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ß3AR-Dependent Brain-Derived Neurotrophic Factor (BDNF) Generation Limits Chronic Postischemic Heart Failure.
Cannavo, Alessandro; Jun, Seungho; Rengo, Giuseppe; Marzano, Federica; Agrimi, Jacopo; Liccardo, Daniela; Elia, Andrea; Keceli, Gizem; Altobelli, Giovanna G; Marcucci, Lorenzo; Megighian, Aram; Gao, Erhe; Feng, Ning; Kammers, Kai; Ferrara, Nicola; Finos, Livio; Koch, Walter J; Paolocci, Nazareno.
Affiliation
  • Cannavo A; Department of Translational Medical Science (A.C., G.R., F.M., D.L., A.E., N. Ferrara), University of Naples Federico II, Italy.
  • Jun S; Center For Translational Medicine LKSOM Temple University, Philadelphia, PA (A.C., F.M., D.L., E.G., W.J.K.).
  • Rengo G; Department of Translational Medical Science (A.C., G.R., F.M., D.L., A.E., N. Ferrara), University of Naples Federico II, Italy.
  • Marzano F; Division of Cardiology, Johns Hopkins University Medical Institutions, Baltimore, MD (S.J., G.K., N.P.).
  • Agrimi J; Department of Translational Medical Science (A.C., G.R., F.M., D.L., A.E., N. Ferrara), University of Naples Federico II, Italy.
  • Liccardo D; Istituti Clinici Scientifici Maugeri IRCC- Scientific Institute of Telese Terme (BN), Italy (G.R., N. Ferrara).
  • Elia A; Department of Translational Medical Science (A.C., G.R., F.M., D.L., A.E., N. Ferrara), University of Naples Federico II, Italy.
  • Keceli G; Center For Translational Medicine LKSOM Temple University, Philadelphia, PA (A.C., F.M., D.L., E.G., W.J.K.).
  • Altobelli GG; Department of Biomedical Sciences (J.A., L.M., A.M., N.P.), University of Padova, Italy.
  • Marcucci L; Department of Translational Medical Science (A.C., G.R., F.M., D.L., A.E., N. Ferrara), University of Naples Federico II, Italy.
  • Megighian A; Center For Translational Medicine LKSOM Temple University, Philadelphia, PA (A.C., F.M., D.L., E.G., W.J.K.).
  • Gao E; Department of Translational Medical Science (A.C., G.R., F.M., D.L., A.E., N. Ferrara), University of Naples Federico II, Italy.
  • Feng N; Division of Cardiology, Johns Hopkins University Medical Institutions, Baltimore, MD (S.J., G.K., N.P.).
  • Kammers K; Department of Advanced Biomedical Sciences (G.A.A.), University of Naples Federico II, Italy.
  • Ferrara N; Department of Biomedical Sciences (J.A., L.M., A.M., N.P.), University of Padova, Italy.
  • Finos L; Department of Biomedical Sciences (J.A., L.M., A.M., N.P.), University of Padova, Italy.
  • Koch WJ; Department of Translational Medical Science (A.C., G.R., F.M., D.L., A.E., N. Ferrara), University of Naples Federico II, Italy.
  • Paolocci N; Center For Translational Medicine LKSOM Temple University, Philadelphia, PA (A.C., F.M., D.L., E.G., W.J.K.).
Circ Res ; 132(7): 867-881, 2023 03 31.
Article in En | MEDLINE | ID: mdl-36884028
ABSTRACT

BACKGROUND:

Loss of brain-derived neurotrophic factor (BDNF)/TrkB (tropomyosin kinase receptor B) signaling accounts for brain and cardiac disorders. In neurons, ß-adrenergic receptor stimulation enhances local BDNF expression. It is unclear if this occurs in a pathophysiological relevant manner in the heart, especially in the ß-adrenergic receptor-desensitized postischemic myocardium. Nor is it fully understood whether and how TrkB agonists counter chronic postischemic left ventricle (LV) decompensation, a significant unmet clinical milestone.

METHODS:

We conducted in vitro studies using neonatal rat and adult murine cardiomyocytes, SH-SY5Y neuronal cells, and umbilical vein endothelial cells. We assessed myocardial ischemia (MI) impact in wild type, ß3AR knockout, or myocyte-selective BDNF knockout (myoBDNF KO) mice in vivo (via coronary ligation [MI]) or in isolated hearts with global ischemia-reperfusion (I/R).

RESULTS:

In wild type hearts, BDNF levels rose early after MI (<24 hours), plummeting at 4 weeks when LV dysfunction, adrenergic denervation, and impaired angiogenesis ensued. The TrkB agonist, LM22A-4, countered all these adverse effects. Compared with wild type, isolated myoBDNF KO hearts displayed worse infarct size/LV dysfunction after I/R injury and modest benefits from LM22A-4. In vitro, LM22A-4 promoted neurite outgrowth and neovascularization, boosting myocyte function, effects reproduced by 7,8-dihydroxyflavone, a chemically unrelated TrkB agonist. Superfusing myocytes with the ß3AR-agonist, BRL-37344, increased myocyte BDNF content, while ß3AR signaling underscored BDNF generation/protection in post-MI hearts. Accordingly, the ß1AR blocker, metoprolol, via upregulated ß3ARs, improved chronic post-MI LV dysfunction, enriching the myocardium with BDNF. Last, BRL-37344-imparted benefits were nearly abolished in isolated I/R injured myoBDNF KO hearts.

CONCLUSIONS:

BDNF loss underscores chronic postischemic heart failure. TrkB agonists can improve ischemic LV dysfunction via replenished myocardial BDNF content. Direct cardiac ß3AR stimulation, or ß-blockers (via upregulated ß3AR), is another BDNF-based means to fend off chronic postischemic heart failure.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Myocardial Ischemia / Ventricular Dysfunction, Left / Heart Failure / Neuroblastoma Type of study: Etiology_studies Limits: Animals / Humans Language: En Journal: Circ Res Year: 2023 Document type: Article
Fulltext
Print
XML
PubMed Links
Search on Google

Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Myocardial Ischemia / Ventricular Dysfunction, Left / Heart Failure / Neuroblastoma Type of study: Etiology_studies Limits: Animals / Humans Language: En Journal: Circ Res Year: 2023 Document type: Article