Beatriz T Magalhães, João T S Coimbra, Raquel M Silva, Mariana Ferreira, Rita S Santos, Paula Gameiro, Nuno F Azevedo, Pedro A Fernandes
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The NAM sequences were composed of locked nucleic acid (LNA) and 2'-O-methyl (2'-OMe) residues, whereas the membrane models were composed of 1-palmitoyl-2-oleoyl-glycero-3-phosphocholine (POPC) or 1-palmitoyl-2-oleoyl-<i>sn</i>-glycero-3-phospho-(1'-rac-glycerol) (POPG) phospholipids. The parametrization protocol followed was validated against literature data and demonstrated the reliability of our approach for simulating NAM sequences. Investigation into the interaction of the sequences with zwitterionic and anionic membranes revealed a preference for hydrogen bond formation with the anionic model over the zwitterionic one. Additionally, potential of mean force (PMF) calculations unveiled a lower free energy barrier for translocation across the zwitterionic bilayer model. Contrarily, the partition constants derived suggested a slightly higher partitioning within the anionic membrane, emphasizing a nuanced interplay of factors. Finally, spectroscopic partition measurements with liposomes presented challenges in quantifying the partition of NAMs due to minimal signal variations. However, a tendency for quenching in anionic vesicles suggested a potential, albeit small, partitioning effect that warrants further investigation. 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引用次数: 0
摘要
核酸模拟物(NAMs)作为抗菌药物具有很大的潜力。然而,很少有研究对其在细菌包膜上的扩散进行评估。在这项工作中,我们利用分子动力学(MD)模拟研究了 NAMs 在模拟细菌外膜的脂质双分子层系统中的扩散情况。此外,我们还研究了 NAM 序列与脂膜的相互作用,并通过 MD 和光谱研究确定了分配常数 (Kp)。NAM序列由锁定核酸(LNA)和2'-O-甲基(2'-OMe)残基组成,而膜模型则由1-棕榈酰-2-油酰-甘油-3-磷酸胆碱(POPC)或1-棕榈酰-2-油酰-sn-甘油-3-磷酸-(1'-rac-甘油)(POPG)磷脂组成。所采用的参数化协议与文献数据进行了验证,证明了我们模拟 NAM 序列方法的可靠性。对序列与齐聚物膜和阴离子膜相互作用的研究表明,与阴离子模型相比,我们更倾向于与齐聚物膜形成氢键。此外,平均力势(PMF)计算揭示了穿过齐聚物双分子层模型的较低自由能障。相反,得出的分配常数表明阴离子膜内的分配率略高,这强调了各种因素之间微妙的相互作用。最后,由于信号变化极小,利用脂质体进行的分光测量在量化 NAM 的分配方面面临挑战。不过,阴离子囊泡中的淬灭趋势表明存在潜在的分区效应,尽管这种效应很小,但值得进一步研究。总之,我们的研究揭示了 NAM 原则上无法通过被动扩散穿过完整的细菌外膜。
Crosstalk of Nucleic Acid Mimics with Lipid Membranes: A Multifaceted Computational and Experimental Study.
Nucleic acid mimics (NAMs) have demonstrated high potential as antibacterial drugs. However, very few studies have assessed their possible diffusion across the bacterial envelope. In this work, we studied NAMs' diffusion in lipid bilayer systems that mimic the bacterial outer membrane using molecular dynamics (MD) simulations. Additionally, we examined the interactions of a NAM sequence with lipid membranes and ascertained the partition constants (Kp) through MD and spectroscopic investigations. The NAM sequences were composed of locked nucleic acid (LNA) and 2'-O-methyl (2'-OMe) residues, whereas the membrane models were composed of 1-palmitoyl-2-oleoyl-glycero-3-phosphocholine (POPC) or 1-palmitoyl-2-oleoyl-sn-glycero-3-phospho-(1'-rac-glycerol) (POPG) phospholipids. The parametrization protocol followed was validated against literature data and demonstrated the reliability of our approach for simulating NAM sequences. Investigation into the interaction of the sequences with zwitterionic and anionic membranes revealed a preference for hydrogen bond formation with the anionic model over the zwitterionic one. Additionally, potential of mean force (PMF) calculations unveiled a lower free energy barrier for translocation across the zwitterionic bilayer model. Contrarily, the partition constants derived suggested a slightly higher partitioning within the anionic membrane, emphasizing a nuanced interplay of factors. Finally, spectroscopic partition measurements with liposomes presented challenges in quantifying the partition of NAMs due to minimal signal variations. However, a tendency for quenching in anionic vesicles suggested a potential, albeit small, partitioning effect that warrants further investigation. In summary, our study revealed that NAMs will not, in principle, be able to cross an intact bacterial outer membrane by passive diffusion.
期刊介绍:
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