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首页> 外文期刊>Journal of liquid chromatography and related technologies >Mass Spectrometric Analysis of Noncovalent Complexes Between Synthetic Peptides from Human Ribosomal Protein L7 and Protein G
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Mass Spectrometric Analysis of Noncovalent Complexes Between Synthetic Peptides from Human Ribosomal Protein L7 and Protein G

机译:人体核糖体蛋白L7和蛋白G的合成肽之间非共价复合物的质谱分析

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摘要

In order to gain a comprehensive insight into the complexes of human ribosomal protein L7 with protein G in a certain degree, an investigation on the complexes of five synthetic L7 peptides, containing the basic-region-leucine-zipper (BZIP)-like domain (aa 15-49), with protein G was performed using nanoelectrospray ionization mass spectrometry (nanoESI-MS). Circular dichroism (CD) was used to characterize the secondary structures of L7 peptides. The characteristics of the complexes between L7 peptides and protein G were studied under various conditions, such as molar ratio of ligands, solvent condition, declustering potential, and peptide sequence. The stability of the complexes is found to decrease with increased declustering potential (>20V), decreased pH (<5), increased pH (>5), while L7 peptide sequence had no obvious effect on the complex formation. Taken together, the complexes of L7 peptides with protein G are specific noncovalent binding with 1:1 stoichiometry. Because of the availability of synthetic L7 peptides, they might be used as baits to discover the binding partners of protein L7. Furthermore, the elaboration of the binding mechanisms of L7 peptides with protein G could benefit further application of protein G.
机译:为了在一定程度上全面了解人核糖体蛋白L7与蛋白G的复合物,研究了五个合成的L7肽的复合物,它们包含基本区域-亮氨酸拉链(BZIP)-样结构域( (氨基酸15-49),使用纳米电喷雾电离质谱(nanoESI-MS)进行蛋白质G的分析。圆二色性(CD)用于表征L7肽的二级结构。研究了L7肽与蛋白G的复合物在各种条件下的特性,例如配体的摩尔比,溶剂条件,脱簇电位和肽序列。发现复合物的稳定性随着解簇电位的增加(> 20V),pH值的降低(<5),pH值的增加(> 5)而降低,而L7肽序列对复合物的形成没有明显影响。总之,L7肽与蛋白质G的复合物是具有1:1化学计量比的特异性非共价结合。由于合成L7肽的可用性,它们可能被用作诱饵来发现蛋白L7的结合伴侣。此外,阐述L7肽与蛋白G的结合机制可能有益于蛋白G的进一步应用。

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