Systemic Platelet-activating Factor Receptor Activation Augments Experimental Lung Tumor Growth and Metastasis.

Cancer growth and metastasis Pub Date : 2014-06-19 eCollection Date: 2014-01-01 DOI:10.4137/CGM.S14501

Patrick C Hackler, Sarah Reuss, Raymond L Konger, Jeffrey B Travers, Ravi P Sahu

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引用次数: 30

Abstract

Pro-oxidative stressors including cigarette smoke (CS) generate novel lipids with platelet-activated factor-receptor (PAF-R) agonistic activity mediate systemic immunosuppression, one of the most recognized events in promoting carcinogenesis. Our previous studies have established that these oxidized-PAF-R-agonists augment murine B16F10 melanoma tumor growth in a PAF-R-dependent manner because of its effects on host immunity. As CS generates PAF-R agonists, the current studies sought to determine the impact of PAF-R agonists on lung cancer growth and metastasis. Using the murine Lewis Lung Carcinoma (LLC1) model, we demonstrate that treatment of C57BL/6 mice with a PAF-R agonist augments tumor growth and lung metastasis in a PAF-R-dependent manner as these findings were not seen in PAF-R-deficient mice. Importantly, this effect was because of host rather than tumor cells PAF-R dependent as LLC1 cells do not express functional PAF-R. These findings indicate that experimental lung cancer progression can be modulated by the PAF system.

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系统性血小板活化因子受体激活增强实验性肺肿瘤生长和转移。

包括香烟烟雾(CS)在内的促氧化应激源产生具有血小板活化因子受体(PAF-R)激动活性的新型脂质介导全身免疫抑制，这是促进癌变的最公认的事件之一。我们之前的研究已经证实，这些氧化的paf - r激动剂以paf - r依赖的方式促进小鼠B16F10黑色素瘤肿瘤的生长，因为它对宿主免疫有影响。由于CS产生PAF-R激动剂，目前的研究试图确定PAF-R激动剂对肺癌生长和转移的影响。使用小鼠Lewis肺癌(LLC1)模型，我们证明了用PAF-R激动剂治疗C57BL/6小鼠以PAF-R依赖的方式增强肿瘤生长和肺转移，因为这些发现在PAF-R缺乏的小鼠中没有看到。重要的是，这种影响是由于宿主而不是肿瘤细胞依赖PAF-R，因为LLC1细胞不表达功能性PAF-R。这些发现表明，PAF系统可以调节实验性肺癌的进展。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Cancer growth and metastasis

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