M-CSF 依赖性单核细胞衍生的人类巨噬细胞中的 TLR7 激活可增强炎症反应并促进中性粒细胞的招募。

IF 4.7 3区 医学 Q2 IMMUNOLOGY
Journal of Innate Immunity Pub Date : 2023-01-01 Epub Date: 2023-04-11 DOI:10.1159/000530249
Miriam Simón-Fuentes, Cristina Herrero, Lucia Acero-Riaguas, Concha Nieto, Fatima Lasala, Nuria Labiod, Joanna Luczkowiak, Bárbara Alonso, Rafael Delgado, Maria Colmenares, Ángel L Corbí, Ángeles Domínguez-Soto
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引用次数: 0

摘要

Toll 样受体 7(TLR7)是一种内泌体病原体相关分子模式(PAMP)受体,它能感知单链 RNA(ssRNA),当病毒暴露于 TLR7 时,TLR7 会产生 I 型 IFN 和促炎细胞因子。最近的遗传学研究证实,TLR7 启动的信号传导功能失调与炎症反应的发生直接相关。我们有证据表明,在 M-CSF (M-MØ)存在的情况下,单核细胞衍生的巨噬细胞会优先表达 TLR7。我们现在证明,M-MØ 中的 TLR7 激活会引发微弱的 MAPK、NFκB 和 STAT1 激活,并导致 I 型 IFN 的低产。值得注意的是,TLR7 的参与将 MAFB+ M-MØ 重新编程为亲炎性转录谱,其特征是中性粒细胞吸引趋化因子(CXCL1-3、CXCL5、CXCL8)的表达,而这些趋化因子的表达依赖于转录因子 MAFB 和 AhR。此外,TLR7 激活的 M-MØ 表现出更强的促炎反应,并在二次刺激时产生更强的中性粒细胞吸引趋化因子。由于 TLR7 信号传导异常和肺中性粒细胞/淋巴细胞比率升高与病毒诱导的炎症反应解决能力受损有关,这些结果表明,针对巨噬细胞 TLR7 可能是病毒感染的一种治疗策略,在病毒感染中,单核细胞衍生的巨噬细胞表现出致病作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

TLR7 Activation in M-CSF-Dependent Monocyte-Derived Human Macrophages Potentiates Inflammatory Responses and Prompts Neutrophil Recruitment.

TLR7 Activation in M-CSF-Dependent Monocyte-Derived Human Macrophages Potentiates Inflammatory Responses and Prompts Neutrophil Recruitment.

TLR7 Activation in M-CSF-Dependent Monocyte-Derived Human Macrophages Potentiates Inflammatory Responses and Prompts Neutrophil Recruitment.

TLR7 Activation in M-CSF-Dependent Monocyte-Derived Human Macrophages Potentiates Inflammatory Responses and Prompts Neutrophil Recruitment.

Toll-like receptor 7 (TLR7) is an endosomal pathogen-associated molecular pattern (PAMP) receptor that senses single-stranded RNA (ssRNA) and whose engagement results in the production of type I IFN and pro-inflammatory cytokines upon viral exposure. Recent genetic studies have established that a dysfunctional TLR7-initiated signaling is directly linked to the development of inflammatory responses. We present evidence that TLR7 is preferentially expressed by monocyte-derived macrophages generated in the presence of M-CSF (M-MØ). We now show that TLR7 activation in M-MØ triggers a weak MAPK, NFκB, and STAT1 activation and results in low production of type I IFN. Of note, TLR7 engagement reprograms MAFB+ M-MØ towards a pro-inflammatory transcriptional profile characterized by the expression of neutrophil-attracting chemokines (CXCL1-3, CXCL5, CXCL8), whose expression is dependent on the transcription factors MAFB and AhR. Moreover, TLR7-activated M-MØ display enhanced pro-inflammatory responses and a stronger production of neutrophil-attracting chemokines upon secondary stimulation. As aberrant TLR7 signaling and enhanced pulmonary neutrophil/lymphocyte ratio associate with impaired resolution of virus-induced inflammatory responses, these results suggest that targeting macrophage TLR7 might be a therapeutic strategy for viral infections where monocyte-derived macrophages exhibit a pathogenic role.

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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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