Title: Zeldox
1Zeldox
- First Line in Schizophreniaand Bipolar Mania
2Contents
- General considerations
- Ziprasidone Receptor profile
- Zeldox in Schizophrenia
- Zeldox in Bipolar Mania
- Pharmacokinetics and Dosing
- Switching to Zeldox
3General considerations
4Aetiology neuropathology of schizophrenia
current understanding
- Multiple genetic loci may be involved1
- Life events may be associated with onset2
- Biochemical theories dopamine and glutamate
hypotheses3,4 - Aberrations in cerebral structure identified5
- Neurodevelopmental hypothesis genetic and
environmental factors interact to affect brain
development with psychosis emerging in early
adulthood6 - Recent neuroimaging studies demonstrate a
progressive component6 - Effective treatment at first onset may improve
outcomes7
- McDonald C, Murphy KC. Psychiatr Clin North Am.
200326(1)41-63. - Castine MR. et al. J Psychiatr Res.
199832(5)283-8. - Seeman P. Synapse. 19871(2)133-52.
- Goff DC, Coyle JT. Am J Psych. 2001158(9)1367-77
. - Lawrie SM, Abukmei SS. Br J Psych.
1998172110-20. - Jarskog LF. et al. Ann Rev Med. 20075849-61.
- Lieberman JA. J Clin Psych. 199960 Suppl129-12.
5Schizophrenia opportunities for earlier
intervention
Timeline of Patient Presentations
Progression of symptoms
Functional decline begins
Behavioural changes and incipient delusions
0 months
44 months
12 months
25 months
7 months
Onset of experiential changes
First wave of presentation
Second wave of presentation
Schizophrenia diagnosis
Schizotaxia period
Adapted from Bota RG, et al. CNS Spectr.
200510(12)937-42.
6Neurophysiology of schizophrenia dopamine
pathways
a) Nigrostriatal system gt movement
control b) Mesolimbic system gt positive
symptoms of psychosis c) Mesocortical system
gt negative/cognitive symptoms of
psychosis d) Tuberoinfundibular system
gt prolactin secretion
Basal Ganglia
a
c
Nucl. accumbens
b
Substantia nigra
Hypothalamus
d
Tegmentum
Adapted from Stahl SM. Essential
psychopharmacology. Cambridge University Press
20002nd edn375.
7Major serotonergic pathways
Neocortex Anxiolytic andantidepressant effects
Basal ganglia Control movements (akathisia,
agitation) and relief obsessive-compulsive
behavior
Raphe Nucleus
Hypothalamus Regulates/dampen appetiteand eating
behavior
Limbic system Involved in agitation, anxiety and
panic reactions
Brainstem Regulates sleep and dampen sexual
response
Adapted from Stahl SM. Essential
psychopharmacology neuroscientific basis and
practical application. Cambridge University Press
20002nd edn182.
8Actions of antipsychotic agents
Stahl SM. Essential Psychopharmacology.
2000402-406, 414-24.
9Factors that influence patient compliance to
medication
Treatment-Related Factors
Patient-Related Factors
Side effects Route of administration Pattern of
dosing Length of treatment Costs of
treatment Polypharmacy
Psychopathology Cognitive impairment Age Co-morbid
ity Gender
COMPLIANCE
Physician-Related Factors
Environment-Related Factors
Following accepted treatment guidelines Belief in
treatment Doctor-patient relationship Aftercare
management Provision of information
Social support Financial support Attitude toward
treatment Supervision of treatment Social rank of
illness Location of treatment provision
Adapted from Fleischhacker WW, et al. J Clin
Psychiatry. 200364 Suppl 1610-3.
10Zeldox Receptor profile
11Ziprasidone a distinct receptor profile Relative
receptor binding affinities of atypical
antipsychotics
Clozapine
Risperidone
Ziprasidone
H1
D1
D2
D1
D2
5-HT1A
H1
?1
D2
?1
5-HT1A
5-HT1D
5-HT2C
5-HT1D
H1
5-HT2C
5-HT1D
5-HT2A
5-HT2C
5-HT2A
5-HT2A
?1
Olanzapine
Quetiapine
Aripiprazole
?1
D1
D2
5-HT2C
D1
5-HT1A
D2
H1
5-HT1A
5-HT2A
H1
5-HT1D
5-HT2A
5-HT1A
5-HT2A
?1
?1
H1
5-HT2C
D2
Farah A. Primary Care Companion J Clin
Psychiatry. 20057268-74.
12Ziprasidone potential clinical implications of
receptor profile
Treatment of Positive and Negative Symptoms1
with the Highest 5HT2A/D2 Receptor Affinity
Ratio in Class2
- Agonist of 5-HT1A receptors for relief of
anxiety and depression2,4
D2
5-HT1A
- Antagonist of 5-HT2C receptors for predicted
cognitive improvements2
5-HT2C
- Low affinity for H1 receptors for low sedation
and weight gain3,4
Relative Receptor Affinity6
- 5-HT/noradrenaline (NA) reuptake inhibition -
unique amongst atypical antipsychotics - for
possible antidepressive action2,5
5-HT2A
5-HT1D
?1
- Negligible affinity for M1 muscarinic receptors
- low propensity for cognitive impairment3
H1
Measured in vitro
1. Daniel DG, et al. Neuropsychopharmacology.
199920491-505. 2. Stahl SM, Shayegan DK. J Clin
Psychiatry. 200364 Suppl 19S6-12. 3. Finkel S.
J Am Geriatr Soc. 2004 Dec52 Suppl 12S258-65.
4. Shayegan DK, Stahl SM. CNS Spectr. 2004
Oct96-14. 5. Schmidt AW, et al. Eur J
Pharmacol. 2001 Aug 17425(3)197-201. 6. Farah
A. Primary Care Companion J Clin Psychiatry.
20057268-74.
13Zeldox in Schizophrenia
14Ziprasidone vs placebo (6-week study)
- Evaluate efficacy, safety, and tolerability of
ziprasidone in schizophrenia and schizoaffective
disorder
- Double-blind, short-term (6-week), fixed-dose,
placebo-controlled, multicentre study - Patients were hospitalised with acute
exacerbation of chronic or subchronic
schizophrenia or schizoaffective disorder - All patients had a minimum duration of disease of
6 months and had been hospitalised within the
previous 4 weeks
- Patients were randomised to receive
- Placebo (N92)
- Ziprasidone 80mg/day (given as 40mg BID) (N106)
- Ziprasidone 160mg/day (given as 80mg BID) (N104)
- 80mg/day for Days 1 and 2, then 160mg/day for
remainder of study
- PANSS total score, PANSS negative subscale score,
BPRSd total score, BPRSd core items score,
CGI-S, and CGI-I
Daniel DG, et al. Neuropsychopharmacology.
199920491-505.
15Efficacy in overall psychopathologysignificant
improvement as early as week 1 Ziprasidone vs
placebo (6-week study)
PANSS Total Score
0
-5
Improvement
Mean Change from Baseline (LOCF)
-10
-15
-20
0
1
2
3
4
5
6
Weeks
PANSS Positive and Negative Syndrome Scale.
LOCF Last Observation Carried Forward.
Plt0.05, Plt0.001 vs placebo
Daniel DG, et al. Neuropsychopharmacology.
199920491-505.
16Significant symptom improvement as early as week
1 Ziprasidone vs placebo (6-week study)
BPRSd Core Items Score
Ziprasidone 80mg/day (N104)
Improvement
Mean Change from Baseline (LOCF)
0
1
2
3
4
5
6
Weeks
BPRSd Brief Psychiatric Rating Scale Core Items
Score. LOCF Last Observation Carried Forward.
Plt0.05, Plt0.001 vs placebo
Daniel DG, et al. Neuropsychopharmacology.
199920491-505.
17Efficacy in negative symptomssignificant
improvement as early as week 1 Ziprasidone vs
placebo (6-week study)
PANSS Negative Subscale Score
Ziprasidone 80 mg/day (N104)
Improvement
Mean Change from Baseline (LOCF)
0
1
2
3
4
5
6
Weeks
PANSS Positive and Negative Syndrome Scale.
LOCF Last Observation Carried Forward.
Plt0.05, Plt0.001 vs placebo
Daniel DG, et al. Neuropsychopharmacology.
199920491-505.
18Efficacy in depressive symptomssignificant
improvement at 160mg/day Ziprasidone vs placebo
(6-week study)
Patients with a Baseline MADRS Score 14
0
-1
-2
-3
-2.9
-3.1
-4
Change in MADRS Score from Baseline
-5
Placebo (N54)
-6
-7
-7.5
-8
Week 6
MADRS Montgomery Åsberg Depression Rating
Scale Plt0.05 vs placebo. Associated with
schizophrenia
Daniel DG, et al. Neuropsychopharmacology.
199920491-505.
19Efficacy in symptoms of cognitive
impairment Significant improvement by week
1 Ziprasidone vs placebo (6-week study)
PANSS Cognition Subscale
0
-1
-2
Improvement
Change from Baseline
-3
Placebo (N91)
-4
-5
0
1
2
3
4
5
6
Weeks
PANSS Positive and Negative Syndrome Scale.
Plt0.05, Plt0.01 vs baseline.
Pfizer Inc., Data on file.
20Relapse can have serious consequences !
Kane JM. CNS Spectr. 20071210(Suppl 17)21-6.
21Ziprasidone vs placebo (ZEUS 1-year relapse
prevention study)
- Prospective evaluation of
- The efficacy of ziprasidone in the prevention of
relapse in patients with stable, chronic
schizophrenia
- Double-blind, parallel group, placebo controlled,
randomised - 294 inpatients with chronic schizophrenia
- Patients were assigned fixed daily doses of
ziprasidone 40mg, 80mg, or 160mg/day, or placebo
for 1 year - Patients were immediately withdrawn if they met
criteria for impending relapse
- Patients assigned to 160mg/day were given
80mg/day for 2 days, then 160mg/day for the
remainder of the study
- Primary efficacy measures
- Time to impending relapse
Arato M, et al. Int Clin Psychopharmacol.
200217207-15.
22Long-term efficacy in overall psychopathology red
uced rate of relapse ziprasidone vs placebo
(ZEUS 1-year relapse prevention study)
Placebo (N71)Ziprasidone 40mg/day
(N71) Ziprasidone 80mg/day (N68) Ziprasidone
160mg/day (N67)
Proportion Free of Impending Relapse
0
10
20
30
40
50
52
Weeks
Plt0.01, Plt0.001 vs placebo at 1 year.
Overall log-rank P value0.0001.
Arato M, et al. Int Clin Psychopharmacol.
200217207-15.
23MOZART ziprasidone vs clozapine in
treatment-resistant/intolerant schizophrenia 18-we
ek double-blind study
- Double-blind, multicentre comparison of the
efficacy and tolerability of ziprasidone vs
clozapine in schizophrenic patients resistant
and/or intolerant to antipsychotic therapy
Sacchetti E, et al. Presented at the 159th
American Psychiatric Association Annual Meeting.
2006 May 20-25 Toronto, Canada poster.
24MOZART overall psychopathology and severity of
illness 18-week double-blind study
Primary Outcome Mean Change in PANSS Total
Score (LOCF)
Primary Outcome Mean Change in CGI-S Score
(LOCF)
120
6
110
5.5
100
Mean Score
Mean Score
5
90
4.5
80
70
4
0
2
4
6
8
10
12
14
16
18
0
2
4
6
8
10
12
14
16
18
Study Week
Study Week
PANSS Positive and Negative Syndrome Scale.
CGI-S Clinical Global Impression of Severity.
LOCF Last Observation Carried Forward.
Sacchetti E, et al. Presented at the 159th
American Psychiatric Association Annual Meeting.
2006 May 20-25 Toronto, Canada poster..
25Ziprasidone vs clozapine PANSS responder
rates 18-week double-blind study
97.8
100
90
77.8
80
67.6
70
54.8
60
PANSS Responders ()
50
40
30
20
N45
N45
N71
N73
10
0
ITT-Completers (OC)
ITT-LOCF
PANSS Positive and Negative Syndrome Scale. ITT
Intent-to-treat. Baseline-to-end point
reduction in PANSS total score 20. Baseline
values were 108.5 for ziprasidone and 106.6 for
clozapine. Observed cases. Plt0.007. vs
clozapine
Sacchetti E, et al. Presented at the 159th
American Psychiatric Association Annual Meeting.
2006 May 20-25 Toronto, Canada poster..
26Ziprasidone vs Clozapine comparable or greater
improvements in cognition 18-week randomised,
double-blind study
Trail Making Test Parts A and B
180
160
ziprasidone Trails B
140
clozapine Trails B
120
100
Mean Time to Completion (sec)
80
60
ziprasidone Trails A
clozapine Trails A
40
20
0
Baseline
Week 12
Week 18
Note. Observed cases only unadjusted means
Harvey PD, et al. Schizophrenia Res. 2007.
(doi10.1016/j.schres.2007.11.014).
27Low discontinuation rates vs placebo Ziprasidone
vs placebo (1-year study)
Discontinued Due to Adverse Event
50
40
30
Patients ()
20
15
10
10
7
10
0
placebo (N71)
ziprasidone 40mg/day (N72)
ziprasidone160mg/day (N67)
ziprasidone80mg/day (N68)
Arato M, et al. Int Clin Psychopharmacol.
200217(5)207-15.
28Metabolic Effects
29Metabolic adverse events
Risk factors and monitoring recommendations
- Risk factors for cardiovascular disease are more
common in people with schizophrenia than in the
general population and may be compounded by some
atypicals, including
- weight gain/obesity
- diabetes
- dyslipidaemia
- Patients should be monitored at baseline and
regularly thereafter for possible metabolic side
effects of atypical antipsychotics - Consider switching medication if it is causing
excessive weight gain, diabetes or other
metabolic side effects
De Hert M.et al. Int Clin Psychopharmacol 200621
Suppl2S11-5. American Diabetes Association.
Diabetes Care. 200427596-601. Tschoner A, et
al. Int J Clin Pract. 2007611356-70.
30Estimated weight gain after 10 weeks of
antipsychotic therapy Meta-analysis of published
data
Placebo
6
Conventional antipsychotics
Novel antipsychotics
5
Non-pharmacologic control
4
3
2
95 Confidence Interval for Weight Change (kg)
1
0
-1
-2
-3
Placebo
Clozapine
Molindone
Ziprasidone
Haloperidol
Thioridazine/Mezoridazine
Olanzapine
Fluphenazine
Risperidone
Polypharmacy
Sertindole
Chlorpromazine
Non-pharmacologic control
Allison DB, et al. Am J Psychiatry.
19991561686-96.
31One-year weight gain while on antipsychotic
treatment Review of long-term clinical trials
Mean Change from Baseline Weight
14
14
olanzapine (12.517.5mg) olanzapine (all
doses) quetiapine risperidone ziprasidone aripipra
zole
12
12
10
10
8
8
Change from baseline weight (kg)
6
6
4
4
2
2
0
0
52
48
44
40
36
32
28
24
20
16
12
8
4
0
0
Weeks
Casey DE. Am J Med. 2005118(suppl 2)S15-22.
32Ziprasidone the only atypical associated with
improvement in 4 metabolic parameters in the
CATIE study CATIE Phase I
Change in Metabolic Parameters in Phase I of CATIE
Glycosylated haemoglobin levels
Weight change
9.4
10
10
7.5
7.5
5
5
0.41
2.5
IMPROVEMENT
2.5
IMPROVEMENT
0.10
Mean change in glycosylated hemoglobin () from
baseline
0.08
Mean change in weight (lb) from baseline
0.8
1.1
0.05
0
0
-2.5
-2.5
-0.10
-1.6
-2.0
-5
-5
-7.5
-7.5
Cholesterol levels
Triglycerides
12
48
9.7
42.9
9
36
5.3
6
24
19.2
3
IMPROVEMENT
8.3
Mean change in cholesterol (mg/dL) from baseline
12
IMPROVEMENT
0.5
Mean change in triglyceride (mg/dL) from baseline
0
0
-3
-2.6
-12
-2.1
-6
-24
-18.1
-9
-36
-9.2
ziprasidone
risperidone
quetiapine
olanzapine
perphenazine
At baseline, gt40 of patients met the criteria
for metabolic syndrome, an important risk factor
for cardiovascular disease.
Lieberman JA, et al. N Engl J Med.
2005353(12)1209-23.
33Favorable metabolic profile of ziprasidone
ADA/APA consensus statement
The Risk of Obesity, Diabetes, and Dyslipidaemia
Differs Among Second-Generation Antipsychotics
(SGAs)
- Consideration of metabolic risk when starting
SGA - If a patient gains 5 of his or her initial
weight during therapy, one should consider
switching the SGA - If a patient develops worsening glycaemia or
dyslipidaemia while on antipsychotic therapy,
consider switching to an SGA that is not
associated with weight gain or diabetes
Increased effect - No effect D
Discrepant results.
American Diabetes Association. Diabetes Care.
200427(2)596-601.
34ADA/APA consensus statement on atypical therapy
monitoring protocol
More frequent assessments may be warranted based
on clinical status.
American Diabetes Association. Diabetes Care.
200427596-601.
35Zeldox in Bipolar Mania
36Response rates in acute bipolar mania Ziprasidone
in acute mania 3-week studies
Keck et al. 20031
Potkin et al. 20052
ziprasidone
placebo
60
50
50
46
40
35
Patients ()
Patients ()
29
30
20
10
N125
N137
N65
N64
0
Response defined as 50 improvement in Manie
Rating Scale (MRS) score at endpoint. Plt0.05 vs
placebo.
1. Keck PE, et al. Am J Psychiatry.
2003160(4)741-8. 2. Potkin S, et al. J Clin
Psychopharmacol. 200525(4)301-10.
37Improvement in acute bipolar mania Study I Keck
et al 2003
Change in MRS Score
ziprasidone (N131)
placebo (N66)
Mean Change in MRS Scores from Baseline
0
2
4
7
14
21
Day
MRS Mania Rating Scale. LOCF Last Observation
Carried Forward. Baseline scores placebo, 26.7
ziprasidone, 27.0. Plt0.003 Plt0.001 vs placebo.
Keck PE, et al. Am J Psychiatry.
2003160(4)741-8.
38Improvements in acute bipolar mania Study II
Potkin et al 2005 - replication study
Change in MRS Score From Baseline
0
ziprasidone (N135)
-2
placebo (N62)
-4
-6
Mean Change in MRS Scores from Baseline
-8
-10
-12
-14
0
2
4
7
14
21
Day
MRS Mania rating scale. Baseline values mania
rating scale Placebo, 26.42 ziprasidone,
26.19 or early discontinuation Mean dose
ziprasidone day 15-21 126.5mg/day Plt0.05 vs
placebo P0.01 vs placebo.
Potkin S, et al. J Clin Psychopharmacol.
200525(4)301-10.
39Improvement in severity in acute bipolar
mania Study II Potkin et al 2005 - replication
study
Change in CGI-S Scores
ziprasidone (N137)
placebo (N65)
Change in CGI-S Score (LOCF)
Day
CGI-S Clinical Global Impression of Severity
LOCF Last Observation Carried Forward. Mean
dose ziprasidone day 15-21 126.5mg/day. Plt0.05
P0.01 P0.001 vs placebo.
Potkin S, et al. J Clin Psychopharmacol.
200525(4)301-10.
40Pooled studies PANSS positive subscale items
PANSS Positive Subscale
Conceptual disorganisation
Hallucinatorybehaviour
Suspiciousness/persecution
Delusions
Excitement
Grandiosity
Hostility
Mean Change from Baseline to Endpoint (LOCF)
Consistent withimprovement in coremanic symptoms
-1
-1
ziprasidone placebo
PANSS Positive and Negative Syndrome Scale
LOCF Last Observation Carried Forward. Plt0.01
Plt0.001 N247 (ziprasidone) N120 (placebo).
Pfizer Inc., Data on file.
41Pooled studies improvement in manic and mixed
episodes
Change in MRS Score From Baseline
Mixed episode
Manic episode
0
0
ziprasidone (N101 BL 23.64) placebo (N50 BL
23.16)
ziprasidone (N167 BL 28.74) placebo (N81 BL
28.62)
-2
-2
-4
-4
-6
-6
Change in MRS Score (LOCF)
-8
-8
-10
-10
-12
-12
-14
-14
Day
Day
MRS Mania Rating Scale LOCF Last Observation
Carried Forward. BL Baseline. Plt0.05 Plt0.01.
Keck PE, et al. Presented at the American
Psychiatric Association 56th Institute on
Psychiatric Services October 6-10, 2004
Atlanta, Ga poster.
42Pooled studies improvement in manic and mixed
episodes
Change in MRS Score
Psychotic symptoms
No psychotic symptoms
ziprasidone (N167 BL 25.28) placebo (N79 BL
24.73)
ziprasidone (N101 BL 29.37) placebo (N50 BL
29.12)
0
0
-2
-2
-4
-4
-6
Change in MRS Score (LOCF)
-8
-6
-10
-8
-12
-10
-14
-16
-12
Day
Day
MRS Mania Rating Scale LOCF Last Observation
Carried Forward. BL Baseline. Plt0.05 Plt0.01.
Keck PE, et al. Presented at the American
Psychiatric Association 56th Institute on
Psychiatric Services October 6-10, 2004
Atlanta, Ga poster.
43Pharmacokinetics and Dosing
44For optimal efficacy, oral ziprasidone requires
administration with food
- Food doubles the bioavailability of ziprasidone
- Ziprasidone must be administered with food to
achieve the necessary plasma concentration for
effective symptom control
AUC Fed
AUC Fasted
AUC (ng-h/mL)
Dose (mg)
Ziprasidone was administered with a standard FDA
meal.
Lombardo I, et al. Presented at American
Psychiatric Association 58th Institute of
Psychiatric Services October 5-8, 2006 New
York.
45For optimal efficacy, oral ziprasidone requires
administration with food
- Food doubles the bioavailability of ziprasidone
- Ziprasidone must be administered with food to
achieve the necessary plasma concentration for
effective symptom control
Fed
Fasting
Ziprasidone trough plasma level (ng/ml)
60 D2 occupancy
ziprasidone dose (mg)
Pfizer Inc., Data on file.
46Effective D2 receptor occupancy is dependent on
ziprasidone plasma levels Pharmacokinetics
- Clinical response occurs at approximately 60 D2
receptor occupancy1 - 60 D2 receptor occupancy corresponds to a plasma
level of approximately 50ng/ml - A plasma level of 50ng/ml corresponds to about
120mg/day of ziprasidone1,2
Ziprasidone Plasma Level vs. D2 Occupancy 12 hr
Post-Dose
14-16 hours post dose
1. Mamo D, et al. Am J Psychiatry.
2004161(5)818-25. 2. Miceli JJ, et al. Br J
Clin Pharmacol. 200049 Suppl 1S5-13.
47For optimal efficacy, titrate ziprasidone to
120-160mg/day with food1-4
Day 3 If indicated
Day 1
The recommended starting dose is 80mg/d. If
indicated, the maximum recommended dose may be
reached as early as day 3 of treatment. The full
dose range is 40-160mg/d.1 gt500 kcal
1. Zeldox, Summary of Product Characteristics. 2.
Nemeroff CB, et al. CNS Spectr.
200510(11Suppl17)1-20. 3. Joyce AT, et al.
Schizophr Res. 2006 Apr83(2-3)285-92. 4. Daniel
DG, et al. Neuropsychopharmacology. 1999
May20(5)491-505.
48Greater antipsychotic efficacy with ziprasidone
120-160mg/day in acute schizophrenia Pooled,
short-term, fixed-dose, placebo-controlled trials
BPRS Total, Mean Change from Baseline
P0.036
Effect Size
N335
N220
40-80mg/day
120-160mg/day
Effect size (Cohens d) (ziprasidone
placebo)/pooled SD. BPRSBrief Psychiatric
Rating Scale. Plt0.01, Plt0.001.
Nemeroff CB, et al. CNS Spectr. 200510(11)S1-20.
49Greater adherence rates with higher initial
prescribed ziprasidone doses in
schizophrenia Dosing 6-month retrospective
claims database
Patients () Remaining on Therapy at 6 Months
Initial ziprasidone dose
P0.012
Proportion of Patients Remaining on Therapy at
Endpoint
n220
40-79mg/day (N413)
80-119mg/day (N356)
120-160mg/day (N289)
Joyce AT, et al. Schizophr Res 200683285-92.
50Dosing adjustments of ziprasidone in special
populations
- No dose adjustments are required in patients
with impaired renal function - Dose adjustments with ziprasidone may be
considered in patients over 65 when clinical
factors warrant - In patients with hepatic insufficiency lower
doses should be considered
Zeldox, Summary of Product Characteristics.
51Ziprasidone metabolism Metabolism
Metabolic Pathways to Major Circulating
Metabolites
N-dealkylation CYP3A4
Reduction Aldehyde oxidase (2/3)
ziprasidone
Oxidation
dihydroziprasidone
benzisothiazole (BITP) sulphoxide
S-oxidation (CYP3A4)
S-oxidation (CYP3A4)
S-methylation (S-methyltransferase)
ziprasdione sulphoxide
BITP sulphoxide
S-methyl-dihydroziprasidone
S-oxidation (CYP3A4)
S-oxidation (CYP3A4)
Faeces
S-methyl-dihydroziprasidone sulphoxide
BITP suphone
ziprasdione sulphone
Major inactive circulating metabolites
Major potentially active circulating metabolite
Adapted from Beedham C, et al. J Clin
Psychopharmacol. 2003 Jun23229-32.
52Switching to Zeldox
53Switching to ziprasidone can be effective
irrespective of the switching strategy Ziprasidone
(switch studies)
Stable but Symptomatic Outpatients with
Schizophrenia
conventionals (N108), olanzapine (N104),
risperidone (N58)
Randomly switched to ziprasidone by
Discontinuation abrupt cessation of current
treatment before starting ziprasidone Cross-taperi
ng dose reduction of current treatment when
starting ziprasidone therapy Delayed
withdrawal delayed dose reduction of current
treatment 4 days after ziprasidone initiation
- No significant differences were observed between
switching strategies in changes from baseline to
endpoint PANSS total, BPRSd, PANSS negative
subscale, PANSS positive subscale, CGI-S or CGI-I
scores
Weiden PJ, et al. J Clin Psychiatry.
200364(5)580-8.
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