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Title: Management of Antidepressant-Induced Sexual Dysfunction


1
Management of Antidepressant-Induced Sexual
Dysfunction
Stevens S. Smith, Ph.D. Assistant Professor
(CHS) Department of Medicine / General Internal
Medicine Center for Tobacco Research and
Intervention University of Wisconsin Medical
School
Primary Care Conference Presentation Wednesday,
25 August 2004
2
Disclaimer
  • I have received smoking cessation research
    support from pharmaceutical companies (Elan
    Corporation GlaxoSmithKline) that market
    antidepressants or other medications discussed in
    this presentation.
  • I am not a consultant or paid speaker for any
    pharmaceutical companies.

3
Learning Objectives
  • Brief review of diagnosis and treatment of
    depression by primary care physicians
  • Brief review of sexual dysfunction
  • Prevalence and hypothesized mechanisms of
    antidepressant-induced sexual dysfunction
  • Strategies for managing antidepressant-induced
    sexual dysfunction

4
Case Study
  • 50 year-old male married and sexually active no
    medical complications other than a 10-year
    history of hypertension (controlled with
    enalapril 10 mg daily)
  • At routine check with his primary care physician
    (PCP), the patient mentions feeling depressed for
    several months with increasing problems at work
    and at home he admits to occasional suicidal
    ideation but has no active plans to harm himself
  • Differential diagnosis rules out
    medical/medication causes for the depression
    substance abuse also ruled out
  • Diagnosis first episode of major depression,
    moderate severity

5
Case Study
  • Initial treatment paroxetine 20 mg daily for one
    week followed by dose increase to 30 mg referral
    to psychologist
  • Patient returns after 4 weeks for medication
    check patient reports a small but noticeable
    improvement in symptoms of depression
  • Side effects noted by the patient include nausea
    (improving), drowsiness, night sweats
  • And, oh, by the way, my psychologist said that I
    should mention these other side effects to you
  • - Im not much in the mood for sex
  • - Also, Im having trouble reaching orgasm

6
Major Depression in Primary Care
  • General population estimates for major depression
    in the U.S.1
  • - Lifetime prevalence 16.2
  • - 12-month prevalence rate 6.6
  • Prevalence of depression in adult primary care
    patients tends to be higher especially in the
    presence of chronic health problems2
  • Depression is associated with poor self-care and
    poor adherence to medical treatments
  • Second only to hypertension as the most common
    chronic condition encountered in primary care
    settings

1 Kessler et al., JAMA 2003, 2893095-3105 2
Leon et al., Arch Fam Med 1995, 10857-861
7
Major Depression in Primary Care
  • Primary care physicians are the gatekeepers of
    medical care including depression
  • Primary care physicians (PCPs) outnumber
    psychiatrists 7 to 1 PCPs prescribe the majority
    of antidepressants
  • Outcomes for depression treatment of primary care
    patients do not differ for psychiatrists and
    primary care physicians1

1 Simon et al., Arch Gen Psychiatry 2001,
58395-401.
8
UW Health Treating Major Depression In Adults
in Primary Care (2002)
  • Medication recommended for essentially all
    patients with MDD
  • Mild MDD medication or
    psychotherapy
  • Moderate/severe MDD medication with or
    without psychotherapy
  • Acute phase (first 12 weeks of Tx) Patient
    should be seen a minimum of 3 times (at least
    once with prescriber)
  • Treatment response should be assessed every 4-6
    weeks during drug therapy assess every 4-12
    weeks after remission
  • Patient should continue on medication for at
    least 6 months after symptoms resolve

Source http//www.hosp.wisc.edu/crit/guides/depre
ssion.htm
9
Antidepressant Prescribing in Primary Care
  • Data from National Ambulatory Medical Care
    Survey1
  • Examined data from 89,424 adult primary care
    visits from 1989-2000 (approximately 260 million
    visits per year)
  • From 1989 to 2000, primary care physicians
    increased their prescribing of antidepressants
    from 2.6 of visits to 7.1 of visits
  • Antidepressant prescriptions in 2000 in primary
    care
  • - 18 older agents (e.g., tricyclics, MAOIs,
    trazodone)
  • - 17 newer, non-SSRIs (e.g., bupropion,
    venlafaxine)
  • - 65 SSRIs

1 Pirraglia et al., Primary Care Companion J Clin
Psychiatry 2003, 5153-157.
10
Current Antidepressants
Chemical Class Example Avail.
Selective Serotonin Reuptake Inhibitors (SSRI) Citalopram 6
Norepinephrine Dopamine Reuptake Inhib. (NDRI) Bupropion 1
Selective Serotonin-Norepi. Reuptake Inhib. (SNRI) Venlafaxine Duloxetine 2
Serotonin-2 Antagonists/Reuptake Inhibitors (SARI) Trazodone Nefazodone 2
Noradrenergic/Specific Serotonergic Agent (NaSSA) Mirtazapine 1
Tricyclics / tetracyclics (mixed reuptake Inhibitor / receptor blockers) Imipramine Maprotiline 10
Irreversible monamine oxidase-A-B inhibitors (MAOI) Phenelzine 3
Total 25
Main Source Bezchlibnyk-Butler et al. (Eds.).
Clinical handbook of psychotropic drugs, 13th
revised ed., 2003
11
Antidepressant Efficacy
  • All antidepressants appear to be equally
    efficacious
  • Choice of antidepressant depends on several
    factors
  • - pharmacokinetics
  • - lethality in overdose
  • - prior response in patient or family members
  • - potential medication interactions
  • - medical contraindications
  • - presence of co-morbid conditions (e.g.,
    social anxiety)
  • - side effect profile (e.g., more sedating vs.
    less sedating)

12
Antidepressant Adverse Effects
  • Anticholinergic effects
  • Sedation
  • Activation
  • Weight gain
  • Orthostatic hypotension
  • GI Effects
  • Insomnia
  • Sexual dysfunction
  • Miscellaneous others

?
13
Sexual Dysfunction
  • DESIRE Inhibited or hypoactive sexual desire
  • AROUSAL in males erectile dysfunction
  • AROUSAL in females inadequate lubrication and/or
    diminished/absent physiological changes
    associated with sexual excitement (e.g.,
    swelling of genitalia)
  • ORGASM premature, delayed, or absent orgasm
  • PAIN painful intercourse vaginisimus
  • Classifications lifelong (primary), acquired
    (secondary), generalized, and situational

14
Past-Year Prevalence of Sexual Dysfunction
  • 1992 National Health and Social Life Survey
  • Sampled 1749 women and 1410 men aged 18-59 years
  • Assessed presence of sexual problems in past 12
    months
  • 43 of women and 31 of men reported sexual
    dysfunction

Sexual Dysfunction Females Males
Low sexual desire 22 5
Arousal problems / ED 14 5
Sexual pain 7 -
Premature ejaculation - 21
Source Laumann et al., JAMA, 1999, 281537-544
15
Possible Causes of Sexual Dysfunction
  • Medical conditions (e.g., vascular disease,
    endocrine disorders, neurological conditions)
  • Psychological/psychiatric factors (e.g., history
    of sexual trauma, stress, relationship factors,
    psychiatric disorders such as depression,
    substance abuse)
  • Medications
  • - antihypertensives (e.g., clonidine,
    beta-blockers, CCBs)
  • - sedatives (e.g., alprazolam)
  • - anticonvulsants (e.g., phenytoin,
    carbamazepine,
  • - neuroleptics (e.g., chlorpromazine,
    fluphenazine)
  • - miscellaneous (cimetidine, niacin, digoxin,
    ketoconazol)
  • - antidepressants, especially SSRIs,
    tricyclics, and MAOIs

16
Sexual Dysfunction in Major Depression
  • Sexual functioning is often impaired in MDD due
    to diminished ability to experience pleasure
  • Antidepressant treatment of MDD can cause or
    worsen sexual dysfunction
  • Antidepressant-induced sexual dysfunction can
    exacerbate depression and may influence the
    patient to discontinue antidepressant treatment

17
Impaired Sexual Functioning in MDD Prior to
Antidepressant Treatment
  • Kennedy et al. (1999) studied 55 male and 79
    female patients who met DSM-IV criteria for MDD
    ages 18-64 years
  • Assessed past month sexual functioning prior to
    initiation of antidepressant treatment
  • 39 women (49) and 14 men (26) reported no
    sexual activity in past month

Sexual Dysfunction Females Males
Decrease in sexual drive 50 42
Arousal problems / ED 50 46
Delayed ejaculation - 22
Source Kennedy et al., J Affective Disorders,
1999, 56201-208.
18
Impaired Sexual Functioning in MDD Subsequent to
SSRI Treatment
  • Hu et al. (2004) studied 401 patients, 18-40
    years old, receiving SSRI treatment (paroxetine,
    fluoxetine, sertraline, or citalopram)
  • Assessed 17 SSRI side effects including sexual
    dysfunction in a phone interview 75 to 105 days
    of starting SSRI treatment

Sexual Dysfunction (SD) Measure Percentage
experiencing SD 34
experiencing bothersome SD 17
SD occurred during first two weeks 70
SD continued for 3 months 83
Includes only patients reporting SD
Source Hu et al., J Clin Psychiatry, 2004,
65959-965.
19
Prevalence of Antidepressant-Induced Sexual
Dysfunction
  • Clayton et al. (2002) examined a target
    population of 802 primary care patients who met
    the following criteria 18-40 years old no
    sexual side effects from previous antidepressant
    tx on medication at least 3 months no
    medications or illnesses causing SD history of
    at least some sexual enjoyment
  • Percentage of target population reporting sexual
    dysfunction
  • ?30 - citalopram and venlafaxine
  • ?27 - sertraline and paroxetine
  • ?22 - fluoxetine
  • ? 7 - bupropion

Source Clayton et al., J Clin Psychiatry, 2002,
63357-366.
20
General Findings Regarding Antidepressant-Induced
Sexual Dysfunction
  • Difficult to disentangle depression-related
    sexual dysfunction (SD) from medication-related
    SD
  • Package inserts for antidepressant medications
    typically underestimate the prevalence of SD
  • SD is more likely in patients who do not respond
    well to antidepressant treatment
  • Tolerance to sexual side effects unlikely
  • SD often leads to discontinuation of medication
  • SSRIs are more likely than non-SSRIs to cause
    problems
  • Some studies suggest that males are more likely
    than females
  • to experience problems

21
Why Are SSRIs More Likely to Cause SD?
  • Probable role of neurotransmitters and hormones
    in normal sexual functioning
  • - Desire/libido dopamine, testosterone,
    estrogen ?
  • prolactin ?
  • - Arousal acetylcholine, dopamine, nitric
    oxide ?
  • - Orgasm norepinephrine ?
  • serotonin ?
  • Hypothesized mechanisms of SSRI-related SD
  • - serotonin reputake blockade may reduce
    dopamine activity
  • - SSRIs may increase prolactin levels
  • - SSRIs may interfere with spinal reflex centers
    involved in
  • ejaculation and orgasm

22
Management of Antidepressant-Induced Sexual
Dysfunction
  • Prior to initiation of antidepressant treatment
  • - assess baseline sexual functioning
    (non-depressed)
  • - assess current sexual functioning
  • After antidepressant treatment has started
  • - re-assess sexual functioning to identify any
    changes
  • If SD present, ascertain possible causes and
    treat accordingly

23
Assessing Sexual Functioning
Assess baseline (usual sexual interest and
functioning) and current sexual functioning
continue to monitor during treatment
Sexual Phase Possible Questions
Desire Baseline What is your usual interest in sex? Do you have sexual thoughts or fantasies? Current Has there been any recent changes in your interest in or desire for sex?
Arousal Female Do you usually have (or Have you had any) problems getting wet or lubricated when aroused? Male Do you usually have (or Have you had any) problems getting or keeping an erection?
Orgasm Do you usually have (or Have you had any) difficulty reaching orgasm?
24
Management of SSRI-Induced Sexual Dysfunction
  • If SD is SSRI-induced, consider treatment options

SD Management Strategy Comments
Wait for tolerance to develop Low success rate
Reduce the dose Risk for relapse of depression
Drug holiday Pt may discontinue drug
Switch to another medication Limited evidence
Add another medication e.g., bupropion sildenafil
Combinations of the above Limited evidence base
25
Management of SSRI-Induced Sexual
Dysfunction Switching to Another Antidepressant
  • Antidepressants with lowest incidence of sexual
    side effects (in order of preference)
  • - Bupropion potentiates dopamine
    neurotransmission, no serotonergic effects
  • - Nefazodone blocks post-synaptic 5-HT2
    receptors
  • - Mirtazapine blocks 5-HT2 and 5-HT3
    receptors increases norepinephrine
    neurotransmission
  • Note that the evidence base for switching to any
    of these medications is quite limited.

26
Management of SSRI-Induced Sexual
Dysfunction Adding An Antidote Medication
  • Adding bupropion SR to SSRI treatment
  • - one randomized clinical trial1 showed
    statistically significant increases in desire for
    and frequency of sexual activity but no
    differences in arousal or orgasm
  • - a second randomized clinical trial showed no
    benefit2
  • - use caution in combining bupropion with SSRIs

1 Clayton et al., J Clin Psychiatry 2004,
6562-67 Masand et al., Am J Psychiatry, 2001,
158805-807.
27
Management of SSRI-Induced Sexual
Dysfunction Adding An Antidote Medication
  • Adding sildenafil to SSRI treatment for erectile
    dysfunction (ED)
  • - Nurnberg et al. (2002) reviewed 3 randomized
    clinical trials and retrospective data pooled
    from 10 clinical trials trials included
    depressed men treated or untreated with SSRIs1
  • - Sildenafil was found to be efficacious for
    SSRI-induced ED and for ED unrelated to SSRI
    treatment
  • - Beneficial effects of sildenafil were
    generally replicated in a newer study by Nurnberg
    et al. (2003)2

1 Nurnberg et al., Urology 2002, 60 (Suppl 2B),
58-60 2 Nurnberg et al., JAMA 2003, 28956-64.
28
Management of SSRI-Induced Sexual
Dysfunction Adding An Antidote Medication
  • Other medications have been proposed for treating
    SD
  • - cyproheptadine and other serotonin antagonists
  • - amantadine and other dopamine agonists
  • - buspirone (anxiolytic)
  • - yohimbine (alpha-2 adrenergic receptor
    antagonist)
  • - ginko biloba
  • - dextroamphetamine and other stimulants
  • None of these medications have an adequate
    evidence base

29
Summary
  • Antidepressant-induced sexual dysfunction (SD) is
    very common
  • SSRIs have the highest incidence of
    treatment-emergent SD
  • When treating depressed patients with or without
    antidepressants, it is important to assess usual
    sexual functioning as well as any changes in
    sexual functioning associated with the onset of
    depression and/or the use of medications
  • Consider initial use of antidepressants with
    lower incidence of SD
  • Follow-up with patients to monitor medication
    efficacy and side effects
  • Carefully assess and treat SD no matter what the
    cause(s)
  • The evidence base for most SD treatments is quite
    limited

30
Case Study
  • Primary care physician (PCP) recommended that the
    patient continue on paroxetine for another month
    to see if SD would improve
  • No improvement in SD after two months on
    medication
  • PCP recommended switching to nefazodone
  • Patient stayed on nefazodone for one week
    discontinued medication due to side effects not
    interested in trying other antidepressants
  • Patient continuing in psychotherapy
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