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细胞间通讯在促进C3H/10T1/2细胞转化中的作用。

Role of intercellular communication in the promotion of C3H/10T1/2 cell transformation.

作者信息

Dorman B H, Butterworth B E, Boreiko C J

出版信息

Carcinogenesis. 1983 Sep;4(9):1109-15. doi: 10.1093/carcin/4.9.1109.

Abstract

The effects of 12-O-tetradecanoylphorbol-13-acetate (TPA) upon intercellular communication and promotion were studied in cultures of C3H/10T1/2 mouse embryo fibroblasts. Cell-to-cell communication was quantitated by autoradiographic analysis of [3H]uridine transfer from prelabelled donor cells to an excess of unlabelled recipient cells during a 4 h co-cultivation. Extensive transfer of label was observed from donor to recipient cells in contact. Treatment of non-transformed C3H/10T1/2 cultures with 250 ng/ml TPA at co-cultivation of donor and recipient cells markedly inhibited intercellular communication during the 4 h incubation, producing an 80% reduction in uridine exchange relative to solvent-treated control cultures. Concentrations of TPA ranging from 0.25 to 25 ng/ml were also effective in inhibiting [3H]uridine exchange in a dose dependent fashion from 13% to 74%. This inhibition of intercellular communication was transient; cells exposed to 250 ng/ml TPA for 1.5 h prior to co-cultivation with TPA exhibited a 60% inhibition and the exchange of uridine had increased to control values in cultures pretreated for 12-72 h. An examination of label transfer between non-transformed and transformed C3H/10T1/2 cells indicated that both the extent of inhibition by TPA and the kinetics of communication inhibition were similar to that observed for non-transformed cells. Initiation and promotion experiments demonstrated that exposure to 250 ng/ml TPA for 5 weeks, but not to reduced concentrations of 0.25, 2.5 or 25 ng/ml, was capable of promoting morphological transformation. The lack of correlation between the dose responses of TPA for promotion and for reduction of cell-to-cell communication, and the transient nature of intercellular communication inhibition by TPA, suggests that an inhibition of cell-to-cell communication is not a sufficient event for promotion of oncogenic transformation in these cells.

摘要

在C3H/10T1/2小鼠胚胎成纤维细胞培养物中研究了12 - O - 十四烷酰佛波醇 - 13 - 乙酸酯(TPA)对细胞间通讯和促癌作用的影响。通过放射自显影分析在4小时共培养期间从预先标记的供体细胞向过量未标记受体细胞转移的[3H]尿苷来定量细胞间通讯。观察到标记物从供体细胞广泛转移到接触的受体细胞。在供体细胞和受体细胞共培养时,用250 ng/ml TPA处理未转化的C3H/10T1/2培养物,在4小时孵育期间显著抑制细胞间通讯,相对于溶剂处理的对照培养物,尿苷交换减少了80%。浓度范围为0.25至25 ng/ml的TPA也以剂量依赖性方式有效抑制[3H]尿苷交换,抑制率从13%至74%。这种细胞间通讯的抑制是短暂的;在与TPA共培养前用250 ng/ml TPA处理1.5小时的细胞表现出60%的抑制,而在预处理12 - 72小时的培养物中尿苷交换已增加到对照值。对未转化和转化的C3H/10T1/2细胞之间标记物转移的检查表明,TPA的抑制程度和通讯抑制动力学与未转化细胞中观察到的相似。启动和促癌实验表明,暴露于250 ng/ml TPA 5周,但不是暴露于0.25、2.5或25 ng/ml的较低浓度,能够促进形态转化。TPA促癌作用和细胞间通讯减少的剂量反应之间缺乏相关性,以及TPA对细胞间通讯抑制的短暂性质,表明细胞间通讯的抑制对于这些细胞中致癌转化的促进不是一个充分的事件。

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