AI Article Synopsis

  • Basidalin, derived from the mushroom Leucoagaricus naucina, shows strong antiproliferative effects against human cancer cell lines, building on its known antibacterial and antitumor properties in murine models.
  • The study highlights that basidalin’s anticancer action is linked to the induction of autophagy, with increased LC3-II levels and enhanced autophagic flux occurring independently of mTOR pathways.
  • Additionally, the effectiveness of basidalin and its analogs in combating cancer cells is tied to their structural features, specifically a formyl group that influences their ability to induce autophagy and inhibit cell growth.

Article Abstract

Basidalin, isolated from the basidiomycete Leucoagaricus naucina, has previously demonstrated antibacterial and antitumor properties against murine cancer cells in vivo, but its effects on human cancer cells remain unknown. In this study, we found that basidalin possesses antiproliferative activity against human cancer cell lines. To elucidate the antiproliferative mechanism of basidalin, we focused on autophagy. Treatment with basidalin led to an increase in LC3-II expression level, and accelerated autophagic flux through an mTOR-independent pathway. Moreover, according to the structure-activity relationship analysis-including newly synthesized basidalin analogs-the formyl group, not the amino group, contributes to the antiproliferative activities of basidalin against human cancer cells. Additionally, the antiproliferative activity of basidalin analogs was strongly correlated with autophagy-inducing activity, indicating that basidalin exhibits antiproliferative activity through autophagy induction. These data suggest that basidalin, characterized by its ability to upregulate autophagic flux, emerges as a novel anticancer drug.

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http://dx.doi.org/10.1016/j.bmcl.2024.129713DOI Listing

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