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犬淋巴细胞系中因P-糖蛋白表达增加导致的多药耐药性,一种耐药性犬淋巴瘤的潜在模型。

Multi-drug resistance in a canine lymphoid cell line due to increased P-glycoprotein expression, a potential model for drug-resistant canine lymphoma.

作者信息

Zandvliet M, Teske E, Schrickx J A

机构信息

Department of Clinical Sciences of Companion Animals, Faculty of Veterinary Medicine, Utrecht University, Yalelaan 108, P.O. Box 80154, 3508 TD Utrecht, The Netherlands.

Department of Clinical Sciences of Companion Animals, Faculty of Veterinary Medicine, Utrecht University, Yalelaan 108, P.O. Box 80154, 3508 TD Utrecht, The Netherlands.

出版信息

Toxicol In Vitro. 2014 Dec;28(8):1498-506. doi: 10.1016/j.tiv.2014.06.004. Epub 2014 Jun 26.

DOI:10.1016/j.tiv.2014.06.004
PMID:24975508
Abstract

Canine lymphoma is routinely treated with a doxorubicin-based multidrug chemotherapy protocol, and although treatment is initially successful, tumor recurrence is common and associated with therapy resistance. Active efflux of chemotherapeutic agents by transporter proteins of the ATP-Binding Cassette superfamily forms an effective cellular defense mechanism and a high expression of these transporters is frequently observed in chemotherapy-resistant tumors in both humans and dogs. In this study we describe the ABC-transporter expression in a canine lymphoid cell line and a sub-cell line with acquired drug resistance following prolonged exposure to doxorubicin. This sub-cell line was more resistant to doxorubicin and vincristine, but not to prednisolone, and had a highly increased P-glycoprotein (P-gp/abcb1) expression and transport capacity for the P-gp model-substrate rhodamine123. Both resistance to doxorubicin and vincristine, and rhodamine123 transport capacity were fully reversed by the P-gp inhibitor PSC833. No changes were observed in the expression and function of the ABC-transporters MRP-1 and BCRP. It is concluded that GL-40 cells represent a useful model for studying P-gp dependent drug resistance in canine lymphoid neoplasia, and that this model can be used for screening substances as potential P-gp substrates and their capacity to modulate P-gp mediated drug resistance.

摘要

犬淋巴瘤通常采用基于阿霉素的多药化疗方案进行治疗,尽管治疗初期取得成功,但肿瘤复发很常见且与治疗耐药性相关。ATP结合盒超家族转运蛋白对化疗药物的主动外排形成了一种有效的细胞防御机制,在人类和犬类的化疗耐药肿瘤中经常观察到这些转运蛋白的高表达。在本研究中,我们描述了犬类淋巴细胞系和一个在长期暴露于阿霉素后获得耐药性的亚细胞系中ABC转运蛋白的表达情况。该亚细胞系对阿霉素和长春新碱更具耐药性,但对泼尼松龙不耐药,并且P-糖蛋白(P-gp/abcb1)的表达和对P-gp模型底物罗丹明123的转运能力显著增加。P-gp抑制剂PSC833完全逆转了对阿霉素和长春新碱的耐药性以及罗丹明123的转运能力。未观察到ABC转运蛋白MRP-1和BCRP的表达及功能发生变化。得出的结论是,GL-40细胞是研究犬类淋巴瘤中P-gp依赖性耐药性的有用模型,并且该模型可用于筛选作为潜在P-gp底物的物质及其调节P-gp介导的耐药性的能力。

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