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Walker-256 尾静脉注射大鼠模型的早期尿蛋白质组变化。

Early urine proteome changes in the Walker-256 tail-vein injection rat model.

机构信息

Department of Biochemistry and Molecular Biology, Beijing Normal University, Gene Engineering Drug and Biotechnology Beijing Key Laboratory, Beijing, 100875, China.

Department of Biochemistry and Molecular Biology, College of Basic Medicine, Chongqing Medical University, Chongqing, 400016, China.

出版信息

Sci Rep. 2019 Sep 24;9(1):13804. doi: 10.1038/s41598-019-50301-1.

Abstract

Detection of cancer at its early stage is important for treatment. Urine, which is not regulated by homeostatic mechanisms, reflects early systemic changes throughout the whole body and can be used for the early detection of cancer. In this study, the Walker-256 tail-vein injection rat model was established to find whether the urine proteome could reflect early changes if tumor grown in lung. Urine samples from the control group (n = 7) and Walker-256 tail-vein injection group (n = 7) on days 2, 4, 6 and 9 were analyzed by label-free proteomic quantitative methods. On day 2, when lung tumor nodules did not appear, 62 differential proteins were identified. They were associated with epithelial cell differentiation, regulation of immune system processes and the classical complement activation pathway. On day 4, when lung tumor nodules appeared, 72 differential proteins were identified. They were associated with the innate immune response and positive regulation of phagocytosis. On day 6, when body weight began to decrease, 117 differential proteins were identified. On day 9, the identified 125 differential proteins were associated with the B cell receptor signaling pathway and the positive regulation of B cell activation. Our results indicate that (1) the urine proteome changed even on the second day after tail-vein injection of Walker-256 cells and that (2) compared to previous studies, the urine proteomes were different when the same cancer cells were grown in different organs.

摘要

早期发现癌症对于治疗非常重要。尿液不受体内平衡机制的调节,反映了全身早期的系统性变化,可用于癌症的早期检测。在本研究中,建立了 Walker-256 尾静脉注射大鼠模型,以确定如果肿瘤在肺部生长,尿液蛋白质组是否可以反映早期变化。通过无标记蛋白质组定量方法分析了对照组(n=7)和 Walker-256 尾静脉注射组(n=7)在第 2、4、6 和 9 天的尿液样本。在第 2 天,当肺部肿瘤结节尚未出现时,鉴定出 62 个差异蛋白。它们与上皮细胞分化、免疫系统过程的调节和经典补体激活途径有关。在第 4 天,当肺部肿瘤结节出现时,鉴定出 72 个差异蛋白。它们与先天免疫反应和吞噬作用的正调节有关。在第 6 天,当体重开始下降时,鉴定出 117 个差异蛋白。在第 9 天,鉴定出的 125 个差异蛋白与 B 细胞受体信号通路和 B 细胞激活的正调节有关。我们的研究结果表明:(1)即使在 Walker-256 细胞尾静脉注射后的第二天,尿液蛋白质组也发生了变化;(2)与之前的研究相比,当相同的癌细胞在不同的器官中生长时,尿液蛋白质组是不同的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3818/6760176/bc33878df6d9/41598_2019_50301_Fig1_HTML.jpg

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