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Walker-256 肿瘤生长受到鲨鱼肝和鱼油的独立或联合慢性摄入的抑制:这种反应与 Wistar 大鼠腹腔巨噬细胞亚硝酸盐生成的增加有关。

Walker-256 tumor growth is inhibited by the independent or associative chronic ingestion of shark liver and fish oil: a response linked by the increment of peritoneal macrophages nitrite production in Wistar rats.

机构信息

Department of Physiology, Federal University of Paraná, Curitiba-PR, Brazil.

出版信息

Nutr Res. 2010 Nov;30(11):770-6. doi: 10.1016/j.nutres.2010.09.015.

DOI:10.1016/j.nutres.2010.09.015
PMID:21130296
Abstract

Fish oil (FO) is widely known by its capacity to positively modulate immune parameters and decrease the growth of some tumors. Despite the enormous number of studies addressing the effects of FO, there are few reports showing similar results using other marine sources of lipid compounds with biologic importance. This study aimed to compare the effects of shark liver oil (SLO), which is a source of omega-3 fatty acids and alkylglycerols, with those obtained with FO administration, or the association of both, on tumor growth and the innate immune system in Walker-256 tumor-bearing rats. Beginning at 21 days of age, Wistar rats were fed regular chow and/or FO and/or SLO supplement (1 g/kg body weight per day) for 14 weeks. Walker-256 tumor cells were inoculated on the 90th day. As expected, 14 days after inoculation, rats fed with FO presented tumor weights that were 50% lower than the control tumors (P < .05). The association of both FO and SLO and ingestion of SLO alone also reached the same reduction level. Except for adhesion, all macrophage parameters assayed were 200% higher in rats fed with FO and those supplemented with both FO and SLO compared with control rats. Only reactive nitrogen species production was increased by SLO. These results suggest that SLO might also have indirect antitumor properties. Conversely, there were no additive effects when SLO was administered with FO. Therefore, SLO is another marine compound with in vivo antitumor effects, but its action mechanisms seem not to be related to major modifications on macrophage function.

摘要

鱼油(FO)以其能够正向调节免疫参数和抑制某些肿瘤生长的能力而广为人知。尽管有大量研究探讨了 FO 的作用,但很少有报道显示使用其他具有生物学重要性的海洋脂质化合物来源的类似结果。本研究旨在比较鲨鱼肝油(SLO)的作用,SLO 是 ω-3 脂肪酸和烷氧基甘油的来源,与 FO 给药或两者联合使用对 Walker-256 荷瘤大鼠肿瘤生长和固有免疫系统的影响。从 21 天大开始,Wistar 大鼠喂食常规饲料和/或 FO 和/或 SLO 补充剂(每天 1 g/kg 体重)14 周。在第 90 天接种 Walker-256 肿瘤细胞。正如预期的那样,接种后 14 天,喂食 FO 的大鼠的肿瘤重量比对照肿瘤低 50%(P<0.05)。FO 和 SLO 的联合以及单独摄入 SLO 也达到了相同的降低水平。除了黏附,与对照大鼠相比,喂食 FO 和 FO 和 SLO 联合补充的大鼠的所有巨噬细胞参数均增加了 200%。只有 SLO 增加了活性氮物种的产生。这些结果表明 SLO 也可能具有间接的抗肿瘤特性。相反,当 SLO 与 FO 一起给药时,没有相加作用。因此,SLO 是另一种具有体内抗肿瘤作用的海洋化合物,但它的作用机制似乎与巨噬细胞功能的重大改变无关。

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Walker-256 tumor growth is inhibited by the independent or associative chronic ingestion of shark liver and fish oil: a response linked by the increment of peritoneal macrophages nitrite production in Wistar rats.Walker-256 肿瘤生长受到鲨鱼肝和鱼油的独立或联合慢性摄入的抑制:这种反应与 Wistar 大鼠腹腔巨噬细胞亚硝酸盐生成的增加有关。
Nutr Res. 2010 Nov;30(11):770-6. doi: 10.1016/j.nutres.2010.09.015.
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引用本文的文献

1
Antitumor and anti-cachectic effects of shark liver oil and fish oil: comparison between independent or associative chronic supplementation in Walker 256 tumor-bearing rats.鲨鱼肝油和鱼油的抗肿瘤和抗恶病质作用:在 Walker 256 荷瘤大鼠中分别或联合进行慢性补充的比较。
Lipids Health Dis. 2013 Oct 16;12:146. doi: 10.1186/1476-511X-12-146.
2
The effectiveness of fish oil supplementation in asthmatic rats is limited by an inefficient action on ASM function.鱼油补充剂对哮喘大鼠的有效性受到其对气道平滑肌(ASM)功能作用效率低下的限制。
Lipids. 2013 Sep;48(9):889-97. doi: 10.1007/s11745-013-3804-4. Epub 2013 Jun 7.