Alamandin and especially melatonin attenuate pulmonary arterial hypertension induced by monocrotalin

Author:

Ayik Seyhan1ORCID,Gunata Mehmet1ORCID,Ozhan Onural1ORCID,Yildiz Azibe2ORCID,Vardi Nigar2ORCID,Sonmez Emre3ORCID,Ermis Necip3ORCID,Ates Nilay4ORCID,Kilic Ertugrul5ORCID,Noma Samir Abbas Ali6,Ulu Ahmet6ORCID,Inan Seyfullah Taha1ORCID,Acet Haci Ahmet1ORCID,Parlakpinar Hakan1ORCID

Affiliation:

1. Department of Medical Pharmacology Inonu University Malatya Turkey

2. Department of Histology and Embryology Inonu University Malatya Turkey

3. Department of Cardiology Inonu University Malatya Turkey

4. Department of Medical Pharmacology Istanbul Medipol University Istanbul Turkey

5. Department of Physiology Istanbul Medipol University Istanbul Turkey

6. Biochemistry and Biomaterials Research Laboratory, Department of Chemistry Inonu University Malatya Turkey

Abstract

AbstractBackgroundDespite the available treatments, pulmonary arterial hypertension (PAH) prognosis is poor.ObjectivesWe aimed to investigate the effects of the alamandine (ALA), melatonin (MEL), and ALA + MEL in PAH.MethodsThe rats were randomly divided into Control (n = 10), monocrotaline (MCT) (n = 12), ALA (n = 12), MEL (n = 12), and ALA + MEL (n = 12) groups. PAH was induced by MCT. The ALA, MEL, and ALA + MEL groups received 50 μg/kg/day ALA, 10 mg/kg/day MEL, and ALA + MEL, respectively, for 35 days. Echocardiographic and hemodynamic measurements and tissue analyses (morphometric, histopathological, ELISA, and western blot) were performed.ResultsMonotherapies, especially MEL, reduced the right ventricular (RV) systolic pressure. Only MEL increased the pulmonary artery acceleration time. MCT increased the RV/left ventricle (LV) + interventricular septum (IVS) ratio. While ALA and ALA + MEL slightly decreased the RV/(LV + IVS), MEL significantly restored it. MCT increased the tunica intima‐media (TIM) thickness, PCNA and α‐SMA of pulmonary arterioles, histopathological score (HS) (inflammatory infiltration etc.) of the lung, and RV. All treatments reduced the TIM thickness (especially MEL), PCNA, and α‐SMA. All treatments significantly decreased the HS of the lung; however, MEL and ALA + MEL produced greater benefits. All treatments attenuated the HS of RV. MCT caused a significant increase in lung lysyl oxidase (LOX) activity. All treatments restored the LOX; however, MEL and ALA + MEL provided greater improvement. While lung Nrf‐2 was increased in MCT‐treated rats, MEL reduced it.ConclusionALA, MEL, and ALA + MEL attenuate PAH and protect RV via antiproliferative, anti‐remodeling, antihypertrophic, anti‐inflammatory, and free radical scavenging (only MEL) capabilities. Overall, MEL produced the best outcomes.

Funder

Inönü Üniversitesi

Publisher

Wiley

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