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Neuropsychology of Depression

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Title: Neuropsychology of Depression


1
Neuropsychology of Depression
  • David J. Schretlen, PhD
  • The Johns Hopkins University

Charles University 3 October 2008 Praha, Czech
Republic
2
Major Depressive Disorder
  • Marked sadness or irritability for at least 2
    weeks, along with several physiological changes
  • Disturbed sleep, appetite, low energy,
    constipation
  • Slowed speech, actions
  • Decreased experience of pleasure, sexual desire
  • Altered self-attitude, feeling guilty or
    worthless
  • Crying, thoughts of death or suicide
  • Trouble concentrating and making decisions
  • Interferes with work and family relations

3
Major Depressive Episode
  • Can occur once or repeatedly
  • A small percentage have manic episodes
  • Expansive mood, heightened activity, euphoria,
    etc.
  • These can alternate over brief intervals (mixed
    state)
  • Pathogenic overlap, but likely a distinct illness
  • Variations in course and features
  • Psychosis, melancholia, catatonia, post-partum
    onset
  • Anxiety as symptom vs. additional disorder
  • Double depression

4
Genetics
  • Twin studies show heritability of 37
  • This is much lower than the heritability of SZ
    (75)
  • Partly due to heritable depressive personality
    traits
  • Family studies show MDD is not single gene
    disease
  • Some chromosomal loci of linkage have been
    replicated
  • But none has been replicated in every family study

5
  • Surveyed gt37,000 individuals from 10 countries
    using the WHO-CIDI (Composite International
    Diagnostic Interview)
  • Lifetime prevalence 3.0 (Japan) to 16.9
    (USA)
  • Female/male ratio 1.2 (Czech Republic) to 2.5
    (Japan)
  • Not married/married 1.1 (Brazil) to 2.5
    (Germany)
  • Birth cohort 14-24/45 2.2 (Brazil) to 10.9
    (Japan)

6
Age of onset and comorbidity
  • Odds of MDD in
  • Agoraphobia 16.8
  • Gen. anxiety disorder 81.6
  • Obsessive-compulsive 52.7
  • Panic disorder 43.5
  • Post-traumatic stress 9.4
  • Simple phobia 10.7
  • Soc. anxiety disorder 11.9

7
Possible Mechanisms
  • Monoamine-deficiency hypothesis depression
    caused by deficiency of serotonin and
    norepinephrine
  • Antidepressants block the reuptake of 5-HT and NE
  • Good predictive power Almost every compound that
    blocks 5-HT and NE reuptake has antidepressant
    properties
  • But studies of plasma, urine CSF have yet to
    identify deficiency

8
Possible Mechanisms
  • Hypothalamic-pituitary-cortisol hypothesis
    Depression caused by excess cortisol
  • Stress causes release of corticotropin-releasing
    hormone (CRH), which stimulates the adrenal
    cortices to secrete cortisol
  • Depressed patients have elevated cortisol in
    plasma
  • In response to dexamethasone, the normal
    cortisol-suppression is absent in about half of
    severely depressed patients
  • Other hypotheses Abnormal or altered
    glutamatergic or GABAergic neurotransmission,
    circadian rhythms, etc.

9
Possible Contributions of Neural Circuits
  • Orbitofrontal cortex Depressed patients respond
    faster to sad words, more to negative feedback,
    and have smaller volumes
  • Anterior cingulate gyrus Show decreased
    metabolism, have smaller volumes, and respond
    faster to sad words
  • Dorsolateral prefrontal cortex Show increased
    activation by emotional Stroop, but reduced
    metabolism overall
  • Hippocampus Depressed elderly adults shown
    reduced volume findings are mixed in younger
    adults, but more consistent in those with
    recurrent depression

10
Neurocognitive Impairment in MDD
  • A mood disorder, but it involves cognitive
    dysfunction
  • Standard neuropsychological tests used to study
  • Severity and pattern of deficits (attention,
    effortful)
  • Severity/type of MDD (psychotic, melancholic)
  • State vs. trait and phase of episode
  • Interactions with age (young vs. old, early- vs.
    late-onset)
  • Effects of co-morbid conditions (dementia, MCI)
  • Experimental measures have been used to examine
    biases in information processing

11
  • Conducted meta-analysis of 22 studies of MDD
  • 726 patients 795 healthy controls (58 women)
  • Mean age 57 years mean education 13 years
  • Computed effect sizes (Cohens d) for 75 measures
  • Mdn d 0.52 (PIQ, Vocabulary) 67 ranged from
    0.310.97
  • 12 of 19 timed measures were above the median 7
    below (n.s.)
  • Largest effects for RAVLT, CFT smallest for
    CVLT, PASAT, CFT

12
Subtypes of MDD
  • Melancholic depression
  • Severe anhedonia, psychomotor slowing, diurnal
    variation with mood lowest in morning, early
    awakening, appetite and weight loss, excessive
    guilt
  • Is this a distinct subtype or simply severe
    depression?
  • Motor as opposed to psychomotor slowing might
    be unique to melancholic MDD (Pier et al, 2004)
  • Psychotic depression
  • Fairly consistent evidence of greater cognitive
    impairment
  • Verbal memory, psychomotor speed, executive
    functioning, etc. Overall, good evidence of
    greater but non-specific impairment

13
State vs. Trait Effects
  • Cognitive dysfunction is common during acute
    episodes
  • Melancholic MDD patients perform significantly
    better on testing in the evening compared to the
    morning (Moffoot et al, 1994)
  • Can persist following remission, but evidence is
    inconsistent
  • Remitted, drug-free MDD patients show mild
    deficits on selected executive and attention
    tests (Weiland-Fiedler et al, 2004)
  • Healthy twins discordant for unipolar depression
    performed poorly across multiple cognitive
    domains (Christensen et al, 2006)
  • Memory deficits might be state-dependent, while
    executive and attention deficits might be more
    trait-dependent (Porter et al, 2007)

14
Age Interactions
  • Greater cognitive impairment is seen in depressed
    patients gt60 than those lt60 years old
    (Christensen et al, 1997)
  • Fewer studies have considered age of illness
    onset
  • Late-onset (LOD) vs. early-onset (EOD)
    depression
  • LOD has lower rate of family history, higher rate
    of dementia, and more white matter
    hyperintensities than EOD
  • EOD patients have greater hippocampal volume loss
    than LOD, possibly due to effects of excess
    glucocorticoid effects

15
  • Meta-analysis of 10 studies of 351 LOD, 174
    EOD, and 413 elderly NCs
  • Executive deficits are typical of LOD
  • Memory and psychomotor speed deficits are
    common to both

16
Depression, MCI, and Dementia
  • Disproportionate cerebral ischemia on MRI in
    patients with LOD led to notion of vascular
    depression (Krishnan et al, 1997)
  • Co-morbidity of depression and cognitive
    impairment in the elderly Does the denominator
    make a difference?
  • Cognitive impairment occurs 2555 (or more) of
    depressed elderly adults (Butters et al, 2000
    Lee et al, 2007 Lockwood et al, 2000)
  • Depression occurs in 1050 of community samples
    of adults with MCI (Apostolova Cummings, 2008)
  • Depression occurs in 50 or more patients with AD
    (Starkstein Mizrahi, 2006 Lyketsos et al, 2002)

17
  • Treated 73 elderly adults with major depressive
    disorder
  • Tested patients and 21 NCs at baseline, 1, 4,
    6, and 12 weeks
  • 32 patients responded to treatment with
    paroxetine (Paxil)
  • Rx responders did not improve on any cognitive
    measure

18
A Few Words about Treatment
NEJM, 2008
PLoS, 2008
2008
19
  • Identified 74 clinical trials of 12 drugs
    registered with FDA
  • Extracted efficacy data from these double-blind,
    placebo-controlled studies of short term
    treatment of depression
  • Recorded FDAs judgment (positive, negative,
    questionable)
  • Reviewed published studies identified best
    match
  • Categorized trials on basis of FDA regulatory
    decision
  • Computed effect size for each trial
  • Found that 12,564 patients participated in these
    trials
  • Data from 3449 (27) were not published
  • Data from 1843 (15) published in contradiction
    to FDAs finding
  • Effect sizes smaller for unpublished than
    published studies and for journal than FDA reports

20
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21
(2007)
  • 7 studies (n 903) 459 psychotherapy vs. 444
    combined
  • All studies involved adult patients with MDD
  • Mean baseline Hamilton DRS scores 17 (mild) to
    27 (severe)
  • 820 weeks treatment 1624 sessions mostly
    cognitive therapy
  • Dropout rates did not differ (25 combined 24
    psychotherapy)

22
Case S. O.
  • 63-year-old, married, retired electrical engineer
  • Chief complaint HPI
  • Complains of memory failures over past 3-4 years
    forgets church sermons, appointments, telephone
    numbers, chores, family events
  • Consulted neurologist, brain MRI showed scattered
    WMH, ? atrophy
  • Family history
  • Father died of Alzheimer disease at age 88
    mother died of cancer at age 77 patient has no
    siblings, but has 3 adult children, all healthy
  • Medical/psychiatric history
  • Hypertension, high cholesterol, acid reflux, and
    low mood/anxiety. Medications Lisinopril,
    Crestor, Niaspan, guanfacine, omeprazole,
    aspirin, Lexapro, Trazodone, and vitamins

23
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24
Conclusions
  • MDD is very prevalent, afflicts more women than
    men, and can emerge at almost any age
  • Frequently preceded or accompanied by other
    conditions
  • Likely caused by both genetic and non-genetic
    factors, but its pathophysiology remains poorly
    understood
  • More evidence points to monoamine deficiency
    and/or HPA abnormalities than other putative
    mechanisms
  • Neuroimaging studies suggest that abnormalities
    in several neural structures might play a role in
    MDD

25
Conclusions
  • Studies show state- and trait-like cognitive
    impairments of mild to moderate severity
  • Might vary with age of onset and co-morbid
    illnesses
  • Deficits more severe in elderly patients with
    depression
  • Executive deficits might be more specific to LOD
    decreased speed and memory are common to both EOD
    and LOD
  • Combined treatment better than monotherapy
  • However, psychotherapy leads to remission of
    symptoms in up to 50 of individuals with
    mild-moderate MDD
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