Oxidative stress, innate immunity, and age-related macular degeneration.

IF 0.7 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY
AIMS Molecular Science Pub Date : 2016-01-01 Epub Date: 2016-05-11 DOI:10.3934/molsci.2016.2.196
Peter X Shaw, Travis Stiles, Christopher Douglas, Daisy Ho, Wei Fan, Hongjun Du, Xu Xiao
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引用次数: 148

Abstract

Age-related macular degeneration (AMD) is a leading cause of vision loss affecting tens of millions of elderly worldwide. Early AMD is characterized by the appearance of soft drusen, as well as pigmentary changes in the retinal pigment epithelium (RPE). These soft, confluent drusen can progress into two forms of advanced AMD: geographic atrophy (GA, or dry AMD) or choroidal neovascularization (CNV, or wet AMD). Both forms of AMD result in a similar clinical progression in terms of loss of central vision. The exact mechanism for developing early AMD, as well as triggers responsible for progressing to advanced stage of disease, is still largely unknown. However, significant evidence exists demonstrating a complex interplay of genetic and environmental factors as causes of AMD progression. Multiple genes and/or single nucleotide polymorphisms (SNPs) have been found associated with AMD, including various genes involved in the complement pathway, lipid metabolism and extracellular matrix (ECM) remodeling. Of the known genetic contributors to disease risk, the CFH Y402H and HTRA1/ARMS polymorphisms contribute to more than 50% of the genetic risk for AMD. Environmentally, oxidative stress plays a critical role in many aging diseases including cardiovascular disease, cancer, Alzheimer's disease and AMD. Due to the exposure to sunlight and high oxygen concentration, the oxidative stress burden is higher in the eye than other tissues, which can be further complicated by additional oxidative stressors such as smoking. Increasingly, evidence is accumulating suggesting that functional abnormalities of the innate immune system incurred via high risk genotypes may be contributing to the pathogenesis of AMD by altering the inflammatory homeostasis in the eye, specifically in the handling of oxidation products. As the eye in non-pathological instances maintains a low level of inflammation despite the presence of a relative abundance of potentially inflammatory molecules, we have previously hypothesized that the tight homeostatic control of inflammation via the innate immune system is likely critical for avoidance of disease progression. However, the presence of a multitude of potential triggers of inflammation results in a sensitive balance in which perturbations thereof would subsequently alter the inflammatory state of the retina, leading to a state of chronic inflammation and pathologic progression. In this review, we will highlight the background literature surrounding the known genetic and environmental contributors to AMD risk, as well as a discussion of the potential mechanistic interplay of these factors that lead to disease pathogenesis with particular emphasis on the delicate control of inflammatory homeostasis and the centrality of the innate immune system in this process.

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氧化应激、先天免疫和老年性黄斑变性。
年龄相关性黄斑变性(AMD)是影响全球数千万老年人视力丧失的主要原因。早期AMD的特点是软性囊肿的出现,以及视网膜色素上皮(RPE)的色素改变。这些柔软的、融合的结节可发展为两种形式的晚期AMD:地理性萎缩(GA,或干性AMD)或脉络膜新生血管(CNV,或湿性AMD)。两种形式的AMD在中心视力丧失方面的临床进展相似。发展早期AMD的确切机制,以及导致疾病进展到晚期的触发因素,在很大程度上仍然未知。然而,有重要证据表明遗传和环境因素的复杂相互作用是导致AMD进展的原因。已经发现多个基因和/或单核苷酸多态性(snp)与AMD相关,包括参与补体途径、脂质代谢和细胞外基质(ECM)重塑的各种基因。在已知的疾病风险遗传因素中,CFH Y402H和HTRA1/ARMS多态性对AMD的遗传风险贡献超过50%。在环境方面,氧化应激在许多衰老疾病中起着关键作用,包括心血管疾病、癌症、阿尔茨海默病和AMD。由于暴露在阳光和高氧浓度下,眼睛的氧化应激负担比其他组织更高,而吸烟等额外的氧化应激源可能会使情况进一步复杂化。越来越多的证据表明,由高风险基因型引起的先天免疫系统功能异常可能通过改变眼部炎症稳态,特别是氧化产物的处理,导致AMD的发病机制。由于在非病理性情况下,尽管存在相对丰富的潜在炎症分子,但眼睛保持低水平的炎症,我们先前假设通过先天免疫系统对炎症的严格稳态控制可能是避免疾病进展的关键。然而,许多潜在的炎症触发因素的存在导致了一个敏感的平衡,其中扰动将随后改变视网膜的炎症状态,导致慢性炎症和病理进展的状态。在这篇综述中,我们将重点介绍有关AMD风险的已知遗传和环境因素的背景文献,以及这些因素导致疾病发病机制的潜在机制相互作用的讨论,特别强调炎症稳态的微妙控制和先天免疫系统在这一过程中的中心作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
AIMS Molecular Science
AIMS Molecular Science BIOCHEMISTRY & MOLECULAR BIOLOGY-
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