Catecholamine-Dependent β-Adrenergic Signaling in a Pluripotent Stem Cell Model of Takotsubo Cardiomyopathy

Research output: Contribution to journalResearch articleContributedpeer-review

Contributors

  • Thomas Borchert - , University of Göttingen (Author)
  • Daniela Hübscher - , University of Göttingen (Author)
  • Celina I. Guessoum - , University of Göttingen (Author)
  • Tuan Dinh D. Lam - , University of Göttingen (Author)
  • Jelena R. Ghadri - , University of Zurich (Author)
  • Isabel N. Schellinger - , University of Göttingen (Author)
  • Malte Tiburcy - , University of Göttingen (Author)
  • Norman Y. Liaw - , University of Göttingen (Author)
  • Yun Li - , University of Göttingen (Author)
  • Jan Haas - , Heidelberg University  (Author)
  • Samuel Sossalla - , University of Göttingen, University of Regensburg (Author)
  • Mia A. Huber - , University of Zurich (Author)
  • Lukas Cyganek - , University of Göttingen (Author)
  • Claudius Jacobshagen - , University of Göttingen (Author)
  • Ralf Dressel - , University of Göttingen (Author)
  • Uwe Raaz - , University of Göttingen (Author)
  • Viacheslav O. Nikolaev - , University Hospital Hamburg Eppendorf (Author)
  • Kaomei Guan - , Institute of Pharmacology and Toxicology, TUD Dresden University of Technology (Author)
  • Holger Thiele - , University of Cologne (Author)
  • Benjamin Meder - , Heidelberg University  (Author)
  • Bernd Wollnik - , University of Göttingen (Author)
  • Wolfram Hubertus Zimmermann - , University of Göttingen (Author)
  • Thomas F. Lüscher - , University of Zurich (Author)
  • Gerd Hasenfuss - , University of Göttingen (Author)
  • Christian Templin - , University of Zurich (Author)
  • Katrin Streckfuss-Bömeke - , University of Göttingen (Author)

Abstract

Background Takotsubo syndrome (TTS) is characterized by an acute left ventricular dysfunction and is associated with life-threating complications in the acute phase. The underlying disease mechanism in TTS is still unknown. A genetic basis has been suggested to be involved in the pathogenesis. Objectives The aims of the study were to establish an in vitro induced pluripotent stem cell (iPSC) model of TTS, to test the hypothesis of altered β-adrenergic signaling in TTS iPSC-cardiomyocytes (CMs), and to explore whether genetic susceptibility underlies the pathophysiology of TTS. Methods Somatic cells of patients with TTS and control subjects were reprogrammed to iPSCs and differentiated into CMs. Three-month-old CMs were subjected to catecholamine stimulation to simulate neurohumoral overstimulation. We investigated β-adrenergic signaling and TTS cardiomyocyte function. Results Enhanced β-adrenergic signaling in TTS-iPSC-CMs under catecholamine-induced stress increased expression of the cardiac stress marker NR4A1; cyclic adenosine monophosphate levels; and cyclic adenosine monophosphate–dependent protein kinase A–mediated hyperphosphorylation of RYR2-S2808, PLN-S16, TNI-S23/24, and Cav1.2-S1928, and leads to a reduced calcium time to transient 50% decay. These cellular catecholamine-dependent responses were mainly mediated by β1-adrenoceptor signaling in TTS. Engineered heart muscles from TTS-iPSC-CMs showed an impaired force of contraction and a higher sensitivity to isoprenaline-stimulated inotropy compared with control subjects. In addition, altered electrical activity and increased lipid accumulation were detected in catecholamine-treated TTS-iPSC-CMs, and were confirmed by differentially expressed lipid transporters CD36 and CPT1C. Furthermore, we uncovered genetic variants in different key regulators of cardiac function. Conclusions Enhanced β-adrenergic signaling and higher sensitivity to catecholamine-induced toxicity were identified as mechanisms associated with the TTS phenotype.

Details

Original languageEnglish
Pages (from-to)975-991
Number of pages17
JournalJournal of the American College of Cardiology
Volume70
Issue number8
Publication statusPublished - 22 Aug 2017
Peer-reviewedYes

External IDs

PubMed 28818208

Keywords

Keywords

  • broken heart syndrome, catecholamine, electrical activity, iPSC cardiomyocytes, lipotoxicity, TTS pathogenesis