1. Medical Management of Depression Public Health Detailers’ Training
NYC Department of Health and Mental Hygiene
Jorge R. Petit, MD
Associate Commissioner, Bureau of Program Services
2. Overview Depression management
Types of antidepressants
Choosing an antidepressant
PCP concerns: suicide risk, misdiagnosis of bipolar
PHQ9 as a monitoring tool
Treatment algorithm
3. Overview Acute, Maintenance, Continuation Phases
Ongoing monitoring
Referral to Psychiatry
Involvement of non-physician staff
4. Depression Management Once a diagnosis has been made, effective management in primary care includes:
Medication management (Pharmacotherapy)
Patient education
Self management support
Ongoing monitoring, including monitoring of concurrent psychotherapy
5. Pharmacotherapy: Types of Meds Selective serotonin uptake inhibitors (SSRIs)
Other newer antidepressants (norepinephrine plays a key role)
Tricyclic antidepressants (not considered a first-line antidepressant)
MAO Inhibitors (rarely used by primary care physicians)
6. SSRIs� Citalopram (Celexa)
Escitalopram (Lexapro)
Fluoxetine (Prozac)
Paroxetine (Paxil, Paxil CR)
Setraline (Zoloft)
Duloxetine (Cymbalta)
7. SSRIs Potential side effects:
GI (N/V, diarrhea)
Activation/insomnia
Sexual Dysfunction
Neurological (headaches, etc)
Weight changes
Serotonin syndrome
Drug Interactions (MAOIs)
9. Dopamine-norepinephrine reuptake inhibitor Buproprion (Wellbutrin SR, Wellbutrin XL)
Potential side effects:
Neurological/seizures
Insomnia
GI upset
Psychotic symptoms
10. Norepinephrine serotonin neurotransmission enhancer Mirtazapine (Remeron)
Potential side effects
Sedation
Dry mouth
Weight gain
Increase serum cholesterol
11. Serotonin-norepinephrine reuptake inhibitor Venlafaxine (Effexor XR)
Potential side effects:
Similar side effect profile to SSRIs, including N/V, sexual dysfunction, and activation
Possible dose-related increase in BP
13. Tricyclics As effective as newer agents
Side effects potentially more dangerous:
dry mouth, constipation, bladder problems, sexual dysfunction, blurred vision, dizziness, drowsiness and increased heart rate.
Cheaper-especially generic forms
May be good for selected patients
15. Choosing an antidepressant In general, no particular antidepressant is more effective than another
Choice should be based on:
Family history of response
Safety and side effect profiles
Ease of use
Consider symptom profile/presence of comorbidities, ie. anxious, obsessive compulsive
cost
16. 1st line antidepressants All categories mentioned with the exception of trycyclics, MAOs
1st line antidepressants have these factors in common:
Once a day dosing (ease of use aids compliance)
Favorable side-effect profile (also aids compliance)
Safety in overdose
Broad efficacy for mood disorders
17. 1st line antidepressants Using these better tolerated, newer meds can:
prevent the need for complicated titration-allowing for a quicker response
improve compliance
Lead to fewer office visits
Result in less overall cost
18. Suicide Risk FDA Public Health Advisory March, 2004: possible risk of worsening depression and suicidality in patients taking antidepressants
Done in reaction to reports of suicidal ideation and attempts in treatment of major depression in pediatric patients.
Black box warning for children / adolescents September, 2004
19. FDA Public Health Advisory Points out the need to closely monitor patients receiving antidepressants for worsening and suicidality especially at beginning of treatment and with changes in dosage
Also need to instruct patients and families to be alert for worsening or suicidal thoughts and to immediately report such symptoms
20. Misdiagnosis of Bipolar Patients Potential risks from antidepressants
May induce mania or hypomania
Can cause rapid cycling
Requires mood stabilizer (e.g. lithium or valproic acid) before brief use of antidepressant
Generally need psychiatry consultation or referral
21. Quantifies the severity of depression (gives a number)
Provides measurement over the time which aids in assessing effectiveness of chosen treatment course
Follow-up PHQ9s should be conducted every month in person or over the phone
PHQ-9 as a monitoring tool
22. Remission Goal of treatment: full remission (absence of symptoms)
Monitoring with the PHQ9 can assist in the process of achieving full remission
A score of 5 or less on the PHQ9 = full remission
Once remission is achieved, patient should remain on the current dose of medication for 6-9 months to prevent relapse
23. Treatment Algorithm Decision support tool PCPs can use to manage depression
Assists with monitoring of medication and psychotherapy over all phases of treatment
Provides timeframes for effective monitoring
Pocket size version available
24.
25. Phases of Treatment Acute
Continuation
Maintenance
26. Acute Phase Usually 6-12 weeks
Effective treatment response is usually obtained in this phase--initial remission
27. Continuation Phase Usually 6-9 months
Residual symptoms can continue to impair patients and complicate co-morbid medical illness
Patients are prone to relapse during this phase
Important to continue full therapeutic dose during this phase
28. Maintenance Phase >9 months
If 1st episode, meds should be tapered and discontinued
If recurrent episode, long term maintenance should be considered, generally at the therapeutic dose established in acute phase
29. Maintenance Phase Other factors that would extend a course of antidepressant treatment include:
patient preference
illness severity and related disability when affected
30. Important for practices to have some sort of system in place for monitoring
Close follow up by telephone and or visits until stable
Severity tool (PHQ-9) to assess progress
Titrate dose for total remission
Ongoing Monitoring
31. Ongoing Monitoring Maintain effective dose for 4 to 9 months (continuation phase)
Monitor for early signs of recurrence
Consider maintenance therapy
32.
��Consider referral to psychiatrist if:
33. Requires specialized treatment (MAO inhibitors, ECT)
Deteriorates quickly
Has unclear diagnosis
Consider referral to psychiatrist if:
34. To Locate a Psychiatrist American Psychiatric Association Answer Center:
apa@psych.org or (888) 35-PSYCH
LIFENET (accessible 24/7):
1-800-LIFENET (800-543-3638) or call 311 and ask for LIFENET
35. Patient Education Key to promoting compliance with the treatment plan, patient becomes partner in care
Dispels negative perceptions/addresses stigma that may contribute to non-adherence
If patients know what to expect will be less likely to discontinue meds prematurely
36. Patient Education Compare depression to other treatable medical illnesses to help patients feel less stigmatized
Inform patients that antidepressant medication helps correct imbalances in brain chemicals
Educate about medication options
Effectiveness, onset of action, potential adverse side effects
All patients should be cautioned not to expect immediate symptom relief
may need to take antidepressants for as long as 6 weeks before they experience benefits
37. Key Educational Messages For patients starting antidepressant meds:
Antidepressants only work if taken every day
Antidepressants are not addictive
Benefits from meds appear slowly
Continue meds even after you feel better
38. Key Educational Messages For patients starting antidepressant meds, cont:
Mild side effects are common and usually improve with time
Some medications must be stopped gradually. Always consult a doctor before changing, reducing, or stopping a drug regimen.
The goal of treatment is complete remission; sometimes it takes a few tries.
39. Use of Non-physician and Support Staff Many of the monitoring and education functions important in the care of depressed patients can be handled by support staff, including:
Administration/scoring of PHQ to monitor symptoms
Providing educational materials
Explaining care plan, what to expect, side effects
40. Scheduling follow-up visits
Assisting with referral process
Care management
active patient follow-up through regularly scheduled phone contacts or visits
Use of Non-physician and Support Staff
