Structural Elucidation of Rift Valley Fever Virus L Protein towards the Discovery of Its Potential Inhibitors

Rift valley fever virus (RVFV) is the causative agent of a viral zoonosis that causes a significant clinical burden in domestic and wild ruminants. Major outbreaks of the virus occur in livestock, and contaminated animal products or arthropod vectors can transmit the virus to humans. The viral RNA-d...

Descripción completa

Detalles Bibliográficos
Autores principales: Alamri, Mubarak A., Mirza, Muhammad Usman, Adeel, Muhammad Muzammal, Ashfaq, Usman Ali, Tahir ul Qamar, Muhammad, Shahid, Farah, Ahmad, Sajjad, Alatawi, Eid A., Albalawi, Ghadah M., Allemailem, Khaled S., Almatroudi, Ahmad
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9228520/
https://www.ncbi.nlm.nih.gov/pubmed/35745579
http://dx.doi.org/10.3390/ph15060659
_version_ 1784734498956509184
author Alamri, Mubarak A.
Mirza, Muhammad Usman
Adeel, Muhammad Muzammal
Ashfaq, Usman Ali
Tahir ul Qamar, Muhammad
Shahid, Farah
Ahmad, Sajjad
Alatawi, Eid A.
Albalawi, Ghadah M.
Allemailem, Khaled S.
Almatroudi, Ahmad
author_facet Alamri, Mubarak A.
Mirza, Muhammad Usman
Adeel, Muhammad Muzammal
Ashfaq, Usman Ali
Tahir ul Qamar, Muhammad
Shahid, Farah
Ahmad, Sajjad
Alatawi, Eid A.
Albalawi, Ghadah M.
Allemailem, Khaled S.
Almatroudi, Ahmad
author_sort Alamri, Mubarak A.
collection PubMed
description Rift valley fever virus (RVFV) is the causative agent of a viral zoonosis that causes a significant clinical burden in domestic and wild ruminants. Major outbreaks of the virus occur in livestock, and contaminated animal products or arthropod vectors can transmit the virus to humans. The viral RNA-dependent RNA polymerase (RdRp; L protein) of the RVFV is responsible for viral replication and is thus an appealing drug target because no effective and specific vaccine against this virus is available. The current study reported the structural elucidation of the RVFV-L protein by in-depth homology modeling since no crystal structure is available yet. The inhibitory binding modes of known potent L protein inhibitors were analyzed. Based on the results, further molecular docking-based virtual screening of Selleckchem Nucleoside Analogue Library (156 compounds) was performed to find potential new inhibitors against the RVFV L protein. ADME (Absorption, Distribution, Metabolism, and Excretion) and toxicity analysis of these compounds was also performed. Besides, the binding mechanism and stability of identified compounds were confirmed by a 50 ns molecular dynamic (MD) simulation followed by MM/PBSA binding free energy calculations. Homology modeling determined a stable multi-domain structure of L protein. An analysis of known L protein inhibitors, including Monensin, Mycophenolic acid, and Ribavirin, provide insights into the binding mechanism and reveals key residues of the L protein binding pocket. The screening results revealed that the top three compounds, A-317491, Khasianine, and VER155008, exhibited a high affinity at the L protein binding pocket. ADME analysis revealed good pharmacodynamics and pharmacokinetic profiles of these compounds. Furthermore, MD simulation and binding free energy analysis endorsed the binding stability of potential compounds with L protein. In a nutshell, the present study determined potential compounds that may aid in the rational design of novel inhibitors of the RVFV L protein as anti-RVFV drugs.
format Online
Article
Text
id pubmed-9228520
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-92285202022-06-25 Structural Elucidation of Rift Valley Fever Virus L Protein towards the Discovery of Its Potential Inhibitors Alamri, Mubarak A. Mirza, Muhammad Usman Adeel, Muhammad Muzammal Ashfaq, Usman Ali Tahir ul Qamar, Muhammad Shahid, Farah Ahmad, Sajjad Alatawi, Eid A. Albalawi, Ghadah M. Allemailem, Khaled S. Almatroudi, Ahmad Pharmaceuticals (Basel) Article Rift valley fever virus (RVFV) is the causative agent of a viral zoonosis that causes a significant clinical burden in domestic and wild ruminants. Major outbreaks of the virus occur in livestock, and contaminated animal products or arthropod vectors can transmit the virus to humans. The viral RNA-dependent RNA polymerase (RdRp; L protein) of the RVFV is responsible for viral replication and is thus an appealing drug target because no effective and specific vaccine against this virus is available. The current study reported the structural elucidation of the RVFV-L protein by in-depth homology modeling since no crystal structure is available yet. The inhibitory binding modes of known potent L protein inhibitors were analyzed. Based on the results, further molecular docking-based virtual screening of Selleckchem Nucleoside Analogue Library (156 compounds) was performed to find potential new inhibitors against the RVFV L protein. ADME (Absorption, Distribution, Metabolism, and Excretion) and toxicity analysis of these compounds was also performed. Besides, the binding mechanism and stability of identified compounds were confirmed by a 50 ns molecular dynamic (MD) simulation followed by MM/PBSA binding free energy calculations. Homology modeling determined a stable multi-domain structure of L protein. An analysis of known L protein inhibitors, including Monensin, Mycophenolic acid, and Ribavirin, provide insights into the binding mechanism and reveals key residues of the L protein binding pocket. The screening results revealed that the top three compounds, A-317491, Khasianine, and VER155008, exhibited a high affinity at the L protein binding pocket. ADME analysis revealed good pharmacodynamics and pharmacokinetic profiles of these compounds. Furthermore, MD simulation and binding free energy analysis endorsed the binding stability of potential compounds with L protein. In a nutshell, the present study determined potential compounds that may aid in the rational design of novel inhibitors of the RVFV L protein as anti-RVFV drugs. MDPI 2022-05-25 /pmc/articles/PMC9228520/ /pubmed/35745579 http://dx.doi.org/10.3390/ph15060659 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Alamri, Mubarak A.
Mirza, Muhammad Usman
Adeel, Muhammad Muzammal
Ashfaq, Usman Ali
Tahir ul Qamar, Muhammad
Shahid, Farah
Ahmad, Sajjad
Alatawi, Eid A.
Albalawi, Ghadah M.
Allemailem, Khaled S.
Almatroudi, Ahmad
Structural Elucidation of Rift Valley Fever Virus L Protein towards the Discovery of Its Potential Inhibitors
title Structural Elucidation of Rift Valley Fever Virus L Protein towards the Discovery of Its Potential Inhibitors
title_full Structural Elucidation of Rift Valley Fever Virus L Protein towards the Discovery of Its Potential Inhibitors
title_fullStr Structural Elucidation of Rift Valley Fever Virus L Protein towards the Discovery of Its Potential Inhibitors
title_full_unstemmed Structural Elucidation of Rift Valley Fever Virus L Protein towards the Discovery of Its Potential Inhibitors
title_short Structural Elucidation of Rift Valley Fever Virus L Protein towards the Discovery of Its Potential Inhibitors
title_sort structural elucidation of rift valley fever virus l protein towards the discovery of its potential inhibitors
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9228520/
https://www.ncbi.nlm.nih.gov/pubmed/35745579
http://dx.doi.org/10.3390/ph15060659
work_keys_str_mv AT alamrimubaraka structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT mirzamuhammadusman structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT adeelmuhammadmuzammal structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT ashfaqusmanali structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT tahirulqamarmuhammad structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT shahidfarah structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT ahmadsajjad structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT alatawieida structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT albalawighadahm structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT allemailemkhaleds structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors
AT almatroudiahmad structuralelucidationofriftvalleyfeverviruslproteintowardsthediscoveryofitspotentialinhibitors

Ejemplares similares