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首页> 外文期刊>Proteins: Structure, Function, and Genetics >Design of human granzyme B variants resistant to serpin B9
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Design of human granzyme B variants resistant to serpin B9

机译:抗丝氨酸蛋白酶抑制剂B9的人类颗粒酶B变体的设计

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摘要

Human granzyme B (hGB) is a serine protease involved in immune-mediated apoptosis. Its cytotoxicity makes it potentially applicable in cancer therapy. However, the effectiveness of hGB can be hampered by the cytosolic expression of a natural protein inhibitor, human Serpin B9 (hSB9). Here, we used computational approaches to identify hGB mutations that can affect its binding to hSB9 without significantly decreasing its catalytic efficiency. Alanine-scanning calculations allowed us to identify residues of hGB important for the interaction with hSB9. Some variants were selected, and molecular dynamic simulations on the mutated hGB in complex with hSB9 in aqueous solution were carried out to investigate the effect of these variants on the stability of the complex. The R28K, R201A, and R201K mutants significantly destabilized the interaction of the protein with hSB9. Consistently, all of these variants also retained their activity in the presence of the Serpin B9 inhibitor in subsequent in vitro assays of wild-type and mutated hGB. In particular, the activity of R201K hGB with and without Serpin B9 is very similar to that of the wild-type protein. Hence, R201K hGB emerges as a promising species for antitumoral therapy applications.
机译:人粒酶B(hGB)是一种丝氨酸蛋白酶,参与免疫介导的细胞凋亡。它的细胞毒性使其有可能应用于癌症治疗。但是,hGB的有效性可能会受到天然蛋白抑制剂人Serpin B9(hSB9)的胞质表达的影响。在这里,我们使用计算方法来鉴定可影响其与hSB9结合而不显着降低其催化效率的hGB突变。丙氨酸扫描计算使我们得以鉴定对于与hSB9相互作用重要的hGB残基。选择了一些变体,并在水溶液中与hSB9进行了复合物中突变的hGB分子动力学模拟,以研究这些变体对复合物稳定性的影响。 R28K,R201A和R201K突变体极大地破坏了蛋白质与hSB9的相互作用。一致地,在随后的野生型和突变hGB体外测定中,所有这些变体在Serpin B9抑制剂存在下也保留了其活性。特别地,具有和不具有丝氨酸蛋白酶抑制剂B9的R201K hGB的活性与野生型蛋白的活性非常相似。因此,R201K hGB成为抗肿瘤治疗应用的有前途的物种。

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