The Study of Lucid Consciousness

Another Great Blog

Recently I have been going around reading up on some of my old time pasts blogs, one of them being “Ask Dr. Shulgin Online” a blog about compounds. It is hosted by Dr. Alexander Shulgin author of one of the most popular compound related books Pihkal and designer of over 200 novel compounds with visionary properties. People on the blog are allowed to ask questions to Dr. Shulgin about different compounds or ideas in making new research.

To me, psychedelics are a great tool to be uses in understanding the mind, just as a hammer is a great tool for putting in a nail into the wall… without the hammer, its a lot harder to get your picture hanging on the wall. Dr. Shulgin has given many different tools to help accomplish this goal and for that he should be recognized. I think his blog and many blogs like his give credit where credit is due, to the creative.

Visit his blog here: “Ask Dr. Shulgin Online“

Podcast 175 – “The Intelligent Use of Psychedelic Drugs”

Another interesting post from one of my favorite podcast by Lorenzo Hagerty who this time had a guest speaker Dr. Timothy Leary. I am not the largest supporter in Dr. Leary’s views on psychedelic uses as myself and a lot of others tend to blame Dr. Leary for a lot of the regulation on the uses of psychedelics today. Psychedelics as stated by me many times before can be a great tool to understanding the mind and along with that psychology and dream disorders. Unfortunately a lot of the events that took place during the 60′s allowed fuel to the already burning fire to cause higher regulation on the drug use in America. Its important to understand our history in order to not make the same mistakes with this tool, and Leary though a great mind and knowledgeable users of the psychedelics may have gone around the wrong way of spreading the word. In the words of Dr. Leary, “The problem with drugs is that stupid people use drugs stupidly.”

Hear the podcast here: Podcast 175 – “The Intelligent Use of Psychedelic Drugs”

-L

Posters Question

I wanted to post this comment that I read today about sleep paralysis. I found it very interesting and I tried to answer the question asked:

Question:
nice post – I never thought about SP in regards to the terrible biochemical combination of intense fear and muscle paralysis. it’s a rough place for consciousness! I’m reading Hufford’s classic right now and the accounts are fascinating. do you have any ideas about the phenomenon of the “stranger” (that sometimes accompanied the experience of SP) in terms of brain activity?

Ryan,
Sleep paralysis has been a long time been something that I have researched since I used to have it affect my life. The stranger you asked about I believe (if were thinking of the same thing) has been referenced by some people in the lucid dreaming community as the dweller. It seems to be the occurrence of a type of thing that exists in the dream that sometimes tries to scare the dreamer. At time this “dweller” has even been known to have long conversations with people of why it tries to scare people once the dreamer shows their inability to be scared by the object. I remember one account where someone ones reported that after having the conversation with the dweller, another dweller entered the room and explained to the other that it was time to go. Interesting enough I see the same references during psychedelic uses in the way they describe some of the “guides” that are experienced during some drug trips.

In trying to understand the brain chemistry that is causing this dweller effect, the easiest explanation that was explained in many of the books I have read about the processes of sleep, is that during the transitional phases between NREM and REM sleep the subconscious dominate. If by some chance there is a hiccup in this process (which is normally the case) the subconscious could become aware of the conscious mind and it causes an interaction. The amygdala being over active at this time and I believe a good explanation of why fear is the most referenced the interaction between the two. Psychedelic drugs could also cause a type of lucid state during the trip experience and cause the same type of interaction between the subconscious and conscious just on a larger scale. The relationship presented by Dr. Strassman and his work on DMT shows that the dream state and alteration of consciousness during sleep could very well be more psychedelic then we currently believe, and would explain more why the dweller effect happened in both cases.

I would be glad to hear more about what you have been reading, feel free to post your comments and ill try to get post more.

Sleep Paralysis

I wanted to post some helpful questions and answers that I continually see on the internet to specific problems with sleep. I have posted many answers to questions on yahoo questions and answers but I wanted to write up some generic answers for specific disorders.

Sleep Paralysis

History of sleep paralysis

If you look back into the history of sleep paralysis you will find that many of the old stories of demon possession. This same event of sleep paralysis is also the reason we have the word nightmare as it comes the Goddess name of Mara. Mara was a type of demon that would sit on the chest of others holding them down while tormenting humans in their sleep making it so that the sleeper or dreamer could not move (paralyzed).

Paralysis and terrifying events:

Sleep paralysis often brings along with it terrifying hallucinations as based on the history is understandable. One reason that people experience anxiety based hallucinations during this period of sleep is because during the transformation phase between NREM and REM (where sleep paralysis accurse) our brains are going through a type of modulation or the shutting down and starting up of specific areas. One of these key points in our brain that is activated is the amygdala which in some research has shown to be the start to the process of dreaming itself. The amygdala is this one specific area of our brain that causes us to feel fear and anxiety and if it becomes activated to the point it does in sleep, well then you very well can have a very scary dream. The paralysis either shortly follows this process or is activated slightly before so that the body doesn’t act out its dreams. Some research has shown that this is normal process; however remembering or being fully conscious during the transition is out of the norm as our brain also shuts down a specific area of our brain that is involved with processing long term memory possibly because of the absence of serotonin during sleep.

Supporting the normal brain:

Though many doctors would never recommend vitamins or supplements to support your body in ridding any type of issue, many different supplements have shown to produce remarkable results even publishable results in the area of sleep. In the area of sleep issues, helping the brain transition between non-REM and REM. 5-HTP, niacin, and choline salts, are all supplements that are precursors into producing specific neurotransmitters involved in sleep however it is recommended that you consult a doctor before taking any supplements. If you are unwilling to take supplements to help you sleep, it is a good idea to visit a doctor in order to get medication that will help produce better sleep.

Travel and Some

Well summer has officially started for me and I have been doing a lot of running around trying to figure out how to relax some. I have started to go through some of my old books and read some of the notes produced by those authors to find some good information for references to read up and post about. Until I get a good grasp on that information I wanted to start to post some other information that I think is supporting to sleep and our conscious mind.

Psychedelic use has been around as long as humans have been, maybe even before as some animals have been shown to take part in eating plant matter and “tripping” out after doing so. As I wrote many times before, I think it’s important to understand the use of psychedelics and the possible help it may produce into the changes of our consciousness, let that be sleep or other. If you haven’t read my recent post with the information I found for my paper then you may not see why psychedelics are important in sleep, but if you took the time to read it you would find that supporting evidence has allowed us to understand that some type of endogenous psychedelic may be the whole cause for our dreaming. At any rate, there have been countless reports of psychedelic like dreams and vice versa. I still do believe that there is still a good amount of useless information found in the psychedelic experiences but enough quality information in understanding the mind, that it shouldn’t be overlooked.

One of my favorite podcasters Lorenzo Hagerty, has posted a number of great pod casts. Here is one of his recent podcasts.

Podcast 184 – “The Boundaries of the Human Mind”
http://www.matrixmasters.net/blogs/

Here are the notes from the podcast:

“What Damasio is showing is that people who, in the lab, get a huge amount of cognitive stimulus all the time start to have no access to the emotional part [of themselves] at all. They can’t store to it, and they can’t retrieve from it. They become what he calls emotionally neutral.”
“So if ANY crisis arises you have the wrong people [in charge], probably, because the things that put them there, and the constituencies that wanted them there, create a person who is incapable of handling a real crisis.”
“If you want a future, you have to take charge of your own thoughts.”

-L

Sleep Mentations and Other Cognitive Realities

Humans have long been interested in the alteration of their consciousness. They have done so through a variety of means, including external chemicals, physical stressors and mental disciplines. Humans have also taken great care to pay attention to their dreams’ actions in which regularly provides an altered state in which the experience inadvertently interacts with their so called subconscious. No matter what path individuals take to reach these altered states, the states themselves bear striking similarities to one another. By understanding the baseline connections between the disassociation (change in normal consciousness) of individuals in both dreams and in the use of drugs, one may be able to understand the waking consciousness better or conscious altered type disorders. In the past, few researchers have suggested the connection between psychedelics and sleep menations but due to lack in technological they were unable to test humans for such indigenous psychoactive drugs. Theses purposed hypothesis are becoming more and more popular as new technology and further research into the reasons for sleep and its chemical relationship to our minds become supported.

Sleep Modulation
The mind prepares the body for sleep about 12 hours prior to the actual initiation of sleep onset (Barrett & McNamara, 2007). This transition is controlled by what is called the circadian rhythm, a brainstem controlled mechanism for keeping time, heartbeat, heat control, and many other automatic functions (Barrett & McNamara, 2007). The one aspect of circadian rhythm that deals mainly with sleep is the temperature control (Barrett & McNamara, 2007). Temperature control during the 24 hours cycle of the circadian rhythm allows our core temperature to change from cold to hot or hot to cold depending on the phase in the 24 hour cycle (Barrett & McNamara, 2007). During sleep onset our circadian rhythm automatically lowers the body’s core temperature using the body as a radiator. This change in temperature is one of the first signs of brainstem activation which precedes further demodulation and modulation of specific brain areas during the 5 sleep stages. The decrease in body temperature is greatly supported by the production of melatonin synthesized in the pineal gland in the brain (Callaway, 1988) (Strassman, 2001) and shows that in relation to circadian rhythm, melatonin supports peak core body temperature drop at early morning hours when melatonin levels are highest (Strassman, 2001). Secretions of melatonin into the hypothalamus help in sustaining this process. Research has shown that micro injections of melatonin have the same effect as this process (Cramer, Rudolph, Consbruch, & Kendel, 1974). Supporting this transition from waking to NREM sleep, prostaglandin (PG) D2 is also secreted into the cerebrospinal fluid as an indigenous sleep aid, serving the mind in preparation for REM and recovery of fatigue (Huang, Mochizuki, Eguchi, Watanabe, Urade, & Hayaiski, 2001) (Moussard, Albert, Mozer, & Henry, 1994). Sleep modulation specifically is broken up into two categories Non-REM (NREM) and REM. NREM is broken up into 4 different stages: drowsiness, light sleep, deep sleep, and delta waves. REM represents the last of the sleep phases as stage 5 or Rapid Eye Movement (Yuschak, 2006). These phases are graphically depicted in figure 1.

Determining when these stages start and stop is an extremely difficult process since each phase transitions flawlessly into the next and sometimes seems similar to each other. One extremely complex stage of sleep, where the majority of our definition of dreaming or mentation comes from, is the REM stage. Although 80% of sleep is spent in the NREM phase (Barrett & McNamara, 2007), a particular amount of attention should be spent on the REM stage and transitional phases to REM since that is where the majority of dream like induced hallucinations occur.

Once activated by the circadian rhythm and supported by melatonin production, the brainstem starts to modulate the brain through physical activation or deactivation of specific areas. These same changes that happen during the sleep transition of NREM to REM are apparent in the onset of all forms of altered consciousness as they ultimately rely on the brainstem for any physical changes in the brain. This brainstem activation either modulates or demodulates different area of the brain depending on what type of activation signal is represented; either by external or indigenous chemical induction.

Possibly one of the most complex stages of our sleep is REM. REM is characterized by the rapid side to side movement of the eyes and the paralysis experienced by the sleeper from the chin down (Yuschak, 2006). Rapid eye movement and dreaming is not limited only to the REM stage but is also experienced during the last stages of NREM or the transitional phase between NREM and REM. The average person experiences 25% of their dreams during the transition from NREM to REM (Hobson, 2002). NREM dreams are described by patients that experience them as less vivid and shorter than those experienced during REM sleep. The differences in intensity of dreams between these stages are attributed to the amount of time spent in sleep, or the length of time the brain has had to produce dream related chemicals. The processes of activation and deactivation of specific parts of the brain during NREM and REM transitions are graphically depicted in figure 2.

Activation and Deactivation
The transition from NREM to REM is described by Allen Hobson and Robert McCarley in their proposed hypothesis of activation synthesis as a process of modulation and demodulation of specific areas of the brain in which mentations are produced (Barrett & McNamara, 2007) (Hobson, 2002). This activation synthesis hypothesis builds its foundation on the concepts produced by the REM Dream Theory. In REM Dream Theory, specific neurotransmitters acetylcholine (ACh) and histamine REM on, as well as serotonin REM off cause either modulation or demodulation of the brainstem (Hobson, 2002). The activation synthesis theory states that during the transitional phase between NREM and REM sleep, the brainstem has already systematically deactivated the aminergic systems ,which disengages the dorsolateral prefrontal cortex and blocks muscle motor function via the pontine brainstem’s deactivation of the anterior horn cells. The now deactivated aminergic system results in the loss of the ability to process new memories, cognitive functions of the ego, and the paralysis that inhibits the acting out of dreams (Hobson, 2002). This deactivation accounts for the common occurrence of amnesia that many people experience during sleep, the inability to understand self and to recognize the bizarreness of dreams, as well as the inability to move which has been experienced by some lucid dreamers, night terror patients, and narcoleptic patients (Hobson, 2002) (Lucidology, 2008) (Richard, 2006). Other areas such as the pons, the amygdala, the pariental operculum, the deep frontal white matter, and the parahippocampal cortex show evidence of having higher neuron function during NREM and REM transition as well as REM sleep phase than in waking (Barrett & McNamara, 2007). This modulation of specific areas of the brain is due to the increase in acetylcholine and results from the activation of the cholergenic REM on system (Hobson, 2002). The activation of the amygdala, due to the cholergenic system, can explain why the majority of dreams are experienced as fearful, full of emotion or nightmarish in nature due to the nature of the amygdalae in an over active state causing fearful emotions(Barrett & McNamara, 2007) (Hobson, 2002).

Using Dr. Hobson’s activation synthesis theory as a model, we can understand the reasons for the type of mentations or dreams that are experienced during NREM phase 2, and REM stage 5 of sleep. However we still have no understanding of what makes theses mentations occur. These occurrences may be explained by the remarkable correlation between the pineal gland and the synthesis of specific neurotransmitters that may contain psychoactive properties.

Mentations and the Pineal Gland
Neurotransmitters are the basis of how we perceive the world around us. They are the basic communication tool between neurons as well as activators and deactivators of multiple functions. Not one neurotransmitter completes only one function, on the contrary they sometimes complete functions that are in opposition of each other and brain function, competing for a completed task (Hobson, 2002). The more research is conducted on sleep and mentation the easier it is to understand how complex and integrated with neurotransmitter function sleep really is. In dealing with sleep and mentation we can break neurotransmitters into two basic groups – the aminergic system, comprised of the neurotransmitters dopamine, noradrenaline, and serotonin, as well as the cholinergic system, composed of the neurotransmitters acetylecholine, and histamine. The process of how the aminergic and cholinergic systems function in sleep can be described as a REM-on and REM-off type switch. Research has shown that the orexin or the hypocretines system is involved in controlling these two systems (Kaslin, Nystedt, Ostergard, Peitsaro, & Panula, 2004).

The pineal gland is a chemical production factory, either producing melatonin or serotonin depending on the presence of absence of light. In this process, light source information is relayed from the eyes via the optic nerves and results in the activation of synthesizers that either produces melatonin in the absence of light or serotonin in the presence of light, becoming the brains largest producer of serotonin. Also in the absence of light, other process are continued as melatonin is then processed into tryptamine and pinoline. Pinoline is a beta-carbolin called 6-Methoxytetrahydro-beta-carboline and acts as a monoamine oxidase-A inhibitor (MAOI) which in turn allows for the increases concentrations of serotonin (Callaway, 1988). The synthesis of tryptamines and pinoline is most dominate during the REM stage of sleep but also shows partial activation during NREM phases 2 as well as during highly stressful situations in animal and human lives (Strassman, 2001). In relation these stressful events, mentations also turn out to occur during this time. Some beta-carbolines and tryptamines have also been known to cause psychedelic hallucinations as they deal directly with brainstem modulation (Hobson, 2002) (Callaway, 1988). Melatonin has also been reported as having hallucinogenic effects on the brain; however, recent studies have shown negative evidence of such a relationship and that the further chemical breakdown of the beta-carbolines and tryptamines from melatonin are the results of these experiences (Cramer, et al., 1974) (Strassman, 2001). The buildup of these two known types of hallucinogens in the form of pinoline and tryptamines could easily explain the visual mentations experienced during specific pineal gland stimulation. “A shunt of serotonin metabolism to a pathway that occurs and leads to accumulations of abnormal amounts of such potentially pschotomimetic compounds” (Callaway, 1988) could explain many other hallucinogenic based abnormal brain dysfunctions such as schizophrenia. Blinding of the nerve fibers from cervical ganglion and the pineal causing inactivation of the melatonin process has been suggested as a way to reduced waking hallucinations in schizophrenic syndromes and shows support towards the pineal glands involvement in dream mentations (Maurizi, 1985). The processes of chemical conversion inside the pineal gland during different stages of sleep and light interaction are graphically depicted in figure 3.

Pineal Location in Relation to the Brain
The location of the pineal gland is also very important in supporting how an indigenous psychedelic excretion from this gland would cause the described effects of dreaming. The pineal gland is located directly over the colliculi and is surrounded by the limbic system (Strassman, 2001). If hallucinogenic chemicals excreted from the pineal gland, the result could be a barrage of emotional thoughts with respect to the involvement of the limbic system and a combination of audio and visual alterations in the colliculi experienced during dreaming. Due to the position of the pineal gland, blood flow is not necessary for the transfer of hallucinogens to the regions of the brain most affected. It can be assumed then, that mentations could occur at the point of death in the patient and possibly explaining out of body exerpences and other religious experiences.
The question still presents itself of what indigenous tryptamine based psychedelic would produce such mentations since beta-carboline pinoline may be psychedelic in nature but most likely not potent enough to cause full blown psychedelic experiences as experienced in dreams. It has been hypothesized that the indigenous psychedelic Di-methyle-trypamine (DMT) and LSD-25 could be the answer (Shulgin and Shulgin, 1991).

DMT, LSD-25, and Other Psychedelics
Understanding the different key precursors needed to make indigenous DMT and LSD-25 is an important part in understanding why the pineal gland has been selected as a possible production tool for tryptamine based psychedelics. The pineal gland, in addition to having its serotonin production properties also has the highest concentration of serotonin in the body (Strassman, 2001). Methyltransferases are necessary enzymes that have the ability to convert serotonin, melatonin, or tryptamine into psychedelics by methylating them (Strassman, 2001). Pinoline as well as other beta-carbolines may support this process by inhibiting the breakdown and extending the effects of tryptamine based psychedelics. With the abundance of serotonin, the transforming based methyltransferases, and the amplification ability of beta-carbolines, the pineal gland is one of the most logical places for indigenous DMT synthesis (Strassman, 2001). Also chemically similar to melatonin is LSD-25, which relates specifically to the activity on the raphe nucleus (a control center for serotonin release) (Maurizi, 1985) (Hobson, 2002). Few studies into the relationship of the formation of DMT or LSD-25 in the pineal gland have been conducted; however, indigenous DMT has been found in the lungs and brain of humans.
Though DMT, LSD-25, and other psychedelic drugs are similar in structure, the effects of these drugs are sometimes dramatically different. These differences are based on the individual as well as the environment of the individual taking the drug. A few instances have occurred where the same psychedelic trip has been described by different people taking the same drug. The amount of drug administered is also another key factor in how the effects of the drugs will be experienced. Dream mentations seem to follow the same trend as psychedelic as they are normally random and differ in intensity from dream to dream and person to person as well as setting. Vividness as well as intensity of the dream also increases with the amount of sleep the individual receives. This is due to the longer lengths of REM sleep as well as if they have a fully active pineal gland. With these common experiences, it is easy justify a relationship between dreams, psychedelic experiences, and the pineal gland.

Degrees of Disassociation
Contrary to the dream type experience, waking life, or normal consciousness, is kept in equilibrium during the day. Only with the administration of psychedelic drugs or sleep like alterations of the mind do we see a change in the consciousness or a degree of disassociation. The differences between sleep modulation and how psychedelic drug induce these changes is the speed of onset in which the mentations occur, the amount of allowed outside stimulation that can affect the patient, and the different areas of the brain affected by different types of drugs. These alterations in the consciousness seem to be in common with specific events that indicate different levels of disassociation or degrees away from the equilibrium of normal consciousness. The onset of psychedelic and dream like mentations all have in common the precursor effects of this consciousness change. Those effects are described by individuals as a feeling of heaviness, change in core body temperature, a relaxing feeling, audible buzzing sounds, and an increase in perceived bodily movement. These same events are described by patients that experience REM behavior disorder (RBD), sleep paralysis, perceived out of the body experiences, (OBE) and lucid dreaming (LD) (Yuschak, 2006) (LaBerg & Rheingold 1997) (Lucidology, 2008) (Richard, 2006).
During the transitional phase of NREM to REM, consciousness is also playing its part in changes in phase. In stage 2 of NREM sleep the thalamus becomes partially activated, allowing for conscious thinking, while in REM sleep the thalamus becomes fully activated mimicking our waking life allowing for full conscious thought (Barrett & McNamara, 2007). As we can see, the main difference in waking and REM sleep is the deactivation of the prefrontal cortex disengaging our brain from remembering the majority of our events. Individuals that practice lucid dreaming and experience out of the body type occurrences pay close attention to improving their memories of dreams as well as the transitional phase between NREM stage 2 and REM. It could be hypothesized that the techniques used to improve memory allow for the activation of the prefrontal cortex during REM sleep and allowing them to remembering these nightly events and allow for more psychedelic type of dream experiences.

Disguise Censorship
Much of the information that supports the theory of activation synthesis as well as the proposed hypotheses of psychoactive drug synthesis during REM sleep is contrary to Sigmund Freud’s theory of disguise censorship. Sigmund Freud used the disguised-censorship hypothesis in parallel with his practice of psychoanalysis in order to explain the aspect of sleep. In the disguised-censorship hypothesis, the brain is made up of a distinct subconscious and conscious. During sleep the left side of our brain being responsible mainly for logical thinking and ego, is less activated than our right side of our brain the side responsible for the id. Because of this the id is able to act out its wants and needs while still hidden from our ego by the amnesia felt after awakening and hidden interpretations of these signals produced into dreams. In addition to Freud’s dream hypothesis is that dreams are only produced moments before awakening (Barrett & McNamara, 2007). This difference is supported based on the concept that menations are experienced during NREM and REM and not as Freud theorized as only during the moments right before waking. Also Freud supported his theory with explaining that dreams have no randomness to them as they are childhood repressed wants and needs, and is kept in our subconscious to protect our conscious mind from damaging thoughts. As explained earlier there is evidence that dreams are sometimes random, remembered, and closely related chemically to psychedelic experiences.

Discussion
Using psychedelic experiences as a model for dream mentaions we can explore the effects of altered states of mind while subjects are fully conscious. Further research into this field could give scientist a better understanding of the subconscious minds true intent in altered states as well as possibly answering the question of why dreams occur. Research into understanding the true purpose of the pineal gland and its production of indigenous tryptamine based psychedelics may also help in understanding sleep disorders such as night terrors, sleep paralysis, and narcolepsy. This type of research should be conducted in a controlled environment to increase manipulation of the dependent variables and maximizing the authority of such research. Development of more sensitive testing assay for indigenous psychedelic drugs allowing for baseline values in normal patients should be developed before future research is conducted.

 
References
Barrett, D., & McNamara, P. (2007). The New Science of Dreaming. Greenwood Publishing Group.

Callaway, J (1988).Proposed Mechanism for the Visions of Dream Sleep. Medical Hypotheses. 26, 119-124.

Hobson, A. J. (2002). The Dream Drugstore: Chemically Altered States of Consciousness. MIT Press.

Cramer, H., Rudolph, J., Consbruch, U., & Kendel, K., (1974) On the Effects of Melatonin on Sleep and Behavior in Man. Advances in Biochemical Psychopharmacology, 11.

Huang, Z.-L., Qu, W.-M., Li, W.-D., Mochizuki, T., Eguchi, N., Watanabe, T., Urade, Y., & Hayaishi, O. (2001). Arousal effect of orexin A depends on activation of the histaminergic system. Proc. Natl. Acad. Sci USA, 98, 9965-9970.

Kaslin, J., Nystedt, J. M., Ostergard, M., Peitsaro, N., & Panula, P. (2004). The orexin/hypocretin system in zebrafish is connected to the aminergic and cholinergic systems.
The Journal of Neuroscience , 2678-2689.

LaBerg, Stephen, & Rheingold, Howard (1997). Exploring the World of Lucid Dreaming.Ballantine Books.

Lucidology, (2008). Lucid Dream Forum, OBE Forum. Retrieved March 30, 2009, from Saltcube Lucid Dream and OBE Forum Web site: http://www.saltcube.com

Maurizi, C (1985).The Anatomy and Chemistry of Hallucinations and a Rational Surgical Approach to the Treatment of Some Schizophrenic Syndromes. Medical Hypotheses. 17, 227-229.

Moussard, C., Alber, D., Mozer, J. L., & Henry, J. C., (1994). Effect of Chronic REM Sleep Deprivation on Pituitary, Hypothalamus and Hippocampus PGE2 and PGD2 Biosynthesis In the Mouse. Prostaglandins Leukotrienes and Essential Fatty Acids. 51, 369-372.

Richards, David (2006). Night Terros Resource Center Forum. Retrieved March 30, 2009, from Night Terrors Resource Center Web site: http://www.nightterrors.org

Strassman, Rick (2001). DMT: Spirit Molecule. Rochester: Park Street Press.

Shulgin, Alexander, & Shulgin, Ann (1991). Pihkal .Transform Press.

Yuschak, T. (2006). Advanced Lucid Dreaming – The Power of Supplements. Lulu.com

Question of the week: "Sleep paralysis night terrors about angels vs demons?"

Question:

I’ve had 2 “night terror” type incidents in the past 6 months, where I’ve been half awake and aware of my surroundings but totally paralyzed. This is, obviously, terrifying. But the weird thing is both incidents have involved good vs. bad, or angels vs. demons. The first was 2 loud voices talking in each ear talking about stealing something, one good, one bad, kind of like the angel/devil on shoulder metaphor you see in films. And the other was after a dream about angels and demons fighting, and then during my sleep paralysis I imagined a demon-like creature approaching me. In both incidents, the “bad” has seemed to win or have the last say. Is this significant in any way?

Answer:

Unfortunately I think that you have experienced something that is common in a lot of religious circles when dealing with sleep paralysis. If you look back into the history of sleep paralysis you will find that many of the old stories of demon possession ties into this. This same event is also the cause for the word “nightmare” comes from the name Mara as it was a type of demon that would sit on the chest of others holding them down while tormenting them.

One reason that people experience anxiety based hallucinations during this period of sleep is because during the transformation phase between NREM and REM (where sleep paralysis accurse) our brains are going through a type of modulation or the shutting down and starting up of specific areas. One of these key points in our brain that is activated is the amygdala which in some research has shown to be the start to the process of dreaming itself. The amygdala is this one specific area of our brain that causes us to feel fear and anxiety and if it becomes activated to the point it does in sleep, well then you very well can have a very scary dream. The paralysis either shortly follows this process or is activated slightly before so that the body doesn’t act out its dreams. Some research has shown that this is normal process; however remembering or being fully conscious during the transition is out of the norm.

Researchers still do not know why we dream or even how we dream, though they are continuing to research the area and understand more. It is important to not take our dreams too serious but also to not over look them, as they may have some underlying information of what we want, or how we perceive things. In a short answer your dreams may have meaning but no one can answer that question for you but yourself.

-L

Poster Support

R and I started this blog in order to help other people but after a good 6 months of posting R and I have become very busy with school/work and have little time to gather the information needed for new and informative posts. It is my goal with this blog to have information posted at least 3 times a week with questions, answers, and studies that could help others to gain a better understanding of sleep and better sleep. Our view on how to approach this information is by supported research into the areas that are related to sleep and to exclude any type of information that may be highly speculative. If you notice, we also try to leave out words such as “proven” and “truth” and “fact” as science does neither of those things.

I am interested in a few individuals to help out with the blog that have a passion for those things posted above. I will also be continuing to post as I am currently but I would like to get some more knowledgeable individuals to join the group. If you are interested feel free to e-mail me at cyristvirus@gmail.com with some information about yourself, such as education level, years of experience in the sleep community, and why you would like to help out.

Thanks and stay alter for further posts about sleep.

-L

Dr. Strassman Interview

Today I got the chance to ask a few questions to Dr. Strassman, author of “DMT: The Spirit Molecule” and co author of “Inner Paths to Outer Space.” Questions range from the upcoming movie titled DMT: The Spirit Molecule (yes just as the book) and about the future research being done on the topic of DMT. Here is what Dr. Strassman had to say:

What got you interested in researching psychedelics or the pursuit into how our brains possibly formulate indigenous psychedelics?

I was struck by how similar reports of mystical experiences were to those made by people experiencing big psychedelic trips. I thought that mystical experiences may be related to endogenous psychedelics.

In relation to sleep, Dr. Callaway seemed to pave the way for many of your ideas into the possibility for an indigenous psychedelic being produced at that time. Do you support the idea that indigenous DMT is the possible cause for our dreams during REM sleep?

Jace suggests that pinoline, a pineal MAOI, allows endogenous DMT to be more effective during REM sleep. We don’t know the dynamics of endogenous DMT, so that’s why the LSU group is developing a new generation assay to more accurately and sensitively measure DMT and related compounds in humans. Once we’ve got normal values in normal people during normal wakefullness, we can start looking at differences in states, conditions, and so on.

In your book “DMT: The Spirit Molecule” you proposed the hypothesis that DMT is synthesized in the pineal gland. I have noticed that many websites and forums misquote you about DMT being factually formulated there. I know that you never said it was, but has there been any further research into the area and what has become of that hypothesis since your last study?

I regret not being more clear about the hypothetical nature of the DMT-pineal link. There is one paper in which human pineal tissue is ground up and put into a test tube; then the precursors for 5-methoxy-DMT are added, stirred, and warmed, and out comes 5-methoxy-DMT. We have no data on intact, in-person pineal gland DMT synthesis. That’s one of the questions we hope to answer with our new assay at LSU. While the pineal link remains speculative, it is established that lung makes lots of DMT.

What was the most profound idea that you took from your research on DMT at the New Mexico clinic?

There is a spiritual level of reality, and it does not depend upon our observing it.

I remember reading in your book “DMT: The Spirit Molecule” that you took a break from research into the psychedelics. I have recently read that you may recently be conducting further research into psychedelics. If so what got you back into that work and what type of new research are you working on?

I set up a foundation, Cottonwood Research Foundation, to see if we could get a free-standing institute off the ground to perform research less constrained by University logistics. Right now it’s mostly functioning as a clearing-house and think tank. I’m collaborating with several other researchers in the development of research protocols and/or interpretation of their data. I’m working on another book project, which takes all my time, so Cottonwood isn’t getting the attention it deserves.

According to the website http://www.thespiritmolecule.com/ they are producing a movie based on the title of your book. What type of involvement (if any) have you contributed to the movie?

I’m a co-producer, have rounded up most of the interviewees, and performed most of the interviews.

In respects to current laws on psychedelic drugs, what do you see as happening in the future with how psychedelics are controlled?

Schedule I is a bit unwieldy, as these drugs are being used safely in research and are generating important data – that is 2 of the 3 criteria for Schedule I (not safe; no use) are being made irrelevant by current research projects. Perhaps a new Schedule could emerge which requires significant additional training in order to use these drugs in non-research settings, once some utility is established for them.

What do you see as some of the positive uses of psychedelics being in relation to psychiatry?

These drugs help us understand the biology of consciousness; and they may be helpful in treatment of various conditions or problems.

If you could start over, would you have done the research into DMT or what other area of research would you spend more of your time on?

I needed more of a peer group within which to do my research, but that’s usually the case when you’re doing something no-one else has done for such a long time.

Thanks for your time Dr.

Hope that’s helpful.

-L