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首页> 外文期刊>The Prostate >Cytotoxic sensitivity to tumor necrosis factor-alpha in PC3 and LNCaP prostatic cancer cells is regulated by extracellular levels of SGP-2 (clusterin).
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Cytotoxic sensitivity to tumor necrosis factor-alpha in PC3 and LNCaP prostatic cancer cells is regulated by extracellular levels of SGP-2 (clusterin).

机译:PC3和LNCaP前列腺癌细胞对肿瘤坏死因子-α的细胞毒敏感性受细胞外SGP-2(簇蛋白)水平的调节。

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摘要

BACKGROUND: SGP-2 is a ubiquitous secreted glycoprotein that prevents cellular apoptosis. This study was carried out to determine the extracellular action of SGP-2 in a model of tumor necrosis factor-alpha (TNF)-induced cytotoxicity using two human prostatic cancer lines, LNCaP and PC3. These two lines were selected because LNCaP cells are highly sensitive to the cytotoxic effect of TNF, while PC3 cells are resistant to TNF at 24 hr. METHODS: Cells were cultured in the presence or absence of TNF (10 ng/ml). LNCaP cells were treated with varying concentrations of exogenous SGP-2, while PC3 cells were treated with antisera to SGP-2 with and without exogenous SGP-2. Following a 24-hr treatment, cultures were assessed by counting of cell number and by the trypan blue exclusion assay. RESULTS: Western blot analysis of conditioned media revealed that PC3 secreted more SGP-2 than did LNCaP. The sensitivity to TNF in LNCaP cells was reduced by the addition of exogenous SGP-2. PC3 cells became sensitive to TNF when SGP-2 antibody was added to the culture. The effect of SGP-2 antibody on PC3 cells was reversed by the addition of exogenous SGP-2 to the culture. CONCLUSIONS: These results suggest that SGP-2 can act as an extracellular mediator of anti-TNF-induced cytotoxicity.
机译:背景:SGP-2是一种普遍存在的分泌糖蛋白,可防止细胞凋亡。这项研究是为了确定SGP-2在使用两种人前列腺癌LNCaP和PC3的肿瘤坏死因子-α(TNF)诱导的细胞毒性模型中的细胞外作用。选择这两个系是因为LNCaP细胞对TNF的细胞毒性作用高度敏感,而PC3细胞在24小时对TNF具有抗性。方法:在存在或不存在TNF(10 ng / ml)的情况下培养细胞。 LNCaP细胞用不同浓度的外源SGP-2处理,而PC3细胞用有或没有外源SGP-2的SGP-2抗血清处理。处理24小时后,通过计数细胞数和台盼蓝排除法评估培养物。结果:条件培养基的蛋白质印迹分析表明,PC3分泌的SGP-2比LNCaP分泌的更多。加入外源SGP-2可降低LNCaP细胞对TNF的敏感性。当向培养物中添加SGP-2抗体时,PC3细胞对TNF敏感。通过向培养物中添加外源SGP-2,可以逆转SGP-2抗体对PC3细胞的作用。结论:这些结果表明SGP-2可以作为抗TNF诱导的细胞毒性的细胞外介质。

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