"SMART DRUGS" FAQ

Cognition-Enhancement Drugs

The authors of this article are Michael Hutchison and John Morgenthaler. Michael Hutchison is the editor and publisher of MEGABRAIN REPORT and can be contacted there (see the address above). He is also the author of the books, MegaBrain: New Tools and Techniques For Brain Growth and Mind Expansion, The Book of Floating, and the recently published Anatomy of Sex and Power: An Investigation of Mind Body Politics.

John Morgenthaler is the co-author with Ward Dean, MD, of a full length book on over thirty cognition enhancing compounds. The book includes an index, references, and sources of compounds. John can be contacted at

COGNITION-ENHANCEMENT DRUGS

Picture this: You have a business meeting tomorrow with your Japanese distributor. This meeting requires that you be in top form for some critical negotiations. You have several reports to go over, many facts to memorize, and above all you have to get some rest.

Your first step? A trip to the drug store, of course. A meeting like this is much too important to take on without fine-tuning your biochemistry. You must create the optimal neurochemical conditions for learning and creativity. You ask the druggist, who then points you towards the shelf of cognitive enhancement compounds. You load up your basket with bottles of piracetam, vasopressin, hydergine, choline, DMAE, and maybe a little centrophenoxine.

After arriving home, and taking the appropriate doses of each of these you go into your study to slip on your cranial electric stimulator along with your light and sound device. You know from your experience and that of many pioneers in the consciousness revolution that this particular combination of chemicals and brain machines has a synergistic effect that will create the optimal psychobiological state for the tasks that lie ahead. You can be sure that your Japanese counterparts are engaged in a similar manner.

After an hour in your study you feel very different. You are relaxed, yet alert and creative. Your brainwave activity has altered, and an EEG would show that it has become more regular and has increased in amplitude in certain frequencies, causing you to feel simultaneously profoundly relaxed yet in a state of intense concentration, loose and creative as well as mentally quick and alert. A brain-mapping device would show that the two hemispheres of your brain were in a state of "superconnection," with an enormous increase in the amount of information flowing between the hemispheres. At the same time, the rate of metabolism and the energy level of your brain cells has sharply increased. You are now in the optimal state to imprint new memories, to plan new and more creative strategies, to visually rehearse every detail of your upcoming meeting...

Sound far-fetched? Well, both the brain machines and the cognitive enhancement compounds already exist. Megabrain described a variety of devices that show evidence of enhancing cognition (for a summary of several recent studies suggesting that CES devices can have clear cognition-boosting effects see the "Research Update" elsewhere in this issue); and the book also mentioned the cognition-enhancing effects of such neurochemicals as vasopressin and MSH-ACTH 4-10. Since then other mind- magnifying drugs have emerged as well as even more astonishing evidence of their ability to amplify learning, memory and thinking. What we don't know is how to best use them together, or even whether they should be used together.

That's what we want to find out. The problem, as many of you are aware, is that it is extremely difficult for those interested in performing research into the effects of brain machines to obtain the necessary funding and support. Mainstream science, particularly those elements in control of doling out grants and funds to support research, and many of the universities and institutions engaged in research, seem to have little interest in investigating these machines. What research is done usually involves the therapeutic applications of the devices rather that the induction of peak performance brain states.

On the other hand, huge amounts of money are being spent for research into cognition enhancing drugs. But much of the research is being done by the big pharmaceutical companies, who are racing with each other to develop patentable memory enhancement drugs and to obtain FDA approval for these compounds. Since the FDA is primarily oriented toward treating diseases in a medical context, and has not shown much interest in giving its approval to drugs that simply improve people's memories or boost intelligence, the pharmaceutical companies are directing their efforts toward gaining approval for their cognition-enhancement drugs as treatments for medical problems such as Alzheimer's disease, multiple-infarct dementia and senility. Since financial analysts estimate that such cognitive drugs could quickly produce sales of well over a billion dollars a year in the U.S. alone, and ultimately outsell antibiotics and tranquilizers, the competition is fierce, and these companies are in no mood to investigate ways their substances might work synergistically or in combination with other substances or other mechanisms such as mind machines.

Also, since their efforts are directed toward drugs that are patentable, these companies have little interest in exploring the cognition enhancement properties of substances that cannot be patented. Vitamin C is a good example: in a controlled study in which healthy individuals were tested both for levels of vitamin C and IQ, those with higher levels of the vitamin averaged 5 points higher in IQ; when those with the lower levels of the vitamin were given vitamin C supplements, their IQ scores increased by over 3.5 points. In some way, Vitamin C is a cognition-enhancing substance. But, of course no one can patent vitamin C, which is cheap and readily available.

In another example, one widely available and unpatentable substance (DHEA) is rumored to have demonstrated in a recent study some success in, among other things, treating AIDS, as well as cognition enhancement; however, the drug company involved in the experiments is now apparently trying to conceal the discoveries about DHEA until it can develop some variant that is patentable (i.e. has commercial value), and has obtained a court order forbidding the scientist in charge of the study to even speak with anyone about the matter.

WE HAVE MET THE GUINEA PIG AND IT IS US

However, we do have reason to believe that many of you are by nature curious, given to exploration and even experimentation-- that, in fact, many of you are already making use of some of these cognition-boosting nutrients. This being so, it seems clear to us that you have information that would be of interest and value to the rest of us. It's also clear that if there are hundreds or even thousands of you with such information, then by gathering it together, we can synthesize it, analyze it, begin to search for trends, tendencies, proclivities, and perhaps even make some important connections.

The first part of the survey is intended to be an open-ended exploration rather that a rigorous scientific study or an attempt to confirm an existing hypotheses. We hope not for solid conclusions or hard data, but rather to discover and delineate some interesting avenues for future research.

In a later issue, we will report on the early survey results. It's possible--though we cannot guarantee it--that in investigating the subjective responses we hope to receive from MEGABRAIN REPORT readers we will discover some trends. We can use this information to guide us in designing a more focused study for part two of the survey.

For example, we might receive many reports that the effects of piracetam are amplified when used with the light and sound devices. Then we could plan to focus more deeply on the particular machine/compound interaction, investigating the interactive effects over differing periods of time, using different sound and light frequencies and modes, and in various areas, such as memory, reaction speed, creativity and so on.

In this issue, we will introduce some of the more interesting compounds for cognitive enhancement, provide information about how to obtain each of them, present some methods for assessing and evaluating your own brain state and tracing your progress, and present a simple questionnaire. These self-assessment methods and our initial survey appear at the end of this article. First we will describe a few of the most promising cognition enhancing substances.

NOOTROPIC DRUGS

PIRACETAM

Piracetam has been the subject of intensive research for over 15 years, and has not only proven to be a powerful intelligence booster and cerebral stimulant, but also, even in massive acute and chronic dosages, appears to be nontoxic and to produce no side effects (it's so nontoxic one FDA employee reportedly claimed that since huge doses produce no toxic effects, it can't possibly have any pharmacological effects and must be physiologically inert). It is so remarkable in its effects and safety that its discovery by UCB Laboratories in Belgium sent virtually every other major pharmaceutical company scrambling to develop its own cerebral stimulant. This "Smart pill race" has resulted in the creation of a new drug category called the nootropics, from the Greek words noos (mind) and tropein (turn), meaning "acting on the mind".

Some of the nootropic drugs being tested now on humans include vinpocetine (being developed by Ayerst Laboratories), which speeds up learning, improves memory and recall and seems to block the action of substances that disrupt memory; aniracetam (Hoffman-La Roche), which appears to be about ten times more potent in improving and protecting memory than piracetam, pramiracetam (Warner-Lambert/Parke Davis), which seems to improve learning and memory by enhancing the firing of neurons in the hippocampus (a key to the formation of long-term memories), and oxiracetam (Ciba-Geigy), apparently two to three times as powerful as piracetam (intriguingly, research shows that when oxiracetam is given to pregnant rats their offspring proved more intelligent that control groups--similar findings have been reported for the offspring of pregnant rats kept in "enriched environments," as described in the "Research Update" elsewhere in this issue). All of these substances seem remarkably nontoxic and free of side effects.

As yet, there is no nootropic drug that is approved by the FDA for sale in the US, but, keenly aware of the multi-billion dollar potential of nootropics, the drug companies are pouring big bucks into research that will satisfy FDA requirements by proving how they work (still not well understood), and by proving their effectiveness in treating medical problems such as Alzheimer's disease and senility. In this article we will focus on the most extensively tested and widely available nootropic compound, piracetam.

Piracetam has been proven to boost learning and memory in normal subjects as well as those who suffer cognitive deficits, and is also a cognitive enhancer under conditions of hypoxia, or too little oxygen (recent expeditions to climb Mt. Everest have included piracetam as an "essential" medication to treat frostbite and memory lapses causes by altitude). A variety of clinical studies with human subjects, including studies of young healthy volunteers, healthy middle-aged subjects with some memory decline, elderly subjects, elderly subjects with senility, and alcoholics, have proven that piracetam enhances cortical vigilance, improves integration of information processing, improves attention span and concentration, and can produce dramatic improvements in both direct and delayed recall of verbal learning.

It's effective in the treatment of dyslexia, stroke, alcoholism, vertigo, senile dementia, sickle-cell anemia, and many other conditions, enhances the brain's resistance to various injuries and boosts its ability to recover from injuries, protects the brain against chemicals such as barbiturates and cyanides, and is widely used throughout Europe and Latin America (where it is sold over the counter).

The subjective effect described by a lot of people is that it "wakes up your brain". In fact, it selectively stimulates the anterior or frontal part of the forebrain--that part of the brain that has evolved most recently, rapidly and remarkably in the course of our evolution from ape to human, and which is the seat of our "higher functions."

Piracetam works in a number of ways to increase energy within the brain. First, it steps up the production of adenosine triphosphate (ATP), the energy storage and energy generating molecules within our cells. It also boosts cerebral metabolism by improving cerebral microcirculation (blood flow), increasing the brain's use of glucose, and increasing the brain's oxygen utilization. It also seems to enhance protein syntheses in the brain (it's been proven that protein synthesis is an essential step in laying down long-term memories).

SUPERCONNECTING THE BRAIN.

Piracetam's capacity to superconnect the hemispheres becomes even more intriguing in light of the evidence indicating that many of the most widely used mind machines and techniques for brain enhancement (such as binaural beat frequencies and the sound and light machines) function in part by facilitating integrated hemispheric functioning. This raises the possibility that since both the machines and piracetam seem to facilitate interhemispheric communication, there might be a potentiating or synergistic effect when such mind machines are used in combination with piracetam, resulting in a quantum leap in brain- enhancement effects.

PRECAUTIONS:

DOSAGE:

SOURCES:

HYDERGINE

A wealth of research going back over 20 years suggests that Hydergine may be what psychologist-pharmacist Ross Pelton calls "the ultimate smart pill." The substance, whose generic name is ergoloid mesylates, is made from a natural, organic source: the ergot fungus of rye plants (it was discovered at Sandoz laboratories by the visionary chemist Dr. Albert Hofmann, also known for his discovery of another ergot derivative, LSD 25). It increases mental abilities, prevents damage to brain cells, and may even be able to reverse existing damage to brain cells.

Hydergine acts in several ways to enhance mental capabilities and to slow down or reverse the aging processes in the brain. A few of the huge number of beneficial effects scientists have attributed to Hydergine include: increased protein syntheses in the brain; reduced accumulation of lipofuscin in the brain; increased quantities of blood and oxygen delivered to the brain; improvement of memory, learning and intelligence; beneficial improvements in brainwave activity; increased metabolism in brain cells; normalization of blood pressure; and increased production of such neurotransmitters as dopamine and norepinephrine (neurochemical messengers essential to the formation of memory, and also associated with arousal, alertness, elation and pleasure). Hydergine also functions as a powerful antioxidant and thus protects the brain against the damage caused by those infamous rascally free radicals (unstable and extremely reactive molecules produced by normal metabolism, which cause damage associated with aging, cancer and cardiovascular disease).

One way that Hydergine may enhance brain functioning is by mimicking the effect of a substance called nerve growth factor (NGF). NGF promotes the growth of dendrites--the long branching fibers by which neurons receive information from other neurons. Scientists studying the effects of learning on the brain have found it is directly related to dendritic growth. Hydergine seems to work by the same neurochemical pathway as NGF to produce neural growth.

While Hydergine is widely used for the treatment of senility, scientists have also studied its effects, both short term and long term, in normal healthy humans; these studies noted significant improvements in a variety of cognitive function, including alertness, memory, reaction time, abstract reasoning and cognitive processing ability.

PRECAUTIONS

DOSAGE:

SOURCES:

VASOPRESSIN

"I have smoked pot on a more or less (usually more) daily basis for 20 years. When I read that vasopressin is inhibited by pot, I found a source for buying some. Now I notice that when I use vasopressin with marijuana I still get stoned, but I have little or none of the 'dummying down' effect of the pot. And what a surprise to find that vasopressin intensifies orgasms!"

Vasopressin, called "the memory hormone," is a natural brain peptide, stimulated by acetylcholine and released in the pituitary. It actually helps create, imprint, and store memories, and is essential to remembering. Apparently vasopressin is involved in picking out and chunking together related bits of information from the stream of consciousness, integrating these chunks into coherent structures, and then "imprinting" these images or concepts into long-term memory by transforming electrical impulses into complex proteins that contain memories and are stored away in the brain. The act of remembering the stored information is also mediated by vasopressin.

Over 20 years ago scientists discovered that vasopressin had extraordinary effects on the memory of laboratory animals-- preventing chemically and electrically induced amnesia, actually reversing amnesia, and dramatically boosting the memory and intelligence of normal animals. These findings spurred much research into the cognition-enhancement effect of vasopressin on humans. Among the key findings are that small doses of the hormone can have striking success in quickly reversing traumatic amnesia (amnesia caused by injuries such as car crashes), can reverse age-related memory loss and actually restore lost memories, and can produce sharp improvements in learning and memory using measures such as abstract and verbal memory, organizational capacities, recall, attention, concentration, focus, short-term memory, optical memory, and long-term memory. It also boosts performance in such areas as reaction speed, visual discrimination, and coordination.

Vasopressin pours out during moments of trauma or extreme arousal, which may explain why those times seem to be so deeply imprinted in our brains, and are remembered with such clarity. Vasopressin is also released by cocaine, LSD, amphetamines, Ritalin, and Pemoline (Cylert). Those who make frequent use of these drugs deplete their brain's vasopressin supply. The result is depression, and a decline in cognitive function. The frequent user's response to this depression is to take more of the drug, thus trying to wring more vasopressin out of their depleted brain: ultimately the well runs dry. Vasopressin, however, is not a drug but the actual brain hormone that has been depleted, so it can produce dramatic and virtually instantaneous improvements in mood and mental functioning.

Unlike stimulants, alcohol and marijuana do not deplete but actually suppress the release of vasopressin, which could account for the loss of memory many have noticed when drunk or stoned, or when trying to remember events that occurred while they were high. Vasopressin can reduce the harmful effects of these drugs and enhance alertness, reaction speed and concentration.

Anecdotal evidence suggests that vasopressin can produce a state of euphoria accompanied by self-confidence, energy, assertiveness, and a sensation of extreme mental clarity. Many believe it is ideal for situations in which lots of new information needs to be processed and remembered--such as studying for an exam, learning a language, ploughing through difficult or complex works. Some use it for more mundane purposes, such as when they have to drive late at night and want to remain alert.

PRECAUTIONS

DOSAGE:

SOURCES:

HOW TO OBTAIN COGNITION-ENHANCEMENT SUBSTANCES BY MAIL ORDER.

In the April, 1982 issue of the FDA Drug Bulletin, the agency included a policy statement clarifying the question of "unapproved" uses for drugs, clearly stating that "'unapproved' uses may be appropriate and rational in certain circumstances, and may, in fact, reflect approaches to drug therapy that have been extensively reported in medical literature... Valid new uses for drugs already on the market are often first discovered through serendipitous observations and therapeutic innovation." In sum, the FDA clearly approves of the "unapproved" uses as an important means for innovation and discovery.

Also, though it is not widely known, a July, 1989 FDA ruling now makes it quite legal to import effective drugs used elsewhere but not available in the U.S. The FDA now allows the importation and mail shipment of a three month supply of drugs, for personal use, as long as they are regarded as safe in other countries. The new ruling, FDA pilot guidelines chapter 971, was made as a result of heavy pressure from AIDS political action groups, which insisted AIDS sufferers were denied access to potentially life-saving substances that were widely used abroad but were still unapproved for use in the U.S.

InHome Health Services, a mail order pharmacy in Switzerland, is one of a number of companies established in response to this new FDA ruling. InHome carries a wide variety of drugs for cognitive enhancement, life extension, and the treatment of AIDS which are not available in the US.

All of the drugs discussed here can be purchased without a prescription. You can request a full price sheet by writing to: InHome Health Services,

• Centrophenoxine (250mg x 60) $19
• Hydergine (4.5mg x 28 tablets) $16.50
• Phenytoin (Generic Dilantin, 100mg x 100) $8.80
• Piracetam (800mg x 60 tablets) $16.60
• Sulbutiamine (200mg x 30) $12.50
• Vasopressin (5ml spray) $8.75

Another company with higher prices, but possibly faster service is:

INTERLAB

~References:

Piracetam

• Anderson, K., Anderson, L. Orphan Drugs. Los Angeles, CA: The Body Press, 1983, p. 169.
• Bartus, Raymond T., et al. "Profound Effects of Combining Choline and Piracetam on Memory Enhancement and Cholinergic Function in Aged Rats." Neurobiology of Aging. 1981, Vol. 2, pp. 105-11.
• Buresova, O., Bures, J. "Piracetam-Induced Facilitation of Interhemispheric Transfer of Visual Information in Rats." Psychopharmacologia (Berlin). 1976, Vol. 46, pp. 93-102.
• Bylinsky, G. "Medicine's Next Marvel: The Memory Pill." Fortune. January 20, 1986, pp. 68-72.
• Chase, C.H., et al. "A New Chemotherapeutic Investigation: Piracetam Effects on Dyslexia." Annals of Dyslexia. 1984, Vol. 34, pp. 29-48.
• Conners, et al. "Piracetam and Event-Related Potentials in Dyslexic Children." Psychopharmacology Bulletin. 1984, Vol. 20, pp. 667-73.
• Dimond, S.J., Browers, E.Y.M. "Increase in the Power of Human Memory in Normal Man Through the Use of Drugs." Psychopharmacology. 1976, Vol. 49, pp. 307-9.
• Dilanni, M., et al. "The Effects of Piracetam in Children with Dyslexia." Journal of Clinical Psychopharmacology. 1985, Vol. 5, pp. 272-8.
• Donaldson, T. "Therapies to Improve Memory." Anti-Aging News. 1984, No. 4, pp. 13-21.
• Ferris, S.H., et al. "Combination of Choline/Piracetam in the Treatment of Senile Dementia." Psychopharmacology Bulletin. 1982, Vol. 18, pp. 94-8.
• Friedman, E., et al. "Clinical Response to Choline Plus Piracetam in Senile Dementia: Relation to Red-Cell Choline Levels." The New England Journal of Medicine. 1981, 304, No. 24, pp. 1490-1.
• Giurgea, C.E. "The 'Nootropic' Approach to the Pharmacology of the Integrative Activity of the Brain." Conditional Reflex. 1973, Vol. 8, No. 2, pp. 108-15.
• Ibid. "A Drug for the Mind." Chemtech. June 1980, pp. 360-65.
• Giurgea, C.E., Salama, M. "Nootropic Drugs." Progress in Neuropsychopharmacology. 1977, Vol. 1, pp. 235-47.
• Kent, S. "Piracetam Increases Brain Energy." Anti-Aging News. 1981, Vol. 2, No. 10, pp. 65-69.
• Mindus, P., et al. "Piracetam-Induced Improvement of Mental Performance: A Controlled Study on Normally Aging Individuals." ACTA Psychiatrica Scandinavia. 1976, Vol. 54, pp. 150-60.
• Mondadori, C., et al. "Effects of Oxiracetam on Learning and Memory in Animals: Comparison with Piracetam." Clinical Neuropharmacology. 1986, Vol. 9, Supp. 13. New York: Raven Press, pp. S27-S37.
• Nickerson, V.J., Wolthuis, O.L. "Effect of the Acquisition-Enhancing Drug Piracetam on Rat Cerebral Energy Metabolism Comparison with Naftidrofuryl and Methamphetamine." Biochemical Pharmacology. 1976, Vol. 25, pp. 2241-4.
• Parducz, A. "Depletion of Synaptic Vesicle Lipids in Stimulated Cholinergic Nerve Terminals." Alzheimer's Disease: Advances in Basic Research and Therapies. Proceedings of the Third Meeting of the International Study Group of the Treatment of memory Disorders Associated with Aging. Zurich, Switzerland, 1984, pp. 217-26.
• Pearson, D., Shaw, S. Durk Pearson & Sandy Shaw's Life Extension Newsletter. October 1988, Vol 1, Number 8, p. 65.
• Pellegata, R., et al. "Cyclic Gaba-Gabob Analogues." Presented at VI International meeting of the International Society For Neurochemistry, Copenhagen, August 21-26, 1977.
• Pelton, R., Pelton, T.C. Mind Food & Smart Pills. New York: Doubleday, 1989.
• Pepeu, G., and Spignoli, G. Neurochemical Actions of "Nootropic Drugs". Advances in Neurology. Vol. 51: Alzheimer's Disease. New York: Raven Press, Ltd., 1990.
• Pilch, H., et al. "Piracetam Elevates Muscarinic Cholinergic Receptor Density in the Frontal Cortex of Aged But Not of Young Mice." Psychopharmacology. 1988, 94, pp. 74-8.
• Poschel, B.P.H. "New Pharmacologic Perspectives on Nootropic Drugs." Handbook of Psychopharmacology. 1988, pp. 11-18, pp. 24-5.
• Stegink, A.J. "The Clinical Use of Piracetam, a New Nootropic Drug." Arzneimittelforschung. 1972, Vol. 22, No. 6, pp. 975-7.
• U.B.C. Laboratories, Pharmaceutical Division. "Basic Scientific and Clinical Data of Nootropil." Brussels, Belgium: U.B.C. Laboratories, 1977.
• Wilsher, C.R. "Piracetam and Dyslexia: Effects on Reading Tests." Journal of Clinical Psychopharmacology. 1987, Vol. 7, No. 4, pp. 230-7.
• Wurtman, R.J., et al. "Piracetam Diminishes Hippocampal Acetylcholine Levels in Rats." Life Science. 1981, Vol. 28, Neupp. 1091-3.
• Zhang, S., et al. "Effects of Cerebral GABA Level on Learning and Memory." Pharmacologica Sinica. 1989 10(1): pp. 10-2.

Hydergine

• Branconnier, R. "The Efficacy of the Cerebral Metabolic Enhancers in the Treatment of Senile Dementia." Psychopharmacology Bulletin. 1983, 19(2), pp. 212-20.
• Copeland, R.L., Jr., et al. "Behavioral and Neurochemical Effects of Hydergine in Rats." Archives of International Pharmacodynamics. 1981, Vol. 252, pp. 113-23.
• Emmenegger, H., Meier-Ruge, W. "The Actions of Hydergine on the Brain." Pharmacology. 1968, Vol. 1, pp. 65-78.
• Exton-Smith, A.N., et al. "Clinical Experience with Ergot Alkaloids." Aging. New York: Raven Press, 1983, Vol. 23, p. 323.
• Fanchamps, A. "Dihydroergotoxine in Senile Cerebral Insufficiency." Aging. New York: Raven Press, 1983, Vol. 23, pp. 311-22.
• Hindmarch, I., et al. "The Effects of an Ergot Alkaloid Derivative (Hydergine) on Aspects of Psychomotor Performance, Arousal, and Cognitive Processing Ability." The Journal of Clinical Pharmacology. November-December 1979, pp. 726-31.
• Hughes, J.R., et al. "An Ergot Alkaloid Preparation (Hydergine) in the Treatment of Dementia: A Critical Review of the Clinical Literature." Journal of the American Geriatrics Society. 1976, Vol. 24, pp. 490-97.
• Kleimola, T. "Generic Bioavailability Test." Turku, Finland: Leiras Pharmaceuticals, 1982.
• Nandy, K., Schneider, F.H. "Effects of Dihydroergotoxine Mesylate on Aging Neurons in vitro." Gerontology. 1978, Vol. 24, pp. 66-70.
• Otomo, E., et al. "Comparison of Vipocetine with Ifenprodil Tartrate and Dihydroergotoxine Mesylate Treatment and Results of Long-Term Treatment with Vinpocetine." Current Therapeutic Research. 1985, Vol. 37, No. 5, pp. 811-21.
• Pearson, D., Shaw, S. Life Extension: A Practical Scientific Approach. New York: Warner Books, 1982.
• Pelton, R., Pelton, T.C. Mind Food & Smart Pills. New York: Doubleday, 1989.
• Rao, D.B., Norris, J.R.. "A Double-Blind Investigation of Hydergine in the Treatment of Cerebrovascular Insufficiency in the Elderly." Johns Hopkins Medical Journal. 1971, Vol. 130, pp. 317-23.
• Spiegel, R., et al. "A Controlled Long-Term Study with Ergoloid Mesylates (Hydergine) in Healthy, Elderly Volunteers: Results After Three Years." Journal of the Geriatrics Society. 1983, Vol. 31, No. 9, pp. 549-55.
• Weil, C., ed. "Pharmacology and Clinical Pharmacology of Hydergine." Handbook of Experimental Pharmacology. New York: Springer-Verlag 1989.
• Yesavage, J.A., et al. "Dihydroergotoxine: 6-Mg versus 3-Mg Dosage in the Treatment of Senile Dementia. Preliminary Report." Journal of the American Geriatrics Society. 1979, Vol. 27, No. 2, pp. 80-82.
• Yoshikawa, M., et al. "A Dose-Response Study with Dihydroergotoxine Mesylate in Cerebrovascular Disturbances." Journal of the American Geriatrics Society. 1983, Vol. 31, No. 1, pp. 1-7.

Vasopressin

• De Wied, D., et al. "Vasopressin and Memory Consolidation." Perspectives in Brain Research. New York: Elsevier Scientific Publishing, 1975.
• Gold, P.W., et al. "Effects of l-Desamo-8-Arginine Vasopressin on Behavior and Cognition in Primary Affective Disorders." The Lancet. November 10, 1979, pp. 992-94.
• Laczi, F., et al. "Effects of Lysine-Vasopressin and l-Deamino-8-D-Arginine-Vasopressin on Memory in Healthy Individuals and Diabetes Insipidus Patients." Psychoneuroendocrinology. 1982, Vol. 7, No. 2, pp. 185-92.
• Legros, J. J., et al. "Influence of Vasopressin on Learning and Memory." The Lancet. January 7, 1978, pp. 41-42.
• Oliveros, J.C., et al. "Vasopressin in Amnesia." The Lancet. January 7, 1978, p. 42.
• Pearson, D., Shaw, S. Life Extension: A Practical Scientific Approach. New York: Warner Books, 1982.
• Pelton, R., Pelton, T.C. Mind Food & Smart Pills. New York: Doubleday, 1989

Additional stuff

PIRACETUM

DMAE

HYDERGINE

OTHERS

That about does it. So far, DMAE seems like the only real win, since it appears to cut need for sleep by a bit---therefore, more day to work with. More experimentation will certainly be conducted.

> From Max More

My own experience is with piracetam, centrophenoxine (Lucidril), and vasopressin (Diapid). Piracetam might have had some effects, but made my eyes so red on the days that I took it that I decided it was not worth continuing. Vasopressin, as Max said, is mainly useful when the brain's supply of neurotransmitters is either depleted (following a caffeine or other stimulant binge) or suppressed (by alcohol or other CNS depressant) -- I consider it the long-sought "sober-up" treatment.

Centrophenoxine gave me the most dramatic results -- I did not measure them by any kind of psychometric tests, but I felt more alert, and experienced faster and more reliable recall than previously. Since Lucidril works by making a permanent brain change (enabling brain metabolism to remove life-long accumulations of the aging pigment lipofuscin from the neurons), its effects are cumulative -- you continue to feel sharper even after you quit taking the drug.

Yours truly and sign it!"
Dave Krieger

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