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Lactoferrin: an important host defence against microbial and viral attack

机译:乳铁蛋白:抵抗微生物和病毒攻击的重要宿主防御

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The first function attributed to lactoferrin (Lf), an iron binding protein belonging to the non-immune natural defences, was antimicrobial activity that depended on its capacity to sequester iron. Iron-independent microbicidal activities, requiring direct interaction between this cationic protein and microbial surface components, were later demonstrated. Many other anti-microbial and anti-viral functions have since been ascribed to Lf. In mucosal secretions, iron and Lf modulate the motility and aggregation of pathogenic bacteria. Lf inhibits bacterial adhesion on abiotic surfaces through ionic binding to biomaterials, or specific binding to bacterial structures or both. Lf inhibition of bacterial adhesion to host cells requires Lf binding to bacteria and/or host cells. Lf hinders microbial internalization by binding to both glycosaminoglycans and bacterial proteins which can be degraded by Lf-mediated proteolysis. Moreover, Lf internalisation and localisation to the host cell nuclei could modulate bacterial entry into cells through gene regulation. Finally, the capability of Lf to exert antiviral activity, through its binding to host cells and/or viral particles, strengthens the idea that it is an important brick in the mucosal wall, effective against both microbial and viral attacks.
机译:乳铁蛋白(Lf)是一种属于非免疫自然防御系统的铁结合蛋白,其第一个功能是抗菌活性,这取决于其螯合铁的能力。后来证明了铁独立的杀微生物活性,需要这种阳离子蛋白和微生物表面组分之间的直接相互作用。此后,许多其他的抗微生物和抗病毒功能都归因于Lf。在粘膜分泌物中,铁和Lf调节病原菌的运动和聚集。 Lf通过离子结合生物材料或特异性结合细菌结构或同时抑制两者,抑制细菌在非生物表面上的粘附。 Lf对细菌粘附于宿主细胞的抑制作用要求Lf与细菌和/或宿主细胞结合。 Lf通过与糖胺聚糖和细菌蛋白结合而阻碍微生物内在化,而这些蛋白可以被Lf介导的蛋白水解作用降解。此外,Lf内在化和定位到宿主细胞核可以通过基因调控来调节细菌进入细胞。最后,Lf通过与宿主细胞和/或病毒颗粒结合而发挥抗病毒活性的能力,进一步增强了Lf是粘膜壁上重要的砖块的功效,可有效抵抗微生物和病毒的侵袭。

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