Jitka Hüttlová Department of Psychiatry, University Hospital Brno and Faculty of Medicine of Masaryk University Treatment in Psychiatry Treatment in Psychiatry ›A. BIOLOGICAL treatment ›Psychopharmacotherapy ›Electroconvulsive Therapy (ECT) ›Repetitive Transcranial Magnetic Stimulation (rTMS) ›Deep Brain Stimulation (DBS) ›Vagus Nerve Stimulation ›Light Therapy › ›B. PSYCHOSOCIAL treatment ›Psychotherapy ›Psychiatric rehabilitation ›Other (music therapy, art therapy, ergotherapy…) › › Treatment in Psychiatry Main Psychopharmacological Drugs ›1. Antidepressants ›2. Mood stabilizers ›3. Antipsychotics ›4. Anxiolytics ›5. Hypnotics ›6. Cognition-Enhancing Drugs ›7. Psychostimulants Psychopharmacotherapy General guidelines for antidepressant use ›Antidepressant efficacy is very similar so selection is based on past history of a response, side effect profile and coexisting medical conditions. ›There is a delay typically of 2-4 weeks after a therapeutic dose is achieved before symptoms improve. ›If no improvement is seen after a trial of adequate length and adequate dose, either switch to another antidepressant or augment with another agent. › 1.Antidepressants Neurobiology ›Lack of monoamine neurotransmitters → depression ›Increase in monoamine neurotransmitters → treatment of depression › › › › › (Stahl 1997) › › 1.Antidepressants Neurotransmitter Reuptake Inhibition and Binding Affinity to Receptors Obrázek1 1.Antidepressants › Classification Name Example st generation Tricyclics (TCAs) and tetracyclics (TeCAs) amitriptyline clomipramine 2nd generation viloxazine 3rd generation SSRI (Selective Serotonin Reuptake Inhibitors ) citalopram escitalopram sertralin SARI (Serotonin antagonist and reuptake inhibitor) trazodon NRI (Nor-Adrenaline Reuptake inhibitors) reboxetin 4th generation SNRI (Serotonin/Norepinephrine reuptake inhibitors) venlafaxine milnacipran DNRI (Dopamine/Norepinephrine reuptake inhibitors bupropione Other Blockators of α2 -adrenoceptors mirtazapin mianserin (MAOIs) Monoamine Oxidase Inhibitors moclobemide selegiline Classification Name Mechanism of Therapeutic Efficacy Specific character Examples 1st generation Tricyclics (TCAs) and tetracyclics (TeCAs) •Inhibition of Serotonin and/or Norepinephrine reuptake followed by increase of their concentrations in synaptic cleft (react with other types of receptors → more side effects) •Severe side effects - antihistaminic (sedation, weight gain), anticholinergic (dry mouth, constipation, potentially delirium), antiadrenergic (orthostatic hypotension, sexual dysfunction) •Can cause dangerous QT lengthening •Danger of Intoxication •Many Interactions amitriptyline nortriptyline clomipramine dosulepin Classification Mechanism of Therapeutic Efficacy Specific character Examples 2nd generation Norepinephrine Reuptake Inhibition •Less anticholinergic side effects then 1st generation viloxazine Classification Name Mechanism of Therapeutic Efficacy Specific character Examples 3rd generation SSRI (Selective Serotonin Reuptake Inhibitors ) Block the presynaptic serotonin reuptake •The most commonly used •Side effects: GI upset, sexual dysfunction, anxiety, restlessness, insomnia, fatigue or sedation, dizziness •Very little risk of cardiotoxicity in overdose citalopram escitalopram sertralin fluoxetin fluvoxamin paroxetin Classification Name Mechanism of Therapeutic Efficacy Specific character Examples 3rd generation SARI (Serotonin antagonist and reuptake inhibitor) Antidepressants with Doubled Serotonergic Efficacy •A risk of serotonin syndrome trazodon NRI (Selective Nor-Adrenaline Reuptake inhibitors) Increase norepinephrine reboxetin Classification Name Mechanism of Therapeutic Efficacy Specific character Examples 4th generation SNRI (Serotonin/Norepinephrine reuptake inhibitors ) Inhibit both serotonin and noradrenergic reuptake •Side effects: nauzea, dizziness, blood preasure increase venlafaxine milnacipran DNRI (Dopamine/Norepinephrine reuptake inhibitors) Inhibit Dopamine and Norepinephrine reuptake •No weight gain, no sexual side effects, no sedation or cardiac interactions bupropione Classification Name Mechanism of Therapeutic Efficacy Specific character Examples other Blockators of α2-adrenoceptors Increasing Synthesis and Releasing of Norepinephrine, Blockade Alpha-2 Adrenoceptors on Serotonergic Neurons and Increasing Production and Releasing of Serotonin •Side effects: Weight gain, sedation, mirtazapin mianserin Classification Name Mechanism of Therapeutic Efficacy Specific character Examples Other (MAOIs) Monoamine Oxidase Inhibitors Bind irreversibly to monoamine oxidase thereby preventing inactivation of biogenic amines such as norepinephrine, dopamine and serotonin leading to increased synaptic levels. •Side effects: weight gain, dry mouth, sedation, sexual dysfunction and sleep disturbance •Hypertensive crisis can develop when MAOI’s are taken with tyramine-rich foods or sympathomimetics moclobemide selegiline Main Psychopharmacological Drugs ›1. Antidepressants ›2. Mood stabilizers ›3. Antipsychotics ›4. Anxiolytics ›5. Hypnotics ›6. Cognition-Enhancing Drugs ›7. Psychostimulants Psychopharmacotherapy Mood stabilizers ›Indications: Bipolar, cyclothymia, schizoaffective, impulse control and intermittent explosive disorders. ›Classes: Lithium, anticonvulsants, antipsychotics ›Which you select depends on what you are treating and again the side effect profile. › › › 2. Mood stabilizers Classification Example Characteristics Lithium Lithium •Only medication to reduce suicide rate •I:Effective in long-term prophylaxis of both mania and depressive episodes •SE: Thyroid abnormalities, Polyuria/polydypsia , intention tremor •BS: examination of renal, cardiac and thyreoidal function, pregnancy Antiepil. 2nd generation carbamazepine •I: acute mania and mania prophylaxis •SE: Rash, nauzea, vomiting, drug interactions!!! •BS: baseline liver function tests, CBC and an EKG salts of valproic acid •I: as effective as Lithium in mania prophylaxis but is not as effective in depression prophylaxis Effective in dysforic mania •SE: Thrombocytopenia and platelet dysfunction, transaminitis, sedation •BS: liver function, CBC, pregnancy Antiepil. 3rd generation lamotrigine •I: Also used for neuropathic/chronic pain •SE: Nausea/vomiting, dizziness, toxic epidermal necrolysis and Stevens Johnson's Syndrome BS: liver function gabapentine Main Psychopharmacological Drugs ›1. Antidepressants ›2. Mood stabilizers ›3. Antipsychotics ›4. Anxiolytics ›5. Hypnotics ›6. Cognition-Enhancing Drugs ›7. Psychostimulants Psychopharmacotherapy Neurobiology ›Excess of DOPAMINE → schizophrenia ›Decrease in Dopamine → treatment of schizophrenia › 3. Antipsychotics Neurobiology ›MESOCORTICAL- associated with negative and cognitive symptoms ›MESOLIMBIC- associated with positive symptoms (hallucinations, delusions, and thought disorders) ›NIGROSTRIATAL- associated with movement regulation, Parkinsonian movements i.e. rigidity, bradykinesia, tremors), akathisia and dystonia ›TUBEROINFUNDIBULAR - associated with hyperprolactinemia(gynecomastia/galactorrhea/decreased libido/menstrual dysfunction). › 3. Antipsychotics Classification ›A. Typical antipsychotics (=1st generation antipsychotics, classical neuroleptics,) ›B. Atypical antipsychotics (=2nd generation antipsychotics) 3. Antipsychotics A.Typical antipsychotics (1st generation) ›previous generation ›are D2 dopamine receptor antagonists ›High potency typical antipsychotics bind to the D2 receptor with high affinity. As a result they have higher risk of extrapyramidal side effects. ›Examples: fluphenazine, haloperidol, flupenthixol ›Low potency typical antipsychotics have less affinity for the D2 receptors but tend to interact with nondopaminergic receptors resulting in more cardiotoxic and anticholinergic adverse effects including sedation, hypotension. ›Examples: chlorpromazine, thioridazine › › › › 3. Antipsychotics B.Atypical Antipsychotics (2nd generation) ›dopamine D2 receptor-blocking effect is lowered in affinity ›combined with effects on other receptors ›better influencing of negative and affective symptoms ›significantly reduce or prevent the cognitive impairment ›signifinantly less side effects ›examples: risperidon, olanzapin, quetiapin 3. Antipsychotics Adverse effects ›Extrapyramidal side effects (EPS): Acute dystonia, Parkinson syndrome, Akathisia ›Neuroleptic Malignant Syndrome (NMS): Characterized by severe muscle rigidity, fever, altered mental status, autonomic instability, elevated WBC, CPK Potentially fatal. ›Weight gain, sedation, dyslipidemia, hyperprolactinemia, agranulocytosis, sexual dysfunctions… › › 3. Antipsychotics Main Psychopharmacological Drugs ›1. Antidepressants ›2. Mood stabilizers ›3. Antipsychotics ›4. Anxiolytics ›5. Hypnotics ›6. Cognition-Enhancing Drugs ›7. Psychostimulants Psychopharmacotherapy General information ›Used to treat many diagnoses including panic disorder, generalized anxiety disorder, substance-related disorders and their withdrawal, insomnias and parasomnias. ›In anxiety disorders often use anxiolytics in combination with SSRIS or SNRIs for treatment. ›Main group – Benzodiazepines – cave – the risk of addiction !!!! 4. Anxiolytics Action Profiles of Benzodiazepines 4. Anxiolytics Examples ›Short-term: oxazepam, lorazepam ›Medium-term: alprazolam, bromazepam ›Long-term: diazepam, clonazepam 4. Anxiolytics Non-benzodiazepine anxiolytics ›Non-addictive ›Delayed onset of therapeutic effect › ›Examples: guaiphenesine, hydroxyzine, buspirone › 4. Anxiolytics Main Psychopharmacological Drugs ›1. Antidepressants ›2. Mood stabilizers ›3. Antipsychotics ›4. Anxiolytics ›5. Hypnotics ›6. Cognition-Enhancing Drugs ›7. Psychostimulants Psychopharmacotherapy General information ›drugs with sedative effect ›primary function is to induce sleep and to be used in the treatment of insomnia › 5. Hypnotics Classification Name Example 1st Generation barbiturates phenobarbital 2nd Generation benzodiazepines midazolam, flunitrazepam, cinolazepam 3rd Generation Z-drugs zolpidem, zopiclone, zaleptone Other Drugs with Hypnotic Efficacy Antihistaminics promethazine antidepressants mirtazapine, trazodone melatonins antipsychotics quetiapin Main Psychopharmacological Drugs ›1. Antidepressants ›2. Mood stabilizers ›3. Antipsychotics ›4. Anxiolytics ›5. Hypnotics ›6. Cognition-Enhancing Drugs ›7. Psychostimulants Psychopharmacotherapy General information ›improve cognition ›to treat Alzheimer's disease and other cognitive deficits ›A. ACETYLCHOLINESTERASE INBITORS ›-rivastigmine, donepezil › ›B. NMDA (N-methyl-D-aspartate) RECEPTOR ANTAGONISTS ›-memantine › 6. Cognition-Enhancing Drugs Main Psychopharmacological Drugs ›1. Antidepressants ›2. Mood stabilizers ›3. Antipsychotics ›4. Anxiolytics ›5. Hypnotics ›6. Cognition-Enhancing Drugs ›7. Psychostimulants Psychopharmacotherapy General information ›reduce fatigue, promote alertness and wakefulness and have possible mood enhancing properties ›indicated for attention deficit hyperactivity disorder (ADHD), narcolepsy ›Blocators of re-uptake dopamine and norephinephrine→ increase of dopamine and norephinephrine in synaptic cleft ›Adverse effects: insomnia, agitation, anxiety and confusion ›Methylphedinate, atomoxetine 7. Psychostimulants Main Psychopharmacological Drugs ›1. Antidepressants ›2. Mood stabilizers ›3. Antipsychotics ›4. Anxiolytics ›5. Hypnotics ›6. Cognition-Enhancing Drugs ›7. Psychostimulants Psychopharmacotherapy Treatment in Psychiatry ›A. BIOLOGICAL treatment ›Psychopharmacotherapy ›Electroconvulsive Therapy (ECT) ›Repetitive Transcranial Magnetic Stimulation (rTMS) ›Deep Brain Stimulation (DBS) ›Vagus Nerve Stimulation ›Light Therapy › ›B. PSYCHOSOCIAL treatment ›Psychotherapy ›Psychiatric rehabilitation ›Other (music therapy, art therapy, ergotherapy…) › › Treatment in Psychiatry Electroconvulsive therapy ›procedure, in which small electric currents are passed through the brain, intentionally triggering a brief seizure ›ECT seems to cause changes in brain chemistry that can quickly reverse symptoms of certain mental illnesses ›when other treatments are unsuccessful ECT Electroconvulsive therapy ›informed consent must be signitured ›ECT is administered under anesthetic with a muscle relaxant ›ECT can differ in its application in three ways: electrode placement, frequency of treatments, and the electrical waveform of the stimulus. ›side effects: confusion and memory lost ›main indications: major depressive disorder, mania, and catatonia › › ECT Repetitive transcranial magnetic stimulation (rTMS) ›a magnetic method used to stimulate small regions of the brain ›a magnetic field generator, or "coil", is placed near the head ›The coil produces small electric currents in the region of the brain just under the coil via electromagnetic induction. The coil is connected to a pulse generator, or stimulator, that delivers electric current to the coil. ›Indication: major depressive disorder, negative symptoms of schizophrenia, auditory hallucinations, ›Side effects: epileptiform paroxysm, mild headaches › rTMS Deep brain stimulation (DBS) ›a neurosurgical procedure ›involving the implantation of a medical device called a neurostimulator (sometimes referred to as a 'brain pacemaker'), which sends electrical impulses, through implanted electrodes, to specific targets in the brain (brain nuclei) for the treatment of movement and neuropsychiatric disorders (major depression, OCD) ›has been used in a small number of clinical trials › › DBS Vagus nerve stimulation ›is a medical treatment that involves delivering electrical impulses to the vagus nerve. It is used as an adjunctive treatment for certain types of intractable epilepsy and treatment-resistant depression. ›the device sends electrical signals along the vagus nerve to the brainstem, which then sends signals to certain areas in your brain. › Vagus nerve stimulation Light Therapy › involves daily scheduled exposure to bright artificial light ›During light therapy, you sit or work near a device called a light therapy box. The box gives off bright light that mimics natural outdoor light. ›Light therapy is thought to affect brain chemicals linked to mood and sleep ›Biorhythm ›Indication: treatment for SAD (Seasonal Affective Disorder), other types of depression, sleep disorders and other conditions ›Side effects: eye strain, headache, nausea, irritability or agitation › › Light Therapy Treatment in Psychiatry ›Thank you very much for your attention