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大鼠发情前期/发情期转移易感性增加:雌二醇和自然杀伤细胞的可能作用。

Increased susceptibility to metastasis during pro-oestrus/oestrus in rats: possible role of oestradiol and natural killer cells.

作者信息

Ben-Eliyahu S, Page G G, Shakhar G, Taylor A N

机构信息

Department of Psychology, Tel Aviv University, Israel.

出版信息

Br J Cancer. 1996 Dec;74(12):1900-7. doi: 10.1038/bjc.1996.651.

Abstract

It has been suggested that tumour development and immunocompetence are affected by the menstrual and the oestrous cycle, and sex hormones have been shown to modulate lymphokine production, neuroendocrine activity and immunity. In this study, we assessed natural killer cell activity and host susceptibility to metastasis during the oestrous cycle in the Fischer 344 inbred rat strain. Females were inoculated intravenously with MADB106 tumour cells, a syngeneic mammary adenocarcinoma cell line that metastasises only to the lungs. The susceptibility to metastatic development of this tumour was found to be significantly higher during pro-oestrus and oestrus than during metoestrus and dioestrus. Two days of exposure to oestradiol benzoate caused similar effects in ovariectomised females, and a single administration of progesterone reduced this effect of oestradiol to a statistically non-significant level. The tumour was found to be negative for oestradiol receptors, and its in vitro proliferation rate was not affected by oestradiol or progesterone, suggesting that the effects of sex hormones on the metastatic process are not attributable to a direct effect on tumour cells. Because the metastatic process of MADB106 tumour cells is known, and confirmed here, to be highly controlled by large granular lymphocyte/natural killer (LGL/NK) cell activity, we assessed their role in mediating the effects of the oestrous cycle. The number and activity levels of circulating blood LG/NK cells (NKR-PI+ bright) were studied. Findings indicated oestrous-dependent alterations in the number of LGL/NK cells and suggested a diminished NK activity per LGL/NK cell during pro-oestrus/ oestrus, the same phases that were characterised by higher susceptibility to metastatic development. These findings provide the first empirical evidence for a causal relationship between a short-term exposure to elevated oestradiol/low progesterone levels and decreased resistance to tumour metastasis, and it is hypothesised that an alteration in LGL/NK cell activity underlies these effects. Homologies and relevance to clinical phenomena are discussed.

摘要

有人提出,肿瘤发展和免疫能力受月经周期和发情周期影响,并且已表明性激素可调节淋巴因子产生、神经内分泌活动和免疫力。在本研究中,我们评估了Fischer 344近交系大鼠发情周期期间自然杀伤细胞活性及宿主对转移的易感性。雌性大鼠经静脉接种MADB106肿瘤细胞,这是一种仅转移至肺部的同基因乳腺腺癌细胞系。发现该肿瘤在发情前期和发情期的转移易感性显著高于动情后期和间情期。对去卵巢雌性大鼠给予两天苯甲酸雌二醇导致类似效应,而单次给予孕酮可将雌二醇的这种效应降低至统计学上无显著意义的水平。发现该肿瘤雌激素受体呈阴性,其体外增殖率不受雌二醇或孕酮影响,这表明性激素对转移过程的影响并非归因于对肿瘤细胞的直接作用。由于已知且在此证实MADB106肿瘤细胞的转移过程受大颗粒淋巴细胞/自然杀伤(LGL/NK)细胞活性高度控制,我们评估了它们在介导发情周期效应中的作用。研究了循环血液中LG/NK细胞(NKR-PI + 明亮)的数量和活性水平。研究结果表明LGL/NK细胞数量存在发情期依赖性改变,并提示在发情前期/发情期每个LGL/NK细胞的NK活性降低,而这两个时期的特征是对转移发展的易感性较高。这些发现为短期暴露于升高的雌二醇/低孕酮水平与肿瘤转移抵抗力降低之间的因果关系提供了首个实证依据,并且据推测LGL/NK细胞活性的改变是这些效应的基础。文中还讨论了与临床现象的同源性和相关性。

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