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巨噬细胞在静脉注射含巨噬细胞激活剂的脂质体后对已形成转移灶的清除作用。

Involvement of macrophages in the eradication of established metastases following intravenous injection of liposomes containing macrophage activators.

作者信息

Fidler I J, Barnes Z, Fogler W E, Kirsh R, Bugelski P, Poste G

出版信息

Cancer Res. 1982 Feb;42(2):496-501.

PMID:7055801
Abstract

Liposomes containing encapsulated lymphokines or muramyl dipeptide (MDP), when injected i.v. into C57BL/6 mice, produced significant destruction of established lung and lymph node metastases from a s.c. highly metastatic B16-BL6 melanoma. We present evidence that eradication of the metastases is mediated by the activation of host macrophages to the tumoricidal state. Results from three separate types of experiments support this conclusion. (a) When macrophage-activating agents such as lymphokines of MDP were delivered in liposomes that were not efficiently retained in the lung, little or no activation of lung macrophages was observed, and growth of metastases was unaltered. (b) Eradication of metastases was not observed when tumor-bearing animals were treated with agents that impaired macrophage function (e.g., silica, carrageenan, hyperchlorinated drinking water) prior to systemic therapy with liposome-encapsulated lymphokines or liposome-encapsulated MDP. (c) Macrophages activated in vitro by liposome-encapsulated MDP and then injected i.v. into mice bearing experimental lung metastases also significantly inhibited lung metastases. These results suggest that the augmented host response against pulmonary and lymph node metastases generated by the systemic administration of liposome-encapsulated lymphokines or MDP is mediated via activated cytotoxic macrophages.

摘要

将包裹有淋巴因子或胞壁酰二肽(MDP)的脂质体经静脉注射到C57BL/6小鼠体内后,可使皮下高度转移性B16 - BL6黑色素瘤所形成的已有的肺和淋巴结转移灶受到显著破坏。我们提供的证据表明,转移灶的消除是通过将宿主巨噬细胞激活至杀肿瘤状态来介导的。来自三种不同类型实验的结果支持这一结论。(a)当巨噬细胞激活剂如MDP的淋巴因子通过不能有效滞留于肺内的脂质体递送时,未观察到肺巨噬细胞的激活,转移灶的生长也未改变。(b)在用脂质体包裹的淋巴因子或脂质体包裹的MDP进行全身治疗之前,用损害巨噬细胞功能的试剂(如二氧化硅、角叉菜胶、高氯饮用水)处理荷瘤动物时,未观察到转移灶的消除。(c)用脂质体包裹的MDP在体外激活巨噬细胞,然后经静脉注射到患有实验性肺转移的小鼠体内,也能显著抑制肺转移。这些结果表明,通过全身给予脂质体包裹的淋巴因子或MDP所产生的增强的宿主对肺和淋巴结转移灶的反应是通过激活的细胞毒性巨噬细胞介导的。

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