Therapeutic drug monitoring for optimizing amisulpride therapy in patients with schizophrenia.

6533b85dfe1ef96bd12bf238

RESEARCH PRODUCT

Therapeutic drug monitoring for optimizing amisulpride therapy in patients with schizophrenia.

Franz X. Eich Matthias J. Müller Boris Regenbogen Christoph Hiemke Sebastian Härtter

subject

Adult Male medicine.medical_specialty Dyskinesia Drug-Induced Adolescent medicine.drug_class Statistics as Topic Atypical antipsychotic Pharmacology Gastroenterology Extrapyramidal symptoms Internal medicine Germany medicine Humans Amisulpride Biological Psychiatry Aged Retrospective Studies Aged 80 and over Neurologic Examination Psychiatric Status Rating Scales Receiver operating characteristic medicine.diagnostic_test Dose-Response Relationship Drug business.industry Dopamine antagonist Middle Aged medicine.disease Psychiatry and Mental health Dose–response relationship ROC Curve Schizophrenia Therapeutic drug monitoring Schizophrenia Female medicine.symptom Amisulpride Drug Monitoring Sulpiride business medicine.drug Antipsychotic Agents

description

Amisulpride is a clinically effective antipsychotic drug in a broad dose range with low propensity for extrapyramidal symptoms (EPS). Daily doses and plasma levels of amisulpride were analyzed within a large-scale therapeutic drug monitoring (TDM) survey to find plasma level ranges for optimized treatment under naturalistic conditions. Data of 378 schizophrenic patients treated with amisulpride (100-1550 mg) were included (40% female). Amisulpride plasma levels were analyzed at steady state; assessment comprised improvement (CGI-I) and side-effects, particularly EPS. For detection of cut-off values regarding non-response or EPS, receiver operating characteristics (ROC) curves were applied and the area under the ROC curve (AUC) was calculated. Amisulpride daily doses (594+/-262 mg) and plasma levels (315+/-277 ng/ml) were significantly correlated (r=0.53; P<0.0001). Patients with non-response to amisulpride (8.9%) had significantly (P<0.05) lower plasma levels (248+/-291 ng/ml) than patients with at least moderate improvement (316+/-253 ng/ml) despite comparable amisulpride doses (628+/-253 vs. 590+/-263 mg). Patients with EPS (14.6%) had significantly (P<0.05) higher amisulpride plasma levels (377+/-290 ng/ml) than patients without EPS (305+/-274 ng/ml) despite similar doses in both groups (595+/-266 vs. 594+/-246 mg). ROC analyses revealed significant predictive properties of amisulpride plasma levels (P<0.05) for non-response (AUC=0.65+/-0.05) and EPS (AUC=0.62+/-0.05), respectively. Daily amisulpride doses did not significantly predict non-response or EPS. Optimal amisulpride plasma level values to avoid non-response and EPS were 100 or 320 ng/ml, respectively. Analysis of clinical utility revealed that blood levels must be analyzed in 7 patients until one patient benefits from the TDM procedure by avoiding non-response or EPS. Although our results were mainly explorative, TDM of amisulpride seems very useful for clinical decision making.

year	journal	country	edition	language
2005-07-28	Journal of psychiatric research

10.1016/j.jpsychires.2005.10.003 https://pubmed.ncbi.nlm.nih.gov/16324716