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Intracellular distribution of HMG1, HMG2 and UBF change following treatment with cisplatin

机译:顺铂处理后HMG1,HMG2和UBF的细胞内分布发生变化

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Cisplatin (CDDP) is a widely used cancer diemotlierupeulic agent. CDDP forms well characterized intrastrand cross-links between adjacent purities in genomic DNA. In mammalian cells, these lesions are repaired by the nucleotide excision repair system. An early event in the recognition and processing of cis-Pt-DNA adducts may well involve the binding of specific proteins to the sites of damage. Several proteins have been identified, including high mobility group (HMG) proteins 1 and 2 and upstream binding factor (UBF), which recognize CDDP-DNA. However, the physiological significance of this binding has not been established. In this study, we have utilized antibodies to these proteins to examine the effect of CDDP on their intracellular distribution. Marked changes in the immunofluorescent staining pattern of HMG 1 /IIMG2 were noted in cells treated with CDDP. At higher drug concentrations, the distribution of UBF also changed, from a clustered appearance associated with the nucleoli to more diffuse nuclear staining. These results demonstrate that HMG1/HMG2 and UBF respond to drug treatment, presumably by recognizing cis-Pt-DNA adduct formation in intact cells. Hence, lliese proteins may play an important role in directing the response of tumor cells following exposure to CDDP.
机译:顺铂(CDDP)是一种广泛使用的癌症二茂铁制剂。 CDDP在基因组DNA的相邻纯度之间形成了特征明确的链内交联。在哺乳动物细胞中,这些损伤通过核苷酸切除修复系统修复。顺式-Pt-DNA加合物的识别和加工的早期事件很可能涉及特定蛋白质与损伤部位的结合。已经鉴定出几种蛋白质,包括识别CDDP-DNA的高迁移率族(HMG)蛋白质1和2和上游结合因子(UBF)。但是,这种结合的生理意义尚未确定。在这项研究中,我们利用了针对这些蛋白质的抗体来检查CDDP对它们的细胞内分布的影响。在用CDDP处理的细胞中,HMG 1 / IIMG2的免疫荧光染色模式发生了明显变化。在较高的药物浓度下,UBF的分布也发生了变化,从与核仁相关的簇状外观到更弥散的核染色。这些结果表明,HMG1 / HMG2和UBF对药物治疗有反应,大概是通过识别完整细胞中顺式-Pt-DNA加合物的形成来实现的。因此,在暴露于CDDP后,百合蛋白可能在指导肿瘤细胞的应答中起重要作用。

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