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门静脉接种肿瘤细胞对抗肿瘤免疫潜能的抑制作用。

Suppressive effect of portal venous inoculation with tumor cells on the anti-tumor immune potential.

作者信息

Kokudo S, Qian J H, Fujiwara H, Hamaoka T

机构信息

Department of Oncogenesis, Osaka University Medical School.

出版信息

Jpn J Cancer Res. 1987 Sep;78(9):946-51.

PMID:3117751
Abstract

The effect of portal venous (pv) administration of syngeneic tumor cells on the potential to generate anti-tumor immune resistance was examined. C3H/He mice were inoculated with syngeneic X5563 tumor cells via the pv or intravenous (iv) route. A single pv administration of 10,000 R X-irradiated X5563 cells into C3H/He mice not only failed to induce anti-X5563 immunity but also abolished the capability of the mice to develop anti-X5563 in vitro cytotoxic and in vivo protective immunity as induced by intradermal (id) inoculation of viable X5563 cells followed by the surgical resection of the tumor (immunization procedure). Such immunosuppression was also obtained by pv inoculation of tumor cells after the above immunization procedure. The immunosuppression induced by the pv injection of tumor cells before or after the immunization procedure was tumor-specific, since the pv sensitizing regimen using X5563 tumor cells did not interfere with the generation of immunity against another syngeneic tumor, MH134. More importantly, the pv route-induced suppression contrasted with the lack of inhibiting effect of iv inoculation with tumor cells on the induction of the tumor immunity. These results indicate that the host's tumor-specific immune capability is markedly suppressed in an anti-tumor sensitizing stage-independent manner when tumor cells enter the pv circulation.

摘要

研究了经门静脉(pv)注射同基因肿瘤细胞对产生抗肿瘤免疫抗性潜力的影响。通过门静脉或静脉内(iv)途径给C3H/He小鼠接种同基因X5563肿瘤细胞。对C3H/He小鼠经门静脉单次注射10,000 R X射线照射的X5563细胞,不仅未能诱导抗X5563免疫,而且还消除了小鼠经皮内(id)接种活X5563细胞随后手术切除肿瘤(免疫程序)所诱导的产生体外抗X5563细胞毒性和体内保护性免疫的能力。在上述免疫程序后经门静脉接种肿瘤细胞也可获得这种免疫抑制。免疫程序之前或之后经门静脉注射肿瘤细胞所诱导的免疫抑制具有肿瘤特异性,因为使用X5563肿瘤细胞的门静脉致敏方案不干扰针对另一种同基因肿瘤MH134的免疫产生。更重要的是,门静脉途径诱导的抑制与静脉接种肿瘤细胞对肿瘤免疫诱导缺乏抑制作用形成对比。这些结果表明,当肿瘤细胞进入门静脉循环时,宿主的肿瘤特异性免疫能力在与抗肿瘤致敏阶段无关的情况下受到明显抑制。

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