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首页> 外文期刊>Toxicology in vitro: an international journal published in association with BIBRA >A human-derived prostate co-culture microtissue model using epithelial (RWPE-1) and stromal (WPMY-1) cell lines
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A human-derived prostate co-culture microtissue model using epithelial (RWPE-1) and stromal (WPMY-1) cell lines

机译:使用上皮细胞(RWPE-1)和基质(WPMY-1)细胞系的人源前列腺共培养微型仪模型

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摘要

The development and normal function of prostate tissue depends on signalling interactions between stromal and epithelial compartments. Development of a prostate microtissue composed of these two components can help identify substance exposures that could cause adverse effects in humans as part of a non-animal risk assessment. In this study, prostate microtissues composed of human derived stromal (WPMY-1) and epithelial (RWPE-1) cell lines grown in scaffold-free hydrogels were developed and characterized using immunohistochemistry, light microscopy, and qRT-PCR. Within 5 days after seeding, the microtissues self-organized into spheroids consisting of a core of stromal WPMY-1 cells surrounded by epithelial RWPE-1 cells. The RWPE-1 layer is reflective of intermediate prostatic epithelium, expressing both characteristics of the luminal (high expression of PSA) and basal (high expression of cytokeratins 5/6 and 14) epithelial cells. The response of the microtissues to an androgen (dihydrotestosterone, DHT) and an anti-androgen (flutamide) was also investigated. Treatment with DHT, flutamide or a mixture of DHT and flutamide indicated that the morphology and self-organization of the microtissues is androgen dependent. qRT-PCR data showed that a saturating concentration of DHT increased the expression of genes coding for the estrogen receptors (ESR1 and ESR2) and decreased the expression of CYP1B1 without affecting the expression of the androgen receptor. With further development and optimization RWPE-1/WPMY-1 microtissues can play an important role in non-animal risk assessments.
机译:前列腺组织的发展和正常功能取决于基质和上皮隔间之间的信号相互作用。由这两种组分组成的前列腺微生物的发展可以帮助鉴定可能导致人类不利影响的物质暴露,作为非动物风险评估的一部分。在本研究中,开发了由人衍生的基质(WPMY-1)和上皮(RWPE-1)和上皮(RWPE-1)细胞系组成的前列腺微调,并使用免疫组织化学,光学显微镜和QRT-PCR表征。在播种后5天内,将微小发出的微观组织成球状体,由由上皮RWPE-1细胞包围的基质WPMY-1细胞的核心组成。 RWPE-1层反射中间前列腺上皮,表达腔(PSA高表达)的特征和基础(细胞角蛋白5/6和14的高表达)上皮细胞。还研究了微小发酵给雄激素(Dihydrotestorone,DHT)和抗雄激素(氟胺)的响应。用DHT,氟胺或DHT和氟胺的混合物治疗表明,微生物诱导的形态和自组织是雄激素依赖性的。 QRT-PCR数据显示DHT的饱和浓度增加了编码雌激素受体(ESR1和ESR2)的基因的表达,并降低CYP1B1的表达而不影响雄激素受体的表达。随着进一步的开发和优化RWPE-1 / WPMY-1微调可以在非动物风险评估中发挥重要作用。

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