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一种用于肢体黑色素瘤的肢体隔离灌注的新型小鼠模型。

A novel mouse model of isolated limb perfusion for extremity melanoma.

机构信息

Department of Immunology, Roswell Park Cancer Institute, Buffalo, New York 14263, USA.

出版信息

J Surg Res. 2012 Nov;178(1):294-8. doi: 10.1016/j.jss.2012.03.032. Epub 2012 Apr 5.

Abstract

BACKGROUND

Isolated limb perfusion (ILP) for extremity melanoma has been used clinically for over half a century. Mouse modeling of ILP may offer significant experimental advantages compared with existing models. We propose a novel mouse model and report our initial experience.

METHODS

We injected female C57BL/6 mice (22-25 g) with 1 × 10(6) B16 melanoma cells subcutaneously in the distal right thigh. After 7 d of tumor establishment, we cannulated the superficial femoral artery (inflow) and vein (outflow) of anesthetized mice and placed a proximal tourniquet. Non-oxygenated perfusate included low-dose or high-dose melphalan and saline (control). We analyzed endpoints of cannulation time, procedural complications, morbidity, toxicity, and tumor response.

RESULTS

We performed 11 superficial femoral vessel cannulations. Median cannulation time was 19 min (range, 15-32 min). Intact perfusion models were obtained in 10 of 11 cases (91%); one case failed owing to superficial femoral vein dissection. Morbidity rate was 20% (one wound dehiscence and one hematoma). Both high- and low-dose melphalan perfusion groups (4 mice/group) trended to growth delay and regression compared with saline-perfused groups. Toxicity was greater in the high-dose melphalan-treated mice.

CONCLUSIONS

We have established the first reproducible mouse model of ILP for melanoma. Future experiments will take advantage of the large number of established mouse knockout models and reagents to dissect the precise mechanisms of tumor control after ILP, and examine to novel agents.

摘要

背景

肢体黑色素瘤的孤立肢体灌注(ILP)已经在临床上应用了半个多世纪。与现有的模型相比,ILP 的小鼠模型可能具有重要的实验优势。我们提出了一种新的小鼠模型,并报告了我们的初步经验。

方法

我们将 1×10(6)B16 黑色素瘤细胞皮下注射到雌性 C57BL/6 小鼠(22-25g)的右大腿远端。在肿瘤建立 7 天后,我们对麻醉小鼠的股浅动脉(入流)和静脉(出流)进行了套管,并放置了一个近端止血带。非含氧灌注液包括低剂量或高剂量美法仑和生理盐水(对照)。我们分析了套管时间、手术并发症、发病率、毒性和肿瘤反应的终点。

结果

我们进行了 11 次股浅血管套管。中位套管时间为 19 分钟(范围 15-32 分钟)。在 11 例中有 10 例(91%)获得了完整的灌注模型;一例因股浅静脉剥离而失败。发病率为 20%(一例伤口裂开,一例血肿)。与生理盐水灌注组相比,高剂量和低剂量美法仑灌注组(每组 4 只)的肿瘤生长均有延迟和消退的趋势。高剂量美法仑治疗组的毒性更大。

结论

我们已经建立了第一个用于黑色素瘤的可重复的 ILP 小鼠模型。未来的实验将利用大量已建立的小鼠基因敲除模型和试剂来剖析 ILP 后肿瘤控制的确切机制,并研究新的药物。

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