首页> 外文期刊>The Prostate >Proliferation of prostate cancer cells and activity of neutral endopeptidase is regulated by bombesin and IL-1beta with IL-1beta acting as a modulator of cellular differentiation.
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Proliferation of prostate cancer cells and activity of neutral endopeptidase is regulated by bombesin and IL-1beta with IL-1beta acting as a modulator of cellular differentiation.

机译:胰岛素和IL-1β调节前列腺癌细胞的增殖和中性内肽酶的活性,IL-1β作为细胞分化的调节剂。

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BACKGROUND: Neutral endopeptidase (NEP) is a cell-surface bound enzyme that cleaves and inactivates neuropeptides such as bombesin and substance P and is involved in the transition from hormonally regulated androgen-dependent prostate cancer (PC) to androgen-independent PC. Neuropeptides are implicated in growth regulation of different cell types and function as transmitters between the neuroendocrine and the immune system. METHODS: NEP-expression, enzymatic activity of the membrane bound protein, cell proliferation, procalcitonin (PCT) production, and secretion as well as changes in cell morphology of prostatic cells were evaluated after treatment with the immunomodulatory cytokine interleukin-1beta (IL-1beta), neuropeptides (bombesin, substance P), and neuropeptide-conditioned media derived from a human neuroendocrine cell line. RESULTS: Incubation of LNCaP tumor cells with IL-1beta resulted in a diminished proliferative activity, induction of neurite-like outgrowth which was accompanied by the formation of tubular-type mitochondria typical for neuronaleuroendocrine cells, and an increased production and secretion of PCT. Conversely, proliferation of prostatic stromal cells was enhanced by the cytokine coming along with an increased number of Golgi-apparatuses and ER-cisternae. Bombesin had an antimitotic effect on LNCaP, but not on stromal cells. Substance P did not influence the growth of any of the cell types investigated, whereas neuropeptide-conditioned media exerted a slightly mitogenic effect on both cell types. The activity of LNCaP cell-surface bound NEP was enhanced by bombesin, but was diminished by substance P and neuropeptide-conditioned media. CONCLUSIONS: Proliferation and activity of neuropeptide degrading NEP is regulated differently by immunomodulatory substances in PC cells and cells derived from the prostatic stroma with IL-1beta being a potent modulator of cellular differentiation and a potential target for anticancer drug design in PC cells.
机译:背景:中性内肽酶(NEP)是一种细胞表面结合酶,可裂解和灭活神经肽(如蛙粉和P物质),并参与从激素调节的雄激素依赖性前列腺癌(PC)到非雄激素依赖性PC的转变。神经肽与不同细胞类型的生长调节有关,并作为神经内分泌和免疫系统之间的递质。方法:免疫调节细胞因子白介素-1β(IL-1beta)处理后,评估了NEP的表达,膜结合蛋白的酶活性,细胞增殖,降钙素原(PCT)的产生以及前列腺细胞的分泌以及细胞形态的变化。 ),神经肽(轰炸蛋白,P物质)和源自人神经内分泌细胞系的神经肽条件培养基。结果:将LNCaP肿瘤细胞与IL-1beta一起孵育会导致增殖活性降低,诱导神经突样生长,并伴随着神经元/神经内分泌细胞典型的管状线粒体的形成,并增加PCT的产生和分泌。相反,随着细胞因子的增加以及高尔基体和ER池的增加,前列腺基质细胞的增殖得以增强。 Bombesin对LNCaP具有抗有丝分裂作用,但对基质细胞无抗分裂作用。 P物质不影响所研究的任何细胞类型的生长,而神经肽条件培养基对这两种细胞类型均具有轻微的促有丝分裂作用。 Lombasin增强了LNCaP细胞表面结合的NEP的活性,但P物质和神经肽条件培养基却降低了其活性。结论:降解神经肽的NEP的增殖和活性受PC细胞和前列腺基质细胞的免疫调节物质的调节不同,IL-1β是细胞分化的有效调节剂,是PC细胞中抗癌药物设计的潜在靶标。

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