Your search keyword '"Semkum P"' showing total 5 results

1. Naturally Derived Terpenoids Targeting the 3D pol of Foot-and-Mouth Disease Virus: An Integrated In Silico and In Vitro Investigation.

Author

Mana N, Theerawatanasirikul S, Semkum P, and Lekcharoensuk P

Subjects

Animals, Cell Line, Virus Replication drug effects, Computer Simulation, RNA-Dependent RNA Polymerase metabolism, RNA-Dependent RNA Polymerase antagonists & inhibitors, Cricetinae, Molecular Docking Simulation, Foot-and-Mouth Disease virology, Foot-and-Mouth Disease drug therapy, Diterpenes pharmacology, Diterpenes chemistry, Foot-and-Mouth Disease Virus drug effects, Antiviral Agents pharmacology, Antiviral Agents chemistry, Terpenes pharmacology, Terpenes chemistry

Abstract

Foot-and-mouth disease virus (FMDV) belongs to the Picornaviridae family and is an important pathogen affecting cloven-hoof livestock. However, neither effective vaccines covering all serotypes nor specific antivirals against FMDV infections are currently available. In this study, we employed virtual screening to screen for secondary metabolite terpenoids targeting the RNA-dependent RNA polymerase (RdRp), or 3D pol , of FMDV. Subsequently, we identified the potential antiviral activity of the 32 top-ranked terpenoids, revealing that continentalic acid, dehydroabietic acid (abietic diterpenoids), brusatol, bruceine D, and bruceine E (tetracyclic triterpenoids) significantly reduced cytopathic effects and viral infection in the terpenoid-treated, FMDV-infected BHK-21 cells in a dose-dependent manner, with nanomolar to low micromolar levels. The FMDV minigenome assay demonstrated that brusatol and bruceine D, in particular, effectively blocked FMDV 3D pol activity, exhibiting IC50 values in the range of 0.37-0.39 µM and surpassing the efficacy of the antiviral drug control, ribavirin. Continentalic acid and bruceine E exhibited moderate inhibition of FMDV 3D pol . The predicted protein-ligand interaction confirmed that these potential terpenoids interacted with the main catalytic and bystander residues of FMDV 3D pol . Additionally, brusatol and bruceine D exhibited additive effects when combined with ribavirin. In conclusion, terpenoids from natural resources show promise for the development of anti-FMD agents.

Published

2024

2. Small Molecules Targeting 3C Protease Inhibit FMDV Replication and Exhibit Virucidal Effect in Cell-Based Assays.

Author

Theerawatanasirikul S, Lueangaramkul V, Pantanam A, Mana N, Semkum P, and Lekcharoensuk P

Subjects

Animals, Molecular Docking Simulation, Endopeptidases, Antiviral Agents pharmacology, 3C Viral Proteases, Peptide Hydrolases, Foot-and-Mouth Disease Virus

Abstract

Foot-and-mouth disease (FMD) is a highly contagious disease in cloven-hoofed animals, caused by the foot-and-mouth disease virus (FMDV). It is endemic in Asia and Africa but spreads sporadically throughout the world, resulting in significant losses in the livestock industry. Effective anti-FMDV therapeutics could be a supportive control strategy. Herein, we utilized computer-aided, structure-based virtual screening to filter lead compounds from the National Cancer Institute (NCI) diversity and mechanical libraries using FMDV 3C protease (3C pro ) as the target. Seven hit compounds were further examined via cell-based antiviral and intracellular protease assays, in which two compounds (NSC116640 and NSC332670) strongly inhibited FMDV, with EC50 values at the micromolar level of 2.88 µM (SI = 73.15) and 5.92 µM (SI = 11.11), respectively. These compounds could inactivate extracellular virus directly in a virucidal assay by reducing 1.00 to 2.27 log TCID50 of the viral titers in 0-60 min. In addition, the time-of-addition assay revealed that NSC116640 inhibited FMDV at the early stage of infection (0-8 h), while NSC332670 diminished virus titers when added simultaneously at infection (0 h). Both compounds showed good FMDV 3C pro inhibition with IC50 values of 10.85 µM (NSC116640) and 4.21 µM (NSC332670). The molecular docking of the compounds on FMDV 3C pro showed their specific interactions with amino acids in the catalytic triad of FMDV 3C pro . Both preferentially reacted with enzymes and proteases in physicochemical and ADME analysis studies. The results revealed two novel small molecules with antiviral activities against FMDV and probably related picornaviruses.

Published

2023

3. Non-Nucleoside Inhibitors Decrease Foot-and-Mouth Disease Virus Replication by Blocking the Viral 3D pol .

Author

Theerawatanasirikul S, Semkum P, Lueangaramkul V, Chankeeree P, Thangthamniyom N, and Lekcharoensuk P

Subjects

Animals, Antiviral Agents pharmacology, Antiviral Agents metabolism, RNA-Dependent RNA Polymerase metabolism, Virus Replication, Foot-and-Mouth Disease Virus genetics, Foot-and-Mouth Disease

Abstract

Foot-and-mouth disease virus (FMDV), an economically important pathogen of cloven-hoofed livestock, is a positive-sense, single-stranded RNA virus classified in the Picornaviridae family. RNA-dependent RNA polymerase (RdRp) of RNA viruses is highly conserved. Compounds that bind to the RdRp active site can block viral replication. Herein, we combined double virtual screenings and cell-based antiviral approaches to screen and identify potential inhibitors targeting FMDV RdRp (3D pol ). From 5596 compounds, the blind- followed by focus-docking filtered 21 candidates fitting in the 3D pol active sites. Using the BHK-21 cell-based assay, we found that four compounds-NSC217697 (quinoline), NSC670283 (spiro compound), NSC292567 (nigericin), and NSC65850-demonstrated dose-dependent antiviral actions in vitro with the EC50 ranging from 0.78 to 3.49 µM. These compounds could significantly block FMDV 3D pol activity in the cell-based 3D pol inhibition assay with small IC50 values ranging from 0.8 nM to 0.22 µM without an effect on FMDV's main protease, 3C pro . The 3D pol inhibition activities of the compounds were consistent with the decreased viral load and negative-stranded RNA production in a dose-dependent manner. Conclusively, we have identified potential FMDV 3D pol inhibitors that bound within the enzyme active sites and blocked viral replication. These compounds might be beneficial for FMDV or other picornavirus treatment.

Published

2022

4. Natural Phytochemicals, Luteolin and Isoginkgetin, Inhibit 3C Protease and Infection of FMDV, In Silico and In Vitro.

Author

Theerawatanasirikul S, Thangthamniyom N, Kuo CJ, Semkum P, Phecharat N, Chankeeree P, and Lekcharoensuk P

Subjects

3C Viral Proteases chemistry, 3C Viral Proteases genetics, 3C Viral Proteases metabolism, Animals, Antiviral Agents chemistry, Biflavonoids chemistry, Computer Simulation, Enzyme Inhibitors chemistry, Foot-and-Mouth Disease Virus chemistry, Foot-and-Mouth Disease Virus genetics, Humans, Luteolin chemistry, Phytochemicals chemistry, Phytochemicals pharmacology, 3C Viral Proteases antagonists & inhibitors, Antiviral Agents pharmacology, Biflavonoids pharmacology, Enzyme Inhibitors pharmacology, Foot-and-Mouth Disease virology, Foot-and-Mouth Disease Virus drug effects, Foot-and-Mouth Disease Virus enzymology, Luteolin pharmacology

Abstract

Foot-and-mouth-disease virus (FMDV) is a picornavirus that causes a highly contagious disease of cloven-hoofed animals resulting in economic losses worldwide. The 3C protease (3C pro ) is the main protease essential in the picornavirus life cycle, which is an attractive antiviral target. Here, we used computer-aided virtual screening to filter potential anti-FMDV agents from the natural phytochemical compound libraries. The top 23 filtered compounds were examined for anti-FMDV activities by a cell-based assay, two of which possessed antiviral effects. In the viral and post-viral entry experiments, luteolin and isoginkgetin could significantly block FMDV growth with low 50% effective concentrations (EC50). Moreover, these flavonoids could reduce the viral load as determined by RT-qPCR. However, their prophylactic activities were less effective. Both the cell-based and the fluorescence resonance energy transfer (FRET)-based protease assays confirmed that isoginkgetin was a potent FMDV 3C pro inhibitor with a 50% inhibition concentration (IC50) of 39.03 ± 0.05 and 65.3 ± 1.7 μM, respectively, whereas luteolin was less effective. Analyses of the protein-ligand interactions revealed that both compounds fit in the substrate-binding pocket and reacted to the key enzymatic residues of the 3C pro . Our findings suggested that luteolin and isoginkgetin are promising antiviral agents for FMDV and other picornaviruses.

Published

2021

5. A Novel Plasmid DNA-Based Foot and Mouth Disease Virus Minigenome for Intracytoplasmic mRNA Production.

Author

Semkum P, Kaewborisuth C, Thangthamniyom N, Theerawatanasirikul S, Lekcharoensuk C, Hansoongnern P, Ramasoota P, and Lekcharoensuk P

Subjects

Animals, Antiviral Agents chemistry, Antiviral Agents pharmacology, Cell Line, Foot-and-Mouth Disease drug therapy, Foot-and-Mouth Disease Virus drug effects, Gene Order, Humans, Models, Molecular, Molecular Structure, RNA, Messenger chemistry, Structure-Activity Relationship, Transfection, Virus Replication drug effects, Foot-and-Mouth Disease virology, Foot-and-Mouth Disease Virus genetics, Gene Expression Regulation, Viral, Genome, Viral, Plasmids genetics, RNA, Messenger genetics

Abstract

Picornaviruses are non-enveloped, single-stranded RNA viruses that cause highly contagious diseases, such as polio and hand, foot-and-mouth disease (HFMD) in human, and foot-and-mouth disease (FMD) in animals. Reverse genetics and minigenome of picornaviruses mainly depend on in vitro transcription and RNA transfection; however, this approach is inefficient due to the rapid degradation of RNA template. Although DNA-based reverse genetics systems driven by mammalian RNA polymerase I and/or II promoters display the advantage of rescuing the engineered FMDV, the enzymatic functions are restricted in the nuclear compartment. To overcome these limitations, we successfully established a novel DNA-based vector, namely pKLS3, an FMDV minigenome containing the minimum cis-acting elements of FMDV essential for intracytoplasmic transcription and translation of a foreign gene. A combination of pKLS3 minigenome and the helper plasmids yielded the efficient production of uncapped-green florescent protein (GFP) mRNA visualized in the transfected cells. We have demonstrated the application of the pKLS3 for cell-based antiviral drug screening. Not only is the DNA-based FMDV minigenome system useful for the FMDV research and development but it could be implemented for generating other picornavirus minigenomes. Additionally, the prospective applications of this viral minigenome system as a vector for DNA and mRNA vaccines are also discussed.

Published

2021