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description: Racetams__The word nootropic was coined upon discovery of the effects of piracetam, developed in the 1960s. Studies of the racetams have revealed that these structurally similar compounds often act vi ...
Racetams__
The word nootropic was coined upon discovery of the effects of piracetam, developed in the 1960s.[14] Studies of the racetams have revealed that these structurally similar compounds often act via different mechanisms. Notable drugs include pramiracetam, oxiracetam, and aniracetam. Their mechanisms of action are not fully understood. Piracetam and aniracetam are known to act as positive allosteric modulators of AMPA receptors and appear to modulate cholinergic systems.[15] Although aniracetam and nebracetam show affinity for muscarinic receptors, only nefiracetam shows it at the nanomolar range. Racetams have been called "pharmacologically safe" drugs.[12]

Vitamins and supplements__
B Vitamins—may influence cognitive function through an effect on methylation and homocysteine levels, as excess homocysteine has been associated with cognitive impairment and the B vitamins work to reduce homocysteine.[16] However, although epidemiological evidence shows an association, two studies did not find B vitamin supplementation improves cognitive function, and another that found an association was criticized.[17] In 2008 a systematic review of trials found "little evidence of a beneficial impact" from supplements on cognitive function later in life.[18] A randomized, placebo-controlled trial in 168 70 year olds with mild cognitive impairment showed that a mix of B vitamins slowed the rate of brain atrophy; the slowing was related to a decrease in homocysteine levels.[19]
Choline— Higher concurrent choline intake was related to better cognitive performance.[20] It improves long-term memory in animal models.[21]
ω-3 fatty acids have been linked to the maintenance of brain function. Omega-3's provide DHA, important in the function and growth of nervous tissue. It is especially important during brain development.[22] A study preformed in Norway[23] demonstrated a potential link between Omega-3 consumption during pregnancy and child intelligence test scores.[24] A cross-sectional population-based study of 1,613 subjects found an association between PUFA intake and decreased risk for impairment of cognitive function & cognitive speed.[25] Another study showed that boys with lower levels of Omega-3 had more behavior issues, including ADHD.[26]
Isoflavones—may be related to cognitive function.[27] A double-blind, placebo-controlled study showed improvement in spatial working memory after administration of an isoflavone combination containing daidzein, genistein & glycitein.[28] In a randomized, double-blind, placebo-controlled study of older, non-demented men & women, soy isoflavone supplementation improved performance on 6 of 11 cognitive tests, including visual-spatial memory and construction, verbal fluency and speeded dexterity; unexpectedly, the placebo group performed better on 2 tests of executive function.[29]
Vitamin D—has positive effects on cardiovascular health and may have positive effects on cognitive function separately; the active form of Vitamin D seems to be involved in brain development and in adult brain function. In particular, metabolic pathways for Vitamin D in the hippocampus and cerebellum have been found. Epidemiological data show that higher Vitamin D levels (>20 ng/mL or 50nmol/L) are associated with better cognitive function, but do not seem to be associated with better memory performance.[30] Vitamin D has also been shown to be necessary in the production of dopamine [31]
Vitamin C— has been shown to help reduce brain injury and also reduce the amount of Cortisol in the body. High levels of Cortisol have been linked to Alzheimer's Disease.[32][medical citation needed]
Vitamin E—protects neurons from injury caused by Free Radicals.[33][medical citation needed]
A 2007 survey of online databases for herbs used in traditional herbal medicine to treat cognitive decline – without any proof of safety or efficacy – found over 150 plant species, such as Ginkgo biloba and Epimedium which is commonly call 'Goat weed'.[34]
Stimulants__
Stimulants are often seen as smart drugs, but may be more accurately termed productivity enhancers. These typically improve concentration and a few areas of cognitive performance, but only while the drug is still in the blood at therapeutic concentrations. Some scientists recommend widespread use of stimulants such as methylphenidate and amphetamines by the general population to increase brain power.[8][35]

Amphetamines
Amphetamine (Adderall, Dexedrine)—TA1 agonist and consequently a catecholamine releasing agent
Lisdexamfetamine (Vyvanse)—dextroamphetamine prodrug
Adrenergics
Dimethylamylamine—Non addictive stimulant. Once used in the treatment of ADHD and Burnout, but later discontinued.
Atomoxetine—norepinephrine reuptake inhibitor; uncompetitive NMDA antagonist; clinically used in the treatment of ADHD
Reboxetine—Norepinephrine reuptake inhibitor; approved in Europe for clinical depression but may also be used off-label to treat ADHD
Synephrine—endogenous trace amine found in significant concentrations in the Bitter orange;agonist at α1 adrenergic receptors
Cholinergics
Arecoline—nicotinic agonist and partial agonist at muscarinic receptors M1-4[36][37][38]
Nicotine A meta-analysis of 41 double-blind, placebo-controlled studies concluded that nicotine or smoking had significant positive effects on fine motor, alerting attention-accuracy and response time (RT), orienting attention-RT, short-term episodic memory-accuracy, and working memory-RT.[39]
Eugeroics ("Wakefulness Enhancers")—unproven primary mechanisms but proven efficacy as a Nootropic
Adrafinil
Armodafinil
Modafinil
CRL-40,941
Xanthines—reduces fatigue perception via adenosine receptor antagonism.
Caffeine—shown to increase alertness, performance, and in some studies, memory.[40] Children and adults who consume low doses of caffeine showed increase alertness, yet a higher dose was needed to improve performance.[41]
Paraxanthine
Theobromine
Theophylline.
Concentration and memory enhancement__
The nootropics in this section are purported or shown to enhance concentration or the recollection and formation of memories.

Cholinergics__
Cholinergics are substances that affect the neurotransmitter acetylcholine or the components of the nervous system that use acetylcholine. Acetylcholine is a facilitator of memory formation. Increasing the availability of this neurotransmitter in the brain may improve these functions. Cholinergic nootropics include acetylcholine precursors and cofactors, and acetylcholinesterase inhibitors:

Precursors
Choline—precursor of acetylcholine and phosphatidylcholine
DMAE—precursor of acetylcholine;Template:Medial citation needed appears promising in treating ADHD, though results are inconclusive[42]
Meclofenoxate—probable precursor of acetylcholine, approved for Dementia and Alzheimer's
Alpha-GPC
Cofactors
Acetylcarnitine—amino acid that functions in acetylcholine production by donating the acetyl portion to the acetylcholine molecule
Vitamin B5—cofactor in the conversion of choline into acetylcholine
Acetylcholinesterase inhibitors
Galantamine—also allosterically modulates certain nicotinic receptors to facilitate acetylcholine release[43]
Ipidacrine (Neiromidin) is a reversible cholinesterase inhibitor used in memory disorders of different origins.
Lycoris radiata (Red Spider Lily)—natural source for galantamine
Huperzine A—also shown to act as an NMDA antagonist and appears to increase nerve growth factor levels in rats[44]
Donepezil
Rosemary
Sage
Celastrus paniculatus
cannabis Due to its AChE-inhibiting properties, Cannabis appears to increase acetylcholine levels and therefore studies suggest it as a treatment for Alzheimer's.[45] Anxiolytic and analgesic found in cannabis. Neuroprotectant, possible Alzheimer's prevention and possible neurogenesis inducer.[46] Possible neurotoxic effects of a notable constituent, THC, have been documented[47]
Reuptake inhibitors and enhancers
Coluracetam— Increases high affinity choline uptake[48]
Piracetam— Increases high affinity choline uptake[49]
Oxiracetam— Increases high affinity choline uptake[49]
Pramiiracetam— Increases high affinity choline uptake[50]
Sulbutiamine— Increases high affinity choline uptake[51]
Ginsenosides
Agonists
AR-R17779
Arecoline
GTS-21
Ispronicline
Nicotine
PHA-543,613
PHA-709,829
SSR-180,711
WAY-317,538
GABA blockers__
The GABAA α5 receptor site has recently displayed memory improvements when inverse agonized.

α5IA—α5 inverse agonist. A number of α5IA analogues exist that, like α5IA, selectively and partially agonize some GABA receptor subtypes while inverse agonizing others, which may provide a nootropic effect without the associated anxiogenic effects of GABA inverse agonism.Template:Medial citation needed
Suritozole—α5 partial inverse agonist
Pantogam has a direct effect on the GABA-B receptor-channel complex.[52]
Glutamate modulators__
See also: AMPAkine
Ligands and modulators of the AMPA receptor, an ionotropic glutamate receptor, are being researched for a myriad of conditions, from Alzheimer's to ADHD. Although there are many AMPAkines being researched, those mentioned here show signs of entering the market in the near future. Other notable drugs with AMPA-modulating activity include aniracetam and tianeptine.

CX-717—pending FDA approval for memory-impairing illnesses and ADHD
IDRA-21—believed to improve memory by significantly enhancing long-term potentiation but used only in animals; incredibly potent
LY-503,430—under development for Parkinson's but showing increase in BDNF, specifically in areas of memory and higher cognitive skills
cAMP__
Cyclic adenosine monophosphate is a secondary messenger that may improve certain aspects of memory if increased. Common research tools for this purpose include PDE4 inhibitors, which prevents cAMP catabolism, and forskolin, a stimulator of adenylate cyclase.

Forskolin—stimulates adenylate cyclase[53]
Propentofylline—nonselective phosphodiesterase inhibitor with some neuroenhancement
Rolipram—PDE4 inhibitor, shows alertness enhancement, long term memory improvement and neuroprotection
Mesembrine—PDE4-inhibitor with possible serotonergic activity
Other__
α2A receptors are concentrated heavily in the prefrontal cortex and the locus coeruleus, with the potential to improve attention abilities via modulating post-synaptic α2A receptors in the prefrontal cortex.[54]

Guanfacine is an α2A receptor agonist, FDA approved the treatment of ADHD.[55][56] Guanfacine has been found to strengthen working memory, reduce distractibility, improve response inhibition, increase regional cerebral blood flow, reduce locomotor hyperactivity, and improve attentional control in animal models, as well as enhance memory function in humans.[57] Another study found no effect on healthy male adult's executive functions and working memory, and small decrements on 2 tasks relating to the sedative effect of guanfacine.[58]
PRL-8-53 is a potent hypermnesic drug that significantly increases long term memory with a currently unknown mechanism of action involving cholinergic and dopaminergic activation.[59][60]
Serotonergics__
Serotonin is a neurotransmitter with various effects on mood and possible effects on neurogenesis. Serotonergics are substances that affect the neurotransmitter serotonin or the components of the nervous system that use serotonin. Serotonergic nootropics include serotonin precursors and cofactors, and serotonin reuptake inhibitors:

Precursors
5-HTP—precursor (intermediate between tryptophan and serotonin)
Tryptophan—essential amino acid precursor; multiple neurotoxic metabolites[61]
Cofactors
Pyridoxal-phosphate (or PLP, pyridoxal-5'-phosphate, P5P, active form of Vitamin B6)—plays role in conversion of 5-HTP into serotonin (via the enzyme aromatic L-amino acid decarboxylase).[62][63]
Reuptake inhibitors
SSRIs—class of antidepressants that increase active serotonin levels by inhibiting reuptake, also shown to promote Neurogenesis in the hippocampus
Sceletium tortuosum—active constituent mesembrine shown to act as an SSRI[64] and PDE4 inhibitor. (Half-life unknown)
Hypericum perforatum—inhibits reuptake of serotonin (as well as Norepinephrine, Dopamine, GABA and Glutamate) via activation of TRPC6
MAO-A inhibitors
Resveratrol[65]
Curcumin[66]
Piperine[67]
Harmal[68] One of the major constituents of harmal, harmaline, has demonstrated acetylcholinesterase inhibition.
Rhodiola rosea[69]
5-HT2A receptor agonists
2C-x—it has been reported that some these compounds causes nootropic, stimulant, or anti-anxiety effects at low doses. 2C-D, 2C-I, and 2C-C are examples. However, at hallucinogenic doses, these chemical compounds may be unpredictable. Research on these chemicals is sparse; they require further investigation.
Other
Tianeptine—atypical antidepressant with anxiolytic properties; a hypothesized mechanism of action revolves around modulation of NMDA and AMPA receptors, based on tianeptine's effect of promoting stress-associated impaired neuroplasticity;[70][71] it increases the extracellular concentration of dopamine in the nucleus accumbens[72] and modulates the D2 and D3 dopamine receptors,[73] but this effect is modest and almost certainly indirect.[70]
Dopaminergics__
Metabolic precursors—raise levels[medical citation needed]
L-Phenylalanine—purported cognitive improvement[citation needed]
L-Tyrosine (or N-Acetyl-L-Tyrosine, more bioavailable form)—purported cognitive improvement
L-DOPA (L-3,4-dihydroxyphenylalanine)—precursor to catecholamines (dopamine); neurotoxic effects documented[74][75][76]
Biopterin—a vitamin (coenzyme) that is synthesized in the pineal gland[77] & crucial to the biosynthesis of dopamine
Pyridoxal-phosphate (or PLP, pyridoxal-5'-phosphate, P5P, active form of Vitamin B6)—cofactor for aromatic L-amino acid decarboxylase, the enzyme that decarboxylases L-DOPA, producing dopamine.
Reuptake inhibitors—stabilize/improve levels[medical citation needed]
Amineptine—mild stimulant
Methylphenidate—stimulant approved for ADHD; potent NDRI and σ1 receptor agonist[78]
Bupropion—atypical antidepressant; weak NDRI[79] and nicotinic antagonist[80]
MAO-B inhibitors—prevent some catabolism of dopamine and β-PEA
Selegiline—irreversible; amphetamine metabolites[81]
Rasagiline—irreversible
Rhodiola rosea—Adaptogenic herb; reversible[69]
Dopamine agonists
Ropinirole—agonist at D2, D3, and D4 receptors
Pramipexole—agonist at D2, D3, and D4 receptors
Amisulpride —atypical antipsychotic with higher affinity for the presynaptic Dopamine D2 receptor than postsynaptic, facilitating dopaminergic transmission in lower doses.[82]
Others
Mucuna pruriens (Velvet Bean)—natural source of L-DOPA
Modafinil—purported dopaminergic activity that exhibits the criteria of a Nootropic
Citicoline (INN) (aka: cytidine diphosphate-choline (CDP-Choline) & cytidine 5'-diphosphocholine)—studies suggest CDP-choline supplements partially prevent the loss of dopamine D2 receptors in aged mice,[83] and that CDP-choline supplementation ameliorates memory impairment caused by environmental conditions (in rats).[84] Preliminary research has found that citicoline may have potential in the treatment of attention deficit-hyperactivity disorder.[85][86]
Sleep__
Sleep is known to be important in memory consolidation, mood, anxiety, appetite, and numerous other physiological processes. Drugs that improve sleep may therefore have an indirect nootropic effect.

See also: Theories about the functions of REM sleep
Melatonin—antioxidant.[87][88] Exogenous melatonin protects against substantia nigra cell loss in ovariectomized rats.[89] May normalize circadian rhythms in humans[90]
Agomelatine— MT1 receptor agonist and 5-HT2C neutral antagonist[91]
Anti-depression, adaptogenic (anti-stress), and mood stabilization__
Stress (specifically elevated levels of circulating corticosteroids) has been associated with the cognitive deficits seen in human aging.[92] Many studies show that stress and fatigue negatively impact cognitive functioning in young adults.[93][94] Some level of stress in the learning environment may aid the ability to focus and retain information. However, stress levels, especially high, sustained or traumatic stressors, hinder declarative memory, spatial reasoning, learning, attention and working memory. Fatigue is also a stressor that impedes attention, processing, retrieval, working memory and short term memory.[93] The effects of stress on cognitive performance seem to be controlled by the sympatho-adrenal system and the hypothalamic-hypophysial-adrenal axis.[94]

Depression and depressed mood negatively affect cognitive performance and memory.[95] Depression was found to increase false memory, especially with negative words or subjects.[95]

It is reasoned that counteracting and preventing depression and stress management may be an effective nootropic strategy.[93][94] Proper nutrition, adequate sleep, and mechanisms for coping with stress, such as meditation, have been shown to improve learning and cognitive functioning both in the short and long term.[93][94]

The term adaptogen applies to most herbal anti-stress claims.[citation needed]

The substances below may not have been mentioned earlier on the page:

Beta blockers—evidence from controlled trials spanning 25 years supports the claim that beta-blockers are effective for reducing anxiety, likely through peripheral blockade of beta-receptors; most data comes from studies of generalized anxiety and acute stress.[96]
Theanine—relaxation; found in green tea; increases nicotinic acetylcholine and reduces nicotinic dopamine[citation needed]
Lemon Balm—displays adaptogen properties; in rats it has been shown to possess GABA transaminase inhibitor activity[97] and in homogenates of human cerebral cortical cell membranes possesses activity at acetylcholine receptors.[98] In a randomized, double-blind, placebo-controlled study of 18 healthy volunteers, 600 mg of 'Melissa officinalis' extract attenuated volunteers' response to a laboratory-induced stress test 1 hour after administration; 300 mg significantly improved speed of mathematical processing 1 hour after administration.[99]
Passion Flower—possible MAOI and neurotransmitter reuptake activity[citation needed]
Rhodiola Rosea—adaptogen; possible MAOI activity[100]
St John's Wort—herbal supplement approved (in Europe) to treat mild depression. Method of action is unproven but exhibits effects similar to both MAOIs and SSRIs.[citation needed] There is evidence that it may decrease the effectiveness of methylphenidate treatment.[101]
Ginseng (including Siberian ginseng)—adaptogenic effects shown[citation needed]
Sutherlandia frutescens—possible anti-inflammatory, reducing pain from those illnesses[citation needed]
Kava—anxiolytic herb[citation needed]
Grape seed extract—has shown some efficacy in reducing bodily stress[citation needed]
Adafenoxate—possible anxiolytic effect[citation needed]
Phenibut GABA receptor agonist excerting anxiolytic effects
Picamilon GABA prodrug which excerts anxiolytic effects by releasing GABA and niacin in the CNS.
Valerian—possible anxiolytic effect through agonism at GABA-A receptors[citation needed]
Butea frondosa—possible anxiolytic effect[102]
Gotu Kola—adaptogen and anxiolytic[citation needed]
Foti[disambiguation needed]—adaptogen; possible MAOI activity[citation needed]
Panax ginseng—Multiple randomized, placebo-controlled studies in healthy volunteers have been performed, results include increases in accuracy of memory, speed in performing attention tasks and improvement in performing difficult mental arithmetic tasks, as well as reduction in fatigue and improvement in mood.[103]
Many Chinese herbs such as Polygala tenuifolia, Acorus gramineus and Huperzia serrata.[104]
Bacopa monnieri[105]
Tulsi (Ocimum sanctum, sweet holy basil)[106]
IAP(5-APDI) Lifts mood and promotes a peaceful mindset. Anti-anxiety.
2-methyl-2-butanol Anti-anxiety that lifts mood and increases sociability. Although it doesn't have the side effects or toxic metabolites that ethanol has, frequent use may cause dependence.[citation needed]
Blood flow and metabolic function__
Brain function is dependent on many basic processes such as the usage of ATP, removal of waste, and intake of new materials. Improving blood flow or altering these processes can benefit brain function. The list below contains only vasodilators that have shown at least probable mental enhancement.

Mildronate may improve the ability of learning and memory, as the drug changes the expression of hippocampal proteins related to synaptic plasticity
Blessed Thistle—increases blood circulation, improving memory[citation needed]
Coenzyme q-10—antioxidant; increases oxygen usage by mitochondria
Creatine—protects ATP during transport
Lipoic acid—improves oxygen usage and antioxidant recycling, possibly improving memory
Pyritinol—Drug similar to B vitamin Pyridoxine
Picamilon—GABA activity and blood flow improver
Ginkgo biloba—vasodilator. Acts as an NRI.[107] A double-blind, placebo-controlled trial in young healthy females showed an improvement in short-term memory performance 1 hour after administration of a 600 mg dose.[108] An analysis of 29 placebo-controlled RCTs showed that "there is consistent evidence that chronic administration improves selective attention, some executive processes and long-term memory for verbal and non-verbal material."[109] A double-blind, placebo-controlled study in 20 young healthy volunteers showed a dose-dependent improvement in speed-of-attention following administration of 240 mg and 360 mg of Ginkgo extract, effects were measured 2.5h after administration and persisted at least until 6h; various other time- and dose-specific changes (some positive, some negative) in other areas were observed.[110]
Vinpocetine— is reported to have cerebral blood-flow enhancing[111] and neuroprotective effects,[112] and is used as a drug in Eastern Europe for the treatment of cerebrovascular disorders and age-related memory impairment.[113] Also shown to inhibit voltage-sensitive Na+ channels—however, through a similar mechanism to reserpine, Vinpocetine may temporarily deplete the monoamines serotonin, dopamine and norepinephrine by inhibiting VMAT, thus preventing them from reaching the synapse.[114] Vinpocetine may therefore induce or exacerbate depressive symptoms as an adverse effect. However, this effect tends to be reversible upon cessation of Vinpocetine administration, with full remission typically occurring within 3–4 weeks. Vinpocetine has been identified as a potent anti-inflammatory agent that might have a potential role in the treatment of Parkinson's disease and Alzheimer's disease.[115][116]
Vincamine—increases blood circulation (vasodilator) and metabolism in the brain; related to vinpocetine; used in sustained release.
Nicergoline—an ergot derivative used to treat senile dementia and other disorders with vascular origins; it has been found to increase mental agility and enhance clarity and perception; it decreases vascular resistance and increases arterial blood flow in the brain, improving the utilization of oxygen and glucose by brain cells; it has been used for more than three decades for the treatment of cognitive, affective, and behavioral disorders of older people.[117]
Experimental histamine antagonists__
The H3-receptor decreases neurotransmitter release: histamine, acetylcholine, norepinephrine, serotonin. Thus, H3-receptor-antagonists increases cognition, vigilance, and wakefulness.

Ciproxifan—produces wakefulness and attentiveness in animal studies, and produced cognitive enhancing effects without prominent stimulant effects at relatively low levels of receptor occupancy, and pronounced wakefulness at higher doses.[118]
A-349,821—It has nootropic effects in animal studies.[119]
ABT-239 – strong H3 receptor inverse agonist that is more active than ciproxifan, but its investigation into human use was dropped after it was discovered to cause QT prolongation in subjects
Betahistine
Modafinil
Nerve growth stimulation and brain cell protection__
Nerves are necessary to the foundation of brain communication and their degeneracy, underperformance, or lacking can have disastrous results on brain functions. Antioxidants may prevent oxidative stress and cell death, therefore exerting a neuroprotective effect.

Idebenone—antioxidant[citation needed]
Glutathione—chief antioxidant[citation needed]
Sesamol—antioxidant [120]
Acetylcarnitine (Acetyl-L-Carnitine Arginate or Hydrochloride)[citation needed]
Inositol—implicated in memory function, deficit linked to some psychiatric illnesses—has been shown particularly efficacious in OCD patients
Anticonvulsants—inhibit seizure related brain malfunction if a person has seizures[citation needed]
Phosphatidylserine—possible membrane stabilizer[citation needed]
Lion's Mane Mushroom—Stimulated myelination in an in vitro experiment[121] and stimulated nerve growth factor in an in vitro experiment with human astrocytoma cells.[122] Also improved cognitive ability, in a double-blind, parallel-group, placebo-controlled trial.[123]
SAM-e (S-Adenosyl methionine)—crucial for cellular regeneration (fuels DNA methylation[124]), also involved with the biosynthesis of dopamine & serotonin[125]
Acetylcysteine (L-cysteine)—precursor to antioxidant glutathione[126]
Uncaria tomentosa (Cat's Claw)—in an in vitro experiment with rats, it inhibited formation of brain beta amyloid deposits,[127] which have been associated with Alzheimer's disease.
(Cannabidiol and Δ9-tetrahydrocannabinol)—Cannabidiol (nonpsychoactive) and Δ9-tetrahydrocannabinol (psychotropic) antioxidant.[128]
Hormones__
These are hormones that have activity not necessarily attributable to another specific chemical interaction, but have shown effectiveness. Only specific nootropic effects are stated.

Vasopressin—memory hormone that improves both memory encoding and recall. Desmopressin (1-desamino-8-D-arginine vasopressin, DDAVP) was given to 17 children with attention & learning disorders daily for 10 days in a placebo-controlled, randomized, double-blind study; memory & learning were improved compared with placebo; the same study failed to find similar benefits after administration of a single dose.[129]
Pregnenolone—increases neurogenesis[medical citation needed]
Orexin or Hypocretin—significant wakefulness promoter
DHEA—precursor to estrogen and testosterone
Unknown enhancement__
Other agents purported to have nootropic effects but do not (yet) have attributable mechanisms or clinically significant effects (but may upon refinement of administration) are listed below.

Nootropics with proven or purported benefits:

Polygala tenuifolia (Yuan Zhi)— A randomized, double-blind, placebo-controlled, parallel-group study of the extract of dried roots of Polygala tenuifolia in healthy adults produced memory-enhancing effects.[130] A similar trial with elderly humans also found significant cognitive improvement.[131]
Bacopa monniera (Brahmi) — Shown to possess adaptogenic properties and enhance memory and concentration.[132] Folk use in Ayurvedic medicine purports "enhancement of curiosity"; Brahmi rasayana has been shown to improve learning and memory in mice[133]
Clitoria ternatea (Shankhpushpi) — In traditional Ayurvedic medicine, it has been used for centuries as a memory enhancer, nootropic, antistress, anxiolytic, antidepressant, anticonvulsant, tranquilizing and sedative agent.
Fipexide—drug for Dementia
Piperic acid—allegedly a mild serotonergic, nootropic, antistress, anxiolytic, and allegedly has mild to moderate memory enhancing effects.
Gerovital H3—famous alleged anti-aging mixture, most effects disproven but some mind enhancement shown
Sulbutiamine—fat soluble vitamin B1 derivative—caused mice to perform better on operant conditioning tests[134] and object recognition tests[135]
Royal Jelly—Increases brain cell growth and diversity, only demonstrated in-vitro, improbable in-vivo (it has been reported to stimulate the growth of glial cells[136] and neural stem cells in the brain.[137])
Curcumin—significant in-vitro activity, but in-vivo activity limited by low bioavailability unless accompanied by ingestion of piperine
Other nootropics__
Other substances sometimes classified as nootropics include jujube, mexidol, hydergine,[12] noopept, selank, semax and bifemelane.
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