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首页> 外文期刊>Oncology letters >Investigation into metastatic processes and the therapeutic effects of gemcitabine on human pancreatic cancer using an orthotopic SUIT-2 pancreatic cancer mouse model
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Investigation into metastatic processes and the therapeutic effects of gemcitabine on human pancreatic cancer using an orthotopic SUIT-2 pancreatic cancer mouse model

机译:使用原位诉讼 - 2胰腺癌小鼠模型对吉西他滨对人胰腺癌的转移过程和治疗作用的研究

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Prognosis of pancreatic cancer is poor, thus the development of novel therapeutic drugs is necessary. During preclinical studies, appropriate models are essential for evaluating drug efficacy. The present study sought to determine the ideal pancreatic cancer mouse model for reliable preclinical testing. Such a model could accurately reflect human pancreatic cancer phenotypes and predict future clinical trial results. Systemic pathology analysis was performed in an orthotopic transplantation model to prepare model mice for use in preclinical studies, mimicking the progress of human pancreatic cancer. The location and the timing of inoculated cancer cell metastases, pathogenesis and cause of fatality were analyzed. Furthermore, the efficacy of gemcitabine, a key pancreatic cancer drug, was evaluated in this model where liver metastasis and peritoneal dissemination occur. Results indicated that the SUIT-2 orthotopic pancreatic cancer model was similar to the phenotypic sequential progression of human pancreatic cancer, with extra-pancreatic invasion, intra-peritoneal dissemination and other hematogenous organ metastases. Notably, survival was prolonged by administering gemcitabine to mice with metastasized pancreatic cancer. Furthermore, the detailed effects of gemcitabine on the primary tumor and metastatic tumor lesions were pathologically evaluated in mice. The present study indicated the model accurately depicted pancreatic cancer development and metastasis. Furthermore, the detailed effects of pancreatic cancer drugs on the primary tumor and on metastatic tumor lesions. We present this model as a potential new standard for new drug development in pancreatic cancer.
机译:胰腺癌的预后差,因此新的治疗药物的发展是必要的。在临床前研究期间,适当的模型对于评估药物功效至关重要。本研究试图确定可靠的临床前测试的理想胰腺癌小鼠模型。这种模型可以准确反映人类胰腺癌表型并预测未来的临床试验结果。在原位移植模型中进行全身病理分析,以制备用于临床前研究的模型小鼠,以模仿人类胰腺癌的进展。分析了接种癌细胞转移,发病机制和死亡原因的位置和定时。此外,在该模型中评估了吉西他滨,吉西他滨的疗效,该模型在发生肝转移和腹膜传播的情况下评估。结果表明,西装 - 2原位胰腺癌模型类似于人类胰腺癌的表型连续进展,具有胰腺癌的腹膜内侵袭,腹膜内传播和其他血液外血管转移。值得注意的是,通过将吉西他滨与转移的胰腺癌​​施用小鼠延长存活。此外,吉西他滨对原发性肿瘤和转移性肿瘤病变的详细效果在小鼠中进行病理评估。本研究表明,模型准确地描绘了胰腺癌发育和转移。此外,胰腺癌药物对原发性肿瘤和转移性肿瘤病变的详细效果。我们将该模型作为胰腺癌新药开发的潜在新标准。

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