Depression and anxiety disorders Flashcards
Current theory
Cortisol is usually elevated in depressed patients; glutamate levels are increase in depression, which can lead to excitotoxicity and apoptosis.
For our purposes, the monoamine theory is the most important relating to medications.
The traditional theory: “Monoamine Hypothesis” – with a deficiency of monoamine neurotransmitters (NA and 5-HT)
What strategies might address a monoamine deficiency?
Theoretically, we must increase or supplement the concentration of neurotransmitter in some way to “fix” or compensate for the shortage;
Strategies used in depression treatment:
• Prevent neurotransmitter from being taken up back into the neuron;
• Prevent neurotransmitter from being enzymatically broken down.
Tricyclic Antidepressants: Imipramine
Imipramine was the first TCA to be developed (late 1950s), and due to their adverse effects they are not now used in first line treatment.
Imipramine is considered for treatment of resistant depression as well as for generalised anxiety disorder.
How do TCAs work
TCAs inhibit the reuptake of both noradrenaline (NET) and serotonin (SERT) into the presynaptic neuron. Sounds great, as we target the two neurotransmitters that have
decreased activity in depressed patients.
TCAs also bind and antagonise histamine H1 receptors (sedation); α-adrenoreceptors (postural hypotension); muscarinic acetylcholine receptors (blurred vision, dry mouth and constipation)
TCA side effects
TCA side effects can be serious and may discourage patients from taking their medication.
Blockade of muscarinic cholinergic receptors may lead to tachycardia due to prolonged QT of the ECG.
• Therefore, overdose of TCAs can be FATAL due to their cardiac effects. TCAs should never by used by someone taking additional drugs which affect the cholinergic system.
• Nevertheless, the good effects outweigh the bad side effects in most cases, and TCAs have helped many patients.
Selective Serotonin Reuptake Inhibitors
SSRIs
SSRIs bind and block SERT proteins, preventing re-uptake and slowing degradation of 5-HT in the presynaptic neuron.
Long term use increases cAMP signalling and phosphorylation of nuclear transcription factor CREB, increases in neurogenesis from progenitor cells of hippocampus as well as downregulation of SERT – leading to elevated 5-HT levels.
• For most patients,, SSRIs are more effective than TCAs in relief of depression, and these are usually the first-line agents used in treatment..
Serotonin and Noradrenaline Reuptake Inhibitors: SNRIs
Both NA and 5-HT synapses are affected simultaneously, but with greater specificity than the TCAs.
• Minimal affinity and thus minimal antagonism of histamine H1 or muscarinic ACh receptors, so reduced sedation or cardiovascular effects.
SNRIs: compare to TCAs and SSRIs?
- Has pharmacological actions similar to both, but fewer of the side effects than TCAs due to lesser affinity for and antagonism of cholinergic and adrenergic receptors.
- SNRIs inhibit SERT, which leads to activation of autoreceptors and then desensitization.
Serotonin Syndrome
Combinations with the following drugs are contraindicated while taking a MAOI (Monoamine oxidase inhibitors) and for 14 days after stopping it because of the possibility of either severe hypertension (resulting from the accumulation of endogenous catecholamines) or the development of serotonin toxicity during this period:
atomoxetine, cocaine, desvenlafaxine, dexamphetamine, dextromethorphan, duloxetine, entacapone, ephedrine, fentanyl, linezolid, methylphenidate, mianserin, pethidine, phentermine, phenylephrine, pseudoephedrine, reboxetine, SSRIs, TCAs, tramadol and venlafaxine.
Be aware that toxicity may result from misuse of drugs, eg amphetamines, cocaine, pethidine, and that the nonselective MAOIs also interact with some illicit drugs, eg ‘ecstasy’, LSD.
MAO (Monoamine oxidase)
These enzymes have major roles in metabolism of exogenous (dietary tyramine) and endogenous (monoamines) compounds.
We have two forms of MAO enzymes in the brain:
MAO-A – located throughout tissues, in gut and CNS; metabolises tyramine in the intestine and preferentailly NA, 5-HT in the CNS.
MAO-B: located in CNS dopaminergic neurons where it preferentially metabolises DA.
MAO-A-inhibitors are used to treat depression, while MAO-B-inhibitors are utilised in Parkinson’s Disease to increase dopamine concentrations.
Some strategies which work across various diseases:
either add neurotransmitter or its precursor
Prevent neurotransmitter from being taken up back into the neuron
Prevent neurotransmitter from being enzymatically broken down.
MAOI mechanisms of action
In some cases, the MAOI covalently binds to MAO-A. This requires the neurons to synthesize new MAO-A enzyme every time antagonism occurs to replenish supply.
In the gut, irreversible inhibition of MAO-A means that tyramine is NOT broken down in the GI tract, and unaltered tyramine can readily enter the blood stream.
Tyramine crosses the BBB, enters neurons by NET, and displaces noradrenaline from synaptic termini, triggering a sudden and dangerous increase in blood pressure.
Patients are placed on tyramine- restricted diets while on MAOI medication: no cheese, yeast (Vegemite!), beer, Chianti wine, avocados, yogurt, soy sauce, bean pods, banana skins; as well as some medications, such as L- DOPA and SSRIs.
If patient ingests these things, they may have skin flushing and strong headaches… a “cheese reaction”
(Monoamine oxidase inhibitors) MAOI - medications
Isocarboxazid, Phenelzine, Selegiline, Tranylcypromine.
Dietary requirements - no food containing tyramine
Adverse effects: HTN, palpitations, chest pain, muscle rigidity, nausea, sedation, confusion.
Selegiline was put on the market in the form of a transdermal patch, which bypasses the digestive tract, and reduces risk of hypertensive crisis.
Good news: more selective MAO-A inhibitors are being found, such as moclobemide, which is short- acting and safer than earlier forms in this class.
Toxicity and major interactions with food make these a less preferred choice for depression.
Other antidepressants
NDRIs - noradrenaline-dopamine reuptake inhibitors
- bupropion IR, SR, XL
(contraindicated in patients with anorexia, bulimia, or seizure disorders)
Mixed action antidepressants - serotonin 5-HT2A receptor antagonists
- mirtazapine, nefazodone, trazodone
Agomelatine (Valdoxan)
(2011): Used to treat anxiety in depressed patients.
• MOA: acts as agonist on melatonin receptors MT1 and MT2 as well as
antagonising 5-HT2C.
• It is thought that agomelatine thus resynchronises circadian rhythms that are disrupted in depressed patients.
• Agomelatine is also a non-monoadrenergic compound; used in depression and anxiety?
Choosing antidepressant class
Approximately half of adults with moderate-to-severe major depression respond to antidepressant treatment, and relapse is relatively common.
• Most antidepressant drugs are approximately equal in efficacy, although individual patient response may vary markedly. Similarly, although the antidepressant classes have different adverse effects, no class is clearly superior in terms of tolerability.
• SSRIs can be regarded as first-line drugs in adults due to their generally favourable risk–benefit ratio.
• Nonselective MAOIs (phenelzine, tranylcypromine) are generally used for those who have previously responded well to them, or when other treatments are ineffective or not tolerated.
