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Peptide-membrane interactions of arginine-tryptophan peptides probed using quartz crystal microbalance with dissipation monitoring.

机译:使用耗散监测的石英晶体微量天平探测精氨酸-色氨酸肽的肽膜相互作用。

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摘要

Membrane-active peptides include peptides that can cross cellular membranes and deliver macromolecular cargo as well as peptides that inhibit bacterial growth. Some of these peptides can act as both transporters and antibacterial agents. It is desirable to combine the knowledge from these two different fields of membrane-active peptides into design of new peptides with tailored actions, as transporters of cargo or as antibacterial substances, targeting specific membranes. We have previously shown that the position of the amino acid tryptophan in the peptide sequence of three arginine-tryptophan peptides affects their uptake and intracellular localization in live mammalian cells, as well as their ability to inhibit bacterial growth. Here, we use quartz crystal microbalance with dissipation monitoring to assess the induced changes caused by binding of the three peptides to supported model membranes composed of POPC, POPC/POPG, POPC/POPG/cholesterol or POPC/lactosyl PE. Our results indicate that the tryptophan position in the peptide sequence affects the way these peptides interact with the different model membranes and that the presence of cholesterol in particular seems to affect the membrane interaction of the peptide with an even distribution of tryptophans in the peptide sequence. These results give mechanistic insight into the function of these peptides and may aid in the design of membrane-active peptides with specified cellular targets and actions.
机译:膜活性肽包括可以穿过细胞膜并传递大分子货物的肽,以及抑制细菌生长的肽。这些肽中的一些可以同时充当转运蛋白和抗菌剂。期望将来自膜活性肽的这两个不同领域的知识结合到具有定制作用的新肽的设计中,所述新肽具有靶向特定膜的作为货物的转运物或作为抗菌物质的作用。我们以前已经表明,氨基酸精氨酸在三个精氨酸-色氨酸肽的肽序列中的位置会影响它们在活哺乳动物细胞中的摄取和细胞内定位,以及它们抑制细菌生长的能力。在这里,我们使用带有耗散监测的石英晶体微量天平来评估由三种肽结合到支持的模型膜(由POPC,POPC / POPG,POPC / POPG /胆固醇或POPC /乳糖基PE组成)引起的诱导变化。我们的结果表明,肽序列中色氨酸的位置会影响这些肽与不同模型膜相互作用的方式,尤其是胆固醇的存在似乎会影响色氨酸在肽序列中均匀分布的膜的相互作用。这些结果使人们对这些肽的功能有了机械的认识,并可能有助于设计具有特定细胞靶标和作用的膜活性肽。

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