http://www.cnr.it/ontology/cnr/individuo/prodotto/ID293918

Mitochondria and Nitric Oxide: Chemistry and Pathophysiology (Articolo in rivista)

Type

Articolo in rivista (Classe)
Prodotto della ricerca (Classe)

Label

Mitochondria and Nitric Oxide: Chemistry and Pathophysiology (Articolo in rivista) (literal)

Anno

2012-01-01T00:00:00+01:00 (literal)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#doi

10.1007/978-94-007-2869-1_4 (literal)

Alternative label

Sarti, Paolo; Arese, Marzia; Forte, Elena; Giuffre, Alessandro; Mastronicola, Daniela (2012)
Mitochondria and Nitric Oxide: Chemistry and Pathophysiology
in Advances in experimental medicine and biology
(literal)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#autori

Sarti, Paolo; Arese, Marzia; Forte, Elena; Giuffre, Alessandro; Mastronicola, Daniela (literal)

Pagina inizio

75 (literal)

Pagina fine

92 (literal)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#numeroVolume

942 (literal)

Rivista

Advances in experimental medicine and biology (Rivista)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#pagineTotali

18 (literal)

Note

ISI Web of Science (WOS) (literal)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#affiliazioni

Sapienza University Rome; Consiglio Nazionale delle Ricerche (CNR) (literal)

Titolo

Mitochondria and Nitric Oxide: Chemistry and Pathophysiology (literal)

Abstract

Cell respiration is controlled by nitric oxide (NO) reacting with respiratory chain complexes, particularly with Complex I and IV. The functional implication of these reactions is different owing to involvement of different mechanisms. Inhibition of complex IV is rapid (milliseconds) and reversible, and occurs at nanomolar NO concentrations, whereas inhibition of complex I occurs after a prolonged exposure to higher NO concentrations. The inhibition of Complex I involves the reversible S-nitrosation of a key cysteine residue on the ND3 subunit. The reaction of NO with cytochrome c oxidase (CcOX) directly involves the active site of the enzyme: two mechanisms have been described leading to formation of either a relatively stable nitrosyl-derivative (CcOX-NO) or a more labile nitrite-derivative (CcOX-NO2-). Both adducts are inhibited, though with different K-I; one mechanism prevails on the other depending on the turnover conditions and availability of substrates, cytochrome c and O-2. SH-SY5Y neuroblastoma cells or lymphoid cells, cultured under standard O-2 tension, proved to follow the mechanism leading to degradation of NO to nitrite. Formation of CcOX-NO occurred upon rising the electron flux level at this site, artifi cially or in the presence of higher amounts of endogenous reduced cytochrome c. Taken together, the observations suggest that the expression level of mitochondrial cytochrome c may be crucial to determine the respiratory chain NO inhibition pathway prevailing in vivo under nitrosative stress conditions. The putative patho-physiological relevance of the interaction between NO and the respiratory complexes is addressed. (literal)

Prodotto di

Autore CNR

ALESSANDRO GIUFFRE' (Unità di personale interno)
DANIELA MASTRONICOLA (Unità di personale esterno)
PAOLO SARTI (Persona)

Insieme di parole chiave

Keywords of "Mitochondria and Nitric Oxide: Chemistry and Pathophysiology" (Insieme di parole chiave)

Incoming links:

Prodotto

Autore CNR di

ALESSANDRO GIUFFRE' (Unità di personale interno)
DANIELA MASTRONICOLA (Unità di personale esterno)
PAOLO SARTI (Persona)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#rivistaDi

Advances in experimental medicine and biology (Rivista)

Insieme di parole chiave di

Keywords of "Mitochondria and Nitric Oxide: Chemistry and Pathophysiology" (Insieme di parole chiave)

data.CNR.it