Saito Hidemi, Inagaki Yukiko, Tsunenari Toshiaki, Ura Masako, Mizuno Hideaki, Fujimoto-Ouchi Kaori, Onuma Etsuro, Sato Koh, Ogata Etsuro, Yamada-Okabe Hisafumi
Pharmaceutical Research Department III, Chugai Pharmaceutical Co., Ltd., Kamakura, Kanagawa, Japan.
Cancer Sci. 2007 Oct;98(10):1563-9. doi: 10.1111/j.1349-7006.2007.00568.x. Epub 2007 Jul 23.
It has been shown that in the mouse colon 26 tumor model, tumors grown in the subcutis (subcutis colon 26) caused early onset of cachectic syndromes, whereas those in the liver (liver colon 26) did not. Both interleukin (IL)-6 and parathyroid hormone-related protein (PTHrP) were involved in the development of cachectic syndromes in this tumor model. However, whether expression of PTHrP and IL-6 is differently regulated in the tumor microenvironment is unclear. In the present study, culturing the colon 26 cells under different conditions in vitro revealed that IL-6 production was increased by monolayer culture under a low-glucose condition but not by spheroid culture. In contrast, PTHrP production was increased by spheroid culture but not by monolayer culture, even under a low-glucose condition. Gene expression profiling revealed that the expression of cyclooxygenase (COX)-2 was up-regulated in both subcutis colon 26 and spheroid cultures, and that COX-2 inhibitor NS-398 suppressed PTHrP production in spheroid cultures. Furthermore, administration of NS-398 decreased the PTHrP level without affecting the tumor growth in mice bearing subcutis colon 26. These results demonstrate that production of PTHrP and IL-6 largely depends on the microenvironments in which tumors are developed or metastasized and that up-regulation of COX-2 in a necrobiotic environment leads to PTHrP production, thereby causing cachectic syndromes.
研究表明,在小鼠结肠26肿瘤模型中,皮下生长的肿瘤(皮下结肠26)会导致恶病质综合征的早期发作,而肝脏中的肿瘤(肝脏结肠26)则不会。白细胞介素(IL)-6和甲状旁腺激素相关蛋白(PTHrP)均参与了该肿瘤模型中恶病质综合征的发生发展。然而,PTHrP和IL-6的表达在肿瘤微环境中是否受到不同调节尚不清楚。在本研究中,体外在不同条件下培养结肠26细胞发现,低葡萄糖条件下单层培养可增加IL-6的产生,但球体培养则不会。相反,即使在低葡萄糖条件下,球体培养可增加PTHrP的产生,而单层培养则不会。基因表达谱分析显示,皮下结肠26和球体培养中环氧合酶(COX)-2的表达均上调,且COX-2抑制剂NS-398可抑制球体培养中PTHrP的产生。此外,给予NS-398可降低皮下结肠26荷瘤小鼠的PTHrP水平,而不影响肿瘤生长。这些结果表明,PTHrP和IL-6的产生很大程度上取决于肿瘤发生或转移的微环境,且在坏死环境中COX-2的上调会导致PTHrP的产生,从而引起恶病质综合征。