首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Structure-based interpretation of the mutagenesis database for the nucleotide binding domains of P-glycoprotein.
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Structure-based interpretation of the mutagenesis database for the nucleotide binding domains of P-glycoprotein.

机译:P糖蛋白核苷酸结合结构域的诱变数据库的基于结构的解释。

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摘要

P-glycoprotein (P-gp) is the most intensively studied eukaryotic ATP binding cassette (ABC) transporter, due to its involvement in the multidrug resistance phenotype of a number of cancers. In common with most ABC transporters, P-gp is comprised of two transmembrane domains (TMDs) and two nucleotide binding domains (NBD), the latter coupling ATP hydrolysis with substrate transport (efflux in the case of P-gp). Biochemical investigations over the past twenty years have attempted to unlock mechanistic aspects of P-glycoprotein through scanning and site-directed mutagenesis of both the TMDs and the NBDs. Contemporaneously, crystallographers have elucidated the atomic structure of numerous ABC transporter NBDs, as well as the intact structure (i.e. NBDs and TMDs) of a distantly related ABC-exporter Sav1866. Significantly, the structure of P-gp remains unknown, and only low resolution electron microscopy data exists. Within the current manuscript we employ crystallographic data for homologous proteins, and a molecular model for P-gp, to perform a structural interpretation of the existing "mutagenesis database" for P-gp NBDs. Consequently, this will enable testable predictions to be made that will result in further in-roads into our understanding of this clinically important drug pump.
机译:P-糖蛋白(P-gp)是最深入研究的真核ATP结合盒(ABC)转运蛋白,因为它参与了许多癌症的多药耐药表型。与大多数ABC转运蛋白一样,P-gp由两个跨膜结构域(TMD)和两个核苷酸结合结构域(NBD)组成,后者将ATP水解与底物转运结合(在P-gp情况下为外排)。在过去的二十年中,生化研究试图通过对TMD和NBD进行扫描和定点诱变来揭示P-糖蛋白的机制。同时,晶体学家已经阐明了许多ABC转运蛋白NBD的原子结构,以及远缘相关的ABC出口商Sav1866的完整结构(即NBD和TMD)。值得注意的是,P-gp的结构仍是未知的,并且仅存在低分辨率电子显微镜数据。在当前的手稿中,我们使用同源蛋白质的晶体学数据和P-gp的分子模型,对P-gp NBD的现有“诱变数据库”进行结构解释。因此,这将使可以进行可测的预测成为可能,从而进一步加深我们对这种具有临床意义的药物泵的理解。

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