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An extensive ß1-adrenergic receptor gene signaling network regulates molecular remodeling in dilated cardiomyopathies.

Tatman, Philip D; Kao, David P; Chatfield, Kathryn C; Carroll, Ian A; Wagner, Jessica A; Jonas, Eric R; Sucharov, Carmen C; Port, J David; Lowes, Brian D; Minobe, Wayne A; Huebler, Sophia P; Karimpour-Fard, Anis; Rodriguez, Erin M; Liggett, Stephen B; Bristow, Michael R.

JCI Insight ; 8(16)2023 08 22.

Article En | MEDLINE | ID: mdl-37606047

We investigated the extent, biologic characterization, phenotypic specificity, and possible regulation of a ß1-adrenergic receptor-linked (ß1-AR-linked) gene signaling network (ß1-GSN) involved in left ventricular (LV) eccentric pathologic remodeling. A 430-member ß1-GSN was identified by mRNA expression in transgenic mice overexpressing human ß1-ARs or from literature curation, which exhibited opposite directional behavior in interventricular septum endomyocardial biopsies taken from patients with beta-blocker-treated, reverse remodeled dilated cardiomyopathies. With reverse remodeling, the major biologic categories and percentage of the dominant directional change were as follows: metabolic (19.3%, 81% upregulated); gene regulation (14.9%, 78% upregulated); extracellular matrix/fibrosis (9.1%, 92% downregulated); and cell homeostasis (13.3%, 60% upregulated). Regarding the comparison of ß1-GSN categories with expression from 19,243 nonnetwork genes, phenotypic selection for major ß1-GSN categories was exhibited for LV end systolic volume (contractility measure), ejection fraction (remodeling index), and pulmonary wedge pressure (wall tension surrogate), beginning at 3 months and persisting to study completion at 12 months. In addition, 121 lncRNAs were identified as possibly involved in cis-acting regulation of ß1-GSN members. We conclude that an extensive 430-member gene network downstream from the ß1-AR is involved in pathologic ventricular remodeling, with metabolic genes as the most prevalent category.

Biological Products , Cardiomyopathy, Dilated , Animals , Mice , Humans , Cardiomyopathy, Dilated/genetics , Gene Regulatory Networks , Signal Transduction , Mice, Transgenic , Receptors, Adrenergic

Myocardial Injury and Altered Gene Expression Associated With SARS-CoV-2 Infection or mRNA Vaccination.

Altman, Natasha L; Berning, Amber A; Saxon, Cara E; Adamek, Kylie E; Wagner, Jessica A; Slavov, Dobromir; Quaife, Robert A; Gill, Edward A; Minobe, Wayne A; Jonas, Eric R; Carroll, Ian A; Huebler, Sophia P; Raines, Joshua; Messenger, John C; Ambardekar, Amrut V; Mestroni, Luisa; Rosenberg, Rachel M; Rove, Jessica; Campbell, Thomas B; Bristow, Michael R.

JACC Basic Transl Sci ; 8(2): 124-137, 2023 Feb.

Article En | MEDLINE | ID: mdl-36281440

SARS CoV-2 enters host cells via its Spike protein moiety binding to the essential cardiac enzyme angiotensin-converting enzyme (ACE) 2, followed by internalization. COVID-19 mRNA vaccines are RNA sequences that are translated into Spike protein, which follows the same ACE2-binding route as the intact virion. In model systems, isolated Spike protein can produce cell damage and altered gene expression, and myocardial injury or myocarditis can occur during COVID-19 or after mRNA vaccination. We investigated 7 COVID-19 and 6 post-mRNA vaccination patients with myocardial injury and found nearly identical alterations in gene expression that would predispose to inflammation, coagulopathy, and myocardial dysfunction.