nutritional, or as a result of disease pathologies such as chronic viral infections. Notably, during infection, Zn levels decrease significantly and a person's requirement for Zn may increase with the severity of the infection. Aged individuals, infants, and chronic alcoholics are particularly more susceptible to Zn deficiency, increasing their chances of acquiring lifethreatening viral infections [45] [46] [47] [48] . As Zn is indispensable for a strong immune response, Zn deficiency (persistent hypozincemia [serum Zn < 70 μg/dL]) can considerably dampen innate as well as adaptive antiviral immunity [4, 5] .

There is very scant information available on the role and effect of Zn in SARS and coronavirus disease, even though literature is rapidly increasing [17, 49] . Much of the current knowledge about the use of Zn as an antiviral therapy and immunomodulatory agent has originated from studies done with other viral diseases (Readers are referred to these specialized articles for role of Zn in viral diseases [4, 5] ). Zn is an essential constituent of thymulin hormone, which is involved in maturation and differentiation of T cells in thymus gland. Zn not only plays an important role in IL-2 and IFN-γ production but also stimulates macrophages to produce IL-12. IL-12 activates the natural killer cells and T cytotoxic cells. Both IFN-γ and IL-12 play a crucial role in destruction of various pathogens. Among anti-inflammatory cytokines, only IL-10 production is affected by Zn deficiency, whose enhanced levels adversely affect the functioning of macrophages and Th1 response [50] . The rationale behind the use of Zn in COVID-19 studies aroused from the observation that Zn ions and Zn ionophores, such as pyrithione (PT), have previously been described as potent inhibitors of various RNA viruses [51] . Also, targeting of RNA-dependent RNA polymerase (RdRps) of RNA viruses like SARS-CoV-2 is more suitable for antiviral drug development as RdRp activity is strictly virus-specific and may be blocked without severely affecting key cellular functions. The basis of Zn therapy in coronavirus infection is shown in Fig. 2 . It is known previously that Zn ions are involved in many different cellular processes, proper folding, and activity of various cellular enzymes and transcription factors. On the other hand, Zn 2+ is probably an important cofactor for numerous viral proteins as well. Zn 2+ can serve as intracellular second messenger and may trigger apoptosis or a decrease in protein s y n t h e s i s a t e l e v a t e d c o n c e n t r a t i o n s [ 5 2 -5 4 ] . Metallothioneins, a family of metal-binding proteins, regulate homeostasis of Zn and copper, alleviate heavy metal poisoning, and lessen the superoxide stress. Various evidence indicates that metallothionein expression is increased in response to bacterial and viral infections, and it is anticipated that upregulated biosynthesis of human metallothionein might play a significant role in nutritional immunity at the time of active infection [55] .

In cell culture studies, inhibition of the replication of various RNA viruses was reported using high Zn 2+ concentrations and addition of compounds that stimulate cellular import of Zn 2+ , such as hinokitiol, pyrrolidine dithiocarbamate, and PT as mentioned above (reviewed in) [5] . Around 10 years ago, an in vitro study demonstrated that the Zn ionophore PT in combination with Zn 2+ is a potent inhibitor of the replication of SARS-CoV-1 [51] . In addition, authors also studied the effect of Zn ions on the RdRp of SARS-CoV-1 and demonstrated that Zn 2+ directly inhibited the in vitro activity of RdRp (Fig. 2) . More specifically, Zn 2+ was found to block the SARS-CoV-1 RdRp elongation step along with reduced template binding. Further strengthening their claim, authors also showed that the Zn 2+mediated RdRp inhibition of SARS-CoV-1 could be reversed through the addition of a Zn 2+ chelator [51] .

Recently, Finzi (2020) has reported that treatment of four COVID-19 cases with high dose of zinc salts initiated the reduction of disease symptoms within 24 h after initiation of high dose zinc salt lozenges [56] . As adjuvant therapy, Zn (in appropriate dose) may provide protection through decreasing lung inflammation, enhancing mucociliary clearance, inhibiting the ventilator-induced lung injury, and immunomodulation in COVID-19 patients [49] .

As of 4 August 2020, 22 studies were found after searching for Zn and COVID-19 at the clinical trial website https:// clinicaltrials.gov/ct2/home. However, upon narrowing down the search criteria, 19 studies were clinical trials and the remaining 3 were observational studies (NCT04326725, NCT04407572, NCT04412746). Furthermore, among the remaining 19 studies, one study (NCT04371952 entitled DYNAMIC Study [DoxycYcliNe AMbulatoIre COVID-19]) was based on the fact that doxycycline, a tetracycline antibiotic, is known to chelate Zn from matrix metalloproteinases, which may help in part to inhibit COVID-19 infection by limiting its ability to replicate in the (6), assembly and maturation (7), and finally viral release (8) . Data from in vitro studies has demonstrated two mechanisms by which zinc interferes with these viruses' replication cycle steps that include viral genome transcription for SARS-Cov-1 (5), and viral protein translation and polypeptide processing for CV (6) . However, to date, no studies have shown zinc-mediated inhibition of SARS-CoV-1 or CV entry, receptor binding, uncoating, assembly, and/or viral particle release. CV, coronavirus; RdRp, RNA-dependent RNA polymerase; SARS, severe acute respiratory syndrome coronavirus; Zn, zinc host. There is no intervention of Zn supplementation to the patient, so this study was ruled out for present review. Three m o r e s t u d i e s ( N C T 0 4 4 8 5 1 3 0 , N C T 0 4 4 9 1 9 9 4 , NCT04485169) also did not use zinc in the experimental arm, so similarly left out from the present article.

Among the remaining 15 studies (Table 1) , 4 studies are exclusively using different combinations of dietary supplement including Zn as an intervention against COVID-19 (NCT04351490, NCT04342728, NCT04323228, NCT04468139 at serial nos. 1, 2, 3, and 4 of Table 1 , respectively). None of the four studies is completed yet at the time of writing this review. The NCT04351490 trial is using combination of vitamin D 3 with Zn gluconate with the rationale that these two micronutrients are able to modulate the immune response by reducing the inflammatory storm. Vitamin D, a steroid hormone synthesized from cholesterol, has recently been reported to have anti-fibrotic, anti-inflammatory, and immunomodulatory properties on the basis of various studies done with hepatitis C virus infection. Vitamin D impedes T cell proliferation, expression of IFN-γ, expression of IL-2, and CD8 T lymphocytemediated cytotoxicity [57] .

The NCT04342728 trial is primarily studying whether ascorbic acid and Zn gluconate either alone or in combination can decrease the duration of symptoms in newly diagnosed COVID-19 patients. Ascorbic acid, also known as vitamin C which has potent antioxidant properties, has a very long history (> 45 years) in combating or relieving the symptoms of rhinoviruses or common cold [58] , and having immune booster properties [59] . Interestingly, various in vitro animal and clinical trials have shown that vitamin C may affect susceptibility to lower respiratory tract infections during the 2003 SARS epidemic [59] . Taking a holistic approach, clinical trial NCT04323228 is using an anti-inflammatory and antioxidant oral nutrition supplement against COVID-19 with rationale that n-3 fatty acids, vitamin A, vitamin C, vitamin E, selenium, and Zn in extraordinary doses may modulate the immune system response and improve the cytokine storm-associated COVID-19 (Readers are referred to specialized articles on antioxidant and/or antiviral properties of various nutrients [4] ).

Four clinical studies (NCT04377646, NCT04335084, NCT04384458, NCT04446104 at serial nos. 5, 6, 7, and 8 in Table 1 , respectively) are preventive studies, which are studying whether hydroxychloroquine and/or vitamin supplements in combination with Zn are effective as a prophylaxis for asymptomatic healthcare workers/general public. Hydroxychloroquine, derivative of chloroquine having antiinflammatory, immunosuppressive, and anti-autophagy activities, is an anti-malarial drug and anti-rheumatologic agent. Besides, both hydroxychloroquine and chloroquine constrain pH-dependent steps of SARS-CoV-2 replication by increasing pH in intracellular vesicles [60] . Due to these properties, hydroxychloroquine with Zn and/or azithromycin has been touted as the medicine and as a prophylactic drug for COVID-19 [61] [62] [63] . More importantly, chloroquine and hydroxychloroquine work as Zn ionophore, thereby increasing the intracellular Zn concentration [64] . This increase of intracellular Zn concentration will in turn may help in the inhibition of RdRp of SARS-CoV-2 (reviewed in) [51, 61] .

The rest of 5 clinical trials (serial nos. 10-15 of Table 1 ) are aimed at finding better treatment option for COVID-19 by using various combinations of antiviral drugs/dietary supplements with Zn. The results of these studies are still awaited. The common denominator among the above mentioned trials is the use of Zn by virtue of its antioxidant, anti-inflammatory, and antiviral properties [4, 5] . Based on its antioxidant properties, Zn can protect against age-associated macular degeneration, induced by oxidative stress [65] . In general, these properties are the therapeutic basis of the indication of Zn for the treatment of wounds, burns, and acne vulgaris. In addition, Zn is very effective in controlling toxic levels of nonceruloplasmin copper in Wilson's disease and other copperrelated diseases [7] . Acting synergistically, various antioxidants and anti-inflammatory nutrients/drugs combined with antiviral drugs may be beneficial at least in alleviating the COVID-19 symptoms or halting the progression to more severe form of COVID-19. For a clear picture, results of these randomized control trials will be eagerly awaited.

The recommended dietary allowance (RDA) for Zn is 11 mg/ day for men and 8 mg/day for women [66] . Zn absorption is influenced by some foods; e.g., animal proteins result in greater Zn absorption, while phytates reduce its absorption (reviewed in [67] ). Zn elimination half-life is in the range of 0.9-1.2 h.

Zn deficiency is far more widespread in population than Zn toxicity (Zn toxicity is very sporadic and occurs very rarely). In comparison to several other metal ions with similar chemical properties, Zn is relatively harmless. Having said that, caution should be practiced against indiscriminate selfmedication and chronic use of Zn supplements without proper medical prescription/monitoring as Zn toxicity has also been reported in the literature [68] [69] [70] . Acute Zn intoxication is a rare event though exposure to high doses leads to toxic effects. However, it is well established that copper deficiency is associated with taking up large doses of supplemental Zn over extended periods of time [71] [72] [73] . In addition, chronic use of Zn as supplements [68] or as a medication [74] can block intestinal absorption of copper [75] . The finely tuned and synchronized systemic homeostasis and efficient regulatory mechanisms keep a check on the cytotoxic doses of exogenous Zn. It is the endogenous Zn that plays a pivotal role in Zn-induced cytotoxic events in single cells. Brain, in particular, is very sensitive to Zn toxicity.

Using Zn as a supplement or treatment adjuvant is a twoedged sword. Large doses of Zn (300 mg/day) over 6 weeks can affect the immune response, impairing lymphocyte, and neutrophil function [76] . On this basis, a concern had arisen that long-term Zn treatment can cause suppression of the immune system. On the similar lines, using excess Zn supplementation as an antiviral therapy can also do harm to the immune system. Maywald et al. have shown in an in vitro study that excess Zn supplementation can in fact reduce the expression of IFN-γ (a key cytokine for T-helper-1 immune reactions) by reducing interferon regulatory factor 1 expression in regulatory T cells [77] . However, it has been shown for elderly persons that zinc supplementation increased interferon-alpha (IFN-α) production by leukocytes in vitro as compared to younger subjects [78] . This observation necessitates the need to continuously monitor the levels of Zn to obtain maximum therapeutic efficacy. Cellular Zn intake can be improved by ionophores including chloroquine and some of its derivatives such as hydroxychloroquine [64] . Alternatively, natural ionophores of potential use with a good tolerability profile are quercetin and epigallocatechin gallate [79] .

With no slowing down of COVID-19 pandemic as indicated by 18 million confirmed cases including 0.69 million deaths worldwide as of August 4, 2020 (https://covid19.who.int/), researchers are seeking ways in which to potentially protect people from the SARS-CoV-2 or to alleviate its effects once caught. One such means is Zn therapy in addition to other antiviral drugs. Zn is well tolerated and it is best known for its antioxidant, anti-inflammatory, immunomodulatory, and antiviral activities, the latter possibly mediated by its ability to inhibit RNA virus RdRp [51] , thus protecting the body's cells and tissues from viral infection, oxidative damage, and dysfunction. Based on the current knowledge of beneficial and harmful effects of Zn (Fig. 1) , it can be safely concluded that risk to reward ratio is in favor of Zn supplementation in COVID-19. However, the clinical and preclinical data on this aspect is very scanty now and results of current clinical trials employing Zn in COVID-19 can somehow shed more light on the efficacy of Zn against viral infections in vivo. The investigators of the different studies hope to complete the trials in the near future.

Basic and experimental research is still at infancy stage with regard to antiviral mechanisms, clinical benefits, and optimal dose of Zn supplementation as a therapeutic treatment as well as a preventative measure for viral infections including SARS-CoV-2. Generous funding is the need of hour to rigorously pursue this aspect of basic research and provide conclusive evidence to the clinical trials and assumptions based on current knowledge. Although the findings of these trials will be too late for the many thousands of people currently infected with COVID-19, these studies will offer valued data as to the potential alleviation of symptoms by adjunct Zn during future viral/COVID-19 outbreaks and provide platform for future research avenues.

Zinc and the zinc proteome

Clinical and experimental. Zinc metabolism in patients with the syndrome of iron deficiency anemia, hepatosplenomegaly, dwarfism, and hypogonadism

Revisiting the old and learning the new of zinc in immunity

The role of micronutrients in the infection and subsequent response to hepatitis C virus

The role of zinc in antiviral immunity

Zinc: an essential but elusive nutrient

Copper and zinc dysregulation in Alzheimer's disease

Zinc in the physiology and pathology of the CNS

Zinc homeostasis and signaling in health and diseases: zinc signaling

Physiological roles of zinc transporters: molecular and Pal et al. genetic importance in zinc homeostasis

Zinc transporters and signaling in physiology and pathogenesis

The role of zinc, copper, manganese and iron in neurodegenerative diseases

Zinc status and autoimmunity: a systematic review and meta-analysis

Immunological orchestration of zinc homeostasis: the battle between host mechanisms and pathogen defenses

Inflammation, genes and zinc in ageing and agerelated diseases

Insight to physiology and pathology of zinc(II) ions and their actions in breast and prostate carcinoma

Can Zn be a critical element in COVID-19 treatment?

COVID-19: pathogenesis, cytokine storm and therapeutic potential of interferons

The pathogenesis and treatment of the 'cytokine storm' in COVID-19

Imbalanced host response to SARS-CoV-2 drives development of COVID-19

Severe acute respiratory syndrome coronavirus open reading frame (ORF) 3b, ORF 6, and nucleocapsid proteins function as interferon antagonists

Haagmans BL (2020) Severe acute respiratory syndrome coronavirus 2-specific antibody responses in coronavirus disease patients

Anti-SARS-CoV IgG response in relation to disease severity of severe acute respiratory syndrome

Serology characteristics of SARS-CoV-2 infection since exposure and post symptom onset

Viral load dynamics and disease severity in patients infected with SARS-CoV-2 in Zhejiang province

Recent advances in CAR Tcell toxicity: mechanisms, manifestations and management

CD3 bispecific antibody-induced cytokine release is dispensable for cytotoxic T cell activity

GM-CSF inhibition reduces cytokine release syndrome and neuroinflammation but enhances CAR-T cell function in xenografts

The TLR-mediated response of plasmacytoid dendritic cells is positively regulated by estradiol in vivo through cell-intrinsic estrogen receptor α signaling

Interferon alfacon-1 plus corticosteroids in severe acute respiratory syndrome: a preliminary study

Dysregulated type I interferon and inflammatory monocyte-macrophage responses cause lethal pneumonia in SARS-CoV-infected mice. Version 2

Aging and impairment of innate immunity

Contributions of age-related thymic involution to immunosenescence and inflammaging

Zinc: role in immunity, oxidative stress and chronic inflammation

Zinc and immune function: the biological basis of altered resistance to infection

Regeneration of T-cell helper function in zinc-deficient adult mice

Cell-mediated cytotoxicity and tumor growth in zincdeficient mice

Zinc and its role in immunity and inflammation

Zinc potentiates the antiviral action of human IFNalpha tenfold

Dysregulation of immune response in patients with COVID-19 in Wuhan, China

Zinc supplementation alters airway inflammation and airway hyperresponsiveness to a common allergen

ZCCHC3 modulates TLR3-mediated signaling by promoting recruitment of TRIF to TLR3

Zinc deficiency enhanced inflammatory response by increasing immune cell activation and inducing IL6 promoter demethylation

Changes in cytokine production and T cell subpopulations in experimentally induced zinc-deficient humans

Infants and elderlies are susceptible to zinc deficiency

Zinc absorption in alcoholics using zinc-65

Nutritional intake of hazardous drinkers and dependent alcoholics in the UK

A study of zinc metabolism in alcoholic cirrhosis

Zinc and respiratory tract infections: perspectives for COVID19 (Review)

Clinical, immunological, anti-inflammatory and antioxidant roles of zinc

Zn(2+) inhibits coronavirus and arterivirus RNA polymerase activity in vitro and zinc ionophores block the replication of these viruses in cell culture

Zinc inhibits protein synthesis in neurons. Potential role of phosphorylation of translation initiation factor-2alpha

The neurobiology of zinc in health and disease

Role of Zn2+ ions in host-virus interactions

Metallothionein: a potential link in the regulation of zinc in nutritional immunity

Treatment of SARS-CoV-2 with high dose oral zinc salts: a report on four patients

Vitamin D deficiency in hepatitis C virus infection: what is old? what is new?

Vitamin C in the prevention and treatment of the common cold

Vitamin C and SARS coronavirus

Mechanisms of action of hydroxychloroquine and chloroquine: implications for rheumatology

Does zinc supplementation enhance the clinical efficacy of chloroquine/hydroxychloroquine to win today's battle against COVID-19?

Review: hydroxychloroquine and chloroquine for treatment of SARS-CoV-2 (COVID-19). Version 2

Chloroquine is a zinc ionophore

Alzheimer's disease and retinal degeneration: a glimpse at essential trace metals in ocular fluids and tissues

Dietary reference intakes: vitamin A, vitamin K, arsenic, boron, chromium, copper, iodine, iron, manganese, molybdenum, nickel, silicon, vanadium, and zinc

Zinc deficiency

Zinc requirements and the risks and benefits of zinc supplementation

Zinc toxicity

The essential toxin: impact of zinc on human health

Studies on growth, copper metabolism of rats fed high levels of zinc

Inhibitory effect of high dietary zinc on copper absorption in rats

Copper interference with the intestinal absorption of zinc-65 by rats

Maintenance zinc therapy after initial penicillamine chelation to treat symptomatic hepatic Wilson's disease in resource constrained setting

Wilson disease

Excessive intake of zinc impairs immune responses

Zinc supplementation induces CD4+ CD25+Foxp3+ antigenspecific regulatory T cells and suppresses IFN-γ production by upregulation of Foxp3 and KLF-10 and downregulation of IRF-1

Zinc supplementation reconstitutes the production of interferon-alpha by leukocytes from elderly persons

Zinc ionophore activity of quercetin and epigallocatechin-gallate: from Hepa 1-6 cells to a liposome model

Publisher's Note Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations

Acknowledgments The authors duly acknowledge the WHO, NCBI, and NIH for providing free online scientific research articles/information/clinical trials pertaining to COVID-19.

Authors' Contributions All authors contributed to the preparation of this review.

Competing Interests Dr. Rosanna Squitti is the Chief Scientific Officer of IGEA Pharma N.V.; she has some shares in IGEA Pharma N.V. The other authors declare no competing financial interest.