Prostaglandin D2 Synthase: A Novel Player in the Pathological Signaling Mechanism of the Aldosterone–Mineralocorticoid Receptor Pathway in the Heart
Ankita Garg, Malte Juchem, Sinje Biss, Carla Nunes Borisch, Julia Leonardy, Christian Bär, Shashi Kumar Gupta, Thomas Thum

TL;DR
This study identifies a new protein involved in heart disease caused by a hormone signaling pathway, suggesting a potential new treatment target.
Contribution
The study discovers that prostaglandin D2 synthase is a novel downstream effector of the Aldo–MR pathway in the heart.
Findings
Overactivation of the Aldo–MR pathway in mice caused heart dysfunction, hypertrophy, and fibrosis.
Ptgds was identified as a key mediator of Aldo-induced cardiac pathologies.
Elevated PTGDS levels were found in human heart failure patients and in lab models of heart stress.
Abstract
Background: A deregulated aldosterone (Aldo)–mineralocorticoid receptor (MR) pathway is linked to cardiovascular disease (CVD), including hypertension and heart failure. Despite the association of elevated plasma Aldo levels with cardiac stress, inflammation, myocardial fibrosis, and cardiac remodeling, the underlying mechanisms remain elusive. Methods: To study the impact of Aldo–MR pathway overactivation on cardiac health, a novel mouse model with AAV9-mediated MR overexpression and Aldo administration via subcutaneous osmotic pumps was generated. Echocardiographic analyses, transcriptome sequencing, and loss-of-function experiments of an identified lead candidate gene were performed. Additionally, cardiac tissue samples from human patients with end-stage heart failure were analyzed in the study. Results: Mice with an overactivated Aldo–MR pathway exhibited increased neutrophil…
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Taxonomy
TopicsHormonal Regulation and Hypertension · Cardiovascular, Neuropeptides, and Oxidative Stress Research · Adrenal Hormones and Disorders
