Journal
PHARMACOLOGICAL RESEARCH
Volume 169, Issue -, Pages -Publisher
ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD
DOI: 10.1016/j.phrs.2021.105631
Keywords
Heart transplantation; Brain stem death; Beta-adrenoceptor; Cardiac contractility
Categories
Funding
- University of Queensland, Australia
- Prince Charles Hospital Foundation, Australia [TM2017-02, RF-04]
- Queensland Health, Australia (Bionics Project)
- Alfred Foundation, Australia
- Metro North Hospital and Health Service, Australia
- Donald and Joan Wilson Foundation, Australia
- National Health and Medical Research Council (NHMRC), Australia [GNT1145761]
- NHMRC Centre for Research Excellence for Advanced Cardiorespiratory Therapies Improving Organ Support (CRE ACTIONS) [GNT1079421]
- Griffith University Postgraduate Research Scholarship
- Prince Charles Hospital Foundation Postdoctoral Fellowship
- New Partnership for Africa's Development Planning and Coordinating Agency (NEPAD Agency)
- Wellcome Trust [107769/Z/10/Z]
- UK government
- Prince Charles Hospital Foundation
- Office of Health and Medical Research Fellowship from the Queensland Government
- Initiative to Develop African Research Leaders, IDeAL-DELTAS Africa Initiative [DEL-15-003]
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The study found that brain stem death and transplantation may impair the contractility of the donor heart, especially the right ventricle. For the donor heart, this contractile dysfunction appears to be independent of changes to beta(1)-adrenoceptor sensitivity.
Background: Heart failure is an inexorably progressive disease with a high mortality, for which heart transplantation (HTx) remains the gold standard treatment. Currently, donor hearts are primarily derived from patients following brain stem death (BSD). BSD causes activation of the sympathetic nervous system, increases endothelin levels, and triggers significant inflammation that together with potential myocardial injury associated with the transplant procedure, may affect contractility of the donor heart. We examined peri-transplant myocardial catecholamine sensitivity and cardiac contractility post-BSD and transplantation in a clinically relevant ovine model. Methods: Donor sheep underwent BSD (BSD, n = 5) or sham (no BSD) procedures (SHAM, n = 4) and were monitored for 24 h prior to heart procurement. Orthotopic HTx was performed on a separate group of donor animals following 24 h of BSD (BSD-Tx, n = 6) or SHAM injury (SH-Tx, n = 5). The healthy recipient heart was used as a control (HC, n = 11). A cumulative concentration-effect curve to (-)-noradrenaline (NA) was established using left (LV) and right ventricular (RV) trabeculae to determine beta(1)-adrenoceptor mediated potency (-logEC(50) [(-)-noradrenaline] M) and maximal contractility (Emax). Results: Our data showed reduced basal and maximal (-)-noradrenaline induced contractility of the RV (but not LV) following BSD as well as HTx, regardless of whether the donor heart was exposed to BSD or SHAM. The potency of (-)-noradrenaline was lower in left and right ventricles for BSD-Tx and SH-Tx compared to HC. Conclusion: These studies show that the combination of BSD and transplantation are likely to impair contractility of the donor heart, particularly for the RV. For the donor heart, this contractile dysfunction appears to be independent of changes to beta(1)-adrenoceptor sensitivity. However, altered beta(1)-adrenoceptor signalling is likely to be involved in post-HTx contractile dysfunction.
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