Inhibition of SARS-CoV-2 (previously 2019-nCoV) infection by a highly potent pan-coronavirus fusion inhibitor targeting its spike protein that harbors a high capacity to mediate membrane fusion

Xia, Shuai; Liu, Meiqin; Wang, Chao; Xu, Wei; Lan, Qiaoshuai; Feng, Siliang; Qi, Feifei; Bao, Linlin; Du, Lanying; Liu, Shuwen; Qin, Chuan; Sun, Fei; Z, Shi; Zhu, Yun; Jiang, Shibo; Lu, Lu

doi:10.1038/s41422-020-0305-x

Cited by 1,162 publications

(1,442 citation statements)

References 37 publications

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“…Transient expression of S-n and S-o glycoproteins produced drastic differences in cell fusion, while their overall protein expression was similar, as evidenced by immunohistochemistry signals obtained at 48 hpt. The enhanced fusogenicity of SARS CoV-2 versus SARS was recently noted in infection of Vero cells (40) further validating that our transient transfection results reflect Spikemediated virus-induced cell fusion differences between SARS and SARS CoV-2. Cell-surface expression of S-n and S-o was comparable suggesting that the observed differences in membrane fusion was due to inherent differences in the structure and function of S-n versus S-o glycoproteins.…”

Section: Discussionsupporting

confidence: 88%

The anti-HIV Drug Nelfinavir Mesylate (Viracept) is a Potent Inhibitor of Cell Fusion Caused by the SARS-CoV-2 Spike (S) Glycoprotein Warranting further Evaluation as an Antiviral against COVID-19 infections

Musarrat

Chouljenko

Nabi

et al. 2020

Preprint

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AbstractCoronaviruses belong to a group of enveloped, positive-single stranded RNA viruses that are known to cause severe respiratory distress in animals and humans. The current SARS coronavirus-2 (SARS CoV-2) pandemic has caused more than 2,000,000 infections globally and nearly 200,000 deaths. Coronaviruses enter susceptible cells via fusion of the viral envelope with the plasma membrane and/or via fusion of the viral envelope with endosomal membranes after endocytosis of the virus into endosomes. Previous results with SARS and MERS CoV have shown that the Spike (S) glycoprotein is a major determinant of virus infectivity and immunogenicity. Herein, we show that expression of SARS CoV-2 S (S-n) glycoprotein after transient transfection of African green monkey kidney (Vero) cells caused extensive cell fusion in comparison to limited cell fusion caused by the SARS S (S-o) glycoprotein. S-n expression was detected intracellularly and on transfected Vero cell surfaces and caused the formation of very large multinucleated cells (syncytia) by 48 hours post transfection. These results are in agreement with published pathology observations of extensive syncytial formation in lung tissues of COVID-19 patients. This differential S-n versus S-o-mediated cell fusion suggests that SARS-CoV-2 is able to spread from cell-to-cell much more efficiently than SARS effectively avoiding extracellular spaces and neutralizing antibodies. A systematic screening of several drugs for ability to inhibit S-n and S-o cell fusion revealed that the FDA approved HIV-protease inhibitor, nelfinavir mesylate (Viracept) drastically inhibited S-n and S-o-mediated cell fusion in a dose-dependent manner. Complete inhibition of cell fusion was observed at a 10 micromolar concentration. Computational modeling and in silico docking experiments suggested the possibility that nelfinavir may bind inside the S trimer structure, proximal to the S2 amino terminus directly inhibiting S-n and S-o-mediated membrane fusion. Also, it is possible that nelfinavir mesylate acts on cellular processes to inhibit S proteolytic processing. These results warrant further investigations of the potential of nelfinavir mesylate as an antiviral drug, especially at early times after SARS-CoV-2 symptoms appear.

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Section: Discussionsupporting

confidence: 88%

The anti-HIV Drug Nelfinavir Mesylate (Viracept) is a Potent Inhibitor of Cell Fusion Caused by the SARS-CoV-2 Spike (S) Glycoprotein Warranting further Evaluation as an Antiviral against COVID-19 infections

Musarrat

Chouljenko

Nabi

et al. 2020

Preprint

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“…This provides a molecular mechanism in the binding of the antibody with S protein of SARS-CoV-2 [114]. In line with this result, recent study demonstrates a highly potent pan-coronavirus fusion inhibitor targeting its spike protein that harbors a high capacity to mediate membrane fusion, and inhibited SARS-CoV-2 infection [115]. The molecular mechanisms of coronavirus invasion into host cells will provide new insights into the development of therapeutic approaches for COVID-19 by targeting spike proteins and ACE2 [116][117][118].…”

Section: Spike Glycoproteins Of Sars-cov-2 and Ace2supporting

confidence: 57%

Pharmacological Therapeutics Targeting RNA-Dependent RNA Polymerase, Proteinase and Spike Protein: From Mechanistic Studies to Clinical Trials for COVID-19

Huang

Song

Huang

et al. 2020

JCM

140

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An outbreak of novel coronavirus-related pneumonia COVID-19, that was identified in December 2019, has expanded rapidly, with cases now confirmed in more than 211 countries or areas. This constant transmission of a novel coronavirus and its ability to spread from human to human have prompted scientists to develop new approaches for treatment of COVID-19. A recent study has shown that remdesivir and chloroquine effectively inhibit the replication and infection of severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2, 2019-nCov) in vitro. In the United States, one case of COVID-19 was successfully treated with compassionate use of remdesivir in January of 2020. In addition, a clinically proven protease inhibitor, camostat mesylate, has been demonstrated to inhibit Calu-3 infection with SARS-CoV-2 and prevent SARS-2-spike protein (S protein)-mediated entry into primary human lung cells. Here, we systemically discuss the pharmacological therapeutics targeting RNA-dependent RNA polymerase (RdRp), proteinase and S protein for treatment of SARS-CoV-2 infection. This review should shed light on the fundamental rationale behind inhibition of SARS-CoV-2 enzymes RdRp as new therapeutic approaches for management of patients with COVID-19. In addition, we will discuss the viability and challenges in targeting RdRp and proteinase, and application of natural product quinoline and its analog chloroquine for treatment of coronavirus infection. Finally, determining the structural-functional relationships of the S protein of SARS-CoV-2 will provide new insights into inhibition of interactions between S protein and angiotensin-converting enzyme 2 (ACE2) and enable us to develop novel therapeutic approaches for novel coronavirus SARS-CoV-2.

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“…Spike protein has 89 been a hotspot in CoV2 genome since the beginning due to the presence of 90 receptor-binding domain. Contact point to the host includes the domains from S1 91 subunit of this S-protein [19]. The mutation observed 23403A>G (D614G) lies in tail 92 region of this S1 subunit and before the cleavage site of another subunit called S2 of 93 S-protein.…”

Section: Mutations In the Different Non-structural Protein (Nsp) Genementioning

confidence: 99%

“…The 440 17 sequences are from different parts of the world including countries from Europe, USA, 18 Middle East, Asia and 28 sequences submitted from India with 11 sequenced in Iran. 19 The data was downloaded from GenBank, GISAID, and SRA. Data was collected for 20 this study last as of 9th April 2020, with 440 genome sequence of the novel and early 21 strains from the world along with 28 sequences from India.…”

mentioning

confidence: 99%

Phylogenetic Analysis of the Novel Coronavirus Reveals Important Variants in Indian Strains

Joshi

Paul

2020

Preprint

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Recently classified as a pandemic by WHO, novel Corononavirus 2019 has affected almost every corner of the globe causing human deaths in a range of hundred thousands. The virus having its roots in Wuhan (China) has been spread over the world by its own property to change itself accordingly. These changes correspond to its transmission and pathogenicity due to which the concept of social distancing appeared into the picture.

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Inhibition of SARS-CoV-2 (previously 2019-nCoV) infection by a highly potent pan-coronavirus fusion inhibitor targeting its spike protein that harbors a high capacity to mediate membrane fusion

Cited by 1,162 publications

References 37 publications

The anti-HIV Drug Nelfinavir Mesylate (Viracept) is a Potent Inhibitor of Cell Fusion Caused by the SARS-CoV-2 Spike (S) Glycoprotein Warranting further Evaluation as an Antiviral against COVID-19 infections

The anti-HIV Drug Nelfinavir Mesylate (Viracept) is a Potent Inhibitor of Cell Fusion Caused by the SARS-CoV-2 Spike (S) Glycoprotein Warranting further Evaluation as an Antiviral against COVID-19 infections

Pharmacological Therapeutics Targeting RNA-Dependent RNA Polymerase, Proteinase and Spike Protein: From Mechanistic Studies to Clinical Trials for COVID-19

Phylogenetic Analysis of the Novel Coronavirus Reveals Important Variants in Indian Strains

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