LIPPSO, Department of Chemistry, Campus Montilivi, Universitat de Girona, 17003 Girona, Spain.
Int J Mol Sci. 2024 Mar 19;25(6):3456. doi: 10.3390/ijms25063456.
The linear undecapeptide KKLFKKILKYL-NH (BP100) highlights for its antibacterial activity against Gram-negative bacteria and its low toxicity. These excellent biological properties prompted the investigation of its mechanism of action, which were undertaken using spectroscopic techniques, biophysical analysis, microscopy, and molecular dynamic simulations. Studies were conducted in different membrane environments, such as anionic, zwitterionic, and mixed membranes, as well as in vesicles (LUVs and GUVs) and bacteria. The findings suggest that BP100 exhibits a preference for anionic membranes, and its mechanism of action involves charge neutralization and membrane permeabilization. In these membranes, BP100 transitions from an unstructured state in water to an α-helix with the axis parallel to the surface. MD simulations suggest that after electrostatic interaction with the membrane, BP100 flips, facilitating the insertion of its hydrophobic face into the membrane bilayer. Thus, BP100 adopts an almost vertical transmembrane orientation with lysine side chains snorkelling on both sides of the membrane. As a result of the rotation, BP100 induces membrane thinning and slow lipid diffusion and promotes water penetration, particularly in anionic lipid membranes. These investigations pointed towards a carpet-like mechanism and are aligned with the biological activity profile described for BP100. This review covers all the studies carried out on the mechanism of action of BP100 published between 2009 and 2023.
线性十一肽 KKLFKKILKYL-NH(BP100)因其对革兰氏阴性菌的抗菌活性和低毒性而备受关注。这些优异的生物学特性促使人们研究其作用机制,研究采用了光谱技术、生物物理分析、显微镜和分子动力学模拟等方法。研究在不同的膜环境中进行,如阴离子、两性离子和混合膜,以及囊泡(LUV 和 GUV)和细菌中。研究结果表明,BP100 优先与阴离子膜结合,其作用机制涉及电荷中和和膜通透性。在这些膜中,BP100 从水中的无规卷曲状态转变为与表面平行的α-螺旋。MD 模拟表明,BP100 与膜静电相互作用后会翻转,从而促进其疏水面插入膜双层。因此,BP100 采用几乎垂直于膜的跨膜取向,赖氨酸侧链在膜两侧潜泳。由于旋转,BP100 诱导膜变薄和脂质扩散缓慢,并促进水渗透,特别是在阴离子脂质膜中。这些研究表明了一种类似地毯的机制,与 BP100 描述的生物学活性特征一致。本综述涵盖了 2009 年至 2023 年期间发表的关于 BP100 作用机制的所有研究。
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