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腹部预先照射对人工和自发性肺转移的抑制作用——II. 靶器官与机制

Inhibition of artificial and spontaneous lung metastases by preirradiation of abdomen--II. Target organ and mechanism.

作者信息

Ando K, Peters L J, Hunter N, Jinnouchi K, Matsumoto T

出版信息

Br J Cancer. 1983 Jan;47(1):73-9. doi: 10.1038/bjc.1983.9.

Abstract

We have previously reported that irradiation of the abdomen of mice before i.v. injection of both immunogenic and nonimmunogenic tumour cells is capable of suppressing their ability to form metastatic lung nodules in a time and dose-dependent fashion. Experiments with segmental exposure indicated the target organ to be located in the ventral half of the abdomen. The effect has now been shown positively to depend upon irradiation of the caecum, and can be abolished either by shielding the caecum from irradiation or by surgically removing it prior to irradiation. Further experiments have shown that the effect cannot be elicited in germ-free mice and that its magnitude is markedly reduced in animals given gut-sterilizing antibiotics. Split-dose irradiation only slightly reduced the magnitude of suppression, provided both doses were given within the time window of effectiveness of single doses. Tumour-growth retardation was observed and spontaneous lung metastases were also suppressed when tumour-bearing mice received abdominal irradiation 7 days after tumour cell transplantation into the leg. However, abdominal irradiation did not significantly reduce subsequent tumour transplantability by the s.c. or i.p. routes. The experimental data are consistent with a mechanism by which transmigration of enteric bacteria across the radiation-damaged mucous membrane of the caecum effectively results in an endogenous infusion of endotoxin.

摘要

我们之前报道过,在静脉注射免疫原性和非免疫原性肿瘤细胞之前对小鼠腹部进行照射,能够以时间和剂量依赖的方式抑制它们形成转移性肺结节的能力。分段照射实验表明靶器官位于腹部的腹侧半部分。现在已经证实,这种效应确实取决于对盲肠的照射,并且通过将盲肠屏蔽于照射之外或在照射前手术切除盲肠,这种效应均可消除。进一步的实验表明,在无菌小鼠中不会引发这种效应,并且在给予肠道杀菌抗生素的动物中其效应程度会显著降低。如果两次分割剂量都在单次剂量的有效时间窗口内给予,那么分割剂量照射只会轻微降低抑制程度。当荷瘤小鼠在肿瘤细胞移植到腿部7天后接受腹部照射时,观察到肿瘤生长延迟,并且自发性肺转移也受到抑制。然而,腹部照射并没有显著降低随后通过皮下或腹腔途径进行肿瘤移植的能力。实验数据与一种机制相符,即肠道细菌通过辐射损伤的盲肠黏膜迁移有效地导致内源性内毒素注入。

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