首页> 美国卫生研究院文献>Elsevier Sponsored Documents >The adult murine heart has a sparse phagocytically active macrophage population that expands through monocyte recruitment and adopts an ‘M2’ phenotype in response to Th2 immunologic challenge
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The adult murine heart has a sparse phagocytically active macrophage population that expands through monocyte recruitment and adopts an ‘M2’ phenotype in response to Th2 immunologic challenge

机译:成年鼠心脏具有稀疏的具有吞噬功能的巨噬细胞可通过募集单核细胞而扩展并针对Th2免疫学挑战采取 M2表型

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摘要

Tissue resident macrophages have vital homeostatic roles in many tissues but their roles are less well defined in the heart. The present study aimed to identify the density, polarisation status and distribution of macrophages in the healthy murine heart and to investigate their ability to respond to immune challenge. Histological analysis of hearts from CSF-1 receptor (csf1-GFP; MacGreen) and CX3CR1 (Cx3cr1GFP/+>) reporter mice revealed a sparse population of GFP positive macrophages that were evenly distributed throughout the left and right ventricular free walls and septum. F4/80+CD11b+ cardiac macrophages, sorted from myocardial homogenates, were able to phagocytose fluorescent beads in vitro and expressed markers typical of both ‘M1’ (IL-1β, TNF and CCR2) and ‘M2’ activation (Ym1, Arg 1, RELMα and IL-10), suggesting no specific polarisation in healthy myocardium. Exposure to Th2 challenge by infection of mice with helminth parasites Schistosoma mansoni, or Heligmosomoides polygyrus, resulted in an increase in cardiac macrophage density, adoption of a stellate morphology and increased expression of Ym1, RELMα and CD206 (mannose receptor), indicative of ‘M2’ polarisation. This was dependent on recruitment of Ly6ChighCCR2+ monocytes and was accompanied by an increase in collagen content.In conclusion, in the healthy heart resident macrophages are relatively sparse and have a phagocytic role. Following Th2 challenge this population expands due to monocyte recruitment and adopts an ‘M2’ phenotype associated with increased tissue fibrosis.
机译:驻留在组织中的巨噬细胞在许多组织中具有重要的稳态作用,但在心脏中它们的作用尚不明确。本研究旨在确定健康鼠心脏中巨噬细胞的密度,极化状态和分布,并研究它们对免疫攻击作出反应的能力。来自CSF-1受体(csf1-GFP; MacGreen)和CX3CR1(Cx3cr1 GFP / + >)记者小鼠心脏的组织学分析显示,GFP阳性巨噬细胞数量稀少。均匀分布在左右心室的游离壁和隔膜。从心肌匀浆中分选出来的F4 / 80 + CD11b +心脏巨噬细胞能够在体外吞噬荧光珠并表达“ M1”(IL-1β,TNF和CCR2)和“ M2”激活(Ym1,Arg 1, RELMα和IL-10),表明健康心肌中无特异性极化。感染蠕虫寄生虫曼氏血吸虫或Heligmosomoides polygyrus的小鼠暴露于Th2攻击,导致心脏巨噬细胞密度增加,星状形态的出现以及Ym1,RELMα和CD206(甘露糖受体)的表达增加,表示为'M2极化。这依赖于Ly6ChighCCR2 +单核细胞的募集,并伴随着胶原蛋白含量的增加。总之,在健康心脏中,驻留的巨噬细胞相对稀疏并具有吞噬作用。 Th2攻击后,该人群由于单核细胞募集而扩大,并采用与组织纤维化增加相关的“ M2”表型。

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