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The Cryptococcus neoformans monocarboxylate transporter Jen4 is responsible for increased 3-bromopyruvate sensitivity

机译:碱性Cococcus neoformans单羧酸酯转运蛋白jen4负责增加的3-溴吡吡喃酸敏感性

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In the last decades, 3-bromopyruvate (3BP) has been intensively studied as a promising anticancer and antimicrobial agent. The transport of this drug inside the cell is a critical step for its toxicity in cancer and microorganisms. The Cryptococcus neoformans is the most sensitive species of microorganisms toward 3BP. Its cells exhibit the highest uptake rate of 3BP among all tested fungal strains. In Saccharomyces cerevisiae cells, the Jen1 transporter was found to be responsible for 3BP sensitivity. The deletion of Jen1 resulted in the abolishment of 3BP mediated transport. We functionally characterized the Jen4 protein, a Jen1 homologue of C. neoformans, and its role in the phenotypic 3BP sensitivity. The deletion of the CNAG_04704 gene, which encodes Jen4, was found to impair the mediated transport of 3BP and decrease 3BP sensitivity. Further heterologous expression of Jen4 in the S. cerevisiae jen1 Delta ady2 Delta strain restored the mediated transport of 3BP. The application of a green fluorescent protein fusion tag with the CNAG_04704, revealed the Jen4 labeled on the plasma membrane. The identification of 3BP transporters in pathogen cells is of great importance for understanding the mechanisms of 3BP action and to anticipate the application of this compound as an antimicrobial drug.
机译:在过去的几十年中,3-溴呢(3BP)被密深为一个有前途的抗癌和抗微生物剂。该药物在细胞内的运输是癌症和微生物中毒性的关键步骤。隐性球菌新族裔是微生物最敏感的微生物朝向3BP。其细胞在所有测试的真菌菌株中表现出3BP的最高摄取率。在酿酒酵母细胞中,发现JEN1转运蛋白负责3bp敏感性。 JEN1的删除导致3BP介导的运输中的废除。我们在功能上表现了JEN4蛋白,Jen1 Neoformans的Jen1同源物,其在表型3BP敏感性中的作用。发现编码JEN4的CNAG_04704基因的缺失损害了介导的3BP迁移并降低了3BP敏感性。 EREVISIAE JEN1 DELTA ADY2 DELTA菌株在S.Cerevisiae jen1ΔAdy2δ的进一步异源表达恢复了3bp的介导的运输。将绿色荧光蛋白融合标签与CNAG_04704的应用揭示了JEN4标记在血浆膜上。鉴定病原体细胞中的3BP转运蛋白是对理解3BP作用的机制并预期该化合物作为抗微生物药物的应用的重要性。

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