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Application of Prostate Cancer Models for Preclinical Study: Advantages and Limitations of Cell Lines, Patient-Derived Xenografts, and Three-Dimensional Culture of Patient-Derived Cells

机译:前列腺癌模型在临床前研究中的应用:细胞系,患者衍生异种移植物和患者衍生细胞三维培养的优缺点

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摘要

Various preclinical models have been developed to clarify the pathophysiology of prostate cancer (PCa). Traditional PCa cell lines from clinical metastatic lesions, as exemplified by DU-145, PC-3, and LNCaP cells, are useful tools to define mechanisms underlying tumorigenesis and drug resistance. Cell line-based experiments, however, have limitations for preclinical studies because those cells are basically adapted to 2-dimensional monolayer culture conditions, in which the majority of primary PCa cells cannot survive. Recent tissue engineering enables generation of PCa patient-derived xenografts (PDXs) from both primary and metastatic lesions. Compared with fresh PCa tissue transplantation in athymic mice, co-injection of PCa tissues with extracellular matrix in highly immunodeficient mice has remarkably improved the success rate of PDX generation. PDX models have advantages to appropriately recapitulate the molecular diversity, cellular heterogeneity, and histology of original patient tumors. In contrast to PDX models, patient-derived organoid and spheroid PCa models in 3-dimensional culture are more feasible tools for in vitro studies for retaining the characteristics of patient tumors. In this article, we review PCa preclinical model cell lines and their sublines, PDXs, and patient-derived organoid and spheroid models. These PCa models will be applied to the development of new strategies for cancer precision medicine.
机译:已经开发出各种临床前模型来阐明前列腺癌(PCA)的病理生理学。由DU-145,PC-3和LNCAP细胞的例子中示例的来自临床转移性病变的传统PCA细胞系是有用的工具,以确定肿瘤发生和耐药性的机制。然而,基于细胞基的实验对临床前研究的局限性是因为这些细胞基本上适应二维单层培养条件,其中大多数初级PCA细胞不能存活。最近的组织工程能够从初级和转移性病变中产生PCA患者衍生的异种移植物(PDX)。与胸肉小鼠的新鲜PCA组织移植相比,在高度免疫缺陷小鼠中,具有细胞外基质的PCA组织的共注入,显着提高了PDX生成的成功率。 PDX模型具有适当概念的优点,可适当地重新延长原始患者肿瘤的分子多重性,细胞异质性和组织学。与PDX模型相反,三维培养的患者衍生的有机体和球形PCA模型是用于保留患者肿瘤特征的体外研究的更可行的工具。在本文中,我们审查了PCA临床前模型细胞系及其寄生,PDX和患者衍生的有机体和球状模型。这些PCA模型将适用于癌症精密药物的新策略。

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