Betulin: a novel triterpenoid anti-cancerous agent targeting cervical cancer through epigenetic proteins.

Mol Divers

Department of Biotechnology, Vignan's Foundation for Science, Technology & Research, Vadlamudi, Guntur, 522213, India.

Published: July 2024

AI Article Synopsis

  • Cervical cancer is a leading cause of death among women, and traditional treatments are costly and have significant side effects, prompting the search for new options.
  • The study identifies Betulin (BE), a triterpenoid, as a promising anti-cancer agent targeting key epigenetic proteins associated with cervical cancer through a series of advanced bioinformatics techniques.
  • Preliminary findings suggest BE has better binding scores and favorable pharmacokinetic properties compared to standard drugs, indicating its potential effectiveness for further research, especially in live models.

Article Abstract

Worldwide, cervical cancer (CCa) is a major killer of women. As the conventional drugs used to treat cervical cancer are expensive and expose severe side effects, there is a growing demand to search for novel modifications. Therefore, in the current investigation employing a bioinformatic approach, we explored triterpenoids for their anti-cancer efficacy by targeting cervical cancer epigenetic proteins, namely DNMT3A, HDAC4, and KMT2C. The study utilized molecular docking, ADMET assay, Molecular Dynamic simulation, and DFT calculation to unveil Betulin (BE) as the potential lead compound. Comparative analysis with that standard drug indicated that BE has a better glide score with the target protein KM2TC (- 9.893 kcal/mol), HDAC4 (- 9.720 kcal/mol), and DNMT3A (- 7.811 kcal/mol), which depicts that BE could be a potent inhibitor of these three epigenetic proteins and exhibits favorable pharmacokinetic, pharmacodynamics and toxicity properties. Molecular Dynamics simulation revealed noteworthy structural stability and compactness. DFT analysis revealed higher molecular activity of BE and showed the most increased kinetic stability (δE = 0.254647 eV). Further, we employed In vitro analysis through MTT assay and found that BE has IC of 15 µg/ml. In conclusion, BE can potentially treat CCa upon further investigations using in vivo models for better understanding.

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Source
http://dx.doi.org/10.1007/s11030-024-10930-9DOI Listing

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