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phenethylamine
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One of the two major chemical classes of
psychedelic drugs
, along with the
tryptamine
family. Examples of phenethylamines are
MDMA
,
mescaline
,
2C-B
, and
DOM
(aka STP).
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Mon Oct 16 2000 at 0:06:34
This is a recipe from
PiHKAL
. If you're interested in how the hardlinks were chosen, read
noding PiHKAL for Everything2
.
#142 PEA
PHENETHYLAMINE
SYNTHESIS:
This compound has been made industrially by a number of routes, the motant being the reduction of
benzyl
cyanide
and the
decarboxylation
of
phenylalanine
. It is offered in the catalogs of all the major chemical supply houses for a few pennies per gram. It is a very strong base with a fishy smell, and rapidly forms a solid
carbonate
salt upon exposure to the air. It is a natural
biochemical
in both plants and animals.
DOSAGE:
greater than 1600 mg.
DURATION:
unknown.
QUALITATIVE COMMENTS:
(with 200, 400, 800 and 1600 mg) No effects.
(with 500 mg) No effects.
(with 800 and 1600 mg) No effects.
(with 25 and 50 mg i.v.) RNo effects.
EXTENSIONS AND COMMENTARY:
Here is the chemical that is central to this entire book. This is the structural point of departure for every compound that is discussed here. It is the RPS in
PIHKAL
. It is without activity in man! Certainly not for the lack of trying, as some of the dosage trials that are tucked away in the literature (as abstracted in the "Qualitative Comments" given above) are pretty heavy duty. Actually, I truly doubt that all of the experimenters used exactly that phrase, "No effects," but it is patently obvious that no effects were found. It happened to be the phrase I had used in my own notes.
This, the simplest of all
phenethylamines
, has always been the darling of the
psychopharmacologists
in that it is structurally clean, it is naturally present in various human fluids and
tissue
s, and because of its close chemical relationship to
amphetamine
and to the
neurotransmitter
s. These facts continuously encourage theories that involve PEA in mental illness. Its levels in urine may be decreased in people diagnosed as being depressed. Its levels may be increased in people diagnosed as being paranoid
schizophrenic
s. Maybe it is also increased in people under extreme stress. The human trials were initially an attempt to provoke some
psychological
change, and indeed some clinicians have reported intense headaches generated in depressives following PEA administration. But then, others have seen nothing. The studies evolved into searches for
metabolic
difference that might be of some diagnostic value. And even here, the jury is still out.
Phen
ethylamine
is found throughout nature, in both plants and animals. It is the end product of
phenylalanine
in the
putrefaction
of
tissue
. One of its most popularized occurrences has been as a major component of
chocolate
, and it has hit the Sunday Supplements as the love-sickness chemical. Those falling out of love are compulsive
chocolate
eaters, trying to replenish and repair the body's loss of this compound--or so the myth goes. But this
amine
is voraciously metabolized to the apparently inactive compound
phenylacetic
acid, and to some
tyramine
as well. Both of these products are also normal components in the body. And, as a wry side-comment,
phenylacetic
acid is a major precursor in the illicit synthesis of
amphetamine
and
methamphetamine
.
Phen
ethylamine
is intrinsically a stimulant, although it doesn't last long enough to express this property. In other words, it is rapidly and completely destroyed in the human body. It is only when a number of
substituent
groups are placed here or there on the molecule that this
metabolic
fate is avoided and
pharmacological
activity becomes apparent.
To a large measure, this book has emphasized the "
phenyl
" end of the
phenethylamine
molecule, and the "what," the "where," and the "how many" of the
substituent
groups involved. There is a broad variety of chemical groups that can be attached to the
benzene
ring, at one or more of the five available positions, and in an unending number of combinations. And, in any given molecule, the greater the number of
substituent
s on the
benzene
ring, the greater the likelihood that there will be
psyche
delic action rather that stimulant action.
But what can be said about the "
ethylamine
" end of the
phenethylamine
molecule? This is the veritable backbone that holds everything tog
ether
, and simple changes here can produce new prototypes that can serve as starting points for the
substituent
game on the
benzene
ring. Thus, just as there is a "family" of compounds based on the foundation of
phenethylamine
itself, there is an equally varied and rich "families" of other compounds that might be based on some
phenethylamine
with a small modification to its backbone.
So, for the moment, leave the aromatic ring alone, and let us explore simple changes in the
ethylamine
chain itself. And the simplest structural unit of change is a single
carbon
atom, called the
methyl
group. Where can it be placed?
The adding of a
methyl
group adjacent to the
amine
produces
phenylisopropylamine
, or
amphetamine
. This has been exploited already as one of the richest families of
psyche
delic drugs; and over half of the recipes in Book II are specifically for
amphetamine
analogue
s with various
substituent
s on the aromatic ring. The further
methylation
of
amphetamine
with yet another
methyl
group, this time on the
nitrogen
atom, yields
methamphetamine
. Here the track record with various
substituent
s on the aromatic ring is not nearly as good. Many have been explored and, with one exception, the quality and potency of human activity is down. But the one exception, the N-
methyl
analogue
of
MDA
, proved to be the most remarkable
MDMA
.
The placement of the
methyl
group between the two
carbon
s (so to speak) produces a
cyclopropyl
system. The simplest example is
2-phenylcyclopropylamine
, a drug with the generic name of
tranylcypromine
and the trade name Parnate. It is a mono-
amine
oxidase
inhibitor and has been marketed as an anti
depressant
, but the compound is also a mild stimulant causing insomnia, restlessness and
photophobia
. Substitutions on the
benzene
ring of this system have not been too promising. The DOM
analogue
,
2,5-dimethoxy-4-methyltranylcypromine
is active in man, and is discussed in its own recipe under DMCPA. The inactive mescaline
analogue
TMT is also mentioned there.
The dropping of one
carbon
from the
phenethylamine
chain gives a
benzyl
amine
, basically an inactive nucleus. Two families deserve mention, however. The
phencylidine
area,
phenylcyclohexylpiperidine
or PCP, is represented by a number of
benzyl
amine
s. Ketamine is also a
benzyl
amine
. These are all
analgesic
s and
anesthetic
s with central properties far removed from the stimulant area, and are not really part of this book. There is a
benzyl
amine
that is a pure stimulant, which has been closely compared to
amphetamine
in its action This is
benzylpiperazine
, a base that is active in the 20 to 100 milligram range, but which has an acceptability similar to
amphetamine
. If this is a valid stimulant, I think that much magic might be found in and around compounds such as (1) the
MDMA
analogue
, N-(
3,4-methylenedioxybenzyl
)
piperazine
(or its N-
methyl
-counterpart N-(
3,4-methylenedioxybenzyl
)-N'-
methylpiperazine
) or (2) the DOM
analogue
,
2,5-dimethoxy-4-methylbenzylpiperazine
. The benzyl
amine
that results by the relocation of the
amine
group of
MDA
from the beta-
carbon
atom to the
alpha-carbon
atom is known, and is active. It, and its N-
methyl
homologue
, are described and discussed in the commentary under
MDA
. Dropping another
carbon
atom gives a yet shorter chain (no
carbon
s at all!) and this is to be found in the
phenylpiperazine
analogue
3-trifluoromethylphenylpiperazine
. I have been told that this base is an active
hallucinogen
as the
dihydrobromide
salt at 50 milligrams sublingually, or at 15 milligrams intravenously in man. The corresponding 3-chloro
analogue
at 20 to 40 milligrams orally in man or at 8 milligrams intravenously, led to panic attacks in some 10% of the experimental subjects, but not to any observed
psyche
delic or stimulant responses.
What happens if you extend the chain to a third
carbon
? The parent system is called the
phenyl-(n)-propylamine
, and the parent chain structure, either as the primary
amine
or as its
alpha-methyl
counterpart, represents compounds that are inactive as stimulants. The DOM-
analogue
s have been made and are, at least in the rabbit rectal
hyperthermia
assay, uninteresting. A commercially available fine chemical known as
piperonylacetone
has been offered as either of two materials. One, correctly called
3,4-methylenedioxyphenylacetone
or
3,4-methylenedioxybenzyl
methyl
ketone
, gives rise upon reductive
amination
to
MDA
(using
ammonia
) or
MDMA
(using
methylamine
). This is an aromatic compound with a three-
carbon
side-chain and the
amine
-
nitrogen
on the beta-
carbon
. The other so-called
piperonylacetone
is really
3,4-methylenedioxybenzylacetone
, an aromatic compound with a four-
carbon
side-chain. It produces, on reductive
amination
with
ammonia
or
methylamine
, the corresponding
alpha-methyl-(n)-propylamines
, with a four-
carbon
side-chain and the
amine
-
nitrogen
on the gamma-
carbon
. They are completely unexplored in man and so it is not known wh
ether
they are or are not
psyche
delic. As possible mis-
synthesize
d products, they may appear quite unintentionally and must be evaluated as totally new materials. The gamma-
amine
analogue
of
MDA
, a
methylenedioxy
substitute
d three
carbon
side-chain with the
amine
-
nitrogen
on the gamma
carbon
, has indeed been made and evaluated, and is discussed under
MDA
. The extension of the chain of mescaline to three atoms, by the inclusion of an oxygen atom, has produced two compounds that have also been assayed. They are mentioned in the recipe for mescaline.
The chain that reaches out to the
amine
group can be tied back in again to the ring, with a second chain. There are 2-aminobenzoindanes which are
phenethylamines
with a one-
carbon
link tying the
alpha-position
of the chain back to the aromatic ring. And there are 2-
aminotetralin
es which are
phenethylamines
which have a two-
carbon
link tying the
alpha-position
of the chain back to the aromatic ring. Both un
substitute
d ring systems are known and both are fair stimulants. Both systems have been modified with the DOM
substituent
patterns (called DOM-AI and DOM-AT respectively), but neither of these has been tried in man. And the
analogue
s with the
MDA
substitution
pattern are discussed elsewhere in this book.
And there is one more obvious remaining
methylation
pattern. What about
phenethylamine
or
amphetamine
compounds with two
methyl
groups on the
nitrogen
? The parent
amphetamine
example, N,N-di
methylamphetamine
, has received much notoriety lately in that it has become a scheduled drug in the United States.
Ephedrine
is a major precursor in the illicit synthesis of
methamphetamine
, and with the increased law-enforcement attention being paid to this process, there has been increasing promotion of the unrestricted
homologue
, N-
methylephedrine
, to the
methamphetamine
chemist. This starting material gives rise to N,N-di
methylamphetamine
which is a material of dubious stimulant properties. A number of N,N-di
methylamphetamine
derivatives, with "
psyche
delic" ring
substituent
s, have been explored as iodinated brain-flow indicators, and they are explicitly named within the appropriate recipes. But none of them have shown any
psyche
delic action.
This is as good a place as any to discuss two or three simple compounds,
phenethylamines
, with only one
substituent
on the
benzene
ring. The 2-
carbon
analog
of
4-MA
, is
4-methoxyphenethylamine
, or MPEA. This is a kissing cousin to DMPEA, of such fame in the search for a urine factor that could be related to schizophrenia. And the end results of the search for this compound in the urine of mentally ill patients are as controversial as they were for DMPEA. There has been no confirmed relationship to the diagnosis. And efforts to see if it is centrally active were failures--at dosages of up to 400 milligrams in man, there was no activity. The 4-chloro-
analogue
is
4-chlorophenethylamine
(4-Cl-PEA) and it has actually been pushed up to even higher levels (to 500 milligrams dosage, orally) and it is also without activity. A passing bit of charming trivia. A positional
isomer
of MPEA is
3-methoxyphenethylamine
(3-MPEA) and, although there are no reported human trials with this, it has been graced with an Edgewood Arsenal code number, vis., EA-1302.
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Psychedelic Guide: Ketamine
Substitute
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