Applying polypharmacology approach for drug repurposing for SARS-CoV2

Jamir, Esther; Sarma, Himakshi; Priyadarsinee, Lipsa; Nagamani, Selvaraman; Kiewhuo, Kikrusenuo; Gaur, Anamika Singh; Rawal, Ravindra K.; Murugan, N.; Subramanian, V.; Sastry, G. Narahari

doi:10.1007/s12039-022-02046-0

Cited by 14 publications

(17 citation statements)

References 76 publications

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“…The docking data suggests that neither GRL-0617 or DDL-701 (Figure 5A and B, respectively) interacts with the active site cysteine-111 residue, but rather are bound to the site around tyrosine-268 which lies outside the tunnel containing the active site residue Cys111. DDL-715 and the reported PL pro inhibitor losartan [22] bind the enzyme similarly to DDL-701, at the site around Tyr268 and at the entrance of the active site tunnel leading to Cys111 (Supplementary Figures S3 and S5, respectively).…”

Section: Modeling and Docking Reveal Ddl-701 And Known Pl Pro Inhibit...mentioning

confidence: 94%

“…Recent studies suggest that the virus could develop resistance to nirmatrelvir through development of mutations in the protease M pro , a phenomenon observed with many antiviral drugs [18,19]. This has raised interest in the development of protease inhibitor cocktail therapy for SARS-CoV-2 [20][21][22][23][24][25][26][27] to increase efficacy and reduce the risk of rebound, which is modeled on the use of protease cocktails for the treatment of HIV and hepatitis C. Use of a protease inhibitor cocktail could help reduce or prevent resistance by making it harder for the virus to evolve around multiple inhibitors.…”

Section: Introductionmentioning

confidence: 99%

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Identification of a Papain-Like Protease Inhibitor with Potential for Repurposing in Combination with an M^pro Protease Inhibitor for Treatment of SARS-CoV-2

Campagna

Jagodzinska

Alvarez

et al. 2022

Preprint

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SARS-CoV-2 requires two cysteine proteases for viral polypeptide processing to allow maturation and replication: the 3C-like protease also known as the Main protease (Mpro) and the papain-like protease (PLpro). In addition to its critical role in viral replication, PLpro removes post-translational modifications like ubiquitin and interferon-stimulated gene product 15 (ISG15) from host proteins through its deubiquitinase domain, leading to host immunosuppression and increased ability of the virus to evade the host antiviral immune response. Through screening of a custom clinical compound library, we identified eltrombopag (DDL-701), a thrombopoietin receptor agonist, as having PLpro inhibitory activity that is sustained in the presence of the Mpro inhibitor nirmatrelvir. DDL-701 also suppressed both the deubiquitinase and ISG15 cleavage activities of PLpro. In addition, DDL-701 partially restored interferon-β induction – an element of the host immune response - in an in vitro model system. Further, modeling and docking studies suggest DDL-701 interacts with the active site region of the PLpro enzyme and pilot pharmacokinetic studies indicate it is brain permeable. DDL-701 is already approved for treatment of thrombocytopenia and has previously been shown to achieve human plasma levels after oral dosing that is above the IC50 needed for it to exert its PLpro inhibitory activity in vivo. In addition, it has also been reported to have antiviral efficacy against SARS-CoV-2. DDL-701 thus represents a drug that can immediately be repurposed and undergo clinical evaluation as a PLpro inhibitor that may be most effectively used in a protease inhibitor cocktail with an Mpro inhibitor such as nirmatrelvir (Paxlovid) for the treatment of COVID-19.

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Section: Modeling and Docking Reveal Ddl-701 And Known Pl Pro Inhibit...mentioning

confidence: 94%

Section: Introductionmentioning

confidence: 99%

Identification of a Papain-Like Protease Inhibitor with Potential for Repurposing in Combination with an M^pro Protease Inhibitor for Treatment of SARS-CoV-2

Campagna

Jagodzinska

Alvarez

et al. 2022

Preprint

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“…Redocking studies were executed to validate the compounds showing the best binding energy obtained by blind docking. We analyzed the active site residues of all three targets from available literature [ 23 , 24 ] and performed individual ligand docking and MLSD with the above protocol [ 25 , 26 ]. The best poses were selected based on maximum interactions depicted for minimum binding energy conformations, and these interactions between protein–ligand complexes were then visualized using the Discovery studio software.…”

Section: Methodsmentioning

confidence: 99%

Computational screening for investigating the synergistic regulatory potential of drugs and phytochemicals in combination with 2-deoxy-D-glucose against SARS-CoV-2

et al. 2022

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COVID-19 disease caused by Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) was declared a global pandemic by the World Health Organization (WHO) in March 2020. Since then, the SARS-CoV-2 virus has impacted millions of lives worldwide. Various preclinical and clinical trials on the treatment of COVID-19 disease have revealed that the drugs that work in combination are more likely to reduce reinfection and multi-organ failure. Considering the combination drug therapy, herein, we performed a systematic computational study starting with the formation of sixty-two combinations of drugs and phytochemicals with 2-deoxy-D-glucose (2-DG). The top nineteen combinations resulting from Drug-Drug Interaction (DDI) analysis were selected for individual and multiple-ligand-simultaneous docking (MLSD) study with a host target Serine Protease (TMPRSS2; PDB ID: 7MEQ) and two viral targets, Main Protease (3CLpro; PDB ID: 6LU7) and Uridylate-Specific Endoribonuclease (NSP15; PDB ID: 6VWW). We found that the resulting drugs and phytochemicals in combination with 2-DG shows better binding than the individual compounds. We performed the re-docking of the top three drug combinations by utilizing the polypharmacology approach to validate the binding patterns of drug combinations with multiple targets for verifying the best drug combinatorial output obtained by blind docking. A strong binding affinity pattern was observed for 2-DG + Ruxolitinib (NIH-recommended drug), 2-DG + Telmisartan (phase 4 clinical trial drug), and 2-DG + Punicalagin (phytochemical) for all the selected targets. Additionally, we conducted multiple-ligand-simultaneous molecular dynamics (MLS-MD) simulations on the selected targets with the 2-DG + Ruxolitinib combination. The MLS-MD analysis of the drug combinations shows that stabilization of the interaction complexes could have significant inhibition potential against SARS CoV-2. This study provides an insight into developing drug combinations utilizing integrated computational approaches to uncover their potential in synergistic drug therapy. Supplementary Information The online version contains supplementary material available at 10.1007/s11224-022-02049-0.

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“…Several studies have reported that dihydroergotamine and ergotamine are having stable interactions with 3CL pro and also it has the polpypharmacology e cacy [46]. In addition, the drugs tirilazad and venetoclax was reported to show stable binding a nity towards multiple targets for SARS-CoV2 which indicates their polypharmacology property suggesting them as potential candidate for drug repurposing [35,47].…”

Section: Analysis Of Drug Molecules In the Active And Inactive Datasetmentioning

confidence: 99%

“…Four drugs (i.e., venetoclax, tirilazad, acetyldigitoxin, and ledipasvir) were chosen based on the docking scores, binding pose and the interaction pattern with the SARS-CoV2 targets [35]. In arriving at the drug repurposing a consensus scoring approach has been adopted [36].…”

Section: Introductionmentioning

confidence: 99%

A structure-based drug repurposing approach by considering the twenty four SARS-CoV2 Targets: A consensus scoring approach

Jamir

Sarma

Priyadarsinee

et al. 2022

Preprint

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Drug repurposing is emerging as a vital approach for identifying known drugs with potential therapeutic indications for COVID-19 disease. This aims to categorize and develop therapeutics by identifying existing approved drugs from drug libraries that can effectively reduce drug development time, cost and safety risk. In the current study, virtual screening of known drugs has been carried out against 24 proteins of SARS-CoV2 (NSP1-NSP16, envelope, membrane, nucleoprotein, spike, ORF3a, ORF6, ORF7a, ORF8, and ORF9b). A total of 4193 approved drugs were screened against these targets using AutoDock Vina. The drugs were classified into active and inactive molecules based on the threshold value of the docking score and the therapeutic indications of top 10 and bottom 10 drugs were analyzed in detail. From the study, it was observed that most of the active drugs have antiviral, antibacterial, anticancer, pain and central nervous system based therapeutic properties. The inactive compounds mainly fall in the categories of anti-depressive, vitamin deficiency molecules, and also antiseptics properties. Overall, the outcome of this study will help in identifying the groups of drugs or scaffold that may have activity against COVID-19 targets.

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Applying polypharmacology approach for drug repurposing for SARS-CoV2

Cited by 14 publications

References 76 publications

Identification of a Papain-Like Protease Inhibitor with Potential for Repurposing in Combination with an M^pro Protease Inhibitor for Treatment of SARS-CoV-2

Identification of a Papain-Like Protease Inhibitor with Potential for Repurposing in Combination with an M^pro Protease Inhibitor for Treatment of SARS-CoV-2

Computational screening for investigating the synergistic regulatory potential of drugs and phytochemicals in combination with 2-deoxy-D-glucose against SARS-CoV-2

A structure-based drug repurposing approach by considering the twenty four SARS-CoV2 Targets: A consensus scoring approach

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Applying polypharmacology approach for drug repurposing for SARS-CoV2

Cited by 14 publications

References 76 publications

Identification of a Papain-Like Protease Inhibitor with Potential for Repurposing in Combination with an Mpro Protease Inhibitor for Treatment of SARS-CoV-2

Identification of a Papain-Like Protease Inhibitor with Potential for Repurposing in Combination with an Mpro Protease Inhibitor for Treatment of SARS-CoV-2

Computational screening for investigating the synergistic regulatory potential of drugs and phytochemicals in combination with 2-deoxy-D-glucose against SARS-CoV-2

A structure-based drug repurposing approach by considering the twenty four SARS-CoV2 Targets: A consensus scoring approach

Contact Info

Product

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Identification of a Papain-Like Protease Inhibitor with Potential for Repurposing in Combination with an M^pro Protease Inhibitor for Treatment of SARS-CoV-2

Identification of a Papain-Like Protease Inhibitor with Potential for Repurposing in Combination with an M^pro Protease Inhibitor for Treatment of SARS-CoV-2