Tongkat Ali and testosterone
Version 1.0, January 2004Unlike other authors who write patchwork articles (sewn together from the work of others) solely for the purpose of promoting their brand, I know exactly how tongkat ali feels (or doesn't feel), and what it does to me, and what it doesn't.I do, provided I have a proper extract, and not just some root powder, and not a shit that has been put on the market solely for the purpose of marketing, by people who know nothing about medicinal herbs, but a lot about spamming the Internet. If you buy tongkat ali root powder from websites by people who have no own stock and act only as agents forwarding drop ship orders, you have reason to feel cheated. I need the equivalent of about 50 gram of tongkat ali root per dosage if I want to achieve an effect, and after using it straight for about 2 weeks, I need the equivalent of 100 gram. I know exactly what the tongkat ali does for me, and what it doesn't, because, over more than a year of usage, I have done multiple challenges.
A "challenge" means: I judge the effect of tongkat ali not only (and not even principally) during periods during which I consume my daily dosage, but also, more importantly, during periods when I am tongkat ali sober. These periods turn out sober indeed. Tongkat ali is a hormonal modulator; as a rule of thumb, unless one ingests huge over dosages of hormonal products, one doesn't feel hormones (except thyroid). I have used growth hormone over months, and I did get the edema that is a typical side effect, but I never felt anything from growth hormone. I also didn't feel anything different during growth hormone off cycles. Growth hormone has likely been the most expensive placebo I ever tried. I also tried the full range of testosterone products: oral testosterone, Andriol and Proviron, testosterone patches and cream, aromatase inhibitors like anastrozole, and hypothalamic stimulators like clomiphene. Proviron feels like speed, and Andriol and testosterone patches and cream feel like nothing. Anastrozole, in combination with clomiphene or alone, may make me more aggressive (but I'm not 100 percent sure about this either), and provide no benefit sexually. I stop taking certain products when I have a sexual failure in spite of using them. And I initially became increasingly interested in tongkat ali because during periods during which I took my daily dosage, I never had a failure. And when I stopped using it, I do have my failures. I know for sure that genetically (and when I am sober) I do not have aggressive testosterone levels. I just have to take a look into the mirror to be sure of that. My hairline now (age 50) is exactly where it was 25 years ago. No pattern baldness. I also know it from my mother who told me that my father stopped having sex in his early 40s. And I remember when I was in my early teens, I once stumbled across a package of a testosterone capsules, which were the medication of my father. I am an apostle of sex, or even a sex maniac, not because I would be blessed with unlimited sexual desires, but for philosophical reasons. I find no solace whatsoever in religion, and I can't be mislead by Kantian stupidity, but I know how extremely good it feels to be engulfed by libido, and to have an explosive orgasm. I can't see any other purpose in life. I have elaborated further on my philosophy on the domain www.Kreutz-Philosophy.com. I have become an expert on sexual enhancement, because I need it. I have a very hard time to have an erection without Viagra or yohimbe. I will almost certainly not be able to have an erection in a sober state, even when I am together for the first time with a beautiful young woman. I can engineer erections with yohimbe or Viagra (50 to 100 mg). Yohimbe will even give me some libido; but yohimbe is a heavy-caliber drug. It makes me totally agitated, gives me tachycardia and palpitations, robs my sleep for at least 20 hours after ingesting it (which can easily add up to 30 hours without sleep if I take my dosage on the tenth hour of being awake). Yohimbe, for me, is an experience like an LSD trip. And I am totally worthless on the following day. Yohimbe is a prohibited drug in Australia, and I am surprised that it isn't (yet) in the US. But it weren't really the dreadful side effects that got me entirely off yohimbe. It was the fact that after hundreds of usages, my orgasmic pleasure vanished. I could have rock-hard erections (and I do mean: a tissue consistency of a stone), and be very focused mentally on what I was doing when I was doing it, and then I would have an orgasm which I hardly felt. My next phase were dopaminergics, and I did have great sex, and specifically great orgasms, with several of them. But dopaminergics work only a few times, unless one takes dosages appropriate for Parkinson's patients. Take bromocriptine: initially, one fourth of a 2.5 milligram tablet would allow me to totally forget myself during intercourse, and to enjoy pre-orgasmic plateaus that would last for minutes. Now I can take 2 tablets of 2.5 milligram and just feel no enhancement at all. I just get nauseated. I started taking a proper tongkat ali extract about a year ago, and it has been my mainstay since. So, what do I feel after ingesting about 1 gram of a 1:50 tongkat ali extract? Initially, I felt a slight hot-headedness, but this side effect has since subsided. Now, when I ingest 1 to 2 grams of tongkat ali extract, I feel … nothing. Please note: tongkat ali alone doesn't even give me erections. I still need the Viagra. I know when I have taken Viagra. I get an erection when I ought to. So, why bother with the tongkat ali? Yes, I have asked myself exactly this question quite a number of times. When I first took the tongkat ali 1:50 extract, and combined it with the Viagra, I did have good, proper sex every day. But I really didn't feel anything from the tongkat ali extract. At that time, I thought of myself that, man, you are in proper shape, and all you need is the Viagra. So I stopped taking the tongkat ali extract. For two or three days after stopping the tongkat ali extract, things were still just fine. And then I started failures in spite of having ingested the Viagra. The failure was not that I wouldn't have had an erection. Provided I had taken the Viagra, I did get sufficient erections. But I lacked libido. I could stop intercourse in the midst of it, and not even become frustrated or disappointed. I just wasn't sufficiently interested, even not with a new conquest. This happened two or three times, and then I did know that "no, things are not in order". Back on my daily dosage of about 1 gram of tongkat ali extract, such libido failures no longer occurred. This is a reliable test result. I can repeat it any time. I get off my daily tongkat ali dosage, and some two to 4 days later, I will have my first clear libido failure. I go back on the tongkat ali, and I seem to reach a peak after four to eight days: teeth-clinching sex; during these peak days, I know how a violent rapist must feel: "This bone must penetrate this hole. No matter what comes after. No, I cannot stop. I will not stop. No unfinished business. They can lock me up for 30 years, or hang me at the next tree, but here and now, this will go on until I have unloaded." If this is what goes on in the minds of rapists, then I envy them. Not for the 30 years or the next tree. But for their powerful libido, which really is the essence of life. I can taste this level of libido (and I am extremely thankful for it) when I am about a week into a tongkat ali cycle. I cannot plan the best episodes. Sometimes, I have absolutely extraordinary sex with a girl that is below my average, and no, it's not some hidden qualities of the girl that make for absolutely great sex, but it's me. It's my testosterone levels. It's the tongkat ali. I know from numerous challenges that this is how tongkat ali affects me. I never have really bad sex when on a combination of Viagra and tongkat ali extract. It's always satisfying. And sometimes it's blasting. I will have episodes of absolutely extraordinary sex at the beginning of a tongkat ali cycle, some 4 to 8 days into it. The tongkat ali will still work well in the second week, but in the third week, I will usually no longer be in the frame of mind for extraordinary sex on a 1-gram-a-day dosage. At that stage, I can still get a kick out of increasing the dosage to 2 gram a day, but after some 20 days into a cycle, the effect of tongkat ali will flatten. I will still have good sex, but it will not be teeth-clinching. Then it is about time to give the tongkat ali a break. For the first two to four days off, sex will still be satisfying, though lacking zest. And then the clear failures set in. Not erectile failures (as I still take my daily Viagra… which does not have to be cycled), but libido failures. Lack of interest. During my first off-cycles, I attributed the libido failures to the girl. She may not entirely be my type. But I know my type. And if I land one in bed, I should be properly aroused. I don't want to think: "Well, maybe better for the relationship if we first get to know each other. I mean, before penetration. No, that's wrong. I don't want to think like that. What I want to think is: "I want it now. All of it. And I don't give a damn if that is not-so-good for the relationship. I need it now. All of it." I can take libido failures only for a few days. Libido failures totally undermine my self-esteem. Tongkat ali is a God-sent for me. Up to now, through many months of usage, I have always been able to re-engineer teeth-clinching libido by entering a new tongkat ali cycle. It has no other effect on me. I don't know about others. Actually, I can imagine that for young men with no testosterone deficiency, tongkat ali makes no difference. If tongkat ali cures libido failures, or libido deficiencies, then this effect can be felt only by those who actually do have libido failures, or at least deficiencies. It may have other effects on other people. I have heard that bodybuilders use it as a mild substitute for steroids, and that some (previously) obese women swear on it as a slimming agent. I leave these fields of research to others. My specialty is sexual enhancement. And for that, tongkat ali works according to the pattern outlined above.
Dostinex and prolactin
Version 2.1, April 2003
Dostinex is a medication based on ergot alkaloids. Ergot, of course, is the fungal disease of rye and other grasses, and a potent neurotoxin. Ergot alkaloids heavily interfere with neurotransmitter activity. Probably the best known ergot derivate is LSD, which strongly messes with the neurotransmitter serotonin.
There are a good number of ergot alkaloids that are used in conventional medicine. Usually, these medications are developed for their dopaminergic capabilities. Such medications are needed to treat the severe deficiency of the neurotransmitter dopamine that leads to Parkinson's.
The ergot alkaloid bromocriptine (Parlodel) can be used for its sexuality enhancing properties. Actuality, of all substances I have tested on myself for their sexuality-enhancing properties, bromocriptine, as well as Dostinex, are among the few for which I can attest effectiveness. However, bromocriptine has to be taken in a specific manner to avoid the nausea that otherwise would overshadow its sexuality-enhancing properties. Please see the bromocriptine articles on apomorphine.org for details. Dostinex is largely free of negative side effects, at least in me.
Of all dopaminergic medications used for the treatment of Parkinson's, Dostinex and Parlodel are the most similar to each other, with their double action of enhancing dopamine levels and inhibiting the secretion of the hormone prolactin from the anterior pituitary gland.
I am convinced that this dual action is crucial to sexual enhancement. Prolactin, the hormone, which has been named for its function of inducing lactation in women, directly interferes with sex drive in both women and men. It controls to a certain extent the secretion of gonadotropin, the hormone, which, one step further down the chain, controls the secretion of testosterone in both men and women. Regardless of which hormonal constellation in this sequence is responsible for a lowered sex drive, the reversal of the sequence through drugs like Dostinex and Parlodel clearly supports sexual desire.
As sexuality is the main source of happiness for practically all forms of higher living, including man, and as utmost sexual satisfaction can only be experienced as a sequence to sexual desire, it is a logical quest to provide ourselves with a better long-term hormonal profile than intended by our genetic blueprints. Anti-sexual changes of our hormonal levels as a consequence of the aging process is an unacceptable provision, which nature, our enemy, has designed in order to install the specific generation turnover rate of humans (20 to 30 years).
Increasing prolactin levels and, at the same time, decreasing testosterone levels are two inter-linked causes why aging men don't have as much sex drive as younger men, why they don't have orgasms as powerful as they used to have, and why they don't get as much pleasure out of their sex lives as they did when they were in their 20's.
To interfere with this chain of events isn't easy. Testosterone supplementation often doesn't do the trick. Each person's body has its own genetically set ideas what the person's age-appropriate testosterone levels ought to be. Supplying additional testosterone will, in healthy subjects, just provoke the body to down-regulate its own testosterone production, as well as to initiate other measures by which the testosterone balance returns to the aforementioned genetically set levels.
Willfully oversupplying testosterone, or supplementing with synthetic steroids is usually useless, at least for men. Women, if they don't mind the androgenic side effects (increased muscle buildup), may be able to increase desire and orgasmic capacity through both testosterone and synthetic steroid supplementation.
But for men, forcing testosterone levels beyond the genetic set points, mainly through the supplementation with synthetic steroids, has some very counterproductive side effects. It will, for example, result in shrinkage of the male organ, and problems achieving an erection.
The prolactin reduction pathway doesn't seem to be bedeviled in the same manner. I can attest from my own experience that Dostinex and bromocriptine enhance sexual functionality as well as the intensity of orgasm. (Please see my articles on bromocriptine for the finer points on how to dose bromocriptine for sexual enhancement, and how to avoid the nausea.) On the other hand, my own experimentation with the supplementation of testosterone (Andriol capsules) had no measurable effect on sexual desire at all, not immediate and not long-term.
There are an enormous number of compounds, both herbal and synthetic, which can kill sex drive and interfere with sexual performance. There are also a good number of products, both herbal and synthetic, which are sold with the promise that they help to overcome a lack of sexual desire or so-called erectile dysfunction.
I have been writing about pharmacological sexual enhancement for years, and I take the matter seriously. I have tried almost everything that is available under the sun, whether from below (ginseng) or above (ginkgo) the grass line, and both natural and synthetic (such as Viagra).
While Viagra definitely works for erections, I feel that Viagra alone does not provide any kick in the desire or orgasm departments. A combination with other drugs, especially Dostinex, can bring out the best in Viagra.
Tongkat ali studied as cancer treatment
Version 1.0, December 2004
When your average pharmaceutical product gets into the headlines because of side effects, than it's almost always because of some unwanted effects that have been discovered "later on".
With tongkat ali, it's a different story. The more research is done into tongkat ali, the more surprising positive side effects, or medical applications, are discovered for it. Not that this would be news to Southeast Asian shamans who have been using the root for centuries. In Vietnam, for example, the local name of tongkat ali translates as "the plant that cures a hundred diseases". Or was it a thousand?
The latest lab reports indicate, for example, that tongkat ali (Eurycoma longifolia by its Latin, scientific name) may be a powerful weapon against lung cancer and breast cancer.
The following is the abstract of a scientific article that has recently been included at the Medline database. You can read the abstract here:
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve
&db=pubmed&dopt=Abstract&list_uids=14738962
Chairman MAO
Version 2.1, April 2002 (rev.)
Are yohimbe
and/or yohimbine MAO inhibitors? There seems to be a fair bit of confusion. The
confusion is caused by the fact that while yohimbe and yohimbine are not MAO
inhibiting in the same manner as drugs used expressively as MAO inhibitors (see
list at the end of this article), there indeed seems to be some influence on
MAO activity.
Ellen
Coleman, RD, MA, MPH, claims on the Health Care Reality Check web site (quoted
August 19, 1999):
"Yohimbine
is a monoamine oxidase inhibitor which means that tyramine containing foods
(red wine, liver, cheese) and nasal decongestants or diet aids containing
phenylpropaanolamine should be rigorously avoided if it is used to prevent a
hypertensive crisis."
While the
Health Care Reality Check web site is dedicated to the noble task (as are we)
of protecting consumers from quacks who will sell anything as remedy against
any condition as long as it earns them a buck, they exaggerated their reporting
on yohimbe and yohimbine:
"According
to the FDA, documented health hazards include low blood pressure, weakness, and
nervous stimulation, followed by paralysis, fatigue, stomach disorders, kidney
failure, seizures and death. The FDA has declared yohimbine unsafe and
ineffective for over the counter sale."
This is
simply wrong. Yohimbine may not be an over-the-counter medication. But
yohimbine is a FDA-approved prescription drug. If it were inappropriate, the
FDA approval would be withdrawn. And as far as "documented health
hazards" are concerned, well, death, and a variety of diseases leading to
it, are documented health hazards for many antibiotics. And like antibiotics,
yohimbine is useful in spite of documented health hazards associated with it.
But the topic
of this article is neither the Health Care Reality Check web site nor the
documented health hazards of yohimbe and yohimbine in general. The topic is
yohimbe / yohimbine and MAO inhibition.
Monoamine
oxidase (MAO) inhibition is a profound physiological event, definitely not
something to be overlooked in the description of any medication. Chairman MAO
is an enzyme present in various parts of the body, primarily in the digestive
system and the central nervous system. Its function is the deamination of foods
and neurotransmitters.
The crucial
impact of monoamine oxidase (MAO) inhibitors is related to this parallel
occurrence of monoamines in food and catecholamine neurotransmitters such as
dopamine, epinephrine (adrenaline), and norepinephrine (noradrenaline). If the
action of the MAO enzyme is interrupted, the breakdown of these catecholamine
neurotransmitters is hindered. This is, to a certain degree, wished for in the
treatment of Parkinson’s, a disease characterized by a depletion of dopamine.
MAO inhibitors
are "dangerous" medications because they not only inhibit the
breaking down of monoamine neurotransmitters but also can interfere with the
deamination of monoamines in the digestive tract. If then, monoamines make
their way past the digestive tract they can start acting in the same manner as
neurotransmitters, primarily norepinephrine, on a number of physiological
functions, especially blood pressure. A combination of MAO inhibiting drugs
with many ordinary foods that contain tyramines is a sure recipe for
hypertensive shock and death.
Usually,
red wine, chocolate, and cheeses are given as examples of foods containing
tyramines, but tyramines can occur in many other foods as well. Also, the
tyramine content of foods is difficult to predict. The content of tyramines in
many foods tends to increase with storage. In a fresher state, many different
kinds of food have a lower (or insignificant) content of tyramines, while after
having been stored for some time, the contents of tyramines are higher. There
are very long and explicit lists on tyramine contents in specific foods,
compiled for patients who have to take MAO inhibitors to control Parkinson’s.
Obviously,
the above is not a complete characterization of chairman MAO and MAO
inhibitors. For example, we have not discussed the difference between MAO-A and
MAO-B, as well as the effects of MAO on behavior (low levels of MAO are
associated with criminal behavior as well as with a polygamous lifestyle).
Nevertheless, the above may already give the reader an idea why it is very
unlikely that with a prescription medication such as yohimbine, there wouldn't
be an explicit warning if it were a MAO inhibitor.
Yohimex is
one of several brands of yohimbine tablets sold in the US. Yohimex is a prescription drug with 5.4 milligram of yohimbine hydrochloride as active
ingredient, manufactured by Jones Medical Industries in Canton, OH 44702, and distributed by Kramer Laboratories in Miami FL 33174. As Yohimex is a
prescription drug, it had to be reviewed by the FDA. It's hard to believe that
if yohimbine were indeed a definite MAO inhibitor, a specific note on the
subject matter would be missing from the brochure accompanying every bottle of
Yohimex.
Alas, the
package literature contains no reference claiming that yohimbine would be a MAO
inhibitor. The package literature has the following to say about the clinical
pharmacology of yohimbine hydrochloride:
"Yohimbine
blocks presynaptic alpha-2 adrenergic receptors. Its action on peripheral blood
vessels resembles that of reserpine, though it is weaker and of short duration.
Yohimbine's peripheral autonomic nervous system effect is to increase
parasympathetic (cholinergic) and decrease sympathetic (adrenergic) activity.
It is to be noted that in male sexual performance, erection is linked to
cholinergic activity and to alpha-2 adrenergic blockade which may theoretically
result in increased penile inflow, decreased penile outflow or both. Yohimbine
exerts a stimulating action upon the mood and may increase anxiety. Such
actions have not been adequately studied or related to dosage although they
appear to require higher doses of the drug…."
No word on
MAO inhibition. The Mosby RxList website also does not mention yohimbine as MAO
inhibitor.
(Reserpine
is a white to yellowish powder isolated from the roots of certain species of
Rauwolfia and used as a sedative and an antihypertensive.)
Well,
yohimbine and yohimbe are not exactly the same. Yohimbe is the raw tree bark,
and yohimbine is just one of its active ingredients that has been extracted.
Even if yohimbine is not a MAO inhibitor, it may still be the case that yohimbe
is.
We have
seen a number of web sites that claim that either yohimbine or yohimbe is a MAO
inhibitor, or that yohimbine isn't but yohimbe is.
However, we
haven't seen any conclusive study on yohimbe and MAO inhibition. If yohimbe
were a strong and definite MAO inhibitor, one would have to expect fatalities
if the usual precautions against tyramine-containing foods were not heeded. Any
herb that functioned as a definite MAO inhibitor would long ago have been
classified as a poison. But yohimbe has been sold as a supplement for years. If
incidences of death would have occurred after ingesting yohimbe because of
yohimbe being a MAO inhibitor, it's unlikely this fact would not be reported
widely. Alas, there are no widely circulating reports of yohimbe causing deaths
because of its effects as MAO inhibitor.
Sure,
yohimbe and yohimbine cause side effects, which could be interpreted as an
effect of MAO inhibition, mainly nervousness. But yohimbe usually does not
cause an increase in blood pressure.
A safe
assessment is that even if both yohimbine and yohimbe are not definite MAO
inhibitors, they shouldn't be taken together with MAO inhibitors. I would add
that people who are on MAO inhibition medication are anyway not physically well
enough to take an additional leisure medication as strong as yohimbe or
yohimbine.
Now, while
yohimbe and yohimbine are not MAO inhibitors to the extent in which the term
"MAO inhibitor" is pharmacologically understood, there is
nevertheless some correlation between yohimbine and MAO activity.
It has been
documented that yohimbine is an anxiogenic agent, a substance that can induce
anxiety in humans and other higher animals. The Yohimex package literature
states: "Yohimbine exerts a stimulating action upon the mood and may
increase anxiety. Such actions have not been adequately studied or related to
dosage although they appear to require higher doses of the drug…."
Anxiety is
the missing link between yohimbine / yohimbe and MAO inhibition, and it points
to a possible explanation why yohimbine / yohimbe act as aphrodisiacs, apart
from facilitating erections.
In 1996, a
study on the effects of some anxiogenic agents on brain monoamine oxidase
inhibitory activity was conducted at the Department of Pharmacology, Banaras Hindu University, Varanasi, India (Bhattacharya SK; Chakrabarti A; Sandler M; Glover
V). The study was done on rats, not on humans, as it involved dosages of
yohimbine far too high to be used for sexual stimulation. The study came to the
conclusion that in a state of anxiety induced by a sufficiently high dosage of
yohimbine, there has been a noticeable increase of MAO-inhibitory activity
without specific MAO-inhibitory pharmaceutical agents having been added.
This is of
course not surprising as in any stress situation, there will likely be
increased epinephrine (adrenaline) activity in any higher animal. Epinephrine
activity in the body is regulated twofold: as secretion and as deactivation
through chairman MAO. Additional secretion and inhibition of deamination by
chairman MAO have comparative effects: an increased epinephrine level, with the
typical stress-related symptoms.
A
reasonable hypothesis regarding the aphrodisiac properties of yohimbe and
yohimbine would probably have to consider the effect of the bark and its active
ingredient on the neurotransmitter dopamine. While the usual aim of any
treatment with MAO inhibitors is to raise levels of dopamine to control
Parkinson’s disease, it has been noted that raised dopamine levels normally
also bring about sexual agitation.
The link
between dopamine and sexual urge is so strong that scientific studies have been
undertaken to check to what extent measurable dopamine levels correlate to
sexual perversion (paraphilic disorder).
A 1995
research on "Dopamine and sexual behavior" at the Bernard B. Brodie
Department of Neuroscience, University of Cagliari, Italy, came to the
following result: "Despite some differences, most studies show that
treatments that increase or decrease, respectively, brain dopaminergic activity
improve or worsen, respectively, several parameters of copulatory activity,
supporting a facilitatory role of dopamine in male sexual behavior."
And a 1997
study at the Harvard Medical School in Boston on "A monoamine hypothesis
for the pathophysiology of paraphilic disorders" drew the following
conclusion:
"A
monoamine pathophysiological hypothesis for paraphilias in males is based on
the following data: (i) the monoamines norepinephrine, dopamine, and serotonin
are involved in the appetitive dimension of male sexual behavior in laboratory
animals; (ii) data gathered from studying the side effect profiles of
antidepressant psychostimulant, and neuroleptic drugs in humans suggest that
alteration of central monoamine neurotransmission can have substantial effects
on human sexual functioning, including sexual appetite; (iii) monoamine
neurotransmitters appear to modulate dimensions of human and animal
psychopathology including impulsivity, anxiety, depression, compulsivity, and
pro/antisocial behavior, dimensions disturbed in many paraphiliacs; (iv)
pharmacological agents that ameliorate psychiatric disorders characterized by
the aforementioned characteristics, especially central serotonin enhancing
drugs, can ameliorate paraphilic sexual arousal and behavior."
The study
refers to the well-known fact that many medications for Parkinson’s disease,
which all aim to increase levels of dopamine, have an increased sexual appetite
as a common side effect. Many, but not all Parkinson’s medications are MAO
inhibitors. If scientific studies were to be undertaken on any aphrodisiac
effect of yohimbine or yohimbe (apart from their well-documented effect of
making better erections), they would have to check on what effect yohimbine and
yohimbe have on dopamine levels, either through MAO modulation or via any
alternative pathway.
MAO
inhibitors, generic names and brand names:
benmoxin - Nerusil, Neuralex
echinopsidine iodide - Adepren
etryptamine - Monase
iproclozide - Sinderesin, Sursum
iproniazid - Iprozid, Ipronid, Marsilid, Rivivol, Propilniazida
isocarboxazid - Enerzer, Marplan, Marplon
mebanazine - Actamol
metfendrazine - H.M.-11
moclobamide - Aurorix, Manerix (reversible inhibitor)
nialamide - Espril, Isalazina, Mygal, Niamid, Niaquitil, Nuredal, Psicomidina,
Surgex
pargyline - Eudatine, Eutonyl, Tenalin
phenelzine - Nardil, Stinerval, Monofen, Fenelzin, Kalgan, Nardelzine
pheniprazine - Catron, Catroniazide, Cavodil, Fenizin
phenoxypropazine - Drazine
pivhydrazine - Neomarsilid, Tersavid
safrazine - Safra
selegiline, l-deprenyl - Eldeprine, Eldepryl, Jumex, Jumexal, Lesotal, Movergan
(selective MAO-B inhibitor)
toloxatone - Hymoryl, Perenum (selective MAO-A inhibitor)
tranylcypromine - Parnate, Sicoton, Transamin, Transapin, Tylciprine
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