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Overview. DSM criteria for PTSDTreatmentTreatment of choiceIssues with pharmacological treatmentLimitations of research studiesMedicationsImplications for clinical practice. DSM Criteria. A. Exposed to a traumatic event: experience, witness, or confronted with event(s) with actual/threatene
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1. Pharmacological Treatment of PTSD Margarita Tartakovsky
March 22, 2006
2. Overview DSM criteria for PTSD
Treatment
Treatment of choice
Issues with pharmacological treatment
Limitations of research studies
Medications
Implications for clinical practice
3. DSM Criteria A. Exposed to a traumatic event:
experience, witness, or confronted with event(s) with actual/threatened death/ serious injury AND
response involved intense fear, helplessness, or horror
B. Event persistently re-experienced:
recurrent and intrusive distressing recollections/dreams
acting or feeling as if the traumatic event were recurring
Intense psychological distress at exposure to things reminiscent of event
physiological reactivity
4. DSM Criteria C. Persistent avoidance associated with trauma:
efforts to avoid thoughts, feelings
avoidance of people, places associated with trauma
recall inability
diminished interest
detachment feelings
restricted range of emotions
negative outlook toward future
5. DSM Criteria D. Persistent symptoms of increased arousal:
2 or more of the following
difficulty falling or staying asleep
irritability or outbursts of anger
difficulty concentrating
hypervigilance
exaggerated startle response
6. DSM Criteria E.Duration of symptoms is more than 1 month
F.Causes clinically significant distress and/or
impairment in social, occupational, and/or other important areas of functioning
Acute: less than 3 months Chronic: more than 3 months Delayed Onset: onset of symptoms is at least 6 months after the incident
7. Symptom Clusters Re-experiencing: intrusive recollections, recurrent dreams, dissociative flashbacks
Avoidance and numbness: avoidance of cognitions/activities related to trauma, decreased interest, feeling detached
Hyperarousal: hypervigilance, insomnia, exaggerated startle response
8. Systems involved in PTSD Neurotransmitter sensitization
? release of noradrenaline and ? autonomic activity
Dopamine
Amygdala and the hippocampus
Amygdala involved in fear conditioning and extinction
Hippocampus plays important role in memory; involved in mediating traumatic memories and learned responses to cues
PET studies = veterans show ? right amygdala activity when exposed to combat movies
MRI studies = male combat veterans + female survivors of childhood sexual abuse have shrunken hippocampal volumes
9. More on systems Excessive cortisol and glutamate activity
Human + animal studies = immediately after severe trauma, ? in cortisol and glutamate can reach toxic levels + damage parts of brain (affect regulation)
Serotonin
Preclinical studies = serotonergic pathways project to areas crucial in fear responses
Clinical studies = serotonin agonist, mCPP provokes PTSD sxs
Important to note: kindling effect repeated traumatic episodes change brain functioning and brain morphology
10. Treatment Psychotherapy is the treatment of choice
Meds are not the primary treatment but should target specific symptoms as they arise
Restoring a sense of control over emotions
11. Issues with pharmacological treatment Efficacy across symptom clusters
Comorbidity/Associated sxs
depression and substance abuse common
guilt, shame, distrust
significant marital, occupational, financial, health problems
Discontinuation of meds ? original symptoms returning
Response to meds not guaranteed
Changes not necessarily large
12. Methodological issues in research studies (1) Placebo effect
(2) Small samples
(3) SSRIs studies with mostly female participants
(4) Exclusion of patients with comorbid substance abuse
13. Meds Tricyclic Antidepressants (TCAs)
Benzodiazepines
Antipsychotics
Selective Serotonin Reuptake Inhibitors
14. TCAs 1st antidepressants used
Prevent reuptake of monoamines (serotonin or norepinephrine) by the presynaptic neurons in the CNS, thus prolonging the effects of these NTs
Numerous side effects: blurred vision, dry mouth, constipation, weight gain, dizziness when changing position, increased sweating, difficulty urinating, changes in sexual desire, decrease in sexual ability, muscle twitches, fatigue and weakness
Overdose ? delirium, hypotension, cardiac arrhythmias and death.
15. Benzodiazepines Relatively fast-acting
Use has declined
concerns over dependence and abuse
Lower anxiety by ?vigilance, eliminating muscle tension, and causing sedation
act on the g-aminobutyric acid (GABA)/benzodiazepine (BZ) receptor complex
Side effects: concentration problems, a mild form of amnesia, drowsiness and a loss of coordination; fatigue and mental slowing or confusion
dangerous to drive or operate heavy machinery
16. Antipsychotics Traditional antipsychotic meds rarely considered for use unless psychotic symptoms present
Atypical antipsychotics used to treat some core symptoms
Helpful with severe treatment resistant PTSD
17. SSRIs 1st line of treatment
Antidepressants that block reuptake of serotonin at presynaptic neurons in the brain
Side effects: nausea, sweating, fatigue, sleepiness, and sexual side effects.
Generally safer than TCAs if overdose is taken
18. SSRIs available in U.S. Generic Name Brand Name
citalopram Celexa / Cipramil
fluoxetine Prozac
fluvoxamine Luvox
paroxetine Paxil / Seroxat
sertraline Zoloft / Lustral
Note: Right now sertraline and paroxetine have FDA approval for
treating PTSD
http://www.twilightbridge.com/psychiatryproper/ailmentguide/ptsd/medication.htm
19. Going to Meds for treatment Psychotherapy or exposure-based treatment intolerant
Low level of cognitive functioning
When sxs become too intense or interfere with daily life, short-term meds:
Intrusive experiences, flashbacks
Transient psychosis
Marked derealization
Avoidance/numbing
Longer term meds: major depression, panic disorder, persistent psychotic sxs
20. Considerations for clinical practice No empirical data for prescribing decisions
Clinical judgment important!
21. Resources Cooper, J., Carty, J., & Creamer, M. (2005). Pharmacotherapy for posttraumatic stress disorder: Empirical review and clinical recommendations. Australian and New Zealand Journal of Psychiatry, 39, 674-682.
Preston, J.D., ONeal, J. H., & Talaga, M.C. (2005). Post-Traumatic Stress Disorder. Handbook of clinical psychopharmacology for therapists. Harbinger Publications, 129-136.
Ratna, L., & Barbenel, D. (1997). The pharmacotherapy of post traumatic stress disorder. A literature review and case report of treatment with nefazodone. International Journal of Psychiatry in Clinical Practice, 1, 169-177.
http://www.ncptsd.va.gov/facts/disasters/fs_medication_disaster.html
http://www.nimh.nih.gov/publicat/reliving.cfm
http://ptsd.factsforhealth.org/medfaq.html