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Design, Optimization, and Structural Characterization of an Apoptosis-Inducing Factor Peptide Targeting Human Cyclophilin A to Inhibit Apoptosis Inducing Factor-Mediated Cell Death

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Figshare2021-08-02 更新2026-04-28 收录
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https://figshare.com/articles/dataset/Design_Optimization_and_Structural_Characterization_of_an_Apoptosis-Inducing_Factor_Peptide_Targeting_Human_Cyclophilin_A_to_Inhibit_Apoptosis_Inducing_Factor-Mediated_Cell_Death/15091155
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Blocking the interaction between the apoptosis-inducing factor (AIF) and cyclophilin A (CypA) by the AIF fragment AIF(370–394) is protective against glutamate-induced neuronal cell death and brain injury in mice. Starting from AIF(370–394), we report the generation of the disulfide-bridged and shorter variant AIF(381–389) and its structural characterization by nuclear magnetic resonance (NMR) in the free and CypA-bound state. AIF(381–389) in both the free and bound states assumes a β-hairpin conformation similar to that of the fragment in the AIF protein and shows a highly reduced conformational flexibility. This peptide displays a similar in vitro affinity for CypA, an improved antiapoptotic activity in cells and an enhanced proteolytic stability compared to the parent peptide. The NMR-based 3D model of the AIF(381–389)/CypA complex provides a better understanding of the binding hot spots on both the peptide and the protein and can be exploited to design AIF/CypA inhibitors with improved pharmacokinetic and pharmacodynamics features.
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2021-08-02
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