首页> 外文会议>Conference on ophthalmic technologies XXVII >Longitudinal visualization of vascular occlusion, reperfusion, and remodeling in a zebrafish model of retinal vascular leakage using OCT angiography
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Longitudinal visualization of vascular occlusion, reperfusion, and remodeling in a zebrafish model of retinal vascular leakage using OCT angiography

机译:OCT血管造影的Zebrafish血管泄漏斑马鱼模型中血管闭塞,再灌注和重塑的纵向可视化

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Diabetic retinopathy (DR) and age-related macular degeneration (AMD) are two of the leading causes of blindness and visual impairment in the world. Neovascularization results in severe vision loss in DR and AMD and, thus, there is an unmet need to identify mechanisms of pathogenesis and novel anti-angiogenic therapies. Zebrafish is a leading model organism for studying human disease pathogenesis, and the highly conserved drug activity between zebrafish and humans and their ability to readily absorb small molecules dissolved in water has benefited pharmaceutical discovery. Here, we use optical coherence tomography (OCT) and OCT angiography (OCT-A) to perform noninvasive, in vivo retinal imaging in a zebrafish model of vascular leakage. Zebrafish were treated with diethylaminobenzaldehyde (DEAB) to induce vascular leakage and imaged with OCT and OCT-A at six time points over two weeks: baseline one day before treatment and one, three, six, eight, and ten days post treatment. Longitudinal functional imaging showed significant vascular response immediately after DEAB treatment. Observed vascular changes included partial or complete vascular occlusion immediately after treatment and reperfusion during a two-week period. Increased vascular tortuosity several days post treatment indicated remodeling, and bifurcations and collateral vessel formation were also observed. In addition, significant treatment response variabilities were observed in the contralateral eye of the same animal. Anatomical and functional normalization was observed in most animals by ten days post treatment. These preliminary results motivate potential applications of OCT-A as a tool for studying pathogenesis and therapeutic screening in zebrafish models of retinal vascular disease.
机译:糖尿病视网膜病变(DR)和年龄相关的黄斑变性(AMD)是世界上失明和视力障碍的两个主要原因。新生血管结果导致博士和AMD中的严重视力丧失,因此,存在未满足的需要识别发病机制和新型抗血管生成疗法的机制。斑马鱼是研究人类疾病发病机制的主要模型生物体,以及斑马鱼和人类之间的高度保守的药物活动及其容易吸收溶解在水中的小分子的能力有利于药物发现。在这里,我们使用光学相干断层扫描(OCT)和OCT血管造影(OCT-A)进行非侵入性,体内视网膜成像在血管泄漏的斑马鱼模型中。斑马鱼用二乙基氨基苯并醛(DEAB)对待,诱导血管泄漏并在10周的六个时间点诱导血管泄漏和成像,在治疗前一天,三个,三,六,八和十天的治疗前一天。纵向功能成像在DEAB处理后立即显示出显着的血管反应。观察到的血管变化包括在为期两周的时间内治疗和再灌注后立即部分或完全血管闭塞。增加血管曲折术后几天治疗表明重塑,并且还观察到分叉和侧支血管形成。此外,在同一动物的对侧观察到显着的治疗反应变性。在治疗后十天的大多数动物中观察到解剖学和功能正常化。这些初步结果激发了OCT-A的潜在应用作为研究视网膜血管疾病斑马鱼模型的发病机制和治疗筛选的工具。

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