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化疗期间膀胱癌中MDR1基因的过表达及启动子区域甲基化程度的改变

MDR1 gene overexpression and altered degree of methylation at the promoter region in bladder cancer during chemotherapeutic treatment.

作者信息

Tada Y, Wada M, Kuroiwa K, Kinugawa N, Harada T, Nagayama J, Nakagawa M, Naito S, Kuwano M

机构信息

Department of Medical Biochemistry, Graduate School of Medical Sciences, Kyushu University, Fukuoka, Japan.

出版信息

Clin Cancer Res. 2000 Dec;6(12):4618-27.

Abstract

Overexpression of the multidrug resistance 1 (MDR1) gene is closely associated with the clinical outcome of hematopoietic malignancies, but the alteration of its expression during chemotherapeutic treatment and the precise mechanism underlying MDR1 gene overexpression in solid tumors remains unclear. We determined the expression and degree of methylation at the promoter of the MDR1 gene in bladder cancer. The mRNA levels of the MDR1 gene were found to be markedly enhanced, 3.5- to 5.7-fold higher in bladder cancers after chemotherapeutic treatment than those in untreated primary tumors. The MDR1 gene was overexpressed in recurrent tumors in 89% of patients who showed rerecurrence, whereas overexpression was observed in 25% of the patients without re-recurrence. A statistically significant inverse correlation existed between MDR1 expression and the methylation of 5'CpG sites at the promoter in patients with bladder cancer after chemotherapeutic treatment, with the degree of methylation at several CpG sites, rather than other specific sites, involved in this regulation. Consistent with the increase in MDR1 expression, the frequency of patients with a hypermethylated promoter decreased to 50 and 17% after intravesical and systemic chemotherapy, respectively. Thus, overexpression of the MDR1 gene might be a prognostic marker for intravesical recurrence, whereas methylation of the promoter region negatively regulates MDR1 expression and the appearance of multidrug resistance mediated by P-glycoprotein in bladder cancers.

摘要

多药耐药1(MDR1)基因的过表达与造血系统恶性肿瘤的临床预后密切相关,但在化疗过程中其表达的变化以及实体瘤中MDR1基因过表达的确切机制仍不清楚。我们测定了膀胱癌中MDR1基因启动子的表达及甲基化程度。发现MDR1基因的mRNA水平显著增强,化疗后的膀胱癌中该基因的mRNA水平比未治疗的原发性肿瘤高3.5至5.7倍。在出现复发的患者中,89%的复发性肿瘤中MDR1基因过表达,而在未复发的患者中,25%观察到过表达。化疗后的膀胱癌患者中,MDR1表达与启动子区5'CpG位点的甲基化之间存在统计学上显著的负相关,参与这种调控的是几个CpG位点而非其他特定位点的甲基化程度。与MDR1表达增加一致,膀胱内化疗和全身化疗后,启动子高甲基化患者的比例分别降至50%和17%。因此,MDR1基因的过表达可能是膀胱内复发的一个预后标志物,而启动子区域的甲基化负向调节MDR1表达以及膀胱癌中由P-糖蛋白介导的多药耐药的出现。

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