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将表达野生型p53的载体转染到两个人类胶质瘤细胞系的细胞中可增强辐射毒性。

Transfection of a vector expressing wild-type p53 into cells of two human glioma cell lines enhances radiation toxicity.

作者信息

Geng L, Walter S, Melian E, Vaughan A T

机构信息

Loyola-Hines Department of Radiotherapy, Cancer Center #338, Maywood, Illinois 60153, USA.

出版信息

Radiat Res. 1998 Jul;150(1):31-7.

PMID:9650599
Abstract

Replication-deficient adenovirus (Adv5)-based vectors containing either wild-type p53 or the beta-gal marker gene were introduced into cells of the T98G (p53 mutant) and U87MG (p53 wild-type) human glioma cell lines. The wild-type p53 gene was successfully expressed in each cell line as shown by flow cytometry and Western blotting. The presence of the p53-expressing vector was toxic in both cell lines compared to control cells or to those containing the beta-gal vector. At levels of Adv5p53 vector that produced detectable toxicity, the effect of irradiation was enhanced, producing a twofold increase in cell killing. In the T98G cells, the presence of the p53 vector resulted in an increase in the number of cells undergoing apoptosis after irradiation, whereas a smaller and only additive response was observed in the U87MG cells. Conversely, an increase in micronucleus formation, indicating corrupt mitotic activity, was observed in irradiated Adv5p53-positive U87MG cells but not in T98G cells. These data suggest that p53-expressing vectors effectively enhance radiation lethality in these human glioma cell lines, but that the mechanism of action cannot be simply related to activation of the p53-dependent pathway to apoptosis.

摘要

将含有野生型p53或β-半乳糖苷酶标记基因的复制缺陷型腺病毒(Adv5)载体导入T98G(p53突变型)和U87MG(p53野生型)人胶质瘤细胞系的细胞中。如流式细胞术和蛋白质免疫印迹法所示,野生型p53基因在每个细胞系中均成功表达。与对照细胞或含有β-半乳糖苷酶载体的细胞相比,表达p53的载体在两种细胞系中均具有毒性。在产生可检测到毒性的Adv5p53载体水平下,辐射效应增强,细胞杀伤增加了两倍。在T98G细胞中,p53载体的存在导致辐射后发生凋亡的细胞数量增加,而在U87MG细胞中观察到的反应较小且只是相加作用。相反,在照射后的Adv5p53阳性U87MG细胞中观察到微核形成增加,表明有丝分裂活性受损,但在T98G细胞中未观察到。这些数据表明,表达p53的载体可有效增强这些人胶质瘤细胞系中的辐射致死性,但作用机制不能简单地与p53依赖性凋亡途径的激活相关。

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