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菊粉在小鼠体内的抗黑色素瘤活性。

The anti-melanoma activity of inulin in mice.

作者信息

Cooper P D, Carter M

出版信息

Mol Immunol. 1986 Aug;23(8):903-8. doi: 10.1016/0161-5890(86)90076-3.

Abstract

Finely divided, insoluble inulin (gamma polymorph), given intraperitoneally (i.p.) to C57BL mice 1-3 days after i.p. B16 melanoma cells, very significantly increased their mean survival time (MST) in low doses (less than or equal to 40 and less than or equal to 100 micrograms/mouse in 50 and 80% of tests, respectively). The gamma inulin was pure and free of endotoxin and soluble inulin, and was developed as a potent reagent specific for activating the alternative pathway of complement (APC). Its antitumour action paralleled its in vitro APC activation, namely, both activities were sharply dose-dependent up to a threshold dose above which they were dose-independent; dissolved inulin was inactive in vitro and in vivo, decreased the MST of the mice and in a mixture antagonized the in vitro and in vivo activities of gamma inulin; the more soluble (alpha) polymorphs were active in proportion to their gamma content but the effects were blocked at higher doses presumably by dissolved inulin. In addition, depletion of host APC with cobra venom factor or inulin before giving B16 cells increased their malignancy and abrogated the subsequent antitumour action of gamma inulin. The minimum i.p. dose of gamma inulin found to activate serum APC in vivo was 50 micrograms (2.5 mg/kg), i.e. close to the minimum antitumour dose. These close correlations and the specificity of the reagent indicate that activation in vivo of the APC (cellular or humoral) is an important first contact in stimulating host antitumour defences in this mouse model.

摘要

在腹腔注射B16黑色素瘤细胞后1 - 3天,给C57BL小鼠腹腔注射细粉状、不溶性菊粉(γ多晶型物),低剂量(分别在50%和80%的试验中小于或等于40微克/小鼠和小于或等于100微克/小鼠)时能非常显著地延长其平均存活时间(MST)。γ菊粉纯净且无内毒素和可溶性菊粉,它是作为一种激活补体替代途径(APC)的有效试剂而研制的。其抗肿瘤作用与其体外APC激活作用平行,即两种活性在达到阈值剂量之前均呈急剧的剂量依赖性,超过该阈值则与剂量无关;溶解的菊粉在体外和体内均无活性,会缩短小鼠的MST,且在混合物中会拮抗γ菊粉的体外和体内活性;更易溶解的(α)多晶型物的活性与其γ含量成比例,但在较高剂量时其作用可能被溶解的菊粉阻断。此外,在注射B16细胞前用眼镜蛇毒因子或菊粉消耗宿主的APC会增加其恶性程度,并消除γ菊粉随后的抗肿瘤作用。发现γ菊粉在体内激活血清APC的最小腹腔注射剂量为50微克(2.5毫克/千克),即接近最小抗肿瘤剂量。这些密切的相关性以及该试剂的特异性表明,在该小鼠模型中,体内APC(细胞或体液)的激活是刺激宿主抗肿瘤防御的重要初次接触。

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