33. Methylenedioxy group as determinant of schisandrin
in enhancing hepatic mitochondrial glutathione in carbon
tetrachloride-intoxicated mice.
Ip SP,
Ma CY,
Che CT,
Ko KM.
Department of Biochemistry, The Hong Kong University
of Science & Technology, Clear Water Bay.
As a preliminary approach to exploring whether the methylenedioxy
group of the dibenzocyclooctadiene skeleton of schisandrins plays an important role in hepatic mitochondrial-reduced
glutathione (GSH) stimulatory activity, we examined the effects of three schisandrins, namely schisandrin
A (Sch A), schisandrin B (Sch B), and schisandrin C (Sch C), on carbon tetrachloride (CCl4) hepatotoxicity
and hepatic mitochondrial GSH status in mice. Pretreating
mice with Sch A at a daily oral dose of 1 mmol/kg for 3 days did not protect against CCl4 hepatotoxicity, whereas pretreatment with Sch B or Sch C at the same dosage
regimen produced almost complete protection. The hepatoprotection
afforded by Sch B or Sch C
pretreatment was associated with significant increases in the hepatic
mitochondrial GSH level and glutathione reductase (EC
1.6.4.2) activity. Our results indicate that the methylenedioxy
group of the dibenzocyclooctadiene skeleton of schisandrin is an important structural determinant in the
stimulation of hepatic mitochondrial GSH, particularly under conditions of CCl4
intoxication.