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在胶质母细胞瘤细胞系中,通过野生型p53基因治疗提高卡氮芥敏感性取决于给药方案。

Increase of BCNU sensitivity by wt-p53 gene therapy in glioblastoma lines depends on the administration schedule.

作者信息

Biroccio A, Bufalo D D, Ricca A, D'Angelo C, D'Orazi G, Sacchi A, Soddu S, Zupi G

机构信息

Experimental Chemotherapy Laboratory, Regina Elena Cancer Institute, Rome, Italy.

出版信息

Gene Ther. 1999 Jun;6(6):1064-72. doi: 10.1038/sj.gt.3300935.

Abstract

In this article, we investigated the effect induced by the reintroduction of wild-type p53 (wt-p53) protein on BCNU sensitivity in the ADF glioblastoma line. Using a wt-p53 recombinant adenovirus (Ad-p53), we demonstrated that exogenous wt-p53 expression was able to increase the sensitivity to BCNU in ADF cells. Interestingly, this effect was more evident when Ad-p53 infection was performed after BCNU treatment compared with the opposite sequence. To understand the biological basis of these different behaviors, we analyzed the cell cycle of the differently treated cells. We found that Ad-p53 infection induced a persistent accumulation of cells in the G0/G1 phase while, as expected, BCNU induced a block in the G2-M phase. Ad-p53-->BCNU sequence did not significantly modify the cell cycle profile in respect of Ad-p53 infected cells. In contrast, BCNU-->Ad-p53 sequence provoked G2-M arrest similar to that observed after treatment with BCNU alone, but prevented the later recovery of the cells through the cell cycle, by driving the cells to apoptotic death. These results demonstrate that the administration sequence is important to increase drug sensitivity. To generalize the phenomenon observed on ADF line, the antiproliferative effect of the two different schedules was analyzed on other glioblastoma lines (A172, CRS-A2, U373MG) with different BCNU sensitivity and p53 status. The data obtained confirm that the wt-p53 gene transfer enhances BCNU sensitivity in glioblastoma cells depending on the administration sequence.

摘要

在本文中,我们研究了野生型p53(wt-p53)蛋白的重新引入对ADF胶质母细胞瘤细胞系中卡莫司汀(BCNU)敏感性的影响。使用wt-p53重组腺病毒(Ad-p53),我们证明外源性wt-p53表达能够增加ADF细胞对BCNU的敏感性。有趣的是,与相反顺序相比,在BCNU处理后进行Ad-p53感染时,这种效应更明显。为了理解这些不同行为的生物学基础,我们分析了不同处理细胞的细胞周期。我们发现Ad-p53感染诱导细胞在G0/G1期持续积累,而正如预期的那样,BCNU诱导细胞在G2-M期阻滞。Ad-p53→BCNU顺序相对于Ad-p53感染的细胞并未显著改变细胞周期分布。相反,BCNU→Ad-p53顺序引发了与单独用BCNU处理后观察到的类似的G2-M期阻滞,但通过促使细胞凋亡死亡,阻止了细胞随后通过细胞周期的恢复。这些结果表明给药顺序对于增加药物敏感性很重要。为了推广在ADF细胞系上观察到的现象,我们分析了两种不同给药方案对其他具有不同BCNU敏感性和p53状态的胶质母细胞瘤细胞系(A172、CRS-A2、U373MG)的抗增殖作用。获得的数据证实,wt-p53基因转移根据给药顺序增强了胶质母细胞瘤细胞对BCNU的敏感性。

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