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多药耐药小鼠P388和B16细胞系中P-糖蛋白基因的扩增与表达

P-glycoprotein gene amplification and expression in multidrug-resistant murine P388 and B16 cell lines.

作者信息

Capranico G, De Isabella P, Castelli C, Supino R, Parmiani G, Zunino F

机构信息

Division of Experimental Oncology B, Istituto Nazionale Tumori, Milan, Italy.

出版信息

Br J Cancer. 1989 May;59(5):682-5. doi: 10.1038/bjc.1989.141.

Abstract

P-glycoprotein gene (mdrl) amplification and expression were examined in murine leukaemia P388/DX and melanoma B16VDXR cell lines, which exhibit a high level of resistance to a selecting agent, doxorubicin, and express a multidrug-resistant phenotype because they are cross-resistant to multiple cytotoxic drugs. The multidrug-resistant phenotype was obtained in different conditions of selection (in vivo and in vitro for P388/DX and B16VDXR, respectively). In both multidrug-resistant cell lines, an increased expression of P-glycoprotein gene (5 kb transcript detected in Northern blots) was observed and the level of P-glycoprotein mRNA correlated with the degree of resistance. In addition, high molecular weight mRNAs homologous to mdrl gene sequence were consistently detected only in P388/DX cells. Overexpression was associated with a high level of gene amplification only in resistant melanoma cells, whereas it occurred in P388/DX cells with a marginal increase in gene copy number. These results, suggesting that different genetic mechanisms could be responsible for P-glycoprotein overexpression, emphasise the complexity of genetic regulation that may affect tumour cell sensitivity to cytotoxic agents.

摘要

在小鼠白血病P388/DX和黑色素瘤B16VDXR细胞系中检测了P-糖蛋白基因(mdrl)的扩增和表达。这两种细胞系对选择剂阿霉素表现出高度抗性,并表达多药耐药表型,因为它们对多种细胞毒性药物具有交叉抗性。多药耐药表型是在不同的选择条件下获得的(分别在体内和体外对P388/DX和B16VDXR进行选择)。在这两种多药耐药细胞系中,均观察到P-糖蛋白基因表达增加(在Northern印迹中检测到5 kb转录本),且P-糖蛋白mRNA水平与耐药程度相关。此外,仅在P388/DX细胞中持续检测到与mdrl基因序列同源的高分子量mRNA。过表达仅在耐药黑色素瘤细胞中与高水平的基因扩增相关,而在P388/DX细胞中过表达时基因拷贝数仅有少量增加。这些结果表明不同的遗传机制可能导致P-糖蛋白过表达,强调了可能影响肿瘤细胞对细胞毒性药物敏感性的遗传调控的复杂性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/52b5/2247236/43f107690572/brjcancer00127-0027-a.jpg

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