Typical Versus Atypical Antipsychotics; Occupation of Striatal Receptors and the Appearance of Extrapyramidal Symptomatology, in Healthy Volunteers

Phase 1

• Conditions: Pharmacogenetics; Healthy
• Interventions: Drug: Risperidone; Drug: Placebo; Drug: Haloperidol

• Registration Number: NCT01259973
• Lead Sponsor: Hospital Clinic of Barcelona

Brief Summary

The purpose of this study is to determine in healthy volunteers treated with typical or atypical antipsychotics -AP-, the relationship between genetic polymorphisms in cytochrome genes CYP2D6 (\*3, \*4, \*5, \*6 and Nxn) and CYP3A5 (\*3) with antipsychotic pharmacokinetics, occupancy of striatal dopaminergic receptors and the appearance of extrapyramidal symptomatology -EPS-.

Detailed Description

Objective:

The preliminary results indicate that pharmacological factors (AP, dose and drug availability depending on cytochrome activity) are risk factors for AP-induced EPS.

In this clinical trial, the investigators will study, in healthy volunteers, the effects on pharmacokinetics, occupancy of striatal dopaminergic receptors and the appearance of EPS according to genetic polymorphisms in cytochrome genes CYP2D6 (\*3, \*4, \*5, \*6 and Nxn) and CYP3A5 (\*3). The investigators will compare a typical AP (Haloperidol) with an atypical AP (Risperidone), both of which are metabolized by CYP2D6 and CYP3A5.

Specific objectives:

* Study the relationship between genetic polymorphisms in cytochrome genes CYP2D6 (\*3, \*4, \*5, \*6 and Nxn) and CYP3A5 (\*3) and plasmatic levels of Haloperidol and Risperidone.

* Study the relationship between genetic polymorphisms in cytochrome genes CYP2D6 (\*3, \*4, \*5, \*6 and Nxn) and CYP3A5 (\*3) and the grade of occupancy of striatal dopaminergic receptors with Haloperidol and Risperidone.

* Study the relationship between plasmatic levels of Haloperidol and Risperidone and the grade of occupancy of striatal dopaminergic receptors with these two drugs.

* Study the relationship between genetic polymorphisms in cytochrome genes CYP2D6 (\*3, \*4, \*5, \*6 and Nxn) and CYP3A5 (\*3), plasmatic levels of Haloperidol and Risperidone, and the grade of occupancy of striatal dopaminergic receptors with these two drugs, with the appearance of AP-induced EPS.

Methodology:

From a cohort of 200 healthy volunteers (males and females with ages between 18-30 years), previously genotyped for CYP2D6 and CYP3A5 genes (from January to June 2010), the investigators have selected subjects depending on their metabolizer phenotype (poor metabolizers, intermediate metabolizers, extensive metabolizers and ultrarapid metabolizers) by DNA extraction from whole blood samples and SNP detection approaches.

Finally, the investigators will include the following four phenotypical groups with 6-8 subjects in each of the groups (a total of N=32 subjects, approximately):

* poor metabolizers (PM) CYP2D6\*

* poor metabolizers (PM) CYP3A5\*\*

* extensive metabolizers (EM) CYP2D6/CYP3A

* ultrarapid metabolizers (UM) CYP2D6\*

The design corresponds to a three ways cross-over randomized and double-blind trial, with a wash-out period of one week among each treatment.

Measurements of occupancy of striatal dopaminergic receptors will be done by single photon emission computed tomography -SPECT- and SEP will be measured based on the Simpson-Angus scale and actimetry.

General protocol:

One week before their participation in the trial, volunteers will undergo clinical and physical explorations (blood test, electrocardiography, urine drug screening...) and will be trained in the different tests of the study (to minimize differences regarding to experience).

During the study, participants will be treated with a single dose of an AP drug (5mg Haloperidol or 2.5mg Risperidone) or a single dose of placebo (2.5mL physiological serum).

Plasma levels will be measured at +0.5h, +1h, +2h, +4h, +6h, +8h and +12h of drug/placebo administration.

The tracer \[123I\]IBZM will be administered at +3h of drug/placebo administration and SPECT will be performed at +5h.

Status of EPS, as well as positive and negative AP-derived symptoms, will be measured at -1h and at different time frames post-drug/placebo administration, beginning at +3h and until +24h (depending on each Scale used).

Participants will be hospitalized for three complete days (separated between them by one wash-out week after each treatment) from 8.00h to 8.00h of the following day at Phase I Unit of "Hospital de Sant Pau i de la Santa Creu", in Barcelona, in order to monitor the results obtained after each treatment. During their hospitalization, participants will be given food and drink every two hours.

This clinical trial will start in February 2011 and finish in November 2011.

Study Timeline

• Study First Submitted: 2010-12-13
• Study First Submitted QC: 2010-12-14
• Study First Posted: 2010-12-15
• Status Verified: 2011-01
• Study Start: 2011-02
• Last Update Submitted: 2011-04-15
• Last Update Posted: 2011-04-18
• Primary Completion: 2011-11
• Study Completion: 2011-12

Recruitment & Eligibility

• Status: UNKNOWN
• Sex: All
• Target Recruitment: 24

Inclusion Criteria

Not provided

Exclusion Criteria

Not provided

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: CROSSOVER

Arm && Interventions

Group	Intervention	Description
Risperidone	Risperidone	-
Placebo	Placebo	-
Haloperidol	Haloperidol	-

Primary Outcome Measures

Name	Time	Method
Changes among genotypes in 24 h monitored Haloperidol and Risperidone pharmacokinetics	+ 0.5h, +1h, +2h, +4h, +6h, +8h, +12h and +24h post-treatment	Through a catheter, blood samples will be obtained at different time frames. Samples will be kept with anticoagulants and centrifuged immediately to separate the plasmatic fraction, which will be kept at -70ºC. In order to determine the concentration of Haloperidol (and reduced Haloperidol) and Risperidone (and 9-OH Risperidone), high performance liquid chromatography -HPLC- will be achieved.; A poblation-pharmacokinetic model of the two AP drugs will be designed, and drug vs. placebo treatment results will be compared.; Parameters determined: AUC, Cmax, Tmax, T(1/2), Vd, CL and MRT.
Changes from placebo in occupancy of striatal dopaminergic receptors by Haloperidol and Risperidone at 5h	+3h post-treatment: tracer injection. +5h post-treatment: image acquisition	The tracer \[123I\]IBZM, a dopaminergic antagonist, will be administered by means of intravenous injection (at +3h post-treatment) at the opposite arm from which blood samples will be obtained. Neuroimaging will be done in SPECT gamma chambers and images will be quantified comparing drug vs. placebo treatment results.; Parameters determined: Average Count Striatum and Count Occipital Cortex, Specific Uptake Ratio, D2 Occupational Receptor.; 100% of volunteers will undergo SPECT after placebo treatment and, among them, 50% after Haloperidol treatment and 50% after Risperidone treatment.
Changes from baseline in Extrapyramidal Symptomatology (EPS) at 3h, measured by Simpson-Angus Rating Scale (SARS)and Barnes Akathisia Rating Scale (BARS), and during 24 h, measured by actimetry	Heteroadministered scales will be measured at -1h pre-treatment (basal level) and at +3h. Actimetry will be measured continuosly since -1h pre-treatment until +24h	AP-induced EPS measured by: * Heteroadministered scales: * Simpson-Angus Rating Scale (SARS). Assesses drug-induced parkinsonism (tremor, hypokinesia, rigidity, and postural instability).; * Barnes Akathisia Rating Scale (BARS). Assesses drug-induced akathisia (restlessness and inability to sit still).; * Actimetry: Continuous recording of movement, in terms of count of movements per minute, by using a wrist actimeter (model AW4) fitted to the arm not used for writing.; Differences observed by comparing EPS after drug vs. placebo treatment will be considered.

Secondary Outcome Measures

Name	Time	Method
Changes from baseline in 24h prolactin kinetics	At -1h pre-treatment (basal level) and at +0.5h, +1h, +2h, +4h, +6h, +8h, +12h and +24h post-treatment	Blood samples analyzed will be the ones obtained for measuring plasmatic levels of antipsychotic drugs.; Plasmatic levels of prolactin will be measured by enzymatic immunoassay approaches.; Differences observed after drug vs. placebo treatment will be compared.
Changes from baseline in Positive and Negative Symptomatology at 3h, measured by Brief Psychiatric Rating Scale (BPRS) and Scale for the Assessment of Negative Symptoms (SANS), and at 24h, measured by Subjective Deficit Syndrome Scale (SDSS)	BPRS and SANS scales will be measured at -1h pre-treatment (basal level) and at +3h. SDSS scale will be measured at -1h pre-treatment (basal level) and at +24h	AP-induced positive/negative symptoms measured by: * Brief Psychiatric Rating Scale (BPRS). Heteroadministered and semi structured interview (20 min) to determine hostility, suspiciousness, hallucination, and grandiosity.; * Scale for the Assessment of Negative Symptoms (SANS). Heteroadministered interview (20 min) to determine affective blunting, alogia, avolition/apathy, anhedonia/asociality and disturbance of attention.; * Subjective Deficit Syndrome Scale (SDSS). Autoadministered interview (20 min) to determine emotionless.; Drug vs. placebo treatment will be compared.
Changes from baseline in anticholinergic activity through Whole Saliva Test (WST) during 8h	At -1h pre-treatment (basal level) and at +1h, +2h, +4h, +6h and +8h post-treatment	Salivette Containers (from Sarstedt) will be used to determine the saliva flow accumulated during 2 min.; Differences observed after drug vs. placebo treatment will be compared.
Changes from baseline in cardiovascular effects through Orthostatism measurement during 8h	At -1h pre-treatment (basal level) and at +1h, +2h, +4h, +6h and +8h post-treatment	In order to determine orthostatic hypotension, Systolic Arterial Pressure (SAP), Diastolic Arterial Pressure (DAP) and Cardiac frequency (CF) will be measured both after 3 min in supine position and after 3 min in erect position.; Differences observed after drug vs. placebo treatment will be compared.
Changes from baseline in sedative effects during 8h	At -1h pre-treatment (basal level) and at +1h, +2h, +4h, +6h and +8h post-treatment	AP-induced sedative effects measured by: * Psychomotricity; * Flicker-Fusion Critical Frequency (FFCF). Detection of a flickering/stable red light.; * Simple Reaction Time (SRT). Detection of a simple red light switched on/off.; * Digit Symbol Substitution Test (DSST). Measures the amount of digits substituted correctly by its corresponding symbol.; * Tapping Test (TT). Average of tappings per second.; * Pupilometry. Detect pupil's response in basal conditions.; * Visual Analog Scales (VAS). Detect agreement to a statement by indicating a position within two end-points.

Trial Locations

Locations (2)

Hospital de la Santa Creu i Sant Pau; 🇪🇸 Barcelona, Spain

Hospital Clinic of Barcelona; 🇪🇸 Barcelona, Spain