Structure-Guided Approach to Identify Potential Inhibitors of Large Envelope Protein to Prevent Hepatitis B Virus Infection

Mehmankhah, Mahboubeh; Bhat, Ruchika; Anvar, Mohammad Sabery; Ali, Shahnawaz; Alam, Aftab; Farooqui, Anam; Amir, Fatima; Anwer, Ayesha; Khan, Sabah; Azmi, Iqbal; Ali, Rafat; Ishrat, Romana; Hassan, Md. Imtaiyaz; Minuchehr, Zarrin; Kazim, Syed Naqui

doi:10.1155/2019/1297484

Cited by 2 publications

(3 citation statements)

References 72 publications

(81 reference statements)

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“…In one of the current studies, computational docking reveals the set of 23 drugs that block the viral infection on CD-81 binding site, but after experimental analysis only one ligand was capable of binding to inhibit the infection of Huh-7 cells. While the binding energy of the drugs ranges from −8.64 to −6.36 [ 52 ], the binding energy of the drugs obtained from our virtual screening ranges from −13.2 to −11.…”

Section: Resultsmentioning

confidence: 99%

“…Some previous studies [ 51 ] show hydrogen and other interactions of sofosbuvir and ribavirin with HCV envelope protein during docking studies. Similarly, in other studies [ 52 ], the envelope protein is targeted for identification of various inhibitory molecules. In total, ZINC11882026, ZINC19741044, ZINC00653293, and ZINC15000762 are identified as potential candidates and recognized as appreciable drugs for viral envelope protein.…”

Section: Resultsmentioning

confidence: 99%

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Identification of Potential HCV Inhibitors Based on the Interaction of Epigallocatechin-3-Gallate with Viral Envelope Proteins

et al. 2021

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Hepatitis C is affecting millions of people around the globe annually, which leads to death in very high numbers. After many years of research, hepatitis C virus (HCV) remains a serious threat to the human population and needs proper management. The in silico approach in the drug discovery process is an efficient method in identifying inhibitors for various diseases. In our study, the interaction between Epigallocatechin-3-gallate, a component of green tea, and envelope glycoprotein E2 of HCV is evaluated. Epigallocatechin-3-gallate is the most promising polyphenol approved through cell culture analysis that can inhibit the entry of HCV. Therefore, various in silico techniques have been employed to find out other potential inhibitors that can behave as EGCG. Thus, the homology modelling of E2 protein was performed. The potential lead molecules were predicted using ligand-based as well as structure-based virtual screening methods. The compounds obtained were then screened through PyRx. The drugs obtained were ranked based on their binding affinities. Furthermore, the docking of the topmost drugs was performed by AutoDock Vina, while its 2D interactions were plotted in LigPlot+. The lead compound mms02387687 (2-[[5-[(4-ethylphenoxy) methyl]-4-prop-2-enyl-1,2,4-triazol-3-yl] sulfanyl]-N-[3(trifluoromethyl) phenyl] acetamide) was ranked on top, and we believe it can serve as a drug against HCV in the future, owing to experimental validation.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Identification of Potential HCV Inhibitors Based on the Interaction of Epigallocatechin-3-Gallate with Viral Envelope Proteins

et al. 2021

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“…Bioinformatic analysis was used to predict the HBsAg structure in our study. [ 15 ] The genotype D HBsAg aa sequence was submitted to the I‐TASSER server, which uses solved protein structures as templates to generate three‐dimensional atomic models. [ 16 ] The simulation acquired from I‐TASSER was further checked for its average and stereochemical quality by the ProTSAV and MolProbity platforms.…”

Section: Methodsmentioning

confidence: 99%

Mapping the conformational epitope of a therapeutic monoclonal antibody against HBsAg by in vivo selection of HBV escape variants

Kim²,

Sun

et al. 2022

Hepatology

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Background and Aims Hepatitis B immunoglobulin (HBIG) has been routinely applied in the liver transplantation setting to block HBV reinfection of grafts. However, new monoclonal anti‐HBV surface antibodies have been developed to replace HBIG. The epitopes of such monoclonal antibodies may affect the emergence of escape variants and deserve study. Approach and Results The conformational epitope of sLenvervimab, a surrogate form of Lenvervimab, which is a monoclonal anti‐HBsAg antibody currently under phase 3 trial, was investigated by selecting escape mutants from a human liver chimeric mouse. HBV‐infected chimeric mice treated with sLenvervimab monotherapy showed an initial decline in circulating HBsAg levels, followed by a quick rebound in 1 month. Sequencing of circulating or liver HBV DNA revealed emerging variants, with replacement of amino acid E164 or T140, two residues widely separated in HBsAg. E164 HBV variants strongly resisted sLenvervimab neutralization in cell culture infection, and the T140 variant moderately resisted sLenvervimab neutralization. Natural HBV variants with amino‐acid replacements adjacent to E164 were constructed and examined for sLenvervimab neutralization effects. Variants with K160 replacement also resisted neutralization. These data revealed the conformational epitope of sLenvervimab. Conclusions Selection of antibody‐escape HBV variants in human chimeric mice works efficiently. Analysis of such emerging variants helps to identify anchor amino‐acid residues of the conformational epitope that are difficult to discover by conventional approaches.

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Structure-Guided Approach to Identify Potential Inhibitors of Large Envelope Protein to Prevent Hepatitis B Virus Infection

Cited by 2 publications

References 72 publications

Identification of Potential HCV Inhibitors Based on the Interaction of Epigallocatechin-3-Gallate with Viral Envelope Proteins

Identification of Potential HCV Inhibitors Based on the Interaction of Epigallocatechin-3-Gallate with Viral Envelope Proteins

Mapping the conformational epitope of a therapeutic monoclonal antibody against HBsAg by in vivo selection of HBV escape variants

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