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眼球生长中视网膜向巩膜信号传递的候选途径。

Candidate pathways for retina to scleral signaling in refractive eye growth.

机构信息

Department of Biomedical Engineering, Georgia Institute of Technology/Emory University, 313 Ferst Drive, Atlanta, GA, 30332, USA; Center for Visual and Neurocognitive Rehabilitation, Atlanta Veterans Affairs Healthcare System, 1670 Clairmont Rd, Atlanta, GA, 30033, USA.

Center for Visual and Neurocognitive Rehabilitation, Atlanta Veterans Affairs Healthcare System, 1670 Clairmont Rd, Atlanta, GA, 30033, USA; Division of Sleep and Circadian Disorders, Brigham and Women's Hospital, Harvard Medical School, 221 Longwood Avenue, Boston, MA, 02115, USA; Division of Sleep Medicine, Harvard Medical School, Boston, MA, 02115, USA; Gangarosa Department of Environmental Health, Emory University, 1518 Clifton Rd, Atlanta, GA, 30322, USA.

出版信息

Exp Eye Res. 2022 Jun;219:109071. doi: 10.1016/j.exer.2022.109071. Epub 2022 Apr 18.

DOI:10.1016/j.exer.2022.109071
PMID:35447101
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9701099/
Abstract

The global prevalence of myopia, or nearsightedness, has increased at an alarming rate over the last few decades. An eye is myopic if incoming light focuses prior to reaching the retinal photoreceptors, which indicates a mismatch in its shape and optical power. This mismatch commonly results from excessive axial elongation. Important drivers of the myopia epidemic include environmental factors, genetic factors, and their interactions, e.g., genetic factors influencing the effects of environmental factors. One factor often hypothesized to be a driver of the myopia epidemic is environmental light, which has changed drastically and rapidly on a global scale. In support of this, it is well established that eye size is regulated by a homeostatic process that incorporates visual cues (emmetropization). This process allows the eye to detect and minimize refractive errors quite accurately and locally over time by modulating the rate of elongation of the eye via remodeling its outermost coat, the sclera. Critically, emmetropization is not dependent on post-retinal processing. Thus, visual cues appear to influence axial elongation through a retina-to-sclera, or retinoscleral, signaling cascade, capable of transmitting information from the innermost layer of the eye to the outermost layer. Despite significant global research interest, the specifics of retinoscleral signaling pathways remain elusive. While a few pharmacological treatments have proven to be effective in slowing axial elongation (most notably topical atropine), the mechanisms behind these treatments are still not fully understood. Additionally, several retinal neuromodulators, neurotransmitters, and other small molecules have been found to influence axial length and/or refractive error or be influenced by myopigenic cues, yet little progress has been made explaining how the signal that originates in the retina crosses the highly vascular choroid to affect the sclera. Here, we compile and synthesize the evidence surrounding three of the major candidate pathways receiving significant research attention - dopamine, retinoic acid, and adenosine. All three candidates have both correlational and causal evidence backing their involvement in axial elongation and have been implicated by multiple independent research groups across diverse species. Two hypothesized mechanisms are presented for how a retina-originating signal crosses the choroid - via 1) all-trans retinoic acid or 2) choroidal blood flow influencing scleral oxygenation. Evidence of crosstalk between the pathways is discussed in the context of these two mechanisms.

摘要

在过去几十年中,近视(即远视)的全球患病率以惊人的速度上升。如果入射光在到达视网膜光感受器之前聚焦,则眼睛为近视,这表明其形状和光学功率不匹配。这种不匹配通常是由于轴向伸长过度引起的。近视流行的重要驱动因素包括环境因素、遗传因素及其相互作用,例如,遗传因素影响环境因素的影响。人们常常假设环境光是导致近视流行的一个因素,因为它在全球范围内发生了巨大而迅速的变化。支持这一观点的是,眼睛大小受到一种自稳态过程的调节,该过程包括视觉线索(正视化)。通过重塑最外层的巩膜,该过程可以通过调节眼睛的伸长率来检测和最小化屈光不正,从而使眼睛能够相当准确和局部地随时间进行矫正。至关重要的是,正视化不依赖于视网膜后处理。因此,视觉线索似乎通过视网膜-巩膜信号级联影响轴向伸长,该信号级联能够将信息从眼睛的最内层传递到最外层。尽管全球研究兴趣显著,但视网膜信号通路的具体细节仍不清楚。虽然一些药物治疗已被证明可有效减缓轴向伸长(最著名的是局部阿托品),但这些治疗的机制仍不完全清楚。此外,已经发现几种视网膜神经调节剂、神经递质和其他小分子会影响眼轴长度和/或屈光不正,或者受近视诱发因素的影响,但在解释起源于视网膜的信号如何穿过富含血管的脉络膜来影响巩膜方面几乎没有取得进展。在这里,我们收集并综合了围绕三个主要候选途径的证据,这些途径受到了广泛关注 - 多巴胺、视黄酸和腺苷。所有这三个候选物都有相关性和因果关系的证据支持它们参与轴向伸长,并被多个独立的研究小组在不同物种中涉及。提出了两种假设的机制来解释起源于视网膜的信号如何穿过脉络膜 - 通过 1)全反式视黄酸或 2)脉络膜血流影响巩膜氧合。在这两种机制的背景下,讨论了途径之间的串扰的证据。

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