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在非粘性聚(甲基丙烯酸羟乙酯)基质上聚集成团生长的黑色素瘤细胞表现出多核细胞增多,但并未发展出更高的转移能力。

Melanoma cells growing in aggregates on a non-adhesive poly(HEMA) substrate exhibit polykaryocytosis but do not develop an increased metastatic capability.

作者信息

Klein P A, Xiang J H, Kimura A K

出版信息

Clin Exp Metastasis. 1984 Oct-Dec;2(4):287-95. doi: 10.1007/BF00135168.

Abstract

B16-F1 melanoma cells were plated onto plastic tissue-culture dishes rendered non-adhesive for cells by coating with 0.12 per cent poly(2-hydroxyethyl methylacrylate), poly(HEMA). These growth conditions caused the normally flat, adherent B16-F1 cells to grow as single cells in suspension. Within 24 hours, the rounded cells formed aggregates and grew at a slower rate than control cells grown at the same density on untreated plastic dishes. Microscopic observations provided evidence that polykaryocytosis was occurring among the aggregates. Following replating onto standard adhesive tissue-culture plastic, 20-30 per cent of the aggregates were observed to contain varying numbers of multinucleated giant cells (polykaryocytes). The study has revealed a previously undescribed propensity of certain B16-F1 cells cultivated as aggregates in suspension to develop into polykaryocytes, most probably as a result of spontaneous tumor cell-tumor cell fusion. The possible relevance of this behavior in vitro to events in tumor progression is discussed. This study, however, does not support the findings of others that the metastatic capability of B16-F1 cells is increased by such non-adherent culture conditions. No increase in metastatic potential was observed for B16-F1 cells, or for a low metastatic clone (F1-7) derived from it, grown for 72 or 96 hours in a spherical configuration compared to control cells grown in a flat, adherent monolayer.

摘要

将B16 - F1黑色素瘤细胞接种到用0.12%聚(甲基丙烯酸2 - 羟乙酯)(聚HEMA)包被而对细胞无黏附性的塑料组织培养皿上。这些生长条件使正常扁平、贴壁生长的B16 - F1细胞以单细胞形式悬浮生长。24小时内,圆形细胞形成聚集体,其生长速度比在未处理的塑料培养皿上以相同密度生长的对照细胞慢。显微镜观察提供了证据,表明聚集体中发生了多核化现象。在重新接种到标准的黏附性组织培养塑料上后,观察到20% - 30%的聚集体含有数量不等的多核巨细胞(多核细胞)。该研究揭示了某些在悬浮状态下聚集成团培养的B16 - F1细胞有此前未被描述的发展为多核细胞的倾向,这很可能是自发肿瘤细胞 - 肿瘤细胞融合的结果。文中讨论了这种体外行为与肿瘤进展事件可能的相关性。然而,本研究并不支持其他研究人员关于这种非黏附培养条件会增加B16 - F1细胞转移能力的发现。与在扁平贴壁单层生长的对照细胞相比,B16 - F1细胞或由其衍生的低转移克隆(F1 - 7)在球形状态下培养72或96小时后,转移潜力并未增加。

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