Risperidone Plasma Levels, Clinical Response and Side-Effects

M. J. Schwarz; I. Spellmann; A. Müller-Arends; M. Strassnig; J. Zach; K. Weber; N. Müller; H. J. Möller; M. Riedel

doi:10.1055/s-2005-862693

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Pharmacopsychiatry 2005; 38 - 80
DOI: 10.1055/s-2005-862693

Risperidone Plasma Levels, Clinical Response and Side-Effects

MJ Schwarz ¹, I Spellmann ¹, A Müller-Arends ¹, M Strassnig ², J Zach ¹, K Weber ¹, N Müller ¹, HJ Möller ¹, M Riedel ¹

¹Klinik für Psychiatrie und Psychotherapie, Ludwig-Maximilians-Universität München, Germany
²Western Psychiatric Institute and Clinic, University of Pittsburgh Medical Center, Pennsylvania, USA

Congress Abstract

Introduction: Assessment of the relation between oral neuroleptic dose, serum drug levels and clinical response may provide important information for rational treatment decisions.

Methods: Risperidone mono-therapy was administered to 82 schizophrenia patients in a 6-week open dose clinical trial. Weekly assessments including CGI and PANSS ratings to assess psychopathology; SAS to assess medication side effects; and blood draws to quantify steady state plasma levels of Risperidone and 9-OH-Risperidone were carried out. Additionally, major CYP2D6 polymorphisms were genotyped.

Results: Mean oral dose of risperidone was 4.4±1.0mg. Mean plasma level of both risperidone and 9-OH-Risperidone together („active moiety“) was 41.6±26.6 ng/ml. There was a positive linear correlation between risperidone plasma levels and dose (r=0.308, p≤.05). Therapy non-responder (PANSS improvement <30%) showed significantly higher plasma levels (p=.032) than responder (PANSS improvement ≥30%) without higher dosages (p=.258). Patients with a duration ≥ 5 years had significantly higher plasma levels than those with a duration <5 years (p=.028). EPS and plasma levels were not correlated (r=.028; p=.843). Patients initially receiving higher oral doses of risperidone were significantly more likely to develop extrapyramidal side effects later in the trial course. Eight of the patients (9.8%) were heterozygous for the CYP2D6 polymorphism. CYP2D6 polymorphisms did not predict clinical response, but tended to predict an increase in the Risperidone/9-OH-Risperidone-Ratio (p=0.095).

Discussion: Several aspects of our study have an important implication for the clinical use:

The higher incidence of EPMS is related to a faster up-titration of Risperidone and higher plasma levels;
Non-responders to risperidone treatment showed higher plasma levels, indicating that a further increase in the daily dose is not recommended;
patients with a longer duration of illness showed higher plasma levels, although receiving the same oral dose.

The therapeutic monitoring of risperidone and 9-OH-risperidone blood levels is thus highly recommended.