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Co-expression of CD147/EMMPRIN with monocarboxylate transporters and multiple drug resistance proteins is associated with epithelial ovarian cancer progression

机译:CD147 / EMMPRIN与单羧酸转运蛋白和多种耐药蛋白的共表达与上皮性卵巢癌的进展有关

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Cancer metastasis and anti-cancer drug resistance are the major reason for the failure of clinical cancer treatment. We evaluated CD147, monocarboxylate transporters (MCT1 and MCT4), and multidrug resistance (MDR) markers (MDR1 and MRP2) in 4 epithelial ovarian cancer (EOC) cell lines and primary tumors (n = 120) along with the matched metastatic lesions (n = 40) with immunofluorescence labeling. We correlated CD147 with MCT1, MCT4, MDR1 and MRP2 markers in primary and metastatic cells in cell lines and tissues using confocal microscopy. We also investigated the relationship of expression of CD147, MCT1 and MCT4 with various progression parameters. Our results indicate that the co-expression of CD147 with MCTs or MDR markers was found in primary and metastatic EOC cells and stromal cells; the over-expression of CD147, MCT1 and MCT4 was found in most primary and the matched metastatic lesions of EOC, and was significantly associated with tumor stage, grade, residual disease status and presence of ascites (P 0.05). These results suggest that over-expression of CD147, MCT1 and MCT4 is correlated with EOC progression, and co-expression of CD147 and MCT1/MCT4 is related to drug resistance during EOC metastasis and could be useful therapeutic targets to prevent the development of incurable, recurrent and drug resistance EOC.
机译:癌症转移和抗癌药耐药性是临床癌症治疗失败的主要原因。我们评估了4种上皮性卵巢癌(EOC)细胞系和原发性肿瘤(n = 120)中CD147,单羧酸转运蛋白(MCT1和MCT4)和多药抗性(MDR)标记(MDR1和MRP2)以及匹配的转移性病变(n = 40),带有免疫荧光标记。我们使用共聚焦显微镜将CD147与细胞系和组织中原代和转移细胞中的MCT1,MCT4,MDR1和MRP2标记相关。我们还研究了CD147,MCT1和MCT4的表达与各种进展参数的关系。我们的结果表明,在原代和转移性EOC细胞和基质细胞中发现了CD147与MCT或MDR标记的共表达。 CD147,MCT1和MCT4的过度表达在大多数原发性和匹配的EOC转移性病变中均发现,并且与肿瘤的分期,分级,残留疾病状态和腹水的存在密切相关(P 0.05)。这些结果表明,CD147,MCT1和MCT4的过度表达与EOC进展相关,而CD147和MCT1 / MCT4的共表达与EOC转移过程中的耐药性相关,并且可能是预防不可治愈的疾病的有用治疗靶点,复发和耐药性EOC。

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