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首页> 外文期刊>Radiation Research: Official Organ of the Radiation Research Society >Cell-cell contact during gamma irradiation is not required to induce a bystander effect in normal human keratinocytes: Evidence for release during irradiation of a signal controlling survival into the medium
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Cell-cell contact during gamma irradiation is not required to induce a bystander effect in normal human keratinocytes: Evidence for release during irradiation of a signal controlling survival into the medium

机译:在正常的人类角质形成细胞中,不需要在γ射线照射下的细胞间接触来引起旁观者效应:在照射信号的过程中释放的证据表明,该信号控制了细胞的存活率

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摘要

Killing of unirradiated cells by medium from cultures of irradiated cells implies the release of a cytotoxic substance by the irradiated cells. The finding of the gamma-ray-induced cytotoxic effect exclusively in epithelial cells and not in fibroblasts suggested that tissue architecture or cell communication might be important, Normal human keratinocytes and fibroblasts and radiosensitive carcinoma cells were irradiated as single cells, microcolonies of three or four cells, or confluent monolayers. The medium was removed and filtered, and cultures which had never been irradiated were seeded at cloning densities and treated with the medium from the irradiated cells. It was found that the degree of cell-cell contact had no effect on the ability of medium from irradiated epithelial cell cultures to reduce the clonogenic survival of unirradiated cells. Cell density was the only important factor. Inhibition of gap junction intercellular communication using the tumor promoter phorbol myristate acid (PMA), which closes gap junctions, increased killing by the bystander effect when the PMA was added to epithelial cells prior to irradiation. Rescue of epithelial cells exposed to the medium from the irradiated cells was not possible even after only 30 min exposure. This suggests that a signal transduction mechanism may control death or survival by the bystander effect rather than by release of a factor which is directly cytotoxic. (C) 1998 by Radiation Research Society. [References: 28]
机译:培养基从辐照细胞的培养物中杀死未辐照细胞意味着被辐照细胞释放细胞毒性物质。仅在上皮细胞而不在成纤维细胞中发现了伽马射线诱导的细胞毒性作用,这表明组织结构或细胞通讯可能很重要。正常人角质形成细胞和成纤维细胞以及放射敏感性癌细胞被辐射为单细胞,三到四个微殖民地细胞或汇合的单层。除去培养基并过滤,以克隆密度接种从未辐照过的培养物,并用来自辐照过的细胞的培养基处理。发现细胞间的接触程度对来自辐照上皮细胞培养物的培养基降低未辐照细胞的克隆形成存活的能力没有影响。细胞密度是唯一重要的因素。当在辐射前将PMA添加到上皮细胞中时,使用封闭的间隙连接的肿瘤启动子佛波肉豆蔻酸(PMA)抑制了间隙连接的细胞间通讯,增加了旁观者的杀伤力。即使仅暴露30分钟,也不可能从受辐照的细胞中拯救暴露于培养基的上皮细胞。这表明信号转导机制可以通过旁观者效应而不是通过释放直接具有细胞毒性的因子来控制死亡或存活。 (C)1998年,辐射研究学会。 [参考:28]

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