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一种使用组织学完整的人肿瘤组织原位移植到裸鼠体内构建的新型人胰腺癌“类患者”治疗模型。

A novel "patient-like" treatment model of human pancreatic cancer constructed using orthotopic transplantation of histologically intact human tumor tissue in nude mice.

作者信息

Furukawa T, Kubota T, Watanabe M, Kitajima M, Hoffman R M

机构信息

Department of Surgery, School of Medicine, Keio University, Tokyo, Japan.

出版信息

Cancer Res. 1993 Jul 1;53(13):3070-2.

PMID:8319214
Abstract

Pancreatic cancer is a disease with essentially no effective treatment. To increase the potential for discovering effective treatment, we have developed a new treatment model whereby a human pancreatic cancer line, PANC-4, was orthotopically transplanted to the pancreas of nude mice as histologically intact tumor tissue. The tumor grew with subsequent invasive local tumor growth and liver and peritoneal metastases. The antitumor activity of 5-fluorouracil (5-FU) and mitomycin C (MMC) against PANC-4 was initially determined in the in vitro collagen-sponge-gel supported histoculture drug-response assay with the 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide end point. Inhibition rates were 5.6% for 5-FU and 39.4% for MMC indicating higher efficacy of MMC than 5-FU against PANC-4. When the antitumor activities of 5-FU and MMC against PANC-4 were determined in vivo using the nude mouse orthotopic transplant treatment model, slight local tumor growth inhibition with equivalent incidence of metastases to the liver and the peritoneum as the control were observed in the mice treated with 5-FU, while those treated with MMC had considerably reduced local tumor growth without liver and peritoneal metastases. Thus the histoculture drug-response assay in combination with the orthotopic transplant metastatic models provides for the first time a paradigm for evaluation of agents which may be effective against not only locally growing human pancreatic cancer but resulting metastases as well.

摘要

胰腺癌是一种基本上没有有效治疗方法的疾病。为了增加发现有效治疗方法的可能性,我们开发了一种新的治疗模型,即将人胰腺癌系PANC - 4作为组织学上完整的肿瘤组织原位移植到裸鼠的胰腺中。肿瘤生长并随后出现局部肿瘤浸润性生长以及肝和腹膜转移。首先在体外胶原海绵凝胶支持的组织培养药物反应试验中,以3 -(4,5 - 二甲基噻唑 - 2 - 基)- 2,5 - 二苯基四氮唑溴盐终点法测定5 - 氟尿嘧啶(5 - FU)和丝裂霉素C(MMC)对PANC - 4的抗肿瘤活性。5 - FU的抑制率为5.6%,MMC的抑制率为39.4%,表明MMC对PANC - 4的疗效高于5 - FU。当使用裸鼠原位移植治疗模型在体内测定5 - FU和MMC对PANC - (4)的抗肿瘤活性时,在用5 - FU治疗的小鼠中观察到局部肿瘤生长略有抑制,肝和腹膜转移的发生率与对照组相当,而用MMC治疗的小鼠局部肿瘤生长明显减少,且无肝和腹膜转移。因此,组织培养药物反应试验与原位移植转移模型相结合,首次提供了一种评估不仅可能对局部生长的人胰腺癌有效,而且对由此产生的转移也有效的药物的范例。

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