Your search keyword '"camostat"' showing total 171 results

1. Dual inhibition of TMPRSS2 and Cathepsin Bprevents SARS-CoV-2 infection in iPS cells

Author

Emi Sano, Rina Hashimoto, Ayaka Sakamoto, Akitsu Hotta, Shinya Yamanaka, Kazuo Takayama, Kazutoshi Takahashi, Sayaka Deguchi, and Renxing Yi

Subjects

Camostat, Proteases, ACE2, camostat, RM1-950, Biology, Cathepsin B, human iPS cells, chemistry.chemical_compound, Drug Discovery, Receptor, TMPRSS2, Cathepsin, Gene knockdown, CA-074 methyl ester, SARS-CoV-2, COVID-19, CRISPRi, Molecular biology, chemistry, Basigin, Molecular Medicine, Original Article, Therapeutics. Pharmacology, Viral load

Abstract

It has been reported that many receptors and proteases are required for severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) infection. Although angiotensin-converting enzyme 2 (ACE2) is the most important of these receptors, little is known about the contribution of other genes. In this study, we examined the roles of neuropilin-1, basigin, transmembrane serine proteases (TMPRSSs), and cathepsins (CTSs) in SARS-CoV-2 infection using the CRISPR interference system and ACE2-expressing human induced pluripotent stem (iPS) cells. Double knockdown of TMPRSS2 and cathepsin B (CTSB) reduced the viral load to 0.036% ± 0.021%. Consistently, the combination of the CTPB inhibitor CA-074 methyl ester and the TMPRSS2 inhibitor camostat reduced the viral load to 0.0078% ± 0.0057%. This result was confirmed using four SARS-CoV-2 variants (B.1.3, B.1.1.7, B.1.351, and B.1.1.248). The simultaneous use of these two drugs reduced viral load to less than 0.01% in both female and male iPS cells. These findings suggest that compounds targeting TMPRSS2 and CTSB exhibit highly efficient antiviral effects independent of gender and SARS-CoV-2 variant., Graphical abstract, Hashimoto et al. used iPS cells and the CRISPRi system to compare the functions of receptors and proteases involved in SARS-CoV-2 infection. Dual inhibition of TMPRSS2 and CTSB prevented SARS-CoV-2 infection. The combination of TMPRSS2 and CTSB inhibitor treatment exhibited highly efficient antiviral effects independent of gender and SARS-CoV-2 variant.

Published

2021

2. Air-liquid interphase culture confers SARS-CoV-2 susceptibility to A549 alveolar epithelial cells

Author

Yasuko Orba, William W. Hall, Shinsuke Toba, Takao Sanaki, Kentaro Uemura, Hirofumi Sawa, Akihiko Sato, Yukari Itakura, Koshiro Tabata, Kittiya Intaruck, Michihito Sasaki, and Mai Kishimoto

Subjects

Camostat, viruses, Biophysics, Cell Culture Techniques, ACE2, Biology, Peptidyl-Dipeptidase A, Biochemistry, Article, Microbiology, chemistry.chemical_compound, Downregulation and upregulation, Viral entry, Humans, A549 cells, Respiratory system, Receptor, Molecular Biology, Cells, Cultured, TMPRSS2, A549 cell, SARS-CoV-2, Serine Endopeptidases, COVID-19, Cell Biology, respiratory system, Mucus, respiratory tract diseases, Up-Regulation, Air-liquid interface, Gene Expression Regulation, Neoplastic, chemistry, Cell culture, Alveolar Epithelial Cells, Disease Susceptibility

Abstract

The human lung cell A549 is susceptible to infection with a number of respiratory viruses. However, A549 cells are resistant to Severe Acute Respiratory Syndrome-Coronavirus-2 (SARS-CoV-2) infection in conventional submerged culture, and this would appear to be due to low expression levels of the SARSCoV-2 entry receptor: angiotensin-converting enzyme-2 (ACE2). Here, we examined SARS-CoV-2 susceptibility to A549 cells after adaptation to air-liquid interface (ALI) culture. A549 cells in ALI culture yielded a layer of mucus on their apical surface, exhibited decreased expression levels of the proliferation marker KI-67 and intriguingly became susceptible to SARS-CoV-2 infection. We found that A549 cells increased the endogenous expression levels of ACE2 and TMPRSS2 following adaptation to ALI culture conditions. Camostat, a TMPRSS2 inhibitor, reduced SARS-CoV-2 infection in ALI-cultured A549 cells. These findings indicate that ALI culture switches the phenotype of A549 cells from resistance to susceptibility to SARS-CoV-2 infection through upregulation of ACE2 and TMPRSS2. (c) 2021 Elsevier Inc. All rights reserved.

Published

2021

3. Improving the Inhibition of TMPRSS2 by Molecular Docking, to Decrease the Process Infection of SARS-CoV-2

Author

J. L. Vique-Sánchez

Subjects

Camostat, Daclatasvir, Darexaban, Sivelestat, Pharmacology, Biochemistry, Otamixaban, Argatroban, chemistry.chemical_compound, Nafamostat, chemistry, Gabexate, medicine, Molecular Medicine, Molecular Biology, Biotechnology, medicine.drug

Abstract

COVID-19 pandemic continues with several works focused on the repositioning of drugs, vaccines, and antibodies against COVID-19, as well as new therapeutic targets on the cellular membrane (ACE2, NRP1, and TMPRSS2) that interacting with SARS-CoV-2 S-protein. This study proposes ten compounds (T1-T10) selected by molecular docking using a library of nearly 500,000 compounds, these ten compounds have better interaction than Daclatasvir, Ombitasvir, Camostat, Edoxaban, NCGC00386477, Nafamostat, NCGC00386945, Otamixaban, Darexaban, Gabexate, Letaxaban, Argatroban, Sivelestat, NCGC00385043, and Bromhexine, and all of them have an inhibitory effect reported at TMPRSS2. The T1-T10 compounds were selected by molecular docking in the catalytic site of TMPRSS2, which could hinder/block the interaction with the S-protein and ACE2. Therefore the initial/early stage of COVID-19 could be avoided or decreased by hindering the fusion between SARS-CoV-2 and the cell membrane and this way to develop a new adjuvant treatment against COVID-19. © 2021 by the authors.

Published

2021

4. Comprehensive Cardiotoxicity Assessment of COVID-19 Treatments Using Human-Induced Pluripotent Stem Cell-Derived Cardiomyocytes

Author

Sayo Hayashi, Atsushi Ono, Ayano Satsuka, Yasunari Kanda, and Shota Yanagida

Subjects

Camostat, Induced Pluripotent Stem Cells, 030204 cardiovascular system & hematology, Pharmacology, Favipiravir, Toxicology, Afterdepolarization, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Humans, Myocytes, Cardiac, 030212 general & internal medicine, Induced pluripotent stem cell, Cells, Cultured, Cardiotoxicity, SARS-CoV-2, business.industry, Hydroxychloroquine, COVID-19 Drug Treatment, Clinical trial, Drug repositioning, chemistry, business, medicine.drug

Abstract

Coronavirus disease 2019 (COVID-19) continues to spread across the globe, with numerous clinical trials underway seeking to develop and test effective COVID-19 therapies, including remdesivir. Several ongoing studies have reported hydroxychloroquine-induced cardiotoxicity, including development of torsade de pointes (TdP). Meanwhile, human-induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) are expected to serve as a tool for assessing drug-induced cardiotoxicity, such as TdP and contraction impairment. However, the cardiotoxicity of COVID-19 treatments has not been fully assessed using hiPSC-CMs. In this study, we focused on drug repurposing with various modes of actions and examined the TdP risk associated with COVID-19 treatments using field potential using multi-electrode array system and motion analysis with hiPSC-CMs. Hydroxychloroquine induced early after depolarization, while remdesivir, favipiravir, camostat, and ivermectin had little effect on field potentials. We then analyzed electromechanical window, which is defined as the difference between field potential and contraction-relaxation durations. Hydroxychloroquine decreased electromechanical window of hiPSC-CMs in a concentration-dependent manner. In contrast, other drugs had little effect. Our data suggest that hydroxychloroquine has proarrhythmic risk and other drugs have low proarrhythmic risk. Thus, hiPSC-CMs represent a useful tool for assessing the comprehensive cardiotoxicity caused by COVID-19 treatments in nonclinical settings.

Published

2021

5. Cross-linking peptide and repurposed drugs inhibit both entry pathways of SARS-CoV-2

Author

Kelvin K. W. To, Hoiyan Lam, Jasper Fuk-Woo Chan, Wan-Mui Chan, Chris Chung-Sing Chan, Jonathan Daniel Ip, Man Lung Yeung, Xinxin Zhou, Kwok-Yung Yuen, Hanjun Zhao, Shibo Jiang, Anna Jinxia Zhang, Jian-Piao Cai, Allen Wing-Ho Chu, Zheng Peng, and Andrew Chak-Yiu Lee

Subjects

0301 basic medicine, Indoles, animal diseases, viruses, General Physics and Astronomy, Pharmacology, medicine.disease_cause, chemistry.chemical_compound, Mice, 0302 clinical medicine, Chloroquine, Chlorocebus aethiops, skin and connective tissue diseases, Coronavirus, Mice, Inbred BALB C, Multidisciplinary, Drug discovery, Serine Endopeptidases, virus diseases, Drug repositioning, 030220 oncology & carcinogenesis, Female, medicine.drug, Camostat, Endosome, Science, Antiviral Agents, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, In vivo, medicine, Animals, Humans, Vero Cells, SARS-CoV-2, HEK 293 cells, fungi, Drug Repositioning, COVID-19, General Chemistry, Virus Internalization, COVID-19 Drug Treatment, 030104 developmental biology, HEK293 Cells, chemistry, Peptides

Abstract

Up to date, effective antivirals have not been widely available for treating COVID-19. In this study, we identify a dual-functional cross-linking peptide 8P9R which can inhibit the two entry pathways (endocytic pathway and TMPRSS2-mediated surface pathway) of SARS-CoV-2 in cells. The endosomal acidification inhibitors (8P9R and chloroquine) can synergistically enhance the activity of arbidol, a spike-ACE2 fusion inhibitor, against SARS-CoV-2 and SARS-CoV in cells. In vivo studies indicate that 8P9R or the combination of repurposed drugs (umifenovir also known as arbidol, chloroquine and camostat which is a TMPRSS2 inhibitor), simultaneously interfering with the two entry pathways of coronaviruses, can significantly suppress SARS-CoV-2 replication in hamsters and SARS-CoV in mice. Here, we use drug combination (arbidol, chloroquine, and camostat) and a dual-functional 8P9R to demonstrate that blocking the two entry pathways of coronavirus can be a promising and achievable approach for inhibiting SARS-CoV-2 replication in vivo. Cocktail therapy of these drug combinations should be considered in treatment trials for COVID-19., Until today effective antivirals for COVID-19 treatment are not widely available. Here, Zhao et al. characterize a dual-functional cross-linking peptide, 8P9R, that can inhibit SARS-CoV-2 virus entry in vitro and suppresses viral replication in vivo in golden Syrian hamster.

Published

2021

6. Pharmacoinformatics-based identification of transmembrane protease serine-2 inhibitors from Morus Alba as SARS-CoV-2 cell entry inhibitors

Author

Siham A. Alissa, Hassna Mohammed Alhajri, Shuchi Nagar, Tahani Mazyad Almutairi, Rupesh V. Chikhale, Surajit Ghosh, Hans Raj Bhat, Ataul Islam, Fatmah A.S. Alasmary, and Anshul Shakya

Subjects

Camostat, Virtual screening, medicine.medical_treatment, 030303 biophysics, Molecular Dynamics Simulation, medicine.disease_cause, urologic and male genital diseases, Catalysis, Inorganic Chemistry, Hydrophobic effect, 03 medical and health sciences, chemistry.chemical_compound, Drug Discovery, Morus alba Linn, medicine, Serine, Humans, Protease Inhibitors, Physical and Theoretical Chemistry, Molecular Biology, TMPRSS2, 030304 developmental biology, Coronavirus, chemistry.chemical_classification, 0303 health sciences, Protease, Chemistry, SARS-CoV-2, Organic Chemistry, General Medicine, Virus Internalization, Transmembrane Protease Serine 2, Transmembrane protein, Amino acid, COVID-19 Drug Treatment, Molecular Docking Simulation, Biochemistry, Molecular docking, Original Article, Morus, Information Systems

Abstract

Abstract Transmembrane protease serine-2 (TMPRSS2) is a cell-surface protein expressed by epithelial cells of specific tissues including those in the aerodigestive tract. It helps the entry of novel coronavirus (n-CoV) or Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) in the host cell. Successful inhibition of the TMPRSS2 can be one of the crucial strategies to stop the SARS-CoV-2 infection. In the present study, a set of bioactive molecules from Morus alba Linn. were screened against the TMPRSS2 through two widely used molecular docking engines such as Autodock vina and Glide. Molecules having a higher binding affinity toward the TMPRSS2 compared to Camostat and Ambroxol were considered for in-silico pharmacokinetic analyses. Based on acceptable pharmacokinetic parameters and drug-likeness, finally, five molecules were found to be important for the TMPRSS2 inhibition. A number of bonding interactions in terms of hydrogen bond and hydrophobic interactions were observed between the proposed molecules and ligand-interacting amino acids of the TMPRSS2. The dynamic behavior and stability of best-docked complex between TRMPRSS2 and proposed molecules were assessed through molecular dynamics (MD) simulation. Several parameters from MD simulation have suggested the stability between the protein and ligands. Binding free energy of each molecule calculated through MM-GBSA approach from the MD simulation trajectory suggested strong affection toward the TMPRSS2. Hence, proposed molecules might be crucial chemical components for the TMPRSS2 inhibition. Graphic abstract

Published

2021

7. Strong Binding of Leupeptin with TMPRSS2 Protease May Be an Alternative to Camostat and Nafamostat for SARS-CoV-2 Repurposed Drug: Evaluation from Molecular Docking and Molecular Dynamics Simulations

Author

Ramakrishnan, Jaganathan, Kandasamy, Saravanan, Iruthayaraj, Ancy, Magudeeswaran, Sivanandam, Chinnasamy, Kalaiarasi, and Poomani, Kumaradhas

Subjects

Camostat, Leupeptins, medicine.medical_treatment, Bioengineering, Molecular dynamics, Molecular Dynamics Simulation, Pharmacology, urologic and male genital diseases, Antiviral Agents, Guanidines, Applied Microbiology and Biotechnology, Biochemistry, Molecular Docking Simulation, Article, chemistry.chemical_compound, medicine, Humans, Molecular Biology, TMPRSS2, Protease, SARS-CoV-2, Chemistry, Serine Endopeptidases, Leupeptin, Drug Repositioning, COVID-19, Respiratory infection, Esters, Repurposed drug, General Medicine, Transmembrane Protease Serine 2, Benzamidines, COVID-19 Drug Treatment, Nafamostat, Binding affinity, Docking (molecular), Molecular docking, Protein Binding, Biotechnology

Abstract

The unprecedented coronavirus SARS-CoV-2 outbreak at Wuhan, China, caused acute respiratory infection to humans. There is no precise vaccine/therapeutic agents available to combat the COVID-19 disease. Some repurposed drugs are saving the life of diseased, but the complete cure is relatively less. Several drug targets have been reported to inhibit the SARS-CoV-2 virus infection, in that TMPRSS2 (transmembrane protease serine 2) is one of the potential targets; inhibiting this protease stops the virus entry into the host human cell. Camostat mesylate, nafamostat, and leupeptin are the drugs, in which the first two drugs are being used for COVID-19 and leupeptin also tested. To consider these drugs as the repurposed drug for COVID-19, it is essential to understand their binding affinity and stability with TMPRSS2. In the present study, we performed the molecular docking and molecular dynamics (MD) simulation of these molecules with the TMPRSS2. The docking study reveals that leupeptin molecule strongly binds with TMPRSS2 protein than the other two drug molecules. The RMSD and RMSF values of MD simulation confirm that leupeptin and the amino acids of TMPRSS2 are very stable than the other two molecules. Furthermore, leupeptin forms interactions with the key amino acids of TMPRSS2 and the same have been maintained during the MD simulations. This structural and dynamical information is useful to evaluate these drugs to be used as repurposed drugs, however, the strong binding profile of leupeptin with TMPRSS2, suggests, it may be considered as a repurposed drug for COVID-19 disease after clinical trial. Supplementary Information The online version contains supplementary material available at 10.1007/s12010-020-03475-8.

Published

2021

8. Spontaneous binding of potential COVID-19 drugs (Camostat and Nafamostat) to human serine protease TMPRSS2

Author

Du Wenhao, Qiang Huang, Andreas Herrmann, Haixia Zhu, Qing Liu, and Menghua Song

Subjects

Camostat, Biophysics, Drug action, Pharmacology, TMPRSS2, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Spontaneous binding simulation, Structural Biology, Genetics, Binding site, ComputingMethodologies_COMPUTERGRAPHICS, 030304 developmental biology, Serine protease, chemistry.chemical_classification, 0303 health sciences, biology, SARS-CoV-2, COVID-19, Computer Science Applications, Nafamostat, chemistry, Drug development, 030220 oncology & carcinogenesis, biology.protein, Glycoprotein, TP248.13-248.65, Research Article, Biotechnology

Abstract

Graphical abstract, Effective treatment or vaccine is not yet available for combating SARS coronavirus 2 (SARS-CoV-2) that caused the COVID-19 pandemic. Recent studies showed that two drugs, Camostat and Nafamostat, might be repurposed to treat COVID-19 by inhibiting human TMPRSS2 required for proteolytic activation of viral spike (S) glycoprotein. However, their molecular mechanisms of pharmacological action remain unclear. Here, we perform molecular dynamics simulations to investigate their native binding sites on TMPRSS2. We revealed that both drugs could spontaneously and stably bind to the TMPRSS2 catalytic center, and thereby inhibit its proteolytic processing of the S protein. Also, we found that Nafamostat is more specific than Camostat for binding to the catalytic center, consistent with reported observation that Nafamostat blocks the SARS-CoV-2 infection at a lower concentration. Thus, this study provides mechanistic insights into the Camostat and Nafamostat inhibition of the SARS-CoV-2 infection, and offers useful information for COVID-19 drug development.

Published

2021

9. Are antibacterial effects of non-antibiotic drugs random or purposeful because of a common evolutionary origin of bacterial and mammalian targets?

Author

Axel Dalhoff

Subjects

0301 basic medicine, Microbiology (medical), Camostat, Reversion of resistance, medicine.medical_treatment, Virulence attenuation, 030106 microbiology, Phosphatase, Virulence, Review, Microbial Sensitivity Tests, beta-Lactams, beta-Lactamases, Serine, 03 medical and health sciences, chemistry.chemical_compound, Bacterial Proteins, medicine, Animals, Threonine, chemistry.chemical_classification, Protease, Bacteria, Kinase, General Medicine, Common ancestry, Anti-Bacterial Agents, Synergy, 030104 developmental biology, Infectious Diseases, Enzyme, Biochemistry, chemistry, Pharmaceutical Preparations, Conserved targets

Abstract

Purpose Advances in structural biology, genetics, bioinformatics, etc. resulted in the availability of an enormous pool of information enabling the analysis of the ancestry of pro- and eukaryotic genes and proteins. Methods This review summarizes findings of structural and/or functional homologies of pro- and eukaryotic enzymes catalysing analogous biological reactions because of their highly conserved active centres so that non-antibiotics interacted with bacterial targets. Results Protease inhibitors such as staurosporine or camostat inhibited bacterial serine/threonine or serine/tyrosine protein kinases, serine/threonine phosphatases, and serine/threonine kinases, to which penicillin-binding-proteins are linked, so that these drugs synergized with β-lactams, reverted aminoglycoside-resistance and attenuated bacterial virulence. Calcium antagonists such as nitrendipine or verapamil blocked not only prokaryotic ion channels but interacted with negatively charged bacterial cell membranes thus disrupting membrane energetics and inducing membrane stress response resulting in inhibition of P-glycoprotein such as bacterial pumps thus improving anti-mycobacterial activities of rifampicin, tetracycline, fluoroquinolones, bedaquilin and imipenem-activity against Acinetobacter spp. Ciclosporine and tacrolimus attenuated bacterial virulence. ACE-inhibitors like captopril interacted with metallo-β-lactamases thus reverting carbapenem-resistance; prokaryotic carbonic anhydrases were inhibited as well resulting in growth impairment. In general, non-antibiotics exerted weak antibacterial activities on their own but synergized with antibiotics, and/or reverted resistance and/or attenuated virulence. Conclusions Data summarized in this review support the theory that prokaryotic proteins represent targets for non-antibiotics because of a common evolutionary origin of bacterial- and mammalian targets resulting in highly conserved active centres of both, pro- and eukaryotic proteins with which the non-antibiotics interact and exert antibacterial actions.

Published

2020

10. In Silico Study of Curcumin and Folic Acid as Potent Inhibitors of Human Transmembrane Protease Serine 2 in the Treatment of COVID-19

Author

Rao Gollapudi, Anuradha Vanam, and Noboru Motohashi

Subjects

chemistry.chemical_classification, Camostat, Protease, medicine.medical_treatment, Pharmacology, Transmembrane Protease Serine 2, TMPRSS2, chemistry.chemical_compound, Nafamostat, Enzyme, chemistry, Curcumin, medicine, Binding site

Abstract

Background. Human transmembrane protease 2 (TMPRSS2) protein is essential for priming spike protein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in association with human angiotensin-converting enzyme 2 (ACE2) surface receptor to facilitate viral invasion into host human cell through ACE2 receptor. Impeding TMPRSS2 protein activity is currently a preferred choice of the treatment of coronavirus disease 2019 (COVID-19) which is caused by SARS-CoV-2. Curcumin and folic acid are potential candidates for inhibiting TMPRSS2. Objective. The present study aimed to demonstrate the inhibitory activities of curcumin and folic acid, along with known human serine protease inhibitors such as nafamostat and camostat, on TMPRSS2. Methods. Curcumin and folic acid, along with nafamostat and camostat, were docked on a modeled human TMPRSS2 protein 3D structure. Nafamostat and curcumin interactions with targeted TMPRSS2 protein were identical whereas camostat and folic acid displayed similar interactions. Results. The hydrogen bond (H-bond) energies of docked curcumin, folic acid, nafamostat, and camostat were −19.86 kJ/mol, −17.63 kJ/mol, −10.53 kJ/mol, and −14.41 kJ/mol, respectively. Higher H-bond energies could strengthen protein-ligand interactions. Our results showed binding site similarities between curcumin and nafamostat as well as folic acid and camostat. Conclusion. The current in silico simulation suggested that curcumin and folic acid displayed binding poses with TMPRSS2 which are similar to nafamostat and camostat. Therefore, curcumin and folic acid could emerge as potential drug candidates to control COVID-19.

Published

2020

11. Targeting Enteropeptidase with Reversible Covalent Inhibitors To Achieve Metabolic Benefits

Author

Xuqing Zhang, James Lenhard, Richard Alexander, Weimei Sun, Maxwell D. Cummings, Bin Zhu, Kamal Albarazanji, Mina Wang, James C. Lanter, Jiejun Wu, James N. Leonard, and Yue-Mei Zhang

Subjects

Blood Glucose, Models, Molecular, 0301 basic medicine, Enteropeptidase, Camostat, Protein Conformation, CHO Cells, Pharmacology, Serine, Eating, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Cricetulus, 0302 clinical medicine, Diabetes Mellitus, Animals, Humans, Structure–activity relationship, Obesity, Enzyme Reactivation, Enzyme Inhibitors, chemistry.chemical_classification, Serine protease, biology, Kinase, Body Weight, Kinetics, Metabolism, 030104 developmental biology, Enzyme, chemistry, biology.protein, Molecular Medicine, 030217 neurology & neurosurgery, Half-Life

Abstract

Inhibition of the serine protease enteropeptidase (EP) opens a new avenue to the discovery of chemotherapeutics for the treatment of metabolic diseases. Camostat has been used clinically for treating chronic pancreatitis in Japan; however, the mechanistic basis of the observed clinical efficacy has not been fully elucidated. We demonstrate that camostat is a potent reversible covalent inhibitor of EP, with an inhibition potency (kinact/KI) of 1.5 × 104 M−1s−1. High-resolution liquid chromatography-mass spectrometry (LC-MS) showed addition of 161.6 Da to EP after the reaction with camostat, consistent with insertion of the carboxyphenylguanidine moiety of camostat. Covalent inhibition of EP by camostat is reversible, with an enzyme reactivation half-life of 14.3 hours. Formation of a covalent adduct was further supported by a crystal structure resolved to 2.19 A, showing modification of the catalytic serine of EP by a close analog of camostat, leading to formation of the carboxyphenylguanidine acyl enzyme identical to that expected for the reaction with camostat. Of particular note, minor structural modifications of camostat led to changes in the mechanism of inhibition. We observed from other studies that sustained inhibition of EP is required to effect a reduction in cumulative food intake and body weight, with concomitant improved blood glucose levels in obese and diabetic leptin-deficient mice. Thus, the structure-activity relationship needs to be driven by not only the inhibition potency but also the mechanistic and kinetic characterization. Our findings support EP as a target for the treatment of metabolic diseases and demonstrate that reversible covalent EP inhibitors show clinically relevant efficacy. SIGNIFICANCE STATEMENT Interest in targeted covalent drugs has expanded in recent years, particularly so for kinase targets, but also more broadly. This study demonstrates that reversible covalent inhibition of the serine protease enteropeptidase is a therapeutically viable approach to the treatment of metabolic diseases and that mechanistic details of inhibition are relevant to clinical efficacy. Our mechanistic and kinetic studies outline a framework for detailed inhibitor characterization that is proving essential in guiding discovery efforts in this area.

Published

2020

12. Virtual Screening on Marine Natural Products for Discovering TMPRSS2 Inhibitors

Author

Mehdi Mahmudpour, Iraj Nabipour, Mohsen Keshavarz, and Maryam Farrokhnia

Subjects

Serine protease, chemistry.chemical_classification, Camostat, Virtual screening, Natural product, biology, Molecular model, SARS-CoV-2, molecular modeling, COVID-19, molecular docking, General Chemistry, tmprss2, urologic and male genital diseases, Chemistry, chemistry.chemical_compound, Enzyme, chemistry, Biochemistry, biology.protein, Homology modeling, QD1-999, Original Research, ADME

Abstract

Although SARS-CoV-2 entry to cells strictly depends on angiotensin-converting enzyme 2 (ACE2), the virus also needs transmembrane serine protease 2 (TMPRSS2) for its spike protein priming. It has been shown that the entrance of SARS-CoV-2 through ACE2 can be blocked by cellular TMPRSS2 blockers. The main aim of this study was to find potential inhibitor(s) of TMPRSS2 through virtual screening against a homology model of TMPRSS2 using the library of marine natural products (MNPs). The homology modeling technique for generating a three-dimensional structure of TMPRSS2 was applied. Molecular docking, MM-GBSA and absorption, distribution, metabolism, excretion (ADME) evaluations were performed to investigate the inhibitory activity of marine natural products (MNPs) against TMPRSS2 and their pharmacokinetic properties. Camostat and nafamostat mesylate were used as the standard inhibitory molecules. Seven MNPs were able to inhibit TMPRSS2 better than the standard compounds. MNP 10 with CAS number 107503-09-3, called Watasenia β-D- Preluciferyl glucopyrasoiuronic acid, was found to be the best inhibitor of TMPRSS2 with acceptable pharmacokinetic properties. Herein, for the first time, a new marine natural product was introduced with potent inhibitory effects against TMPRSS2. MNP 10 exhibited favorable drug-like pharmacokinetic properties and it promises a novel TMPRSS2 blocker to combat SARS-CoV-2.

Published

2021

13. Mechanistic insights of key host proteins and potential repurposed inhibitors regulating SARS-CoV-2 pathway

Author

Debabrata Pramanik, Aiswarya Pawar, Sudip Roy, and Jayant K Singh

Subjects

Camostat, 2019-20 coronavirus outbreak, chemistry.chemical_compound, Drug repositioning, chemistry, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Computational biology, Biology, Repurposing, Virus, Host protein

Abstract

The emergence of pandemic situations originated from SARS-CoV-2 and its new variants created worldwide medical emergencies. Due to the non-availability of efficient drugs and vaccines, hundreds of thousands of people succumbed to death intoxicated by this virus. At these emergency hours, repurposing existing drugs can effectively treat patients critically infected by SARS-CoV-2. Using a high-throughput screening approach, we validated a list of potential repurposed drugs, like Nafamostat, Camostat, Silmitasertib, Valproic acid, Zotatifin, and essential host target proteins HDAC2, eIF4E2, CSK22, that are essential for viral mechanism. We determined multiple dissociation pathways of repurposed drugs, suggesting the availability of sub pockets within the host target proteins. We showed the preferential residues involved in the (un)binding kinetics of the ligands correlated to the underlying mechanism of the host protein activity. Interestingly, the residues we obtained for HDAC2 and CSK22 target proteins, which we highlighted, are also involved in the catalytic activity. The mechanistic insight presented in this work is envisaged to help use these key host proteins and potential repurposed drugs as a treatment for the SARS-CoV-2 virus.

Published

2021

14. Structural Basis of Covalent Inhibitory Mechanism of TMPRSS2-Related Serine Proteases by Camostat

Author

Yaqun Sui, Junlin Ya, Cai Yuan, Longguang Jiang, Yang Zhou, Gaohui Sun, and Mingdong Huang

Subjects

Camostat, Proteases, Serine Proteinase Inhibitors, Immunology, serine protease inhibitor, camostat, Molecular Dynamics Simulation, Pharmacology, Antiviral Agents, Guanidines, Microbiology, Serine, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Protein Domains, Virology, Humans, uPA, Protease inhibitor (pharmacology), TMPRSS2, 030304 developmental biology, Serine protease, 0303 health sciences, biology, SARS-CoV-2, Structure and Assembly, Serine Endopeptidases, COVID-19, Esters, Virus Internalization, Transmembrane Protease Serine 2, COVID-19 Drug Treatment, chemistry, 030220 oncology & carcinogenesis, Insect Science, Carcinoma, Squamous Cell, biology.protein, Mouth Neoplasms, Serine Proteases, Sequence Alignment, Plasminogen activator

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is the viral pathogen causing the coronavirus disease 2019 (COVID-19) global pandemic. No effective treatment for COVID-19 has been established yet. The serine protease transmembrane protease serine 2 (TMPRSS2) is essential for viral spread and pathogenicity by facilitating the entry of SARS-CoV-2 into host cells. The protease inhibitor camostat, an anticoagulant used in the clinic, has potential anti-inflammatory and antiviral activities against COVID-19. However, the potential mechanisms of viral resistance and antiviral activity of camostat are unclear. Herein, we demonstrate high inhibitory potencies of camostat for a panel of serine proteases, indicating that camostat is a broad-spectrum inhibitor of serine proteases. In addition, we determined the crystal structure of camostat in complex with a serine protease (uPA [urokinase-type plasminogen activator]), which reveals that camostat is inserted in the S1 pocket of uPA but is hydrolyzed by uPA, and the cleaved camostat covalently binds to Ser195. We also generated a homology model of the structure of the TMPRSS2 serine protease domain. The model shows that camostat uses the same inhibitory mechanism to inhibit the activity of TMPRSS2, subsequently preventing SARS-CoV-2 spread. IMPORTANCE Serine proteases are a large family of enzymes critical for multiple physiological processes and proven diagnostic and therapeutic targets in several clinical indications. The serine protease transmembrane protease serine 2 (TMPRSS2) was recently found to mediate SARS-CoV-2 entry into the host. Camostat mesylate (FOY 305), a serine protease inhibitor active against TMPRSS2 and used for the treatment of oral squamous cell carcinoma and chronic pancreatitis, inhibits SARS-CoV-2 infection of human lung cells. However, the direct inhibition mechanism of camostat mesylate for TMPRSS2 is unclear. Herein, we demonstrate that camostat uses the same inhibitory mechanism to inhibit the activity of TMPRSS2 as uPA, subsequently preventing SARS-CoV-2 spread.

Published

2021

15. SPIKE-1: A Randomised Phase II/III trial in a community setting, assessing use of camostat in reducing the clinical progression of COVID-19 by blocking SARS-CoV-2 Spike protein-initiated membrane fusion

Author

Sarah Halford, Susan Wan, Ilaria Dragoni, Julie Silvester, Bobojon Nazarov, Daniel Anthony, Suzie Anthony, Emma Ladds, John Norrie, Kevin Dhaliwal, and the CDD SPIKE-1 Project Team

Subjects

Camostat, medicine.medical_specialty, Medicine (General), Letter, Medicine (miscellaneous), camostat, Spike, law.invention, chemistry.chemical_compound, R5-920, Randomized controlled trial, law, Medicine, Pharmacology (medical), protocol, Prospective cohort study, TMPRSS2, Randomised controlled trial, business.industry, Public health, COVID-19, Interim analysis, Clinical trial, chemistry, Emergency medicine, business, Risk assessment, Viral load

Abstract

Objectives The primary objective is to evaluate the efficacy of camostat to prevent respiratory deterioration in patients with Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) infection. Secondary objectives include assessment of the ability of camostat to reduce the requirement for Coronavirus disease 2019 (COVID-19) related hospital admission and to reduce the requirement for supplementary oxygen and ventilation as treatment for SARS-CoV-2 infection, to evaluate overall mortality related to COVID-19 and to evaluate the efficacy of camostat by effect on clinical improvement. Research objectives include to assess change in COVID-19 symptom severity, to evaluate the ability of camostat to reduce viral load throughout duration of illness as well as translational research on host and viral genomics, serum antibody production, COVID-19 diagnostics, and validation of laboratory testing methods and biomarkers. Trial design SPIKE-1 is a randomised, multicentre, prospective, open label, community-based clinical trial. Eligible patients will be randomised 1:1 to the camostat treatment arm and control arm (best supportive care). The trial is designed to include a pilot phase recruiting up to 50 patients in each arm. An initial review at the end of the pilot phase will allow assessment of available data and inform the requirement for any protocol adaptations to include refinement of eligibility criteria to enrich the patient population and sample size calculations. Up to 289 additional patients will be randomised in the continuation phase of the trial. A formal interim analysis will be performed once 50% of the maximum sample size has been recruited Participants The trial will recruit adults (≥ 18 years) who score moderate to very high risk according to COVID-age risk calculation, with typical symptoms of COVID-19 infection as per Public Health England guidance or equivalent organisations in the UK, Health Protection Scotland, Public Health Wales, Public Health Agency (Northern Ireland) and with evidence of current COVID-19 infection from a validated assay. The trial is being conducted in the UK and patients are recruited through primary care and hospital settings. Intervention and comparator Eligible patients with be randomised to receive either camostat tablets, 200 mg four times daily (qds) for 14 days (treatment arm) or best supportive care (control arm). Main outcomes Primary outcome measure: the rate of hospital admissions requiring supplemental oxygen. Secondary outcome measures include: the rate of COVID-19 related hospital admission in patients with SARS-CoV-2 infection; the number of supplementary oxygen-free days and ventilator-free days measured at 28 days from randomisation; the rate of mortality related to COVID-19 one year from randomisation; the time to worst point on the nine-point category ordinal scale (recommended by the World Health Organization: Coronavirus disease (COVID-2019)) or deterioration of two points or more, within 28 days from randomisation. Research outcomes include the assessment of change in COVID-19 symptom severity on days 1-14 as measured by (1) time to apyrexia (maintained for 48 hrs) by daily self-assessment of temperature, time to improvement (by two points) in peripheral oxygenation saturation defined by daily self-assessment of fingertip peripheral oxygenation saturation levels, (3) assessment of COVID-19 symptoms using the Flu-iiQ questionnaire (determined by app recording and/or daily video call (or phone) consultation and (4) assessment of functional score (where possible) at screening, day 7 and 14. The ability of camostat to reduce viral load throughout duration of illness will be assessed by (1) change in respiratory (oropharyngeal/nasopharyngeal swab RT-PCR) log10 viral load from baseline to Days 7 and 14, (2) change in respiratory (saliva RT-PCR) log10 viral load from baseline to Days 1-14 and (3) change in upper respiratory viral shedding at Day 1 -14 measured as time to clearance of nasal SARS-CoV-2, defined as 2 consecutive negative swabs by qPCR. Additional translational research outcomes include assessment of host and viral genomics, serum antibody production and COVID-19 diagnostics at baseline and on Days 7 and 14. Randomisation Eligible patients will be randomised using an interactive web response system (IWRS) in a 1:1 ratio to one of two arms: (1) treatment arm or (2) control arm. Blinding (masking) The trial is open-label. Numbers to be randomised (sample size) The trial is designed to include a pilot and a continuation phase. Up to 100 patients (randomised 1:1 treatment and control arm) will be recruited in the pilot phase and a maximum of 289 patients (randomised 1:1 treatment and control) will be recruited as part of the continuation phase. The total number of patients recruited will not exceed 389. Trial Status Protocol version number v3 25 September 2020. Trial opened to recruitment on 04 August 2020. The authors anticipate recruitment to be completed by October 2021. Trial registration EudraCT 2020-002110-41; 18 June 2020 ClinicalTrials.gov NCT04455815; 02 July 2020 Full protocol The full protocol is attached as an additional file, accessible from the Trials website (Additional file 1). Unpublished PK data provided under confidentiality agreement to the trial Sponsor has been removed from the background section of the protocol to allow for publication of the trial protocol. In the interest in expediting dissemination of this material, the familiar formatting has been eliminated; this Letter serves as a summary of the key elements of the full protocol.

Published

2021

16. The TMPRSS2 Inhibitor Nafamostat Reduces SARS-CoV-2 Pulmonary Infection in Mouse Models of COVID-19

Author

David K. Meyerholz, Paul B. McCray, Jennifer A. Bartlett, and Kun Li

Subjects

0301 basic medicine, medicine.medical_treatment, viruses, coronavirus, Drug Evaluation, Preclinical, K18-hACE2, medicine.disease_cause, Guanidines, chemistry.chemical_compound, MERS-CoV, Mice, nafamostat, Lung, Cells, Cultured, Coronavirus, Host cell surface, Serine Endopeptidases, virus diseases, Esters, respiratory system, QR1-502, Nafamostat, medicine.anatomical_structure, Spike Glycoprotein, Coronavirus, Middle East Respiratory Syndrome Coronavirus, Angiotensin-Converting Enzyme 2, Research Article, Camostat, Proteases, Serine Proteinase Inhibitors, Middle East respiratory syndrome coronavirus, 030106 microbiology, camostat, Mice, Transgenic, Respiratory Mucosa, Microbiology, 03 medical and health sciences, Virology, medicine, Animals, Humans, TMPRSS2, Protease, business.industry, SARS-CoV-2, Ad5-hACE2, COVID-19, Virus Internalization, serine protease inhibitors, respiratory tract diseases, Benzamidines, COVID-19 Drug Treatment, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, chemistry, Immunology, airway epithelia, preclinical drug studies, business, Respiratory tract

Abstract

The coronavirus disease 2019 (COVID-19) pandemic has caused significant morbidity and mortality on a global scale. The etiologic agent, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), initiates host cell entry when its spike protein (S) binds to its receptor, angiotensin-converting enzyme 2 (ACE2). In airway epithelia, the spike protein is cleaved by the cell surface protease TMPRSS2, facilitating membrane fusion and entry at the cell surface. This dependence on TMPRSS2 and related proteases suggests that protease inhibitors might limit SARS-CoV-2 infection in the respiratory tract. Here, we tested two serine protease inhibitors, camostat mesylate and nafamostat mesylate, for their ability to inhibit entry of SARS-CoV-2 and that of a second pathogenic coronavirus, Middle East respiratory syndrome coronavirus (MERS-CoV). Both camostat and nafamostat reduced infection in primary human airway epithelia and in the Calu-3 2B4 cell line, with nafamostat exhibiting greater potency. We then assessed whether nafamostat was protective against SARS-CoV-2 in vivo using two mouse models. In mice sensitized to SARS-CoV-2 infection by transduction with human ACE2, intranasal nafamostat treatment prior to or shortly after SARS-CoV-2 infection significantly reduced weight loss and lung tissue titers. Similarly, prophylactic intranasal treatment with nafamostat reduced weight loss, viral burden, and mortality in K18-hACE2 transgenic mice. These findings establish nafamostat as a candidate for the prevention or treatment of SARS-CoV-2 infection and disease pathogenesis. IMPORTANCE The causative agent of COVID-19, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), requires host cell surface proteases for membrane fusion and entry into airway epithelia. We tested the hypothesis that inhibitors of these proteases, the serine protease inhibitors camostat and nafamostat, block infection by SARS-CoV-2. We found that both camostat and nafamostat reduce infection in human airway epithelia, with nafamostat showing greater potency. We then asked whether nafamostat protects mice against SARS-CoV-2 infection and subsequent COVID-19 lung disease. We performed infections in mice made susceptible to SARS-CoV-2 infection by introducing the human version of ACE2, the SARS-CoV-2 receptor, into their airway epithelia. We observed that pretreating these mice with nafamostat prior to SARS-CoV-2 infection resulted in better outcomes, in the form of less virus-induced weight loss, viral replication, and mortality than that observed in the untreated control mice. These results provide preclinical evidence for the efficacy of nafamostat in treating and/or preventing COVID-19.

Published

2021

17. Protease Inhibitors: Candidate Drugs to Inhibit Severe Acute Respiratory Syndrome Coronavirus 2 Replication

Author

Ryoichi Nagatomi, Akiko Kikuchi, Hidekazu Nishimura, Xue Deng, and Mutsuo Yamaya

Subjects

Camostat, Gabexate, viruses, medicine.medical_treatment, Pneumonia, Viral, Primary Cell Culture, Favipiravir, Virus Replication, Antiviral Agents, Guanidines, General Biochemistry, Genetics and Molecular Biology, Betacoronavirus, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Coronavirus 229E, Human, Humans, Medicine, Protease Inhibitors, 030212 general & internal medicine, Pandemics, Cells, Cultured, Protease, SARS-CoV-2, business.industry, Serine Endopeptidases, COVID-19, virus diseases, Epithelial Cells, Esters, Lopinavir, Common cold, General Medicine, Viral Load, medicine.disease, Virology, Benzamidines, Nasal Mucosa, Nafamostat, chemistry, Cell culture, Culture Media, Conditioned, 030220 oncology & carcinogenesis, Spike Glycoprotein, Coronavirus, Ritonavir, Coronavirus Infections, business, medicine.drug

Abstract

The number of patients infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has rapidly increased, although the WHO declared a pandemic. However, drugs that function against SARS-CoV-2 have not been established. SARS-CoV-2 has been suggested to bind angiotensin-converting enzyme 2, the receptor of the SARS coronavirus. SARS coronavirus and coronavirus 229E, the cause of the common cold, replicate through cell-surface and endosomal pathways using a protease, the type II transmembrane protease. To examine the effects of protease inhibitors on the replication of coronavirus 229E, we pretreated primary cultures of human nasal epithelial (HNE) cells with camostat or nafamostat, each of which has been used for the treatment of pancreatitis and/or disseminated intravascular coagulation. HNE cells were then infected with coronavirus 229E, and viral titers in the airway surface liquid of the cells were examined. Pretreatment with camostat (0.1-10 μg/mL) or nafamostat (0.01-1 μg/mL) reduced the titers of coronavirus 229E. Furthermore, a significant amount of type II transmembrane protease protein was detected in the airway surface liquid of HNE cells. Additionally, interferons have been reported to have antiviral effects against SARS coronavirus. The additive effects of interferons on the inhibitory effects of other candidate drugs to treat SARS-CoV-2 infection, such as lopinavir, ritonavir and favipiravir, have also been studied. These findings suggest that protease inhibitors of this type may inhibit coronavirus 229E replication in human airway epithelial cells at clinical concentrations. Protease inhibitors, interferons or the combination of these drugs may become candidate drugs to inhibit the replication of SARS-CoV-2.

Published

2020

18. Evaluation of intranasal nafamostat or camostat for SARS-CoV-2 chemoprophylaxis in Syrian golden hamsters

Author

Frank McCaughan, Lee Tatham, Joanne Herriott, Steve P. Rannard, Kevin Dhaliwal, Edyta Kijak, James P. Stewart, Henry Pertinez, Joanne Sharp, Anja Kipar, James J. Hobson, Paul Curley, Andrew Owen, Helen Box, Usman Arshad, Anthony Valentijn, Rajith K. R. Rajoli, and Megan Neary

Subjects

Camostat, business.industry, Hamster, Pharmacology, Airborne transmission, Article, Vaccination, chemistry.chemical_compound, Nafamostat, chemistry, Chemoprophylaxis, Medicine, Nasal administration, Dosing, skin and connective tissue diseases, business

Abstract

Successful development of a chemoprophylaxis against SARS-CoV-2 could provide a tool for infection prevention implementable alongside vaccination programmes. Camostat and nafamostat are serine protease inhibitors that inhibit SARS-CoV-2 viral entry in vitro but have not been characterised for chemoprophylaxis in animal models. Clinically, nafamostat is limited to intravenous delivery and while camostat is orally available, both drugs have extremely short plasma half-lives. This study sought to determine whether intranasal dosing at 5 mg/kg twice daily was able to prevent airborne transmission of SARS-CoV-2 from infected to uninfected Syrian golden hamsters. SARS-CoV-2 viral RNA was above the limits of quantification in both saline- and camostat-treated hamsters 5 days after cohabitation with a SARS-CoV-2 inoculated hamster. However, intranasal nafamostat-treated hamsters remained RNA negative for the full 7 days of cohabitation. Changes in body weight over the course of the experiment were supportive of a lack of clinical symptomology in nafamostat-treated but not saline- or camostat-treated animals. These data are strongly supportive of the utility of intranasally delivered nafamostat for prevention of SARS-CoV-2 infection and further studies are underway to confirm absence of pulmonary infection and pathological changes.

Published

2021

19. Human airway lineages derived from pluripotent stem cells reveal the epithelial responses to SARS-CoV-2 infection

Author

Ruobing Wang, Adam J. Hume, Mary Lou Beermann, Chantelle Simone-Roach, Jonathan Lindstrom-Vautrin, Jake Le Suer, Jessie Huang, Judith Olejnik, Carlos Villacorta-Martin, Esther Bullitt, Anne Hinds, Mahboobe Ghaedi, Rhiannon B. Werder, Kristine M. Abo, Andrew A. Wilson, Elke Mühlberger, Darrell N. Kotton, and Finn J. Hawkins

Subjects

Camostat, Cell type, respiratory system, Biology, Epithelium, respiratory tract diseases, Pathogenesis, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Interferon, Immunology, medicine, Respiratory epithelium, Induced pluripotent stem cell, Airway, medicine.drug

Abstract

SummaryThere is an urgent need to understand how SARS-CoV-2 infects the airway epithelium and in a subset of individuals leads to severe illness or death. Induced pluripotent stem cells (iPSCs) provide a near limitless supply of human cells that can be differentiated into cell types of interest, including airway epithelium, for disease modeling. We present a human iPSC-derived airway epithelial platform, composed of the major airway epithelial cell types, that is permissive to SARS-CoV-2 infection. Subsets of iPSC-airway cells express the SARS-CoV-2 entry factors ACE2 and TMPRSS2. Multiciliated cells are the primary initial target of SARS-CoV-2 infection. Upon infection with SARS-CoV-2, iPSC-airway cells generate robust interferon and inflammatory responses and treatment with remdesivir or camostat methylate causes a decrease in viral propagation and entry, respectively. In conclusion, iPSC-derived airway cells provide a physiologically relevant in vitro model system to interrogate the pathogenesis of, and develop treatment strategies for, COVID-19 pneumonia.Highlights and eTOC blurbSubsets of human iPSC-airway epithelial cells express SARS-Co-V entry factors ACE2 and TMPRSS2.iPSC-airway cells are permissive to SARS-CoV-2 infection via multiciliated cells.SARS-CoV-2 infection of iPSC-airway leads to a robust interferon and inflammatory response.iPSC-airway is a physiologically relevant model to study SARS-CoV-2 infection.

Published

2021

20. Identification of 13 Guanidinobenzoyl- or Aminidinobenzoyl-Containing Drugs to Potentially Inhibit TMPRSS2 for COVID-19 Treatment

Author

Xiaoqiang Huang, Yang Zhang, Robin Pearce, and Gilbert S. Omenn

Subjects

urologic and male genital diseases, Guanidines, 01 natural sciences, chemistry.chemical_compound, Catalytic Domain, Biology (General), Spectroscopy, 0303 health sciences, biology, Chemistry, Serine Endopeptidases, drug, Esters, General Medicine, Trypsin, Computer Science Applications, Molecular Docking Simulation, Nafamostat, Biochemistry, docking, Thermodynamics, Serine Proteinase Inhibitors, medicine.drug, Camostat, QH301-705.5, Molecular Dynamics Simulation, Antiviral Agents, Molecular mechanics, Article, Catalysis, Inorganic Chemistry, 03 medical and health sciences, medicine, Humans, Physical and Theoretical Chemistry, QD1-999, Molecular Biology, TMPRSS2, 030304 developmental biology, Serine protease, Binding Sites, 010405 organic chemistry, SARS-CoV-2, Organic Chemistry, COVID-19, Salt bridge (protein and supramolecular), molecular dynamics, Benzamidines, COVID-19 Drug Treatment, 0104 chemical sciences, Docking (molecular), biology.protein

Abstract

Positively charged groups that mimic arginine or lysine in a natural substrate of trypsin are necessary for drugs to inhibit the trypsin-like serine protease TMPRSS2 that is involved in the viral entry and spread of coronaviruses, including SARS-CoV-2. Based on this assumption, we identified a set of 13 approved or clinically investigational drugs with positively charged guanidinobenzoyl and/or aminidinobenzoyl groups, including the experimentally verified TMPRSS2 inhibitors Camostat and Nafamostat. Molecular docking using the C-I-TASSER-predicted TMPRSS2 catalytic domain model suggested that the guanidinobenzoyl or aminidinobenzoyl group in all the drugs could form putative salt bridge interactions with the side-chain carboxyl group of Asp435 located in the S1 pocket of TMPRSS2. Molecular dynamics simulations further revealed the high stability of the putative salt bridge interactions over long-time (100 ns) simulations. The molecular mechanics/generalized Born surface area-binding free energy assessment and per-residue energy decomposition analysis also supported the strong binding interactions between TMPRSS2 and the proposed drugs. These results suggest that the proposed compounds, in addition to Camostat and Nafamostat, could be effective TMPRSS2 inhibitors for COVID-19 treatment by occupying the S1 pocket with the hallmark positively charged groups.

Published

2021

21. Structure, activity and inhibition of human TMPRSS2, a protease implicated in SARS-CoV-2 activation

Author

Ashley Hutchinson, Francois Benard, Sriram Subramaniam, Karoline Leopold, Ruiyan Tan, Cheryl H. Arrowsmith, Dhiraj Mannar, Serap Beldar, Daniel Kwon, Almagul Seitova, Yanjun Li, Bryan J Fraser, Levon Halabelian, and Ryan P Wilson

Subjects

Camostat, Nafamostat, chemistry.chemical_compound, Proteases, Protease, Biochemistry, Ectodomain, Chemistry, Viral entry, medicine.medical_treatment, medicine, Protease inhibitor (pharmacology), TMPRSS2

Abstract

Transmembrane protease, serine 2 (TMPRSS2) has been identified as key host cell factor for viral entry and pathogenesis of SARS-coronavirus-2 (SARS-CoV-2). Specifically, TMPRSS2 proteolytically processes the SARS-CoV-2 Spike (S) Protein, enabling virus-host membrane fusion and infection of the lungs. We present here an efficient recombinant production strategy for enzymatically active TMPRSS2 ectodomain enabling enzymatic characterization, and the 1.95 Å X-ray crystal structure. To stabilize the enzyme for co-crystallization, we pre-treated TMPRSS2 with the synthetic protease inhibitor nafamosat to form a stable but slowly reversible (15 hour half-life) phenylguanidino acyl-enzyme complex. Our study provides a structural basis for the potent but non-specific inhibition by nafamostat and identifies distinguishing features of the TMPRSS2 substrate binding pocket that will guide future generations of inhibitors to improve selectivity. TMPRSS2 cleaved recombinant SARS-CoV-2 S protein ectodomain at the canonical S1/S2 cleavage site and at least two additional minor sites previously uncharacterized. We established enzymatic activity and inhibition assays that enabled ranking of clinical protease inhibitors with half-maximal inhibitory concentrations ranging from 1.7 nM to 120 μM and determination of inhibitor mechanisms of action. These results provide a body of data and reagents to support future drug development efforts to selectively inhibit TMPRSS2 and other type 2 transmembrane serine proteases involved in viral glycoprotein processing, in order to combat current and future viral threats.SUMMARY PARAGRAPHViruses hijack the biochemical activity of host proteins for viral invasion and replication. Transmembrane protease, serine-2 (TMPRSS2) is a surface-expressed protease implicated in the activation of influenza A, influenza B, and coronaviruses, including SARS-CoV-2, to drive efficient infection of the lungs1–5. TMPRSS2 is an attractive target for antiviral therapies, as inhibiting its proteolytic activity blocks efficient viral entry5,6. However, a structural and biochemical understanding of the protease has remained elusive and no selective inhibitors are available. We engineered on-demand activatable TMPRSS2 ectodomain and determined the 1.95 Å X-ray crystal structure of the stabilized acyl-enzyme after treatment with nafamostat, a protease inhibitor under investigation as a COVID-19 therapeutic. The structure reveals unique features of the TMPRSS2 substrate recognition pocket and domain architecture, and explains the potent, but nonselective inhibition by nafamostat. TMPRSS2 efficiently cleaved the SARS-CoV-2 S protein at the canonical S1/S2 site as well as two minor sites previously uncharacterized. We further established a robust enzymatic assay system and characterized inhibition by two additional clinical protease inhibitors under study for COVID-19, camostat and bromhexine. Our results provide a body of data and reagents to enable ongoing drug development efforts to selectively inhibit TMPRSS2 and other TTSPs involved in viral glycoprotein processing, in order to combat current and future viral threats.

Published

2021

22. An update of anti-viral treatment of COVID-19

Author

Feride Ipek Komsuoğlu Çelikyurt and Serap Şimşek-Yavuz

Subjects

Camostat, Pharmacology, Favipiravir, Antiviral Agents, Virus, Article, chemistry.chemical_compound, Viral entry, medicine, Humans, Pandemics, COVID-19 Serotherapy, treatment, business.industry, SARS-CoV-2, Immunization, Passive, COVID-19, Nitazoxanide, Hydroxychloroquine, Lopinavir, General Medicine, antiviral, COVID-19 Drug Treatment, chemistry, Ritonavir, business, medicine.drug

Abstract

Background/aim Currently there is not an effective antiviral treatment for COVID-19, but a large number of drugs have been evaluated since the beginning of the pandemic, and many of them have been used for the treatment of COVID-19 despite the preliminary or conflicting results of the clinical trials. We aimed to review and summarize all of the current knowledge on the antivirals for COVID-19. Results There are 2 main drug groups for SARS-CoV-2: agents that target proteins or RNA of the virus or interfere with proteins or biological processes in the host that support the virus. The main drug groups include inhibitors of viral entry into the human cell (convalescent plasma, monoclonal antibodies, nanobodies, mini proteins, human soluble ACE-2, camostat, dutasteride, proxalutamide, bromhexin, hydroxychloroquine, umifenovir nitazoxanid, niclosamide, lactoferrin), inhibitors of viral proteases (lopinavir/ritonavir, PF-07321332, PF-07304814, GC376), inhibitors of viral RNA (remdesivir, favipiravir, molnupiravir, AT-527, merimepodib, PTC299), inhibitors of host proteins supporting virus (plitidepsin, fluvoxamine, ivermectin), and agents supporting host natural immunity (Interferons). Conclusion When taking into account the results of all the available laboratory and clinical trials on the subject, monoclonal antibodies seem to be the most effective treatment for COVID-19 at the moment, and high-titer convalescent plasma also could be effective when administered during the early phase of the disease. As lopinavir/ritonavir, hydroxychloroquine, merimepodib, and umifenovir were found to be ineffective in RCTs, they should not be used. Additional studies are needed to define the role of remdesivir, favipiravir, interferons, ivermectin, dutasteride, proxulutamide, fluvoxamine, bromhexine, nitazoxanide, and niclosamid in the treatment of COVID-19. Finally, the results of phase trials are waited to learn whether or not the newer agents such as molnupiravir, PF-07321332, PF-07304814, plitidepsin and AT-527 are effective in the treatment of COVID-19.

Published

2021

23. Nafamostat-interferon-alpha combination suppresses SARS-CoV-2 infection by targeting cooperatively host TMPRSS2 in vitro and in vivo

Author

Aleksandr Ianevski, Rouan Yao, Tanel Tenson, Magnar Bjørås, Eva Zusinaite, Denis E. Kainov, Gunnveig Grødeland, Hilde Lysvand, Nicolas Legrand, and Valentin Oksenych

Subjects

Camostat, 0303 health sciences, business.industry, Alpha interferon, 030204 cardiovascular system & hematology, Serpin, medicine.disease_cause, 3. Good health, 03 medical and health sciences, Nafamostat, chemistry.chemical_compound, 0302 clinical medicine, Mediator, chemistry, Viral replication, In vivo, Immunology, Medicine, business, 030304 developmental biology, Coronavirus

Abstract

SARS-CoV-2 and its vaccine/immune-escaping variants continue to pose a serious threat to public health due to a paucity of effective, rapidly deployable, and widely available treatments. Here, we address these challenges by combining Pegasys (IFNa) and nafamostat to effectively suppress SARS-CoV-2 infection in cell culture and hamsters. Our results indicate that Serpin E1 is an important mediator of the antiviral activity of IFNa and that both Serpin E1 and camostat can target the same cellular factor TMPRSS2, which plays a critical role in viral replication. The low doses of the drugs in combination may have several clinical advantages, including fewer adverse events and improved patient outcome. Thus, our study may provide a proactive solution for the ongoing pandemic and potential future coronavirus outbreaks, which is still urgently required in many parts of the world.

Published

2021

24. Blocking the interactions between human ACE2 and coronavirus spike glycoprotein by selected drugs: a computational perspective

Author

Chidi Edbert Duru, Haruna Isiyaku Umar, Lynda Chioma Ngozi-Olehi, Uchechi E. Enenebeaku, Christian Ebere Enyoh, and Ijeoma Akunna Duru

Subjects

0301 basic medicine, Camostat, Ivermectin, Lopinavir, Pharmacology, Angiotensin-converting enzyme 2, medicine.disease_cause, 03 medical and health sciences, chemistry.chemical_compound, Nafamostat, 030104 developmental biology, 0302 clinical medicine, chemistry, Glycoprotein complex, Docking (molecular), Molecular docking, medicine, Ritonavir, Original Article, Spike glycoprotein, 030217 neurology & neurosurgery, Discovery Studio, Coronavirus, medicine.drug

Abstract

The coronavirus disease of 2019 (COVID-19) has become a global pandemic with rapid rate of transmission and fatalities worldwide. Scientists have been investigating a host of drugs that may be rechanneled to fight this malaise. Thus, in this current computational study we carried out molecular docking experiments to assess the bridging potentials of some commercial drugs such as chloroquine, hydroxychloroquine, lopinavir, ritonavir, nafamostat, camostat, famotidine, umifenovir, nitazoxanide, ivermectin, and fluvoxamine at the interface between human ACE2 and the coronavirus spike glycoprotein complex. This is aimed at ascertaining the ability of these drugs to bridge and prevent the complexing of these two proteins. The crystal structure of human ACE2 and the coronavirus spike glycoprotein complex was retrieved from protein database, while the selected drugs were retrieved from PubChem data base. The proteins and drugs were prepared for docking using Cresset Flare software. The docking was completed via AutoDock Vina module in Python Prescription software. The best hit drugs with each receptor were selected and their molecular interactions were analyzed using BIOVIA’s Discovery Studio 2020. The best hit compounds on the human ACE2 were the lopinavir (-10.1 kcal/mol), ritonavir (-8.9 kcal/mol), and nafamostat (-8.7 kcal/mol). Ivermectin, nafamostat, and camostat with binding energy values -9.0 kcal/mol, -7.8 kcal/mol, and -7.4 kcal/mol respectively were the hit drugs on the coronavirus spike glycoprotein. Nafamostat showed a dual bridging potential against ACE2 and spike glycoprotein, and could therefore be a promising lead compound in the prevention and control of this disease.

Published

2021

25. A novel class of TMPRSS2 inhibitors potently block SARS-CoV-2 and MERS-CoV viral entry and protect human epithelial lung cells

Author

Dong Hee Chung, Partha Karmakar, Michael A Tartell, Andrea M. Klingler, Vishnu C. Damalanka, Markus Hoffmann, Cassandra E Thompson, Sean P. J. Whelan, Matthew Mahoney, Stefan Pöhlmann, Paul W. Rothlauf, Melody Lee, Jorine Voss, Anthony J. O’Donoghue, André Luiz Lourenço, Charles S. Craik, Christina L. Stallings, Marc E. Rothenberg, James W. Janetka, Nurit P. Azouz, Anne E. Mayer Bridwell, Dustin Pwee, and Lidija Klampfer

Subjects

Medical Sciences, medicine.medical_treatment, viruses, medicine.disease_cause, Guanidines, Substrate Specificity, chemistry.chemical_compound, Mice, 0302 clinical medicine, Lung, 0303 health sciences, Multidisciplinary, biology, structure-based drug discovery, Serine Endopeptidases, virus diseases, Esters, Biological Sciences, antiviral, 3. Good health, Chemistry, Nafamostat, Infectious Diseases, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Physical Sciences, Pneumonia & Influenza, Middle East Respiratory Syndrome Coronavirus, Development of treatments and therapeutic interventions, Oligopeptides, Camostat, Middle East respiratory syndrome coronavirus, Virus, Article, Cell Line, protease inhibitor, Vaccine Related, Small Molecule Libraries, 03 medical and health sciences, In vivo, Viral entry, Biodefense, medicine, Animals, Humans, Protease inhibitor (pharmacology), Benzothiazoles, 030304 developmental biology, Serine protease, Protease, SARS-CoV-2, Prevention, COVID-19, Epithelial Cells, Pneumonia, Virus Internalization, Virology, Benzamidines, COVID-19 Drug Treatment, Emerging Infectious Diseases, chemistry, Cell culture, Drug Design, biology.protein, PS-SCL

Abstract

Significance MM3122 represents an advanced lead candidate for clinical development as a novel antiviral drug for COVID-19. In addition to being novel drugs, these selective TMRSS2 inhibitors can be used as valuable chemical probes to help elucidate mechanisms of viral pathogenesis. Since TMPRSS2 plays a key role as a viral protein processing protease in the pathogenesis of other coronaviruses (SARS-CoV, MERS-CoV) as well as influenza viruses, MM3122 and this class of TMPRSS2 inhibitors hold much promise as new drugs to not only treat SARS-CoV-2 infections but also potentially represent broad-spectrum antivirals., The host cell serine protease TMPRSS2 is an attractive therapeutic target for COVID-19 drug discovery. This protease activates the Spike protein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and of other coronaviruses and is essential for viral spread in the lung. Utilizing rational structure-based drug design (SBDD) coupled to substrate specificity screening of TMPRSS2, we have discovered covalent small-molecule ketobenzothiazole (kbt) TMPRSS2 inhibitors which are structurally distinct from and have significantly improved activity over the existing known inhibitors Camostat and Nafamostat. Lead compound MM3122 (4) has an IC50 (half-maximal inhibitory concentration) of 340 pM against recombinant full-length TMPRSS2 protein, an EC50 (half-maximal effective concentration) of 430 pM in blocking host cell entry into Calu-3 human lung epithelial cells of a newly developed VSV-SARS-CoV-2 chimeric virus, and an EC50 of 74 nM in inhibiting cytopathic effects induced by SARS-CoV-2 virus in Calu-3 cells. Further, MM3122 blocks Middle East respiratory syndrome coronavirus (MERS-CoV) cell entry with an EC50 of 870 pM. MM3122 has excellent metabolic stability, safety, and pharmacokinetics in mice, with a half-life of 8.6 h in plasma and 7.5 h in lung tissue, making it suitable for in vivo efficacy evaluation and a promising drug candidate for COVID-19 treatment.

Published

2021

26. Topical TMPRSS2 inhibition prevents SARS-CoV-2 infection in differentiated primary human airway cells

Author

Paul J. Lehner, Akhilesh Jha, James A. Nathan, Thomas Wm Crozier, Guo W, Frank McCaughan, Edward J. D. Greenwood, Coates M, Linsey Porter, and McKie M

Subjects

Camostat, business.industry, Cell, Pharmacology, TMPRSS2, Blockade, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, In vivo, medicine, Enzalutamide, Airway, business, Receptor

Abstract

BackgroundThere are limited effective prophylactic treatments for SARS-CoV-2 infection, and limited early treatment options. Viral cell entry requires spike protein binding to the ACE2 receptor and spike cleavage by TMPRSS2, a cell surface serine protease. Targeting of TMPRSS2 by either androgen blockade or direct inhibition is already in clinical trials in early SARS-CoV-2 infection.MethodsThe likely initial cells of SARS-CoV-2 entry are the ciliated cells of the upper airway. We therefore used differentiated primary human airway epithelial cells maintained at the air-liquid interface (ALI) to test the impact of targeting TMPRSS2 on the prevention of SARS-CoV-2 infection.ResultsWe first modelled the systemic delivery of compounds. Enzalutamide, an oral androgen receptor antagonist, had no impact on SARS-Cov-2 infection. By contrast, camostat mesylate, an orally available serine protease inhibitor, blocked SARS-CoV-2 entry. However, camostat is rapidly metabolised in the circulation in vivo, and systemic bioavailability after oral dosing is low. We therefore modelled local airway administration by applying camostat to the apical surface of the differentiated ALI cultures. We demonstrated that a brief exposure to topical camostat is effective at restricting SARS-CoV-2 viral infection.ConclusionThese experiments demonstrate a potential therapeutic role for topical camostat for pre- or post-exposure prophylaxis of SARS-CoV-2, which can now be evaluated in a clinical trial.

Published

2021

27. Computational Identification of a Putative Allosteric Binding Pocket in TMPRSS2

Author

Jacopo Sgrignani and Andrea Cavalli

Subjects

Camostat, QH301-705.5, Allosteric regulation, allosteric pocket, urologic and male genital diseases, Biochemistry, Genetics and Molecular Biology (miscellaneous), Biochemistry, chemistry.chemical_compound, Zymogen, medicine, Molecular Biosciences, Binding site, Biology (General), Molecular Biology, Original Research, Serine protease, biology, Chemistry, molecular modeling, Bromhexine, MD simulation, Nafamostat, Docking (molecular), docking, Biophysics, biology.protein, TMPRSS2 protein, medicine.drug

Abstract

Camostat, nafamostat, and bromhexine are inhibitors of the transmembrane serine protease TMPRSS2. The inhibition of TMPRSS2 has been shown to prevent the viral infection of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and other viruses. However, while camostat and nafamostat inhibit TMPRSS2 by forming a covalent adduct, the mode of action of bromhexine remains unclear. TMPRSS2 is autocatalytically activated from its inactive form, zymogen, through a proteolytic cleavage that promotes the binding of Ile256 to a putative allosteric pocket (A-pocket). Computer simulations, reported here, indicate that Ile256 binding induces a conformational change in the catalytic site, thus providing the atomistic rationale to the activation process of the enzyme. Furthermore, computational docking and molecular dynamics simulations indicate that bromhexine competes with the N-terminal Ile256 for the same binding site, making it a potential allosteric inhibitor. Taken together, these findings provide the atomistic basis for the development of more selective and potent TMPRSS2 inhibitors.

Published

2021

28. Virtual screening by targeting proteolytic sites of furin and TMPRSS2 to propose potential compounds obstructing the entry of SARS-CoV-2 virus into human host cells

Author

Suban K. Sahoo and Seshu Vardhan

Subjects

Camostat, Proteases, Limonin, viruses, Phytochemicals, 0211 other engineering and technologies, 02 engineering and technology, 01 natural sciences, Virus, Article, Microbiology, chemistry.chemical_compound, 021105 building & construction, Pedunculagin, Furin, Protein-protein docking, biology, SARS-CoV-2, food and beverages, COVID-19, Drugs, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Nafamostat, Complementary and alternative medicine, chemistry, Docking (molecular), Molecular docking, biology.protein

Abstract

Background and aim The year 2020 begins with the outbreak of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) that cause the disease COVID-19, and continue till today. As of March 23, 2021, the outbreak has infected 124,313,054 worldwide with a total death of 2,735,707. The use of traditional medicines as an adjuvant therapy with western drugs can lower the fatality rate due to the COVID-19. Therefore, in silico molecular docking study was performed to search potential phytochemicals and drugs that can block the entry of SARS-CoV-2 into host cells by inhibiting the proteolytic cleavage activity of furin and TMPRSS2. Experimental procedure The protein-protein docking of the host proteases furin and TMPRSS2 was carried out with the virus spike (S) protein to examine the conformational details and residues involved in the complex formation. Subsequently, a library of 163 ligands containing phytochemicals and drugs was virtually screened to propose potential hits that can inhibit the proteolytic cleavage activity of furin and TMPRSS2. Results and conclusion The phytochemicals like limonin, gedunin, eribulin, pedunculagin, limonin glycoside and betunilic acid bind at the active site of both furin and TMPRSS2. Limonin and gedunin found mainly in the citrus fruits and neem showed the highest binding energy at the active site of furin and TMPRSS2, respectively. The polyphenols found in green tea can also be useful in suppressing the furin activity. Among the drugs, the drug nafamostat may be more beneficial than the camostat in suppressing the activity of TMPRSS2., Graphical abstract Image 1

Published

2021

29. Identification of Plitidepsin as Potent Inhibitor of SARS-CoV-2-Induced Cytopathic Effect After a Drug Repurposing Screen

Author

Jordi Rodon, Jordana Muñoz-Basagoiti, Daniel Perez-Zsolt, Marc Noguera-Julian, Roger Paredes, Lourdes Mateu, Carles Quiñones, Carles Perez, Itziar Erkizia, Ignacio Blanco, Alfonso Valencia, Víctor Guallar, Jorge Carrillo, Julià Blanco, Joaquim Segalés, Bonaventura Clotet, Júlia Vergara-Alert, Nuria Izquierdo-Useros, Producció Animal, Sanitat Animal, Barcelona Supercomputing Center, and Barcelona Suprcomputing Center

Subjects

Informàtica::Aplicacions de la informàtica::Bioinformàtica [Àrees temàtiques de la UPC], Camostat, Drug, media_common.quotation_subject, synergy, Pharmacology, COVID-19 (Malaltia), Approved drug, chemistry.chemical_compound, COVID-19 (Disease), antivirals, plitidepsin, Viral entry, Medicine, Pharmacology (medical), Cytopathic effect, media_common, Original Research, business.industry, SARS-CoV-2, lcsh:RM1-950, Drugs, Drug repositioning, lcsh:Therapeutics. Pharmacology, Viral replication, chemistry, viral entry, business, Nelfinavir mesylate

Abstract

There is an urgent need to identify therapeutics for the treatment of Coronavirus disease 2019 (COVID-19). Although different antivirals are given for the clinical management of SARS-CoV-2 infection, their efficacy is still under evaluation. Here, we have screened existing drugs approved for human use in a variety of diseases, to compare how they counteract SARS-CoV-2-induced cytopathic effect and viral replication in vitro. Among the potential 72 antivirals tested herein that were previously proposed to inhibit SARS-CoV-2 infection, only 18 % had an IC50 below 25 µM or 102 IU/ml. These included plitidepsin, novel cathepsin inhibitors, nelfinavir mesylate hydrate, interferon 2-alpha, interferon-gamma, fenofibrate, camostat along the well-known remdesivir and chloroquine derivatives. Plitidepsin was the only clinically approved drug displaying nanomolar efficacy. Four of these families, including novel cathepsin inhibitors, blocked viral entry in a cell—type specific manner. Since the most effective antivirals usually combine therapies that tackle the virus at different steps of infection, we also assessed several drug combinations. Although no particular synergy was found, inhibitory combinations did not reduce their antiviral activity. Thus, these combinations could decrease the potential emergence of resistant viruses. Antivirals prioritized herein identify novel compounds and their mode of action, while independently replicating the activity of a reduced proportion of drugs which are mostly approved for clinical use. Combinations of these drugs should be tested in animal models to inform the design of fast track clinical trials. We are grateful to patients at the Hospital Germans Trias i Pujol that donated their samples for research. For his excellent assistance and advice, we thank Jordi Puig from Fundació Lluita contra la SIDA. We are most grateful to Lidia Ruiz and the Clinical Sample Management Team of IrsiCaixa for their outstanding sample processing and management, and to M. Pilar Armengol and the translational genomics platform team at the Institut de Recerca Germans Trias i Pujol. We truly thank B. Trinité for generating the Spike expression plasmid construct used in this study. We thank Pharma Mar, Rubió Laboratories, Janssen and Drs. Cabrera and Ballana form IrsiCaixa; Pascual-Figal, Lax and Asensio-Lopez MC from “Instituto de Investigación Biosanitaria IMIB-Arrixaca” of Murcia; and Fernández-Real and Barretina from the “Institut d'Investigació Biomèdica de Girona Dr Josep Trueta” for providing some of the reagents tested. Peer Reviewed "Article signat per 18 autors/es: Jordi Rodon, Jordana Muñoz-Basagoiti, Daniel Perez-Zsolt, Marc Noguera-Julian, Roger Paredes, Lourdes Mateu, Carles Quiñones, Carles Perez, Itziar Erkizia, Ignacio Blanco, Alfonso Valencia, Víctor Guallar, Jorge Carrillo, Julià Blanco, Joaquim Segalés, Bonaventura Clotet, Júlia Vergara-Alert, Nuria Izquierdo-Useros"

Published

2021

30. Camostat mesylate inhibits SARS-CoV-2 activation by TMPRSS2-related proteases and its metabolite GBPA exerts antiviral activity

Author

Frank Noé, Heike Hofmann-Winkler, Joan C. Smith, Katsura Yamatsuta, Ole S. Søgaard, Lluís Raich, Hirotaka Mizuno, Simon Olsson, Lambert K. Sørensen, Olga Danov, Takashi Yamazoe, Stephan Ludwig, Jason M. Sheltzer, Jørgen B. Hasselstrøm, Michael Winkler, Armin Braun, Danny Jonigk, Tim Hempel, Stefan Pöhlmann, Markus Hoffmann, Mads Kjolby, Nadine Krüger, Prerna Arora, and Publica

Subjects

0301 basic medicine, medicine.medical_treatment, Metabolite, Pharmacology, Guanidines, law.invention, chemistry.chemical_compound, 0302 clinical medicine, Camostat, law, Cricetinae, Chlorocebus aethiops, FOY-251, Lung, Serine Endopeptidases, Esters, General Medicine, 030220 oncology & carcinogenesis, Recombinant DNA, Research Paper, Proteases, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Molecular Dynamics Simulation, Antiviral Agents, TMPRSS2, General Biochemistry, Genetics and Molecular Biology, Article, Cell Line, 03 medical and health sciences, Viral entry, medicine, Animals, Humans, Protease Inhibitors, Protease inhibitor (pharmacology), Vero Cells, Protease, SARS-CoV-2, fungi, GBPA, Membrane Proteins, 500 Naturwissenschaften und Mathematik::570 Biowissenschaften, Biologie::570 Biowissenschaften, Biologie, Virus Internalization, COVID-19 Drug Treatment, HEK293 Cells, 030104 developmental biology, chemistry, Cell culture, Virus Activation, Serine Proteases, Ex vivo

Abstract

Background Antivirals are needed to combat the COVID-19 pandemic, which is caused by SARS-CoV-2. The clinically-proven protease inhibitor Camostat mesylate inhibits SARS-CoV-2 infection by blocking the virus-activating host cell protease TMPRSS2. However, antiviral activity of Camostat mesylate metabolites and potential viral resistance have not been analyzed. Moreover, antiviral activity of Camostat mesylate in human lung tissue remains to be demonstrated. Methods We used recombinant TMPRSS2, reporter particles bearing the spike protein of SARS-CoV-2 or authentic SARS-CoV-2 to assess inhibition of TMPRSS2 and viral entry, respectively, by Camostat mesylate and its metabolite GBPA. Findings We show that several TMPRSS2-related proteases activate SARS-CoV-2 and that two, TMPRSS11D and TMPRSS13, are robustly expressed in the upper respiratory tract. However, entry mediated by these proteases was blocked by Camostat mesylate. The Camostat metabolite GBPA inhibited recombinant TMPRSS2 with reduced efficiency as compared to Camostat mesylate. In contrast, both inhibitors exhibited similar antiviral activity and this correlated with the rapid conversion of Camostat mesylate into GBPA in the presence of serum. Finally, Camostat mesylate and GBPA blocked SARS-CoV-2 spread in human lung tissue ex vivo and the related protease inhibitor Nafamostat mesylate exerted augmented antiviral activity. Interpretation Our results suggest that SARS-CoV-2 can use TMPRSS2 and closely related proteases for spread in the upper respiratory tract and that spread in the human lung can be blocked by Camostat mesylate and its metabolite GBPA. Funding NIH, Damon Runyon Foundation, ACS, NYCT, DFG, EU, Berlin Mathematics center MATH+, BMBF, Lower Saxony, Lundbeck Foundation, Novo Nordisk Foundation.

Published

2021

31. TMPRSS2 inhibitor discovery facilitated through an in silico and biochemical screening platform

Author

Julie M. Garlick, Wu Y, Matthew B. Soellner, Charles L. Brooks, Anna K. Mapp, and Amanda L. Peiffer

Subjects

Camostat, Serine protease, Virtual screening, Protease, Drug discovery, In silico, medicine.medical_treatment, Computational biology, Biology, urologic and male genital diseases, TMPRSS2, Article, chemistry.chemical_compound, Nafamostat, chemistry, medicine, biology.protein

Abstract

The COVID-19 pandemic has highlighted the need for new antiviral targets, as many of the currently approved drugs have proven ineffective against mitigating SARS-CoV-2 infections. The host transmembrane serine protease TMPRSS2 is a highly promising antiviral target, as it plays a direct role in priming the spike protein before viral entry occurs. Further, unlike other targets such as ACE2, TMPRSS2 has no known biological role. Here we utilize virtual screening to curate large libraries into a focused collection of potential inhibitors. Optimization of a recombinant expression and purification protocol for the TMPRSS2 peptidase domain facilitates subsequent biochemical screening and characterization of selected compounds from the curated collection in a kinetic assay. In doing so, we demonstrate that serine protease inhibitors camostat, nafamostat, and gabexate inhibit through a covalent mechanism. We further identify new non-covalent compounds as TMPRSS2 protease inhibitors, demonstrating the utility of a combined virtual and experimental screening campaign in rapid drug discovery efforts., Graphical Abstract

Published

2021

32. Synergistic Interferon Alpha-based Drug Combinations Inhibit SARS-CoV-2 and other viral Infections in Vitro

Author

Laura Sandra Lello, Mona H. Fenstad, Marc P. Windisch, Minna Poranen, Valentyn Oksenych, Eva Zusinaite, Tanel Tenson, Rouan Yao, Kirsti Løseth, Svein Arne Nordbø, Astra Vitkauskiene, Eunji Jo, Aleksandr Ianevski, Denis E. Kainov, Wei Wang, Gunnveig Grødeland, Marius Trøseid, Erlend Ravlo, Jaewon Yang, Pål Aukrust, Anni I Nieminen, Hilde Lysvand, Sainan Wang, Nicolas Legrand, Anu Kantele, Andres Merits, and Magnar Bjørås

Subjects

A549 cell, Drug, Camostat, business.industry, media_common.quotation_subject, Cell, Alpha interferon, Lamivudine, medicine.disease_cause, Virology, In vitro, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Influenza A virus, Medicine, business, media_common, medicine.drug

Abstract

Antiviral drugs are powerful tools to combat emerging viral diseases, one of the leading causes of morbidity and mortality in the world. However, most existing antivirals have failed to cure COVID-19. Accordingly, there is an urgent need for new therapeutics with powerful antiviral and tolerable side effects. Here, we observed that recombinant human interferon-alpha (IFNa) triggered cell intrinsic and extrinsic antiviral responses and reduced replication of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in human lung epithelial Calu-3 cells. However, IFNa alone was insufficient to completely abolish SARS-CoV-2 replication. The combinations of IFNa with camostat, remdesivir, EIDD-2801, cycloheximide or convalescent serum showed strong synergy and, therefore, effectively inhibited SARS-CoV-2 infection. Additionally, we demonstrated synergistic antiviral activity of IFNa2a with pimodivir against influenza A virus (FluAV) infection in human lung epithelial A549 cells, as well as IFNa2a with lamivudine against human immunodeficiency virus 1 (HIV-1) infection in human TZM-bl cells. Our results indicate that IFNa2a-based combinational therapies help to reduce drug dose and improve efficacy in comparison with monotherapies, making them attractive targets for further pre-clinical and clinical development. Additionally, they have powerful treatment potential, and can be leveraged for use in the inhibition of not only emerging or re-emerging viruses, but also immune-evading or drug-resistant viral variants, and viral co-infections.

Published

2021

33. SARS-CoV-2 variants B.1.351 and P.1 escape from neutralizing antibodies

Author

Luise Graichen, Nadine Krüger, Bernd Jahrsdörfer, Alexander S. Hahn, Heike Hofmann-Winkler, Alina Seidel, Jan Münch, Bojan F. Hörnich, Amy Kempf, Hans-Martin Jäck, Sebastian R. Schulz, Martin Sebastian Winkler, Prerna Arora, Rüdiger Groß, Martin Müller, Hubert Schrezenmeier, Markus Hoffmann, Alexander Kleger, and Stefan Pöhlmann

Subjects

Models, Molecular, B.1.351, medicine.disease_cause, Antibodies, Viral, spike protein, Membrane Fusion, Neutralization, P.1, chemistry.chemical_compound, 0302 clinical medicine, antibodies, Neutralizing antibody, Coronavirus, 0303 health sciences, variants, biology, VOC, Serine Endopeptidases, Vaccination, 3. Good health, Spike Glycoprotein, Coronavirus, Antibody, Camostat, variants of concern, General Biochemistry, Genetics and Molecular Biology, Virus, Article, Cell Line, host cell entry, 03 medical and health sciences, Neutralization Tests, Drug Resistance, Viral, medicine, Animals, Humans, B.1.1.7, COVID-19 Serotherapy, 030304 developmental biology, SARS-CoV-2, Immunization, Passive, COVID-19, Virus Internalization, neutralization, Virology, Antibodies, Neutralizing, Kinetics, chemistry, Solubility, Cell culture, biology.protein, escape, 030217 neurology & neurosurgery

Abstract

The global spread of SARS-CoV-2/COVID-19 is devastating health systems and economies worldwide. Recombinant or vaccine-induced neutralizing antibodies are used to combat the COVID-19 pandemic. However, the recently emerged SARS-CoV-2 variants B.1.1.7 (UK), B.1.351 (South Africa), and P.1 (Brazil) harbor mutations in the viral spike (S) protein that may alter virus-host cell interactions and confer resistance to inhibitors and antibodies. Here, using pseudoparticles, we show that entry of all variants into human cells is susceptible to blockade by the entry inhibitors soluble ACE2, Camostat, EK-1, and EK-1-C4. In contrast, entry of the B.1.351 and P.1 variant was partially (Casirivimab) or fully (Bamlanivimab) resistant to antibodies used for COVID-19 treatment. Moreover, entry of these variants was less efficiently inhibited by plasma from convalescent COVID-19 patients and sera from BNT162b2-vaccinated individuals. These results suggest that SARS-CoV-2 may escape neutralizing antibody responses, which has important implications for efforts to contain the pandemic., Graphical abstract, Comparison of the SARS-CoV-2 variants B.1.1.7, B.1.351, and P.1 shows that inhibitors under clinical evaluation are still effective in blocking entry, though the B.1.351 and P.1 variants evade antibody responses induced upon infection as well as vaccination and evade certain therapeutic antibodies.

Published

2021

34. Structural modeling and analysis of the SARS-CoV-2 cell entry inhibitor camostat bound to the trypsin-like protease TMPRSS2

Author

Diego E. Escalante and David M. Ferguson

Subjects

Camostat, Proteases, Stereochemistry, Structure-based design, Molecular dynamics, 01 natural sciences, chemistry.chemical_compound, Homology modeling, General Pharmacology, Toxicology and Pharmaceutics, TMPRSS2, Original Research, Serine protease, biology, SARS-CoV-2, 010405 organic chemistry, Chemistry, Organic Chemistry, Active site, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, biology.protein, Salt bridge, Oxyanion hole, Pharmacophore

Abstract

The type II transmembrane serine protease TMPRSS2 facilitates the entry of coronaviruses, such as SARS-CoV-2, into host cells by cleaving the S1/S2 interface of the viral spike protein. Based on structural data derived from X-ray crystallographic data of related trypsin-like proteases, a homology model of TMPRSS2 is described and validated using the broad spectrum COVID-19 drug candidate camostat as a probe. Both active site recognition and catalytic function are examined using quantum mechanics/molecular mechanics molecular dynamic (QM/MM MD) simulations of camostat and its active metabolite, 4-(4-guanidinobenzoyloxy) phenylacetate (GBPA). Substrate binding is shown to be primarily stabilized through salt bridge formation between the shared guanidino pharmacophore and D435 in pocket A (flanking the catalytic S441). Based on the binding mode of GBPA, residues K342 and W461 have been identified as potential contacts involved in TMPRSS2 selective binding and activity. Additional data is reported that indicates the transition state structure is stabilized through H-bonding interactions with the backbone N–H groups within an oxyanion hole following bottom-side attack of the carbonyl by S441. This is supported by prior work on related serine proteases suggesting further strategies to exploit in the design of more potent inhibitors. Taken overall, the proposed structure along with the key contact sites and mechanistic features identified should prove highly advantageous to the design and rational development of safe and effective therapeutics that target TMPRSS2 and avoid inhibition of other trypsin-dependent processes.

Published

2021

35. Determination of camostat and its metabolites in human plasma - Preservation of samples and quantification by a validated UHPLC-MS/MS method

Author

Mads Kjolby, Jørgen B. Hasselstrøm, Lambert K. Sørensen, Jesper Damsgaard Gunst, and Ole S. Søgaard

Subjects

Camostat, Isoflurophate, Clinical Biochemistry, Phenylacetic acid, Mass spectrometry, Guanidines, Paraoxon, chemistry.chemical_compound, Hydrolysis, Tandem Mass Spectrometry, medicine, FOY-251, Humans, LC-MS/MS, Enzyme Inhibitors, Chromatography, High Pressure Liquid, Whole blood, Reproducibility, Blood Specimen Collection, Chromatography, FOY-305, SARS-CoV-2, GBPA, Esterases, COVID-19, Reproducibility of Results, Esterase inhibitors, Esters, General Medicine, COVID-19 Drug Treatment, chemistry, GBA, Esterase inhibitor, medicine.drug

Abstract

Objectives Camostat mesilate is a drug that is being repurposed for new applications such as that against COVID-19 and prostate cancer . This induces a need for the development of an analytical method for the quantification of camostat and its metabolites in plasma samples. Camostat is, however, very unstable in whole blood and plasma due to its two ester bonds. The molecule is readily hydrolysed by esterases to 4-(4-guanidinobenzoyloxy)phenylacetic acid (GBPA) and further to 4-guanidinobenzoic acid (GBA). For reliable quantification of camostat, a technique is required that can instantly inhibit esterases when blood samples are collected. Design and methods An ultra-high-performance liquid chromatography-tandem mass spectrometry method (UHPLC-ESI-MS/MS) using stable isotopically labelled analogues as internal standards was developed and validated. Different esterase inhibitors were tested for their ability to stop the hydrolysis of camostat ester bonds. Results Both diisopropylfluorophosphate (DFP) and paraoxon were discovered as efficient inhibitors of camostat metabolism at 10 mM concentrations. No significant changes in camostat and GBPA concentrations were observed in fluoride-citrate-DFP/paraoxon-preserved plasma after 24 h of storage at room temperature or 4 months of storage at −20 °C and −80 °C. The lower limits of quantification were 0.1 ng/mL for camostat and GBPA and 0.2 ng/mL for GBA. The mean true extraction recoveries were greater than 90%. The relative intra-laboratory reproducibility standard deviations were at a maximum of 8% at concentrations of 1–800 ng/mL. The trueness expressed as the relative bias of the test results was within ±3% at concentrations of 1–800 ng/mL. Conclusions A methodology was developed that preserves camostat and GBPA in plasma samples and provides accurate and sensitive quantification of camostat, GBPA and GBA by UHPLC-MS/MS.

Published

2021

36. Interferon alpha-based combinations suppress SARS-CoV-2 infection in vitro and in vivo

Author

Tanel Tenson, Erlend Ravlo, Jaewon Yang, Valentyn Oksenych, Hilde Lysvand, Laura Sandra Lello, Minna Poranen, Anni I Nieminen, Rouan Yao, Astra Vitkauskiene, Sainan Wang, Wei Wang, Marius Trøseid, Pål Aukrust, Andres Merits, Eva Zusinaite, Aleksandr Ianevski, Denis E. Kainov, Nicolas Legrand, Anu Kantele, Eunji Jo, Kirsti Løseth, Gunnveig Grødeland, Mona H. Fenstad, Marc P. Windisch, Magnar Bjørås, and Svein Arne Nordbø

Subjects

Camostat, 0303 health sciences, business.industry, Alpha interferon, Pharmacology, Cycloheximide, In vitro, Virus, 3. Good health, Transcriptome, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Viral replication, chemistry, In vivo, Medicine, business, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

There is an urgent need for new antivirals with powerful therapeutic potential and tolerable side effects. In the present study, we found that recombinant human interferon-alpha (IFNa) triggers intrinsic and extrinsic cellular antiviral responses, as well as reduces replication of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in vitro. Although IFNa alone was insufficient to completely abolish SARS-CoV-2 replication, combinations of IFNa with remdesivir or other antiviral agents (EIDD-2801, camostat, cycloheximide, or convalescent serum) showed strong synergy and effectively inhibited SARS-CoV-2 infection in human lung epithelial Calu-3 cells. Furthermore, we showed that the IFNa-remdesivir combination suppressed virus replication in human lung organoids, and that its single prophylactic dose attenuated SARS-CoV-2 infection in lungs of Syrian hamsters. Transcriptome and metabolomic analyses showed that the combination of IFNa-remdesivir suppressed virus-mediated changes in infected cells, although it affected the homeostasis of uninfected cells. We also demonstrated synergistic antiviral activity of IFNa2a-based combinations against other virus infections in vitro. Altogether, our results indicate that IFNa2a-based combination therapies can achieve higher efficacy while requiring lower dosage compared to monotherapies, making them attractive targets for further pre-clinical and clinical development.

Published

2021

37. A SARS-CoV-2 cytopathicity dataset generated by high-content screening of a large drug repurposing collection

Author

Gerd Geisslinger, Jindrich Cinatl, Oliver Keminer, Sandra Westhaus, Maria Kuzikov, Bernhard Ellinger, Sandra Ciesek, Jeanette Reinshagen, Carsten Claussen, Andrea Zaliani, Denisa Bojkova, Markus Wolf, Philip Gribbon, and Publica

Subjects

Statistics and Probability, Camostat, Drug, Data Descriptor, Science, media_common.quotation_subject, Drug Evaluation, Preclinical, Cetylpyridinium, Library and Information Sciences, medicine.disease_cause, Antiviral Agents, Guanidines, Lopinavir, Education, 03 medical and health sciences, chemistry.chemical_compound, Papaverine, medicine, Humans, 030304 developmental biology, Coronavirus, media_common, 0303 health sciences, SARS-CoV-2, 030306 microbiology, Mefloquine, business.industry, Small molecules, Drug Repositioning, virus diseases, COVID-19, Esters, Virology, Benzamidines, Computer Science Applications, Nafamostat, Drug repositioning, Drug screening, chemistry, Viral infection, High-content screening, Caco-2 Cells, Statistics, Probability and Uncertainty, business, Information Systems, medicine.drug

Abstract

SARS-CoV-2 is a novel coronavirus responsible for the COVID-19 pandemic, in which acute respiratory infections are associated with high socio-economic burden. We applied high-content screening to a well-defined collection of 5632 compounds including 3488 that have undergone previous clinical investigations across 600 indications. The compounds were screened by microscopy for their ability to inhibit SARS-CoV-2 cytopathicity in the human epithelial colorectal adenocarcinoma cell line, Caco-2. The primary screen identified 258 hits that inhibited cytopathicity by more than 75%, most of which were not previously known to be active against SARS-CoV-2 in vitro. These compounds were tested in an eight-point dose response screen using the same image-based cytopathicity readout. For the 67 most active molecules, cytotoxicity data were generated to confirm activity against SARS-CoV-2. We verified the ability of known inhibitors camostat, nafamostat, lopinavir, mefloquine, papaverine and cetylpyridinium to reduce the cytopathic effects of SARS-CoV-2, providing confidence in the validity of the assay. The high-content screening data are suitable for reanalysis across numerous drug classes and indications and may yield additional insights into SARS-CoV-2 mechanisms and potential therapeutic strategies., Measurement(s) cytotoxicity • killing by virus of host cell Technology Type(s) bright-field microscopy Factor Type(s) concentration • incubation time Sample Characteristic - Organism Homo sapiens Machine-accessible metadata file describing the reported data: 10.6084/m9.figshare.13562570

Published

2021

38. Screening of FDA-Approved Drugs Using a MERS-CoV Clinical Isolate from South Korea Identifies Potential Therapeutic Options for COVID-19

Author

Ji-Young Min, So Young Chang, David Shum, Magnar Bjørås, Wei Wang, Erlend Ravlo, Anne-Laure Pham Hung d’Alexandry d’Orengiani, Inhee Choi, Marc P. Windisch, Meehyun Ko, Aleksandr Ianevski, Denis E. Kainov, Soo Young Byun, Institute for Molecular Medicine Finland, and University of Helsinki

Subjects

0301 basic medicine, PNEUMONIA, viruses, severe acute respiratory syndrome coronavirus disease, Drug Evaluation, Preclinical, lcsh:QR1-502, Ciclesonide, Pharmacology, Cardiotonic Agents, medicine.disease_cause, high-content screening, lcsh:Microbiology, chemistry.chemical_compound, clinical isolate, Drug Approval, SYNDROME CORONAVIRUS INFECTION, 11832 Microbiology and virology, Alanine, drug repurposing, virus diseases, Drug Synergism, 3. Good health, Drug repositioning, Infectious Diseases, Coronavirus Infections, Atovaquone, medicine.drug, Camostat, drug combinations, FDA-approved drugs, Middle East respiratory syndrome coronavirus, 030106 microbiology, EAST RESPIRATORY SYNDROME, Antiviral Agents, lung organoids, Article, Small Molecule Libraries, 03 medical and health sciences, Virology, medicine, Animals, Humans, Life Cycle Stages, business.industry, SARS-CoV-2, pandemic, Drug Repositioning, COVID-19, medicine.disease, Adenosine Monophosphate, COVID-19 Drug Treatment, Pneumonia, 030104 developmental biology, Nelfinavir, chemistry, REPLICATION, 3111 Biomedicine, business

Abstract

Therapeutic options for coronaviruses remain limited. To address this unmet medical need, we screened 5406 compounds, including United States Food and Drug Administration (FDA)-approved drugs and bioactives, for activity against a South Korean Middle East respiratory syndrome coronavirus (MERS-CoV) clinical isolate. Among 221 identified hits, 54 had therapeutic indexes (TI) greater than 6, representing effective drugs. The time-of-addition studies with selected drugs demonstrated eight and four FDA-approved drugs which acted on the early and late stages of the viral life cycle, respectively. Confirmed hits included several cardiotonic agents (TI &gt, 100), atovaquone, an anti-malarial (TI &gt, 34), and ciclesonide, an inhalable corticosteroid (TI &gt, 6). Furthermore, utilizing the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), we tested combinations of remdesivir with selected drugs in Vero-E6 and Calu-3 cells, in lung organoids, and identified ciclesonide, nelfinavir, and camostat to be at least additive in vitro. Our results identify potential therapeutic options for MERS-CoV infections, and provide a basis to treat coronavirus disease 2019 (COVID-19) and other coronavirus-related illnesses.

Published

2021

39. Molecular mechanism of inhibiting the SARS-CoV-2 cell entry facilitator TMPRSS2 with camostat and nafamostat

Author

Marc E. Rothenberg, Markus Hoffmann, Nurit P. Azouz, Lluís Raich, Andrea M. Klingler, Tim Hempel, Simon Olsson, Stefan Pöhlmann, and Frank Noé

Subjects

Camostat, Population, camostat, 010402 general chemistry, medicine.disease_cause, 01 natural sciences, 03 medical and health sciences, chemistry.chemical_compound, nafamostat, medicine, education, TMPRSS2, 030304 developmental biology, Coronavirus, 0303 health sciences, education.field_of_study, SARS-CoV-2, Activator (genetics), In vitro toxicology, General Chemistry, In vitro, 3. Good health, 0104 chemical sciences, Nafamostat, chemistry, Covalent bond, Biophysics

Abstract

The entry of the coronavirus SARS-CoV-2 into human lung cells can be inhibited by the approved drugs camostat and nafamostat. Here we elucidate the molecular mechanism of these drugs by combining experiments and simulations. In vitro assays confirm that both drugs inhibit the human protein TMPRSS2, a SARS-Cov-2 spike protein activator. As no experimental structure is available, we provide a model of the TMPRSS2 equilibrium structure and its fluctuations by relaxing an initial homology structure with extensive 330 microseconds of all-atom molecular dynamics (MD) and Markov modeling. Through Markov modeling, we describe the binding process of both drugs and a metabolic product of camostat (GBPA) to TMPRSS2, reaching a Michaelis complex (MC) state, which precedes the formation of a long-lived covalent inhibitory state. We find that nafamostat has a higher MC population than camostat and GBPA, suggesting that nafamostat is more readily available to form the stable covalent enzyme-substrate intermediate, effectively explaining its high potency. This model is backed by our in vitro experiments and consistent with previous virus cell entry assays. Our TMPRSS2-drug structures are made public to guide the design of more potent and specific inhibitors.

Published

2021

40. Unravelling high-affinity binding compounds towards transmembrane protease serine 2 enzyme in treating SARS-CoV-2 infection using molecular modelling and docking studies

Author

Kanipakam Hema, Gangavaram Jyothi Reddy, Bharathi Koganti, Sujatha Dodoala, and M. Pooja

Subjects

0301 basic medicine, Camostat, Models, Molecular, Serine Proteinase Inhibitors, Berberine, Drug repurposing, Computational biology, medicine.disease_cause, Meloxicam, TMPRSS2, Antiviral Agents, Guanidines, 03 medical and health sciences, chemistry.chemical_compound, Lactones, Lanosterol, 0302 clinical medicine, Full Length Article, medicine, Proanthocyanidins, Binding site, ADME, Coronavirus, Flavonoids, Pharmacology, Binding Sites, Chemistry, SARS-CoV-2, Serine Endopeptidases, COVID-19, Transmembrane Protease Serine 2, Benzamidines, COVID-19 Drug Treatment, Drug repositioning, 030104 developmental biology, Docking (molecular), Molecular docking, Flavanones, Homology modelling, Diterpenes, 030217 neurology & neurosurgery, Protein Binding

Abstract

The coronavirus disease-19 (COVID-19) outbreak that is caused by a highly contagious severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) has become a zoonotic pandemic, with approximately 24.5 million positive cases and 8.3 lakhs deaths globally. The lack of effective drugs or vaccine provoked the research for drug candidates that can disrupt the spread and progression of the virus. The identification of drug molecules through experimental studies is time-consuming and expensive, so there is a need for developing alternative strategies like in silico approaches which can yield better outcomes in less time. Herein, we selected transmembrane protease serine 2 (TMPRSS2) enzyme, a potential pharmacological target against SARS-CoV-2, involved in the spread and pathogenesis of the virus. Since 3D structure is not available for this protein, the present study aims at homology modelling and validation of TMPRSS2 using Swiss-model server. Validation of the modelled TMPRSS2 using various online tools confirmed model accuracy, topology and stereochemical plausibility. The catalytic triad consisting of Serine-441, Histidine-296 and Aspartic acid-345 was identified as active binding site of TMPRSS2 using existing ligands. Molecular docking studies of various drugs and phytochemicals against the modelled TMPRSS2 were performed using camostat as a standard drug. The results revealed eight potential drug candidates, namely nafamostat, meloxicam, ganodermanontriol, columbin, myricetin, proanthocyanidin A2, jatrorrhizine and baicalein, which were further studied for ADME/T properties. In conclusion, the study unravelled eight high affinity binding compounds, which may serve as potent antagonists against TMPRSS2 to impact COVID-19 drug therapy., Highlights • 3D structure of TMPRSS2 was constructed using Homology modeling and was validated. • 50 K Ligand was utilized to reveal the active site of modelled TMPRSS2. • A total of twenty-five natural and marketed compounds were studied. • Nafamostatat, Meloxicam, Ganodermanontriol, Columbin, Myricetin, Proanthocyanidin A2, Jatrorrhizine and Baicalein shown good binding energies. • These potent TMPRSS2 inhibitors can prevent spread of SARS-CoV-2, aid in treatment of COVID-19.

Published

2021

41. Targeting androgen regulation of TMPRSS2 and ACE2 as a therapeutic strategy to combat COVID-19

Author

Irfan A. Asangani, Ronnie M. Russell, Reyaz ur Rasool, Ramakrishnan Natesan, and Qu Deng

Subjects

S priming, 0301 basic medicine, Camostat, medicine.drug_class, ACE2, 02 engineering and technology, Androgen deprivation therapy, urologic and male genital diseases, TMPRSS2, Article, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, Prostate, Virology, Transcriptional regulation, Medicine, Enzalutamide, Androgen Receptor Antagonists, Receptor, lcsh:Science, Molecular Biology, Multidisciplinary, business.industry, COVID-19, Institutional Animal Care and Use Committee, Transcription regulation, Biological Sciences, 021001 nanoscience & nanotechnology, Androgen, medicine.disease, Androgen receptor, medicine.anatomical_structure, 030104 developmental biology, chemistry, SARS-CoV-2 Spike, Androgen Receptor, Cancer research, lcsh:Q, Cytokine storm, 0210 nano-technology, business

Abstract

Epidemiological data showing increased severity and mortality of COVID-19 in men suggests a potential role for androgen in SARS-CoV-2 infection. Here, we present evidence for the transcriptional regulation of SARS-CoV-2 host cell receptor ACE2 and TMPRSS2 by androgen in mouse and human cells. Additionally, we demonstrate the endogenous interaction between TMPRSS2 and ACE2 in human cells and validate ACE2 as a TMPRSS2 substrate. Further, Camostat – a TMPRSS2 inhibitor, blocked the cleavage of pseudotype SARS-CoV-2 surface Spike without disrupting TMPRSS2-ACE2 interaction. Thus providing evidence for the first time a direct role of TMPRSS2 in priming the SARS-CoV-2 Spike, required for viral fusion to the host cell. Importantly, androgen-deprivation, anti-androgens, or Camostat attenuated the SARS-CoV-2 S-mediated cellular entry. Together, our data provide a strong rationale for clinical evaluations of TMPRSS2 inhibitors, androgen-deprivation therapy/androgen receptor antagonists alone or in combination with antiviral drugs as early as clinically possible to prevent COVID-19 progression., Graphical Abstract

Published

2020

42. Potential therapeutic and pharmacological strategies for SARS-CoV2

Author

Salma A Soudi, Abdulaziz Mohsen Al-mahallawi, Miral G Abd El-Wahab, Marwa Y. Kenawy, Jaillan G Sery, Alshimaa A Abd Elmoneam, Ahmed A Sobhy, Maha A. El-Demellawy, Mohamed M Y Kaddah, Aliaa A Masoud, Inas K Seif, Doaa A. Ghareeb, Mohammed S Nofal, Samar R. Saleh, Salma F Hassan, Shaimaa M Khedr, and Sally A. El-Zahaby

Subjects

medicine.drug_class, Antibiotics, Indomethacin, Pharmaceutical Science, 02 engineering and technology, Review, 010402 general chemistry, 01 natural sciences, Virus, chemistry.chemical_compound, Tocilizumab, Camostat, Pandemic, medicine, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), business.industry, Mortality rate, COVID-19, Hydroxychloroquine, 021001 nanoscience & nanotechnology, 0104 chemical sciences, Drug repositioning, chemistry, Immunology, Teicoplanin, 0210 nano-technology, business, Magic bullet, medicine.drug

Abstract

Background At the end of 2019, the new Coronavirus disease 2019 (COVID-19) strain causing severe acute respiratory syndrome swept the world. From November 2019 till February 2021, this virus infected nearly 104 million, with more than two million deaths and about 25 million active cases. This has prompted scientists to discover effective drugs to combat this pandemic. Area covered Drug repurposing is the magic bullet for treating severe acute respiratory syndrome coronavirus 2 (SARS-CoV2). Therefore, several drugs have been investigated in silico, in vitro, as well as through human trials such as anti-SARS-CoV2 agents, or to prevent the complications resulting from the virus. In this review, the mechanisms of action of different therapeutic strategies are summarized. According to the WHO, different classes of drugs can be used, including anti-malarial, antiviral, anti-inflammatory, and anti-coagulant drugs, as well as angiotensin-converting enzyme inhibitors, antibiotics, vitamins, zinc, neutralizing antibodies, and convalescent plasma therapy. Recently, there are some vaccines which are approved against SARS-CoV2. Expert opinion A complete understanding of the structure and function of all viral proteins that play a fundamental role in viral infection, which contribute to the therapeutic intervention and the development of vaccine in order to reduce the mortality rate. Supplementary Information The online version contains supplementary material available at 10.1007/s40005-021-00520-4.

Published

2020

43. Furin Inhibitors Block SARS-CoV-2 Spike Protein Cleavage to Suppress Virus Production and Cytopathic Effects

Author

Chih Hui Lin, Han Chieh Kao, Tung Ching Ho, Shiou-Hwei Yeh, Sui-Yuan Chang, Wen Hau Lee, Mi-Hua Tao, Yu Hao Pang, Chiao Ling Li, Ya-Wen Cheng, Sheng-Han Wang, Li Ting Jang, Tai Ling Chao, Ping-Yi Wu, Pei-Jer Chen, Mu Fan Chiu, and Ya Min Tsai

Subjects

0301 basic medicine, Camostat, Proteases, viruses, Biology, Cleavage (embryo), Virus Replication, Antiviral Agents, Virus, General Biochemistry, Genetics and Molecular Biology, Article, cytopathic effect, Amino Acid Chloromethyl Ketones, 03 medical and health sciences, chemistry.chemical_compound, Betacoronavirus, 0302 clinical medicine, Viral entry, Chlorocebus aethiops, Animals, Humans, Protease Inhibitors, Furin, Vero Cells, Cytopathic effect, Syncytium, SARS-CoV-2, virus diseases, spike, Fluoresceins, Transmembrane Protease Serine 2, Virology, Cell biology, 030104 developmental biology, chemistry, Proteolysis, Spike Glycoprotein, Coronavirus, biology.protein, furin, 030217 neurology & neurosurgery, syncytium

Abstract

Development of specific antivirals is an urgent unmet need for SARS-coronavirus 2 (SARS-CoV-2) infections. This study focuses on host proteases that proteolytically activate the SARS-CoV-2 spike protein, critical for its fusion after binding to angiotensin-converting enzyme 2 (ACE2), as antiviral targets. We first validated cleavage at a putative furin substrate motif at SARS-CoV-2 spike by expressing it in VeroE6 cells and found prominent syncytium formation. Both cleavage and syncytium were abolished by treatment with furin inhibitors decanoyl-RVKR-chloromethylketone (CMK) and naphthofluorescein but not by transmembrane protease serine 2 (TMPRSS2) inhibitor camostat. CMK and naphthofluorescein showed antiviral effects in SARS-CoV-2-infected cells by decreasing viral production and cytopathic effects. Further analysis revealed that, similar to camostat, CMK blocks virus entry, but it further suppresses the cleavage of spike and syncytium. Naphthofluorescein instead acts primarily by suppressing viral RNA transcription. Therefore, furin inhibitors may become promising antivirals for prevention and treatment of SARS-CoV-2 infections., Graphical Abstract, Highlights ● The furin cleavage site in the SARS-CoV-2 spike protein mediates syncytium formation. ● The SARS-CoV-2 spike-mediated syncytium is suppressed by specific furin inhibitors. ● Furin inhibitors block SARS-CoV-2 viral entry and viral replication. ● Furin inhibitors are potential antivirals for SARS-CoV-2 infection and pathogenesis., Development of effective antivirals is an urgent unmet need for SARS-CoV-2 infections. Cheng et al. find that the cleavage of the furin substrate site in the viral spike protein is critical for viral production and cytopathic effects. Two inhibitors targeting furin are potential antivirals to control SARS-CoV-2 infection and pathogenesis.

Published

2020

44. Human Embryonic Stem Cell-derived Lung Organoids: a Model for SARS-CoV-2 Infection and Drug Test

Author

Xinwen Chen, Yecheng Zhang, Lian Li, Rongjuan Pei, Zhili Rong, Shuqi Xiao, Jiekai Chen, Xuejie Yang, Jiangping He, Ying Lin, Hao Sun, Kun Wen, Hongwei Zhou, Jianqi Feng, and Jin Xiong

Subjects

Camostat, Programmed cell death, Lung, respiratory system, Biology, Embryonic stem cell, Virus, Cell biology, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Cell culture, Cancer cell, medicine, Organoid

Abstract

The coronavirus disease 2019 (COVID-19) pandemic is caused by infection with the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), which is spread primary via respiratory droplets and infects the lungs. Currently widely used cell lines and animals are unable to accurately mimic human physiological conditions because of the abnormal status of cell lines (transformed or cancer cells) and species differences between animals and humans. Organoids are stem cell-derived self-organized three-dimensional culturein vitroand model the physiological conditions of natural organs. Here we demonstrated that SARS-CoV-2 infected and extensively replicated in human embryonic stem cells (hESCs)-derived lung organoids, including airway and alveolar organoids. Ciliated cells, alveolar type 2 (AT2) cells and rare club cells were virus target cells. Electron microscopy captured typical replication, assembly and release ultrastructures and revealed the presence of viruses within lamellar bodies in AT2 cells. Virus infection induced more severe cell death in alveolar organoids than in airway organoids. Additionally, RNA-seq revealed early cell response to SARS-CoV-2 infection and an unexpected downregulation of ACE2 mRNA. Further, compared to the transmembrane protease, serine 2 (TMPRSS2) inhibitor camostat, the nucleotide analog prodrug Remdesivir potently inhibited SARS-CoV-2 replication in lung organoids. Therefore, human lung organoids can serve as a pathophysiological model for SARS-CoV-2 infection and drug discovery.

Published

2020

45. Sex Hormones and Hormone Therapy during COVID-19 Pandemic: Implications for Patients with Cancer

Author

Giacomo Vallome, Maria Maddalena Latocca, Francesco Boccardo, Benedetta Conte, Carlo Cattrini, and Melissa Bersanelli

Subjects

0301 basic medicine, Cancer Research, Bicalutamide, medicine.medical_treatment, ACE2, COVID-19, SARS-CoV-2, TMPRSS2, androgen-deprivation therapy, androgens, camostat, estrogens, progesterone, tamoxifen, testosterone, Bioinformatics, lcsh:RC254-282, Androgen deprivation therapy, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, 0302 clinical medicine, medicine, Enzalutamide, Testosterone, business.industry, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, Perspective, Hormone therapy, business, Tamoxifen, Hormone, medicine.drug

Abstract

The novel coronavirus disease 2019 (COVID-19) shows a wide spectrum of clinical presentations, severity, and fatality rates. The reason older patients and males show increased risk of severe disease and death remains uncertain. Sex hormones, such as estradiol, progesterone, and testosterone, might be implicated in the age-dependent and sex-specific severity of COVID-19. High testosterone levels could upregulate transmembrane serine protease 2 (TMPRSS2), facilitating the entry of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) into host cells via angiotensin-converting enzyme 2 (ACE2). Data from patients with prostate cancer treated with androgen-deprivation therapy seem to confirm this hypothesis. Clinical studies on TMPRSS2 inhibitors, such as camostat, nafamostat, and bromhexine, are ongoing. Antiandrogens, such as bicalutamide and enzalutamide, are also under investigation. Conversely, other studies suggest that the immune modulating properties of androgens could protect from the unfavorable cytokine storm, and that low testosterone levels might be associated with a worse prognosis in patients with COVID-19. Some evidence also supports the notion that estrogens and progesterone might exert a protective effect on females, through direct antiviral activity or immune-mediated mechanisms, thus explaining the higher COVID-19 severity in post-menopausal women. In this perspective, we discuss the available evidence on sex hormones and hormone therapy in patients infected with SARS-CoV-2, and we highlight the possible implications for cancer patients, who can receive hormonal therapies during their treatment plans.

Published

2020

46. Molecular mechanism of SARS-CoV-2 cell entry inhibition via TMPRSS2 by Camostat and Nafamostat mesylate

Author

Tim Hempel, Lluís Raich, Simon Olsson, Nurit P. Azouz, Andrea M. Klingler, Marc E. Rothenberg, and Frank Noé

Subjects

Camostat, education.field_of_study, Chemistry, Population, In vitro toxicology, medicine.disease_cause, In vitro, Virus, Nafamostat, chemistry.chemical_compound, Covalent bond, medicine, Biophysics, education, Coronavirus

Abstract

The entry of the coronavirus SARS-CoV-2 into human cells can be inhibited by the approved drugs camostat and nafamostat. Here we elucidate the molecular mechanism of these drugs by combining experiments and simulations.In vitroassays confirm the hypothesis that both drugs act by inhibiting the human protein TMPRSS2. As no experimental structure is available, we provide a model of the TMPRSS2 equilibrium structure and its fluctuations by relaxing an initial homology structure with extensive 280 microseconds of all-atom molecular dynamics (MD) and Markov modeling. We describe the binding mode of both drugs with TMPRSS2 in a Michaelis complex (MC) state preceding the formation of a long-lived covalent inhibitory state. We find that nafamostat to has a higher MC population, which in turn leads to the more frequent formation of the covalent complex and thus higher inhibition efficacy, as confirmedin vitroand consistent with previous virus cell entry assays. Our TMPRSS2-drug structures are made public to guide the design of more potent and specific inhibitors.

Published

2020

47. An Enzymatic TMPRSS2 Assay for Assessment of Clinical Candidates and Discovery of Inhibitors as Potential Treatment of COVID-19

Author

Philip E. Sanderson, Anton Simeonov, Jonathan H. Shrimp, Matthew D. Hall, Stephen C. Kales, and Min Shen

Subjects

Pharmacology, Camostat, Proteases, Protease, drug repurposing, COVID19, High-throughput screening, medicine.medical_treatment, Metabolite, antiviral, high-throughput screening, Article, law.invention, Drug repositioning, chemistry.chemical_compound, Nafamostat, chemistry, law, Viral entry, Gabexate, medicine, Recombinant DNA, Pharmacology (medical), TMPRSS2

Abstract

SARS-CoV-2 is the viral pathogen causing the COVID19 global pandemic. Consequently, much research has gone into the development of pre-clinical assays for the discovery of new or repurposing of FDA-approved therapies. Preventing viral entry into a host cell would be an effective antiviral strategy. One mechanism for SARS-CoV-2 entry occurs when the spike protein on the surface of SARS-CoV-2 binds to an ACE2 receptor followed by cleavage at two cut sites (“priming”) that causes a conformational change allowing for viral and host membrane fusion. This fusion event is proceeded by release of viral RNA within the host cell. TMPRSS2 has an extracellular protease domain capable of cleaving the spike protein to initiate membrane fusion. Additionally, knock-out studies in mice have demonstrated reduced infection in the absence of TMPRSS2 with no detectable physiological impact; thus, TMPRSS2 is an attractive target for therapeutic development. A validated inhibitor of TMPRSS2 protease activity would be a valuable tool for studying the impact TMPRSS2 has in viral entry and potentially be an effective antiviral therapeutic. To enable inhibitor discovery and profiling of FDA-approved therapeutics, we describe an assay for the biochemical screening of recombinant TMPRSS2 suitable for high throughput application. We demonstrate effectiveness to quantify inhibition down to subnanomolar concentrations by assessing the inhibition of camostat, nafamostat and gabexate, clinically approved agents in Japan for pancreatitis due to their inhibition of trypsin-like proteases. Nafamostat and camostat are currently in clinical trials against COVID19. The rank order potency for the three inhibitors is: nafamostat (IC50 = 0.27 nM), camostat (IC50 = 6.2 nM) and gabexate (IC50 = 130 nM). Further profiling of these three inhibitors against a panel of proteases provides insight into selectivity and potency.

Published

2020

48. Camostat in COVID-19

Author

Mohini Basu and Chinmoy K Bose

Subjects

Camostat, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), business.industry, Hydroxychloroquine, General Medicine, medicine.disease, Gastroenterology, Pathogenesis, chemistry.chemical_compound, chemistry, Internal medicine, medicine, Acute pancreatitis, business, Esophagitis, medicine.drug

Published

2020

49. Generation of human bronchial organoids for SARS-CoV-2 research

Author

Akatsuki Saito, Daisuke Okuzaki, Takuya Yamamoto, Shohei Minami, Takeshi Kobayashi, Daisuke Motooka, Yumi Ito, Tatsuya Suzuki, Toru Okamoto, Yusuke Sakai, and Kazuo Takayama

Subjects

Camostat, Serine protease, viruses, Biology, TMPRSS2, Virology, Virus, Serine, chemistry.chemical_compound, Viral life cycle, chemistry, Interferon, medicine, biology.protein, Receptor, medicine.drug

Abstract

Coronavirus disease 2019 (COVID-19) is a disease that causes fatal disorders including severe pneumonia. To develop a therapeutic drug for COVID-19, a model that can reproduce the viral life cycle and evaluate the drug efficacy of anti-viral drugs is essential. In this study, we established a method to generate human bronchial organoids (hBO) from commercially available cryopreserved human bronchial epithelial cells and examined whether they could be used as a model for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) research. Our hBO contain basal, club, ciliated, and goblet cells. Angiotensin-converting enzyme 2 (ACE2), which is a receptor for SARS-CoV-2, and transmembrane serine proteinase 2 (TMPRSS2), which is an essential serine protease for priming spike (S) protein of SARS-CoV-2, were highly expressed. After SARS-CoV-2 infection, not only the intracellular viral genome, but also progeny virus, cytotoxicity, pyknotic cells, and moderate increases of the type I interferon signal could be observed. Treatment with camostat, an inhibitor of TMPRSS2, reduced the viral copy number to 2% of the control group. Furthermore, the gene expression profile in SARS-CoV-2-infected hBO was obtained by performing RNA-seq analysis. In conclusion, we succeeded in generating hBO that can be used for SARS-CoV-2 research and COVID-19 drug discovery.Graphical abstract

Published

2020

50. Targeting host cell proteases to prevent SARS-CoV-2 invasion

Author

Amit Singh, Luciano Saso, Bisweswar Ojha, Bhairav Kumar Pathak, Upinder Kaur, Sasanka Chakrabarti, and Sankha Shubhra Chakrabarti

Subjects

Camostat, Proteases, Serine Proteinase Inhibitors, viruses, Clinical Biochemistry, Pharmacology, Antiviral Agents, 030226 pharmacology & pharmacy, Virus, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Viral entry, Drug Discovery, Humans, Medicine, Aprotinin, Furin, Cathepsin, Clinical Trials as Topic, biology, SARS-CoV-2, business.industry, Serine Endopeptidases, Drug Repositioning, COVID-19, Virus Internalization, Nafamostat, chemistry, 030220 oncology & carcinogenesis, Spike Glycoprotein, Coronavirus, biology.protein, Molecular Medicine, Angiotensin-Converting Enzyme 2, proteases, SARS-CoV, pharmacology, business, medicine.drug

Abstract

Severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) has spread worldwide and caused widespread devastation. In the absence of definitive therapy, symptomatic management remains the standard of care. Repurposing of many existing drugs, including several anti-viral drugs, is being attempted to tackle the COVID-19 pandemic. However, most of them have failed to show significant benefit in clinical trials. An attractive approach may be to target host proteases involved in SARS-CoV-2 pathogenesis. The priming of the spike (S) protein of the virus by proteolytic cleavage by the transmembrane serine protease-2 (TMPRSS2) is necessary for the fusion of the virus to the host cell after it binds to its receptor angiotensin converting enzyme-2 (ACE2). There are other proteases with varying spatiotemporal locations that may be important for viral entry and subsequent replication inside the cells, and these include trypsin, furin and cathepsins. In this report, we have discussed the tentative therapeutic role of inhibitors of TMPRSS2, cathepsin, trypsin, furin, plasmin, factor X and elastase in infection caused by SARS-CoV-2. Both available evidence, as well as hypotheses, are discussed, with emphasis on drugs which are approved for other indications such as bromhexine, ammonium chloride, nafamostat, camostat, tranexamic acid, epsilon amino-caproic acid, chloroquine, ulinastatin, aprotinin and anticoagulant drugs. Simultaneously, novel compounds being tested and problems with using these agents are also discussed.

Published

2020