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Perspectives on Bipolar Disorder and Psychosis

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Title: Perspectives on Bipolar Disorder and Psychosis

1
Perspectives on Bipolar Disorder and
Psychosis 9th November 2010 Dr Tim
Sales Consultant Psychiatrist Honorary Senior
Clinical Lecturer

2

Structure of talk
Overview of Bipolar Disorder
Overview of Schizophrenia and Psychosis
Question time

Bipolar Disorder need to know
What do you already know?
Where do you get new information from?
Map of Medicine

Bipolar Affective Disorder
Common life time prevalence 1.3
Peak of onset mid teens to mid twenties
50 of patients non-adherent to treatment
as with other long term conditions
10 - 20 suicide rate
46 co-morbid alcohol misuse
41 co-morbid drug misuse

5
Bipolar affective disorder is multi-dimensional
Hypomania
Mania
Mania
Maintenance
Mild depressive episode
Severe depressive episode
6
Ongoing symptoms in Bipolar Disorder
n146 12.8 year follow up
Judd et al 2002
7

Goals in Maintenance Treatment
Symptom control
Prevention of new episodes
Prevention of sub-syndromal episodes
Prevent suicide
Enhance functioning

When to start Maintenance Treatment
Consider long term treatment earlier
1 severe episode of mania
2 less severe episodes of illness
At least 2 years of treatment to maintain
progress

Which Maintenance Treatment?
5 drugs are effective as monotherapy in trials gt
1year
Lithium
Olanzapine
Aripiprazole
Lamotrigine
Quetiapine
1 year data for Sodium Valproate
Avoid routine use of long term anti-depressants

Schizophrenia need to know
What do you already know?
Where do you get new information from?
Map of Medicine

Schizophrenia
Common life time risk 0.5 1.0
Peak of onset mid teens to mid twenties
50 of patients non-adherent to treatment
as with other long term conditions
10 - 20 suicide rate
Higher risk of cardiovascular disease

NICE Guidelines (2009 update)
Recommends anti-psychotics for schizophrenia
non-adherence, troublesome side effects
No specific anti-psychotics are recommended
both 1st and 2nd generation anti-psychotics
recommended

13
CATIE results of Phase I discontinuationLieber
man JA, et al. N Engl J Med 2005353120923
ITT population Any cause Any cause Lack of efficacy Intolerability
Median time (months) Lack of efficacy Intolerability
Olanzapine 64 9.2 15 19
Quetiapine 82 4.6 28 15
Risperidone? 74 4.8 27 10
Perphenazine 75 5.6 25 16
Ziprasidone 79 3.5 24 15
Significantly longer for olanzapine than
quetiapine and risperidone, but not
perphenazine or ziprasidone
Significantly lower for olanzapine vs. all
except ziprasidone
No significant difference
14
CUtLASS 1 SGAs vs. FGAsJones PB, et al. Arch
Gen Psychiatry 200663107987

No advantage of SGAs over FGAs in terms of
quality of life or symptoms over 1 year
There were no significant differences in
symptoms, global functioning, or in rates of
objectively assessed EPS
Total healthcare and social costs (52 weeks) not
significantly different FGAs 18,800, SGAs
20,100
Drug costs were twice as much on SGAs than FGAs
(3.8 vs. 2.1)
No patient preference for any particular drug or
drug group at any stage.

15
Weighing it up SGAs vs. FGAs
Efficacy Safety
Pragmatic studies show no clinically important differences between FGAs and SGAs regarding efficacy and quality of life. All are associated with troublesome side-effects and are poorly tolerated. Side-effect profiles vary with individual agents and doses. In general FGAs more EPS SGAs more weight gain and metabolic effects.
Cost Patient factors
Acquisition costs of FGAs lower than SGAs. No significant difference in cost of care. Side-effects of individual agents may be more acceptable and tolerated by individual patients than others.
16