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Unveiling the Antiviral Efficacy of Forskolin: A Multifaceted In Vitro and In Silico Approach. | LitMetric

Unveiling the Antiviral Efficacy of Forskolin: A Multifaceted In Vitro and In Silico Approach.

Molecules

Department of Pharmacognosy and Medicinal Plants, Faculty of Pharmacy, Al-Azhar University, Cairo 11884, Egypt.

Published: February 2024

AI Article Synopsis

  • The medicinal herb (Willd.) Briq., part of the Lamiaceae family, is native to India and is notable for its edible roots rich in bioactive compounds used to treat conditions like inflammation and viral diseases.
  • This study focused on Forskolin, a naturally occurring derivative from the herb, evaluating its antiviral effects against herpes simplex viruses and hepatitis A, finding promising inhibitory activities.
  • Further analysis identified Cathepsin L as a primary target for Forskolin's antiviral action, demonstrating effective binding interactions that suggest its potential as an antiviral agent.

Article Abstract

(Willd.) Briq. is a medicinal herb of the Lamiaceae family. It is native to India and widely present in the tropical and sub-tropical regions of Egypt, China, Ethiopia, and Pakistan. The roots of are edible, rich with pharmaceutically bioactive compounds, and traditionally reported to treat a variety of diseases, including inflammation, respiratory disorders, obesity, and viral ailments. Notably, the emergence of viral diseases is expected to quickly spread; consequently, these data impose a need for various approaches to develop broad active therapeutics for utilization in the management of future viral infectious outbreaks. In this study, the naturally occurring labdane diterpenoid derivative, Forskolin, was obtained from . Additionally, we evaluated the antiviral potential of Forskolin towards three viruses, namely the herpes simplex viruses 1 and 2 (HSV-1 and HSV-2), hepatitis A virus (HAV), and coxsackievirus B4 (COX-B4). We observed that Forskolin displayed antiviral activity against HAV, COX-B4, HSV-1, and HSV-2 with IC values of 62.9, 73.1, 99.0, and 106.0 μg/mL, respectively. Furthermore, we explored the Forskolin's potential antiviral target using PharmMapper, a pharmacophore-based virtual screening platform. Forskolin's modeled structure was analyzed to identify potential protein targets linked to its antiviral activity, with results ranked based on Fit scores. Cathepsin L (PDB ID: 3BC3) emerged as a top-scoring hit, prompting further exploration through molecular docking and MD simulations. Our analysis revealed that Forskolin's binding mode within Cathepsin L's active site, characterized by stable hydrogen bonding and hydrophobic interactions, mirrors that of a co-crystallized inhibitor. These findings, supported by consistent RMSD profiles and similar binding free energies, suggest Forskolin's potential in inhibiting Cathepsin L, highlighting its promise as an antiviral agent.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10856047PMC
http://dx.doi.org/10.3390/molecules29030704DOI Listing

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