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趋化因子配体5机制在啮齿动物视网膜中的组成型和应激诱导表达

Constitutive and Stress-induced Expression of CCL5 Machinery in Rodent Retina.

作者信息

Duncan D'Anne S, McLaughlin William M, Vasilakes Noah, Echevarria Franklin D, Formichella Cathryn R, Sappington Rebecca M

机构信息

Department of Ophthalmology and Visual Sciences, Vanderbilt Eye Institute, Vanderbilt University Medical Center, USA.

Neuroscience Graduate Program, Vanderbilt University, USA.

出版信息

J Clin Cell Immunol. 2017 Jun;8(3). doi: 10.4172/2155-9899.1000506. Epub 2017 May 24.

DOI:10.4172/2155-9899.1000506
PMID:28936366
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5604884/
Abstract

Signaling by inflammatory cytokines and chemokines is associated with neurodegeneration in disease and injury. Here we examined expression of the β-chemokine CCL5 and its receptors in the mouse retina and evaluated its relevance in glaucoma, a common optic neuropathy associated with sensitivity to intraocular pressure (IOP). Using quantitative PCR, fluorescent hybridization, immunohistochemistry and quantitative image analysis, we found CCL5 mRNA and protein was constitutively expressed in the inner retina and synaptic layers. CCL5 appeared to associate with Müller cells and RGCs as well as synaptic connections between horizontal cells and bipolar cells in the OPL and amacrine cells, bipolar cells and RGCs in the IPL. Although all three high-affinity receptors (CCR5, CCR3, CCR1) for CCL5 were expressed constitutively, CCR5 expression was significantly higher than CCR3, which was also markedly greater than CCR1. Localization patterns for constitutive CCR5, CCR3 and CCR1 expression differed, particularly with respect to expression in inner retinal neurons. Stress-related expression of CCL5 was primarily altered in aged DBA/2 mice with elevated IOP. In contrast, changes in expression and localization of both CCR3 and CCR5 were evident not only in aged DBA/2 mice, but also in age-matched control mice and young DBA/2 mice. These groups do not exhibit elevated IOP, but possess either the aging stress (control mice) or the genetic predisposition to glaucoma (DBA/2 mice). Together, these data indicate that CCL5 and its high-affinity receptors are constitutively expressed in murine retina and differentially induced by stressors associated with glaucomatous optic neuropathy. Localization patterns further indicate that CCL5 signaling may be relevant for modulation of synapses in both health and disease, particularly in the inner plexiform layer.

摘要

炎症细胞因子和趋化因子的信号传导与疾病和损伤中的神经退行性变有关。在此,我们检测了β趋化因子CCL5及其受体在小鼠视网膜中的表达,并评估了其在青光眼(一种与眼内压(IOP)敏感性相关的常见视神经病变)中的相关性。通过定量PCR、荧光杂交、免疫组织化学和定量图像分析,我们发现CCL5 mRNA和蛋白在内层视网膜和突触层中组成性表达。CCL5似乎与穆勒细胞、视网膜神经节细胞(RGC)以及外网层中水平细胞与双极细胞之间、内网层中无长突细胞、双极细胞与RGC之间的突触连接相关。虽然CCL5的所有三种高亲和力受体(CCR5、CCR3、CCR1)均组成性表达,但CCR5的表达显著高于CCR3,而CCR3的表达也明显高于CCR1。组成性CCR5、CCR3和CCR1表达的定位模式不同,尤其是在内层视网膜神经元中的表达。与应激相关的CCL5表达主要在眼压升高的老年DBA/2小鼠中发生改变。相比之下,CCR3和CCR5的表达及定位变化不仅在老年DBA/2小鼠中明显,在年龄匹配的对照小鼠和年轻DBA/2小鼠中也很明显。这些组未表现出眼压升高,但具有衰老应激(对照小鼠)或青光眼遗传易感性(DBA/2小鼠)。总之,这些数据表明CCL5及其高亲和力受体在小鼠视网膜中组成性表达,并受到与青光眼性视神经病变相关应激源的差异诱导。定位模式进一步表明,CCL5信号传导可能在健康和疾病状态下对突触调节都有意义,尤其是在内网层。

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