Pipamperone Population Pharmacokinetics Related to Effectiveness and Side Effects in Children and Adolescents

The study population consisted of two samples. The first sample included children and adolescents who were prospectively enrolled in a Dutch multicenter observational trial (SPACe, NTR6050). Inclusion criteria were: age 6–18 years, documented clinical diagnosis of autism spectrum disorder according to the Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition [23] or Fifth Edition [24] and comorbid behavioral problems, and treatment with pipamperone. Exclusion criteria were: type 1 or 2 diabetes mellitus, congenital or acquired syndrome associated with changes in appetite, body weight or lipid profile (e.g., Prader Willi), treatment with another antipsychotic within the last 6 months, or known Long QT syndrome. Eligible patients were treated in an inpatient or outpatient setting in one of the seven participating centers in the south-west region of the Netherlands (two academic tertiary care centers and five psychiatric secondary care centers). Subjects were prescribed flexible pipamperone dosages once or twice daily, as part of routine clinical care by the treating physician. Pipamperone was prescribed as a tablet formulation or oral solution. Patients were recruited between August 2016 and May 2018. All patients and/or their legal representatives gave written informed consent before entering the study. The study was approved by the Medical Ethics Committee of the Erasmus Medical Centre, the Netherlands (number MEC 2016-124).

The second sample consisted of children and adolescents of whom pipamperone concentrations had been measured as part of the routine therapeutic drug monitoring (TDM) service of the Department of Child and Adolescent Psychiatry, Psychosomatics and Psychotherapy at the University Hospital of Wuerzburg, Germany. Subjects were treated at this clinic or at associated clinics for child and adolescent psychiatry within the competence network of TDM in child and adolescent psychiatry, which is described elsewhere [25]. Patients were prescribed flexible dosages of pipamperone as a tablet or oral solution, being administered once up to five times daily. The pipamperone samples were collected between June 2008 and February 2015 in patients with various psychiatric diagnoses. The Medical Ethics Committee of the University of Wuerzburg approved the study (study number 27/04) and waived informed consent, as drug concentrations were measured as part of routine care. Both studies were conducted in accordance with the Declaration of Helsinki.

In the Dutch trial, a total of six pipamperone drug concentrations per subject were collected at random time points on two separate days during a 6-month follow-up with 3–6 months in between sampling. The time between two samples was at least 1 h. Samples were collected with venipuncture and the dried blood spot (DBS) method. The time of sampling, time of last pipamperone intake, the pipamperone dosages, and comedication during follow-up were recorded. Both samples in steady state and non-steady state were collected. The Dutch samples were analyzed using previously validated, ultra-high performance liquid chromatography-mass spectrometry methods for plasma and DBS [26‐28]. The lower limit of quantification (LLOQ) was 1.5 µg/L. The accuracy of the quality-control samples was well below a limit of relative standard deviation of 15% and the intra- and inter-assay imprecision was less than 15% during the study period.

Within the German TDM service, samples were collected with venipuncture in the morning before the first pipamperone dosage of that day (trough concentrations) [21]. The pipamperone dosage and administration time (morning, midday, evening) were reported on the request form. Only concentrations measured in steady state were included for analyses, as for non-steady state samples previous dosages were not known. The German samples were analyzed with a validated serum high-performance liquid chromatography-ultraviolet (HPLC–UV) method for plasma. The LLOQ was 8 µg/L. The method was linear in a range of 2–1050 µg/L (r² = 0.99952). Concentrations below the LLOQ were excluded, as for these no quantification of the plasma concentration was provided.

In the Dutch trial, measures of clinical effectiveness and side effects were collected at baseline and prospectively during the 6-month follow-up (at 6 months and for a subset of patients at 1 and 3 months). Clinical effectiveness was measured by the Clinical Global Impression (CGI) Scale [29]. This scale describes the severity of psychopathology (CGI-S) and its improvement (CGI-I) by seven categories, rated by the treating physician. The CGI-S describes the severity of illness relative to the physicians’ experience with patients with the same diagnosis: 0 = not assessable; 1 = normal; 2 = borderline; 3 = mildly ill; 4 = moderately ill; 5 = markedly ill; 6 = severely ill; 7 = extremely ill. The CGI-I rates the improvement in comparison to the original medication-naive state of symptoms: 0 = not assessable, 1 = very much better, 2 = much better, 3 = moderately better, 4 = unchanged, 5 = minimally worse, 6 = much worse. Extrapyramidal symptoms were measured with the Abnormal Involuntary Movement Scale (AIMS) (completed by the treating physician or researcher) [29] and sleepiness with the Epworth Sleepiness Scale (completed by parents) [30]. Biochemical laboratory check-ups were performed at baseline, after 6 months, and for a subset of children at 3 months, and included renal function, liver function, fasting glucose, glycosylated hemoglobin, prolactin, cholesterol, fatty acids, and albumin. During follow-up, medication adherence was measured with questionnaires (Medication Adherence Rating Scale, MARS-5 [31], completed by parents, and a visual analog scale, completed by parents and treating physician) and during the last month of follow-up with an electronic monitoring system (MEMS^©) [32]. Weight and height were measured at baseline, at the time of blood sampling and, for a subset of children, after 1 month of follow-up.

At the German TDM service, the following information was recorded on the request form at the time of sampling: renal dysfunction, hepatic dysfunction, smoking status, current infection, comedication, CGI-S, CGI-I, and side effects with the Udvalg for Kliniske Undersøgelser Side Effect Rating Scale [33]. The Udvalg for Kliniske Undersøgelser Side Effect Rating Scale rates the severity of side effects with the following categories: 0 = no side effects; 1 = mild, 2 = moderate, and 3 = severe. The nature of the side effects was also recorded and classified as follows: sedation, dermatological, tension, salivation (more/less), accommodation disorder, polydipsia, delirium, EPS, cardiovascular, gastrointestinal, urogenital, other.

Pharmacokinetic analysis was performed by non-linear mixed-effects modeling using NONMEM^® Version 7.4.2 (FOCE + I; ICON Development Solutions, Ellicott City, MD, USA) and PsN^® Version 4.7.0. Pirana^® software version 2.9.7 was used as an interface between NONMEM^® and R (version 3.4.4).

The medians with 25th–75th percentiles of measured trough concentrations were correlated with CGI-I, EPS, and sedation. As trough pipamperone concentrations were not available for all Dutch patients, individual trough concentrations were also predicted for all patients, next to 24-h area under the concentration–time curves (AUC_24h). These pharmacokinetic parameters were also correlated to CGI-I, EPS, and sedation. A subject was considered a responder when the CGI-I was rated “very much better”, “much better”, or “moderately better”, and a non-responder when another score was given (except from “not assessable”). Extrapyramidal symptoms were scored positive when at least two times “mild” or one time “moderate” in the first seven items had been filled in on the AIMS (Dutch patients), or when “EPS” was filled in as a side effect on the application form (German patients). Sedation was considered as a score ≥ 1 on the Epworth Sleepiness Scale (Dutch patients) or as “sedation” being filled in as side effect on the application form (German patients). The pipamperone trough concentration, predicted trough concentration, and predicted AUC_24h at the time of the first response or side effect (EPS and sedation) was used for the analyses. In this analysis, efficacy was accepted as an endpoint regardless of the time interval since the initiation of treatment (but within the study period). If no response or side effect was observed, the highest concentration during the follow-up was used. Laboratory findings were compared with age- (and if applicable sex-) specific reference values as used in the Erasmus MC, University Medical Center Rotterdam in July 2019 [39]. The Mann–Whitney U test was used to compare trough concentrations and AUC_24h between groups. The Fisher’s Exact test was used to compare proportions. A p value < 0.05 was considered significant. Graphpad Prism 5 (GraphPad Software, La Jolla, CA, USA) was used for the analyses.

Pipamperone concentrations using a twice-daily 30-mg dosing regimen were predicted for a patient of 25, 50, and 75 kg during a 12-h time interval. After graphical inspection, a mg/kg dosage was chosen for optimal attainment of the concentration range associated with response based on pharmacodynamic analyses. This mg/kg dosage was evaluated with additional predictions for a patient of 25, 50, and 75 kg. The population predictions were used as means with a 95% confidence interval based on 1000 simulations of individual predictions.

Predicted concentrations with 95% confidence intervals using a twice-daily 30-mg dosing scheme in steady state for a patient of 25 kg, 50 kg, and 75 kg are shown in Fig. 4a. The means (95% confidence intervals) of the predicted pipamperone trough concentrations (population prediction) after a 30-mg dose were 163.2 (67.3–268.9) µg/L for a patient of 25 kg, 103.9 (49.0–167.2) µg/L for a patient of 50 kg, and 79.3 (38.4–124.4) µg/L for a patient of 75 kg. The same predictions were performed with a 0.6-mg/kg dosage in a twice-daily dosing scheme, showing less variability in pipamperone concentrations and better attainment of the pipamperone trough concentration range that was found to be associated with response (Fig. 4b). The means (95% confidence intervals) of the predicted pipamperone trough concentrations (population prediction) after a 0.6-mg/kg dosage were 81.6 (33.6–134.5) µg/L for a patient of 25 kg, 103.9 (49.0–167.2) µg/L for a patient of 50 kg, and 119.0 (57.6–186.7) µg/L for a patient of 75 kg.