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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Quantitative assessment of peptide-lipid interactions. Ubiquitous fluorescence methodologies.
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Quantitative assessment of peptide-lipid interactions. Ubiquitous fluorescence methodologies.

机译:肽-脂质相互作用的定量评估。无处不在的荧光方法。

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Peptide-membrane interactions have been gaining increased relevance, mainly in biomedical investigation, as the potential of the natural, nature-based and synthetic peptides as new drugs or drug candidates also expands. These peptides must face the cell membrane when they interfere with or participate in intracellular processes. Additionally, several peptide drugs and drug leads actions occur at the membrane level (e.g., antimicrobial peptides, cell-penetrating peptides and enveloped viruses membrane fusion inhibitors). Here we explore fluorescence spectroscopy methods that can be used to monitor such interactions. Two main approaches are considered, centered either on the peptide or on the membrane. On the first, we consider mainly the methodologies based on the intrinsic fluorescence of the aminoacid residues tryptophan and tyrosine. Regarding membrane-centric approaches, we review methods based on lipophilic probes sensitive to membrane potentials. The use of fluorescence constitutes a simple and sensitive method to measure these events. Unraveling the molecular mechanisms that govern these interactions can unlock the key to understand specific biological processes involving natural peptides or to optimize the action of a peptide drug.
机译:肽-膜之间的相互作用越来越重要,主要是在生物医学研究中,因为天然,基于自然和合成的肽作为新药或候选药物的潜力也在不断扩大。这些肽在干扰或参与细胞内过程时必须面对细胞膜。另外,几种肽药物和药物前导作用在膜水平上发生(例如,抗菌肽,穿透细胞的肽和包膜病毒膜融合抑制剂)。在这里,我们探讨了可用于监测此类相互作用的荧光光谱方法。考虑了两种主要方法,以肽或膜为中心。首先,我们主要考虑基于氨基酸残基色氨酸和酪氨酸固有荧光的方法。关于以膜为中心的方法,我们回顾了基于对膜电位敏感的亲脂探针的方法。荧光的使用构成了一种简单而灵敏的方法来测量这些事件。阐明控制这些相互作用的分子机制可以解锁理解天然肽的特定生物学过程或优化肽药物作用的关键。

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