Tumor-specific expression of organic anion-transporting polypeptides: transporters as novel targets for cancer therapy.

Journal of drug delivery Pub Date : 2013-01-01 Epub Date: 2013-02-03 DOI:10.1155/2013/863539
Veronika Buxhofer-Ausch, Lena Secky, Katrin Wlcek, Martin Svoboda, Valentinos Kounnis, Evangelos Briasoulis, Andreas G Tzakos, Walter Jaeger, Theresia Thalhammer
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引用次数: 100

Abstract

Members of the organic anion transporter family (OATP) mediate the transmembrane uptake of clinical important drugs and hormones thereby affecting drug disposition and tissue penetration. Particularly OATP subfamily 1 is known to mediate the cellular uptake of anticancer drugs (e.g., methotrexate, derivatives of taxol and camptothecin, flavopiridol, and imatinib). Tissue-specific expression was shown for OATP1B1/OATP1B3 in liver, OATP4C1 in kidney, and OATP6A1 in testis, while other OATPs, for example, OATP4A1, are expressed in multiple cells and organs. Many different tumor entities show an altered expression of OATPs. OATP1B1/OATP1B3 are downregulated in liver tumors, but highly expressed in cancers in the gastrointestinal tract, breast, prostate, and lung. Similarly, testis-specific OATP6A1 is expressed in cancers in the lung, brain, and bladder. Due to their presence in various cancer tissues and their limited expression in normal tissues, OATP1B1, OATP1B3, and OATP6A1 could be a target for tumor immunotherapy. Otherwise, high levels of ubiquitous expressed OATP4A1 are found in colorectal cancers and their metastases. Therefore, this OATP might serve as biomarkers for these tumors. Expression of OATP is regulated by nuclear receptors, inflammatory cytokines, tissue factors, and also posttranslational modifications of the proteins. Through these processes, the distribution of the transporter in the tissue will be altered, and a shift from the plasma membrane to cytoplasmic compartments is possible. It will modify OATP uptake properties and, subsequently, change intracellular concentrations of drugs, hormones, and various other OATP substrates. Therefore, screening tumors for OATP expression before therapy should lead to an OATP-targeted therapy with higher efficacy and decreased side effects.

Abstract Image

Abstract Image

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有机阴离子转运多肽的肿瘤特异性表达:作为癌症治疗新靶点的转运体。
有机阴离子转运蛋白家族(OATP)的成员介导临床重要药物和激素的跨膜摄取,从而影响药物配置和组织渗透。特别是已知OATP亚家族1介导抗癌药物的细胞摄取(例如,甲氨蝶呤、紫杉醇和喜树碱的衍生物、黄哌啶醇和伊马替尼)。OATP1B1/OATP1B3在肝脏中有组织特异性表达,OATP4C1在肾脏中有组织特异性表达,OATP6A1在睾丸中有组织特异性表达,而其他oatp,如OATP4A1,在多个细胞和器官中表达。许多不同的肿瘤实体显示oops的表达改变。OATP1B1/OATP1B3在肝脏肿瘤中下调,但在胃肠道、乳腺癌、前列腺癌和肺癌中高表达。同样,睾丸特异性OATP6A1在肺癌、脑癌和膀胱癌中表达。由于OATP1B1、OATP1B3和OATP6A1存在于多种癌症组织中,而在正常组织中表达有限,因此它们可能成为肿瘤免疫治疗的靶点。此外,在结直肠癌及其转移中发现了高水平的普遍表达OATP4A1。因此,这种OATP可能作为这些肿瘤的生物标志物。OATP的表达受核受体、炎症细胞因子、组织因子以及蛋白翻译后修饰的调控。通过这些过程,转运蛋白在组织中的分布将被改变,从质膜转移到细胞质室是可能的。它将改变OATP的摄取特性,并随后改变细胞内药物、激素和各种其他OATP底物的浓度。因此,在治疗前对肿瘤进行OATP的表达筛查,应该会导致OATP靶向治疗的更高疗效和更少的副作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of drug delivery
Journal of drug delivery PHARMACOLOGY & PHARMACY-
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