What type of study is this?

This is a In Vitro Study study.

What question did this study set out to answer?

To identify promising chiral flavone derivatives as chemotherapeutic candidates based on their antitumor activity and selectivity.

May 7, 2026Open Access

Enantioselectivity in antitumor activity of flavone derivatives

Key Points

To identify promising chiral flavone derivatives as chemotherapeutic candidates based on their antitumor activity and selectivity.
Screened thirty-two chiral flavone derivatives for antitumor properties.
Conducted cell viability assays on melanoma, breast, lung, and colorectal cancer cell lines.
Characterized metabolic effects by quantifying glucose and lactate levels.
Evaluated apoptosis via Annexin V/PI double staining and flow cytometry.
Assessed P-gp inhibition in HCT-15 cells using Rhodamine 123 exclusion assay.
6HF-DTrp and 7HF-DTrp showed GI50 < 25 µM in multiple cancer cell lines.
7HF-DTrp had a selectivity index of up to 7.94 across all tumor lines.
Both compounds inhibited P-gp in vitro and in silico, enhancing efficacy against multidrug resistance.
The metabolic and apoptotic responses varied by cell type.

Abstract

Background: Nature represents a rich source of bioactive compounds, with flavones standing out as privileged scaffolds owing to their multiple biological activities 1. Their potential as antitumor agents arises from their ability to act on multiple cellular pathways implicated in cancer progression and to attenuate multidrug resistance (MDR) 2. However, to overcome inherent pharmacokinetic drawbacks and target selectivity, flavones are commonly subjected to structural modifications 3. The incorporation of chiral moieties, such as amino acids, is used to improve the pharmacokinetic parameters and selectivity 4. Objective: This study screened a library of thirty-two new chiral flavone derivatives (CDFs) to identify promising chemotherapeutic candidates. Beyond cytotoxicity, their effects on tumor metabolism, cell death mechanisms, and their potential as P-glycoprotein (P-gp) inhibitors to overcome multidrug resistance were evaluated. Methods: Cell viability assays were performed against a panel of four human cancer cell lines: A375-C5 (melanoma), MCF-7 (breast), NCI-H460 (lung), and HCT-15 (colorectal). The most promising CDFs were further characterized with respect to their impact on metabolic profiles through the quantification of extracellular glucose and lactate levels. Additionally, apoptosis induction was evaluated by Annexin V/PI double staining and flow cytometry, while the Rhodamine 123 exclusion assay was conducted in HCT-15 cells to assess the compounds' potential as P-gp inhibitors. Results: Derivatives 6HF-DTrp and 7HF-DTrp were the most potent candidates (GI50 < 25 µM), with 7HF-DTrp displaying high specificity (SI up to 7.94) across all tumor lines. While metabolic and apoptotic responses varied by cell type, both compounds were confirmed as P-gp inhibitors through in vitro and in silico assays. Conclusions: These findings identify 6HF-DTrp and 7HF-DTrp as potent, selective, and P-gp inhibitory leads, highlighting their potential as candidates for both monotherapy and combination strategies in cancer treatment.

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