par Perel, James J.M.;Mendlewicz, Julien 
;Shostak, Michael;Kantor, Shepard S.J.;Glassman, Alexander Howard
Référence Neuropsychobiology, 2, 4, page (193-202)
Publication Publié, 1976
;Shostak, Michael;Kantor, Shepard S.J.;Glassman, Alexander HowardRéférence Neuropsychobiology, 2, 4, page (193-202)
Publication Publié, 1976
Article révisé par les pairs
| Résumé : | On the basis of tentative evidence obtained with 26 patients with unipolar affective illness, the variability in the response to imipramine is mostly due to interindividual differences in hydroxylating microsomal enzymes which are genetically controlled but whose activities are subject to modification by environmental factors such as overall pharmacological exposure and tobacco smoking. Additional significant pharmacodynamic variability (twofold) was found in the range of the volumes of distribution of imipramine in the patients. Clinical outcome was unequivocally related to plasma level. Unipolar nondelu- sional patients with levels less than 180 ng/ml had a low probability of recovery, while levels above 180 ng/ml were associated with a high probability of recovery. Unlike the findings of investigators working with nortriptyline, our data do not suggest an upper limit on plasma levels beyond which clinical response deteriorates. It appears that, on the basis of family studies, similar genetic properties lead to imipramine response among unipolar depressives. Whether the genetic characteristics are related to the ones controlling the pharmacodynamics will be the subject of further examination in our continuing studies. © 1976 S. Karger AG, Basel. |
