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Author Topic: Way beyond maximum dosages in antipsychotics  (Read 1149 times)

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Offline SettleForNothingLess

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Way beyond maximum dosages in antipsychotics
« on: November 27, 2007, 12:47:50 PM »
I seeded thru all of my medication regimen last night. This is just for my abilify.
9/3 thru 9/8   5 Mgs at 5P
9/9 thru 9/12  10mgs at 9PM
9/13 thru 9/15   15 mgs at 9PM
9/16 thru 9/29    20mgs at 9 PM
9/30 thru 10/7    20mgs at 8AM and 20Mgs at 9PM (40 Mgs)
10/8 thru 10/19   40 mgs at 9PM
10/20 thru 10/27  20Mgs at 1PM and 40Mgs at 9PM   (60Mgs)
10/27 thru 10/30    40Mgs at 1PM and 40 Mgs at 9PM (80 Mgs)
10/31 thru 11/2      40 Mgs at 1PM and 60 Mgs at 9PM  (100Mgs)
11/2 thru 11/18     60 Mgs at 1PM and 60 Mgs at 9PM  (120 Mgs)


then when they were getting ready for discharge, it starts going down  drastically.


Aripiprazole (Abilify) for schizophrenia

(ari-pip-rah-zol)
Summary
PBS listing:  Authority required
Schizophrenia
Reason for listing:  Listing was recommended on a cost-minimisation basis against olanzapine, suggesting similar benefits at similar or reduced cost to the PBS.
Place in therapy:  There is presently no evidence to suggest that aripiprazole is more effective than existing antipsychotics in the treatment of schizophrenia but it offers prescribers another treatment option for this illness. Based on its tolerability profile, it can be considered another atypical antipsychotic.
Safety issues:  The risk of extrapyramidal side-effects and hyperprolactinaemia appears low with aripiprazole at recommended doses. In clinical trials, weight gain was less than with olanzapine. Diabetes, hyperlipidaemia, tardive dyskinesia and QT prolongation have not been identified as problems in clinical trials but more post-marketing experience is needed to determine its long-term safety profile. The dose of aripiprazole may need to be adjusted if co-administered with carbamazepine, or inhibitors of enzymes CYP3A4 (e.g. ketoconazole, erythromycin) or CYP2D6 (e.g. fluoxetine, paroxetine).
Dosing issues:  The recommended starting and maintenance dose is 15 mg once daily. The maximum approved dose is 30 mg daily, but there is no evidence that doses over 15 mg are more effective.
PBS listing
Authority required

Schizophrenia.

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Reason for PBS listing
Listing was recommended on a cost-minimisation basis against olanzapine1, suggesting similar benefits at similar or reduced cost to the PBS.

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Place in therapy
Aripiprazole is a new antipsychotic agent. There is presently no evidence to suggest that it is more effective than existing antipsychotics in the treatment of schizophrenia but it offers prescribers another treatment option for this illness. Its efficacy in treatment-resistant schizophrenia is not established; for these patients clozapine is generally considered the drug of choice.2-4

Antipsychotic drugs are generally classified into two groups: the older or 'conventional' agents (e.g. haloperidol, chlorpromazine) and the newer or 'atypical' agents (amisulpride, clozapine, olanzapine, quetiapine and risperidone).

Conventional antipsychotics are effective at reducing positive symptoms of schizophrenia, such as hallucinations and delusions, but are commonly associated with distressing adverse effects such as extrapyramidal side-effects† and hyperprolactinaemia.2-4

Atypical antipsychotics are at least as efficacious at treating positive symptoms as the conventional agents and may be more effective in managing negative symptoms2-4 (see Table 1). Atypical antipsychotics are less likely to cause extrapyramidal effects and hyperprolactinaemia, although both risperidone and amisulpride may induce these effects at higher doses.2,4

While aripiprazole has been described as a 'novel antipsychotic agent'5 (a 'dopamine system stabiliser'6), the clinical relevance of this mechanism of action is as yet unknown. Based on its tolerability profile it can be considered another atypical antipsychotic.7

Atypical antipsychotics are often preferred to conventional agents in the treatment of schizophrenia2,3 but the Therapeutic Guidelines: Psychotropic does not distinguish between the older and newer agents and argues that choice of antipsychotic drug and dose should be individualised to suit the patient.4

†includes Parkinsonism, dystonia, akathisia (restlessness) and tardive dyskinesia.

Table 1: Symptoms of schizophrenia2,4
Positive symptoms


hallucinations
delusions
 Negative symptoms


blunted affect
loss of sense of pleasure (anhedonia)
poor self-care
impoverished speech
apathy/lack of motivation
attentional impairment*
social withdrawal
 Cognitive symptoms


impaired planning and problem-solving (executive functioning)
impaired memory
impaired language processing
 

*also considered a cognitive symptom.

Aripiprazole efficacy studies

Few published studies compare aripiprazole directly with other antipsychotics in the treatment of schizophrenia and it is difficult to draw conclusions about its relative efficacy, particularly compared with other atypical agents. Aripiprazole has been compared with olanzapine in clinical trials8 but, as yet, efficacy data have not been published.

A recent meta-analysis compared the efficacy of atypical and conventional antipsychotics.9 Of the atypicals, only clozapine, amisulpride, risperidone and olanzapine were found to be more effective than the older drugs, but the analysis of aripiprazole was based on limited data.

Aripiprazole 10–30 mg was significantly better than placebo‡ in three short-term (4–6 week) double-blind trials in schizophrenia and schizo-affective disorder, although two earlier dose-ranging studies failed to demonstrate efficacy.10 Some studies included an active control (either haloperidol or risperidone)10-12 but were not powered to allow a direct comparison with aripiprazole.5

Two long-term, double-blind, maintenance studies have been conducted.13,14 A 6-month comparison with placebo found that patients taking placebo relapsed significantly sooner and more frequently than those taking aripiprazole 15 mg.13 In a 52-week study of more than 1200 patients with acute relapse of chronic schizophrenia, aripiprazole was not superior to haloperidol in the primary efficacy endpoint, time-to-failure to maintain response, but was better tolerated.14

Published studies exclude patients with treatment-refractory schizophrenia, a history of suicide attempts or ideation, and/or past or current substance abuse; results therefore cannot be generalised to these patient groups. Only one study enrolled patients aged over 65 years. Patients aged less than 18 years were excluded and the safety and effectiveness of aripiprazole in this age group is not established.5

‡Efficacy was assessed using standardised instruments, including the Positive and Negative Syndrome Scale (PANSS), the Brief Psychiatric Rating Scale (BPRS), and the Clinical Global Impression (CGI).

If switching patients to aripiprazole

An 8-week outpatient study found that any of the following methods could be used if switching patients from other antipsychotics†† to aripiprazole5,15:


immediate initiation of aripiprazole and immediate cessation of current antipsychotic;
immediate initiation of aripiprazole and a 2-week taper of current antipsychotic;
2-week up-titration of aripiprazole with simultaneous taper of current antipsychotic.


Prescribing guidelines generally advocate a simultaneous taper method to minimise antipsychotic withdrawal effects.2,4

††Most patients in the study were taking either olanzapine or risperidone.

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Safety issues
The risk of extrapyramidal side-effects and hyperprolactinaemia appears low with aripiprazole at recommended doses.10 In clinical trials weight gain was less than with olanzapine.5,10 Diabetes, hyperlipidaemia, tardive dyskinesia and QT prolongation have not been identified as problems in clinical trials10 but more post-marketing experience is needed to determine its long-term safety profile. The dose of aripiprazole may need to be adjusted if co-administered with potent CYP2D6 or CYP3A4 inhibitors or inducers (see Drug interactions).5

Contra-indications and precautions

The general contra-indications, warnings and precautions for aripiprazole are similar to those of other atypical antipsychotics; refer to the Abilify product information.5

Aripiprazole demonstrated developmental toxicity in animal studies and if possible should be avoided in pregnancy.5

The UK Committee of Safety of Medicines (CSM) has recently warned that atypical antipsychotics (although not specifically aripiprazole) may increase the risk of stroke in elderly patients with dementia.16

Adverse drug reactions

Weight gain can occur with most atypical agents but clozapine and olanzapine tend to cause the greatest short-term gains in weight.17 Long-term comparisons found aripiprazole was more likely than haloperidol (20% vs. 13%) to be associated with significant weight gain‡‡, but less likely than olanzapine (13% vs. 33%).5,10

A recent consensus statement on antipsychotic drugs, obesity and diabetes concluded that aripiprazole was associated with little or no significant weight gain, diabetes or dyslipidaemia, with the caveat that it had not been used as extensively as other atypical agents.17 Nevertheless, the Food and Drug Administration (FDA) has requested that all atypical antipsychotics include a diabetes warning statement in US product information.18

In short-term trials the incidence of extrapyramidal side-effects was similar to placebo, although akathisia was slightly more common with aripiprazole.5,10 In long-term comparisons the incidence of extrapyramidal effects was comparable to that with olanzapine but significantly less than with haloperidol.5,10

QT prolongation can occur with some antipsychotic drugs and predispose patients to the potentially fatal arrhythmia, torsade de pointes.3,4 QTc prolongation has not been reported with aripiprazole at recommended doses but may be a potential problem in overdose.10

Increased prolactin levels have not been reported with aripiprazole in clinical trials.10

Orthostatic hypotension may occur.5

‡‡≥ 7% increase from baseline

Drug interactions

If potent inhibitors of enzymes CYP2D6 (e.g. fluoxetine, paroxetine) and CYP3A4 (e.g. ketoconazole, erythromycin) are co-administered the dose of aripiprazole may need to be reduced.5

The potent CYP3A4 inducer, carbamazepine, increases the clearance of aripiprazole; if co-administered the dose of aripiprazole should be doubled.5

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Dosing issues
The recommended starting and maintenance dose is 15 mg once daily.5 The maximum approved dose is 30 mg daily5 but there is no evidence that doses over 15 mg are more effective.10

For further information on dosing, drug interactions and adverse effects consult the Australian Medicines Handbook or the Abilify product information.

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Information for patients
As with any antipsychotic therapy, many patients taking aripiprazole may relapse or discontinue therapy in the longer-term.13,14 Poor compliance and substance misuse are common triggers for relapse and patients and carers should be counselled about the dangers of these.2-4

For more detailed information, suggest or provide the Abilify Consumer Medicine Information (CMI).

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References
Department of Health and Ageing. December 2003 PBAC outcomes – positive recommendations.
http://www.health.gov.au/pbs/general/li ... IPIPRAZOLE. (Accessed 11 February 2004).
Lambert TJR, Castle DJ. Med J Aust 2003;178:S57–S61.
Freedman R. N Engl J Med 2003;349:1738–49.
Therapeutic Guidelines: Psychotropic. Version 5, 2003.
Abilify Product Information. Bristol Myers Squibb Pty Ltd. 14 July 2003.
Stahl SM. J Clin Psychiatry 2001;62:11:841–2.
European Agency for the Evaluation of Medicinal Products. Pre-authorisation Evaluation of Medicines for Human Use. Committee for Proprietary Medicinal Products Summary of Opinion for Abilify. London, 26 February 2004. http://www.emea.eu.int/pdfs/human/opinion/563403en.pdf (Accessed 2 February 2004.)
The Cochrane Central Register of Controlled Trials. The Cochrane Library. Issue 1, 2004. (Accessed 26 February 2004.)
Davis JM, Chen N. Arch Gen Psychiatry 2003;60:553–564.
US Food & Drug Administration Center for Drug Evaluation and Research, New and Generic Drug Approvals: Abilify (aripiprazole). 3 July 2003. http://www.fda.gov/cder/approval/index.htm (Accessed December 2003.)
Potkin S, et al. Arch Gen Psychiatry 2003;60:681–90.
Kane JM, et al. J Clin Psychiatry 2002;63:763–71.
Pigott TA, et al. J Clin Psychiatry 2003;64:1048–56.
Kasper S, et al. Int J Neuropsychopharmacol 2003;6:325–37.
Casey DE, et al. Psychopharmacol 2003;166:391–9.
Committee of Safety of Medicines. Atypical antipsychotic drugs and stroke. 9 March 2004. http://medicines.mhra.gov.uk/ourwork/mo ... e_9304.htm (Accessed 10 March 2004.)
American Diabetes Association, American Psychiatric Association, American Association of Clinical Endocrinologists, North American Association for the Study of Obesity. Diabetes Care 2004;27:596–601.
2004 Safety Alert: Zyprexa (olanzapine). US FDA Medwatch. http
« Last Edit: December 31, 1969, 07:00:00 PM by Guest »
Yours Truly,
Ms. Vigilante
Im standing on the frontline, there waiting for you PV bitches. Lets rock n roll.

Offline Anonymous

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Way beyond maximum dosages in antipsychotics
« Reply #1 on: November 27, 2007, 12:52:19 PM »
Some drugs are not efficacious and binding to receptors at recommended doses.

D2 receptor bindings are not present at lower doses.

Were these written by a doc or a staff member , who signed off on them.

Abilify is not just for schizophrenia - it has other uses.
« Last Edit: December 31, 1969, 07:00:00 PM by Guest »

Offline SettleForNothingLess

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« Last Edit: December 31, 1969, 07:00:00 PM by Guest »
Yours Truly,
Ms. Vigilante
Im standing on the frontline, there waiting for you PV bitches. Lets rock n roll.