# Cu Transporting ATPase and Diabetic Vascular Complications

> **NIH NIH R01** · AUGUSTA UNIVERSITY · 2020 · $680,705

## Abstract

This grant will elucidate the novel protective role of “Copper transporting ATPase (ATP7A)” against
impaired reparative neovascularization in diabetic ischemic vascular diseases. Diabetic complication
leads to defective neovascularization in ischemic peripheral vascular disease due to impaired angiogenesis and
endothelial cell (EC) barrier dysfunction with unknown mechanisms. Copper (Cu), an essential micronutrient, is
involved in angiogenesis while excess Cu contributes to inflammatory diseases such as diabetes. Since excess
Cu is toxic, bioavailability of intracellular Cu is tightly controlled by ATP7A which delivers Cu to the secretory Cu
enzymes, or exports Cu to extracellular space. Our lab discovered that ATP7A in VSMC protects against
hypertension. We also identified ‘IQGAP1” as a VEGF receptor2 (VEGFR2) binding scaffold protein promoting
VEGF signaling and post-ischemic angiogenesis. However, role of ATP7A in ECs for defective post-ischemic
revascularization in diabetes is entirely unknown. Preliminary data suggest that ATP7A prevents VEGFR2
degradation through binding to IQGAP1 and maintains basal EC barrier function via regulating VE-cadherin (VE-
Cad). ATP7A expression is markedly decreased in ECs from diabetic mice or microvessels of type2 diabetes
patients. ATP7A mutant (ATP7Amut) mice with reduced Cu transport function or diabetic mice show impaired
ischemia-induced reparative angiogenesis with excess tissue Cu and vascular permeability/tissue damage,
which are rescued by overexpression of ATP7A. We thus hypothesize that ATP7A functions to promote and
integrate key vascular repair programs such as angiogenesis and maintaining endothelial barrier
function in a Cu-dependent manner, which is required for restoring neovascularization in diabetic
ischemic vascular disease. Aim 1 will define the protective role of ATP7A against: i) impaired VEGF-induced
angiogenesis by stabilizing VEGFR2 and ii) endothelial barrier dysfunction by maintaining Cu homeostasis in
ECs isolated from diabetic mice and human microvessels of type2 diabetic patients. Aim 2 will determine the
molecular mechanism by which ATP7A downregulation in diabetes impairs VEGFR2 signaling and endothelial
barrier integrity by focusing on; i) ATP7A binding to IQGAP1 that prevents VEGFR2 ubiquitination/degradation
in a Cu-independent manner, and ii) role of ATP7A in regulating miR-125b that represses VE-Cad via Cu-
dependent transcription factor Atox1. Aim 3 will define the protective role of ATP7A against diabetes-induced
impaired post-ischemic neovascularization and tissue repair in vivo and address underlying mechanisms using
animal model of critical limb ischemia. We will use ATP7Amut and ATP7A transgenic mice; inducible EC-specific
ATP7A-/- or Cu importer CTR1-/- mice or type1 and type2 diabetes mice; innovative ICP-Mass Spec, X-ray
fluorescence microscopy to analyze [Cu]i in cells and tissues; FRET or BiFC-based protein-protein interaction;
and intravital microscopy. Our st...

## Key facts

- **NIH application ID:** 9977232
- **Project number:** 5R01HL133613-04
- **Recipient organization:** AUGUSTA UNIVERSITY
- **Principal Investigator:** TOHRU FUKAI
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $680,705
- **Award type:** 5
- **Project period:** 2017-09-01 → 2022-07-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9977232

## Citation

> US National Institutes of Health, RePORTER application 9977232, Cu Transporting ATPase and Diabetic Vascular Complications (5R01HL133613-04). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/9977232. Licensed CC0.

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