人椎间盘退变中巨噬细胞表型的积累和定位。
Accumulation and localization of macrophage phenotypes with human intervertebral disc degeneration.
机构信息
Leni and Peter W. May Department of Orthopaedics, Icahn School of Medicine at Mount Sinai, 1 Gustave Levy Place, Box 1188, New York, NY 10029-6574, USA.
Spine Research Institute, Department of Biomedical Engineering, The Ohio State University, 140 Baker Systems Engineering, 1971 Neil Ave, Columbus, OH 43210, USA.
出版信息
Spine J. 2018 Feb;18(2):343-356. doi: 10.1016/j.spinee.2017.09.018. Epub 2017 Oct 12.
BACKGROUND CONTEXT
Chronic inflammation is an important component of intervertebral disc (IVD) degeneration, but there is limited knowledge about the identity and source of inflammatory cells involved with the degenerative processes. Macrophages can exhibit multiple phenotypes and are known inflammatory regulators in many tissues, but their phenotypes have not been characterized in IVD degeneration.
PURPOSE
We aimed to characterize accumulation and localization of macrophages in IVD degeneration.
STUDY DESIGN/SETTING: This is an exploratory study to characterize macrophage phenotypes in human cadaver IVDs and the effects of injury and degeneration using multiple immunohistochemistry methods.
OUTCOME MEASURES
Percent positivity of immunohistochemical markers specific for CCR7, CD163, and CD206, and qualitative assessments of dual immunofluorescence and immunostaining localization were the outcome measures.
METHODS
Macrophages were identified in human cadaveric IVDs with immunohistochemistry using cell surface markers CCR7, CD163, and CD206, which are associated with proinflammatory M1, remodeling M2c, and anti-inflammatory M2a phenotypes, respectively. Variations in the accumulation and localization of macrophage markers with degenerative grade across subjects and within donors are described.
RESULTS
Cells expressing all three macrophage markers were found in all degenerative IVDs, but not in the healthiest IVDs. Cells expressing CCR7 and CD163, but not CD206, significantly increased with degenerative grade. Many cells also co-expressed multiple macrophage markers. Across all degenerative grades, CCR7+ and CD163+ were significantly more present in unhealthy nucleus pulposus (NP), annulus fibrosus (AF), and end plate (EP) regions exhibiting structural irregularities and defects. Positively stained cells in the NP and AF closely resembled resident IVD cells, suggesting that IVD cells can express macrophage cell surface markers. In the EP, there were increasing trends of positively stained cells with atypical morphology and distribution, suggesting a source for exogenous macrophage infiltration into the IVD.
CONCLUSIONS
Chronic inflammatory conditions of IVD degeneration appear to involve macrophages or macrophage-like cells, as expression of multiple macrophage markers increased with degeneration, especially around unhealthy regions with defects and the EP. Knowledge of macrophage phenotypes and their localization better elucidates the complex injury and repair processes in IVDs and may eventually lead to novel treatments.
背景
慢性炎症是椎间盘(IVD)退变的一个重要组成部分,但对于参与退变过程的炎症细胞的身份和来源知之甚少。巨噬细胞可以表现出多种表型,并且是许多组织中已知的炎症调节剂,但它们的表型尚未在 IVD 退变中得到描述。
目的
我们旨在描述 IVD 退变中巨噬细胞的积累和定位。
研究设计/设置:这是一项探索性研究,旨在使用多种免疫组织化学方法描述人尸检 IVD 中巨噬细胞表型以及损伤和退变的影响。
观察指标
CCR7、CD163 和 CD206 的免疫组织化学标志物的阳性百分比,以及双免疫荧光和免疫染色定位的定性评估是观察指标。
方法
使用细胞表面标志物 CCR7、CD163 和 CD206 对人尸检 IVD 中的巨噬细胞进行免疫组织化学鉴定,这些标志物分别与促炎 M1、重塑 M2c 和抗炎 M2a 表型相关。描述了在不同个体和同一供体中,随着退行性分级的变化,巨噬细胞标志物的积累和定位的变化。
结果
在所有退行性 IVD 中都发现了表达所有三种巨噬细胞标志物的细胞,但在最健康的 IVD 中没有发现。表达 CCR7 和 CD163 的细胞,但不表达 CD206 的细胞,随着退行性分级的增加而显著增加。许多细胞也同时表达多种巨噬细胞标志物。在所有退行性分级中,CCR7+和 CD163+在结构不规则和缺陷的不健康核髓核(NP)、纤维环(AF)和终板(EP)区域中明显更为存在。NP 和 AF 中染色阳性的细胞与常驻 IVD 细胞非常相似,表明 IVD 细胞可以表达巨噬细胞细胞表面标志物。在 EP 中,随着具有非典型形态和分布的染色阳性细胞的增加趋势,提示外源性巨噬细胞浸润到 IVD 的来源。
结论
IVD 退变的慢性炎症状态似乎涉及巨噬细胞或巨噬细胞样细胞,因为随着退变的发生,多种巨噬细胞标志物的表达增加,尤其是在有缺陷和 EP 的不健康区域周围。对巨噬细胞表型及其定位的了解可以更好地阐明 IVD 中的复杂损伤和修复过程,并最终导致新的治疗方法。
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