Antidepressants

Question 1

Point prevalence of depression

Answer 1

At any point in time, 5-6% of the population is depressed

Question 2

Lifetime prevalence of depression

Answer 2

10% of people may become depressed during their lives

Question 3

How much of the population suffers from a specific form of effective disorder called Bipolar Disorder (Manic- Depressive Illness)?

Answer 3

1.2%

Question 4

T/F Prevalence for depression in men is twice that of women, equal for bipolar disorder.

Answer 4

FALSE; women is TWICE that of men, equal for bipolar disorder

Question 5

How many people do not get treatment for their depressive disease?

Answer 5

up to 2/3

Question 6

How many patients typically respond to available treatments?

Answer 6

85% (70% to drugs, another 15% to ECT)

Question 7

If left untreated, how many depressed adult patients commit suicide?

Answer 7

15-20%

Question 8

What are other patterns of morbidity seen in depressed patients?

Answer 8

(1) Unemployment
(2) Divorce
(3) Alcoholism
(4) Financial ruin
etc. ..

Question 9

Risk of depression increases if: (4)

Answer 9

(1) Family history of depression
(2) During postpartum period
(3) When patient is on certain drugs
(4) Undergoing anticipated stress

Question 10

What is the criteria for Major Depressive Episode? (3)

Answer 10

• Dysphoric mood, loss of interest or pleasure in all or most usual activities and pastimes that used to be pleasurable to them.
• Symptoms cause significant distress or impairment in social, occupational, or other areas
• Not due to general medical condition/substance use/not due to bereavement if loss of loved one occurred less than 2 months ago

Question 11

(Major Depressive Episode) At least 5 of the following symptoms occurring nearly every day for at least 2 weeks: (8)

Answer 11

(1) Poor appetite or significant weight loss (change of more than 5% body weight in a month)
(2) Insomnia or hypersomnia
(3) Psychomotor agitation or retardation
(4) Decrease in sexual drive
(5) Fatigue or loss of energy
(6) Feelings of worthlessness, self reproach, or inappropriate guilt
(7) Diminished ability to think or concentrate
(8) Recurrent thoughts of death, or suicide, or suicide attempt

Question 12

Tricyclic Antidepressants: Drugs

Answer 12

(1) Imipramine

(2) Amitryptiline

Question 13

Why are there so many different types of drugs?

Answer 13

They are all equally effective and variously ineffective because they are dependent upon the person (all are the equally efficacious)

Question 14

What are the 4 classes of Antidepressant drugs?

Answer 14

(1) Tricyclic Antidepressants
(2) Heterocyclic Antidepressants
(3) SSRIs
(4) Monoamine Oxidase Inhibitors (MAO)

Question 15

Heteroyclic Antidepressants: Drugs

Answer 15

(1) Mirtazapine
(2) Venlafaxine
(3) Bupropion

Question 16

Selective Serotonin Reuptake Inhibitors (SSRI): Drugs

Answer 16

(1) Fluoxetine
(2) Paroxetine
(3) Sertraline

Question 17

Monoamine Oxidase (MAO) Inhibitors: Drugs

Answer 17

(1) Phenelzine

Question 18

Therapeutic Mechanism of Antidepressants

Answer 18

Antidepressants either block NE and/or serotonin (5HT) uptake by presynaptic nerve endings (tricyclics, heterocyclics, and SSRIs) or slow down the breakdown or such monoamines. Therefore, it has been hypothesized that increasing the synaptic concentrations of the biogenic amines NE and especially 5HT may be implicated in their mechanism of action.

However, while the pharmacological effects of antidepressants (i.e. inhibition of reuptake or breakdown) occur rapidly, there is a 2-3 week delay in therapeutic relief of depression.

Question 19

What is the biogenic amine hypothesis?

Answer 19

An examination of the several elements in the 5HT signaling pathways, has suggested the following sequence of events:

• The 5HT1A receptors on presynaptic neurons act to inhibit the firing of serotogergic neurons. Additionally, both presynaptic alpha2 adenoreceptors and presynaptic 5-HT receptors act to inhibit the release of serotonin
• Antidepressant drugs prolong the exposure of synaptic receptors to transmitter. However, initially the effects the transmitters on the receptors of the presynaptic cells provide negative feedback which opposes the increase in serotoneric tone.
• After extended treatment, the inhibitory elements desensitize allowing the antidepressant drugs to have increased postsynaptic effects

Question 20

What have animal studies suggested as a model for depression? How?

Answer 20

Chronic stress; it produces long term elevation in corticosteroids which in turn has been shown to produce diminished synaptic plasticity and decreased hippocampal volume

Question 21

What do tricyclic antidepressants do?

Answer 21

block NE and 5-HT uptake

Question 22

What receptors do tricyclic antidepressants block? What do blocking these receptors cause?

Answer 22

(1) Muscarinic-cholinergic
(2) Histaminergic
(3) Alpha-1 adrenergic
- results in significant side effects including atropine-like symptoms of dry mouth, blurring vision, and constipation, hypotension, fatigue

Question 23

What happens if you give a tricyclic antidepressant to a patient with bipolar disorder?

Answer 23

Has been associated with switching into mania.

Question 24

What is the difference between Venlafaxine, Mirtazapine, and Bupropion? (what do they inhibit, side effects, receptor blocking)

Answer 24

(1) Venlafaxine inhibits NE and 5HT without blockade of the receptors seen in tricyclics. Side effects like SSRIs
(2) Mirtazapine enhances NT at serotonin receptors by blocking alpha-1 receptors and presynaptic serotonin receptors. Side efects like SSRIs but not nausea. May have anxiolytic properties
(3) Bupropoin is a monoamine uptake blocker (NE, 5HT, and DA). Special indication for smoking cessation

Question 25

What are SSRIs becoming increasingly utilized?

Answer 25

Because they inhibit reuptake of biogenic amines at the transporter in presynaptic membrane but they are SPECIFIC in blocking reuptake of 5HT.

Question 26

SSRIs: side effects

Answer 26

(1) Nausea
(2) Vomiting
(3) Headache
(4) sexual dysfunction

Question 27

T/F SSRIs inhibit cytochrome P-450 enzymes in liver

Answer 27

TRUE

Question 28

Which SSRI has the longest half life?

Answer 28

Floxetine

Question 29

What are MAO inhibitors used for? What do these enzymes do?

Answer 29

• Reverse psychomotor retardation of depressed patients and also may increase the psychomotor activity to a hypomanic or manic state.
• oxidatively deaminate monoamines including catecholamines, serotonin, and others like tyramine

Question 30

What are 5 negative things related to MAO inhibitors?

Answer 30

(1) Combining MAO with SSRI results in excess serotonin or “central serotonin syndrome” which can lead to hyperpyrexia, confusion, and death
(2) chronic toxicity includes hepatotoxicity, tremors, insomnia, and hyperhidrosis, convulsions
(3) interferes with metabolic degradation of variety of drugs
(4) potentiate CV effects which produces hypertensive crisis
(5) tyramine foods (cheeses, beer, wine, yeast, coffee, etc)

Question 31

Which two drugs are relatively free of the sexual dysfunction side effect?

Answer 31

(1) mirtazapie- works on pre-synpatic receptors
(2) bupropion- direct reinforcing effects
(common for many especially SSRIs)

Question 32

What is bipolar disorder? Name the elevated states.

Answer 32

• Distinct period of persistently elevated or irritable mood for at least one week (following depressive episode)
• gradiosity, decreased sleep, more talkative, racing thoughts, increased distractability, increased motor activity, excessive involvement in high risk activities

Question 33

What are the 3 mood stabilizers that are used in biploar disorder? Which two are anticonvulsants (starred)?

Answer 33

(1) Lithium
(2) Divalproex- for acute mania
(3) Carbamazapine

Question 34

Is schizophrenia classified as part of bipolar disorder?

Answer 34

NO

Question 35

T/F Administration of lithium results in dose dependent disruption of distal tubular secretion in the kidney manifesting in oligouria.

Answer 35

FALSE; disruption of distal tubular reabsorption manifesting in polyuria

Question 36

What is the pharmacology of lithium?

Answer 36

1. Lithium is therapeutically effective in a relatively high concentration range of ≈1 mM. In this concentration range many brain systems may be affected.
2. Some of the potentially most important effects of lithium have been noted on second messengers such as cAMP and intracellular calcium signaling through the phosphoinositide pathway and protein kinase C. These pathways regulate long-term changes in synaptic function (e.g. LTP or LTD).
3. The permeability of lithium through sodium channels and synaptic ion channels (especially glutamate receptors) to may allow lithium to especially accumulate in active neurons.

Question 37

What is the therapeutic uses for lithium?

Answer 37

(1) lithium salts for recurrent episodes of mania/depression
(2) chronic use as prophylaxis
(3) acute treatment of manic phase and adjunct medication with antidepressants for depressive stage

Question 38

T/F Lithium has a low therapeutic index. Stating this, you need an adequate sodium intake to avoid lithium intoxication.

Answer 38

TRUE; low sodium diet and lithium is contraindicated

Question 39

What are other side effects and toxicity for anti-depressants?

Answer 39

1. Orthostatic hypotension (all but SSRIs).
2. Anticholinergic properties (Tricyclics and most hetrocyclics): dry mouth, blurred near vision, constipation, urinary hesitancy or retention; potentially confusion, agitation, delirium, and tachycardia in severe cases.
3. Sedation due to H1 antagonism The tertiary amines are typically more sedating and anticholinergic than the secondary amines. Nortriptyline has the least of these side effects for the tricyclics.
4. Cardiac toxicity: quinidine-like effect slowing intracardiac conduction (tricyclics).
5. Risk of death with overdose.
6. Generally need to monitor blood levels for therapeutic range.

Question 40

What additional potential applications for antidepressants are there? (13)

Answer 40

1. Depression with psychotic features (combined with antipsychotic)
2. During the depressed phase of Bipolar disorder (usually combined with mood stabilizer)
3. Atypical depression (SSRIs or monoamine oxidase inhibitors)
4. Panic disorder
5. Bulimia
6. Neuropathic pain (tricyclic drugs)
7. Enuresis (Imipramine best studied)
8. Obsessive-compulsive disorder (SSRIs and Clomipramine)
9. Attention-deficit/hyperactivity disorder
10. Cataplexy due to narcolepsy
11. Dysthymia (chronic low grade depression)
12. Organic mood disorders (caused by brain injury)
13. Smoking cessation (Bupropion)