Structural aspects of antioxidant activity of flavonoids
Tipo de material:
TextoSeries ; Free Radical Biology & Medicine, 20(3), p.331-342, 1996Trabajos contenidos: - Van Acker, S.A.B.E
- Van Den Berg, D.J
- Tromp, M.J.L
- Griffioen, D.H
- Van Bennekom, W.P
- Van Der Vijgh, W.J.F
- Bast, A
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Flavonoids, a group of naturally occurring antioxidants and iron chelators, might be used as cardioprotective agents in doxorubicin-induced cardiotoxicity, which is believed to be caused by the formation of oxygen free radicals. To investigate the underlying molecular mechanism, we tested a large group of flavonoids from all major structural subclasses on their ability to inhibit doxorubicin (enzymatically)-induced and e2+/ascorbate (nonenzymatically)-induced microsomal lipid peroxidation (LPO)and to chelate Fe 2÷ . In addition, we measured half peak oxidation potentials (Ep/2). LPO inhibition data gave a good qualitative correlation with the oxidation potentials. Most flavonoids tested chelated Fe 2÷, but there were large differences in the chelating capacity. For good scavenging activity, a catechol moiety on ring B is required. The 3-OH moiety can function as a chelation site and can also be oxidized. The 3-OH group in combination with a C2 C3 double bond, increases the cavenging activity. Fe 2÷ chelation only plays a role in the LPO inhibition by less active scavengers. Chelation can then raise the activity to the level of the most active scavengers, possibly by site-specific scavenging. It can be concluded that Ep/2 values and iron chelating activity can almost completely describe the LPO inhibiting behaviour of the flavonoids.
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