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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Membrane activity of the pentaene macrolide didehydroroflamycoin in model lipid bilayers
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Membrane activity of the pentaene macrolide didehydroroflamycoin in model lipid bilayers

机译:戊烯类大环内酯二氢双氢弗拉霉素在模型脂质双层中的膜活性

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Didehydroroflamycoin (DDHR), a recently isolated member of the polyene macrolide family, was shown to have antibacterial and antifungal activity. However, its mechanism of action has not been investigated. Antibiotics from this family are amphiphilic; thus, they have membrane activity, their biological action is localized in the membrane, and the membrane composition and physical properties facilitate the recognition of a particular compound by the target organism. In this work, we use model lipid membranes comprised of giant unilamellar vesicles (GUVs) for a systematic study of the action of DDHR. In parallel, experiments are conducted using filipin III and amphotericin B, other members of the family, and the behavior observed for DDHR is described in the context of that of these two heavily studied compounds. The study shows that DDHR disrupts membranes via two different mechanisms and that the involvement of these mechanisms depends on the presence of cholesterol. The leakage assays performed in GUVs and the conductance measurements using black lipid membranes (BLM) reveal that the pores that develop in the absence of cholesterol are transient and their size is dependent on the DDHR concentration. In contrast, cholesterol promotes the formation of more defined structures that are temporally stable. (C) 2014 Elsevier B.V. All rights reserved.
机译:Didehydroroflamycoin(DDHR)是多烯大环内酯家族最近分离的成员,被证明具有抗菌和抗真菌活性。但是,尚未研究其作用机理。这个家族的抗生素是两亲的。因此,它们具有膜活性,其生物作用位于膜中,并且膜的组成和物理性质有助于靶标生物识别特定化合物。在这项工作中,我们使用由巨大的单层囊泡(GUV)组成的模型脂质膜对DDHR的作用进行系统研究。同时,使用该家族的其他成员菲利普汀III和两性霉素B进行了实验,在这两个经过大量研究的化合物的背景下描述了DDHR的行为。研究表明,DDHR通过两种不同的机制破坏膜,而这些机制的参与取决于胆固醇的存在。在GUV中进行的泄漏测定和使用黑色脂质膜(BLM)进行的电导测量显示,在没有胆固醇的情况下形成的孔是瞬时的,其大小取决于DDHR浓度。相比之下,胆固醇会促进在时间上更稳定的结构的形成。 (C)2014 Elsevier B.V.保留所有权利。

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