Estrogen Receptor-β Agonists Modulate T-Lymphocyte Activation and Ameliorate Left Ventricular Remodeling During Chronic Heart Failure

Background: CD4(+) T cells temporally transition from protective to pathological during ischemic heart failure (HF; 8 weeks postmyocardial infarction). Cellular mechanisms mediating this shift are unknown. Methods: RNA-sequencing of cardiac CD4(+) T cells and flow cytometric analysis of immune cells was conducted. Results: RNA-sequencing of CD4(+) T cells from the failing hearts of male mice indicated activation of ER (estrogen receptor)-alpha signaling. Flow cytometric analysis showed that ER alpha in CD4(+) T cells decreases significantly at 3-day postmyocardial infarction but increases during HF. To antagonize ER alpha, we tested a novel ER beta agonist (OSU-ERb-012) to inhibit T cells and blunt left ventricular remodeling. Proliferation assays showed that OSU-ERb-012 dose-dependently inhibited proliferation and proinflammatory cytokine expression in anti-CD3/CD28 stimulated splenic T cells isolated from both the sexes. For in vivo efficacy, 10- to 12-week-old male and ovariectomized female mice were randomized at 4 weeks postmyocardial infarction and treated with either vehicle or drug (60 mg/kg per day; oral). While vehicle-treated HF mice displayed progressive left ventricular dilatation with significantly increased end-systolic and end-diastolic volumes from 4 to 8 weeks postmyocardial infarction, treatment with OSU-ERb-012 significantly blunted these changes and stopped left ventricular remodeling in both the sexes. Reduction in tibia-normalized heart and left ventricular weights, cardiomyocyte hypertrophy and interstitial fibrosis further supported these results. Additionally, OSU-ERb-012 treatment selectively inhibited cardiac, splenic, and circulating CD4(+) T cells without affecting other myeloid and lymphoid cells in the HF mice. Conclusions: Our studies indicate that ER beta agonists and OSU-ERb-012, in particular, could be used as selective immunomodulatory drugs to inhibit CD4(+) T cells during chronic HF.

Automated summary

The study identified the activation of ER-alpha signaling in CD4(+) T cells during ischemic heart failure and demonstrated the potential of using ER beta agonist OSU-ERb-012 to inhibit T cells and reduce left ventricular remodeling. Treatment with OSU-ERb-012 effectively inhibited proliferation and proinflammatory cytokine expression in T cells, leading to improved cardiac outcomes in a mouse model.