Biomarkers of Early Experimental Glaucoma - Resubmission - 1

早期实验性青光眼的生物标志物 - 重新提交 - 1

• 批准号: 9917397
• 负责人: Gadi Wollstein
• 金额: $ 72.44万
• 依托单位: NEW YORK UNIVERSITY SCHOOL OF MEDICINE
• 依托单位国家: 美国
• 财政年份: 2020
• 资助国家: 美国
• 起止时间: 2020-04-01 至 2024-03-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/9917397
• 关键词: 3-Dimensional; Acute; Angiography; Animal Model; Animals; Astrocytes; Axon; Axoplasmic Streaming; Biological Markers; Biomechanics; Blindness; Blood Vessels; Brain; Characteristics; Chronic; Clinical Treatment; Complex; Contrast Sensitivity; Development; Diagnosis; Diagnostic; Disease; Early Diagnosis; Electroretinography; Ensure; Event; Experimental Designs; Experimental Models; Exposure to; Eye; Functional disorder; Future; Glaucoma; Goals; Health; Health Transition; Human; Imaging technology; In Situ; Individual; Individual Differences; Intervention; Intracranial Pressure; Knowledge; Life; Location; Macaca mulatta; Measurement; Mechanics; Methods; Modeling; Monitor; Morbidity - disease rate; Nutritional Support; Ocular Hypertension; Optic Disk; Optic Nerve; Outcome; Oxygen Consumption; Pattern; Perfusion; Perimetry; Physiologic Intraocular Pressure; Predisposition; Process; Reporting; Research; Research Project Grants; Retina; Retinal Ganglion Cells; Rhesus; Risk; Role; Scanning; Site; Structure; Testing; Thick; Three-dimensional analysis; Time; TimeLine; Tissues; Translating; Travel; Visible Radiation; Vision; base; cell injury; clinical care; clinical diagnostics; early detection biomarkers; follow-up; image processing; in vivo; in vivo imaging; insight; new technology; nonhuman primate; ocular imaging; optic nerve disorder; preservation; pressure; response; retinal damage; spatial relationship; tissue oxygenation; tool

PROJECT SUMMARY Glaucoma is a leading cause of vision morbidity and blindness with irreversible damage to retinal ganglion cells. Identifying biomarkers for early detection of glaucoma are paramount for timely initiation of treatment for preservation of functional vision throughout life. This project uses a chronic ocular hypertension animal model that provides unique insight into the changes the eye undergoes as it transitions from health to fully-manifest glaucoma. Using advanced ocular imaging technologies and state-of-the-art image processing methods we will monitor longitudinal structural and functional ocular changes, both global and local, of each animal as they develop glaucoma. We will determine the response of the optic nerve to two of the major causes of glaucoma – intraocular pressure (IOP) and intracranial pressure (ICP) – by acutely modulating these pressures and quantifying changes in optic nerve deformation at different time points along the course of the follow-up. This will allow determining the role of these pressures at the various stages of glaucoma development and changes in the optic nerve resulting from chronic exposure to elevated IOP, also known as remodeling. Lastly, we will identify structural and functional features and locations in the eye that are associated with future development of glaucomatous damage. The outcome of this project will provide insight into sensitive ocular biomarkers and their timeline of occurrence for early detection of glaucoma. Our model and tools ensure that the results can be translated to humans with substantial impact on clinical care.

项目摘要 青光眼是视力发病率和失明的主要原因，对永久神经节的不可逆转损害 细胞。确定早期检测青光眼的生物标志物对于及时开始治疗至关重要 一生的功能视觉保存。该项目使用慢性眼高血压动物模型 这为眼睛从健康过渡到完全手术时的变化提供了独特的见解 青光眼。使用先进的眼部成像技术和最先进的图像处理方法，我们将 监测每只动物的纵向结构和功能性眼变化，包括每只动物的全球和局部变化 发展青光眼。我们将确定视神经对青光眼的两个主要原因 - 眼内压（IOP）和颅内压（ICP） - 急性调节这些压力和 在随访过程中量化视神经变形的变化。这 将允许确定这些压力在青光眼发展的各个阶段的作用和变化 在长期暴露于升高的IOP（也称为重塑）导致的视神经中。最后，我们会的 确定眼睛中与未来发展相关的结构和功能功能和位置 青光眼损伤。 该项目的结果将提供有关敏感的眼生物标志物及其时间表的见解 早期检测青光眼的发生。我们的模型和工具确保结果可以转化为 对临床护理产生重大影响的人。