实验神经肿瘤学中的大鼠脑肿瘤模型:C6、9L、T9、RG2、F98、BT4C、RT - 2和CNS - 1胶质瘤。
Rat brain tumor models in experimental neuro-oncology: the C6, 9L, T9, RG2, F98, BT4C, RT-2 and CNS-1 gliomas.
作者信息
Barth Rolf F, Kaur Balveen
机构信息
Department of Pathology, The Ohio State University, 165 Hamilton Hall, Columbus, OH 43210, USA.
出版信息
J Neurooncol. 2009 Sep;94(3):299-312. doi: 10.1007/s11060-009-9875-7. Epub 2009 Apr 21.
In this review we will describe eight commonly used rat brain tumor models and their application for the development of novel therapeutic and diagnostic modalities. The C6, 9L and T9 gliomas were induced by repeated injections of methylnitrosourea (MNU) to adult rats. The C6 glioma has been used extensively for a variety of studies, but since it arose in an outbred Wistar rat, it is not syngeneic to any inbred strain, and its potential to evoke an alloimmune response is a serious limitation. The 9L gliosarcoma has been used widely and has provided important information relating to brain tumor biology and therapy. The T9 glioma, although not generally recognized, was and probably still is the same as the 9L. Both of these tumors arose in Fischer rats and can be immunogenic in syngeneic hosts, a fact that must be taken into consideration when used in therapy studies, especially if survival is the endpoint. The RG2 and F98 gliomas were both chemically induced by administering ethylnitrosourea (ENU) to pregnant rats, the progeny of which developed brain tumors that subsequently were propagated in vitro and cloned. They are either weakly or non-immunogenic and have an invasive pattern of growth and uniform lethality, which make them particularly attractive models to test new therapeutic modalities. The CNS-1 glioma was induced by administering MNU to a Lewis rat. It has an infiltrative pattern of growth and is weakly immunogenic, which should make it useful in experimental neuro-oncology. Finally, the BT4C glioma was induced by administering ENU to a BD IX rat, following which brain cells were propagated in vitro until a tumorigenic clone was isolated. This tumor has been used for a variety of studies to evaluate new therapeutic modalities. The Avian Sarcoma Virus (ASV) induced tumors, and a continuous cell line derived from one of them designated RT-2, have been useful for studies in which de novo tumor induction is an important requirement. These tumors also are immunogenic and this limits their usefulness for therapy studies. It is essential to recognize the limitations of each of the models that have been described, and depending upon the nature of the study to be conducted, it is important that the appropriate model be selected.
在本综述中,我们将描述八种常用的大鼠脑肿瘤模型及其在新型治疗和诊断方法开发中的应用。C6、9L和T9胶质瘤是通过向成年大鼠重复注射甲基亚硝基脲(MNU)诱导产生的。C6胶质瘤已被广泛用于各种研究,但由于它起源于远交系Wistar大鼠,与任何近交系都不是同基因的,其引发同种免疫反应的可能性是一个严重的限制。9L胶质肉瘤已被广泛使用,并提供了与脑肿瘤生物学和治疗相关的重要信息。T9胶质瘤虽然一般未被认可,但过去是且可能现在仍然与9L相同。这两种肿瘤都起源于Fischer大鼠,在同基因宿主中可能具有免疫原性,在用于治疗研究时,尤其是以生存为终点时,这一事实必须予以考虑。RG2和F98胶质瘤都是通过向怀孕大鼠施用乙基亚硝基脲(ENU)化学诱导产生的,其后代发生脑肿瘤,随后在体外进行传代培养并克隆。它们要么免疫原性弱,要么无免疫原性,具有侵袭性生长模式和一致的致死性,这使得它们成为测试新治疗方法的特别有吸引力的模型。CNS - 1胶质瘤是通过向一只Lewis大鼠施用MNU诱导产生的。它具有浸润性生长模式,免疫原性弱,这使其在实验神经肿瘤学中应该有用。最后,BT4C胶质瘤是通过向一只BD IX大鼠施用ENU诱导产生的,随后将脑细胞在体外传代培养,直到分离出一个致瘤克隆。这种肿瘤已被用于各种研究以评估新的治疗方法。禽肉瘤病毒(ASV)诱导的肿瘤以及从中衍生出的一个连续细胞系,命名为RT - 2,已用于那些从头诱导肿瘤是重要要求的研究。这些肿瘤也具有免疫原性,这限制了它们在治疗研究中的用途。认识到已描述的每种模型的局限性至关重要,并且根据要进行的研究的性质,选择合适的模型很重要。
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