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作 者:王馨苑[1] 承尧 杜吉佩[2] 陈德高[1] 杨雪杉[1] 杨志梅[1] 黄宁[1]
机构地区:[1]四川大学华西基础医学与法医学院病理生理学教研室,成都610041 [2]四川大学华西基础医学与法医学院法医物证学教研室,成都610041
出 处:《四川大学学报(医学版)》2014年第3期355-361,共7页Journal of Sichuan University(Medical Sciences)
基 金:国家理科人才培养基金--能力提高项目(No.J1103604)资助
摘 要:目的通过联合抑制MEK和AKT信号通路关键靶点分子,探讨克服细胞耐药性的靶向治疗方法。方法体外培养和新鲜分离恶性黑色素瘤细胞株,分别在0.5%和5%血清浓度下单独或同时抑制靶点MEK(U0126,20μmol/L)和AKT(LY294002,20μmol/L),MTT法检测细胞增殖,PI染色流式细胞术检测细胞凋亡情况。结果当培养液血清浓度从0.5%提高到5%时,U0126和LY294002对肿瘤细胞增殖的抑制效应明显降低。LY294002以抑制细胞增殖为主,U0126主要诱导细胞凋亡,二者作用效果与细胞是否具备该通路关键靶点活化变异无关。联合用药时诱导细胞凋亡普遍增强,LY294002和U0126具有协同效应。结论联合抑制MEK/ERK和PI3K/AKT信号通路可较好地克服恶性黑色素瘤细胞的耐药性。Objective The treatment of metastatic melanoma by conventional chemotherapeutic agents remains unsatisfactory. The present study was undertaken to reveal the role of co-inhibition of survival signaling pathways in apoptosis of melanoma cells. Methods A panel of human melanoma cell lines and fresh melanoma isolates was assessed for their sensitivity to the MEK inhibitor U0126 and/or AKT inhibitor LY294002. The proliferation and apoptosis of the cells were examined after treatment with the inhibitors. Results Constitutive activation of ERK1/2 and AKT was closely related to concentrations of serum in the culture medium (extracellular signals). The sensitivity of melanoma cells to apoptosis induced by inhibition of MEK/ERK was not correlated with the active BRAF mutation (BRAFTM ). Inhibition of MEK/ERK predominantly induced apoptosis; whereas inhibition of PI3K/AKT primarily inhibited proliferation. Co-inhibition of MEK/ERK1/2 and PI3K/AKT synergistically induced apoptosis. Conclusion Co-targeting MEK/ERK and PI3K/AKT pathways may further improve treatment for melanoma.
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