4.7 Article

Negative Inotropic Effect of BGP-15 on the Human Right Atrial Myocardium

期刊

JOURNAL OF CLINICAL MEDICINE
卷 9, 期 5, 页码 -

出版社

MDPI
DOI: 10.3390/jcm9051434

关键词

BGP-15; propranolol; atrium; heart; inotropic effect; patients

资金

  1. European Union
  2. State of Hungary
  3. University of Debrecen [GINOP-2.3.2-15-2016-00043, ED_18-1-2019-0028]
  4. Higher Education Institutional Excellence Programme of the Ministry of Innovation and Technology in Hungary, within the framework of the thematic programme of the University of Debrecen [NKFIH-1150-6/2019]

向作者/读者索取更多资源

Cardiovascular morbidity and mortality carry great socioeconomic burden worldwide that mandates the development of new, efficacious therapeutic agents with limited adverse effects. O-(3-piperidino-2-hydroxy-1-propyl) nicotinic acid amidoxime (BGP-15) is a known, well-tolerable drug candidate that exerts beneficial effects in several disease models. As BGP-15 has a significant structural similarity with propranolol, it arose that BGP-15 might also have a direct effect on the heart. Thus, in the present work, we investigated the effect of BGP-15 and propranolol on the contractility of isolated, paced, human right atrial samples (obtained from patients undergone open-heart surgery), with or without previous isoproterenol (ISO) stimulation (evoking an indirect or direct effect, respectively). We found that both BGP-15 and propranolol exerted direct as well as indirect negative inotropic effects on the atrial myocardium, reaching similar maximal response. However, BGP-15 had considerably smaller potency than propranolol regarding both types of negative inotropy. In addition, BGP-15, in contrast to propranolol, had a significantly greater indirect negative inotropic effect on samples exhibiting strong response to ISO. Moreover, the indirect negative inotropic effect of BGP-15 was significantly greater on samples derived from diabetic patients than on samples obtained from non-diabetic ones. Our results suggest that the enhanced ISO sensitivity is associated with the diabetic state, and BGP-15 exerts greater negative inotropic effect on the human atrial myocardium in both conditions (as compared to the atrial tissue that is not ISO oversensitive and/or diabetic). Additionally, the negative inotropic effects of BGP-15 and propranolol seem to be mediated by in part different molecular pathways in the atrial myocardium.

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