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动物模型中的视网膜成像:寻找神经退行性变的生物标志物。

Retinal imaging in animal models: Searching for biomarkers of neurodegeneration.

作者信息

Batista Ana, Guimarães Pedro, Serranho Pedro, Nunes Ana, Martins João, Moreira Paula I, Ambrósio António Francisco, Morgado Miguel, Castelo-Branco Miguel, Bernardes Rui

机构信息

University of Coimbra, Coimbra Institute for Biomedical Imaging and Translational Research (CIBIT), Institute for Nuclear Sciences Applied to Health (ICNAS), Coimbra, Portugal.

Universidade Aberta, Department of Sciences and Technology, Lisbon, Portugal.

出版信息

Front Ophthalmol (Lausanne). 2023 Apr 6;3:1156605. doi: 10.3389/fopht.2023.1156605. eCollection 2023.

Abstract

There is a pressing need for novel diagnostic and progression biomarkers of neurodegeneration. However, the inability to determine disease duration and stage in patients with Alzheimer's disease (AD) hinders their discovery. Because animal models of disease allow us to circumvent some of these limitations, they have proven to be of paramount importance in clinical research. Due to the clear optics of the eye, the retina combined with optical coherence tomography (OCT) offers the perfect opportunity to image neurodegeneration in the retina , non-invasively, directly, quickly, and inexpensively. Based on these premises, our group has worked towards uncovering neurodegeneration-associated changes in the retina of the triple-transgenic mouse model of familial AD (3×Tg-AD). In this work, we present an overview of our work on this topic. We report on thickness variations of the retina and retinal layers/layer aggregates caused by healthy aging and AD-like conditions and discuss the implications of focusing research efforts solely on retinal thickness. We explore what other information is embedded in the OCT data, extracted based on texture analysis and deep-learning approaches, to further identify biomarkers that could be used for early detection and diagnosis. We were able to detect changes in the retina of the animal model of AD as early as 1 month of age. We also discuss our work to develop an optical coherence elastography system to measure retinal elasticity, which can be used in conjunction with conventional OCT. Finally, we discuss the potential application of these technologies in human patients and the steps needed to make OCT a helpful screening tool for the detection of neurodegeneration.

摘要

对于神经退行性变的新型诊断和病情进展生物标志物有着迫切需求。然而,无法确定阿尔茨海默病(AD)患者的疾病持续时间和阶段阻碍了这些标志物的发现。由于疾病动物模型使我们能够规避其中一些限制,它们已被证明在临床研究中至关重要。由于眼睛具有清晰的光学特性,视网膜结合光学相干断层扫描(OCT)提供了一个绝佳机会,可以以非侵入性、直接、快速且低成本的方式对视网膜中的神经退行性变进行成像。基于这些前提,我们团队致力于揭示家族性AD三联转基因小鼠模型(3×Tg-AD)视网膜中与神经退行性变相关的变化。在这项工作中,我们概述了我们在该主题上的工作。我们报告了由健康衰老和类AD状况引起的视网膜及视网膜各层/层聚集体的厚度变化,并讨论了仅关注视网膜厚度的研究工作的意义。我们探索基于纹理分析和深度学习方法从OCT数据中提取的其他信息,以进一步识别可用于早期检测和诊断的生物标志物。我们能够早在1月龄时就检测到AD动物模型视网膜中的变化。我们还讨论了我们开发光学相干弹性成像系统以测量视网膜弹性的工作,该系统可与传统OCT结合使用。最后,我们讨论了这些技术在人类患者中的潜在应用以及使OCT成为检测神经退行性变的有用筛查工具所需的步骤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/08b8/11182266/d0d8f85a9bbb/fopht-03-1156605-g001.jpg

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