# Regulation of Myocardial Phospholipases and Lipases in Diabetic Myocardium

> **NIH NIH R01** · WASHINGTON UNIVERSITY · 2022 · $785,597

## Abstract

ABSTRACT
Heart disease is the most common cause of death in industrialized nations. The presence of underlying diabetes
is the greatest risk factor for the progression of heart disease. During the current grant interval, we have
discovered previously unknown lipid metabolic pathways and signaling molecules which lead to the generation
of eicosanoid-lysophospholipids. Remarkably, the vast majority of eicosanoids in myocardium were found to be
esterified to the glycerol backbone of lysophospholipids. In addition, induction of Type I diabetes in wild-type
mice or ischemic damage in isolated wild-type mouse hearts resulted in dramatic increases in pro-inflammatory
eicosanoid-lysophospholipids. This new class of phospholipids serve as inflammatory mediators by inducing the
release of TNFa from monocytes or macrophages. Importantly, genetic ablation of iPLA2g (PNPLA8)
substantially decreased the levels of eicosanoid-lysophospholipids in myocardium in the diabetic state, during
myocardial ischemia and synergistically decreased their synthesis in diabetic myocardium rendered ischemic.
Accordingly, we propose that iPLA2g plays a central role in the pathophysiologic development of diabetic heart
disease and promotes the lethal sequelae of diabetic cardiomyopathy. In Specific Aim 1, we will utilize stable
isotope labeling of isolated perfused mouse hearts from genetically engineered cardiac myocyte-specific
conditional iPLA2g knockout mice we have generated. These studies will investigate the roles of iPLA2g in the
metabolic flux of: 1) non-esterified and esterified eicosanoids; 2) eicosanoid-lysophospholipids; and 3) other
salient oxidized phospholipids. Stable isotope pulse-chase experiments followed by penetrating bioinformatic
analyses will determine rates of metabolic flux through these newly discovered pathways. Translationally, we
will explore the impact of Type 2 diabetes on myocardial ischemic damage and the potential salvage of ischemic
myocardium in cardiac myocyte-specific iPLA2g KO mice we engineered. Endpoints of analysis include infarct
size, hemodynamic performance, and post-translational modifications of iPLA2g. In Specific Aim 2, we will utilize
cardiac myocyte-specific iPLA2b KO mice we have generated to explore the role of iPLA2b in promoting
myocardial ischemic damage and arrhythmias in WT vs. iPLA2b KO mice in the context of Type II diabetes. Next,
we will determine the ability of iPLA2b to catalyze acyltransferase or transacylase mediated re-esterification of
eicosanoid-lysophospholipids to generate oxidized phospholipids which have been implicated in damage
associated molecular patterns. In Specific Aim 3, the mechanisms through which a high fat diet induces
eicosanoid-lysolipid synthesis accompanied by inflammation and mitochondrial dysfunction will be studied. The
roles of lysophospholipases in modulating eicosanoid-lysophospholipid levels and activation mechanisms for
iPLA2g will be examined. Collectively, the proposed studies wil...

## Key facts

- **NIH application ID:** 10367196
- **Project number:** 2R01HL118639-09A1
- **Recipient organization:** WASHINGTON UNIVERSITY
- **Principal Investigator:** RICHARD W GROSS
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2022
- **Award amount:** $785,597
- **Award type:** 2
- **Project period:** 2013-06-01 → 2026-01-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10367196

## Citation

> US National Institutes of Health, RePORTER application 10367196, Regulation of Myocardial Phospholipases and Lipases in Diabetic Myocardium (2R01HL118639-09A1). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10367196. Licensed CC0.

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