| Literature DB >> 30953888 |
Zhong-Rui Li1, Ting Ma1, Yan-Jia Guo1, Bo Hu1, Sheng-Hui Niu1, Feng-Zhi Suo1, Lin-Na Du1, Ying-Hua You1, Wen-Ting Kang1, Shuan Liu1, Maa Mamun1, Qi-Meng Song1, Jing-Ru Pang1, Yi-Chao Zheng2, Hong-Min Liu3.
Abstract
Sanggenon O (SO) is a Diels-Alder type adduct extracted fromMorus alba, which has been used for its anti-inflammatory action in the Oriental medicine. However, whether it has regulatory effect on human cancer cell proliferation and what the underlying mechanism remains unknown. Here, we found that SO could significantly inhibit the growth and proliferation of A549 cells and induce its pro-apoptotic action through a caspase-dependent pathway. It could also impair the mitochondria which can be reflected by mitochondrial membrane permeabilization. Besides, SQSTM1 up-regulation and autophagic flux measurement demonstrated that exposure to SO led to autophagosome accumulation, which plays a protective role in SO-treated cells. In addition, knocking down of LC3B increased SO triggered apoptotic cell rates. These results indicated that SO has great potential as a promising candidate combined with autophagy inhibitor for the treatment of NSCLC. In conclusion, our results identified a novel mechanism by which SO exerts potent anticancer activity.Entities:
Keywords: Apoptosis; Autophagosome; Cell proliferation; Non-small cell lung cancer; Sanggenon O
Year: 2019 PMID: 30953888 DOI: 10.1016/j.bioorg.2019.03.072
Source DB: PubMed Journal: Bioorg Chem ISSN: 0045-2068 Impact factor: 5.275