Role of macrophages in regression of myocardial fibrosis following alleviation of left ventricular pressure overload.
Lily S NeffRachel M BiggsYuhua ZhangAn O Van LaerCatalin F BaicuSuganya SubramanianStefano BertoKristine Y DeLeon-PennellMichael R ZileAmy D BradshawPublished in: American journal of physiology. Heart and circulatory physiology (2024)
Sustained hemodynamic pressure overload (PO) produced by murine transverse aortic constriction (TAC) causes myocardial fibrosis; removal of TAC (unTAC) returns left ventricle (LV) hemodynamic load to normal and results in significant, but incomplete regression of myocardial fibrosis. However, the cellular mechanisms that result in these outcomes have not been defined. The objective was to determine temporal changes in myocardial macrophage phenotype in TAC and unTAC and determine whether macrophage depletion alters collagen degradation after unTAC. Myocardial macrophage abundance and phenotype were assessed by immunohistochemistry, flow cytometry, and gene expression by RT-PCR in control (non-TAC), 2 wk, 4 wk TAC, and 2 wk, 4 wk, and 6 wk unTAC. Myocardial cytokine profiles and collagen-degrading enzymes were determined by immunoassay and immunoblots. Initial collagen degradation was detected with collagen-hybridizing peptide (CHP). At unTAC, macrophages were depleted with clodronate liposomes, and endpoints were measured at 2 wk unTAC. Macrophage number had a defined temporal pattern: increased in 2 wk and 4 wk TAC, followed by increases at 2 wk unTAC (over 4 wk TAC) that then decreased at 4 wk and 6 wk unTAC. At 2 wk unTAC, macrophage area was significantly increased and was regionally associated with CHP reactivity. Cytokine profiles in unTAC reflected a proinflammatory milieu versus the TAC-induced profibrotic milieu. Single-cell sequencing analysis of 2 wk TAC versus 2 and 6 wk unTAC revealed distinct macrophage gene expression profiles at each time point demonstrating unique macrophage populations in unTAC versus TAC myocardium. Clodronate liposome depletion at unTAC reduced CHP reactivity and decreased cathepsin K and proMMP2. We conclude that temporal changes in number and phenotype of macrophages play a critical role in both TAC-induced development and unTAC-mediated partial, but incomplete, regression of myocardial fibrosis. NEW & NOTEWORTHY Our novel findings highlight the dynamic changes in myocardial macrophage populations that occur in response to PO and after alleviation of PO. Our data demonstrated, for the first time, a potential benefit of macrophages in contributing to collagen degradation and the partial regression of interstitial fibrosis following normalization of hemodynamic load.
Keyphrases
- left ventricular
- adipose tissue
- gene expression
- single cell
- heart failure
- hypertrophic cardiomyopathy
- mitral valve
- drug delivery
- acute myocardial infarction
- machine learning
- cardiac resynchronization therapy
- skeletal muscle
- type diabetes
- big data
- spinal cord
- oxidative stress
- liver fibrosis
- coronary artery
- pulmonary hypertension
- diabetic rats
- artificial intelligence
- tissue engineering
- percutaneous coronary intervention
- drug release
- high throughput
- weight loss
- electronic health record
- congenital heart disease
- real time pcr