Paris saponin II-induced paraptosis-associated cell death increased the sensitivity of cisplatin

巴黎皂苷 II 诱导的副凋亡相关细胞死亡增加了顺铂的敏感性

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作者:Shuli Man, Panpan Lv, Jingxia Cui, Furui Liu, Lei Peng, Long Ma, Changxiao Liu, Wenyuan Gao

Abstract

Paris Saponin II (PSII) has been regarded as an effective and imperative component isolated from Rhizoma Paridis saponins (RPS) and exhibited strong anti-tumor effects on a variety of cancer. Our results revealed that human non-small lung cancer cell lines NCI-H460 and NCI-H520 were exposed to 1 μM of PSII, which inhibited the proliferation of lung cancer cells and activated apoptosis, autophagy and paraptosis. PSII induced paraptosis-associated cell death prior to apoptosis and autophagy. It induced paraptosis based on ER stress through activation of the JNK pathway. Meanwhile, PSII increased the cytotoxicity of cisplatin through paraptosis-associated pathway. All in all, PSII induced paraptosis based on induction of non-apoptotic cell death, which would be a possible approach to suppress the multi-drug resistant to apoptosis.

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