首页> 外文期刊>The Journal of investigative dermatology. >GPVI and Thromboxane Receptor on Platelets Promote Proinflammatory Macrophage Phenotypes during Cutaneous Inflammation
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GPVI and Thromboxane Receptor on Platelets Promote Proinflammatory Macrophage Phenotypes during Cutaneous Inflammation

机译:血小板上的GPVI和血栓素受体促进皮肤炎症的促炎巨噬细胞表型

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摘要

Platelets are well known for their role in hemostasis but are also increasingly recognized for their supporting role in innate immune responses. Here, we studied the role of platelets in the development of peripheral inflammation and found that platelets colocalize with macrophages in the inflamed tissue outside of blood vessels in different animal models for cutaneous inflammation. Collagen-treatment of macrophages isolated from paws during zymosan-induced inflammation induced thromboxane synthesis through the platelet expressed collagen receptor glycoprotein VI. Deletion of glycoprotein VI or its downstream effector thromboxane A2 receptor (TP) reduced zymosan-induced mechanical allodynia without altering macrophage recruitment or formation of macrophage/platelet complexes. Instead, macrophages in inflamed paws of glycoprotein VI- and TP-deficient mice exhibited an increased expression of anti-inflammatory markers and synthesized less proinflammatory mediators (prostaglandin E-2 and IL6). TP expression on platelets was necessary to mediate increased prostaglandin E2 and IL6 synthesis, whereas TP expression on macrophages was sufficient to decrease the expression of the anti-inflammatory macrophage marker CD206, showing that TP activation on platelets and macrophages regulates different aspects of macrophage activation.
机译:血小板以其在止血中的作用众所周知,但也越来越普遍认识到它们在先天免疫应答中的支持作用。在这里,我们研究了血小板在外周炎症的发育中的作用,发现血小板在不同动物模型外的血管外的发炎组织中的巨噬细胞中的巨大化。胶原蛋白诱导炎症期间通过血小板表达胶原受体糖蛋白VI诱导从爪子诱导的血红蛋白合成中巨噬细胞分离的巨噬细胞治疗。缩略糖蛋白VI或其下游效应血栓乳蛋白A2受体(TP)降低了酵母菌诱导的机械异常性病,而不改变巨噬细胞募集或形成巨噬细胞/血小板络合物。相反,糖蛋白和TP缺陷小鼠发炎爪中的巨噬细胞表现出抗炎标志物的表达增加,并合成较少的促炎介质(前列腺素E-2和IL6)。血小板上的TP表达是介导增加的前列腺素E2和IL6合成,而在巨噬细胞上的TP表达足以降低抗炎巨噬细胞标志物CD206的表达,表明血小板和巨噬细胞的TP活化调节巨噬细胞激活的不同方面。

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    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Goethe Univ Frankfurt Ctr Neurosci Inst Klin Neuroanat Frankfurt Germany;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Univ Wurzburg Inst Expt Biomed Univ Klinikum Wurzburg Germany;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Fraunhofer Inst Mol Biol &

    Appl Ecol Project Grp Translat Med &

    Pharmacol IME TMP Frankfurt;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Goethe Univ Frankfurt Ctr Neurosci Inst Klin Neuroanat Frankfurt Germany;

    Univ Wurzburg Inst Expt Biomed Univ Klinikum Wurzburg Germany;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

    Klinikum Goethe Univ Frankfurt ZAFES Inst Klin Pharmakol Pharmazentrum Frankfurt Frankfurt;

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  • 正文语种 eng
  • 中图分类 皮肤病学与性病学;
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