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半胱天冬酰胺氮芥联合O6-苄基-N2-乙酰鸟苷对黑色素瘤细胞的毒性作用

Melanoma-cell toxicity of cystemustine combined with O6-benzyl-N2-acetylguanosine.

作者信息

Buchdahl C, Rolhion C, Glasser A L, Debiton E, Mounetou E, Madelmont J C, Laval F

机构信息

INSERM U484 (ext U71), Clermont-Ferrand, France.

出版信息

Melanoma Res. 1998 Apr;8(2):123-30. doi: 10.1097/00008390-199804000-00004.

Abstract

Cystemustine (N'-(2-chloroethyl)-N-(2-(methylsulphonyl)ethyl)-N'-nitrosourea) is a new chloroethylnitrosourea (CENU) being used in phase II clinical trials of disseminated melanoma. Clinical results show that tumour regression has only been observed in 25% of melanomas treated by CENUs. Tumour resistance to CENU is known to be mainly due to a DNA repair protein, O6-methylguanine-DNA methyltransferase (MGMT). The poor remission rate of melanoma with CENUs is attributed to the fact that metastases contain high MGMT levels. Previously, we have shown that O6-benzyl-N2-acetylguanosine (BNAG), an MGMT inhibitor, can be combined with cystemustine by intravenous administration, and increases the antitumour effect of cystemustine in resistant human melanoma. In the work presented here, we investigated the in vitro pharmacological effect of this combination on the DNA of human melanoma cells (M3Dau cells). A quantitative polymerase chain reaction (QPCR) assay was used to measure DNA damage in a fragment (2.7 kb) of the hprt gene. The results show that treatment with BNAG enhances the number of lesions in the DNA of cystemustine-treated resistant malignant melanocytes, which may account for the high tumour-cell toxicity of the combination of cystemustine and BNAG.

摘要

西司莫司汀(N'-(2-氯乙基)-N-(2-(甲基磺酰基)乙基)-N'-亚硝基脲)是一种新型氯乙基亚硝基脲(CENU),正在用于播散性黑色素瘤的II期临床试验。临床结果显示,在用CENU治疗的黑色素瘤中,仅25%观察到肿瘤消退。已知肿瘤对CENU的耐药性主要归因于一种DNA修复蛋白,O6-甲基鸟嘌呤-DNA甲基转移酶(MGMT)。黑色素瘤对CENU的缓解率低归因于转移灶中MGMT水平较高这一事实。此前,我们已经表明,MGMT抑制剂O6-苄基-N2-乙酰鸟苷(BNAG)可通过静脉给药与西司莫司汀联合使用,并增强西司莫司汀对耐药性人黑色素瘤的抗肿瘤作用。在本文介绍的工作中,我们研究了这种联合用药对人黑色素瘤细胞(M3Dau细胞)DNA的体外药理作用。采用定量聚合酶链反应(QPCR)测定法来测量次黄嘌呤磷酸核糖转移酶(hprt)基因片段(2.7 kb)中的DNA损伤。结果表明,用BNAG处理可增加西司莫司汀处理的耐药性恶性黑色素细胞DNA中的损伤数量,这可能解释了西司莫司汀与BNAG联合用药对肿瘤细胞的高毒性。

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