[Inhibitory effect of cationic liposome-mediated antisense c-myb oligonucleotide on the growth of glioma].

Dongdong Zhao, Chao You, Guangfu Huang, Xiaoling Liao, Haibing Tan
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Abstract

Objective: To aim at demonstrating whether cationic liposome-mediated antisense c-myb oligonucleotide(LipoAON) can inhibit the growth of C6 glioma by intravenous injection.

Methods: Intracerebral C6 glioma cells were implanted into the left caudal nucleus of forty-eight male Wistar rats. There were four groups: LipoAON(n = 12), antisense c-myb oligonucleotide (AON; n = 12), cationic liposome (Lipo; n = 12), and normal saline (NS; n = 12). Six days after tumor implantation, the above-mentioned drugs were injected into the right femoral veins of the rats respectively. Two days later, the same drugs were injected into the left femoral veins. The appetite, motor and weight of every animal were closely observed during the whole experiment. Six rats of each group were respectively killed 4 days and 10 days after the end of administration. The weight change, pathologic examination and immunohistochemical analysis of c-myb expression of the tumor were completed.

Results: In LipoAON group, the growth of the tumors was significantly inhibited in a short time after treatment and c-myb expression was down-regulated. But in the AON group and Lipo group, the growth of the tumors was not inhibited and c-myb expression was not down-regulated, compared with that in NS group. The inhibitory effect of LipoAON on the tumors rapidly declined with time and c-myb expression was again up-regulated.

Conclusion: 1. Cationic liposome (LipofectAMINE) as transfection vehicle makes c-myb easily penetrate BBTB and enter the tumor. The technique is simple, safe, highly effective for the transfection of c-mybAON; 2. LipoAON has marked inhibitory effect on the growth of C6 glioma. The AON technical method for inhibiting the expression of c-myb oncogene has a research perspective in the treatment of glioma; 3. The inhibitory effect of LipoAON on the growth of glioma declines with time. The question about how to make c-myb AON have highly effective, sustained and stable expression in the tumor still requires further research.

阳离子脂质体介导的反义c-myb寡核苷酸对胶质瘤生长的抑制作用。
目的:探讨静脉注射阳离子脂质体介导的反义c-myb寡核苷酸(LipoAON)是否能抑制C6胶质瘤的生长。方法:将脑内C6胶质瘤细胞植入48只雄性Wistar大鼠的左尾核。分为4组:LipoAON(n = 12)、反义c-myb寡核苷酸(AON;n = 12),阳离子脂质体(Lipo;n = 12),生理盐水(NS;N = 12)。肿瘤植入6天后,将上述药物分别注入大鼠右股静脉。两天后,同样的药物被注射到左股静脉。在整个实验过程中密切观察各组动物的食欲、运动和体重。各组大鼠分别于给药结束后第4天和第10天处死6只。完成肿瘤重量变化、病理检查及c-myb表达免疫组化分析。结果:LipoAON组治疗后短时间内肿瘤生长明显受到抑制,c-myb表达下调。但与NS组相比,AON组和Lipo组肿瘤生长未受抑制,c-myb表达未下调。随着时间的推移,LipoAON对肿瘤的抑制作用迅速下降,c-myb的表达再次上调。结论:1。阳离子脂质体(LipofectAMINE)作为转染载体,使c-myb容易穿透BBTB进入肿瘤。该技术简单、安全、高效,可用于c-mybAON的转染;2. LipoAON对C6胶质瘤的生长有明显的抑制作用。抑制c-myb癌基因表达的AON技术方法在胶质瘤治疗中具有研究前景;3.LipoAON对胶质瘤生长的抑制作用随时间的延长而减弱。如何使c-myb AON在肿瘤中高效、持续、稳定的表达,仍需进一步研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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