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首页> 外文期刊>Proteomics >Proteomic characterization of EL4 lymphoma-derived tumors upon chemotherapy treatment reveals potential roles for lysosomes and caspase-6 during tumor cell death in vivo
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Proteomic characterization of EL4 lymphoma-derived tumors upon chemotherapy treatment reveals potential roles for lysosomes and caspase-6 during tumor cell death in vivo

机译:在化疗治疗时EL4淋巴瘤衍生肿瘤的蛋白质组学表征揭示了溶酶体和Caspase-6在体内肿瘤细胞死亡期间的潜在作用

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The murine mouse lymphoblastic lymphoma cell line (EL4) tumor model is an established in vivo apoptosis model for the investigation of novel cancer imaging agents and immunological treatments due to the rapid and significant response of the EL4 tumors to cyclophosphamide and etoposide combination chemotherapy. Despite the utility of this model system in cancer research, little is known regarding the molecular details of in vivo tumor cell death. Here, we report the first in-depth quantitative proteomic analysis of the changes that occur in these tumors upon cyclophosphamide and etoposide treatment in vivo. Using a label-free quantitative proteomic approach a total of 5838 proteins were identified in the treated and untreated tumors, of which 875 were determined to change in abundance with statistical significance. Initial analysis of the data reveals changes that may have been predicted, such as the downregulation of ribosomes, but demonstrates the robustness of the dataset. Analysis of the dataset also reveals the unexpected downregulation of caspase-3 and an upregulation of caspase-6 in addition to a global upregulation of lysosomal proteins in the bulk of the tumor.
机译:小鼠小鼠淋巴细胞淋巴瘤细胞系(EL4)肿瘤模型是在体内凋亡模型中确定的,用于研究新型癌症成像剂和免疫治疗,因为EL4肿瘤与环磷酰胺和依托泊苷组合化疗的快速和显着反应。尽管这种模型系统在癌症研究中效用,但对于体内肿瘤细胞死亡的分子细节很少。在这里,我们报告了在体内环磷酰胺和依托泊苷处理中这些肿瘤中发生的改变的第一种深入定量蛋白质组学分析。使用无标记的定量蛋白质组学方法,在处理和未处理的肿瘤中鉴定了总共5838种蛋白质,其中确定了875个以统计显着性改变丰富。对数据的初始分析显示可能已经预测的变化,例如核糖体的下调,但展示了数据集的鲁棒性。除了肿瘤中溶酶体蛋白的全球性上调之外,数据集还揭示了Caspase-3的意外下调,以及Caspase-6的上调。

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