Mood Disorders Flashcards
Major depressive disorder (MDD)
- Characteristics (3)
- Prevalence
- Sadness
- Hopelessness
- Anhedonia
— - Diagnosed more in women
- Onset 27 years ild
Major depressive disorder (MDD):
- Symptoms (9)
- DSM-5 diagnosis requirements
- Depressed mood
- Anhedonia
- Significant unintentional weight loss or gain
- Insomnia or hypersonbia
- Psychomotor changes (Agitation and slowing)
- Low energy, fatigue, tired ess
- Impaired ability to think, concentrate, make decisions
- Sense of worthlessness or excessive guilt
- Suicidal thoughts
— - Combo of 5+ symptoms during 2-week period; 1 symptom must be depressed mood or anhedonia
- Important not to have history of manic or hypomanic episodes cuz this would be bipolar disorder
MDD risk factors (4)
- Early life trauma
- Recent major life stress
- Family history of depression (esp first-degree)
- Personal history of depression (Relapse)
Areas of volumetric reductions in MDD (5)
- What circuit are some of these a part of?
- Gray matter is lower in what regions w/ early life trauma (CM+), family members (FH+), ppl w/ depression (MDD)
- Anterior cingulate cortex (ACC)
- Orbitofrontal cortex (OFC)
- Hippocampus
- Striatum
- Insula
- Cortico-striatal-pallidal-thalamic circuits (involved in cog and emotional processes)
— - CM+: Hippocampus and ACC
- FH+: Insula, cingulate cortex, OFC
- MDD: Hippocampus, insula, cingulate cortex, OFC
Enhancing NeuroImaging Genetics through Meta-Analysis (ENIGMA) did diffusion tensor imaging (DTI) study
- Found changed in white matter where? (2)
- Diffs not present in who? Not related to what? What are they driven by?
- Corpus callosum
- Cingulum bundle
— - Not present in adolescents and first episode patients
- Not related to symptom severity
- Driven by recurrent MDD
Metabolic activity in MDD:
- Increase where? (2)
- Decrease where? (1)
- Amygdala and OFC
- Increased emotional/threat response
— - Subgenual ACC
- Reduced reward processing
Serotonin:
- Impacts what? (4)
- Reduced 5-HT receptor binding potential where? (3)
- This is a risk factor for what?
- Result of face matching task study w/ fearful/angry faces?
- Mood
- Response to stress
- Sleep-wake cycle
- Memory
— - Hippocampus
- Amygdala
- Raphe nuclei
—
Risk factor for developing MDD
—
Ppl w/ higher than avg amygdala reactions had lower 5HT1A receptor binding - Shows receptor important for regulating responses to negative emotions
MMD treatments:
- SSRI (Selective serotonin reuptake inhibitors); fluoxetine, paroxetine, sertraline
- Effect on symptoms
- Effects related to what changes (2)
- CBT (Cognitive behavioural therapy)
- Compared to medication?
SSRIs:
- Commonly prescribed antidepressants that increase lvls of serotonin in synapse by blocking serotonin transporter involved in reuptaking serotonin into neurons
- Little effect on cognitive symptoms but can increase serotonin within hours; takes 4-8 weeks to impact other symptoms tho
- Effects may be related to change in postsynaptic receptors or neurogenesis; Found in rodents that chronic treatment increased cells in hippocampus and hippocampal gray matter vol in humans after 8 weeks
—
CBT:
- Talk therapy w/ licensed therapist to reframe negative thinking + learn how to respond to challenging situations in more effective ways
- As effective as medicine for MDD and reduced relapse rates
Bipolar disorder (BD):
- Age of onset
- Bipolar I disorder
- Bipolar II disorder
- Cyclothymic disorder (Cyclothymia)
- 25 years old
—
BIPOLAR I: - 1+ manic episodes (no depression) lasting 1 week present most of the day nearly everyday
- At least 3 symptoms of mania (grandiosity, reduced need for sleep, increased talkativeness, flight of ideas, distractibility, increased activity/agitated movements, risky behavs)
- Mood disturbances must cause marked impairment in social/occupational function, necessitate hospitalization or have psychotic features
—
BIPOLAR II: - 1+ hypomanic episode lasting at least 4 days, present most of the day, nearly every day
- Not severe enough to cause marked impairment, hospitalization, or psychotic features
- 1+ major depressive episode
— - At least 2 years, many periods of hypomanic and depressive symptoms but don’t meed criteria for episodes
- Symptoms lasted for at least 1/2 of time and never stopped for more than 2 months
BD risk factors (4)
- Family history (w/ first-degree, 8-10 times more likely)
- Early life trauma (50% dealt with childhood abuse, leads to earlier onset and higher severity)
- Recent negative life events (Increases and lengthens depressive episode but not mania/hypomania)
- Recent goal attainment events (Increases manic/hypomanic but not depressive symptoms)
Gray matter changes in BD (3)
White matter changes according to ENIGMA diffusion tensor imaging (DTI) study
Manic episodes assoc w/ decreased gray matter volume in:
- Dorsolateral PFC
- Inferior frontal cortex
- Anterior cingulate cortex (ACC)
*Euthymic periods had no structural or even increased changes, reflecting recovery mechanisms
—
- Corpus callosum
- Cingulum bundle
BD treatments
- Lithium
- Anticonvulsants (Carbamazepine, divalproex (valproate), lamotrigine)
- Atypical antipsychotics (Risperidone, olanzapine, quetiapine)
- Antidepressants
- Cognitive behavioural therapy (CBT)
LITHIUM:
- Effective for treating mania/hypomania but slow and narrow therapeutic index; Modest effects for classic BD but increase risk of suicide
- Side effects: Nausea, decreased thyroid function, tremor, weight gain, impaired cognition, risk of toxicity
- Mechanisms still unknown but preserves/increases vol of brain structures involved in emotional regulation (PFC, hippocampus, amygdala), inhibits excitatory neurotransmission and increases GABA, targets second-messenger symptoms like protein kinase C (PKC) which is overexpressed in BD
—
ANTICONVULSANTS:
- Carbamezapine and divalproex used to treat mania (esp for mixed state and rapid cycling BD)
- Lamotrigine reduces risk of recurrent depressive eps, but not effective for mania
- Interferes w/ intracellular calcium signalling (blocks Ca2+ channels), agonistic fx on GABAergic neurotransmission (increase GABA receptors to increase release of GABA)
- Side effects: Nausea, dizziness, fatigue, skin rashes, weight gain
—
ANTIPSYCHOTICS:
- Efficacy in treating mania and mixed state BD; Modest effects for BD depression
- Side effects: Tardive dyskinesia, weight gain, diabetes, high cholesterol
—
ANTIDEPRESSANTS:
- Treats BD depression but efficacy and safety controversial
- May lead to mood switches and rapid cycling; requires combo w/ mood stabilizer to reduce risk
—
CBT:
- Treats BD depressuon
- Help identify and monitor early signs of mood changes, manage stress/interpersonal difficulties, encourage medication adherence, and develop/use relapse prevention plans
Reward processing
- 3 broad components
- Reward system brain areas (6)
Encompasses response to rewarding stim, ability to learn from reward, anticipation of future rewards, engagement in goal-directed behavs towards rewards
- Drive toward a reward (motivation), hedonic exp (feelings of pleasure), reward learning (learn from and use rewards to guide behav)
—
- Ventral tegmental area (VTA)
- Ventral striatum (nucleus accumbens)
- Orbitofrontal cortex (OFC)
- Medial prefrontal cortex
- Anterior cingulate cortex (ACC)
- Anterior insula
Reward processing:
- In MMD + reward learning task w/ mouth
- In BD + areas of higher activation (3)
- MMD vs BD rigged monetary reward task w/ cards
- Linked to reduced reward learning
- Task involved identifying if short or long mouth belonged to mouthless cartoon face and were given rigged rewards for correct answer (one mouth gave more rewards)
- MDD/high anhedonia showed reduced reward learning ability and didn’t show reward bias
— - Assoc w/ hyper-responsiveness to reward cues + reduced ability to delay responding for rewards even in euthymic state
- OFC, ventrolateral prefrontal cortex, ventral striatum
— - Guess whether card would be red or black + gain money if right; Rigged so equal wins and losses no matter what
- Wins>Losses would increase activity in ventromedial PFC, ACC, ventral striatum, insula (reward value and reward salience processing)
- Depression (MDD and BD) assoc w/ reduced activation of reward-related regions; BD depression assoc w/ greater activity in left ventral striatum compared to MDD
