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首页> 外文OA文献 >Surfactant Protein A (SP-A)-mediated Clearance of Staphylococcus aureus Involves Binding of SP-A to the Staphylococcal Adhesin Eap and the Macrophage Receptors SP-A Receptor 210 and Scavenger Receptor Class A*
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Surfactant Protein A (SP-A)-mediated Clearance of Staphylococcus aureus Involves Binding of SP-A to the Staphylococcal Adhesin Eap and the Macrophage Receptors SP-A Receptor 210 and Scavenger Receptor Class A*

机译:表面活性剂蛋白A(SP-A)介导的金黄色葡萄球菌清除涉及SP-A与葡萄球菌粘附素Eap和巨噬细胞受体SP-A受体210和清道夫受体A类的结合*

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Staphylococcus aureus causes life-threatening pneumonia in hospitals and deadly superinfection during viral influenza. The current study investigated the role of surfactant protein A (SP-A) in opsonization and clearance of S. aureus. Previous studies showed that SP-A mediates phagocytosis via the SP-A receptor 210 (SP-R210). Here, we show that SP-R210 mediates binding and control of SP-A-opsonized S. aureus by macrophages. We determined that SP-A binds S. aureus through the extracellular adhesin Eap. Consequently, SP-A enhanced macrophage uptake of Eap-expressing (Eap+) but not Eap-deficient (Eap−) S. aureus. In a reciprocal fashion, SP-A failed to enhance uptake of Eap+ S. aureus in peritoneal Raw264.7 macrophages with a dominant negative mutation (SP-R210(DN)) blocking surface expression of SP-R210. Accordingly, WT mice cleared infection with Eap+ but succumbed to sublethal infection with Eap- S. aureus. However, SP-R210(DN) cells compensated by increasing non-opsonic phagocytosis of Eap+ S. aureus via the scavenger receptor scavenger receptor class A (SR-A), while non-opsonic uptake of Eap− S. aureus was impaired. Macrophages express two isoforms: SP-R210L and SP-R210S. The results show that WT alveolar macrophages are distinguished by expression of SP-R210L, whereas SR-A−/− alveolar macrophages are deficient in SP-R210L expressing only SP-R210S. Accordingly, SR-A−/− mice were highly susceptible to both Eap+ and Eap− S. aureus. The lungs of susceptible mice generated abnormal inflammatory responses that were associated with impaired killing and persistence of S. aureus infection in the lung. In conclusion, alveolar macrophage SP-R210L mediates recognition and killing of SP-A-opsonized S. aureus in vivo, coordinating inflammatory responses and resolution of S. aureus pneumonia through interaction with SR-A.
机译:金黄色葡萄球菌在医院引起致命的肺炎,在病毒性流感期间导致致命的超级感染。当前的研究调查了表面活性剂蛋白A(SP-A)在金黄色葡萄球菌的调理作用和清除中的作用。先前的研究表明,SP-A通过SP-A受体210(SP-R210)介导吞噬作用。在这里,我们显示SP-R210通过巨噬细胞介导SP-A调理的金黄色葡萄球菌的结合和控制。我们确定SP-A通过细胞外粘附素Eap结合金黄色葡萄球菌。因此,SP-A增强了表达Eap(Eap +)的巨噬细胞的摄取,但不增强Eap缺乏(Eap-)金黄色葡萄球菌的摄取。以对等的方式,SP-A未能增强具有显性负突变(SP-R210(DN))的腹膜Raw264.7巨噬细胞对Eap +金黄色葡萄球菌的吸收,从而阻断了SP-R210的表面表达。因此,野生型小鼠清除了Eap +的感染,但因金黄色葡萄球菌而致死。但是,SP-R210(DN)细胞通过清除剂受体清道夫受体A类(SR-A)增强了Eap +金黄色葡萄球菌的非调理吞噬作用,从而得到了补偿,而Eap- S.金黄色葡萄球菌的非调理吸收受到了损害。巨噬细胞表达两种同工型:SP-R210L和SP-R210S。结果表明,WT肺泡巨噬细胞通过SP-R210L的表达来区分,而SR-A-/-肺泡巨噬细胞在仅表达SP-R210S的SP-R210L中缺乏。因此,SR-A-/-小鼠对Eap +和Eap-S金黄色葡萄球菌都高度敏感。易感小鼠的肺部产生异常的炎症反应,这与杀伤力和金黄色葡萄球菌感染在肺部的持续存在有关。总之,肺泡巨噬细胞SP-R210L在体内介导SP-A调理的金黄色葡萄球菌的识别和杀伤,通过与SR-A相互作用来协调炎症反应和金黄色葡萄球菌肺炎的消退。

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