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Schizophrenia and Other Psychotic Disorders

Schizophrenia and Other Psychotic Disorders. Clinical Description. Positive symptoms more active manifestations of abnormal behavior, excess or distortion of normal behavior delusions identity persecution grandeur reference control hallucinations. Clinical Description.

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Schizophrenia and Other Psychotic Disorders

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  1. Schizophrenia and Other Psychotic Disorders

  2. Clinical Description • Positive symptoms • more active manifestations of abnormal behavior, excess or distortion of normal behavior • delusions • identity • persecution • grandeur • reference • control • hallucinations

  3. Clinical Description • Negative symptoms • deficits in normal behavior • Avolition: inability to initiate and persist in activities • Alogia: diminished speech • Anhedonia: indifference to pleasurable activities • Affective flattening: don’t show emotions you would expect

  4. Clinical Description • Disorganized symptoms • Disorganized speech • illogical, jump from topic to topic, loose associations • Inappropriate affect • Disorganized behavior • bizarre behavior • catatonic behavior: wild agitation to immobility, waxy flexibility

  5. DSM-IV Criteria • 2 of following x 1 month (or less if treated) • Delusions • Hallucinations • Disorganized speech • Grossly disorganized or catatonic behavior • Negative symptoms • Social/occupational dysfunction • Duration: 6 months

  6. Subtypes • Paranoid • Delusions and hallucinations have theme (persecution or grandeur) • Cognitive skills and affect intact • Better prognosis

  7. Subtypes • Catatonic • Unusual motor behavior • waxy flexibility • remaining in a fixed position • remaining rigid • engaging in excessive activity • Odd mannerisms of body and face • Echolalia • Echopraxia

  8. Subtypes • Disorganized • Marked disruptions in speech and behavior • Flat or inappropriate affect • Delusions lack theme • Undifferentiated • Don’t fit neatly into other previous categories

  9. Subtypes • Residual • “leftover” symtoms • Symptoms present, but in milder form • Unusual ideas that are not fully delusional • Unusual sensory perceptions that are not full blown hallucinations • Negative symptoms: social withdrawal, inactivity, flat affect

  10. Prevalence and Onset • prevalence • 1% • roughly equal for men and women • onset • early adulthood (late teens/early 20s)

  11. Course • onset may be gradual or sudden • complete recovery is rare • minority (22%) have only one episode, with minimal subsequent impairment • most (78%) experience several episodes • fluctuate between severe and moderate levels of impairment throughout life

  12. Other Psychotic Disorders • Brief Psychotic Disorder • Symptoms last more than 1 day and less than 1 month. • Often follows extreme stress • Schizophreniform Disorder • Symptoms last 1-6 months.

  13. Other Psychotic Disorders • Schizoaffective Disorder • Psychotic symptoms and mood symptoms occur together • Psychotic symptoms must be preceded or followed by 2 weeks of delusions or hallucinations without prominent mood symptoms

  14. Other Psychotic Disorders • Delusional Disorder • Delusions without other symptoms of schizophrenia (no negative symptoms) • Delusions are nonbizzarre (could occur in real life)

  15. Causes: Genetic Influences • Genes are responsible for making some people vulnerable to schizophrenia • Twin studies • Adoption studies • Family studies • the closer your genetic relationship to someone with schizophrenia, the higher your risk

  16. Personal risk: given differing degrees of biological relatedness • MZ twin = 48% • DZ twin = 17% • 1 parent = 15% • 1 sibling = 7% • grandparent = 5% • general population = 1%

  17. Genetics: continued • Can be carrier without showing symptoms • if your parent is the MZ twin with schizophrenia, your risk is about 17% • if your parent is the MZ twin without schizophrenia, your risk is still about 17% • Problems with smooth-pursuit eye movement as genetic marker

  18. Causes: Neurobiological Influences • Leading theory • schizophrenia is caused by overactivity at synapses that use dopamine

  19. Dopamine Theory • Evidence supporting: • dopamine antagonists (Haldol) reduce symptoms • drugs appear to block D2 receptors • dopamine antagonists cause side effects similar to Parkinson’s disease (due to insufficient dopamine) • L-dopa (dopamine agonist) produces schizophrenia-like symptoms in some people • amphetamines (dopamine agonists) can make psychotic symptoms worse in some people

  20. Dopamine Theory • Evidence against: • dopamine antagonists don’t help everyone • dopamine antagonists are only partially effective at reducing negative symptoms • although drugs block dopamine quickly, it takes several days or weeks for symptoms to subside • Recent research suggests relation of serotonin to dopamine is important

  21. Causes: Neurobiological Influences • Brain structure • Evidence for neurological damage, pregnancy and delivery complications • Enlarged ventricles • Underactivity in frontal lobes: associated with negative sx • Viral infection • Influenza during 2nd trimester • May disrupt migration of brain cells from inner portion to cortex

  22. Causes: Psychological and Social Influences • Instability of early family rearing environment • may trigger the onset of schizophrenia in people with underlying genetic vulnerability • Stress • May trigger relapse • Families • High expressed emotion (criticism, hostility, emotional overinvolvement) associated with relapse

  23. Treatment: Biological • Neuroleptic medications • Different classes: • Low potency: chlorpromazine (Thorazine), thioridazine (Mellaril) • High potency: haloperidol (Haldol). More effective at reducing symptoms, but more likely to cause EPS • Newer: clozapine (Clozaril), risperidone (Risperdal). Have fewer motor side effects.

  24. Limitations of Meds • Meds are a treatment, not a cure • 55% relapse when go off meds • Meds reduce positive symptoms, but are less effective for negative symptoms • 10% not helped by meds • Side effects

  25. Side Effects • Superficial • Dry mouth, sedation, blurred vision, constipation, weight gain, • EPS (extrapyramidal sx): slowed/awkward motor activity, tremor • Serious • Tardive dyskinesia: involuntary movements of lips, mouth, tongue, face. • Develops in 20%. • Associated with long-term use. Irreversible.

  26. Psychosocial Treatments • Token economies on inpatient units • Improves social skills, self-care, and vocational skills • More likely to be discharged • Social skills training • Initial effects positive, but fade over time • Less likely to relapse than meds alone • Independent living skills training • Teach patients how to identify warning signs of relapse, cope with symptoms, manage meds • Initial results suggest decreased relapse

  27. Psychosocial Treatments • Family therapy • factual information about disease • meds • side effects • identification of warning signs regarding a relapse • decreased expressed emotion • increased support for patient • communication skills • problem solving skills • Reduces relapse better than meds alone

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