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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Interactions of amphipathic alpha-helical MEG proteins from Schistosoma mansoni with membranes
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Interactions of amphipathic alpha-helical MEG proteins from Schistosoma mansoni with membranes

机译:血吸虫曼逊与膜的两性α-螺旋梅格蛋白的相互作用

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Micro Exon Gene (MEG) proteins are thought to play major roles in the infection and survival of parasitic Schistosoma mansoni worms in host organisms. Here, the physical chemical properties of two small MEG proteins found in the genome of S. mansoni, named MEG-24 and MEG-27, were examined by a combination of biophysical techniques such as differential scanning calorimetry, tensiometry, circular dichroism, fluorescence, and electron spin resonance spectroscopies. The proteins are surface active and structurally arranged as cationic amphipathic a-helices that can associate with lipid membranes and cause their disruption. Upon adsorption to lipid membranes, MEG-27 strongly affects the fluidity of erythrocyte ghost membranes, whereas MEG-24 forms pores in erythrocytes without modifying the ghost membrane fluidity. Whole mount in situ hybridization experiments indicates that MEG-27 and MEG-24 transcripts are located in the parasite esophagus and subtegumental cells, respectively, suggesting a relevant role of these proteins in the host-parasite interface. Taken together, these characteristics lead us to propose that these MEG proteins may interact with host cell membranes and potentially modulate the immune process using a similar mechanism as that described for a-helical membrane active peptides.
机译:微外显子基因(MEG)蛋白被认为在宿主生物中寄生血吸虫蠕虫的感染和存活中发挥重大作用。在此,通过差分扫描量热法,张力学,圆形二色性,荧光,荧光,通过生物物理技术的组合来检查在S. Mansoni的基因组中发现的两种小MEG蛋白的物理化学性质。和电子自旋共振光谱。蛋白质是活性的,并且结构地布置为阳离子两亲的A螺旋,其可以与脂质膜相关联并引起它们的破坏。在对脂质膜的吸附后,MEG-27强烈影响红细胞鬼膜的流动性,而MEG-24在红细胞中形成孔而不改变鬼膜流动性。在原位杂交实验中整体安装表明MEG-27和MEG-24转录物分别位于寄生虫食道和副表团中,表明这些蛋白质在寄生虫界面中的相关作用。在一起,这些特性引导我们提出这些MEG蛋白可以与宿主细胞膜相互作用,并使用与α-螺旋膜活性肽描述的类似机制来调节免疫过程。

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