Received: 20 July 2020; Accepted: 10 August 2020; Published: 17 August 2020 ©check for updates
Abstract: The coronavirus disease 2019 (COVID-19) pandemic is a major global threat. With no effective antiviral drugs, the repurposing of many currently available drugs has been considered. One such drug is ivermectin, an FDA-approved antiparasitic agent that has been shown to exhibit antiviral activity against a broad range of viruses. Recent studies have suggested that ivermectin inhibits the replication of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), thus suggesting its potential for use against COVID-19. This review has summarized the evidence derived from docking and modeling analysis, in vitro and in vivo studies, and results from new investigational drug protocols, as well as clinical trials, if available, which will be effective in supporting the prospective use of ivermectin as an alternative treatment for COVID-19.
Keywords: SARS-CoV-2; COVID-19; ivermectin; treatment; antiviral
1.Introduction
In December 2019, the novel coronavirus disease 2019 (COVID-19), caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), emerged in central China [1,2]. As of 30 July 2020, more than 16 million confirmed cases and more than 600,000 deaths have been reported in 188 countries based on the COVID-19 Dashboard database [3]. Most SARS-CoV-2 infections are asymptomatic or result in mild symptoms, such as cough, fatigue, and myalgia [4]; however, up to 20.3% of hospitalized patients require admission to the intensive care unit (ICU) [5]. The data suggest that dysregulation of the host immune response contributes to disease progression and severity [6].
COVID-19 is a global threat to public health and no effective vaccines or pharmaceutical agents against SARS-CoV-2 are available [1,4]. To respond to the pandemic, a long list of potential drugs has been proposed as potential treatments for COVID-19; some of these have been selected for clinical trials in many countries [7,8]. In accordance with the concept of drug repurposing, these prospective drugs, which are either already marketed as antivirals or have been chosen from different pharmacological classes, have been suggested to provide antiviral activity against SARS-CoV-2 infection and/or to improve the pathological symptoms of COVID-19 [7,8]. The drugs span from current antivirals to antiparasitic agents, such as protease inhibitors [9-12], nucleoside analogs [13,14], chloroquine, and hydroxychloroquine [14-17].
Among the drugs repurposed for COVID-19 is ivermectin, an FDA-approved antiparasitic agent with antiviral activity against a broad range of viruses, such as influenza [18], human immunodeficiency virus (HIV) [19], dengue virus [20], West Nile virus [21], and Venezuelan equine encephalitis virus [22]. An initial in vitro study suggested that ivermectin could inhibit SARS-CoV-2 [23]. In this review, we have summarized the evidence from docking and modeling studies, in vitro and in vivo studies, new investigational drug protocols, and, where available, clinical trials; from this evidence, we aim to evaluate the potency of ivermectin for use as a treatment option for COVID-19.
2. Materials and Methods
We searched for relevant articles on PubMed and Google Scholar using the search terms "coronavirus", OR "SARS-CoV", OR "MERS-CoV", OR "SARS-CoV-2" AND "ivermectin" in the title or abstract. Available clinical trials assessing the efficacy of ivermectin were searched for on the ClinicalTrials.gov database. Available publications were discussed based on the study types (in vitro, in vivo, emergency use in hospitals, and clinical trials). All available articles until 10 May 2020were considerate eligible. All studies were discussed narratively. To build our discussion, previous studies assessing the antiviral effect of ivermectin against other viruses and its action mechanisms were also searched and discussed.
3. Ivermectin: An Introduction
Ivermectin is an antiparasitic agent with broad spectrum activity, high efficacy, and a wide safety margin. It has been in common use in veterinary medicine since 1981 for the treatment of onchocerciasis and filariasis [24]. Ivermectin was first used in humans in 1987 for the treatment of onchocerciasis; currently, it is approved in many countries for the treatment of onchocerciasis, filariasis, strongyloidiasis, and scabies [25]. Over the past three decades, approximately 3.7 billion doses of ivermectin have been distributed worldwide through mass drug administration (MDA) campaigns [26].
Ivermectin is available in multiple forms, including tablets, capsules, and an oral solution; however, it is only approved for administration via the oral route for humans. Studies of the metabolism of ivermectin in humans are limited; however, it was suggested that the drug is extensively metabolized in the liver [25]. The elimination half-life of ivermectin is approximately 24 h, although a previous study suggested that the drug persisted for several months after a single dose of ivermectin [27]. Ivermectin is distributed widely throughout the body, owing to its high lipid solubility, and binds strongly to plasma proteins, particularly serum albumin, and is notably excreted in feces [25].
A previous study suggested an antagonistic effect of ivermectin on vitamin K after hematomatous swellings were reported in two out of 28 ivermectin-treated patients, along with a significantly increased prothrombin time of between 1 week and 1 month after drug administration [28]. Notably, even though the reduction of factor II and factor VII levels was reported to occur in most of the patients, bleeding complications were not observed in any patients [28].
Despite being approved as an antiparasitic agent, ivermectin has also been shown to exert antiviral activity against a broad range of viruses in vitro. It was suggested that ivermectin inhibited the action of the integrase of HIV [19] and non-structural protein 5, a polymerase, in dengue virus [20]. In addition, ivermectin exerted inhibitory activities against several RNA viruses, such as West Nile virus [21], Venezuelan equine encephalitis virus (VEEV) [22], and influenza [18]. This antiviral effect was not only demonstrated against RNA viruses, but was also shown to be effective against a DNA virus, pseudorabies virus (PRV), both in vitro and in vivo [29].
Ivermectin binds importin (IMP)a armadillo (ARM) repeat domain, which causes IMPa thermal instability and a-helicity that prevents IMPa-IMP ß 1 interaction [30]. Ivermectin is also able to dissociate the IMPa/ß1 heterodimer, which further inhibits NS5-IMPa interaction within cells [30]. A significant increase in the ratio of free IMPa to IMPa/ß 1 was observed when the IMPa/ß 1 heterodimer was incubated with 12.5 gM ivermectin, suggesting that ivermectin binds IMPa directly to impact the IMPa structure, most likely within the ARM repeat domain [30]. In short, ivermectin affects the IMPa/ß1 recognition of viral and other proteins by preventing its formation or dissociating the heterodimer, which is crucial in the nuclear transport of viral proteins. As the replication cycle of the virus and the inhibition of the host's antiviral response occur in a manner dependent on the nuclear transport of viral proteins, targeting the transport process may be a feasible pharmacological approach for dealing with RNA viral infections [21,30,31]. In PRV, ivermectin inhibited viral entrance into the cell nucleus, as well as viral proliferation, in a dose-dependent manner [29]. The drug significantly reduced viral DNA synthesis, inhibited virus production, and blocked DNA polymerase accessory subunit UL42 entrance into the nucleus by targeting the nuclear localization signal in the transfected cells [29]. Moreover, the administration of ivermectin increased the survival rates of Ross River virus (RRV)-infected mice, most likely by relieving the infection of the infected host [29]. The broad-spectrum antiviral activity of ivermectin is believed to be due to its nuclear inhibitory activity [31,32].
4.Ivermectin and SARS-CoV-2 Infection
There are no antiviral drugs available to treat SARS-CoV-2 infection. However, several clinical trials are in progress to explore the potential antiviral activities of some drugs. Although most of these drugs were initially designed for other pathogens, they appear to have the potential to treat COVID-19, either by acting directly on the virus or modulating the human immune system [30]. One of the drugs with the potential for COVID-19 treatment is ivermectin. This antiparasitic drug has shown potential antiviral activity by inhibiting the nuclear transport of viral proteins [18-22].
Previous studies on SARS-CoV proteins have shown the potential role of IMPa/ß 1 during infection in the signal-dependent nucleocytoplasmic shuttling of the SARS-CoV nucleocapsid protein, which may affect host cell division [21,33]. Moreover, open reading frame (ORF) 6, as the accessory protein of SARS-CoV, has been shown to have an antagonistic effect against the antiviral activity of the STAT1 transcription factor [34]. As ivermectin has shown a potential inhibitory effect on nuclear transport, particularly by preventing IMPa/ß1 binding, it may also act on SARS-CoV-2. As SARS-CoV-2 is very similar to SARS-CoV, it is suggested that ivermectin may also be effective against SARS-CoV-2 by inhibiting its nuclear transport [25]. A proposed schematic figure of the antiviral action of ivermectin against SARS-CoV 2 is depicted in Figure 1.
4.1.In Vitro and 'in Vivo Studies
An in vitro s tudy demonstrated that a single dose of ivermectin was able to limit SARS-CoV-2 replication within 24-48 h, very likely through the inhibition of the IMPaßl-medrnted nuclear import of viral proteins [23]. In that study the levels of "viral RNA released from the mfected cells and cell-assodated viral RINA were significantly reduced by more than 90% and 99%, respectively, tit 24 h post infection. Furthetmore, the treatment of SARS-CoV-2-infected cells with ivermectin for 48 h was shown to result in a dramatic reduction of viral RNA (by -5000-fold) compared with the control group. However, no farther reduction in viral RNA was obierved at 72 It [23]. Lastly, the study suggested that no toxicity of ivermectin was observed in either group at any time point, which agreed with previous studies [19,20,22]. There was no clear explanation of how ivermectin achieved its antiviral properties against SARS-CoV-2, but it was believed to function in same way as it did against other viruses.
SARS-CoV-2 protein is translocated into the nucleus through the nuclear pore complex (NPC) via binding to the importin-a (IMP-a) and importin-ß (IMP-ß) heterodimer. Once in the nucleus, the SARS-CoV-2 protein is released by the importin-a/ß complex. The AARS-CoV-2 protein then promotes host shut-off, which retults in the reduction of the host immune response, theteby allowing the "virus to replicate. Ivermectin inhibits SARS-CoV-2 protein translocation into the nucleus by binding to the imp ortin-a/ß complex and destabtlizing the importin-a/ß heterodimer. The ivermectin treatment mott iikely promotes host immune te sponses to ocour in an efficient manner.
There Iras been increated public interest in ivermectin after the study showed the effect of tine dtug on SARS-CoV-2 in vitro. Tire Food and Drug Administration (FDA) even responded to this study by issuing an official letter to emphasize that research was stiil at the very early stage and to highlight the need to conduct further phases of clinical trials to determine if iverm/ctin is effective in the treatment of COVID-19. Thi- is important, as the study may lead to the high-risk practice of self-medication by consumers [35]. Re.ardless of the controversy, this study il an important milestone for furth/r research! on the effect of ivermectin on SARS-CoV-2 infection.
4.2. Results from Patients
The drug combination of ivermectin and hydroxychloroquine was proposed as a combination therapy for the prophylaxis or treatment of COVID-19. This combination may produce a synergistic effect with the inhibition of both viral entry and viral replication [36]. However, pharmacokinetic analysis indicated that a higher dosage was required to replicate the antiviral activity. Therefore, the recommended inhibitory concentration is very difficult to reach in humans [37]. In addition, although hydroxychloroquine has been approved by the FDA as an Emergency Use Authorization (EUA) against COVID-19, its efficacy is questioned [38] and its usage against SARS-CoV-2 is still highly controversial [39,40]. Further randomized clinical controlled studies are required to come to a conclusion about the efficacy of ivermectin in patients with SARS-CoV-2.
4.3. Ongoing Clinical Trials
Several clinical trials are ongoing in various countries, including India, the USA, Egypt, and Iraq, to assess the efficacy of ivermectin for COVID-19. The list of the current ongoing clinical trials is presented in Table 1. The results of these clinical trials will provide robust information on the efficacy of ivermectin for COVID-19 treatment.
5.Conclusions
Ivermectin is an antiparasitic drug with potential use as a broad-spectrum antimicrobial agent for the treatment of viral infections. Initial evidence indicated that ivermectin, an importin a/ß1-mediated nuclear import inhibitor, inhibited SARS-CoV-2 in vitro. In a small clinical study, the administration of ivermectin (150 gg/kg) in hospitalized patients with COVID-19 was associated with a lower mortality rate and a shorter hospital stay. Several randomized controlled trials are ongoing to investigate the efficacy of ivermectin against COVID-19. In addition to ivermectin, several drugs either currently classified as an antiviral or alternative class of drug, have been the subject of clinical trials as a part of the drug repurposing effort in the fight against COVID-19. The results of these clinical trials are required to confirm the efficacy of these drugs for the treatment of patients with COVID-19.
Author Contributions: Conceptualization, H.H.; validation, M.M., A.Y., F.N., A.F., D.M., A.P., W.M., I.I., K.D., and H.H.; writing-original draft preparation, M.M., A.Y., F.N., D.M., and H.H.; writing-review and editing, M.M., A.Y., F.N., A.F., D.M., A.P., W.M., I.I., K.D., and H.H. All authors have read and agreed to the published version of the manuscript.
Funding: This research received no external funding.
Conflicts of Interest: The authors declare no conflict of interest.
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Abstract
Among the drugs repurposed for COVID-19 is ivermectin, an FDA-approved antiparasitic agent with antiviral activity against a broad range of viruses, such as influenza [18], human immunodeficiency virus (HIV) [19], dengue virus [20], West Nile virus [21], and Venezuelan equine encephalitis virus [22]. [...]ivermectin affects the IMPa/ß1 recognition of viral and other proteins by preventing its formation or dissociating the heterodimer, which is crucial in the nuclear transport of viral proteins. The drug significantly reduced viral DNA synthesis, inhibited virus production, and blocked DNA polymerase accessory subunit UL42 entrance into the nucleus by targeting the nuclear localization signal in the transfected cells [29]. [...]the administration of ivermectin increased the survival rates of Ross River virus (RRV)-infected mice, most likely by relieving the infection of the infected host [29]. Previous studies on SARS-CoV proteins have shown the potential role of IMPa/ß 1 during infection in the signal-dependent nucleocytoplasmic shuttling of the SARS-CoV nucleocapsid protein, which may affect host cell division [21,33]. [...]open reading frame (ORF) 6, as the accessory protein of SARS-CoV, has been shown to have an antagonistic effect against the antiviral activity of the STAT1 transcription factor [34].
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Details
1 Department of Microbiology, School of Medicine, Universitas Syiah Kuala, Banda Aceh, Aceh 2311, Indonesia
2 Medical Research Unit, School of Medicine, Universitas Syiah Kuala, Banda Aceh, Aceh 23111, Indonesia
3 Faculty of Pharmacy, Hasanuddin University, Makassar 90245, Indonesia
4 Research Division for Natural Product Technology (BPTBA), Indonesian Institute of Sciences (LIPI), Wonosari 55861, Indonesia
5 Department of Microbiology and Parasitology, Faculty of Medicine and Health Sciences, Warmadewa University, Denpasar 80239, Indonesia