drugs → brain structures ap mst. bipolar disorder
TRANSCRIPT
Drugs → brain structures
APMST
Bipolar disorder
NICE
Diagnosis
Full history of the patient (family, any episode, symptoms between the episodes)
Symptoms profile, triggers to previous episodes, social and personal functioning, comorbidities, physical health, current psychosocial stressors
Interview a family member
NICE
BE CAREFUL
If (Psychotic symptoms, ↑ suicidal ideation, ↑ drug misuse) → late BD and not SKZ (minorities)
If alcohol | drug → wait 7 days before diagnosis Late onset (>40yrs) → hypothyroidism, stroke,
neurological disorders (dementia)
NICE
Before a rapid cycling BD is diagnosed consider:
Erratic compliance hypothyroidism, AD, suboptimal medication
regimes Lithium withdrawal
NICE
Consider a diagnosis of BD before Axis II if there are mood swings
During treatment consider compliance before considering a personality disorder
NICE
Treatment (1/3)
Inform the patient Contraception and risk of pregnancy See patients once / (1|2) week (for 3 months)
NICE
Treatment (2/3)
Acute mania (and mixed→ AP, valproate, lithium, BDZ
AP (olanz, risp, quet)→ severe manic symptoms | marked behavioral disturbances
Valproate or lithium → previous response, good compliance, augmentation of AP
Lithium → not severe symptoms NOT RECOMMENDED: CBZ, Gabapent, Lamo
NICE
Treatment (3/3)
Acute depression
Add AP (quetiapine) to AD (SSRI better than TCI) No AD → rapid-cycling, recent hypomanic, recent
functional impairing and rapid mood fluctuations Stop AD → after 8 weeks of symptoms relief (parox,
venlafax → higher risk of discontinuation syndrome) Avoid → Lamo a single treatment for BDI
Mania, which treatment ?
3 weeks
Mania, which treatment ?
Mania, which treatment ?
Change in mania rating scores
Mania, which treatment ?
Risk difference for treatment responders
Mania, which treatment ?
Risk difference for drop outs
Conclusion 1
Use second generation AP (risp, olanz, quet) for the treatment of acute mania (3 weeks)
Mood stabilizers are second choice
Acute depression, which treatment ?
Acute depression, which treatment ?
Acute depression, which treatment ?
Symptom remission
Conclusion 2
Use second generation AP (olanz, quet) for the treatment of acute depression during BD
Mood stabilizers are less efficacious
No strong evidence for using SSRI
Maintenance, which treatment ?the same regimen that successfully treated the
acute bipolar mood episode
attempt monotherapy. However, many bipolar patients require medication combinations
First line: lithium, lamotrigine, risperidone (im)
Second line: aripiprazole, valproate, quet, olanz
Suicide risk → lithium
Maintenance → lithium
Lithium 41% vs 61% placebo
Conclusion 3
For maintenance use the same drug started during acute phase
If not possible use lithium, risperidone im, lamotrigine, valp
Start with monotherapy, but multitreatment is more effective
neuroimaging
lithium
neuroimaging
1.9 years base-1st fu4 years base-2nd fu
Valproate and AP
Overall, no significant brain volume modification in bipolar patients taking valproate or AP
Valproate
ant
AP mechanism
Serotonin-glutamate
Type II metabotropic glutamate receptors (mGluRs) and serotonin 5-HT(2A) receptors have been reported to form heterodimers that modulate G-protein-mediated intracellular signaling differentially compared to mGluR2 and 5-HT(2A) homomers
Serotonin-Dopamine-Scaffolding
The scaffolding protein PSD-95 is known to interact with N-methyl-D-aspartate (NMDA), D(2) and 5-HT(2) receptors, regulating their activation state
Homer1a, the inducible member of the Homer family of PSD proteins that is implicated in glutamatergic signal transduction, is induced in striatum by antipsychotics with high dopamine receptor affinity and in the cortex by antipsychotics with mixed serotonergic/dopaminergic profile
Conclusion 4
The molecular events that drive the efficacy of mood stabilizers are related to GSK-3, IPP and
prosurvival genetic expression
The dopaminergic-serotoninergic-glutamatergic balance is central to the activity of AP in the prefrontal cortex. Scaffolding proteins are
thought to be relevant
imaging
Conclusion 5
Lymbic structures and the PFC are key relay points for the efficacy of pharmacological
treatments in BP
Schizophrenia
skz
Treatment
First episode → oral AP, address to specialized unit, write a care plan in collaboration with the patient and send it to the GMP, include a crisis plan
Provide information and discuss the benefits and disadvantages
Chose the AP with the patient, taking into consideration extrapyramidal side effects and metabolic side effects
Assess the cardiovascular risk (ECG)
skz
Start with the lower dose of AP Justify and record reasons for dosages outside the
range given by guidelines Monitor efficacy, side effects, adherence, physical health Record the rationale for continuing, changing or stopping
medication and the effects of such changes Trials for one medication should last 4-6 weeks Do not “neuroleptisize” your patient Rapid tranquillization
skz
Which drug ?
Conclusion 6
Second generation AP are more effective for the treatment of Skz
Use Olanzapine and Risperidone when possible
The side efffect profile must nevertheless guide the clinical choices
imaging
Conventional antipsychotic agents led to an increase of basalganglia volume while ongoing multifocal gray matter loss
Modern atypical agents rather tend to turn increased basal ganglia volumeback to normal while increasing the volume of thalamus and of
gray matter in different key regions
II AP → ↑ glutamatergic turnover and inhibit NMDA receptors
17 (8m/9f) acute psychotic recurrent-episode (chronic) patients treated with
haloperidol or risperidone
30 medication-naive first-episode patients and 36 matchedhealthy controls participatedAtypical antipsychotic treatment
Effect of practice on brain activation in the left dorsolateral prefrontal cortex (DLPFC)
8 skz and 8 controls
Treated with risperidone for 6 weeks
Conclusion 7
II AP increase the DLPC activity This event correlates with outcome
Variations in the NAc may be involved during withdrawal