# Molecular Mechanisms Regulating Endothelial Dysfunction

> **NIH NIH R01** · BOSTON CHILDREN'S HOSPITAL · 2020 · $676,330

## Abstract

ABSTRACT
Atherosclerosis is the primary cause of coronary heart disease (CHD), ischemic stroke, and peripheral arterial
disease. Despite effective lipid-lowering therapies and prevention programs, atherosclerosis is still the leading
cause of mortality in the United States. Moreover, the prevalence of CHD in developing countries worldwide is
rapidly increasing at a rate expected to overtake those of cancer and diabetes. Among prominent risk factors,
hardening of arteries resulting from endothelial cell (EC) dysfunction, plays a causative role in promoting
atherosclerosis initiation and progression. However, owing to the complexity of the endothelium and scarcity of
proper molecular targets, it is widely recognized that hindering dysfunctional endothelium to prevent atheroma
progression is a seemingly daunting question. Our long-term goal is to uncover and dissect molecular
mechanisms governing endothelial dysfunction, and to aid rapid identification of a new class of potential
regulators responsible. To this end, we show that epsins 1 and 2 are upregulated in atheromas in
apolipoprotein E-deficient (ApoE-/-) mice fed with western diet (WD). Consequently, EC-specific epsins
deficiency results in striking attenuation of atherosclerosis in WD fed ApoE-/- mice. Moreover, we observe that
upregulation of epsins associates with downregulation of IP3R1 in both mouse and human atherosclerotic
lesions. Interestingly, atherogenic mediators induce epsin binding to IP3R1 and IP3R1 downregulation in
endothelial cells. Accordingly, IP3R1 loss augments ER stress, while epsin deficiency prevents IP3R1 loss and
therefore attenuates ER stress. Despite these novel observations, whether sufficient IP3R1 is required for
keeping ER stress at bay and blocking atheroma progression is unclear. Likewise, whether epsins promote
atherosclerosis in part via mediating IP3R1 downregulation is unknown. Given that downregulation of ER
stress sensors including XBP-1 correlates with IP3R1 stabilization, the ability of XBP-1 to potentiate ERAD and
thereby mediate epsin-dependent IP3R1 degradation is unexplored. In pursuit of answers to these highly
significant and original questions, we have formulated the central hypothesis that epsin promotes
atherosclerosis by inducing downregulation of IP3R1, exacerbating ER stress, and causing endothelial
dysfunction. To test our hypothesis, we propose to use novel atherosclerosis mouse models including inducible
EC-specific IP3R1 deficient mice (EC-IP3R1iKO), inducible EC-specific epsin DKO mice (EC-iDKO) on EC-
specific IP3R1 heterozygous background (EC-iDKO/EC-IP3R1het), and EC-specific XBP-1 deficient mice (EC-
XBP-1KO) on ApoE null background. We are poised to determine the molecular mechanisms underlying epsins
mediating IP3R1 degradation in atherosclerosis; and molecular mechanisms by which ER stress sensors
potentiate epsin-mediated IP3R1 degradation. If fruitful, our findings will hold a high probability of uncovering a
counter-intuiti...

## Key facts

- **NIH application ID:** 9964885
- **Project number:** 5R01HL137229-04
- **Recipient organization:** BOSTON CHILDREN'S HOSPITAL
- **Principal Investigator:** Hong Chen
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $676,330
- **Award type:** 5
- **Project period:** 2017-07-20 → 2023-06-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9964885

## Citation

> US National Institutes of Health, RePORTER application 9964885, Molecular Mechanisms Regulating Endothelial Dysfunction (5R01HL137229-04). Retrieved via AI Analytics 2026-05-26 from https://api.ai-analytics.org/grant/nih/9964885. Licensed CC0.

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