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Published
in The Townsend Magazine for Doctor's & Patients
Decrease
Cirrhosis of the Liver
By Extreme Health and Dr. C. Cochran
Artichoke
Bud / Sarsaparilla Root Extract (ASE)
This extremely effective combination of ingredients has Double Blind
Studies to verify the decreases in degenerative liver damage in
patients with chronic liver disease (cirrhosis of the liver) in
as few as 30 to 90 days. This combination has proven studies for
detoxifying the liver normalizing liver metabolism and preventing
further liver damage due to internal and external toxins like alcohol
cigarettes and environmental poisons
DESCRIPTION
The artichoke bud / sarsaparilla extract is an entirely unique complex
of phytochemicals extracted from the bud of a hybrid artichoke plant
(Cynara floridanum) and the root of the sarsaparilla plant (Smilax
officinalis).
The proprietary extraction process uses a method in which all plant
materials are first combined macerated and put into a distilled
water / ethanol solvent. This allows the plant materials to interact
within the solvent resulting in an exceptional health-providing
formulation of polyphenols and flavonoids.
FEATURES
· ASE is a complex of liver-supportive detoxifying phytonutrients
that are extracted using a proprietary two-step method. It is unlike
anything in the marketplace today. Partial analysis has revealed
a quite extraordinary complex of flavonoids including quercetin
rutin - (+) catechin hesperidin kaempferol isorhamnetin cynarin
silymarin caffeic acid and chlorogenic acid. Phytosterols including
ß-sitosterol campesterol and stigmasterol have also been
detected.
· ASE has been created by combining materials from two plants
that have been historically used as liver regenerative detoxifying
and blood-purifying agents.
BENEFITS
· ASE has been used to normalize liver and gall bladder function
in clinical settings for over 20 years.
· ASE is well tolerated and completely safe with no known
side effects. Contraindications include allergies to artichoke or
sarsaparilla and biliary duct obstruction such as with gallstones.
· ASE functions as a gentle detoxifier; digestive aid; and
a liver gall bladder and bowel normalizer.
PHYSIOLOGY
· Extracts of artichoke leaf have been found to stimulate
bile production in the liver and bile release from the gall bladder
and thus found effective in helping to eliminate toxic substances
normalizing blood cholesterol levels lowering blood lipids and
providing liver protective qualities.
· The root of the sarsaparilla plant is considered by European
physicians to be an alterative tonic blood purifier diuretic (increases
urine output) and diaphoretic (increases perspiration).
CLINICAL
INDICATIONS
· Inhabit or work in toxic environments
· Abnormal liver enzymes or history of liver disease including
alcoholic liver disease
· For those who smoke drink alcoholic beverages or take
drugs
· Abnormal blood lipids (cholesterol and triglycerides)
· Digestive or bowel disorders very effective for irritable
bowel syndrome
· Those with surgically removed gall bladders (cholecystectomy)
· Hepatitis patients
· Overweight patients and during weight loss programs
· Skin disorders including psoriasis and adult onset acne
1st
Double Blind Study
INTERPRETATION
OF RESULTS OBTAINED IN A DOUBLE BLIND TEST
MADE IN THE GENERAL HOSPITAL MEXICO WITH
THE PRODUCT LIVER SUPPORT ON PATIENTS HAVING
CHRONIC ALCOHOLIC HEPATIC DISEASE.
In order to analyze carefully the results
of this study it is necessary to know the
importance of the two clinical and laboratory
parameters intervening in the calculations
of Orrego and Maddrey Indexes.
We
will compare the results of the parameters the placebo control
and the Liver Support groups on both indexes. The results are presented
as percentages of recovery and are obtained from the data obtained
from each group of 30 patients we will get an average of those
results at the beginning and at the end of the study. Both averages
will give us a final recovery compared to the initial values. This
way we may demonstrate the effectiveness of Liver Support.
DEFINTIONS
AND RESULTS OF PARAMETERS
ASCITES-
Effusion and accumulation of serous fluid
in the abdominal cavity. experimental group
(Liver Support) experienced a 28.8% reduction
of ascites while the placebo group experienced
no change The.
ENCEPHALOPATHY-
a DEGENERATIVE DISEASE OF THE BRAIN.
Hepatic encephalopathy- a condition usually
occurring secondarily to advanced disease
of the liver. It is marked by disturbances
of consciousness that may progress to deep
coma (hepatic coma) psychiatric changes
of varying degree flapping tremor and fetor
hepaticas. Also called portal-systemic encephalopathy.
Patients on Liver Support experienced a
34.55% reduction of hepatic encephalopathy.
The placebo group experienced a 5.5% reduction.
SPLENOMEGALIA-
Enlargement of the spleen. An 18.18% reduction
was observed in the Liver Support group
and a 55% reduction was observed in the
placebo group.
WEAKNESS-
Lacking physical strength or vigor marked
by asthenia atony cardiasthena enervation
fatigue and lassitude. The Liver Support
group experienced an 83.45% decrease in
the incidence of weakness while the placebo
group reported no change.
PERIPHERAL
EDEMA- A condition in which the
body tissues contain an excess amount of
fluid. The Liver Support Group experienced
an 11.10% reduction in peripheral edema
while the placebo group had a 0.69% reduction.
HEMORRHAGES-
Bleeding. This was one of the most important
benefits observed in the Liver Support group.
The Liver Support group had an 89.41% reduction
in hemorrhages while the placebo had a 31%
reduction.
ANOREXIA-
Loss of appetite. Seen in depression malaise
commencement of fevers and illness also
in disorders of the alimentary tract especially
of the stomach and as a result of alcoholic
excess and drug addiction. Anorexia was
diminished by 86.07% in the Liver Support
group. There was no change in the placebo
group.
TOTAL
BILIRUBIN LEVEL - The predominant
pigment of human bile. Total serum bilirubin
may be increased in cirrhosis of the liver
and acute viral hepatitis. The Liver Support
group obtained 25.11% reduction in bilirubin
whereas the placebo group had a 7.2% increase.
OGT
- (Oxalacetic Glutamic Transaminase). It
is distributed all over body tissue especially
in the heart and liver. Fewer amounts are
found in the spleen pancreas kidneys lungs
and brain. Any lesion of a tissue leads
to the secretion of this enzyme to the blood
stream. The activity of OGT is risen under
hepatic necrosis cirrhosis of the liver
or hepatic metastasis. In those patients
who received Liver Support this level diminished
22.56% in only 15 days of treatment and
in the placebo group it diminished 8.51%.
PROTHROMBINE
TIME - A test of clotting time
made by determining the time for clotting
to occur after thromboplastin and calcium
are added to decalcified plasma. There was
30.82% reduction in prothrombin time for
Liver Support patients whereas the placebo
group's time increased 1.25%. This is very
important data because it means that Liver
Support helps the healing of wounds faster.
SERUM
ALBUMIN - One of a group of simple
proteins widely distributed in tissues.
Albumin is a constituent of blood. Low levels
of albumin in blood plasma are associated
with a pathologic condition of the liver.
The Liver Support group experienced an increase
of 8.85% of total albumin levels while the
placebo group experienced a 5.35% increase.
2nd
Double Blind Study
COMPARATIVE
STUDY BETWEEN A COMPLEX OF FLAVONOIDS AND
POLYPHENOLS CREATED FROM EXTRACTS OF ARTICHOKE
AND SARSAPRILLA AND A PLACEBO IN ALCOHOL
RELATED LIVER DISEASE
DECEMBER
12 1998
In
a previous study completed over two years ago in this same hospital
an extract of artichoke (Cynara Floridanum) and sarsaparilla (Smilax
Aristolochiaefolia) was evaluated in addressing the symptoms related
to alcoholic liver disease. This study was accomplished over a fifteen-day
period with exceptional results. Because of these results noted
over a very short period of time the hospital researchers were
anxious to set up the same study over a longer period (30 days).
Please refer to the July 3 1996 study for descriptions of symptoms
and study parameters. Results of this study are as follows:
ASCITES
A 72.38% reduction of the accumulation of serous abdominal fluid
was noted in the treated group. The placebo saw a 6.35% increase
in abdominal fluid.
ENCEPHALOPATHY
A 66.08% reduction of symptoms related to encephalopathy was noted
in the treated group. The placebo group saw a 12.24% increase in
these symptoms.
HEPATOMEGALY
The treated group experienced a 93.33% reduction in enlarged livers.
In the placebo group their livers continued to enlarge by another
7.14%.
SPLENOMEGALY
An 88.40% reduction in spleen enlargement was noted with the treated
group. The placebo group worsened by 11.54%.
WEAKNESS
The treated group noted a 73.64% increase in strength. There was
a decrease in muscle strength by 7.41% in the placebo group.
PERIPHERAL
EDEMA
Edema in the extremities of the treated patients decreased by 48.21%.
There was no change in the placebo group.
HEMORRHAGES
The treated group noted a 100% decrease in capillary hemorrhaging
in the skin gums and nasal membranes. The placebo group saw an
increase of 28.57% in hemorrhaging.
ANOREXIA
Loss of appetite decreased in the treated group by 76.98%. The placebo
group noted a decrease of 3.70%.
ABDOMINAL
WALL VEINS
The treated group experienced a 60.62% decrease in tortuous veins
in the abdomen related to ascites. The placebo group saw a 3.33%
decrease.
PALMAR
ERYTHEMA
The treated group noted a 26.67% decrease in red and swollen palms.
In the placebo group there was no change.
TELANGIECTASIA
A 60.00% reduction in vascular lesions was noted in the treated
group. A 3.33%
reduction was seen in the placebo group.
TOTAL
BILIRUBIN
The treated group noted a reduction of total bilirubin by 38.95%.
The placebo group increased by 5.68%.
ALKALINE
PHOSPHATASE
The treated group obtained 25.91% reduction in alkaline phosphates.
There was an 11.69% increase in the placebo group.
SERUM
GLUTAMIC OXALCETIC TRANSAMINASE (SGOT)
The treated group noted a decrease of 23.83% in SGOT levels. The
placebo group experienced a worsening of 11.71%.
PROTHROMBIN
TIME
A 42.00% reduction in clotting time was noted with the treated group.
An increase in clotting time was noted in the placebo group of 6.60%.
SERUM
ALBUMIN
An increase of 37.27% in serum albumin was noted in the treated
group. There was a decrease in the placebo group of 1.95%.
GAMMA
GLUTAMYL TRANSPEPTIDASE (GGT)
The treated group noted a reduction of 23.79% in GGT. The placebo
group experienced an increase of 9.92%.
DR. CHARLES COCHRAN
SCIENTIFIC
RESEARCH
Beneficial effects of flavonoids have been described for successfully
treating many health conditions including cancer viral infections
diabetes headaches liver disease ulcers and allergies. They
can also bind to enzymes and DNA chelate heavy metals and play
a role in electron transport.
Van Acker S. et al; Structural Aspects of Antioxidant Activity
of Flavonoids Flavonoids in Health and Disease Rice-Evans C.
editor Marcel Dekker Inc. 1998.
It
is highly unlikely that the therapeutic value of medicinal plants
is due to either one flavonoid or an entire flavonoid fraction alone.
Packer Lester et al; Ginkgo biloba Extract Egb 761; Biological
Actions Antioxidant Activity and Regulation of Nitric Oxide Synthase
Flavonoids in Health and Disease Rice-Evans C. editor Marcel Dekker
Inc. 1998.
Phytosterols
are plant fats. Plants do not contain cholesterol but phytosterols
play a similar role in plants to that of cholesterol in humans
primarily the forming of cell membrane structures sources of fuel
for storage and transport and protective surface coatings. The
most common plant sterols are ß-sitosterol campesterol and
stigmasterol. Recent studies have shown that phytosterols have antihyperglycemic
and insulin-releasing effects anti-inflammatory and antipyretic
activities and important immune regulating and T-cell proliferative
activities.
Ivorra MD et al; Antihyperglycemic and Insulin-releasing Effects
of ß-sitosterol 3-B-glucoside and Its Aglycone ß-sitosterol
Archives of the International Phamnacodyn V. 296 April 1988 224-231.
Gupta R. et al; Anti-inflammatory and Antipyretic Activities of
ß-sitosterol Planta Medica (Journal of Plant Medicine) V.
39 1980 157-163.
Pegel Karl The Importance of Sitosterol and Sitosterolin in Human
and Animal Nutrition South African Journal of Science V. 93 June
1997 263-268.
Extracts
of the artichoke leaf stimulates bile production in the liver and
increased bile release from the gall bladder and thus has been
effective in helping to eliminate toxic substances normalizing
blood cholesterol levels lowering blood lipids and providing liver
protective qualities.
Adzet T et al; Hepatoprotective Activity of Polyphenolic Compounds
from Cynara Scolymnus Against CC14 Toxicity in Isolated Rat Hepatocytes
Journal of Natural Products 50: 612 1987.
Gebhart R; Inhibition of Cholesterol Biosynthesis in Primary Cultured
Rat Hepatocytes by Artichoke Extracts. J Pharmacol Exp Ther 286;
3 1998.
Fintelmann V; Therapeutic Profile and Mechanism of Action of Artichoke
Leaf Extract; Hypolipemic Antioxidant Hepatoprotective and Choleretic
Properties. Phytomedicine 1996. Supplement 1:50.
Kirchoff R et al; Increase in Choleresis By Means of Artichoke
Extract. Results of a Randomized Placebo-controlled Double-blind
study. Phytomedicine 1: 107 1994.
European
physicians consider sarsaparilla root as
an alterative tonic blood purifier diuretic
and diaphoretic. With its clinical uses
as a blood purifier it was registered as
an official herb in the U.S. Pharmacopoeia
as a treatment for syphilis from 1820 to
1910. Clinical observations in China demonstrated
that sarsaparilla is effective in about
90% of acute cases and 50% of chronic cases
of syphilis. In 1942 it was shown to dramatically
improve psoriasis and in the 1950's the
antibiotic properties of sarsaparilla were
documented.
An herbal Saudi Arabian drug created from
sarsaparilla has been used for many years
to treat rheumatism and various forms of
arthritis. Further studies showed that sarsaparilla
inhibited carrageenan-induced inflammation
in rats. Recent research from China has
shown that an extract of sarsaparilla was
able to prevent immunological liver damage.
And three studies performed between 1994
and 1999 have shown that extracts of sarsaparilla
have snake venom inhibitory activity.
Hobbs C; Sarsaparilla A Literature Review
HerbalGram No. 17 1988.
Lung A Foster S; Encyclopedia of Common
Natural Ingredients John Wiley & Sons
Inc. New York 1996.
Thurman FM; The Treatment of Psoriasis with
Sarsaparilla Compound New England Journal
of Medicine 337 128-133 1942.
D'Amico ML; Ricerche Sulla Presenza Di Sostanze
Ad Azione Antiiotica Nelle Piante Superiori
Fitoterapia 21(1) 77-79 1950.
Fitzpatrick FK; Plant Substances Active
Against Mycobacterium Tuberculosis Antibiotics
and Chemotherapy 4(5) 528-536 1954.
Ageel AM et al; Experimental Studies on
Antirheumatic Crude Drugs Used in Saudi
Traditional Medicine College of Pharmacy
Kind Daud University Riyadh Saudi Arabia
Drugs Exp Clin Res 1989 15(8): 369-372.
Chen T et al; A New Flavanone Isolated From
Rhizoma Smilacis Glabrae and the Structural
Requirements of Its Derivatives for Preventing
Immunological Hepatocyte Damage. Planta
Med 1999 Feb;65(1):56-59.
Alam MI et al; Isolation Purification and
Partial Characterization of Viper Venom
Inhibiting Factor from the Root Extract
of the Indian Medicinal Plant Sarsaparilla
Toxicon 1994 Dec;32(12): 1551-1557.
Castro O et al: Neutralization of the Hemorrhagic
Effect Induced by Bothrops Asper (Serpentes
Viperidae) Venom with Tropical Plant Extracts
Rev Biol Trop 1999 Sep: 47(3): 605-616.
COMPARISON
WITH OTHER NATURAL SUBSTANCES
Oftentimes ASE is compared with extracts of milk thistle alpha-lipoic
acid other artichoke extracts N-acetyl cysteine and nucleic acids
in its effectiveness to support liver detoxification and aid in
liver disease. Since no side-by-side studies have been performed
comparing these nutrients we cannot say that anyone of these natural
very valuable substances is better than the other. However clinically
we have found that by combing the ASE with any of the above-mentioned
nutrients results can be enhanced tremendously. Another very effective
common method is to alternate nutrients. This keeps the body from
developing sensitivities or desensitivities to any one nutrient
during prolonged treatments.
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