The genetic control of sparteine and debrisoquine metabolism in man with new methods of analysing bimodal distributions.

Abstract: SUMMARY Debrisoquine and sparteine tests were carried out in 215 random white British subjects. There is a high degree of correlation between the urinary 'metabolic ratios' of the two drugs. New A polymorphism has also been described for the metabolism of sparteine, an alkaloid which has been used as an anti-arrhythmic and oxytocic drug. One phenotype with a frequency of 0-05 in the German population was unable to metabolise the compound. The other phenotype produced two substances thought to result from N-… Show more

“…The metabolic ratio (MR) was calculated by dividing the % of debrisoquine excreted by the % of the 4-hydroxy metabolite excreted in urine. Poor metabolizers are usually assigned a MR > 12.6 (Evans et al, 1983).…”

Polymorphism of debrisoquine hydroxylation among Finns and Lapps.

“…The metabolic ratio (MR) was calculated by dividing the % of debrisoquine excreted by the % of the 4-hydroxy metabolite excreted in urine. Poor metabolizers are usually assigned a MR > 12.6 (Evans et al, 1983).…”

Polymorphism of debrisoquine hydroxylation among Finns and Lapps.

“…However, assessment of sparteine oxidation based on the peak area MR cannot distinguish the two genotypes within the dominant phenotype (Eichelbaum et al, 1979;Evans et al, 1983). Combined family and population data have indicated that sparteine metabolism is impaired in heterozygotes compared with homozygous dominants (Evans et al, 1983 The aim of the present study was to examine the urinary excretion pattern of sparteine and dehydrosparteines in the three genotypes.…”

“…Thus, two phenotypes are clearly defined: poor metabolizers (PM), who are homozygous for a recessive allele, and an extensive metabolizer (EM) phenotype comprising both heterozygotes and homozygous dominants (Eichelbaum et al, 1979;Evans et al, 1983). Earlier studies demonstrated coregulation of sparteine and debrisoquine oxidation (Eichelbaum et al, 1982;Inaba et al, 1983) but conflicting data have recently appeared (Evans et al, 1983;Eichelbaum & Woolhouse, 1985).…”

“…Combined family and population data have indicated that sparteine metabolism is impaired in heterozygotes compared with homozygous dominants (Evans et al, 1983 The aim of the present study was to examine the urinary excretion pattern of sparteine and dehydrosparteines in the three genotypes. Therefore, siblings and parents of 20 unrelated PM probands volunteered to take a test dose of sparteine.…”

“…Thus, two phenotypes are clearly defined: poor metabolizers (PM), who are homozygous for a recessive allele, and an extensive metabolizer (EM) phenotype comprising both heterozygotes and homozygous dominants (Eichelbaum et al, 1979;Evans et al, 1983). Earlier studies demonstrated coregulation of sparteine and debrisoquine oxidation (Eichelbaum et al, 1982;Inaba et al, 1983) but conflicting data have recently appeared (Evans et al, 1983;Eichelbaum & Woolhouse, 1985). Poor metabolism of sparteine and debrisoquine is associated with poor hydroxylation of imipramine (Br0sen et al,in preparation) and likewise the oxidation of metoprolol (Lennard et al, 1982), nortriptyline (Mellstrom et al, 1981) and desipramine (Bertilsson & Aberg-Wisted, 1983) is impaired in poor metabolizers of debrisoquine.…”

Sparteine oxidation polymorphism: a family study.

Pharmacogenetics of Antidepressant Drug Metabolism and Its Clinical Implications