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Involvement of the Multidrug Resistance Protein 3 in Drug Sensitivity and Its Expression in Human Glioma

机译:多药耐药蛋白3参与药物敏感性及其在人胶质瘤中的表达

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摘要

The multidrug resistance protein (MRP) family belongs to the ATP‐binding cassette superfamily (ABC) of transporters, which are involved in ATP‐dependent transport of hydrophobic compounds. One of the MRP family, MRP1, is partially associated with the multidrug resistance phe‐notype in brain tumors. In this study, we asked whether another MRP family gene, MRP3, could affect drug sensitivity to anticancer agents in human glioma cell lines and clinical glioma specimens. We first produced two antisense transfectants by introduction of antisense MRP3 cDNA into the glioma cell line NHG2, which endogenously expresses MRP3. The two MRP3 antisense transfectants showed 2‐ to 5‐fold increases in drug sensitivity to etoposide and cisplatin compared with NHG2 cells, but their sensitivity to vincristine or nitrosourea was not changed. Two MRP3 cDNA sense transfectants of pig kidney cell lines showed 4‐ to 6‐fold drug resistance to etoposide, but only 1.4‐ to 1.5‐fold to cisplatin. We next compared the mRNA levels of four ABC transporters, multi‐drug resistance 1 (MDR1), MRP1, MRP2 and MRP3 in clinical samples, including 34 patients with gliomas, by quantitative RT‐PCR analysis. In some of the clinical samples, increased expression of MRP1 and MRP3 was apparent in malignant gliomas. In situ hybridization revealed that glioma cells were stained with MRP3 probe. MRP3 may modulate drug sensitivity to certain anticancer agents in human gliomas.
机译:多药耐药蛋白(MRP)家族属于转运蛋白的ATP结合盒超家族(ABC),与疏水化合物的ATP依赖性转运有关。 MRP家族之一MRP1与脑肿瘤的多药耐药表型部分相关。在这项研究中,我们询问另一个MRP家族基因MRP3是否会影响人类神经胶质瘤细胞系和临床神经胶质瘤标本对抗癌药的药物敏感性。我们首先通过将反义MRP3 cDNA引入神经胶质瘤细胞系NHG2(内源性表达MRP3)中,产生了两种反义转染子。与NHG2细胞相比,两种MRP3反义转染子对依托泊苷和顺铂的药物敏感性提高了2到5倍,但它们对长春新碱或亚硝基脲的敏感性没有改变。猪肾细胞系的两种MRP3 cDNA有义转染子对依托泊苷的耐药性为4到6倍,对顺铂的耐药性仅为1.4到1.5倍。接下来,我们通过定量RT-PCR分析比较了临床样本(包括34例神经胶质瘤患者)中四种ABC转运蛋白,多重耐药性1(MDR1),MRP1,MRP2和MRP3的mRNA水平。在某些临床样品中,恶性神经胶质瘤中MRP1和MRP3的表达明显升高。原位杂交显示神经胶质瘤细胞被MRP3探针染色。 MRP3可能会调节人胶质瘤对某些抗癌药的药物敏感性。

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