髓系细胞中甲酰肽受体 2 型缺乏会加重败血症诱发的心脏功能障碍

IF 4.7 3区 医学 Q2 IMMUNOLOGY
Journal of Innate Immunity Pub Date : 2023-01-01 Epub Date: 2023-04-17 DOI:10.1159/000530284
Jianmin Chen, Shani Austin-Williams, Caroline Elizabeth O'Riordan, Pol Claria-Ribas, Michelle A Sugimoto, Lucy V Norling, Christoph Thiemermann, Mauro Perretti
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引用次数: 0

摘要

我们利用全局性甲酰肽受体(Fpr)2基因敲除小鼠群,报道了这种促进溶解的受体在多微生物败血症中的调节特性。hFPR2 小鼠和骨髓细胞特异性 hFPR2 KO(KO)小鼠接受了盲肠结扎和穿刺(CLP)诱导的多微生物败血症。与 hFPR2 小鼠相比,CLP 加剧了 KO 小鼠的心脏功能障碍(通过超声心动图评估),恶化了临床结果,并损害了细菌清除。与这种病理情况同时出现的是,KO 小鼠心脏内促炎性单核细胞招募增加,M2 样巨噬细胞减少。在 KO 小鼠的腹腔渗出液中,我们发现中性粒细胞和 MHC II+ 巨噬细胞数量增加,但单核细胞/巨噬细胞和 MHC II- 巨噬细胞招募减少。给予 FPR2 激动剂附件素 A1(AnxA1)可改善 hFPR2 败血症小鼠的心脏功能,但对 KO 小鼠的益处有限,因为 FPR2 配体未能使巨噬细胞极化为 MHC II 表型。总之,髓系细胞中的 FPR2 缺乏会加重心脏功能障碍,并恶化多微生物败血症的临床预后。AnxA1 对心脏功能和宿主免疫反应的改善在 hFPR2 正常的脓毒症小鼠中更为有效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Formyl Peptide Receptor Type 2 Deficiency in Myeloid Cells Amplifies Sepsis-Induced Cardiac Dysfunction.

Formyl Peptide Receptor Type 2 Deficiency in Myeloid Cells Amplifies Sepsis-Induced Cardiac Dysfunction.

Formyl Peptide Receptor Type 2 Deficiency in Myeloid Cells Amplifies Sepsis-Induced Cardiac Dysfunction.

Formyl Peptide Receptor Type 2 Deficiency in Myeloid Cells Amplifies Sepsis-Induced Cardiac Dysfunction.

Using a global formyl peptide receptor (Fpr) 2 knockout mouse colony, we have reported the modulatory properties of this pro-resolving receptor in polymicrobial sepsis. Herein, we have used a humanized FPR2 (hFPR2) mouse colony, bearing an intact or a selective receptor deficiency in myeloid cells to dwell on the cellular mechanisms. hFPR2 mice and myeloid cell-specific hFPR2 KO (KO) mice were subjected to cecal ligation and puncture (CLP)-induced polymicrobial sepsis. Compared with hFPR2 mice, CLP caused exacerbated cardiac dysfunction (assessed by echocardiography), worsened clinical outcome, and impaired bacterial clearance in KO mice. This pathological scenario was paralleled by increased recruitment of pro-inflammatory monocytes and reduced M2-like macrophages within the KO hearts. In peritoneal exudates of KO mice, we quantified increased neutrophil and MHC II+ macrophage numbers but decreased monocyte/macrophage and MHC II- macrophage recruitment. hFPR2 upregulation was absent in myeloid cells, and local production of lipoxin A4 was reduced in septic KO mice. Administration of the FPR2 agonist annexin A1 (AnxA1) improved cardiac function in hFPR2 septic mice but had limited beneficial effects in KO mice, in which the FPR2 ligand failed to polarize macrophages toward an MHC II- phenotype. In conclusion, FPR2 deficiency in myeloid cells exacerbates cardiac dysfunction and worsens clinical outcome in polymicrobial sepsis. The improvement of cardiac function and the host immune response by AnxA1 is more effective in hFPR2-competent septic mice.

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来源期刊
Journal of Innate Immunity
Journal of Innate Immunity 医学-免疫学
CiteScore
10.50
自引率
1.90%
发文量
35
审稿时长
7.5 months
期刊介绍: The ''Journal of Innate Immunity'' is a bimonthly journal covering all aspects within the area of innate immunity, including evolution of the immune system, molecular biology of cells involved in innate immunity, pattern recognition and signals of ‘danger’, microbial corruption, host response and inflammation, mucosal immunity, complement and coagulation, sepsis and septic shock, molecular genomics, and development of immunotherapies. The journal publishes original research articles, short communications, reviews, commentaries and letters to the editors. In addition to regular papers, some issues feature a special section with a thematic focus.
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