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Despite the successful development and active administration of several commercially available vaccines and antivirals, the suffering inflicted by the coronavirus disease 2019 (COVID-19) pandemic seems likely to continue for the foreseeable future. The emergence of more contagious variants of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is further aggravating the already-devasted healthcare systems around the world. The classification of SARS-CoV-2 as a biosafety level 3 (BSL-3) pathogen due to its relatively high fatality rate has restricted its accessibility to the scientific community for research purposes. This has been one of the biggest hurdles to overcome in the prompt development of effective vaccines and therapeutics against COVID-19. In this regard, human coronavirus OC43 (HCoV-OC43) has gained new attention as an attractive and safe model to study coronaviruses in the low-risk research setting (BSL-2). To better understand its utility as an alternative to SARS-CoV-2 research, the history and classification of HCoV-OC43 together with the clinical manifestations associated with its infection are first summarized. The characteristics of its viral genomes and genes are also presented in comparison with SARS-CoV-2. Then, its evolution process in the context of interspecies and intraspecies perspectives is further explained. The host–virus interaction sections cover the host factors necessary to support the viral life cycle of HCoV-OC43, followed by a description of the innate—as well as adaptive—immunological responses to HCoV-OC43 infection. The development and application of in vitro and in vivo models to study HCoV-OC43 and the discovery of potential antivirals for COVID-19 by using HCoV-OC43 models are also discussed.

In general, all coronaviruses are members of the Coronaviridae family of the order Nidovirales. Mammals including bats, cows, mice, birds, and humans serve as their natural hosts [1]. Based on sequence homology, they are further classified into four genera including alpha, beta, gamma, and delta coronaviruses. Endemic strains of human coronavirus such as 229E and NL63 are typical examples of alpha coronaviruses. The genus beta coronavirus is further divided into 2a (OC43 and HKU1), 2b (SARS), and 2c (middle east respiratory syndrome, MERS) coronaviruses [2,3,4]. Animal viruses such as mouse hepatitis virus (MHV) and bovine coronavirus (BCoV) also belong to the genus beta coronavirus. HCoV-229E, HCoV-NL63, HCoV-HKU1, and HCoV-OC43 are four typical co-circulating low-risk human coronaviruses. They are predominantly associated with mild infection of the upper respiratory tract [5]. They have become endemic respiratory coronaviruses since their introduction into the human population [2]. Due to their zoonotic origin, all these endemic strains are thought to have broken the interspecies barrier, resulting in altered tropism for humans [6]. With regard to the zoonosis of SARS-CoV-2, the origin of SARS-CoV-2 infection in the wild was proposed to begin from bats based on sequencing results of bat coronaviruses [7,8]. In the wild, reptiles, horses, camels, sheep, llamas, marine mammals, and badgers were suspected to be infected with SARS-CoV-2 with no experimental evidence [9]. Although some cases of SARS-CoV-2 infection in pigs, birds, and cows were reported, they all seem to be inconclusive or lack experimental evidence [9]. Interestingly, the transmission of SARS-CoV-2 from human to animals including cats, dogs, tigers, lions, and mink has also been confirmed [9]. As experimental models to study SARS-CoV-2, mice, hamsters, and ferrets are generally used for this purpose [9,10].

As explained previously, HCoV-OC43 is one of the seasonally circulating community-acquired coronaviruses, together with other three endemic strains. HCoV-OC43 was first discovered by using a human embryonic tracheal organ culture (OC) technique [11,12]. An examination of nasopharyngeal washings from an acute respiratory tract disease patient led to the recovery of multiple strains of infectious agents. Their sensitivity to ether indicated the requirement of a lipid-containing protein coat for productive infection [11,12]. Among them, two of the six strains, designated OC38 and OC43, were able to cause encephalitis when inoculated into newborn mice, highlighting their distinct neurotrophic pathogenesis despite their respiratory origin [13]. Due to the morphological resemblance to avian infectious bronchitis virus (IBV), HCoV-OC43 has initially been named an “IBV-like” virus [11,14]. A hemagglutination inhibition test was frequently utilized as a preferred method for its characterization [15]. In addition, owing to its close structural similarity to MHV, an adaptation of OC43 to the suckling-mouse brain was empirically tested and successfully utilized for its efficient propagation [12,13].

In general, infection with human coronaviruses is responsible for common colds. Some patients show symptoms of diarrhea and enterocolitis. Roughly, 15 to 35% of all common colds are estimated to be attributed to coronavirus infection [12,16,17]. On occasion, they have been associated with neurologic disorders such as multiple sclerosis [18]. According to surveillance data, HCoV-OC43 has been regarded as the most frequently found strain responsible for coronavirus-associated mild colds [19]. In particular, among all respiratory viruses identified in respiratory infection samples, 4.7% turned out to be related to HCoV-OC43 [20]. Along with HCoV-229E and HCoV-NL63, HCoV-OC43 has also been shown to be a primary etiological agent for mild upper respiratory tract infections in children [12,20,21,22]. In line with this, a higher rate of infections with HCoV-OC43 has been consistently reported [23,24,25,26,27]. Although HCoV-OC43 infections are generally mild, subclinical, and self-limited [28], more severe respiratory tract infections including bronchiolitis and pneumonia have been reported in high-risk groups. These are infants, elderly individuals, and immunocompromised patients [29,30,31]. Despite the potential involvement of HCoV-OC43 in neurologic diseases, its association with neurotrophic etiology has never been validated [32,33]. The main symptoms of HCoV-OC43 infection are similar to respiratory tract infection symptoms like fever and cough [20]. Infection with other respiratory viruses has also been suggested as one of the contributing factors to the development of lower respiratory tract infections by HCoV-OC43 [20].

Unlike common community-acquired endemic human coronaviruses, recently emerged novel coronaviruses such as SARS-CoV-1, SARS-CoV-2, and MERS-CoV can cause a highly severe clinical course of infection and fatality mainly in elderly patients, particularly those with previous chronic medical conditions [34]. However, given the gradually decreased clinical severity shown in recently reported variants, SARS-CoV-2 seems to be in the process of establishing itself as one of these endemic human respiratory coronaviruses [2]. In addition, several reports suggest a protective role of pre-existing cross-immunity against endemic human coronaviruses in SARS-CoV-2 patients [35]. Therefore, understanding the mutual relationship between high- and low-risk coronaviruses will be critical not only for the development of effective countermeasures against current pandemics but also for the correct prediction of the evolutionary direction of current high-risk coronaviruses in the future.

Structurally, the single-stranded RNA genome of coronavirus is encapsidated in a helical nucleocapsid [28]. In general, the initial portion of the coronavirus genome encodes two long open reading frames (ORF1a and 1b), which generate sixteen non-structural (NS) proteins necessary for viral replication. Four structural proteins and accessory proteins (NS2a and NS5a) are translated from their separate subgenomic RNAs. Viral structural proteins include spike (S), envelope (E), matrix (M), and nucleocapsid (N) proteins [36] (Figure 1). The complete genome sequence of SARS-CoV shares 53.1% identity with that of HCoV-OC43, suggesting its significant relation to HCoV-OC43 [31,37]. In particular, comparisons with the SARS-CoV nucleotide and amino acid sequences suggest that HCoV-OC43 shares highly homologous motifs necessary for viral replication and pathogenesis [31]. In this regard, HCoV-OC43 can be regarded as a good alternative model to study SARS-CoV biology without the need for level three containment facilities [31]. However, unlike SARS-CoV, HCoV-OC43 and HCoV-HKU1 contain extra NS2a and hemagglutinin-esterase (HE) genes in front of the S gene (Figure 2). The relatively high homology (92%) of the HCoV-OC43 NS2a protein with that of BCoV strongly suggests its bovine origin [38]. As shown in Figure 2, the 3′ terminal region of the HCoV-OC43 genome encodes the NS2a, HE, S, NS5a, E, M, and N genes in order [28,39,40,41]. The exact roles of the accessory proteins such as NS2a and 5a in the life cycle of HCoV-OC43 are unknown, although they are suggested to be associated with the host immune evasion process [42,43].

Thus far, only three papers have described the functions of the NS proteins of HCoV-OC43 in the context of HCoV-OC43 biology [38,44,45]. Mounir et al. characterized the nucleotide and amino acid sequences of NS2 [45]. Labonte et al. confirmed the expression of the NS2 protein in HCoV-OC43-infected HRT-18 cells. Dolliver et al. showed the inhibitory ability of the NS1 protein of HCoV-OC43 against stress granule formation [44]. Since most of early studies examined the functions of the structural proteins of HCoV-OC43, we focus on the description of characteristics of the structural proteins of HCoV-OC43 in the following section.

The mutating abilities of coronaviruses and their high recombination frequencies have been the main driving forces for introducing a new coronavirus from animals to humans [70,71]. In particular, cattle and swine have served as intermediate hosts for interspecies transmission [28,72]. Therefore, its constant genetic recombination with different coronaviruses in animal populations is thought to have contributed to its evolution into the current form of HCoV-OC43 [36,73].

Understanding the adaptive process of an animal coronavirus to a human host is a prerequisite to revealing the origin of the COVID-19 pandemic [28]. Remarkable antigenic and genetic similarities have been consistently found between HCoV-OC43 and BCoV [28,74,75,76,77]. In essence, HCoV-OC43 appears to have emerged from a spillover of BCoV [60]. The sequence analysis of the S gene of BCoV and HCoV-OC43 indicates a high probability of a recent host jump from animals to humans [28]. Specifically, HCoV-OC43 was postulated to have diverged from BCoV in 1890 [28]. The absence of 290 nucleotides from the S gene of HCoV-OC43 compared with that of BCoV seems to have been necessary for HCoV-OC43 to adapt to a new host. However, despite their high levels of similarity, HCoV-OC43 has maintained several unique features distinct from BCoV. First, two coding regions located downstream of the S gene of BCoV are missing in HCoV-OC43 [78]. In addition, HCoV-OC43 has also abandoned the HE lectin function as an adaptive effort to become a human pathogen [60]. This carbohydrate-binding activity seems to be provided by the S protein, instead. In addition to interspecies evolution, the co-circulation of numerous recombinant variants seems to give rise to the intra-species variability in HCoV-OC43 [79]. In particular, the genetic instability of the S gene seems to be pivotal for genotype persistence in human populations [64]. The generation of a novel genotype by natural recombination appears likely to continue for the foreseeable future [41]. In addition, regions of the viral S protein of HCoV-OC43 are continually exposed to human humoral immunity. Since HCoV-OC43 will undergo adaptive evolution in these regions, these adaptive alterations in antigenic regions of the virus will require the continual reformulation of already-made vaccines [80].

Several antiviral candidates for coronavirus infection were identified by using HCo-OC43 to treat endemic coronavirus infections. Since the COVID-19 pandemic, the utility of HCoV-OC43 has been further applied to the discovery of anti-SARS-CoV-2 compounds due to its low-risk potential. Degiaggi et al. found that phosphatidyl-serine was able to inhibit HCoV-OC43 (Table 3) [126]. Cystatin C and D, potent inhibitors of cysteine proteases such as papain and cathepsin B, were also shown to inhibit HCoV-OC43 at its physiologic concentration (Table 3) [127,128]. Chloroquine, which once showed promise as a new class of SARS-CoV-2 drugs, potently suppressed HCoV-OC43 replication in vitro, with an IC₅₀ of 0.33 μM by using the HCoV-OC43 reporter virus with a renilla luciferase gene (Table 3) [129]. Chloroquine was also able to reduce the mortality of HCoV-OC43-infected newborn C57BL/6 mice after transplacental or maternal milk delivery [130]. Emodin, an active component of several plants used in traditional Chinese medicine was able to inhibit the 3a ion channel of coronavirus SARS-CoV and HCoV-OC43 (Table 3) [131]. Meanwhile, memantine, an NMDA receptor antagonist was demonstrated to attenuate mortality rates and body weight loss in the HCoV-OC43-infected mice (Table 3) [132]. HTCC, a cationically modified chitosan, inhibited the replication of several endemic strains of human coronaviruses, including HCoV-NL63, HCoV-OC43, and HCoV-HKU1 replication in human airway epithelial cells, by disrupting the virus–receptor interactions (Table 3) [133]. The mechanism of the antiviral actions of this polymer seems to involve the blockage of virus entry into the host cell by interaction with the S protein [134]. Lycorine, a toxic crystalline alkaloid found in various Amaryllidaceae, was able to reduce the fatality of BALB/c mice by HCoV-OC43 by attenuating the viral spread in the CNS of infected mice (Table 3) [135]. Kim et al. reported that bis-benzylisoquinoline alkaloids were able to significantly inhibit HCoV-OC43-induced cell death at the early step of the virus life cycle (Table 3) [136]. Amiloride, which is a diuretic to treat hypertension, was shown to inhibit HCoV-OC43 replication via specific interactions with stem-loop structures of viral RNAs (Table 3) [137]. Tylophorine-based compounds and natural cardiotonic steroids such as cardenolides and bufadienolides were also able to inhibit HCoV-OC43 with nanomolar EC₅₀ values (Table 3) [138]. Kurarinone, a flavanone from Sophora flavescens roots, inhibited HCoV-OC43 infection in human lung fibroblasts with an IC₅₀ of 3.458 μM by impairing the virus-induced autophagy (Table 3) [139]. An anti-protozoal drug, emetine, has also been reported to have anti-coronavirus activity (Table 3) [140]. This compound was again found as an HCoV-OC43 inhibitor in HCT-8 cells (Table 3) [141]. The in vitro inhibitory capacity of the redox-active oxysterol 27-hydroxycholesterol against SARS-CoV-2 was further verified by using HCoV-OC43 (Table 3) [142]. Valinomycin, a naturally occurring dodecadepsipeptide, has been used as an antibiotic; its broad-spectrum antiviral activity was further confirmed by using HCoV-OC43 (Table 3) [40]. AT-527, a prodrug of a guanosine nucleotide analog was identified as a potent inhibitor of both SARS-CoV-2 and HCoV-OC43 in vitro (Table 3) [143]. Epigallocatechin gallate (EGCG), which is a green tea polyphenol, was able to decrease the 3CL-protease activity of HCoV-OC43 and HCoV-229E. In addition, EGCG treatment attenuated HCoV-OC43-associated cytotoxicity (Table 3) [144]. Lactoferrin is a multifunctional protein of the transferrin family. The broad-spectrum antiviral activity of lactoferrin was also confirmed by using HCoV-OC43. The binding of lactoferrin to heparan sulfate proteoglycans seems to be responsible for blocking viral attachment to the host cell (Table 3) [145].

In this review paper, we overviewed the history, classification, and clinical manifestations of HCoV-OC43. The characteristics of its genomes and genes and its evolution process were further explored. The essential host factors for the viral life cycle and the innate, as well as adaptive, immunological responses were also summarized. Finally, the available in vitro and in vivo systems to study HCoV-OC43 and its application to the discovery of potential antivirals for COVID-19 were also presented. HCoV-OC43 should provide a valuable tool, not only for the general study of coronavirus biology but also for the rapid identification of promising drugs against coronaviruses without the drawbacks of biosafety level 3 confinement.