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多药耐药基因(MRP)与小细胞肺癌异种移植瘤中MDR1的表达:与化疗反应的关系

Multidrug resistance genes (MRP) and MDR1 expression in small cell lung cancer xenografts: relationship with response to chemotherapy.

作者信息

Canitrot Y, Bichat F, Cole S P, Deeley R G, Gerlach J H, Bastian G, Arvelo F, Poupon M F

机构信息

Cancer Research Laboratories, Queen's University, Kingston, Ontario, Canada.

出版信息

Cancer Lett. 1998 Aug 14;130(1-2):133-41. doi: 10.1016/s0304-3835(98)00128-1.

Abstract

Intrinsic or acquired drug resistance is a major limiting factor of the effectiveness of chemotherapy. Increased expression of either the MRP gene or the MDR1 gene has been demonstrated to confer drug resistance in vitro. In this study, we examined MRP and MDR1 gene expression in a panel of 17 small cell lung cancers (SCLC) xenografted into nude mice from treated and untreated patients using an RT-PCR technique. For some of them, the outcome of the corresponding patients was known and we related MDR1/MRP expression with the xenograft response to C'CAV (cyclophosphamide, cisplatin, adriamycin and etoposide) combined chemotherapy. Fifteen (88%) of the 17 cases of SCLC were found to be positive for either MDR1 or MRP. MRP gene expression was present in 12 (71%) of 17 cases, whereas MDR1 gene expression was detected in eight (50%) of 16 cases. For six SCLC, the survival duration of patients differed, with three patients surviving for more than 30 months after therapy. Among these six turnours, five expressed MRP and/or MDR1. These six xenografts responded to the C'CAV treatment but a significant rate of cure was obtained in only three cases. No obvious relationship was observed between the response to this treatment and MRP or MDR1 expression. However, the remarkably high levels and frequency of MRP expression in some SCLC samples indicate that future developments in chemotherapy of this tumour type should anticipate that drugs which are substrates of MRP may be of limited effectiveness.

摘要

内在性或获得性耐药是化疗有效性的主要限制因素。已证实在体外,MRP基因或MDR1基因的表达增加可导致耐药。在本研究中,我们使用逆转录聚合酶链反应(RT-PCR)技术检测了17例来自经治疗和未经治疗患者的小细胞肺癌(SCLC)裸鼠异种移植瘤中MRP和MDR1基因的表达。对于其中一些病例,相应患者的预后是已知的,我们将MDR1/MRP表达与异种移植瘤对C'CAV(环磷酰胺、顺铂、阿霉素和依托泊苷)联合化疗的反应相关联。17例SCLC病例中有15例(88%)被发现MDR1或MRP呈阳性。17例中有12例(71%)存在MRP基因表达,而16例中有8例(50%)检测到MDR1基因表达。对于6例SCLC,患者的生存时间不同,3例患者在治疗后存活超过30个月。在这6个肿瘤中,5个表达MRP和/或MDR1。这6个异种移植瘤对C'CAV治疗有反应,但仅3例获得了显著的治愈率。未观察到对该治疗的反应与MRP或MDR1表达之间有明显关系。然而,一些SCLC样本中MRP表达的水平和频率非常高,这表明这种肿瘤类型化疗的未来发展应预期MRP底物药物的有效性可能有限。

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