2. Academic Validation
  3. Scaffold hopping for designing of potent and selective CYP1B1 inhibitors to overcome docetaxel resistance: synthesis and evaluation

Scaffold hopping for designing of potent and selective CYP1B1 inhibitors to overcome docetaxel resistance: synthesis and evaluation

  • J Biomol Struct Dyn. 2024 Feb 14:1-19. doi: 10.1080/07391102.2024.2310770.
Baddipadige Raju 1 Gera Narendra 1 Himanshu Verma 1 Manoj Kumar 1 Bharti Sapra 1 Gurleen Kaur 2 Subheet Kumar Jain 2 Padakanti Sandeep Chary 3 Neelesh Kumar Mehra 3 Om Silakari 1
Affiliations

Affiliations

  • 1 Molecular Modeling Lab (MML), Department of Pharmaceutical Sciences and Drug Research, Punjabi University, Patiala, Punjab, India.
  • 2 Center for Basic and Translational Research in Health Sciences, Guru Nanak Dev University, Amritsar, Punjab, India.
  • 3 Pharmaceutical Nanotechnology Research Laboratory, Department of Pharmaceutical, National Institute of Pharmaceutical Science and Drug Research, Hyderabad, Telangana, India.
PMID: 38356135 DOI: 10.1080/07391102.2024.2310770
Abstract

Cytochrome P450 1B1, a tumor-specific overexpressed Enzyme, significantly impairs the pharmacokinetics of several commonly used Anticancer drugs including docetaxel, paclitaxel and cisplatin, leading to the problem of resistance to these drugs. Currently, there is no CYP1B1 inhibition-based adjuvant therapy available to treat this resistance problem. Hence, in the current study, exhaustive in-silico studies including scaffold hopping followed by molecular docking, three-dimensional quantitative structure-activity relationships (3D-QSAR), molecular dynamics and free energy perturbation studies were carried out to identify potent and selective CYP1B1 inhibitors. Initially, scaffold hopping analysis was performed against a well-reported potent and selective CYP1B1 inhibitor (i.e. compound 3n). A total of 200 scaffolds were identified along with their shape and field similarity scores. The top three scaffolds were further selected on the basis of these scores and their synthesis feasibility to design some potent and selective CYP1B1 inhibitors using the aforementioned in-silico techniques. Designed molecules were further synthesized to evaluate their CYP1B1 inhibitory activity and docetaxel resistance reversal potential against CYP1B1 overexpressed drug resistance MCF-7 cell line. In-vitro results indicated that compounds 2a, 2c and 2d manifested IC50 values for CYP1B1 ranging from 0.075, 0.092 to 0.088 μM with at least 10-fold selectivity. At low micromolar concentrations, compounds 1e, 1f, 2a and 2d exhibited promising cytotoxic effects in the docetaxel-resistant CYP1B1 overexpressed MCF-7 cell line. In particular, compound 2a is most effective in reversing the resistance with IC50 of 29.0 ± 3.6 μM. All of these discoveries could pave the way for the development of adjuvant therapy capable of overcoming CYP1B1-mediated resistance.Communicated by Ramaswamy H. Sarma.

Keywords

CYP1B1; chemo-resistance; docetaxel; inhibitors; selectivity.

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