| Literature DB >> 33948359 |
Solbi Kim1, Sang-Il Lee2, Nayoung Kim1, Mina Joo1, Kyung-Ha Lee2, Myung-Won Lee3, Heung Jin Jeon4, Hyewon Ryu3, Jin-Man Kim5, Ji-Young Sul2, Gyu-Yong Song6, Ji-Yeon Kim2, Hyo Jin Lee3,4.
Abstract
Autophagy plays an important role in the survival of cancer cells under stressful conditions, such as nutrient or oxygen deficiency. Therefore, autophagy inhibition is being considered as a novel therapeutic strategy for cancer. Decursin is a natural compound derived from Angelica gigas; it has been used in the treatment of various diseases, including cancer. However, the mechanism by which decursin regulates autophagy in gastric cancer and other carcinomas remains unclear. Here, we demonstrated that decursin reduced the growth and induced cell cycle arrest in gastric cancer cells in vitro. Decursin blocked autophagic flux by reducing the expression of lysosomal protein cathepsin C (CTSC) and attenuating its activity, thereby causing autophagic dysregulation (i.e., accumulation of LC3 and SQSTM1). Decursin also inhibited cell proliferation and cell cycle progression by inhibiting CTSC and E2F3, both of which were linked to gastric cancer aggressiveness. The antitumor effects of decursin were confirmed in vivo. We established spheroid and patient-derived organoid models and found that decursin decreased the growth of spheroids and patient-derived gastric organoids, as well as modulated the expression of CTSC and autophagy-related proteins. Hence, our findings uncovered a previously unknown mechanism by which decursin regulates cell growth and autophagy and suggests that decursin may act as a potential therapeutic agent that simultaneously inhibits cell growth and autophagy. AJCREntities:
Keywords: Autophagy; E2F3; cathepsin C; cell cycle; decursin; gastric cancer; patient-derived gastric organoid
Year: 2021 PMID: 33948359 PMCID: PMC8085838
Source DB: PubMed Journal: Am J Cancer Res ISSN: 2156-6976 Impact factor: 6.166