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A patient-derived orthotopic xenograft model enabling human high-grade urothelial cell carcinoma of the bladder tumor implantation growth angiogenesis and metastasis

机译:一种源自患者的原位异种移植模型可实现人类膀胱癌的高级尿路上皮细胞移植生长血管生成和转移

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摘要

High-grade urothelial cell carcinoma of the bladder has a poor prognosis when lymph nodes are involved. Despite curative therapy for clinically-localized disease, over half of the muscle-invasive urothelial cell carcinoma patients will develop metastases and die within 5 years. There are currently no described xenograft models that consistently mimic urothelial cell carcinoma metastasis. To develop a patient-derived orthotopic xenograft model to mimic clinical urothelial cell carcinoma progression to metastatic disease, the urothelial cell carcinoma cell line UM-UC-3 and two urothelial cell carcinoma patient specimens were doubly tagged with Luciferase/RFP and were intra-vesically (IB) instilled into NOD/SCID mice with or without lymph node stromal cells (HK cells). Mice were monitored weekly with bioluminescence imaging to assess tumor growth and metastasis. Primary tumors and organs were harvested for bioluminescence imaging, weight, and formalin-fixed for hematoxylin and eosin and immunohistochemistry staining. In this patient-derived orthotopic xenograft model, xenograft tumors showed better implantation rates than currently reported using other models. Xenograft tumors histologically resembled pre-implanted primary specimens from patients, presenting muscle-invasive growth patterns. In the presence of HK cells, tumor formation, tumor angiogenesis, and distant organ metastasis were significantly enhanced in both UM-UC-3 cells and patient-derived specimens. Thus, we established a unique, reproducible patient-derived orthotopic xenograft model using human high-grade urothelial cell carcinoma cells and lymph node stromal cells. It allows for investigating the mechanism involved in tumor formation and metastasis, and therefore it is useful for future testing the optimal sequence of conventional drugs or the efficacy of novel therapeutic drugs.
机译:当涉及淋巴结转移时,膀胱高级尿路上皮细胞癌预后较差。尽管对局部疾病进行了治愈性治疗,但仍有一半以上的肌肉浸润性尿路上皮细胞癌患者会发生转移并在5年内死亡。目前还没有描述能够持续模拟尿路上皮细胞癌转移的异种移植模型。为了建立源自患者的原位异种移植模型以模拟临床尿路上皮细胞癌发展为转移性疾病,将尿路上皮细胞癌细胞系UM-UC-3和两个尿路上皮细胞癌患者标本用荧光素酶/ RFP双重标记,并在膀胱内进行(IB)注入有或没有淋巴结基质细胞(HK细胞)的NOD / SCID小鼠中。每周用生物发光成像监测小鼠,以评估肿瘤的生长和转移。收集原发性肿瘤和器官进行生物发光成像,称重,并用福尔马林固定进行苏木精和曙红染色以及免疫组织化学染色。在这种源自患者的原位异种移植模型中,异种移植肿瘤的植入率比目前使用其他模型报道的要好。异种移植肿瘤在组织学上类似于患者植入前的原始标本,表现出肌肉侵袭性生长模式。在存在HK细胞的情况下,UM-UC-3细胞和患者标本均显着增强了肿瘤形成,肿瘤血管生成和远处器官转移。因此,我们使用人类高级尿路上皮细胞癌细胞和淋巴结基质细胞建立了一个独特的,可复制的患者源性原位异种移植模型。它允许研究与肿瘤形成和转移有关的机制,因此对于将来测试常规药物的最佳顺序或新型治疗药物的功效很有用。

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