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A 2H Solid-State NMR Study of Lipid Clustering by Cationic Antimicrobial and Cell-Penetrating Peptides in Model Bacterial Membranes

机译:2 H固态核磁共振研究模型细菌膜中的阳离子抗菌肽和细胞穿透肽的脂质聚集。

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摘要

Domain formation in bacteria-mimetic membranes due to cationic peptide binding was recently proposed based on calorimetric data. We now use 2H solid-state NMR to critically examine the presence and absence of domains in bacterial membranes containing zwitterionic 1-palmitoyl-2-oleoyl-sn-glycero-3-phosphatidylethanolamine (POPE) and anionic 1-palmitoyl-2-oleoyl-sn-glycero-3-phosphatidylglycerol (POPG) lipids. Chain-perdeuterated POPE and POPG are used in single-component membranes, binary POPE/POPG (3:1) membranes, and membranes containing one of four cationic peptides: two antimicrobial peptides (AMPs) of the β-hairpin family of protegrin-1 (PG-1), and two cell-penetrating peptides (CPPs), HIV TAT and penetratin. 2H quadrupolar couplings were measured to determine the motional amplitudes of POPE and POPG acyl chains as a function of temperature. Homogeneously mixed POPE/POPG membranes should give the same quadrupolar couplings for the two lipids, whereas the presence of membrane domains enriched in one of the two lipids should cause distinct 2H quadrupolar couplings that reflect different chain disorder. At physiological temperature (308 K), we observed no or only small coupling differences between POPE and POPG in the presence of any of the cationic peptides. However, around ambient temperature (293 K), at which gel- and liquid-crystalline phases coexist in the peptide-free POPE/POPG membrane, the peptides caused distinct quadrupolar couplings for the two lipids, indicating domain formation. The broad-spectrum antimicrobial peptide PG-1 ordered ∼40% of the POPE lipids while disordering POPG. The Gram-negative selective PG-1 mutant, IB549, caused even larger differences in the POPE and POPG disorder: ∼80% of POPE partitioned into the ordered phase, whereas all of the POPG remained in the disordered phase. In comparison, TAT rigidified POPE and POPG similarly in the binary membrane at ambient temperature, indicating that TAT does not cause dynamic heterogeneity but interacts with the membrane with a different mechanism. Penetratin maintained the POPE order but disordered POPG, suggesting moderate domain separation. These results provide insight into the extent of domain formation in bacterial membranes and the possible peptide structural requirements for this phenomenon.
机译:最近基于量热数据提出了由于阳离子肽结合而在模拟细菌膜中形成的结构域。现在,我们使用 2 H固态NMR严格检查细菌膜中含有两性离子1-棕榈酰基-2-油酰基-sn-甘油-3-磷脂酰乙醇胺(POPE)和阴离子的细菌膜的存在与否1-棕榈酰基-2-油酰基-sn-甘油-3-磷脂酰甘油(POPG)脂质。链式氘代POPE和POPG用于单组分膜,二元POPE / POPG(3:1)膜以及包含四种阳离子肽之一的膜:protegrin-1的β-发夹家族的两种抗菌肽(AMP) (PG-1)和两种穿透细胞的肽(CPP),HIV TAT和渗透肽。测量了 2 H四极偶合,以确定POPE和POPG酰基链的运动幅度随温度的变化。均质混合的POPE / POPG膜应为两种脂质提供相同的四极偶合,而富含两种脂质之一的膜结构域的存在应引起反映不同链紊乱的独特的 2 H四极偶合。在生理温度(308 K)下,我们观察到在存在任何阳离子肽的情况下POPE和POPG之间没有或只有很小的偶联差异。但是,在无肽POPE / POPG膜中凝胶相和液晶相共存的环境温度(293 K)附近,这些肽引起两种脂质的明显四极偶合,表明结构域形成。广谱抗菌肽PG-1在使POPG紊乱的同时订购了约40%的POPE脂质。革兰氏阴性选择性PG-1突变体IB549在POPE和POPG疾病中引起了更大的差异:约80%的POPE分配为有序相,而所有POPG仍处于无序状态。相比之下,TAT在环境温度下类似地使二元膜中的POPE和POPG硬化,表明TAT不会引起动态异质性,但会以不同的机理与膜相互作用。 Penetratin维持POPE秩序,但POPG紊乱,表明中等域分离。这些结果提供了对细菌膜中结构域形成程度的深入了解,以及对该现象可能的肽结构要求。

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