Targeted Overexpression of Mitochondrial ALDH2 in Coronary Endothelial Cells Mitigates HFpEF in a Diabetic Mouse Model

Authors

Guodong Pan, Henry Ford HealthFollow
Bipradas Roy, Henry Ford HealthFollow
Emmanuel Oppong Yeboah, Henry Ford HealthFollow
Thomas Lanigan
Roland Hilgarth
Rajarajan A Thandavarayan
Michael C Petriello
Shailendra Giri, Henry Ford HealthFollow
Suresh S. Palaniyandi, Henry Ford HealthFollow

Recommended Citation

Pan G, Roy B, Yeboah EO, Lanigan T, Hilgarth R, Thandavarayan RA, Petriello MC, Giri S, and Palaniyandi SS. Targeted Overexpression of Mitochondrial ALDH2 in Coronary Endothelial Cells Mitigates HFpEF in a Diabetic Mouse Model. Biomolecules 2025;15(7).

Document Type

Article

Publication Date

7-16-2025

Publication Title

Biomolecules

Abstract

Heart failure (HF) has become an epidemic, with a prevalence of ~7 million cases in the USA. Despite accounting for nearly 50% of all HF cases, heart failure with a preserved ejection fraction (HFpEF) remains challenging to treat. Common pathophysiological mechanisms in HFpEF include oxidative stress, microvascular dysfunction, and chronic unresolved inflammation. Our lab focuses on oxidative stress-mediated cellular dysfunction, particularly the toxic effects of lipid peroxidation products like 4-hydroxy-2-nonenal (4HNE). Aldehyde dehydrogenase 2 (ALDH2), a mitochondrial enzyme, plays a vital role in detoxifying 4HNE and thereby protecting the heart against pathological stress. ALDH2 activity is reduced in various metabolic stress-mediated cardiac pathologies. The dysfunction of coronary vascular endothelial cells (CVECs) is critical in initiating HFpEF development. Thus, we hypothesized that ectopic overexpression of ALDH2 in CVECs could mitigate metabolic stress-induced HFpEF pathogenesis. In this study, we tested the efficacy of intracardiac injections of the ALDH2 gene into CVECs in db/db mice-a model of obesity-induced type 2 diabetes mellitus (T2DM)-and their controls, db/m mice, by injection with ALDH2 constructs (AAV9-VE-cadherin-hALDH2-HA tag-P2A) or control constructs (AAV9-VE-cadherin-HA tag-P2A-eGFP). We found that intracardiac ALDH2 gene transfer increased ALDH2 levels specifically in CVECs compared to other myocardial cells. Additionally, we observed increased ALDH2 levels and activity, along with decreased 4HNE adducts, in the hearts of mice receiving ALDH2 gene transfer compared to control GFP transfer. Furthermore, ALDH2 gene transfer to CVECs improved diastolic function compared to GFP control alone. In conclusion, ectopic ALDH2 expression in CVECs can contribute, at least partially, to the amelioration of HFpEF.

Medical Subject Headings

Animals; Aldehyde Dehydrogenase, Mitochondrial; Mice; Endothelial Cells; Heart Failure; Disease Models, Animal; Mitochondria; Male; Stroke Volume; Diabetes Mellitus, Experimental; Coronary Vessels; Oxidative Stress; Diabetes Mellitus, Type 2; Mice, Inbred C57BL

PubMed ID

40723901

Volume

15

Issue

7