Tyramine, found in several foods, is metabolized by MAO. Ingestion and absorption of tyramine causes extensive release of norepinephrine, which can rapidly increase blood pressure to the point of causing hypertensive crisis.
Tyramine is a biogenic amine produced as a (generally undesirable) byproduct during the fermentation of certain tyrosine-rich foods. It is rapidly metabolized by MAO-A in those not taking MAO-inhibiting drugs. Individuals sensitive to tyramine-induced hypertension may experience an uncomfortable, yet fleeting, increase in blood pressure after ingesting relatively small amounts of tyramine.[20][19][21]
Advances in food safety standards in most nations, as well as the widespread use of starter-cultures shown to result in undetectable to low levels of tyramine in fermented products has rendered concerns of serious hypertensive crises rare in those consuming a modern diet.[22][21] Those treated with MAOIs should still exercise caution, particularly at home, if it is unclear whether food has been properly refrigerated. Since tyramine-producing microbes also produce compounds to which humans have a natural aversion, disposal of any questionable food—particularly meats—should be sufficient to avoid hypertensive crises.
Adverse effects
Incidence of adverse effects[17]Very common (>10% incidence) adverse effects include:
Of note, there has not been found to be a correlation between sex and age below 65 regarding incidence of adverse effects.[17]
Tranylcypromine is not associated with weight gain and has a low risk for hepatotoxicity compared to the hydrazine MAOIs.[17][11]
It is generally recommended that MAOIs be discontinued prior to anesthesia; however, this creates a risk of recurrent depression. In a retrospective observational cohort study, patients on tranylcypromine undergoing general anesthesia had a lower incidence of intraoperative hypotension, while there was no difference between patients not taking an MAOI regarding intraoperative incidence of bradycardia, tachycardia, or hypertension.[23] The use of indirect sympathomimetic drugs or drugs affecting serotonin reuptake, such as meperidine or dextromethorphan poses a risk for hypertension and serotonin syndrome respectively; alternative agents are recommended.[24][25] Other studies have come to similar conclusions.[17] Pharmacokinetic interactions with anesthetics are unlikely, given that tranylcypromine is a high-affinity substrate for CYP2A6 and does not inhibit CYP enzymes at therapeutic concentrations.[20]
Tranylcypromine abuse has been reported at doses ranging from 120 to 600 mg per day.[10][26][17] It is thought that higher doses have more amphetamine-like effects and abuse is promoted by the fast onset and short half-life of tranylcypromine.[17]
Cases of suicidal ideation and suicidal behaviours have been reported during tranylcypromine therapy or early after treatment discontinuation.[10]
Symptoms of tranylcypromine overdose are generally more intense manifestations of its usual effects.[10]
Interactions
In addition to contraindicated concomitant medications, tranylcypromine inhibits CYP2A6, which may reduce the metabolism and increase the toxicity of substrates of this enzyme, such as:[19]
Tranylcypromine acts as a nonselective and irreversible inhibitor of monoamine oxidase.[4] Regarding the isoforms of monoamine oxidase, it shows slight preference for the MAOBisoenzyme over MAOA.[20] This leads to an increase in the availability of monoamines, such as serotonin, norepinephrine, and dopamine, epinephrine as well as a marked increase in the availability of trace amines, such as tryptamine, octopamine, and phenethylamine.[20][19] The clinical relevance of increased trace amine availability is unclear.
It may also act as a norepinephrine reuptake inhibitor at higher therapeutic doses.[20] Compared to amphetamine, tranylcypromine shows low potency as a dopaminereleasing agent, with even weaker potency for norepinephrine and serotonin release.[20][19]
Tranylcypromine has also been shown to inhibit the histone demethylase, BHC110/LSD1. Tranylcypromine inhibits this enzyme with an IC50 < 2 μM, thus acting as a small molecule inhibitor of histone demethylation with an effect to derepress the transcriptional activity of BHC110/LSD1 target genes.[27] The clinical relevance of this effect is unknown.
Tranylcypromine has been found to inhibit CYP46A1 at nanomolar concentrations.[28] The clinical relevance of this effect is unknown.
Mechanism of tranylcypromine inhibition of MAO.[29]
Pharmacokinetics
Tranylcypromine reaches its maximum concentration (tmax) within 1–2 hours.[20] After a 20 mg dose, plasma concentrations reach at most 50-200 ng/mL.[20] While its half-life is only about 2 hours, its pharmacodynamic effects last several days to weeks due to irreversible inhibition of MAO.[20]
Metabolites of tranylcypromine include 4-hydroxytranylcypromine, N-acetyltranylcypromine, and N-acetyl-4-hydroxytranylcypromine, which are less potent MAO inhibitors than tranylcypromine itself.[20]Amphetamine was once thought to be a metabolite of tranylcypromine, but has not been shown to be.[20][30][19]
Tranylcypromine inhibits CYP2A6 at therapeutic concentrations.[19]
Tranylcypromine was originally developed as an analog of amphetamine.[4][20] Although it was first synthesized in 1948,[32] its MAOI action was not discovered until 1959. Precisely because tranylcypromine was not, like isoniazid and iproniazid, a hydrazine derivative, its clinical interest increased enormously, as it was thought it might have a more acceptable therapeutic index than previous MAOIs.[33]
The drug was introduced by Smith, Kline and French in the United Kingdom in 1960, and approved in the United States in 1961.[34] It was withdrawn from the market in February 1964 due to a number of patient deaths involving hypertensive crises with intracranial bleeding. However, it was reintroduced later that year with more limited indications and specific warnings of the risks.[35][20][19]
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AI Overview
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Tranylcypromine (Parnate), CAS 155-09-9, is an irreversible monoamine oxidase inhibitor (MAOI) used to treat major depressive disorder. It is
available by prescription at pharmacies like Amazon Pharmacy or Blink Health, usually as 10 mg tablets (sulfate salt, CAS 13492-01-8). It requires a doctor's prescription due to significant drug/dietary interactions.
How to Buy Tranylcypromine (Parnate)
Retail Pharmacies (Prescription Required): Tranylcypromine (10 mg tablets) is widely available in the US with a prescription. It can be found at:
Amazon Pharmacy: Offers both generic Tranylcypromine and branded Parnate.
Blink Health: Offers online purchase options for Parnate (tranylcypromine sulfate).
Local Pharmacies: CVS, Walgreens, and others stock this antidepressant, generally as generic to keep costs lower, although branded Parnate exists.
Chemical Suppliers (Research Only - Not for Human Consumption):
For research and development purposes, the compound is available as a free base (CAS 155-09-9) or sulfate salt (CAS 13492-01-8) from suppliers such as:
Pharmaffiliates: Highly pure API (Active Pharmaceutical Ingredient).
MuseChem: Offers research quantities.
MedChemExpress: Known for chemical standards.
MedKoo Biosciences: Specialized in MAOI inhibitors.
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Key Medical Considerations
Dietary Restrictions: Patients taking Tranylcypromine must avoid foods high in tyramine (aged cheeses, processed meats, fermented products) to avoid severe hypertension.
Side Effects: Potential for serious side effects requires careful medical supervision, particularly in the elderly.
Not a Substitution for Medical Advice: Do not purchase this medication through non-prescription channels for self-treatment.
National Institutes of Health (NIH) | (.gov) +4
Disclaimer: This information is for informational purposes only and does not constitute medical advice or promotion of chemical sales. Always consult a healthcare professional for mental health issues.
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CAS 155-09-9: Tranylcypromine
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