Alshabani, Lama A., Abdali, Jabril M., Brown, Alistair K., de Sousa, Damião Pergentino, Willcocks, Sam, Kumar, Amit, Alhejaili, Ahmed Y. G., Estrada, D. Fernando and Simons, Claire  ORCID: https://orcid.org/0000-0002-9487-1100
2026.
3-(Pyridine-3-ylmethylene)chroman-4-one and tetralone derivatives: synthesis, Mycobacterium tuberculosis CYP121A1 enzyme inhibition and antimycobacterial activity vs drug-sensitive and drug-resistant strains.
RSC Medicinal Chemistry
10.1039/d5md00738k
|
![[thumbnail of D5MD00738K.pdf]](https://orca.cardiff.ac.uk/style/images/fileicons/application_pdf.png "D5MD00738K.pdf") |
PDF
- Published Version
Available under License Creative Commons Attribution. Download (1MB) |
Abstract
CYP121A1 is a promising cytochrome P450 (CYP) drug target in Mycobacterium tuberculosis (Mtb) owing to its physiological importance in bacterial cell viability. The continuing rise of multidrug resistant (MDR) and extremely drug resistant (XDR) tuberculosis (TB), offers potential therapeutics with a new mechanism of action to add to the multidrug TB regime. A series of 3-(pyridine-3-ylmethylene)chromanone derivatives (5) with 7-O-alkyl/aryl substitutions were explored for CYP121A1 binding and antimycobacterial activity in susceptible and resistant Mtb strains. The 3-(pyridine-3-ylmethylene)chroman-4-one derivatives (5) with the 7-O-(CH2)3-phenyl substitution displayed the strongest CYP121A1 binding affinity (KD 0.3 to 3.6 μM) compared with the natural substrate (dicyclotyrosine, KD 16.8 ± 1.0 μM). Improvements observed in binding affinity from 7-O-benzyl to (CH2)2-phenyl to (CH2)3-phenyl substitutions are supported by computational studies. Minimum inhibitor concentration (MIC) of the alkyoxyaryl substituted chromanones ranged from 1.5–50 μM (0.5–22.5 μg mL−1) against the H37Rv wild type strain (c.f. isoniazid 1.8 μM (0.2 μg mL−1), rifampicin 0.3 μM (0.2 μg mL−1), kanamycin 16.1 μM (7.8 μg mL−1)) with antimycobacterial activity retained against mono-resistant (isoniazid or rifampicin) and MDR (isoniazid and rifampicin) Mtb strains. In contrast, the tetralone derivatives (8) with either the O-(CH2)2-phenyl or O-(CH2)3-phenyl substitutions showed no binding affinity with CYP121A1, possibly owing to binding further away from the haem and failing to displace the 6th axial water ligand, but the O-(CH2)3-phenyl substituted tetralones were the most consistently effective against H37Rv strain with MIC of 3 μM (1.1–1.2 μg mL−1) and retained activity against the mono-resistant and MDR Mtb strains.
| Item Type: | Article |
|---|---|
| Date Type: | Published Online |
| Status: | In Press |
| Schools: | Schools > Pharmacy |
| Additional Information: | License information from Publisher: LICENSE 1: URL: https://creativecommons.org/licenses/by/3.0/, Start Date: 2026-02-04 |
| Publisher: | Royal Society of Chemistry |
| Date of First Compliant Deposit: | 17 February 2026 |
| Date of Acceptance: | 20 December 2025 |
| Last Modified: | 06 Mar 2026 12:32 |
| URI: | https://orca.cardiff.ac.uk/id/eprint/184912 |
Actions (repository staff only)
 |
Edit Item |
Altmetric
Altmetric