Abstract
Several months ago, an outbreak of pneumonia of unknown aetiology was detected in Wuhan City (China) and the aetiological agent of the atypical pneumonia was isolated by the Chinese authorities as novel coronavirus (2019‐nCoV or SARS‐CoV‐2). The WHO announced this new disease was to be known as “COVID‐19.” When looking for new antiviral compounds, knowledge of the main viral proteins is fundamental. The major druggable targets of SARS‐CoV‐2 include 3‐chymotrypsin‐like protease (3CLpro), papain‐like protease (PLpro), RNA‐dependent RNA polymerase, and spike (S) protein. Quercetin inhibits 3CLpro and PLpro with a docking binding energy corresponding to −6.25 and −4.62 kcal/mol, respectively. Quercetin has a theoretical, but significant, capability to interfere with SARS‐CoV‐2 replication, with the results showing this to be the fifth best compound out of 18 candidates. On the basis of the clinical COVID‐19 manifestations, the multifaceted aspect of quercetin as both antiinflammatory and thrombin‐inhibitory actions, should be taken into consideration.
Keywords: COVID‐19, infectious diseases, nutraceutical, quercetin, SARS‐CoV‐2
Abbreviations
- ARDS
acute respiratory distress syndrome
- MERS‐CoV
middle east respiratory syndrome coronavirus
- MODS
multiple organ dysfunction syndrome
- SARS‐CoV‐1
severe acute respiratory syndrome coronavirus‐1
- SARS‐CoV‐2
severe acute respiratory syndrome coronavirus‐2
- WHO
World Health Organization
1. INTRODUCTION
Viral diseases continue to pose a serious threat to public health. The world has witnessed several viral epidemics over the past 20 years, including severe acute respiratory syndrome (SARS) coronavirus (SARS‐CoV‐1) in 2003, the influenza disease called H1N1 in 2009, and the middle east respiratory syndrome (MERS) coronavirus (MERS‐CoV) in 2012. Several months ago, an outbreak of pneumonia of unknown aetiology was detected in Wuhan City, Province of Hubei (China) and reported to the China Country Office of the World Health Organization (WHO) on December 31, 2019. The National Health Commission of China reported the outbreak was associated with exposure in one seafood market in Wuhan City. The aetiological agent of the atypical pneumonia was isolated on January 7, 2020 by the Chinese authorities as novel coronavirus (2019‐nCoV). The date of January 22, 2020 is important as it is thought to be when the virus appeared in Europe. The virus was isolated in Bavaria (Germany) from a German patient infected by an individual from Shanghai (China). Subsequently, the virus was present in Italy on January 25, 2020. The unsuspecting individuals infected with the virus are thought to have been able to circulate in the area of Basso Lodigiano with few symptoms or with symptoms mistaken for those of influenza.
On January 30, 2020, the WHO declared the situation a public health emergency of international concern (World Health Organization, 2020a) and on February 11, 2020, the WHO announced that the disease caused by this new virus was to be known as “COVID‐19,” which is an acronym of “coronavirus disease‐2019.”
On February 20, 2020, the first symptomatic COVID‐19 patient was identified in Italy at the Emergency Department of Codogno Hospital, Basso Lodigiano, Province of Lodi.
On February 26, 2020, the Director‐General of the WHO announced that the number of new cases of the viral disease, now officially known as COVID‐19, reported outside China since the day before had for the first time exceeded the number of new cases in China (World Health Organization, 2020b). On March 11, 2020, the WHO declared this viral disease to be a pandemic.
2. AETIOLOGY
Coronaviruses constitute a large family of viruses. They are single‐stranded RNA viruses, with a crown‐like appearance under an electron microscope.
Coronaviruses were identified in the mid‐1960s and are known to infect humans and certain animals (including birds and mammals). The primary target cells are the epithelial cells of the respiratory and gastrointestinal tracts.
SARS‐CoV‐2 is a single‐stranded, positive‐sense RNA virus, having a diameter of 60–140 nm with a round or elliptic shape; however, it often exists in a pleomorphic state. Its RNA genome contains 29,891 nucleotides, encoding 9,860 amino acids, and shares 99.9% sequence identity compared to bat genome (bat‐SL‐CoVZC45), suggesting a very recent host shift into humans. Like other CoVs, it is sensitive to ultraviolet rays and heat. In addition, these viruses can be effectively inactivated by lipid solvents including chloroform, ether (75%), ethanol, peroxyacetic acid, and chlorine‐containing disinfectant. Chlorhexidine does not inactivate this virus (Chan et al., 2013; Chen et al., 2020).
3. TRANSMISSION
The new CoV, SARS‐CoV‐2, is a respiratory virus that spreads mainly through contact with the breath droplets of infected individuals, for example, through: (a) saliva, coughing, and sneezing; (b) direct personal contact; (c) hands, for example, by touching the mouth, nose, or eyes with contaminated (unwashed) hands. SARS‐CoV‐2 then uses the angiotensin‐converting enzyme II (ACE2) receptor expressed by human cells to attach to these, as with SARS‐CoV‐1 (Li et al., 2020). Studies have shown the virus survives on different surfaces for days and remains viable in aerosols for hours (van Doremalen et al., 2020). It is possible that transmission occurs via the faecal–oral route. Transmission of the virus from asymptomatic patients has been reported, with a high viral load in pharyngeal samples from minimally symptomatic patients during the initial period of the disease. This is different to what is seen with SARS and MERS, where infectivity peaks relatively later during symptomatic infection, and may account for the much greater spread of COVID‐19. However, the highest transmission rates have been reported to correlate with disease severity and are particularly pronounced in hospital settings, just as for SARS and MERS. The incubation period is thought to vary from 3 to 14 days, while onset of symptoms has been reported up to 14 days after exposure (Lauer et al., 2020) providing the basis for the length of quarantine/self‐isolation. A possible scenario resulting from this could therefore be potential transmission before the onset of symptoms: in fact, many cases were, unfortunately, isolated after the onset of symptoms (He et al., 2020).
4. CLINICAL PATTERNS
The symptoms that patients with COVID‐19 may exhibit are variable. Generally, patients are characterised by three main symptoms: (a) fever, (b) dry cough, and (c) dyspnoea.
We can classify the infection as symptomatic or asymptomatic. In addition, there are prodromal signs such as conjunctivitis (often the first sign) or gastrointestinal symptoms such as nausea, vomiting, abdominal pain, and diarrhoea.
Some patients may present without fever, but with abdominal pain, anorexia, and dyspnoea. Less frequently occurring, but particularly typical of this new pathology, are anosmia and dysgeusia, often accompanied by gastrointestinal symptoms (Huang et al., 2020).
Negative prognostic epidemiological risk factors are older age, male sex, and smoking and poor prognostic clinical risk factors include associated comorbidities such as obesity, hypertension, diabetes mellitus, cardiovascular disease, chronic kidney disease, as well as—of course—respiratory diseases. The greater the number of risk factors and associated pathologies, the higher the risk of a poor prognosis (Chen et al., 2020). A mild symptomatology can resolve itself even without particular medical treatment at home or, instead, it can progress towards pneumonia (bilateral interstitial pneumonia) and respiratory failure, thereby requiring hospitalisation of the patient. Patients can progress rapidly towards acute respiratory distress syndrome (ARDS) with multiple organ dysfunction syndrome (MODS) and death (Wang et al., 2020).
5. THERAPY
Currently, COVID‐19 therapy is only supportive and prevention is the only way to reduce transmission and limit spread. From a pharmacological perspective, initial treatment with lopinavir/ritonavir and with chloroquine was attempted. Due to a lack of chloroquine, hydroxychloroquine was then used (Dong, Hu, & Gao, 2020).
In addition, a number of antibiotics have been used, such as ceftriaxone with azithromycin or piperacillin/tazobactam and doxycycline, and then back to azithromycin alone.
From mid‐March 2020, lopinavir/ritonavir was replaced with remdesivir and the use of tocilizumab, and immediately after, heparin was suggested as a potential treatment. It was then proposed that glucocorticoids could be beneficial in the early stages of the disease; these had also been used in China, but there is currently some disagreement regarding their efficacy (Zhang et al., 2020).
Currently, the use of plasma with antibodies obtained from patients who have had COVID‐19 seems to have a good rationale, although the initial data from a limited number of patients are not encouraging (Zeng et al., 2020).
6. THE FLAVONOID QUERCETIN
Quercetin (Figure 1), chemical name 2‐(3,4‐dihydroxyphenyl)‐3,5,7‐trihydroxychromen‐4‐one or 3,3′,4′,5,7‐pentahydroxyflavone, is classified as a flavonol, one of the six subcategories of flavonoid compounds, and is the major polyphenolic flavonoid found in various vegetables and fruits, such as berries, lovage, capers, cilantro, dill, apples, and onions (Anand, Arulmoli, & Parasuraman, 2016). It is yellow in colour and completely soluble in lipids and alcohol, insoluble in cold water, and sparingly soluble in hot water. “Quercetin” derives from the Latin word “quercetum,” meaning “oak forest,” and as a flavonol, is not produced in the human body (Lakhanpal & Rai, 2007). Quercetin is one of the most important plant molecules, showing pharmacological activity such as antiviral, anti‐atopic, pro‐metabolic, and antiinflammatory effects. It has also been demonstrated to have a wide range of anticancer properties, and several reports indicate its efficacy as a cancer‐preventing agent. Quercetin also has psychostimulant properties and has been documented to prevent platelet aggregation, capillary permeability, lipid peroxidation, and to enhance mitochondrial biogenesis (Aguirre, Arias, Macarulla, Gracia, & Portillo, 2011; Dabeek & Marra, 2019).
7. QUERCETIN AND MOLECULAR DOCKING
Recently, in order to find new candidates expressing potential activity against SARS‐CoV‐2 viral targets, a number of studies reporting the use of computer modelling for screening purposes have been published (Liu & Zhou, 2005; Lung et al., 2020; Toney, Navas‐Martín, Weiss, & Koeller, 2004; Wang et al., 2007; Zhang et al., 2020). Typically, these models determine the free energy of binding between a ligand and a receptor (Forli et al., 2016). A lower binding free energy indicates a stronger ligand–receptor interaction. Although obtaining comparable results via different modelling approaches can be a challenge (Aldeghi, Heifetz, Bodkin, Knapp, & Biggin, 2016), computer‐based molecular docking allows visualisation of the relative binding affinity of thousands of molecules for the above‐listed viral receptors.
In addition to the speed and versatility of this method for rapidly finding a potent inhibitor of SARS‐CoV‐2, another advantage of molecular docking screening is the reduction of the high costs associated with physically screening the activity of large banks of natural substances (Chen, de Bruyn, & Kirchmair, 2017). Compounds that through this method demonstrate significant interaction with viral receptors can then be moved onto cell‐based assays to verify effectiveness and toxicity. Confirmatory results can then accelerate testing in animals and clinical trials.
Recently, the virtual screening (Lung et al., 2020) of 83 compounds commonly used in Chinese traditional medicine for activity against the RNA‐dependent RNA polymerase of SARS‐CoV‐2 identified the aflavin, an antioxidant polyphenol, as a potential inhibitor. Similarly, virtual screening of 115 compounds used within Chinese traditional medicine highlighted 13 for further studies (Zhang et al., 2020). Some of these were naturally occurring polyphenolic compounds such as quercetin and kaempferol, which have already received considerable attention for the treatment of other disease types (Cassidy et al., 2020; Khan et al., 2019; Tomé‐Carneiro & Visioli, 2016). In particular, the study showed a significant inhibition by quercetin of 3CLpro and PLpro with a docking binding energy corresponding to −6.25 and −4.62 kcal/mol, respectively (Zhang et al., 2020).
Moreover, Smith and Smith (2020) demonstrated for quercetin a theoretical, but significant, capability to interfere with SARS‐CoV‐2 replication, with the results showing this to be the fifth best compound out of 18 candidates. In fact, a reasonable target for structure‐based drug discovery was identified to be the disruption of the viral S protein‐ACE2 receptor interface (Figure 2). Once again, a computational docking model was used to identify small molecules that were able to bind to either the isolated viral S protein at its host receptor binding region or to the S protein–human ACE2 receptor interface, to potentially limit viral recognition of host cells and/or to disrupt host–virus interactions. Among the natural compounds tested, quercetin was identified as being between the top scoring ligands for the S protein:ACE2 receptor interface, further confirming its role as a promising antiviral agent that should be further investigated.
An in vitro molecular docking study was also performed to analyse the probability of molecular docking between quercetin and viral protease. Proteases play essential roles in viral replication, and specifically, 6LU7 was determined to be the main protease (Mpro) found in SARS‐CoV‐2. Quercetin formed H‐bonds with the 6LU7 amino acids His164, Glu166, Asp187, Gln192, and Thr190, with all of the H‐bonds interacting with amino acids in the virus Mpro active site (Khaerunnisa, Kurniawan, Awaluddin, Suhartati, & Soetjipto, 2020). The genome of SARS‐CoV‐2 is approximately 79% identical to that of SARS‐CoV‐1 (Hui et al., 2020). It is therefore not surprising that quercetin showed an IC50 of 8.6 ± 3.2 μM against SARS‐CoV‐1 PLpro (Park et al., 2017).
Nevertheless, 3 years have passed since this evidence was obtained, and unfortunately, no cell‐based assay of antiviral activity has been performed. Very recently, quercetin was reported to have antiviral activity with respect to SARS‐CoV‐1 by inhibiting also 3CLpro (Jo, Kim, Shin, & Kim, 2020).
8. MULTIFACETED QUERCETIN AND ITS CLINICAL RELEVANCE
On the basis of the results obtained by computational methods on molecular docking, it is anticipated that quercetin could have an effect on SARS‐CoV‐2 by interacting with 3CLpro, PLpro, and/or S protein. In addition to these targets, other findings could prompt us to consider quercetin as being endowed with a general, that is, not specific only for CoV, antiviral role (Chiow, Phoon, Putti, Tan, & Chow, 2016; Fanunza et al., 2020; Jo, Kim, Kim, Shin, & Kim, 2019; Mani et al., 2020; Nguyen et al., 2012; Park, Yoon, Kim, Lee, & Chong, 2012; Song, Shim, & Choi, 2011). In any case, based on the strong inflammatory cascade and the blood clotting phenomena triggered during SARS‐CoV‐2 infection, the multifaceted aspect of quercetin, which has been well described as exerting both antiinflammatory (quercetin dose‐dependently decreases the mRNA and protein levels of ICAM‐1, IL‐6, IL‐8, and MCP‐1) and thrombin‐inhibitory actions (Chen et al., 2011; Cheng, Huang, Pang, Wu, & Cheng, 2019; Liu et al., 2010), should be taken into consideration.
To date, a considerable amount of data has been accumulated describing the potential antiviral role (among others) of quercetin (Table 1). Indeed, several studies, using computational models and in vitro and in vivo assays, would seem to confirm this. At the present time, however, the critical lack of high‐quality clinical data must be highlighted, although some empirical and/or case–control clinical evaluations would appear encouraging. A randomised study performed a decade ago enrolled 1,002 adult subjects affected by viral infections of the upper respiratory tract; this showed that quercetin administered at very high dosages (1,000 mg/dose) for 12 weeks reduced the days of illness in middle‐aged and elderly subjects (Heinz et al., 2010). More recently, an empirical study conducted at a Wuhan hospital showed that an approach where, in addition to conventional therapies, patients were treated with traditional Chinese medicine remedies, including herbs with a high quercetin content, was medically safe, free from particular side effects additional to those obtained with the conventional approach alone, and was able to improve the symptoms of patients with COVID‐19 (Luo et al., 2020); (Table 1).
TABLE 1.
Author | Year | Duration | Botanical compound | Species | Parameters | Results |
---|---|---|---|---|---|---|
Chen et al. | 2011 | 48 hr | Houttuynia cordata Thunb., a plant containing flavonoids like quercetin, quercitrin, and isoquercitrin | Vero cells | The effect on HSV‐2 infection was determined by measuring cell viability using MTT assay | Quercetin, quercitrin, or isoquercitrin at 10 μM showed significant activity against HSV‐2 infection through inhibition of NF‐κB activation, while naringenin, a dihydroflavonoid from grape fruit showed no effect against HSV‐2 infection, indicating that the flavonoids are responsible for anti‐HSV‐2 activity in hot water extract of Houttuynia cordata |
Cheng et al. | 2019 | Quercetin at various concentrations (2.5–20 μM) | ARPE‐19 cells | Quercetin effects on interleukin‐1β (IL‐1β)‐induced production of inflammatory cytokines and chemokines in ARPE‐19 cells | Quercetin could dose‐dependently decrease the mRNA and protein levels of ICAM‐1, IL‐6, IL‐8, and monocyte chemoattractant protein‐1 (MCP‐1). It also attenuated the adherence of the human monocytic leukaemia cell line THP‐1 to IL‐1β‐stimulated ARPE‐19 cells | |
Fanunza et al. | 2020 | A small set of flavonoids including quercetin and wogonin | Quercetin and wogonin can suppress the VP24 effect on IFN‐I signalling inhibition. Quercetin showed a half‐maximal inhibitory concentration (IC50) of 7.4 μM, and it was characterised to significantly restore the IFN‐I signalling cascade, blocked by VP24, by directly interfering with the VP24 binding to karyopherin‐α and thus restoring P‐STAT1 nuclear transport and IFN gene transcription. Quercetin significantly blocked viral infection, specifically targeting EBOV VP24 anti‐IFN‐I function | |||
Heinz et al. | 2010 | 12 weeks | Two quercetin doses (500 and 1,000 mg/day) | 1,002 subjects | Upper respiratory tract infection rates | For all subjects combined, quercetin supplementation over 12 weeks had no significant influence on upper respiratory tract infection rates or symptomatology compared to placebo. A reduction in upper respiratory tract infection total sick days and severity was noted in middle aged and older subjects ingesting 1,000 mg quercetin/day for 12 weeks who rated themselves as physically fit |
Luo et al. | 2020 | 8.96 days | Herbs with a high quercetin content | 54 patients with novel coronavirus pneumonia | Hemogram, days of hospitalisation | The clinical results of our study showed that 54 patients with novel coronavirus pneumonia enhanced immune ability against COVID‐19 by detecting blood samples after traditional Chinese medicine treatment and category of invigorating spleen and removing dampness appears to shorten patients' hospitalisation day |
9. CONCLUSION
In the recent past, there have been several pandemics. Within the context of globalisation, some of these pandemics have truly raised the global risk to humankind. The COVID‐19 pandemic is the latest of these and is, so far, completely unresolved. In the meantime, as we await the development of an effective vaccine, researchers worldwide must focus all their efforts on selecting possible effective treatments, bearing in mind that the plant kingdom supplies chemical skeletons that, since ancient times, have provided humans with “drugs.” As a recent example, we remember the anti‐malarial drug artemisinin obtained from Artemisia annua, the studies on which resulted in 2015 in a Nobel Prize being awarded to the researcher Tu Youyou (Mikić, 2015).
Although a repeat of the artemisinin success story may be unlikely, the volume of data that recommends quercetin as a potential molecule candidate for an anti‐COVID‐19 role strongly supports the execution of a case–control clinical study with the aim of realising its possible efficacy within the context of this disease. On the basis of its poor pharmacokinetics profile, any galenic formulation aimed to improve its rate of absorption should be considered important. At our knowledge, the Phytosome form of quercetin could be a possible candidate.
CONFLICT OF INTEREST
The authors have no relevant affiliations or financial involvement with any organisation or entity with a financial interest in or financial conflict with the subject matter or materials discussed in the manuscript. This includes employment, consultancies, honoraria, stock ownership or options, expert testimony, grants or patents received or pending, or royalties. No writing assistance was utilised in the production of this manuscript.
AUTHOR CONTRIBUTIONS
All authors equally contributed in writing the manuscript.
Derosa G, Maffioli P, D'Angelo A, Di Pierro F. A role for quercetin in coronavirus disease 2019 (COVID‐19). Phytotherapy Research. 2021;35:1230–1236. 10.1002/ptr.6887
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