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首页> 外文期刊>FEMS Yeast Research >ABC transporter Cdr1p harbors charged residues in the intracellular loop and nucleotide-binding domain critical for protein trafficking and drug resistance
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ABC transporter Cdr1p harbors charged residues in the intracellular loop and nucleotide-binding domain critical for protein trafficking and drug resistance

机译:ABC转运蛋白Cdr1p在细胞内环中包含带电荷的残基和核苷酸结合结构域,对蛋白质运输和耐药性至关重要

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摘要

The ABC transporter Cdr1 protein of Candida albicans, which plays a major role in antifungal resistance, has two transmembrane domains (TMDs) and two nucleotide-binding domains (NBDs). The 12 transmembrane helices of TMDs that are interconnected by extracellular and intracellular loops (ICLs) mainly harbor substrate recognition sites where drugs bind while cytoplasmic NBDs hydrolyze ATP which powers drug efflux. The coupling of ATP hydrolysis to drug transport requires proper communication between NBDs and TMDs typically accomplished by ICLs. This study examines the role of cytoplasmic ICLs of Cdr1p by rationally predicting the critical residues on the basis of their interatomic distances. Among nine pairs that fall within a proximity of <4 angstrom, an ion pair between K577 of ICL1 and E315 of NBD1 was found to be critical. The substitution, swapping and changing of the length or charge of K577 or E315 by directed mutagenesis led to a misfolded, non-rescuable protein entrapped in intracellular structures. Furthermore, the equipositional ionic pair-forming residues from ICL3 and NBD2 (R1260 and E1014) did not impact protein trafficking. These results point to a new role for ICL/NBD interacting residues in PDR ABC transporters in protein folding and trafficking.
机译:白色念珠菌的ABC转运蛋白Cdr1蛋白在抗真菌抗性中起主要作用,具有两个跨膜结构域(TMD)和两个核苷酸结合结构域(NBD)。通过细胞外和细胞内环(ICL)相互连接的TMD的12个跨膜螺旋主要包含药物结合的底物识别位点,而胞质NBD水解ATP促进药物外排。 ATP水解与药物运输的耦合要求NBD和TMD之间通常通过ICL完成适当的通讯。这项研究通过根据原子间距离合理预测关键残基来研究Cdr1p胞质ICL的作用。在落在<4埃范围内的9对离子对中,ICL1的K577和NBD1的E315之间的离子对至关重要。通过定向诱变对K577或E315的长度或电荷进行替换,交换和改变,导致细胞内结构中存在错误折叠的,不可挽回的蛋白质。此外,ICL3和NBD2(R1260和E1014)形成等离子对的残基不影响蛋白质运输。这些结果指出了PDR ABC转运蛋白中ICL / NBD相互作用残基在蛋白质折叠和运输中的新作用。

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