 vinpocetine
print version
Vinpocetine, The Superior Cerebral Enhancer
And Protector
By James South MA
Vincamine (VCM) is an
alkaloid extracted from the Periwinkle plant, Vinca minor. Vinpocetine (VPC) is
produced slightly altering the VCM molecule. VPC is more technically referred
to as "ethyl apovincaminate."
VCM and VPC have been widely
researched and used clinically for over 25 years, in disorders ranging from cerebral
arteriosclerosis and senile dementia, to Meniere's disease, tinnitus, and diabetic
retinopathy.
Research has gradually shown VPC to be the superior Vinca
alkaloid, usually having a few (and minor) if any side effects and a greater range
of clinical and metabolic benefits than VCM.
Vinpocetine's actions
VPC has been shown to be a cerebral metabolic enhancer and a selective cerebral
vasodilator (1,2). VPC has been shown to enhance oxygen and glucose uptake from
blood by brain neurons, and to increase neuronal ATP bio-energy production, even
under hypoxic (low oxygen) conditions (3,4).
VPC has been shown to reduce
the cell death that normally occurs when a brain region is temporarily but severely
deprived of blood flow (5).
The human brain and its energy
To fully appreciate the medical and life enhancement importance of these key aspects
of VPC pharmacology, it is first necessary to review some basics of brain physiology
and biochemistry.
The human brain typically weighs about 3 pounds (1-3%
of total bodyweight). The brain is generally estimated to contain 10-100 billion
neurons (electrically active nerve cells), and approximately 10 times as many
glial cells, which are structural and nutritional support cells surrounding neurons.
The brain normally receives 15-20% of the body's total blood supply, and uses
15-20% of the body's total inhaled oxygen.
The brain must use this oxygen,
along with its chief fuel- glucose- to produce and use 15-20% of the body's total
ATP energy.
Unlike most other cells, which can burn either fat or sugar
(glucose) for their energy production needs, neurons can only burn glucose under
normal, non-starvation conditions, and they typically consume 50% of the total
blood sugar. Unlike liver and muscle cells, which can store large amounts of sugar
as glycogen, neurons can only store at most a minute or two's worth of glucose,
and so they are dependant upon a continuous and uninterrupted blood supply to
maintain normal energy metabolism and avoid injury or death.
Most other
cells (except heart and skeletal muscle cells) reproduce continually throughout
a lifetime yet after the brain reaches a full complement of neurons (birth to
2 years of age), neurons never reproduce, they are an irreplaceable essential
of life.
Under normal conditions of adequate oxygen supply, neurons convert
glucose into energy (ATP) through a 3-phase process.
The first phase
occurs in the cytoplasm of the cell (the gel-like stuff between the nucleus and
outer cell membrane), and is called "aerobic [oxygen using] glycolysis."
As each molecule of glucose is metabolized through aerobic glycolysis, two molecules
of ATP are produced. In addition, two other by-products result which are used
to make further ATP in the next two phases of energy production.
The
"ash" from aerobically burning glucose is pyruvic acid, which is then
converted to acetyl-coenzyme A (ACoA).
ACoA is then metabolized through
the Kreb's or citric acid cycle to generate more ATP. The Kreb's cycle occurs
inside the mitochondria, the "power plants" of the cell. The other energy-rich
substance produced through aerobic glycolysis is NADH- the active coenzyme of
vitamin B3.
Aerobic glycolysis produces two molecules of NADH for each
molecule of glucose burned. The NADH is then transported to the mitochondria,
where it serves as a fuel in the third phase of energy metabolism- the electron
transport side chain (ETSC). Each NADH run through the ETSC, with adequate oxygen,
produces 3 molecules of ATP. Eventually, through the successful interaction of
aerobic glycolysis, the Kreb's/ citric acid cycle, and the ETSC, a single molecule
of glucose can yield a maximum of 38 molecules of ATP bio-energy, assuming adequate
oxygen for both glycolysis and mitochondrial "respiratory" metabolism.
When neurons are under-supplied with oxygen, however, different forms of
sugar burning occurs- anaerobic (without oxygen) glycolysis.
For each
molecule of glucose burned, anaerobic glycolysis yields two molecules of ATP.
However, instead of producing the valuable Kreb's cycle fuel, pyruvic acid, anaerobic
glycolysis produces the somewhat toxic waste product, lactic acid. And anaerobic
glycolysis yields no bonus of NADH to be converted to ATP through the ETSC. And
with inadequate oxygen, mitochondrial metabolism proceeds poorly, it at all.
Thus anaerobic glycolysis produces a total of only two ATP's for each glucose
burned. In other words, when glucose brain fuel is burned without adequate oxygen,
it produces only 5% as much ATP energy as when glucose is burned with adequate
oxygen!
There are 3 main uses for ATP inside neurons- the "housekeeping-maintenance,"
electrical and neurotransmitter functions. Since neurons don't reproduce and must
last a lifetime, they are continually expending energy to repair or replace various
cell components- cell membrane segments, microtubules, mitochondria, etc.
Neurons also use ATP to produce, transport, package, secrete and reuptake
neurotransmitters, which provide cell to cell communication. And massive amounts
of ATP are necessary to facilitate the frequent discharges of electrical energy
from the receiving end of the neuron- the dendrites- through the cell body, where
signal processing occurs, and down the transmitting end- the axon. For this electrical
process to occur there must be a rapid and continuous exchange of sodium and potassium
ions back and forth across the neuronal membranes.
This exchange process depends
on sodium-potassium pumps, powered by sodium-potassium ATPase enzyme systems.
Some physiologists estimate as much as 45% of a neuron's ATP may be used
to power the sodium-potassium pumps.
Brain disorders
It should
now be evident why unconsciousness rapidly occurs if breathing stops, or brain
blood flow is interrupted even briefly.
As the delivery of oxygen to
the brain halts, neurons rapidly shift from aerobic to anaerobic energy metabolism,
with a consequent drop in energy production, up to 95%!
There will simply
not be enough ATP energy to facilitate neuronal electrical activity and neurotransmitter
discharge- the electrochemical basis for consciousness. And if aerobic metabolism
ceases for too long, eventually either irreparable damage or even cell death may
occur, as even the "housekeeping-maintenance" neuronal activities fall
behind or fail due to energy shortage.
For most of us, falling unconscious
or suffering brain death due to cessation of breathing or brain blood flow is
not a regular problem to contend with! However, a more subtle, insidious, slow-developing
form of brain energy crisis can and does occur in most people to some degree over
a lifetime, in the form of cerebral arteriosclerosis, ministrokes, or transient
ischaemic attacks (brief interruptions of brain blood supply, often due to blood
vessel spasm).
In its early stages, this brain energy crisis may lead
to only the slightest of symptoms- subtle memory impairment, occasional confusion
or lapses in concentration, slightly more difficulty in learning etc.
At a more advanced stage the brain energy crisis may show itself as senility or
senile dementia, and eventually may terminate in coma or death.
Thus
as Branconnier notes "...the severity of the dementia is directly correlated
to the loss of functional brain tissue, independent of the primary neuropathology.
This view is consistent with evidence from studies of cerebral blood flow, oxygen
uptake, and glucose utilization that have shown that brain carbohydrate metabolism
(BCM) is impaired in a variety of dementias and that the degree of reduction in
BCM is correlated with the severity of the dementia..." (6)
Orthomolecular
psychiatry pioneer Abram Hoffer has suggested that when the brain oxygenation
becomes chronically deficient enough, neurons switch to anaerobic glycolysis as
their main energy source. This may provide (barely) enough energy for the neurons
to survive, but it will not provide enough energy to power their functional roles
as electrochemical signal processors/ transmitters. Then the affected neurons
will be "off-line," in an electrically quiescent "idling"
state.
However, if normal aerobic metabolism is restored before irreparable
cell damage or death occurs, then the neurons and their functions can be restored
(7).
Vinpocetine's clinical trials
Both animal experimental
and human clinical research have shown VPC to restore impaired brain carbohydrate/
energy metabolism.
In 1976 Vamosi and colleagues reported their favorable
results comparing VPC with Xanthinol Nicotinate in treating 143 patients with
various cerebrovascular diseases.
They measured a large number of blood
and cerebrospinal fluid variables before and after treatment, such as glucose,
lactate, pyruvate, oxygen, pH, electrolyte levels, etc. They concluded from their
study "Though not all the changes are significant statistically, yet connected
with each other they prove that Cavinton [VPC] enhances both glycolytic and oxidative
reactions of glucose breakdown in CNS [brain]. The changes in the concentration
of K [potassium] and Mg [magnesium]... may be considered a sign of recovery of
the energy metabolism of the nerve cells." (1)
Vamosi's study also
demonstrated a superior clinical efficacy of VPC over Xanthinol Nicotinate.
In his review on the use of Vinca alkaloids in dementia, Nicholson observed that
"...vincamine increases mitochondrial respiratory rate in mitochondrial suspensions...,
indicating that vinca alkaloids can increase the rate of ATP synthesis... In addition,
elevation of cortical cyclic AMP levels may increase ATP availability... and this
may contribute to the metabolic activity of vinpocetine." (8)
Karpati
and Szporny resulted favorable results of VPC used to treat anaesthetized dogs.
Anesthetics reduce brain aerobic metabolism and ATP production- this is a key
aspect of their ability to produce unconsciousness. Based on their experiments
they note that "Increase of cerebral arterial-venous oxygen difference, cerebral
metabolic rate for oxygen and cerebral oxygen utilization indicate that RGH-4405
[vinpocetine] affects cerebral metabolism, with a dose-dependant rise in endogenous
respiration of cerebral tissue... Our results indicate that rate of cerebral [energy
production] metabolism is increased by [vinpocetine]."
Karpati and
Szporny conducted a study with cats that were subjected to repeated episodes of
brain hypoxia. They reported that "... transitory and partial interference
even with normal cerebral circulation caused an increase of Neurochemical disturbances
due to hypoxia... deficient formation of intermediaries in the Krebs cycle was
observed, mainly due to shortage of oxygen.
These and cytological studies
refer to a selective failure of mitochondrial metabolism... RGH-4405 [VPC] had
favorable effects on these parameters... It seems probable that the effect of
RGH-4405 [VPC] is even more pronounced in vascular insufficiency..." (9)
These are just a few of the many reports indicating the ability of VPC to safely
and effectively restore failing neuronal energy metabolism, even under hypoxic
or ischaemic (poor blood flow) conditions.
Vinpocetine's unique and
selective affects
VPC has also been shown to be a unique, selective cerebral
vasodilator. Solti and co-workers reported their results using VPC with 10 men
suffering from cerebrovascular disorders (average age: 49). They conclude; "Cavinton
[VPC] belongs to the rather few drugs which exert a potent, favorable effect on
the cerebral circulation. The effect of Cavinton [VPC] on the cerebral circulation
has two main features;
1. It strongly reduces cerebral vascular resistance,
which is typically high in cerebral vascular disease;
2. Cerebral fraction
of cardiac output is increased. No marked effect on systemic circulation, blood
pressure and total vascular resistance decreased very slightly on acute Cavinton
effect. Since the drug, far from increasing RATHER reduces effort of the heart,
its effects may be assumed to be favorable in cerebral alterations associated
with heart disease and hypertension." (2)
Hadjiev and Yancheva also
reported favorable clinical results with 50 patients suffering cerebral circulation
impairment. They noted that VPC does not elicit the "steal effect" that
occurs with non-selective vasodilators. (The "steal effect" occurs when
a vasodilator opens up blood vessels in brain regions that do not suffer from
reduced circulation even more than it opens up blood vessels in regions suffering
damaged circulation. This causes a net shift of cerebral blood flow away from
the injured area, causing even further damage to the already blood starved part).
(10)
Vinpocetine and the eyes
In another study with 100 patients
suffering from poor blood circulation to the eye, Kahan and Olah note VPC's inhibition
of platelet aggregation. The microvessels that feed neurons in the brain and retina
are smaller in diameter than a single red blood cell- they are easily "clogged
up" by clumps of platelets, impairing local microcirculation. This provides
another mechanism of action for VPC's ability to enhance cerebral blood flow-
inhibition of unnecessary platelet aggregation, which may be triggered by a high
fat diet, magnesium deficiency, and stress hormones, among other factors (11).
Vinpocetine and brain aging
Another key benefit from VPC derives
from its activating effect on the noradrenaline nerve cluster in the reticular
activating system called the "locus coeruleus." Olpe and co-workers
have shown that VCM and some of its derivatives (VPC) to be some of the most effective
activators of locus coeruleus (LC) neurons. This small group of neurons extends
its noradrenaline-secreting nerve fibers diffusely throughout the cerebral cortex
(the thinking, planning, integrative brain).
Olpe notes that LC neurons
decline in number with increasing age, with degeneration advancing slightly faster
in men than women. The lessening number and activity of LC neurons that occurs
with aging is known to play a significant role in the reduction of concentration,
alertness, and information processing speed and ability that occurs with aging.
Thus VPC's ability to improve the cerebral cortical activating power of remaining
LC neurons makes it a true "cognition enhancing" agent (12).
Vinpocetine, EEG and aging
Saletu and Grunberger have published considerable
pioneering research on EEG correlates of vigilance, and the effects of various
drugs on EEG recordings. They report that "Human brain function as measured
by... electroencephalogram (EEG) shows significant alterations in normal and pathological
aging characterized by an increase of [slow wave] delta and theta activity and
a decrease of alpha and ... beta activity [fast wave] as well as by slowing of
the dominant [EEG] frequency.
These changes are indicative of deficits
in the vigilance regulatory systems, [which includes the LC neurons]. By the term
vigilance we [mean] the... dynamic state of total neural activity... Elderly subjects
with bad memory exhibit slower [EEG] activity and less alpha and alpha-adjacent
beta activity than those with good memory... Antihypoxidotic/ nootropic drugs
such as... vincamine-alkaloids [VCM and VPC] induce interestingly just oppositional
changes [to the age related slowing of EEG waves] in human brain function, thereby
improving vigilance." (13)
Vinpocetine's side effects
VPC thus possesses a unique profile; Potent metabolic enhancer; selective (non
"steal effect") cerebral blood flow enhancer; neural oxygenator; anti-platelet
aggregation blood thinner; locus coeruleus activator; EEG normalizing vigilance
enhancer. And yet human and animal studies consistently show a remarkable safety
profile and freedom from side effects. Thus, in a study on VPC's ability to improve
sensorineural hearing disorders, Ribari and colleagues note that "The drug
[VPC] has no side effects." (14)
In their extremely detailed examination
of VPC use in 100 patients with neuro-vascular diseases Szobor and Klein report
that "Laboratory tests, urinalysis, blood picture, blood sugar, liver function,
SGOT, SGPT, CN, electrolytes, cholesterol and total [lipids] did not change...
The glucose tolerance did not deteriorate in the diabetic patients." (4)
In a highly successful double-blind placebo study of VPC with 84 elderly
patients suffering from chronic vascular senile brain dysfunction, Balestreri
et al, found only 12 adverse effect reports in the VPC group (mostly digestive
complaints) versus 17 in the placebo group! No significant adverse laboratory
findings were found in either group (15). A major Japanese study by Otomo and
colleagues with 207 patients suffering various cerebral disorders found only a
2% incidence of mild adverse side effects- anorexia in 2 patients, hives and stomach
pain in 1 and hot flashes in 1. No significant adverse laboratory findings occurred
in the 207 VPC patients (16).
In their summary of various animal safety
tests, Cholnoky and Domok found the oral LD50 for VPC (the dose lethal for 50%
of the test animals) to be 534mg/ Kg of bodyweight for mice, 503 mg/Kg of bodyweight
for rats.
This would equate to approximately 35,000mg for a 150 pound human.
The usual therapeutic dose for VPC for humans is 15-30mg per day!
Because
of side effects at high doses when used with pregnant rats (uterine bleeding in
some), Cholnoky and Domok caution against using VPC in pregnant women, or those
trying or expecting to get pregnant (17).
Overall, VPC side effects reported
in the literature are rare, usually minor, frequently disappear with prolonged
use, and rarely require discontinuance of the drug. Stomach/ GI upset; dry mouth,
rapid heart beat, low blood pressure, and rash/ hives are the main (rarely occurring)
reported side effects.
Who might benefit from Vinpocetine?
1. Anyone over 40, cerebral arteriosclerosis is less well known to the public
than heart disease, but it is just as common, and develops gradually over a lifetime.
By the time serious symptoms develop, as with heart disease, the blood vessel
occlusion is usually well advanced. VPC can minimize the structural/ functional
damage to brain neurons that may accompany gradually developing cerebral arteriosclerosis.
2. Anyone who has noticed a decrease in memory, alertness, concentration,
learning speed/ ability, neuro-muscular co-ordination and reaction time, vision,
hearing, or who suffers from tinnitus.
3. Anyone who suffers from, or
is known to be at risk for, various cerebral disorders- cerebral hemorrhage, stroke,
senile dementia, transient ischaemic attacks, chronic cerebral circulatory insufficiency,
etc.
4. Anyone wishing to use a generally very safe, low side effect,
brain metabolism enhancing, vigilance enhancing, cognition activating "smart
drug."
Vinpocetine's doses and uses
VPC is normally taken
orally, 5-10mg, two or three times daily. Some people report feeling "over-revved"
from higher/ more frequent dosing, and report as little as 2.5mg once or twice
daily to be useful but not over-stimulating. Mild and transient nausea, though
rare, is more likely to occur when VPC is taken on an empty stomach.
Sublingually VPC may allow lower dose (2.5mg) use, with quicker and sometimes
more noticeable effect.
While VPC may need to be used for weeks or months
before seeing major improvement in medical situations, the cognitive enhancement
benefits may be noticeable from even a single dose, or within the first several
days' use. Improvements in cerebral disorders and in hearing and vision problems
may last only as long as the drug continues to be taken.
Because VPC
enhances cerebral blood flow, it may potentate other nootropic/ cerebro-active
drugs taken simultaneously, thus allowing/ requiring then to be taken in lower
doses.
References
(1). B. Vamosi et al (1976)
"Comparative study of the effect of Ethyl Apovincaminate and Xanthinol Nicotinate
in cerebrovascular diseases" Arzneim Forsch (drug research) 28, 1980-84.
Hereafter abbreviated "AF (DR)")
(2). F. Solti et al (1976) "Effect
of Ethyl Apovincaminate on the cerebral circulation" AF(DR) 28, 1945-47.
(3).E. Karpaty & L. Szporny (1976) "General and cerebral harmodynamic
activity of Ethyl Apovincaminate" AF(DR)28, 1908-12.
(4). A. Szobor and
M. Klein (1976) "Ethyl Apovincaminate therapy in neurovascular disease"
AF(DR) 28, 1984-89.
(5). D. Sauer et al (1988) "Vinpocetine prevents
ischaemic cell damage in rat hippocampus" Life Sci. 43, 1733-39.
(6).
R. Branconnier (1983) "The efficacy of the cerebral metabolic enhancers in
the treatment of senile dementia." Psychopharm Bull 19, 212-19.
(7).
A. Hoffer & M. Walker, Smart Nutrients, Garden City Park, NY: Avery, 1994.
(8). C. Nicholson (1990) "Pharmacology of nootropics and metabolically active
compounds in relation to their use in dementia." Psychopharm 101, 147-59.
(9). K. Biro et al (1976) "protective activity of Ethyl Apovincaminate on
ischaemic anoxia of the brain" AF(DR)28, 1918-20.
(10). D. Hadjiev &
S. Yancheva (1976) "Rheoencephalographic and psychological studies with Ethyl
Apovincaminate in cerebral vascular insufficiency" AF(DR)28, 1947-50.
(11). A. Kaham & M. Olah (1976) "Use of Ethyl Apovincaminate in ophthalmological
therapy" AF(DR)28, 1969-72.
(12). H. Olpe et al (1985) "Locus Coeruleus
as a target for psychogeriatric agents" Ann NY Acad Sci 444, 399-405.
(13). B. Saletu & J. Grunberger (1985) "Memory dysfunction and vigilance;
neurophysiological and psychopharmacological aspects" Ann NY Acad Sci 444,
406-27.
(14). O. Ribari et al (1976) "Ethyl Apovincaminate in the treatment
of sensorineuronal impairment of hearing" AF(DR)28, 1977-80.
(15). R.
Balestreri et al (1987) "A double blind placebo controlled evaluation of
the safety and efficacy of vinpocetine in the treatment of patients with chronic
vascular senile cerebral dysfunction." J. Am Geriatr Soc 35, 525-30.
(16). E. Otomo et al (1985) "Comparison of vinpocetine with Ifenprodil Tartrate
and Dihyroergotoxine Mesylate treatment and results of long term treatment with
vinpocetine." Curr Ther Res 37, 811-21.
(17). E. Cholnoky & L. Domok
(1976) "Summary of safety tests of Ethyl Apovincaminate" AF(DR)28, 1938-44.
DISCLAIMER: ALL INFORMATION IS EDUCATIONAL AND PROVIDED UNDER ETERNITY MEDICINE
TERMS AND CONDITIONS. IT DOES NOT, AND SHOULD NOT, REPLACE THE ADVICE OF YOUR
PHYSICIAN.
Last Updated: Wednesday, March 21, 2001
Vinpocetine
Home
Vinpocetine Ingredients
and Applications Purchase
Vinpocetine
 print
version FULL
SUMMARY ABOUT SELECT VINPOCETINE (PDF Format)
 |
Please
note that it is required that you have Acrobat Reader installed on your system
to view the above documents.
You can download the latest version by clicking
here. | 
|
