Xue Ting, Liu Ping, Zhou Yong, Liu Kun, Yang Li, Moritz Robert L, Yan Wei, Xu Lisa X
1. Key Laboratory of Systems Biomedicine (MOE), Shanghai Center for Systems Biomedicine, the School of Biomedical Engineering and MED-X Research Institute, Shanghai Jiao Tong University, Shanghai, China.
2. Institute for Systems Biology, Seattle, WA, USA.
Theranostics. 2016 Mar 21;6(6):773-94. doi: 10.7150/thno.14394. eCollection 2016.
Cryo-thermal therapy has been emerged as a promising novel therapeutic strategy for advanced breast cancer, triggering higher incidence of tumor regression and enhanced remission of metastasis than routine treatments. To better understand its anti-tumor mechanism, we utilized a spontaneous metastatic mouse model and quantitative proteomics to compare N-glycoproteome changes in 94 serum samples with and without treatment. We quantified 231 highly confident N-glycosylated proteins using iTRAQ shotgun proteomics. Among them, 53 showed significantly discriminated regulatory patterns over the time course, in which the acute phase response emerged as the most enhanced pathway. The anti-tumor feature of the acute response was further investigated using parallel reaction monitoring target proteomics and flow cytometry on 23 of the 53 significant proteins. We found that cryo-thermal therapy reset the tumor chronic inflammation to an "acute" phenotype, with up-regulation of acute phase proteins including IL-6 as a key regulator. The IL-6 mediated "acute" phenotype transformed IL-4 and Treg-promoting ICOSL expression to Th1-promoting IFN-γ and IL-12 production, augmented complement system activation and CD86(+)MHCII(+) dendritic cells maturation and enhanced the proliferation of Th1 memory cells. In addition, we found an increased production of tumor progression and metastatic inhibitory proteins under such "acute" environment, favoring the anti-metastatic effect. Moreover, cryo-thermal on tumors induced the strongest "acute" response compared to cryo/hyperthermia alone or cryo-thermal on healthy tissues, accompanying by the most pronounced anti-tumor immunological effect. In summary, we demonstrated that cryo-thermal therapy induced, IL-6 mediated "acute" microenvironment shifted the tumor chronic microenvironment from Th2 immunosuppressive and pro-tumorigenic to Th1 immunostimulatory and tumoricidal state. Moreover, the magnitude of "acute" and "danger" signals play a key role in determining the efficacy of anti-tumor activity.
冷冻热疗法已成为一种有前景的晚期乳腺癌新型治疗策略,与常规治疗相比,其引发肿瘤消退的发生率更高,转移缓解效果更好。为了更好地理解其抗肿瘤机制,我们利用自发转移小鼠模型和定量蛋白质组学比较了94份治疗前后血清样本中N-糖蛋白质组的变化。我们使用iTRAQ鸟枪法蛋白质组学对231种高度可信的N-糖基化蛋白进行了定量。其中,53种蛋白在整个时间过程中显示出显著不同的调控模式,其中急性期反应是增强最明显的途径。我们使用平行反应监测靶向蛋白质组学和流式细胞术对53种显著蛋白中的23种进行进一步研究,以探究急性期反应的抗肿瘤特征。我们发现冷冻热疗法将肿瘤慢性炎症重置为“急性”表型,关键调节因子包括IL-6在内的急性期蛋白上调。IL-6介导的“急性”表型将促进IL-4和调节性T细胞的ICOSL表达转变为促进Th1的IFN-γ和IL-12产生,增强补体系统激活以及CD86(+)MHCII(+)树突状细胞成熟,并增强Th1记忆细胞的增殖。此外,我们发现在这种“急性”环境下肿瘤进展和转移抑制蛋白的产生增加,有利于抗转移作用。此外,与单独的冷冻/热疗或对健康组织进行冷冻热疗相比,对肿瘤进行冷冻热疗诱导出最强的“急性”反应,并伴随着最显著的抗肿瘤免疫效应。总之,我们证明冷冻热疗法诱导的、IL-6介导的“急性”微环境将肿瘤慢性微环境从Th2免疫抑制和促肿瘤状态转变为Th1免疫刺激和杀肿瘤状态。此外,“急性”和“危险”信号的强度在决定抗肿瘤活性的疗效中起关键作用。
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