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首页> 外文期刊>Italian Journal of Anatomy and Embryology >Effects of conditioned medium from human amniotic mesenchymal tissue cell cultures on prostate cancer cells
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Effects of conditioned medium from human amniotic mesenchymal tissue cell cultures on prostate cancer cells

机译:人羊膜间质组织细胞培养条件培养基对前列腺癌细胞的影响

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摘要

It has been recently demonstrated that human amniotic mesenchymal tissue cells (hAMTC) derived from term placenta inhibit lymphocyte proliferation and significantly reduce the growth of haemopoietic and non haemopoietic cancer cell lines (HeLa and Saos cells) in vitro (1). The aim of our study was to evaluate the effects of hAMTC-conditioned medium (CM) on two human prostate cancer cells lines: LNCaP, androgen responsive and well differentiated, and PC-3, androgen unresponsive and less differentiated. Cells were grown in their standard culture conditions in the absence or in the presence of various concentrations (0.001–50%) of hAMTC-CM or their own exhausted medium. Cell numbers were determined by using a haemocytometer, after three days. Moreover, E- and N-cadherin expression was evaluated in PC-3 cells cultured in medium with 0.01, 1 or 25% hAMTC-CM by Immunocytochemistry and Western blot analysis. Our findings indicate that hAMTC-CM reduces the growth of both PC-3 and LNCaP cells. The effect is more pronounced in PC-3 cells in which inhibition is about 25% vs control (p0.001) at a very low concentration (0.001%) and reaches the maximum (about 55% vs control, p0.001) with the highest concentration used (50%). In LNCaP cells only the highest concentration of hAMTC-CM (50%) inhibits cell proliferation (about 40% vs control, p0.001). Interestingly, growth of LNCaP cells is reduced by their own exhausted medium, while proliferation of PC-3 cells is not affected by their spent medium. Both E- and N-cadherin expression have been detected at the membrane level in untreated PC-3 cells and the localization does not change in hAMTC-CM-treated cells. Preliminary data obtained by Western blot analysis seem to indicate an increase in both E- and N-cadherin levels. Our findings show that hAMTC-CM reduces prostate cancer cell proliferation in relationship to their androgen sensitivity and modifies the expression levels of adhesion molecules. Experiments are in progress to determine the mechanisms which underlie the observed effects and assess if hAMTC-CM can determine any variation in the differentiation status of prostate cancer cells.
机译:最近已证明,源自足月胎盘的人羊膜间充质组织细胞(hAMTC)在体外抑制淋巴细胞增殖并显着降低造血和非造血癌细胞系(HeLa和Saos细胞)的生长(1)。我们研究的目的是评估hAMTC条件培养基(CM)对两种人类前列腺癌细胞系的影响:LNCaP,雄激素反应性和分化良好,以及PC-3,雄激素反应性和分化程度较低。在不存在或存在各种浓度(0.001–50%)的hAMTC-CM或它们自己的耗尽培养基的情况下,细胞在其标准培养条件下生长。三天后,通过使用血细胞计数器测定细胞数。此外,通过免疫细胞化学和蛋白质印迹分析评估了在含有0.01%,1%或25%hAMTC-CM的培养基中培养的PC-3细胞中E-和N-钙粘蛋白的表达。我们的发现表明,hAMTC-CM降低了PC-3和LNCaP细胞的生长。这种作用在PC-3细胞中更为明显,在PC-3细胞中,在非常低的浓度(0.001%)时抑制率相对于对照(p <0.001)大约达到最大值(相对于对照,约55%,p <0.001)。最高使用浓度(50%)。在LNCaP细胞中,只有最高浓度的hAMTC-CM(50%)抑制细胞增殖(相对于对照,约40%,p <0.001)。有趣的是,LNCaP细胞的生长因其自身耗尽的培养基而减少,而PC-3细胞的增殖不受其所用培养基的影响。在未处理的PC-3细胞中,已在膜水平上检测到E-和N-钙粘蛋白的表达,并且在经hAMTC-CM处理的细胞中,定位没有变化。通过蛋白质印迹分析获得的初步数据似乎表明E-和N-钙粘蛋白水平均增加。我们的发现表明,hAMTC-CM降低了与雄激素敏感性相关的前列腺癌细胞增殖,并修饰了粘附分子的表达水平。实验正在进行中,以确定观察到的效应的基础,并评估hAMTC-CM是否可以确定前列腺癌细胞分化状态的任何变化。

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