salvianolic-acid-B and cholesteryl-ester-hydroperoxide

salvianolic-acid-B has been researched along with cholesteryl-ester-hydroperoxide* in 1 studies

Other Studies

1 other study(ies) available for salvianolic-acid-B and cholesteryl-ester-hydroperoxide

Article	Year
Comparison of the inhibitory effect against copper ion-induced oxidation in rat plasma after oral administration of salvianolic acid B and its decocted solutions. Journal of medicinal food, 2013, Volume: 16, Issue:3 The effects of salvianolic acid B (Sal B) decoction on antioxidative activities were evaluated. The 2,2-diphenyl-1-picrylhydrazyl (DPPH) radical-scavenging activity, Fe(2+)-chelating activity, reducing power, and total phenolic content of the Sal B-decocted solutions did not change significantly after decoction in an aqueous solution. However, the formation of cholesteryl ester hydroperoxide (CE-OOH) in rat blood plasma containing the Sal B-decocted solutions was more effectively inhibited than that of plasma containing the Sal B solution, regardless of the decoction time. In addition, the accumulation of CE-OOH in rat plasma after oral administration of the Sal B-decocted solutions was more effectively suppressed than when the Sal B solution was administered, considering the lag time. It is likely that the decoction was partly responsible for the increased antioxidant activity in blood plasma. Therefore, the Sal B-decocted solution may contribute more to antioxidant defense in blood than a Sal B solution that is not decocted. Topics: Administration, Oral; Animals; Antioxidants; Benzofurans; Biphenyl Compounds; Chelating Agents; Cholesterol Esters; Copper; Ions; Male; Oxidation-Reduction; Phenols; Picrates; Plant Extracts; Plant Preparations; Rats; Rats, Sprague-Dawley; Salvia	2013

Article

Year

Comparison of the inhibitory effect against copper ion-induced oxidation in rat plasma after oral administration of salvianolic acid B and its decocted solutions.

Journal of medicinal food, 2013, Volume: 16, Issue:3

The effects of salvianolic acid B (Sal B) decoction on antioxidative activities were evaluated. The 2,2-diphenyl-1-picrylhydrazyl (DPPH) radical-scavenging activity, Fe(2+)-chelating activity, reducing power, and total phenolic content of the Sal B-decocted solutions did not change significantly after decoction in an aqueous solution. However, the formation of cholesteryl ester hydroperoxide (CE-OOH) in rat blood plasma containing the Sal B-decocted solutions was more effectively inhibited than that of plasma containing the Sal B solution, regardless of the decoction time. In addition, the accumulation of CE-OOH in rat plasma after oral administration of the Sal B-decocted solutions was more effectively suppressed than when the Sal B solution was administered, considering the lag time. It is likely that the decoction was partly responsible for the increased antioxidant activity in blood plasma. Therefore, the Sal B-decocted solution may contribute more to antioxidant defense in blood than a Sal B solution that is not decocted.

Topics: Administration, Oral; Animals; Antioxidants; Benzofurans; Biphenyl Compounds; Chelating Agents; Cholesterol Esters; Copper; Ions; Male; Oxidation-Reduction; Phenols; Picrates; Plant Extracts; Plant Preparations; Rats; Rats, Sprague-Dawley; Salvia

2013