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Peptide Fibrils with Altered Stability, Activity, And Cell Selectivity

机译:具有改变的稳定性,活性和细胞选择性的肽原纤维

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Peptides have some unique and superior features compared to proteins. However, the use of peptides as therapeutics is hampered by their low stability and cell selectivity. In this study, a new lytic peptide (CL-1, FLGALFRALSRLL) was constructed. Under the physiological condition, peptide CL-1 self-assembled into dynamically stable aggregates with fibrils-like structures. Aggregated CL-1 demonstrated dramatically altered activity and stability in comparison with single molecule CL-1 and other lytic peptides: when incubated with cocultured bacteria and tissue cells, CL-1 aggregates killed bacteria selectively but spared cocultured human cells; CL-1 aggregates were kept intact in human serum for more than five hours. Peptide-cell interaction studies performed on lipid monolayers and live human tissue cells revealed that in comparison with monomeric CL-1, aggregated CL-1 had decreased cell affinity and membrane insertion capability on tissue cells. A dynamic process involvmg aggregate dissociation and rearrangement seemed to be an essential step for membrane bound CL-1 aggregates to realize its cytotoxicity to tissue cells. Our study suggests that peptide aggregation could be as important as the charge and secondary structure of a peptide in affecting peptide-cell interactions. Controlling peptide self-assembly represents a new way to increase the stability and cell selectivity of bioactive peptides for wide biomedical applications.
机译:与蛋白质相比,肽具有一些独特和优越的功能。然而,由于其低的稳定性和细胞选择性,阻碍了肽作为治疗剂的使用。在这项研究中,构建了新的裂解肽(CL-1,FLGALFRALSRLL)。在生理条件下,肽CL-1自组装成具有纤维状结构的动态稳定聚集体。与单分子CL-1和其他裂解肽相比,聚集的CL-1表现出显着改变的活性和稳定性:与共培养的细菌和组织细胞孵育时,CL-1选择性地杀死了细菌,但保留了未培养的共培养的人类细胞。 CL-1聚集体在人血清中保持完整状态超过五个小时。在脂质单层和人类活组织细胞上进行的肽-细胞相互作用研究表明,与单体CL-1相比,聚集的CL-1在组织细胞上的细胞亲和力和膜插入能力降低。涉及聚集体解离和重排的动态过程似乎是膜结合的CL-1聚集体实现其对组织细胞的细胞毒性的必要步骤。我们的研究表明,在影响肽-细胞相互作用中,肽聚集可能与肽的电荷和二级结构一样重要。控制肽的自组装代表了一种增加生物活性肽在广泛的生物医学应用中的稳定性和细胞选择性的新方法。

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