# Cardiac dysfunction after ischemic AKI in mice

> **NIH NIH R01** · UNIVERSITY OF COLORADO DENVER · 2021 · $592,494

## Abstract

Abstract
The overall goal of this proposal is to determine the mechanisms by which acute kidney injury (AKI) leads to
acute cardiac dysfunction. Clinically, AKI-mediated cardiac dysfunction is known as cardiorenal syndrome type
3 (CRS3). The mechanisms underpinning CRS3 are not well understood and few plausible mediators of CRS3
have been identified. We recently demonstrated that ischemic AKI causes cardiac dysfunction in mice which
was associated with a 50% reduction in cardiac ATP levels. Thus, cardiac energy metabolism and production
is impaired during AKI and is a fundamental characteristic of CRS3. To identify mediators of CRS3, we
examined plasma and cardiac metabolites. We expected to identify increased levels of circulating metabolites
that might affect cardiac energy metabolism. Rather, we found that numerous metabolites necessary to
maintain cardiac energy production and anti-oxidant defense were deficient in the plasma and heart after AKI,
including over a dozen amino acids and the anti-oxidant glutathione. During cardiac stress, amino acids are
essential substrates for ATP production. Glutamine is particularly important since it can be metabolized to
substrates for both ATP and glutathione synthesis. Glutathione is the most abundant anti-oxidant in the heart
and is critical to maintain normal energy production since excess reactive oxygen species (ROS) impairs
mitochondrial function and inhibits oxidative phosphorylation (OXPHOS). OXPHOS occurs within mitochondria
and is normally the major mechanism of cardiac ATP production. Our preliminary data demonstrate that during
AKI: 1) cardiac mitochondrial function and OXPHOS are impaired, 2) cardiac superoxide (O2●-, an ROS) is
significantly increased, 3) glutamine significantly increases cardiac ATP and reduces O2●-. Based on these
data, our overall hypothesis is that the deficiency of energy substrates and glutathione precursors during AKI
results in increased reactive oxygen species, reduced OXPHOS, reduced ATP production, and cardiac
dysfunction. We have 3 Aims. Aim 1: Determine the effect of AKI on cardiac energy metabolism via metabolic
flux analysis. Aim 2: Determine the mechanisms by which glutamine improves cardiac ATP production after
AKI, in vivo, with the hypothesis that glutamine will reduce cardiac O2●-, increase ATP production, and improve
mitochondrial and cardiac function. Aim 3: Determine the substrates of glutamine metabolism that improve
cardiac ATP production after AKI, ex vivo, with the hypothesis that metabolism to glutathione is the primary
mechanism of glutamine benefit. Since the complications of AKI have long been considered to be due to the
accumulation of metabolic wastes and other substances that may be removed by dialysis for patient benefit,
our overall hypothesis that substrate deficiency is a mechanisms of harm is a paradigm shift that challenges
one of the most fundamental notions in nephrology and will have wide ranging implications regarding the care
of ...

## Key facts

- **NIH application ID:** 10217436
- **Project number:** 1R01HL157973-01
- **Recipient organization:** UNIVERSITY OF COLORADO DENVER
- **Principal Investigator:** Sarah G Faubel
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $592,494
- **Award type:** 1
- **Project period:** 2021-05-10 → 2025-04-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10217436

## Citation

> US National Institutes of Health, RePORTER application 10217436, Cardiac dysfunction after ischemic AKI in mice (1R01HL157973-01). Retrieved via AI Analytics 2026-05-24 from https://api.ai-analytics.org/grant/nih/10217436. Licensed CC0.

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