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血清淀粉样蛋白P成分和C反应蛋白通过小鼠Fcγ受体介导吞噬作用。

Serum amyloid P component and C-reactive protein mediate phagocytosis through murine Fc gamma Rs.

作者信息

Mold C, Gresham H D, Du Clos T W

机构信息

Department of Molecular Genetics and Microbiology, Veterans Affairs Medical Center, and Department of Medicine, University of New Mexico, Albuquerque, NM 87131, USA.

出版信息

J Immunol. 2001 Jan 15;166(2):1200-5. doi: 10.4049/jimmunol.166.2.1200.

Abstract

The pentraxins, serum amyloid P component (SAP) and C-reactive protein (CRP) are acute-phase serum proteins in mice and humans, respectively. Although SAP binds to DNA and chromatin and affects clearance of these autoantigens, no specific receptor for SAP has been identified. CRP is an opsonin, and we have shown that it binds to FcgammaR. Mice deficient in FcgammaR were used to assess the role of these receptors in phagocytosis by pentraxins using zymosan as a ligand. Phagocytosis of zymosan by bone marrow macrophages (BMM) was enhanced by opsonization with SAP or CRP. BMM from mice deficient in all three FcgammaR or in gamma-chain ingested unopsonized zymosan, but phagocytosis of SAP- or CRP-opsonized zymosan was not enhanced. SAP binding to BMM from gamma-chain-deficient mice was also greatly reduced, indicating little or no binding of SAP to FcgammaRII. SAP and CRP opsonized zymosan for phagocytosis by BMM from mice deficient in FcgammaRII or FcgammaRIII. SAP, but not CRP, opsonized zymosan for uptake by neutrophils that express only low levels of FcgammaRI. Together these results indicate that FcgammaRI and FcgammaRIII are receptors for SAP in the mouse. Opsonization of zymosan by CRP is mediated through FcgammaRI. Pentraxins are major proteins of the innate immune system and arose earlier in evolution than Igs. The use of FcgammaR by the pentraxins links innate and adaptive immunity and may have important consequences for processing, presentation, and clearance of the self-Ags to which these proteins bind.

摘要

五聚素、血清淀粉样蛋白P成分(SAP)和C反应蛋白(CRP)分别是小鼠和人类的急性期血清蛋白。尽管SAP能与DNA和染色质结合并影响这些自身抗原的清除,但尚未鉴定出SAP的特异性受体。CRP是一种调理素,我们已经证明它能与FcγR结合。利用缺乏FcγR的小鼠,以酵母聚糖作为配体,评估这些受体在五聚素介导的吞噬作用中的作用。用SAP或CRP进行调理可增强骨髓巨噬细胞(BMM)对酵母聚糖的吞噬作用。来自缺乏所有三种FcγR或γ链的小鼠的BMM可摄取未调理的酵母聚糖,但对SAP或CRP调理的酵母聚糖的吞噬作用并未增强。SAP与γ链缺陷小鼠的BMM的结合也大大减少,这表明SAP与FcγRII的结合很少或没有。SAP和CRP可调理酵母聚糖,使其被缺乏FcγRII或FcγRIII的小鼠的BMM吞噬。SAP可调理酵母聚糖,使其被仅表达低水平FcγRI的中性粒细胞摄取,但CRP则不能。这些结果共同表明,FcγRI和FcγRIII是小鼠体内SAP的受体。CRP对酵母聚糖的调理作用是通过FcγRI介导的。五聚素是先天免疫系统的主要蛋白质,在进化上比免疫球蛋白出现得更早。五聚素对FcγR的利用将先天免疫和适应性免疫联系起来,可能对这些蛋白质所结合的自身抗原的加工、呈递和清除产生重要影响。

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