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同基因小鼠对肿瘤细胞的强烈破坏作用:巨噬细胞、补体激活及肿瘤细胞因子的作用

Intense tumour-cell destruction by syngeneic mice: role of macrophages, complement activation and tumour-cell factors.

作者信息

Orbach-Arbouys S, Lheritier J, Allouche M, Pouillart P

出版信息

Br J Cancer. 1977 Dec;36(6):743-50. doi: 10.1038/bjc.1977.257.

Abstract

When injected i.p. and in large numbers (10(7)) into syngeneic mice, 125IUdR-labelled L1210 cells are rapidly destroyed in a small proportion of animals, while in the other animals the lysis is low. This bimodal distribution is clearly visible 24 h after cell injection. The intense lysis occurs in fewer animals when macrophage-derived lysosomal enzymes are inhibited by trypan blue and if the complement is depleted by high doses of cobra venom factor (CVF). The intense destruction occurs in more animals after adjuvant treatment, if the mice are latently contaminated, after a moderate production of C3b by low doses of CVF, or after the injection of a tumour-cell dialysate. The destruction seems to be the result of positive feedback reaction which involves at least macrophages and complement activation.

摘要

当将大量(10⁷)经125IUdR标记的L1210细胞腹腔注射到同基因小鼠体内时,一小部分动物体内的这些细胞会迅速被破坏,而在其他动物中细胞裂解程度较低。细胞注射24小时后,这种双峰分布清晰可见。当巨噬细胞衍生的溶酶体酶被台盼蓝抑制且补体被高剂量眼镜蛇毒因子(CVF)耗尽时,发生强烈裂解的动物数量减少。如果小鼠被潜在污染、经低剂量CVF适度产生C3b后或注射肿瘤细胞透析液后进行佐剂治疗,更多动物会发生强烈破坏。这种破坏似乎是一种正反馈反应的结果,该反应至少涉及巨噬细胞和补体激活。

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