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血行性B16黑色素瘤变异体在硬脑膜中的肿瘤生长差异与肿瘤-宿主细胞反应有关。

Differential tumor growth of blood-borne B16 melanoma variants in cerebral dura mater is related to tumor-host cell reactions.

作者信息

Kawaguchi T, Kawaguchi M, Lembo T M, Nicolson G L

机构信息

Second Department of Pathology, Fukushima Medical College, Japan.

出版信息

Clin Exp Metastasis. 1989 Jan-Feb;7(1):1-14. doi: 10.1007/BF02057177.

Abstract

Intracarotid injection of B16-B14b or B16-B15b melanoma cells, previously established from B16-F1 melanoma by in vivo selection fourteen- or fifteen-times, respectively, for brain surface colonization, preferentially produced tumor nodules in mice at brain surface sites, most frequently in the dura mater, followed by the leptomeninges and cerebral cortex. There was a marked difference, however, in tumor growth at these sites using the two B16 sublines. Intracarotid injection of B16-B14b cells rarely produced visible tumors, whereas B16-B15b cells formed deeply pigmented tumors up to 7 mm in diameter in the brain menings of almost all mice examined. Histologic and electron microscopic investigation revealed that B16-B14b tumors evoked dramatic immunocyte cell infiltration and granulomatous reactions, while B16-B15b tumors were accompanied by much less tumor-host cell reactions. Splenectomy or laparotomy 1-2 weeks before or after intracarotid injection of B16-B14b cells dramatically enhanced tumor growth in the dura mater without extensive tumor-host cell reactions. The results suggest that the differential growth of B16-B14b and B16-B15b tumor cells in the cerebral dura mater is based, in part, on the abilities of these melanoma cells to elicit host cell reactions.

摘要

分别通过体内筛选14次或15次从B16-F1黑色素瘤建立的、用于脑表面定植的B16-B14b或B16-B15b黑色素瘤细胞,经颈内注射后,优先在小鼠脑表面部位产生肿瘤结节,最常见于硬脑膜,其次是软脑膜和大脑皮层。然而,使用这两个B16亚系时,这些部位的肿瘤生长存在显著差异。经颈内注射B16-B14b细胞很少产生可见肿瘤,而B16-B15b细胞在几乎所有检测的小鼠脑脑膜中形成直径达7毫米的深色肿瘤。组织学和电子显微镜研究表明,B16-B14b肿瘤引发显著的免疫细胞浸润和肉芽肿反应,而B16-B15b肿瘤伴随的肿瘤-宿主细胞反应则少得多。在经颈内注射B16-B14b细胞之前或之后1-2周进行脾切除术或剖腹术,可显著增强硬脑膜中的肿瘤生长,且无广泛的肿瘤-宿主细胞反应。结果表明,B16-B14b和B16-B15b肿瘤细胞在脑硬脑膜中的差异生长部分基于这些黑色素瘤细胞引发宿主细胞反应的能力。

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