Derived from fangchinoline, LYY-35 exhibits an inhibiting effect on human NSCLC cancer A549 cells
Bo Wang, Shan Long, Junjie Lan, Kaixiong Luo, Wangming Zhang, Xiaosong Li, Weidong Pan, Jielin Liu

TL;DR
A new compound derived from fangchinoline, LYY-35, shows promise in inhibiting lung cancer cell growth and promoting cell death.
Contribution
LYY-35, a fangchinoline derivative, demonstrates anti-cancer effects in NSCLC cells through multiple mechanisms.
Findings
LYY-35 reduces A549 cell viability, alters morphology, and increases cell debris.
It inhibits cancer cell migration, proliferation, and invasion while sparing normal lung cells.
LYY-35 induces apoptosis, increases ROS, causes DNA damage, and blocks the cell cycle in G0/G1 phase.
Abstract
Although fangchinoline has been widely used as an adjunct therapy for a variety of inflammatory and cancerous diseases, its mechanism of action on tumor cells remains unclear. Fangchinoline derivative LYY-35 reduced the number of A549 cells, deformed cell morphology and increased cell debris. Cell viability was significantly reduced, while the same concentration of LYY-35 had little effect on BEAS-2B viability of normal lung epithelial cells. In addition, LYY-35 can also reduce the migration, proliferation and invasion ability of A549 cells. Levels of β-catenin, ZO-1 and ZEB-1 proteins, biomarkers of cell adhesion and epithelial mesenchymal transformation, were significantly reduced. The levels of superoxide dismutase and lactate dehydrogenase decreased gradually, while the levels of glutathione, malondialdehyde and intracellular and extracellular ROS increased significantly. At the…
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Taxonomy
TopicsMarine Sponges and Natural Products · Microbial Natural Products and Biosynthesis · Carbohydrate Chemistry and Synthesis
