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胰腺癌原位切除小鼠模型

An Orthotopic Resectional Mouse Model of Pancreatic Cancer.

作者信息

Pang Tony C Y, Xu Zhihong, Mekapogu Alpha Raj, Pothula Srinivasa, Becker Therese M, Goldstein David, Pirola Romano C, Wilson Jeremy S, Apte Minoti V

机构信息

Pancreatic Research Group, South Western Sydney Clinical School, University of New South Wales; Ingham Institute for Applied Medical Research; Surgical Innovations Unit, Westmead Hospital; Westmead Clinical School, University of Sydney;

Pancreatic Research Group, South Western Sydney Clinical School, University of New South Wales; Ingham Institute for Applied Medical Research.

出版信息

J Vis Exp. 2020 Sep 24(163). doi: 10.3791/61726.

Abstract

There is a lack of satisfactory animal models to study adjuvant and/or neoadjuvant therapy in patients being considered for surgery of pancreatic cancer (PC). To address this deficiency, we describe a mouse model involving orthotopic implantation of PC followed by distal pancreatectomy and splenectomy. The model has been demonstrated to be safe and suitably flexible for the study of various therapeutic approaches in adjuvant and neo adjuvant settings. In this model, a pancreatic tumor is first generated by implanting a mixture of human pancreatic cancer cells (luciferase-tagged AsPC-1) and human cancer associated pancreatic stellate cells into the distal pancreas of Balb/c athymic nude mice. After three weeks, the cancer is resected by re-laparotomy, distal pancreatectomy and splenectomy. In this model, bioluminescence imaging can be used to follow the progress of cancer development and effects of resection/treatments. Following resection, adjuvant therapy can be given. Alternatively, neoadjuvant treatment can be given prior to resection. Representative data from 45 mice are presented. All mice underwent successful distal pancreatectomy/splenectomy with no issues of hemostasis. A macroscopic proximal pancreatic margin greater than 5 mm was achieved in 43 (96%) mice. The technical success rate of pancreatic resection was 100%, with 0% early mortality and morbidity. None of the animals died during the week after resection. In summary, we describe a robust and reproducible technique for a surgical resection model of pancreatic cancer in mice which mimics the clinical scenario. The model may be useful for the testing of both adjuvant and neoadjuvant treatments.

摘要

目前缺乏令人满意的动物模型来研究拟行胰腺癌(PC)手术患者的辅助和/或新辅助治疗。为了弥补这一不足,我们描述了一种小鼠模型,该模型包括将PC原位植入,随后进行远端胰腺切除术和脾切除术。已证明该模型对于辅助和新辅助治疗中各种治疗方法的研究是安全且具有适当灵活性的。在该模型中,首先通过将人胰腺癌细胞(荧光素酶标记的AsPC-1)和人癌相关胰腺星状细胞的混合物植入Balb/c无胸腺裸鼠的远端胰腺来生成胰腺肿瘤。三周后,通过再次剖腹手术、远端胰腺切除术和脾切除术切除肿瘤。在该模型中,生物发光成像可用于追踪癌症发展进程以及切除/治疗的效果。切除后可给予辅助治疗。或者,可在切除前给予新辅助治疗。展示了来自45只小鼠的代表性数据。所有小鼠均成功进行了远端胰腺切除术/脾切除术,无止血问题。43只(96%)小鼠的胰腺近端宏观切缘大于5mm。胰腺切除的技术成功率为100%,早期死亡率和发病率为0%。术后一周内无动物死亡。总之,我们描述了一种用于小鼠胰腺癌手术切除模型的强大且可重复的技术,该技术模拟了临床情况。该模型可能有助于辅助治疗和新辅助治疗的测试。

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