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一种用于研究大鼠和人类膀胱癌侵袭与转移的新型体内模型。

A new in vivo model for studying invasion and metastasis of rat and human bladder carcinomas.

作者信息

Kameyama S, Kawamata H, Kawai K, Oyasu R

机构信息

Department of Pathology, Northwestern University Medical School, Chicago, IL 60611.

出版信息

Carcinogenesis. 1993 Aug;14(8):1531-5. doi: 10.1093/carcin/14.8.1531.

DOI:10.1093/carcin/14.8.1531
PMID:8353837
Abstract

The biological potential of tumor cells is best evaluated at the organ site orthotopic to the tumor cells. Recent studies have documented site-specific differences in the potential of tumor cell growth. However, orthotopic implantation of bladder cancer cells into bladders of nude mice only resulted in a low tumor yield. We have developed a new model that consists of a rat bladder transplanted into the retroperitoneal space and connected to a reservoir s.c. placed in a nude mouse. Rat malignant bladder cancer cells (MYU3L and LMC19) transfected with the human growth hormone (hGH) gene as a biomarker were introduced into the transplanted bladder by percutaneous puncture of the attached reservoir. Successful uptake was indicated by a progressive rise in the hGH level in the bladder aspirate. When examined at 6-16 weeks post transplantation, all mice that had received MYU3L (n = 6) or LMC19 (n = 6) cells were found to have invasive carcinomas. MYU3L was highly invasive, forming multiple peritoneal implants, but was not metastatic. LMC19 was deeply invasive and metastasized to the retroperitoneal and subclavian lymph nodes and the lungs (4/6). Of two human bladder cancer cell lines (RT4 and T24) tested, RT4 formed multiple minute papillary tumors in five of six bladders, two of which were minimally invasive to the muscle layer. T24 cells formed only one to two small tumors in three of six bladders, and these were confined to the lamina propria. This system appears promising for studies of the mechanism of tumor invasion and metastasis and for evaluation of antineoplastic agents.

摘要

肿瘤细胞的生物学潜能在与肿瘤细胞原位的器官部位评估最佳。最近的研究记录了肿瘤细胞生长潜能的位点特异性差异。然而,将膀胱癌细胞原位植入裸鼠膀胱仅产生低肿瘤发生率。我们开发了一种新模型,该模型由移植到腹膜后间隙并与皮下放置在裸鼠体内的储液器相连的大鼠膀胱组成。将转染有人生长激素(hGH)基因作为生物标志物的大鼠恶性膀胱癌细胞(MYU3L和LMC19)通过经皮穿刺附着的储液器引入移植的膀胱。膀胱吸出物中hGH水平的逐渐升高表明摄取成功。在移植后6 - 16周检查时,发现所有接受MYU3L(n = 6)或LMC19(n = 6)细胞的小鼠都有浸润性癌。MYU3L具有高度侵袭性,形成多个腹膜种植,但不转移。LMC19具有深度侵袭性,转移至腹膜后和锁骨下淋巴结及肺(4/6)。在所测试的两个人膀胱癌细胞系(RT4和T24)中,RT4在六个膀胱中的五个中形成多个微小乳头状肿瘤,其中两个对肌层有最小程度的侵袭。T24细胞在六个膀胱中的三个中仅形成一到两个小肿瘤,且这些肿瘤局限于固有层。该系统对于研究肿瘤侵袭和转移机制以及评估抗肿瘤药物似乎很有前景。

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