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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Comparison of the membrane interaction mechanism of two antimicrobial RNases: RNase 3/ECP and RNase 7.
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Comparison of the membrane interaction mechanism of two antimicrobial RNases: RNase 3/ECP and RNase 7.

机译:比较两种抗菌RNase:RNase 3 / ECP和RNase 7的膜相互作用机理。

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Eosinophil cationic protein (ECP/RNase 3) and the skin derived ribonuclease 7 (RNase 7) are members of the RNase A superfamily. RNase 3 is mainly expressed in eosinophils whereas RNase 7 is primarily secreted by keratinocytes. Both proteins present a broad-spectrum antimicrobial activity and their bactericidal mechanism is dependent on their membrane destabilizing capacities. Using phospholipid vesicles as membrane models, we have characterized the protein membrane association process. Confocal microscopy experiments using giant unilamellar vesicles illustrate the morphological changes of the liposome population. By labelling both lipid bilayers and proteins we have monitored the kinetic of the process. The differential protein ability to release the liposome aqueous content was evaluated together with the micellation and aggregation processes. A distinct morphology of the protein/lipid aggregates was visualized by transmission electron microscopy and the proteins overall secondary structure in a lipid microenvironment was assessed by FTIR. Interestingly, for both RNases the membrane interaction events take place in a different behaviour and timing: RNase 3 triggers first the vesicle aggregation, while RNase 7 induces leakage well before the aggregation step. Their distinct mechanism of action at the membrane level may reflect different in vivo antipathogen functions.
机译:嗜酸性粒细胞阳离子蛋白(ECP / RNase 3)和皮肤来源的核糖核酸酶7(RNase 7)是RNase A超家族的成员。 RNase 3主要在嗜酸性粒细胞中表达,而RNase 7主要由角质形成细胞分泌。两种蛋白质均具有广谱抗菌活性,其杀菌机理取决于其膜的去稳定能力。使用磷脂囊泡作为膜模型,我们表征了蛋白质膜缔合过程。使用巨型单层囊泡的共聚焦显微镜实验说明了脂质体群体的形态变化。通过标记脂质双层和蛋白质,我们已经监测了该过程的动力学。与胶束化和聚集过程一起评估了蛋白质释放脂质体含水量的差异能力。蛋白质/脂质聚集体的独特形态通过透射电子显微镜观察,并且脂质微环境中蛋白质的总体二级结构通过FTIR评估。有趣的是,对于两种RNase,膜相互作用事件均以不同的行为和时间发生:RNase 3首先触发囊泡聚集,而RNase 7则在聚集步骤之前就引发了渗漏。它们在膜水平上的独特作用机制可能反映了体内抗病原体的不同功能。

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