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口服螺旋藻提取物增强小鼠抗肿瘤自然杀伤细胞的激活

Enhancement of antitumor natural killer cell activation by orally administered Spirulina extract in mice.

作者信息

Akao Yuusuke, Ebihara Takashi, Masuda Hisayo, Saeki Yoshiko, Akazawa Takashi, Hazeki Kaoru, Hazeki Osamu, Matsumoto Misako, Seya Tsukasa

机构信息

Department of Microbiology and Immunology, Hokkaido University Graduate School of Medicine, Kita-15, Nishi-7, Kita-ku Sapporo 060-8638, Japan.

出版信息

Cancer Sci. 2009 Aug;100(8):1494-501. doi: 10.1111/j.1349-7006.2009.01188.x. Epub 2009 May 6.

Abstract

Oral administration of hot-water extract of Spirulina, cyanobacterium Spirulina platensis, leads to augmentation of NK cytotoxicity in humans. Here, we applied to syngeneic tumor-implant mice (C57BL/6 versus B16 melanoma) Spirulina to elucidate the mechanism of raising antitumor NK activation. A B16D8 subcell line barely expressed MHC class I but about 50% expressed Rae-1, a ligand for NK activation receptor NKG2D. The Rae-1-positive population of implant B16 melanoma was effectively eliminated in the tumor mass progressed in mice. This antitumor activity was induced in parallel with IFN-gamma and abolished in mice by treatment with asialoGM-1 but not CD8beta Ab, suggesting the effector is NK cell. NK cell activation occurred in the spleen of wild-type mice medicated with Spirulina. This Spirulina-mediated enhanced NK activation was abrogated in MyD88 -/- mice but not in TICAM-1 -/- mice. The NK activating properties of Spirulina depending on MyD88 were confirmed with in vitro bone marrow-derived dendritic cells expressing TLR2/4. In D16D8 tumor challenge studies, the antitumor effect of Spirulina was abolished in MyD88 -/- mice. Hence, orally administered Spirulina enhances tumoricidal NK activation through the MyD88 pathway. Spirulina exerted a synergistic antitumor activity with BCG-cell wall skeleton, which is known to activate the MyD88 pathway via TLR2/4 with no NK enhancing activity. Spirulina and BCG-cell wall skeleton synergistically augmented IFN-gamma production and antitumor potential in the B16D8 versus C57BL/6 system. We infer from these results that NK activation by Spirulina has some advantage in combinational use with BCG-cell wall skeleton for developing adjuvant-based antitumor immunotherapy.

摘要

口服蓝藻螺旋藻热水提取物可增强人体自然杀伤细胞(NK)的细胞毒性。在此,我们将螺旋藻应用于同基因肿瘤植入小鼠(C57BL/6小鼠与B16黑色素瘤模型),以阐明其增强抗肿瘤NK细胞活性的机制。B16D8亚细胞系几乎不表达MHC I类分子,但约50%表达Rae-1,Rae-1是NK激活受体NKG2D的配体。在小鼠体内肿瘤进展过程中,植入的B16黑色素瘤中Rae-1阳性群体在肿瘤块中被有效清除。这种抗肿瘤活性与干扰素-γ平行诱导产生,在用去唾液酸GM-1处理的小鼠中被消除,但用CD8β抗体处理则无此效果,这表明效应细胞是NK细胞。在用螺旋藻给药的野生型小鼠脾脏中发生了NK细胞激活。螺旋藻介导的NK细胞激活增强在MyD88基因敲除小鼠中被消除,但在TICAM-1基因敲除小鼠中未被消除。通过体外表达TLR2/4的骨髓来源树突状细胞证实了螺旋藻依赖MyD88的NK激活特性。在D16D8肿瘤攻击实验中,螺旋藻的抗肿瘤作用在MyD88基因敲除小鼠中被消除。因此,口服螺旋藻通过MyD88途径增强了具有杀肿瘤活性的NK细胞激活。螺旋藻与卡介苗细胞壁骨架发挥了协同抗肿瘤活性,已知卡介苗细胞壁骨架通过TLR2/4激活MyD88途径且无增强NK细胞活性的作用。在B16D8与C57BL/6系统中,螺旋藻和卡介苗细胞壁骨架协同增强了干扰素-γ的产生及抗肿瘤潜力。从这些结果我们推断,在基于佐剂的抗肿瘤免疫治疗的联合应用中,螺旋藻激活NK细胞具有一定优势。

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