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Advanced Xenograft Model with Cotransplantation of Patient-Derived Organoids and Endothelial Colony-Forming Cells for Precision Medicine

机译:具有患者衍生的有机体和内皮菌落形成细胞的患者培养的先进的异种移植模型进行精密药物

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Preclinical evaluation models have been developed for precision medicine, with patient-derived xenograft models (PDXs) and patient-derived organoids (PDOs) attracting increasing attention. However, each of these models has application limitations. In this study, an advanced xenograft model was established and used for drug screening. PDO and endothelial colony-forming cells (ECFCs) were cotransplanted in NRGA mice (PDOXwE) to prepare the model, which could also be subcultured in Balb/c nude mice. Our DNA sequencing analysis and immunohistochemistry results indicated that PDOXwE maintained patient genetic information and tumor heterogeneity. Moreover, the model enhanced tumor growth more than the PDO-bearing xenograft model (PDOX). The PDO, PDOXwE, and clinical data were also compared in the liver metastasis of a colorectal cancer patient, demonstrating that the chemosensitivity of PDO and PDOXwE coincided with the clinical data. These results suggest that PDOXwE is an improvement of PDOX and is suitable as an evaluation model for precision medicine.
机译:已经开发了临床前评估模型用于精密药,具有患者衍生的异种移植模型(PDX)和患者衍生的有机体(PDOS)吸引了不断的关注。但是,这些模型中的每一个都具有应用限制。在这项研究中,建立了一种先进的异种移植模型并用于药物筛选。 PDO和内皮菌落形成细胞(ECFC)在NRGA小鼠(PDOXWE)中是COTASANTED以制备模型,其也可以在BALB / C裸鼠中转移。我们的DNA测序分析和免疫组织化学结果表明,PDoxWe维持患者遗传信息和肿瘤异质性。此外,模型增强了肿瘤生长多于PDO轴承的异种移植模型(PDOX)。在结肠直肠癌患者的肝转移中也比较了PDO,PDOXWE和临床数据,证明了PDO和PDOXWE的化学敏感性与临床数据一致。这些结果表明,PdoxWe是PDOX的改进,适合作为精密药物的评估模型。

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