Promotion of L1210 tumour growth by macrophages.

R P Huget, H D Flad, H G Opitz
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Abstract

Low numbers (10(4)) of peritoneal exudate L1210 mouse lymphoma cells were injected into DBA/2 mice subcutaneously and the development of tumours was followed. Tumour takes occurred in 100% of the animals within 9 days after tumour transplantation. The latent period of tumour development was prolonged by 6-10 days when tumour cells of the peritoneal exudate, depleted of adherent/phagocytic cells, were used in the inoculum or when tumour cells derived from continuous cell cultures were used. Addition of adherent cells in high numbers to in-vitro-derived L1210 cells accelerated tumour growth. This effect was found to be not specific for adherent/phagocytic cells, as liver cells had the same influence on tumour growth. It is concluded that, under certain experimental conditions, a cell population with the functional properties of macrophages is able to promote tumour development, most likely due to their non-specific effect on the micro-environment of the growing tumour.

巨噬细胞促进L1210肿瘤生长。
将少量(10(4))腹腔渗出液L1210小鼠淋巴瘤细胞皮下注射到DBA/2小鼠体内,观察肿瘤的发展情况。100%的动物在肿瘤移植后9天内发生肿瘤。当将腹膜渗出液中的肿瘤细胞用于接种或使用连续细胞培养的肿瘤细胞时,肿瘤发展的潜伏期延长了6-10天。在体外培养的L1210细胞中大量添加贴壁细胞可加速肿瘤生长。研究发现,这种效应对粘附细胞/吞噬细胞不具有特异性,因为肝细胞对肿瘤生长具有相同的影响。综上所述,在一定的实验条件下,具有巨噬细胞功能特性的细胞群能够促进肿瘤的发展,这很可能是由于它们对生长肿瘤的微环境具有非特异性作用。
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