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Introduction
Androgenic Alopecia, an autosomally mediated
chronbiologic phenomenon, affects over 40 million men as well as
20 million women in America.1 To date, there has been no
safe, efficacious method of treating and/or reversing the
progression of this disorder without presenting known negative
side effects. There have been numerous proposed treatments
for baldness, but only a few have provided effective treatment
over a wide range of patients, and none have been based on
naturally occurring substances. Androgenic Alopecia (AGA) which
describes male pattern alopecia, is considered to be a genetically
based disorder 2 and commonly characterized by thinning and loss
of hair in affected individuals within a given pattern on the
scalp of the head. This disorder progresses by causing the
affected hair follicles to become smaller and correspondingly, the
hair becomes finer. Eventually, the fine hairs may be lost
and, thus, baldness results in the affected area. Hair has
been classified as being of at least two distinct types, terminal
and vellus.3 A vellus hair is short, fine, thin, and
non-pigmented, with the bulb of the hair follicle seated
superficially in the dermis of the scalp. Terminal hairs are
long, coarse and pigmented, with the bulb of the follicle seated
deep in the dermis. During the thinning stage of alopecia, the
hairs in the affected area are believed to transform from
terminal to vellus. It is this transformation to vellus hairs that
is equated to baldness. The core of the phenomenon is
associated with structural miniaturization.
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Background
Androgenic Alopecia (AGA)
as well as Benign Prostatic Hyperplasia (BPH) are believed
to result from a genetic predisposition associated with 5alpha
dihydrotestosterone4, which is a highly bio-active metabolite
of the androgenic hormone testosterone. Although these disorders
are vastly different in physiology and presentation, the etiology
of each stems from this specific hormonal metabolism. In
developing treatment for AGA, various hormones such as
estrogen and other anti androgens have been tested and found
unsuitable due to undesirable side effects6, such as feminization
of male subjects. Therefore, it would be desirable to find a
treatment for AGA that minimizes the use of bio-effecting
drugs. It would be expected that natural ingredients will be
biologically more friendly to the user and suitable for long term
use with minimal side effects.
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Mechanism of Action
A natural or organic
composition and method of treatment for Androgenic Alopecia (AGA)
to reduce or arrest the abnormal hair loss. More specifically,
revitalize existing hair by interfering with the mechanism that
causes thinning, and thus may act to reverse the process. The
preferred formulation employs beta sitosterol, saw palmetto berry
extract, lecithin, inositol, phosphatidyl choline, niacin, and
biotin in orally administered dosages. The method of
treatment is administering a dosage of the stated
ingredients. In one embodiment, the dosages may be combined in a
single soft gel capsule. The preferred quantities of each
are shown in the following Table 1:
|
CAPSULE DOSAGE
|
|
INGREDIENT
|
DOSAGE
|
|
|
|
Beta Sitosterol
|
50 mg
|
|
Saw Palmetto Berry Extract
(Standardized 85% to 95% liposterolic content)
|
200 mg
|
|
Lecithin
|
50 mg
|
|
Inositol
|
100 mg
|
|
Phophatidyl Choline
|
25 mg
|
|
Niacin
|
15 mg
|
|
Biotin
|
100 mcg
|
The preferred dosage is stated with respect to cholestatin 45%
beta sitosterol. A dosage from 40 mg to 60 mg each twelve hours
has been found most effective. According to the capsule
formulation of Table 1, a gel capsule containing 50 mg of
beta sitosterol is taken twice per day such as each morning and
evening. The preferred dosage is stated with respect to an
extract of standardized 85 % to 95% liposterolic content. A
dosage of from 160 mg to 240 mg each twelve hours has been found
most effective. According to the capsule formulation of Table 1, a
gel capsule containing 200 mg of standardized saw palmetto extract
is taken twice per day such as each morning and each evening. .
According to another aspect, the invention provides a means for
emulsifying beta sitosterol and saw palmetto extract, or an
emulsifier system component that aids the other components
in penetrating the stomach lining. A suitable emulsifier is
lecithin, inositol, or preferably a mixture of both. The preferred
dosage of Table I is stated with respect to lecithin consisting
of 61-64% phosphatides, for which the dosage is 50 mg each twelve
hours. The preferred dosage of inositol is 100 mg each twelve
hours. These emulsifier system components can be varied in dosage
by a large factor without harm or toxicity.
As means of protecting follicles from degeneration due to
oxidation, free radicals and metabolic by-products, the
treatment provides and antioxidant component such as phosphatidyl
choline. An orally administered dosage of 25 mg per twelve
hours provides a general antioxidant prophylactic effect
throughout the body.
A vasodilator component is also provided, wherein preferred
elements are niacin, biotin, and preferably both. Niacin, or
vitamin B3, generally promotes circulation and is beneficial
in maintaining and promoting circulation to the follicles.
D-Biotin, or vitamin H, compliments the effects of niacin.
These dosages are approximate and may be varied by a large factor
such as 50% or more.
The shell of a gel capsule may be formed of gelatin, glycerin,
water, titanium dioxide, and such other pigments as may be
desired. The preferred dosage of Table I provides a suitable
quantity of each ingredient for treatment at twelve hour
intervals.
In the dosages and treatments, beta sitosterol and saw palmetto
berry extract are considered the active ingredients. Their
disclosed dosage is suitable for achieving effective
treatment with intermittent administration approximately at
twelve hour intervals. The remaining components are administered
in a mixture with the active ingredients for internal
administration and may be considered supplemental to enhance the
action of the active ingredients.
The formulation is believed to function on a molecular level via
competitive mechanical inhibition of the T1 and T2 5alphaDHT
cellular and nuclear androgen receptor sites found within
susceptible scalp hair follicles. Unbound 5alphaDHT is thus
metabolized out of the body via primary excretion pathways
without triggering the secondary and pathological cascade of
events associated with this disorder.
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Study Overview
The goal of this follow up study is to compile
additional research data in order to either challenge or
corroborate data previously gathered within the clinical
research study titled "NON-RANDOMIZED UNCONTROLLED CLINICAL
STUDY TO DETERMINE THE EFFICACY OF A NEW TREATMENT FOR ANDROGENIC
ALOPECIA (AGA)" 5/97 through 2/98. Statistical analysis to be
determined by gross clinical evaluation, patient reporting, and
baseline, intra-study, and end point photographic evidence.
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Treatment Protocol
Orally, 1 softgel b.i.d. (twice a day). participants to be
followed over the course of six months time period. Participants
to report to clinic one time per month during this period for
follow up investigator evaluation.
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Adverse Events
Any participant adverse
event reported during this study to be fully documented per
standard protocol parameters.
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Inclusion Parameters
Males and females between the ages of 18 and 65 who are
experiencing Androgenic Alopecia as determined by the
Hamilton/Norwood Class Scale, via investigator evaluation.
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Exclusion Parameters
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Participants with undetermined
reason for hairloss
-
Participants using other
medications on the scalp
-
Participants with no family
history of hair loss
-
Participants with red, inflamed,
infected, irritated or painful scalp
-
Participants who participated in
the initial study
-
Participants who have been
diagnosed with alopecia aereota, lupus, erythematosus,
or other non-male pattern alopecia.
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Clinical Impression Legend
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S=SUBJECTIVE
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S-1
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Follow
up evaluation
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S-2
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Other
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O=OBJECTIVE
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0-*
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Unable
to determine benefit
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0-1
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Hairloss
continuing, no benefit
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0-2
|
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Hairloss
arrested, no further loss
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0-3
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Hairloss
reversed, noticeable thickening
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|
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0-4
|
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Dramatic
thickening **
|
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P=PLAN
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P-1
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Continuing
treatment
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P-2
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Discontinuing
treatment
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|
P-3
|
|
Modifying
treatment
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Evaluation Analysis
(see accompanying statistics)
Incidence and degree of side effects, If any:
0% of participants reported drug interaction or side effects.
Incidence and degree of adverse events, If any:
0% of participants reported any adverse events.
Reduction in rate of hairloss, If any:
100% of participants reported hairloss arrested, no further loss.
Aesthetically meaningful change In caliber of affected scalp
hair, If any, as evidenced by clinical photography, patient
reporting and Investigator clinical Impression:
33% of participants reported hair loss reversed, noticeable
thickening via continued treatment.
Dramatic thickening reported:
7% of participants reported dramatic thickening.
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Study Synopsis
This follow up research
study comprising a six month time period of treatment did not
reveal any side effects, drug interactions or adverse
events. Based on the data gathered, all participants (100%) in
this study reported an arresting of syptomotology commonly
associated with Androgenic Alopecia and 33% reported an
aesthetically meaningful change in the caliber of the
affected scalp hair. These findings were determined via
investigator observation, baseline, intra study, and endpoint
photographic evidence, as well as patient reporting. This
study reinforces the effacious and safe nature of this treatment
methodology suggested by the initial study titled
"NON-RANDOMIZED UNCONTROLLED CLINICAL STUDY TO DETERMINE THE
EFFICACY OF A NEW TREATMENT FOR ANDROGENIC ALOPECIA (AGA)"
5/97 through 2/98. It is contemplated that independent and
controlled study of this treatment formulation would be an
appropriate next step in the ongoing evaluation of it's potential
benefit.
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Exhibit A: Clinical Study Statistics
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Exhibit B: Before and After Photos
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Exhibit C: Before and After Photos
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Exhibit D: Norwood Scale
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References
The Bald Truth, Fischer, David, US News and World Report,
v123n5, pp 44-50 August 4, 1997
His Health: The Buzz on Baldness, Leaf, Clifton, American
Health vl5, n9 November, 1996 pp 34-35
HAIR! From personal Statement to Personal Problem, Pine, Devera,
FDA Consumer, December 1991 25(10): pp 20-23
Management of Alopecia, Source: UTMB Dept of Otolaryngology
Grand Rounds Presentation, September 9, 1998. Facility: Karen
Calhoun, MD Resident: Kyle Kennedy, MD
Alopecia, (Baldness), Source: UTMB Dept of Otolaryngology Grand
Rounds, April 30, 1997, Resident Physician: Chris
Thompson, MD, Faculty: Karen Calhoun, MD, FACS, Series Editor:
Francis B. Quinn, Jr., MD, FACS
Management of Alopecia, Source: UTMB Dept of Otolaryngology
Grand Rounds Presentation, September 9, 1998. Facility: Karen
Calhoun, MD Resident: Kyle Kennedy, MD
The Bald Truth, Fischer, David, US News and World Report,
v123n5, pp 44-50 August 4, 1997
Management of Alopecia, Source: UTMB Dept of Otolaryngology
Grand Rounds Presentation, September 9, 1998. Facility: Karen
Calhoun, MD Resident: Kyle Kennedy, MD
Estrogen-induced gynecomastia following use of
estrogen-containing local agents. Schmidt KU: Wagner G;
Mensing H, Dtsch Med Wochenschr, 112: 23, 1987 Jun 5, 9268
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