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DPPC 双层结构在包含抗菌阳离子双子表面活性剂时的变化。

Structural Modifications of DPPC Bilayers upon Inclusion of an Antibacterial Cationic Bolaamphiphile.

机构信息

CSGI and Department of Chemistry "Ugo Schiff" , University of Florence , Sesto Fiorentino (FI) 50019 , Italy.

出版信息

Langmuir. 2018 Jul 31;34(30):8952-8961. doi: 10.1021/acs.langmuir.8b01689. Epub 2018 Jul 18.

DOI:10.1021/acs.langmuir.8b01689
PMID:29976066
Abstract

The emergence of antibiotic-resistant bacterial strains has fostered fundamental research to develop alternative antimicrobial strategies. Among the several systems proposed so far, the association complexes (nanoplexes) formed by transcription factor decoys (TFDs), i.e., short oligonucleotides targeting a crucial bacterial transcription factor, and a bolaform cationic amphiphile, 10,10'-(dodecane-1,12-diyl)-bis-(9-amino-1,2,3,4-tetrahydroacridinium) chloride (12-bis-THA), have demonstrated their potential in vitro and in vivo. The application of these nanoplexes is hampered by a scarce colloidal stability, which can be addressed by including the bolaamphiphile in a liposomal carrier, which is then associated to the TFD. The present study reports an investigation on the effects of 12-bis-THA on the structure of synthetic lipid bilayers to assess the morphology of the mixed assemblies, gain insight into the location of the host within the bilayer, and determine the loading capacity of the carrier. Our results demonstrate that 12-bis-THA promptly inserts within 1,2-dipalmitoyl- sn-glycero-3-phosphocholine (DPPC) bilayers, bending its C-12 spacer chain to adopt a conelike shape and shifting the gel-liquid crystalline transition of the chains to lower temperatures. The host liposomal structure is retained for a bolaamphiphile concentration of up to 3.2% mol to DPPC, whereas higher concentrations lead to the destabilization by means of a detergency-like mechanism, with the simultaneous existence of different lamellar-based structures, such as liposomes, bicelles, and rafts, in which DPPC and 12-bis-THA could be present in different molar ratios. Overall, these results shed light on the interaction of the bolaamphiphile with a lipid bilayer and provide valuable insight to better formulate the antimicrobial amphiphile in liposomal carriers to circumvent the colloidal instability of nanoplexes.

摘要

抗生素耐药菌的出现促进了基础研究,以开发替代抗菌策略。迄今为止,已经提出了几种系统,其中转录因子诱饵(TFD)形成的结合复合物(纳米复合物),即针对关键细菌转录因子的短寡核苷酸,和一种棒状阳离子两亲物,10,10'-(十二烷-1,12-二基)-双-(9-氨基-1,2,3,4-四氢吖啶)氯化物(12-双-THA),已在体外和体内证明了它们的潜力。这些纳米复合物的应用受到胶体稳定性差的限制,可以通过将棒状两亲物包含在脂质体载体中来解决,然后将其与 TFD 相关联。本研究报告了对 12-双-THA 对合成脂质双层结构的影响的研究,以评估混合组装体的形态,深入了解宿主在双层中的位置,并确定载体的载药量。我们的结果表明,12-双-THA 立即插入 1,2-二棕榈酰基-sn-甘油-3-磷酸胆碱(DPPC)双层中,弯曲其 C-12 间隔链以采用锥形形状,并将链的凝胶-液晶晶转变移至更低的温度。在高达 3.2%mol DPPC 的两亲物浓度下,宿主脂质体结构得以保留,而更高的浓度则通过类似去污剂的机制导致失稳,同时存在不同的基于层状的结构,例如脂质体、双型胶束和筏,其中 DPPC 和 12-双-THA 可以以不同的摩尔比存在。总体而言,这些结果阐明了两亲物与脂质双层的相互作用,并为更好地在脂质体载体中配制抗菌两亲物以避免纳米复合物的胶体不稳定性提供了有价值的见解。

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