首页> 外文期刊>Immunological Investigations: A Journal of Molecular and Cellular Immunology >Differential Gene Expression Profiles Reflecting Macrophage Polarization in Aging and Periodontitis Gingival Tissues
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Differential Gene Expression Profiles Reflecting Macrophage Polarization in Aging and Periodontitis Gingival Tissues

机译:差异基因表达谱反映巨噬细胞极化在衰老和牙周炎牙龈组织中

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摘要

Recent evidence has determined a phenotypic and functional heterogeneity for macrophage populations. This plasticity of macrophage function has been related to specific properties of subsets (M1 and M2) of these cells in inflammation, adaptive immune responses and resolution of tissue destructive processes. This investigation hypothesized that targeted alterations in the distribution of macrophage phenotypes in aged individuals, and with periodontitis would be skewed towards M1 inflammatory macrophages in gingival tissues. The study used a non-human primate model to evaluate gene expression profiles as footprints of macrophage variation in healthy and periodontitis gingival tissues from animals 3-23 years of age and in periodontitis tissues in adult and aged animals. Significant increases in multiple genes reflecting overall increases in macrophage activities were observed in healthy aged tissues, and were significantly increased in periodontitis tissues from both adults and aged animals. Generally, gene expression patterns for M2 macrophages were similar in healthy young, adolescent and adult tissues. However, modest increases were noted in healthy aged tissues, similar to those seen in periodontitis tissues from both age groups. M1 macrophage gene transcription patterns increased significantly over the age range in healthy tissues, with multiple genes (e.g. CCL13, CCL19, CCR7 and TLR4) significantly increased in aged animals. Additionally, gene expression patterns for M1 macrophages were significantly increased in adult health versus periodontitis and aged healthy versus periodontitis. The findings supported a significant increase in macrophages with aging and in periodontitis. The primary increases in both healthy aged tissues and, particularly periodontitis tissues appeared in the M1 phenotype.
机译:最近的证据已经确定了巨噬细胞群体的表型和功能异质性。巨噬细胞功能的这种可塑性与这些细胞在炎症中的亚群(M1和M2)的特定特性,适应性免疫反应以及组织破坏性过程的消退有关。这项研究假设,老年个体和牙周炎中巨噬细胞表型分布的靶向改变会偏向于牙龈组织中的M1炎性巨噬细胞。这项研究使用了非人类的灵长类动物模型来评估基因表达谱,作为健康人和3岁至23岁动物的牙周炎牙龈组织以及成年和成年动物牙周炎组织中巨噬细胞变异的足迹。在健康的老年组织中观察到反映巨噬细胞活性总体增加的多个基因的显着增加,并且在成年和老年动物的牙周炎组织中显着增加。通常,在健康的年轻人,青少年和成人组织中,M2巨噬细胞的基因表达模式相似。但是,在健康的老年组织中注意到适度的增加,这与两个年龄组的牙周炎组织中观察到的相似。在健康组织中,M1巨噬细胞基因转录模式随年龄增长而显着增加,而在老年动物中,多个基因(例如CCL13,CCL19,CCR7和TLR4)显着增加。此外,M1巨噬细胞的基因表达模式在成人健康与牙周炎以及老年健康与牙周炎中显着增加。这些发现支持巨噬细胞随着年龄增长和牙周炎的显着增加。在健康的老年组织中,特别是在牙周炎组织中,M1表型的主要增加。

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