摘要
目的研究吴茱萸碱(evodiamine)诱导人黑色素瘤A375S2细胞死亡的作用机制及其与细胞因子人白介素1(interleukin1,IL1)信号转导途径之间的关系。方法MTT检测法,DNA凝胶电泳法及Westernblot法。结果IL1受体拮抗因子(IL1receptorantagonist,IL1ra)在24h时能够部分抑制吴茱萸碱诱导的A375S2细胞死亡。吴茱萸碱在诱导A375S2细胞死亡的过程中,Fas配体(Fasligand,FasL)的蛋白表达量升高,激活其下游的caspase8和caspase3,进而引起DNA的损伤并激活p53蛋白,同时Bax/Bcl2的蛋白表达比例被上调。在经过IL1ra预处理后,这些变化均被部分的抑制或逆转。结论吴茱萸碱诱导A375S2细胞死亡的作用是部分通过IL1介导的信号转导途径而实现的。
Aim To study the mechanism of evodiamine-induced A375-S2 cell death and the relationship of signal transduction pathways between evodiamine and IL-1. Methods MTT assay, agarose gel electrophoresis and Western blot analysis were carried out. Results IL-1 receptor antagonist ( IL-1 ra ) partially inhibited evodiamine-induced cell death in A375-S2 cells. In A375-S2 cell death, evodiamine increased the expression of Fas-ligand (Fas-L) and caused the cleavage of procaspas-8 and -3. Subsequently, evodiamine induced p53 activation, up-regulation of Bax/ Bcl-2 ratio and DNA degradation. Whereas pretreatment of IL-lra was capable of partially attenuating or reversing these changes induced by evodiamine. Conclusion Evodiamine induced human melanoma A375- S2 cell death partially through interleukin 1-mediated signal pathway.
出处
《中国药理学通报》
CAS
CSCD
北大核心
2005年第12期1478-1481,共4页
Chinese Pharmacological Bulletin
