Before starting this section on bliss I wish to
clarify that the experience of spiritual awakening is not "just" a
bunch of chemicals. Just because a particular subjective experience can
be the "cause of" or "caused by" a particular release of chemical or
electrical phenomena, doesn't mean to say that the subjective
experience can be reduced "down" to that physical chemistry. All
manifestation has its atomic, chemical and electrical component. The
apperception of "interiors" realized in the subjective experience of
phenomena is what makes us human.
During and forever after a kundalini awakening there is constant bliss
to varying degrees. Some of the chemicals involved in bliss include the
endorphins, endogenous cannaboids, sex hormones, nitric oxide,
dopamine, oxytocin, ionized cerebrospinal fluid, dopamine,
phenylethylamine and possibly the ATP molecule itself. The
concentrations of these various bliss agents change with the different
kundalini events, the stages and the seasonal and lunar variations in
the flux of kundalini.
Normally we just hum along in our conditioned everyday
consciousness, and then life seems to perturb this throwing us into
heaven or hell depending on the circumstances. Hell...the death of a
loved one, a breakup, losses of various kinds can be a direct route to
Heaven. Any arousal of the Hypothalamic-Pituitary-Adrenal Axis will
cause increased activation of the opiate systems, whether the arousal
be stress, shock, trauma, freeze, sports activity or sexual attraction.
Kundalini represents perhaps the greatest ongoing efflux of opiates.
Sometimes the bliss is so acute that it makes rational thought all but
impossible. The point is not to fight the bliss, or fall into
compulsive degradation using the bliss as though it were a drug or
alcohol binge. While undergoing excessive bliss there is indeed a need
to rehabilitate ones faculties by pursuing challenging cognitive tasks.
If this is not done chances are one could remain a spiritual bum for
the rest of ones life, riding on the high of ones own internal
chemistry.
Bliss might be directly associated with healing energy for it does
dissolve the pain-body and impact of past trauma on the body and it
does dissociate one from ones past pain, however it doesn't
automatically create happiness. One can be blissed out and simultaneous
be in ennui and depression due to cortisol burnout and
hyper-parasympathetic activity. Kundalini can leave one both less
functional and with a reduction in spiritual faculty while at the same
time being blissed out of our tree. So the whole thing is very complex
and to navigate such waters we need to stay focused on the creation and
integration of the Whole Human.
Although there may be a deepening or change of flavor of the bliss
and a rounding out of other functions to rise above the dysfunction of
being blissed out, I don't think one could classify bliss in stages and
lines of consciousness, other than to say that bliss affects all
states, lines and stages. The good news is that when we are well into
our substantiation phase we can have our bliss and our high cognitive
function too.
Bliss appears to be kundalini phenomena especially related to heart
expansion and is a consequence of increased energy flow in the nerves.
One of the functions of spiritual bliss is to incapacitate the higher
cortical functions rendering the individual "childlike" soft, maluable,
changable, open and to conserve energy and internal resources for the
metamorphosis of the physical body that occurs. Normally our
conditioned "I" is kept so busy, hypervigilant and preoccupied by the
tasks of daily life and obligations that this "fall" into the
spiritually receptive state doesn't occur. Hence the preponderance of
unpopped humans populating the planet, all vigilantly remembering who
they are.
Memory takes tremendous energy. The energy used in an effort to
maintain the sense of who we are right now prevents us from discovering
what we might become. Thus the normal tight hold (neurosis) we have
over who we are, our place in the world, and our past...keeps kundalini
at bay. Once lit however kundalini dissolves our neurosis, our
pain-body, accumulated stress and trauma, and does so by essentially
flooding the limbic brain with bliss making us somatically forgetting
our past. All parts of the body can experience the flow of bliss, I
have had bliss move through the digestive system, spleen, liver,
pelvis, lungs etc... I have experienced bliss throughout the entire
body, but I don't ever remember my adrenal-kidney area being in bliss
The loss of memory and mental faculty experienced from bliss,
expanded states and kundalini occurs because the body's forgetting
chemicals: anandamide, enkephalins, endorphins are produced in large
amounts in the hippocampus and amygdala, and hypothalamus (limbic
system). The increase in charge through these areas heightens the
body's cannaboid and optiate systems. This acts in a healing fashion,
to help our Pavlov's dog brain to forget past trauma, but it can
incapacitate one to varying degrees. Thing to do is to not get anxious
on top of the loss of faculty because that will only increase the
stress, thereby increasing the "numbing/forgetting" chemistry.
To balance out the bliss, overcome the diffusion and lack of focus
and recover our edge we need to drink lots of water, reduce food
intake, breath into the belly, jump into cold water to regain lucidity,
take long walks in nature, get around falling water, take doses of
spirulina and yerba mate etc... The Nootropic Formula listed in the
supplement section might help with overcoming the bliss by stimulating
higher cortical function. But I think that a serious attempt at
addressing bliss overload requires more environmental stimulation, like
radical sports, radical nature or radical social events to produce
endogenous wakeup chemicals. I think there might be something in
pinching the end of the nose, for during evolution the limbic system
grew out of the olfactory system, giving the end of the nose a sharp
pinch seems to wake the brain up a little.
There is a tendency while in ecstasy to think: "I better not
meditate or I will increase the bliss and become a total basketcase."
This is a very common situation with active kundalini. Whereas forms of
meditation or focusing the energy in different parts of the brain and
heart really helps us to cope with excessive bliss. You see the bliss
can put one into a narcotic sleep--a mythic uroboric dreamland in which
we are no longer functional to ourselves or others. One can also
automatically resist the bliss and then it becomes just another thing
to run from with our addictions or small-nature. However by drawing the
energy up, maintaining a seat in the Mind's Eye and deep
breathing one can essentially ride the dragon, (like riding the spice
worms in Dune). Meditation while already blissed out with active
kundalini is the most effective period for growth. There is a chance of
regression, brain damage and resorting to addictions and distractions
if we do not "actively cultivate" the Force. (See Mind's Eye in Down Is
Up).
WITHDRAWAL SYMPTOMS
Neuroadaptation is the principle element of physical
addiction and drug tolerance. When the brain is frequently exposed to a
drug it adapts to compensate for the presence of the drug; so that if
the drug is stopped, it leaves the brain 'overcompensating' and in
disequilibrium in an unaccustomed way. Whatever pain or anxiety
condition the drug was masking returns with a vengeance in a "rebound"
experience. During kundalini ecstatic peak events and stages our brain
would become neuroadapted to excessive levels of "up" chemicals, so
that when that cycle is over and chemistry flips the other way we can
go through an extreme withdrawal. Hence both the Dark Night experience
and the exhaustion phase are often accompanied by withdrawal symptoms
such as anxiety, depression, memory problems, lack of motivation, and
feelings of emptiness. Because of both neuroadaptation and neuron
damage kundalini awakenings can be just as much a downer trip as a
high, especially to the uninformed.
Nathan Luno has an amazing website on the use of the drug Ecstasy;
especially check out his neurotoxicity section. Kundalini researches
might be interested in this as an info source. Specifically in the area
of how like Ecstasy, kundalini might create excess dopamine release
that could damage serotonin receptors in the brain. Kundalini is likely
to increase the release of transmitters from synapses because of the
increased charge in nerves, increased Ca2+, NO and ATP, heightened
adrenaline and norepinehrine. The enzyme monoamine oxidase (MAO) breaks
down the neurotransmitters norepinephrine, serotonin and dopamine in
the brain. MAO's occur in high concentrations in the blood, liver,
stomach, brain and intestines. During Kundalini or Ecstasy use however
the brain may be so loaded with neurotransmitters that the available
MAO may be insufficient to deal effectively with them. So during the
extreme ecstasy (up) and dark night (down) events there is likely to be
dopamine damage to the serotonin receptors, similar to that which
occurs on the drug Ecstasy. "The dopamine, once in the serotonin
cell, gets broken down by the monoamine oxidase into hydrogen peroxide
which oxidizes a healthy cell into a deformed and no longer fully
functioning one." ~ thedea.org/neurotoxicity.html
KUNDALINI AND THE MUNCHIES
Kundalini can stimulate compulsivity, until we reach the
point where we can dive into the bliss and Emptiness without
resistance. It's like the blissed brain is seeking to drown itself in
more and more bliss. There is less self-control somehow, probably
through limbic override of the prefrontal cortex.
Since raised kundalini means an activation of the sympathetic nervous
system the demand for energy generation goes up, just as it does with
the fight flight response. Besides the use of glucose and fat for
energy, Dr. Batmanghelidj says that that body uses water for the
generation of hydroelectric energy, especially in the neurotransmission
mechanisms. Thus the demand for water increases during kundalini. If
however we do not drink extra water, we may read the cues for thirst as
the desire for the energy to be obtained from sugar and carbohydrates.
If we take in simple sugars instead of water, we will get a temporary
energy boost, followed by a depletion of energy reserves. Plus since
the immune system is compromised by hypertonal sympathetic activation,
this means the sugar is likely to feed yeast and pathogen growth. The
solution is to read Dr. Batmanghelidj's Your Body's Many Cries for
Water...and drink 5 pints (10 cups) of water a day, and perhaps even
more during peak events.
There are natural cannaboids in the brain (eg:anandamide), as part
of the bliss, pleasure-reward, and anaethetizing/numbing function. I
suspect the extra kundalini firing through the brainstem, limbic
system, amygdala etc... turns on the bliss making chemistry pretty
permanently. This has many consequences: modulating the raw,
unrepressed emotionality that occurs on kundalini, giving a background
of bliss to all kundalini events and phenomena. But it can also reduce
motivation, make one loose one's sense of self, and could promote a
false sense of security while one's life tumbles down around one.
Considering the loss of normal adaptive left-brain functions that can
occur with kundalini, the bliss gives a background of equanimity and
grace, and helps to reduce the terror, worry and anxiety that would
normally arise in association with incapacitation of our faculties. The
world could be going to hell in a hand-basket, but it all looks
wonderful to us.
The level of cannabinoids in the hypothalamus is controlled by a
fat-regulating hormone, called leptin. This hormone keeps tabs on the
energy status of the body and helps regulate body weight. Leptin is the
primary signal through which the hypothalamus senses nutritional state
and modulates food intake and energy balance. Leptin reduces food
intake by upregulating appetite-reducing neuropeptides, and
downregulating appetite-stimulating factors. When leptin levels are
low, cannabinoid levels rise to stimulate appetite. Marijuana
overwhelms the normal system and swamps the receptors, making pot
smokers want to eat everything in sight.
There are three groups of opiate neuropeptides--Endorphins, Enkephalins and Dynorphins. It
is the levels of these neurotransmitters in your brain that governs
your mood and degree of compulsive behavior. Anything that disrupts
their natural balance will interfere with character, will, morality and
resolve. Insufficient enzymes available for the manufacture of these
neurotransmitters will reduce their number in the brain. An increase in
blood acidity decreases the permeability of the Blood Brain Barrier,
this reduces the supply of the amino acids that are the precursors to
these neurotransmitters. Remember body acidity rises with too much
animal protein, fats and processed foods, too much coffee and soda, too
little vegetables and alkaline mineral reserves, too little exercise
and oxygen. Fear, anger and other negative emotions also increase body
acidity. Positive ions (H+) in the air such as during a thunderstorm,
in urban environments and in hot winds like the Santa ana or Chinook
also increase body acidity, this explains the increase of violent
behavior under these conditions.
Genetically obese people and binge eaters release abnormally large
amounts of these opioid neurotransmitters in response to food. These
opioids mediate the cravings for foods high in fats and sugars. The
opioid receptors in the brains of these people are probably working
overtime resulting in an artificially high need for these opioids. Like
heroine these opioids are addictive. Substances which block the opioid
receptors or prevent the breakdown of the opioids can help reduce the
craving for foods high in fat and sugar. Very high doses of vitamin C
such as 6Ð8 gms per day may reduce the addictive withdrawal symptoms of
dieting or caffeine because it slows down the breakdown of the opioids
in the brain. The amino acids DÐphenylalanine and DÐleucine both retard
the breakdown of opioids in the brain so can be used to reduce food
cravings and drug addiction.
I wish to add a caution against using cannabis while in active
kundalini. Using dope on top of the huge increase in opiates would
probably add to the general anaethetization. Leading to an inability to
form a self-center of focused-ego and personal-drive. Personally I
think there is so much unusual stuff going on in the transmuting body I
would want to get a clear witness to the natural phenomena and
unfoldment of symptoms. I however still drink coffee, which is
grounding and helps the energy to return to the egoic-prefrontal lobe
function in order to "fend" for oneself in the world. But even coffee
on a nervous system that is in sublime reconstruction is not a good
idea.
Until we stop resisting the Kundalini we may try to stimulate
ourselves with sugar, caffeine and/or drown ourselves in fat and
protein. Because we are more limbicly and sensorally activated we could
have problems with run away urges. The increased compulsivity is the
result of both the egoic self-seeking comfort for the loss of
"self-ground" and running from the larger sense of being; but it is
also caused by the changes that go on in the brain. We need to study
this intently and work out what needs to be done in order to support
our growth without becoming radically compulsive. Deliverance of our
appetites to a higher power and purpose like the 12 step program might
work. When we stop resisting we learn to thrive on the pure energy of
our Self, and to clarify, purify, and deepen our experience of Being.
ERASING FEAR
Endocannabinoids made by the body, extinguish the memory of adverse
stimulation. Studies found that a process involving activation of
endocannabinoid receptors is essential in the extinction of conditioned
fear. The release of such opiates during the excessive firing of
kundalini is one of the main ways that the brain is eventually rewired
to a less hypertonal and less defensive (reptilian) nature. The
synaptic plasticity to change fear related memories requires activation
of NMDA receptors.
The 'endocannabinoid' system is involved in the extinguishing fear-related memories.
The amygdala, is crucial in acquiring and, possibly, storing the memory
of conditioned fear. The extinction of the memory of fear requires
neurons in the basolateral amygdala, and changes in the strength of
their connection with other neurons ('synaptic plasticity') that depend
on the NMDA glutamate receptors. There seems little doubt that
activation of these glutamate receptors in the basolateral amygdala is
somehow required for extinction.
The receptors for the endocannabinoids anandamide and 2-arachidonylglycerol,
are some of the most abundant neuromodulatory receptors in the central
nervous system and are expressed at high levels in the limbic system,
cerebellum and basal ganglia. The classical behavioral effects of
exogenous cannabinoids such as sedation and memory changes have been
correlated with the presence of these receptors in the limbic system
and striatum. Endocannabinoid release serves to increase synaptic
plasticity and inhibition of neuron firing.
The depolarization of neurons by repetitive activity led to the
release of endocannabinoids, which diffused to the terminals of other
neurons and inhibited neurotransmitter release. This effect was
found to be transient in the hippocampus and cerebellum and long
lasting in the striatum. The endocannabinoids reduce GABA release in interneurons
of the basolateral amygdala, thereby helping to extinguish the
fear-conditioned response. Not sure why inhibiting GABA release will
reduce fear memory, although GABA which is normally inhibitory,
sometimes works in cahoots with glutamate as an excitatory
neurotransmitter. GABA release is active in the immobilization of the
freeze mechanism, and the calming down after flight-fight, so GABA
might serve to lock nerves into a certain fear conditioning and reduce
synaptic plasticity.
ANANDAMIDE THE SELF TRANSCENDENCE CHEMICAL
Anandamide is a recently discovered messenger molecule that plays a
role in pain, depression, appetite, memory, and fertility. Its name
comes from ananda, the Sanskrit word for "bliss." Anandamide is
synthesized enzymatically in areas of the brain that are important in
memory and higher thought processes, and in areas that control
movement. This implies that anandamide's function is not just to
produce bliss.
The ability of brain tissue to enzymatically synthesize anandamide
and the presence of specific receptors for it, suggest the presence of
anandamide-containing neurons. Anandamide is an eicosanoid, that is it
belongs to a group of substances that are derived from arachidonic
acid, including leukotrienes, prostaglandins, and thromboxanes.
Anandamide is basically a compound that reduces activity, such as
reducing the formation of many stimulatory neurotransmitters. The human
brain muscarinic acetylcholine receptor (mAChR), which is involved in
memory function is inhibited by arachidonic acid and is also inhibited
by anandamides.
Anandamide's long hydrocarbon tail makes it fat-soluble and allows
it to easily slip across the hydrocarbon-rich blood-brain barrier. Its
shape strongly resembles that of THC (tetrahydrocannibol, the active
ingredient in marijuana), but unlike THC, anandamide is fragile. It
breaks down very quickly in the body, which is why anandamide doesn't
produce a perpetual natural 'high'. Scientists reasoned that since THC
is not naturally present in the body, there must be a natural key
molecule with a very similar shape that activates this receptor. The
key was isolated by Israeli scientist Raphael Mechoulam in 1992 as
being arachidonyl ethanolamide, later called 'anandamide':
Learning and memory is established by connections between nerve
cells by either making new connections or breaking old ones. Repeated
use of a connection makes it grow stronger while lack of use can cause
the connection to be lost. Some biochemical evidence suggests that
anandamide plays a role in the making and breaking of shortterm neural
connections. Anandamide might be one of the bliss making chemicals that
helps to produce a self-forgetfulness by which we can separate more
fully from our past. Animal studies suggest that anandamide induces
forgetfulness and calm. Animals treated with anandamide walk less and
lay down more; they have reduced body temperature and slower
respiration.
Three anandamide-like compounds were found in dark chocolate by
Daniele Piomelli and co-workers at the Neurosciences Institute in San
Diego [Piomelli, 1996]. www.nsi.edu
Eating chocolate is not advisable due to the negative effects of sugar
on protein structures, the feeding of candida, and fermenting GI Tract
contents. However raw cacao beans might be just the thing for
overcoming down-cycle blues. They can be purchased at www.rawfood.com
as Cacao Nibs (peeled raw/organic cacao beans). Apparently raw cacao
beans provide MAO inhibiters which increases the serotonin and other
neurotransmitters circulating in the brain. Cacao beans are said to
help reduce appetite, however we all know that marijuana increases
appetite, so I don't know the role these endogenous cannabinoids have
on appetite.
Anandamide is not the only THC-like molecule used for signalling in
the brain. Piomelli's group has found a new molecular key that closely
resembles anandamide [Piomelli, 1997]. Naturally produced sn-2
arachidonylglycerol (2-AG) can also lock into the bliss receptor. 2-AG
is present at 170 times the concentration of anandamide in some regions
of the brain. Piomelli thinks that 2-AG and anandamide perform
complementary functions.
The endogenous cannabinoids anandamide and 2-arachidonylglycerol may
be produced under distinct physiological conditions or in distinct
brain regions. Anandamide activity was found to be highest in the hippocampus, followed by the thalamus, cortex, and striatum, and lowest in the cerebellum, pons, and medulla.
Outside the brain, anandamide acts as a chemical messenger between
the embryo and uterus during implantation of the embryo in the uterine
wall. Thus it's one of the first communications that occurs between
mother and child. In animal studies the highest concentrations of
anandamide were found not in the brain, but in the uterus just before
embryo implantation. Anandamides play a survival role for young mammals
in their instinctive suckling behavior and lack of anandamide levels
can cause spontaneous abortions in mammals.
There areimportant functional relationships between endogenous
cannabinoid and opioid systems. Levels of the endogenous opiate
anandamide in the hypothalamus regulate compulsivity and appetite
initiation. Research found endocannabinoids are involved in retrograde synaptic inhibition
in the hippocampus, in long-term potentiation and memory, in the
development of opiate dependence, and in the control of appetite and
food intake. They also suggested the existence of as yet unidentified
cannabinoid receptors in the cardiovascular and central nervous systems
and in macrophage-mediated helper T cell activation.
A decrease in GABA inhibition both facilitates the induction of long-term potentiation (LTP),
and promotes the hyperexcitability of epileptic seizure. Scientists
investigated how the nervous system maintains its discriminating
control on GABA's inhibitory effect, in order to promote memory by LTP
and prevent seizure. They found that pyramidal cells, the ones towards
which inhibition is directed, may regulate their own state of
inhibition by sending a signal backwards across the synaptic junctions
(retrograde synaptic inhibition) and thereby causing the inhibitory
interneurons to stop releasing GABA temporarily. This signal from the
pyramidal cell to the interneuron is the endocannabinoid molecule
anandamide.
The cerebellum is a brain structure vital to many functions
including learning and memory. These functions are controlled by ion
channels in the Purkinje cells of the cerebellar cortex. This is a
specific type of nerve cell with more branches than any other kind of
nerve cell, which carries information output by the cerebellum and
possess a great deal of control over the refinement of motor
activities. It was found that Purkinje cells release endogenous
cannabinoids in response to elevated calcium, thereby inhibiting
presynaptic calcium entry and suppressing transmitter release.
These endogenous cannabinoids mediate retrograde signals from
postsynaptic neurons to presynaptic terminals in the CNS.
Endocannabinoids can be released from postsynaptic neurons following
depolarization-induced elevation of intracellular Ca2+ concentration.
The released endocannabinoids act retrogradely onto presynaptic
cannabinoid CB1 receptors and suppress inhibitory or excitatory
neurotransmitter release. This type of modulation has been termed
depolarization-induced suppression of inhibition (DSI) or
depolarization-induced suppression of excitation (DSE).
The endocannabinoid-mediated retrograde modulation is an important
and widespread mechanism for the regulation of synaptic transmission in
the CNS. Endocannabinoid release and resultant retrograde suppression
of transmitter release are also triggered by activation of certain
glutamate receptors (mGluRs) or acetylcholine receptors (mAChRs) in the
postsynaptic neurons. This pathway can work independently or
cooperatively of the depolarization-induced mechanism. It is shown that
DSI is enhanced significantly when these glutamate and acetycholine
receptors are activated simultaneously, and that this enhancement is
much greater than expected and cannot be attributed to mere increases
in Ca2+.
MORPHINE
Nerve cells communicate by releasing special 'key' molecules that
are intercepted by other nerve cells downstream. When the key molecule
at right locks into the receptor on the surface of a nerve cell, it
opens a door in the membrane that allows chloride ions to flood into
the cell. This equalizes charges inside and outside the cell and
prevents the cell from firing. The keys must be removed again from the
lock somehow, or the nerve cell will be permanently prevented from
firing. Certain enzymes are produced that remove (by degrading and
destroying) the keys after a certain amount of time, so that the nerve
cell can go back to work.
Drugs that have a powerful effect on the central nervous system
often mimic natural molecular keys. For example, morphine is a potent
pain killer that was found to lock into an 'opiate receptor' present on
nerve cells and blocks enkephalins out. The body's key removing enzymes
can't pry it from the receptors. The endogenus equivalent to morphine
are enkephalins. Although morphine is just a forgery of
enkephalins, it's much more powerful (and more addictive) than the
enkephalins because the key-removing enzymes can't pry it from the
receptors.
Christina Grof had an experience of morphine stopping kundalini during childbirth.
"During the birth of my first child, for which I had
prepared with the Lamaze method of breathing (very much like yogic
pranayama), this enormous spiritual force was released in me. Of
course, I didn't understand it and was given morphine to stop it as
soon as the baby was born.... Then the same thing happened when my
second child was born. This all led to more and more experiences. I
threw myself into yoga, although still not acknowledging it as a
spiritual tool. My meeting with Swami Muktananda really blew the lid
off everything. He served as a catalyst to awaken what I had been
resisting, which was kundalini (the universal life force). I felt
something snap inside me. A powerful force was unleashed in my body,
and I began to shake uncontrollably. Electrical tremors ran from my
toes and legs through my spine to the top of my head, where brilliant
mosaics of white light exploded. A new, involuntary breathing rhythm
overrode my practiced Lamaze pattern. I was excited and terrified. As
soon as my son Nathaniel was born, I was given two shots of morphine,
which returned me to normal. I felt fearful, and very embarrassed that
I had cost control of myself. A more powerful version of the same thing
happened two years later, when I delivered my daughter Sarah." ~ Christina Grof
PHENYLETHYLAMINE
Increase in vasopressin during the heart expansions and
inner-conjunctions might be one of the factors involved in cortical
shutdown during extreme kundalini events. Vasopressin (VP) is a peptide
neurotransmitter in the limbic system synthesized in the medial
amygdaloid nucleus in the presence of sex steroids, transported to
other limbic structures such as the hippocampus and septum and secreted
there by a calcium-dependent process. Its excitatory action on the
inhibitory interneurons produces near-total shutdown of electrical
activity of the efferent fibers of pyramidal cells, the projection
neurons of the hippocampus.
During the Inner-Conjunction/silver cord when massive orgasmic
energy streams through the body (what I call the peak of the influx
stage), the dominant hormone might be the amphetamine-like love
chemical Phenylethylamine (PEA). This neurotransmitter occurs
during the infatuation state of romantic love to promote elevated mood,
promotes alertness, confidence, openness to risk, essentially leading
to a state of excitement. The levels of this stimulant also spike at
orgasm and ovulation.
The drug Ecstasy (MDMA) is a phenylethylamine, and there are
similarities in the symptoms of kundalini and use of Ecstasy: expanded
heart, feeling of love, oneness with others, amplified senses and
increased energy. Phenylethylamine along with dopamine no doubt propel
us into the "super-sensoral realm" associated with the peak of
awakening. When all senses are greatly heightened, one has
transcendental vision, celestial music plays in one's head and the muse
is practically sitting on one's shoulder. The incredible love and heart
expansions that occur during the influx and transmutation are similar
to the heart opening that happens on Ecstasy. Nitric oxide, oxytocin
and vasopressin are probably key in the dilation of the vascular system
that occurs during heart expansions.
Levels of PEA are increased by monoamine oxidase inhibitors.
Moderate exercise raises PEA levels for most people. Interestingly PEA
might be the agent of bliss associated with Eureka experiences,
profound insight, thrill seeking and risk. As such geniuses and
daredevils no doubt produce more than the average person.
Our bodies can convert the amino acid phenylalanine to tyrosine and
PEA. Tyrosine is a precursor to norepinephrine and dopamine.
D-phenylalanine, which does not normally occur in the body or in food,
is metabolized to PEA. Although L-phenylalanine can be converted to PEA
it is preferentially converted to L-tyrosine. Since D-phenylalanine is
not widely available the mixture DL-phenylalanine is most often used as
an anti-depressant. Because other amino acids compete with
phenylalanine for entry into the brain it needs to be taken on an empty
stomach. This shortens the time it takes for the brain to convert it to
norepinephrine. (See Neurotransmitter Food Formula.)
©2006
Biology of Kundalini by Jana Dixon