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计算机辅助设计蜂毒素样肽可产生具有延长抗菌特性的无毒变体。

Computer-Aided Design of Mastoparan-like Peptides Enables the Generation of Nontoxic Variants with Extended Antibacterial Properties.

机构信息

Programa de Pós-Graduação em Patologia Molecular, Faculdade de Medicina , Universidade de Brasília , Brasília 70910900 , Brazil.

S-Inova Biotech, Programa de Pós-Graduação em Biotecnologia , Universidade Católica Dom Bosco , Campo Grande 79117900 , Brazil.

出版信息

J Med Chem. 2019 Sep 12;62(17):8140-8151. doi: 10.1021/acs.jmedchem.9b00915. Epub 2019 Aug 26.

Abstract

Diverse peptides have been evaluated for their activity against pathogenic microorganisms. Here, five mastoparan variants were designed based on mastoparan-L, among which two (R1 and R4) were selected for in-depth analysis. Mastoparan-L (parent/control), R1, and R4 inhibited susceptible/resistant bacteria at concentrations ranging from 2 to 32 μM, whereas only R1 and R4 eradicated biofilms at 16 μM. Moreover, the toxic effects of mastoparan-L toward mammalian cells were drastically reduced in both variants. In skin infections, R1 at 64 μM was the most effective variant, reducing bacterial counts 1000 times on day 4 post-infection. Structurally, all of the peptides showed varying levels of helicity and structural stability in aqueous and membrane-like conditions, which may affect the different bioactivities observed here. By computationally modifying the physicochemical properties of R1 and R4, we reduced the cytotoxicity and optimized the therapeutic potential of these mastoparan-like peptides both in vitro and in vivo.

摘要

已经有多种肽类物质因其对致病微生物的活性而被评估。在这里,基于 mastoparan-L 设计了五个 mastoparan 变体,其中两个(R1 和 R4)被选来进行深入分析。Mastoparan-L(亲本/对照)、R1 和 R4 在 2 至 32 μM 的浓度范围内抑制敏感/耐药细菌,而只有 R1 和 R4 在 16 μM 时能消除生物膜。此外,这两种变体极大地降低了 mastoparan-L 对哺乳动物细胞的毒性作用。在皮肤感染中,64 μM 的 R1 是最有效的变体,在感染后第 4 天可将细菌数量减少 1000 倍。在结构上,所有的肽类物质在水相和类膜条件下都表现出不同程度的螺旋和结构稳定性,这可能会影响到这里观察到的不同的生物活性。通过计算上修饰 R1 和 R4 的物理化学性质,我们降低了这些 mastoparan 样肽的细胞毒性,并优化了它们在体外和体内的治疗潜力。

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