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首页> 外文期刊>Proteins: Structure, Function, and Genetics >A model for the nucleotide-binding domains of ABC transporters based on the large domain of aspartate aminotransferase.
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A model for the nucleotide-binding domains of ABC transporters based on the large domain of aspartate aminotransferase.

机译:基于天冬氨酸转氨酶大结构域的ABC转运蛋白核苷酸结合结构域模型。

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摘要

ABC transporters are a large superfamily of integral membrane proteins involved inATP-dependent transport across biological membranes. Members of this superfamily play roles in a number of phenomena of biomedical interest, including cystic fibrosis (CFTR) and multidrug resistance (P-glycoprotein, MRP). Most ABC transporters are predicted to consist of four domains, two membrane-spanning domains and two cytoplasmic domains. The latter contain conserved nucleotide-binding motifs. Attempts to determine the structure of ABC transporters and of their separate domains are in progress but have not yet been successful. To aid structure determination and possibly learn more about the domain boundaries, we set out to model nucleotide-binding domains (NBDs) of ABC transporters based on a known structure. Previous attempts to predict the 3D structure of NBDs were based solely on sequence similarity with known nucleotide-binding folds. We have analyzed the sequences of a number of nucleotide-binding domains with the algorithm THREADER, developed by D.T. Jones, and a possible fold was found in the structure of aspartate aminotransferase. We present a model for the N-terminal NBD of CFTR, based on the large domain of the A chain of aspartate aminotransferase. The model is refined using multiple sequence alignment, secondary structure prediction, and 3D-1D profiles. Our model seems to be in good agreement with known properties of nucleotide-binding domains and has some appealing characteristics compared with the previous models.
机译:ABC转运蛋白是一个完整的膜蛋白超大家族,涉及跨生物膜的ATP依赖性转运。这个超家族的成员在许多生物医学感兴趣的现象中起作用,包括囊性纤维化(CFTR)和多药耐药性(P-糖蛋白,MRP)。预测大多数ABC转运蛋白由四个结构域,两个跨膜结构域和两个胞质结构域组成。后者含有保守的核苷酸结合基序。正在尝试确定ABC转运蛋白及其单独域的结构,但尚未成功。为了帮助确定结构并可能更多地了解域边界,我们开始基于已知结构对ABC转运蛋白的核苷酸结合域(NBD)进行建模。先前预测NBD 3D结构的尝试仅基于与已知核苷酸结合折叠的序列相似性。我们已经用D.T. Jones开发的THREADER算法分析了许多核苷酸结合域的序列,发现天冬氨酸转氨酶的结构可能存在折叠。基于天冬氨酸转氨酶A链的大域,我们提出了CFTR N末端NBD的模型。使用多个序列比对,二级结构预测和3D-1D配置文件完善模型。我们的模型似乎与核苷酸结合域的已知特性非常吻合,并且与以前的模型相比具有一些吸引人的特征。

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