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免疫抑制猫体内大型动物人脑肿瘤异种移植模型的建立。

Development of a large-animal human brain tumor xenograft model in immunosuppressed cats.

作者信息

Krushelnycky B W, Farr-Jones M A, Mielke B, McKean J D, Weir B K, Petruk K C

机构信息

Department of Surgery, University of Alberta, Edmonton, Canada.

出版信息

Cancer Res. 1991 May 1;51(9):2430-7.

PMID:2015604
Abstract

A large-animal model was developed to facilitate the noninvasive investigation of the effect on the human glioma-derived D-54 MG (glioblastoma multiforme) continuous cell line of a variety of therapeutic regimens. Twenty random-bred male cats were inoculated intracerebrally with 1 x 10(7) D-54 MG tumor cells after being initiated on one of three preparatory regimens of cyclosporin A p.o. Reproducible success of D-54 MG xenotransplantation (100%, 6 of 6 cats) was achieved only after pretreatment with 120 mg cyclosporin A p.o. (24-30 mg/kg) daily for greater than or equal to 10 days prior to tumor implantation. High-performance liquid chromatography-derived whole blood cyclosporin A 12-h trough levels of greater than or equal to 640 ng/ml were seen in successful implants. Lesions ranging from 2 to 20 mm in diameter were seen in cats sacrificed 27-44 days after implantation with no growth seen in control animals. Histopathological examination revealed the tumors to be well-circumscribed anaplastic intracerebral tumors with some invasion into surrounding host parenchyma. Perivascular lymphocytic cuffing was observed, but intratumoral lymphocytic infiltration was minimal. Gadolinium-EDTA-enhanced nuclear magnetic resonance imaging provided accurate tumor localization in T1-weighted images (TE 26 ms; TR 600 ms). Biochemical tests of kidney, liver, and hematological function were within normal limits, although 10% (2 of 20) of the animals developed gingival hyperplasia, and 5% (1 of 20) developed intussusception. The reproducible growth of the D-54 MG human glioblastoma cell line in a large-animal model eliminates many of the limitations associated with the standard nude mouse/rat model, thereby providing a novel test bed for a variety of imaging modalities as well as for drug immunoconjugate localization and toxicity studies.

摘要

开发了一种大型动物模型,以促进对多种治疗方案对源自人胶质瘤的D-54 MG(多形性胶质母细胞瘤)连续细胞系影响的无创研究。20只随机繁殖的雄性猫在口服环孢素A的三种预处理方案之一开始后,脑内接种1×10(7)个D-54 MG肿瘤细胞。仅在肿瘤植入前每天口服120 mg环孢素A(24 - 30 mg/kg)≥10天进行预处理后,才实现了D-54 MG异种移植的可重复成功(100%,6只猫中的6只)。成功植入的动物中,高效液相色谱法测定的全血环孢素A 12小时谷浓度≥640 ng/ml。在植入后27 - 44天处死的猫中可见直径为2至20 mm的病变,对照动物未见生长。组织病理学检查显示肿瘤为边界清楚的间变性脑内肿瘤,有一些侵入周围宿主实质。观察到血管周围淋巴细胞套袖状浸润,但肿瘤内淋巴细胞浸润极少。钆喷替酸葡甲胺增强核磁共振成像在T1加权图像(TE 26 ms;TR 600 ms)中提供了准确的肿瘤定位。肾脏、肝脏生化检查和血液学功能均在正常范围内,尽管10%(20只中的2只)动物出现牙龈增生,5%(20只中的1只)出现肠套叠。D-54 MG人胶质母细胞瘤细胞系在大型动物模型中的可重复生长消除了与标准裸鼠/大鼠模型相关的许多局限性,从而为各种成像方式以及药物免疫缀合物定位和毒性研究提供了一个新的试验平台。

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