The compromised viability and function of cardiovascular cells are rescued by small molecules of triazole de-rivatives (Tzs), identified as 3a and 3b, by preventing mitochondrial dysfunction. The oxidative phosphorylation improves the respiratory control rate in the presence of Tzs independently of the substrates that energize the mitochondria. The F1FO-ATPase, the main candidate in mitochondrial permeability transition pore (mPTP) formation, is the biological target of Tzs and hydrophilic F-1 domain of the enzyme is depicted as the binding region of Tzs. The protective effect of Tz molecules on isolated mitochondria was corroborated by immortalized cardiomyocytes results. Indeed, mPTP opening was attenuated in response to ionomycin. Consequently, increased mitochondrial roundness and reduction of both length and interconnections between mitochondria. In in-vitro and ex-vivo models of cardiovascular pathologies (i.e., hypoxia-reoxygenation and hypertension) were used to evaluate the Tzs cardioprotective action. Key parameters of porcine aortic endothelial cells (pAECs) oxidative metabolism and cell viability were not affected by Tzs. However, in the presence of either 1 mu M 3a or 0.5 mu M 3b the impaired cell metabolism of pAECs injured by hypoxia-reoxygenation was restored to control respiratory profile. Moreover, endothelial cells isolated from SHRSP exposed to high-salt treatment rescued the Complex I activity and the endothelial capability to form vessel-like tubes and vascular function in presence of Tzs. As a result, the specific biochemical mechanism of Tzs to block Ca2+-activated F1FO-ATPase protected cell viability and preserved the pAECs bioenergetic metabolism upon hypoxia-reoxygenation injury. Moreover, SHRSP improved vascular dysfunction in response to a high-salt treatment.

1,5-disubstituted-1,2,3-triazoles counteract mitochondrial dysfunction acting on F1FO-ATPase in models of cardiovascular diseases / Algieri, Cristina; Bernardini, Chiara; Marchi, Saverio; Forte, Maurizio; Tallarida, Matteo Antonio; Bianchi, Franca; La Mantia, Debora; Algieri, Vincenzo; Stanzione, Rosita; Cotugno, Maria; Costanzo, Paola; Trombetti, Fabiana; Maiuolo, Loredana; Forni, Monica; De Nino, Antonio; Di Nonno, Flavio; Sciarretta, Sebastiano; Volpe, Massimo; Rubattu, Speranza; Nesci, Salvatore. - In: PHARMACOLOGICAL RESEARCH. - ISSN 1096-1186. - 187:(2023), pp. 1-16. [10.1016/j.phrs.2022.106561]

1,5-disubstituted-1,2,3-triazoles counteract mitochondrial dysfunction acting on F1FO-ATPase in models of cardiovascular diseases

Bernardini, Chiara;Forte, Maurizio;Stanzione, Rosita;Cotugno, Maria;Di Nonno, Flavio;Sciarretta, Sebastiano;Volpe, Massimo;Rubattu, Speranza;
2023

Abstract

The compromised viability and function of cardiovascular cells are rescued by small molecules of triazole de-rivatives (Tzs), identified as 3a and 3b, by preventing mitochondrial dysfunction. The oxidative phosphorylation improves the respiratory control rate in the presence of Tzs independently of the substrates that energize the mitochondria. The F1FO-ATPase, the main candidate in mitochondrial permeability transition pore (mPTP) formation, is the biological target of Tzs and hydrophilic F-1 domain of the enzyme is depicted as the binding region of Tzs. The protective effect of Tz molecules on isolated mitochondria was corroborated by immortalized cardiomyocytes results. Indeed, mPTP opening was attenuated in response to ionomycin. Consequently, increased mitochondrial roundness and reduction of both length and interconnections between mitochondria. In in-vitro and ex-vivo models of cardiovascular pathologies (i.e., hypoxia-reoxygenation and hypertension) were used to evaluate the Tzs cardioprotective action. Key parameters of porcine aortic endothelial cells (pAECs) oxidative metabolism and cell viability were not affected by Tzs. However, in the presence of either 1 mu M 3a or 0.5 mu M 3b the impaired cell metabolism of pAECs injured by hypoxia-reoxygenation was restored to control respiratory profile. Moreover, endothelial cells isolated from SHRSP exposed to high-salt treatment rescued the Complex I activity and the endothelial capability to form vessel-like tubes and vascular function in presence of Tzs. As a result, the specific biochemical mechanism of Tzs to block Ca2+-activated F1FO-ATPase protected cell viability and preserved the pAECs bioenergetic metabolism upon hypoxia-reoxygenation injury. Moreover, SHRSP improved vascular dysfunction in response to a high-salt treatment.
2023
binding sites; cardiovascular diseases; f(1)f(o)-atpase; mitochondria; permeability transition pore; triazoles
01 Pubblicazione su rivista::01a Articolo in rivista
1,5-disubstituted-1,2,3-triazoles counteract mitochondrial dysfunction acting on F1FO-ATPase in models of cardiovascular diseases / Algieri, Cristina; Bernardini, Chiara; Marchi, Saverio; Forte, Maurizio; Tallarida, Matteo Antonio; Bianchi, Franca; La Mantia, Debora; Algieri, Vincenzo; Stanzione, Rosita; Cotugno, Maria; Costanzo, Paola; Trombetti, Fabiana; Maiuolo, Loredana; Forni, Monica; De Nino, Antonio; Di Nonno, Flavio; Sciarretta, Sebastiano; Volpe, Massimo; Rubattu, Speranza; Nesci, Salvatore. - In: PHARMACOLOGICAL RESEARCH. - ISSN 1096-1186. - 187:(2023), pp. 1-16. [10.1016/j.phrs.2022.106561]
File allegati a questo prodotto
File Dimensione Formato  
Algieri_1,5-disubstituted_2023.pdf

accesso aperto

Note: lavoro pubblicato
Tipologia: Versione editoriale (versione pubblicata con il layout dell'editore)
Licenza: Creative commons
Dimensione 8.97 MB
Formato Adobe PDF
8.97 MB Adobe PDF

I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.

Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1677871
Citazioni
  • ???jsp.display-item.citation.pmc??? 5
  • Scopus 9
  • ???jsp.display-item.citation.isi??? 10
social impact