# "Implementing a novel multimode 3D retinal imaging system to investigate metabolism and vascular disruptions in diabetic retinopathy"

> **NIH NIH R15** · UNIVERSITY OF WISCONSIN MILWAUKEE · 2020 · $98,843

## Abstract

Diabetes causes microvascular and cellular redox complications in the retina and development of diabetic
retinopathy (DR). The early mechanisms by which diabetes adversely affects retinal neurovascular function and
integrity, and diabetic retinopathy progression, are poorly understood. This lack of understanding is hampered
by the inability to detect and study these changes early and non-invasively. There is a crucial need for
noninvasive imaging tools and quantitative biomarkers as indicators of diabetes’ adverse effect on the retinal
neurovasculature, metabolism, and function. The main premise of this study is addressing the significant gap in
existing tools to simultaneously and noninvasively measure mitochondrial redox state, and retinal neurovascular
integrity during diabetes. These measurements will provide biomarkers, which could be used in primary care
settings.
 The main hypothesis of this AREA project is that diabetes stimulates mitochondrial dysfunction,
increased OxS, and neurovascular disruption in the retina that can be detected non-invasively. Our team will
implement a MM- cSLO to evaluate these changes in diabetic Akita/+ mice to test that early disruption of
mitochondrial redox states and neurovascular integrity is critical in retinal dysfunction. There are three specific
aims to test these hypotheses.1) Design and implement a multimodal confocal scanning laser ophthalmoscope
(MM-cSLO) for high resolution spatiotemporal imaging of DR biomarkers. 2) Determine changes in the retinal
vascular network, oxygenation, and mitochondrial dysfunction during diabetes.
 The outcome of these studies will establish the course of mitochondrial dysfunction and neurovascular
disruption in early diagnosis of diabetes changes. The use of this non-invasive imaging modality could permit
detection and treatment of patients with diabetes based upon individualized risk versus benefit assessments in
real time. Correlation of anatomical and functional information from retinal imaging could help elucidate the
functional consequences of the findings of retinal imaging and provide further support for their use as outcomes
measures of therapeutic intervention. If these detection and treatment methods are proven effective, they could
be immediately evaluated in translational research.
 This AREA application will lead to a unique interdisciplinary educational platform for training UWM
undergraduate and graduate students. There is a very broad and very rich educational opportunity for students
to learn about electronics, optics, instrumentation, biology, biochemistry, computer programing wrapped in
specific research project that can only be accomplished in such an interdisciplinary approach. Such an
educational platform would increase the participation of UWM’s undergraduates majoring in electrical
engineering and biomedical engineering in research. Successful implementation of these research activities will
facilitate the long term, sustainable goal of translat...

## Key facts

- **NIH application ID:** 9971990
- **Project number:** 1R15EY031533-01
- **Recipient organization:** UNIVERSITY OF WISCONSIN MILWAUKEE
- **Principal Investigator:** Mahsa Ranji
- **Activity code:** R15 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $98,843
- **Award type:** 1
- **Project period:** 2020-06-01 → 2020-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9971990

## Citation

> US National Institutes of Health, RePORTER application 9971990, "Implementing a novel multimode 3D retinal imaging system to investigate metabolism and vascular disruptions in diabetic retinopathy" (1R15EY031533-01). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/9971990. Licensed CC0.

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