| United States Patent Application |
20050065159
|
| Kind Code
|
A1
|
|
Adams, Kenneth W.
|
March 24, 2005
|
Penis enlargement
Abstract
A method for causing a permanent increase in the length and girth of a
male subject's penis, the method comprising treatment comprising the step
of (a) administering to the male an effective amount of a vasodilator
selected from the group consisting of a vasodilator per se and
compositions thereof comprising a pharmaceutically-acceptable diluent or
carrier, to induce a cumulative prolonged engorgement of the subject's
penis; and (b) repeating step (a) as necessary to cause the increase
during the treatment. A potentiator which enhances the effect of the
vasodilator may also be used.
| Inventors: |
Adams, Kenneth W.; (North York, CA)
|
| Correspondence Name and Address:
|
MORGAN LEWIS & BOCKIUS LLP
1111 PENNSYLVANIA AVENUE NW
WASHINGTON
DC
20004
US
|
| Serial No.:
|
986027 |
| Series Code:
|
10
|
| Filed:
|
November 12, 2004 |
| U.S. Current Class: |
514/252.16 |
| U.S. Class at Publication: |
514/252.16 |
| Intern'l Class: |
A61K 031/519 |
Foreign Application Data
| Date | Code | Application Number |
|---|
| Jul 25, 2003 | WO | PCT/CA03/01139 |
Claims
1. A method for causing a permanent increase in the length and girth of a
male subject's penis, said method comprising treatment comprising the
step of (a) administering to said male an effective amount of a
vasodilator selected from the group consisting of a vasodilator p se and
compositions thereof comprising a pharmaceutically-acceptable diluent or
carrier, to induce a cumulative prolonged engorgement of the subject's
penis; and (b) repeating step (a) as necessary to cause said increase
during said treatment.
2. A method as defined in claim 1, wherein said vasodilator is in
admixture with a pharmaceutically-acceptable diluent or carrier.
3. A method as defined in claim 1, wherein said administration is such
that said prolonged engorgement is sustained for at least 3.5 hours.
4. A method as defined in claim 3, wherein said prolonged engorgement is
sustained for at least 4 hours.
5. A method as defined in claim 1, wherein said vasodilator is
administered as one dose in said treatment step throughout the prolonged
engorgement.
6. A method as defined in claim 1, wherein said vasodilator is
administered as at least two doses as defined in said treatment
throughout the prolonged engorgement.
7. A method as defined in claim 6, wherein the engorgement comprises a
first erectile response of at least 65%, and a second dose or subsequent
doses are administered after the first erectile response falls below 65%
during said treatment.
8. A method as defined in claim 5 or claim 6, wherein said treatment is
applied to said patient at least two times per week for a period of at
least one month.
9. A method as defined in claim 8, wherein said treatment is applied to
said patient at least four times per week for a period of at least 3
months.
10. A method as defined in claim 1, wherein the length of the fully erect
penis has increased by at least 5% after a treatment period of 12 to 18
months.
11. A method as defined in claim 10, wherein the length of the fully erect
penis is increased by at least 30% after a treatment period of 12 to 18
months.
12. A method as defined in claim 1, wherein the girth of the fully erect
penis is increased by at least 5% after a treatment period of 12 to 18
months.
13. A method as defined in claim 12, wherein the girth of the fully erect
penis is increased by at least 30% after a treatment period of 12 to 18
months.
14. A method as defined in claim 1, wherein said engorgement comprises a
75-100% erectile response for at least 90% of the time of the prolonged
engorgement.
15. A method as defined in claim 1, wherein said engorgement comprises a
75-100% erectile response for 50-90% of the time of the prolonged
engorgement.
16. A method as defined in claim 1, wherein said engorgement comprises a
75-100% erectile response for up to 50% of the time of the prolonged
engorgement.
17. A method as defined in claim 1, wherein said engorgement comprises a
40-75% erectile response for at least 3 hours.
18. A method as defined in claim 1, wherein said vasodilator is selected
from the group consisting of nitrovasodilators, ACE inhibitors,
angiotensin receptor antagonists, phosphodiesterase inhibitors, direct
vasodilators, adrenergic receptor antagonists, calcium channel blocking
drugs, alpha blockers, beta blockers, lymphthomimetics, vitamins, organic
nitrates, serotonin receptor-blocking agents, angina blocking agents,
other hypertensive agents, cardiac stimulating agents, agents which
improve renal, vascular function, sympathomimetic amine, and salts,
derivatives precursors, pharmaceutically active sequences or regions,
peptidomimetics, mimetics, and mixtures thereof.
19. A method as defined in claim 18, wherein said vasodilator is selected
from the group consisting of papaverine, chlorpromazine, atropine,
phentolamine, and prostaglandin E1, or a mixture thereof.
20. A method as defined in claim 19, wherein said vasodilator is
prostaglandin E1.
21. A method as defined in claim 1, wherein said vasodilator is formulated
for administration by direct injection to the cavernosal tissue, by
needle, auto-injector, slow sustained injection pump, high pressure
injection device, microinfusion pump, urethral suppository, or
implantable sustained release drug or device.
22. A method as defined in claim 1, wherein said vasodilator is formulated
for systemic administration by oral, sublingual, or suppository
administration, intravenous administration by needle, auto-injector, slow
sustained injection pump, high pressure injection device, microinfusion
pump, or implantable sustained release drug or device, or topical
administration, such as through the use of creams, lotions or patches.
23. A method as defined in claim 1, wherein said vasodilator is
administered to the dense connective tissue surrounding the erectile
tissue of the penis by a deep injection that goes below the dermis and
subcutaneous tissues.
24. A method as defined in claim 1, wherein said vasodilator is
administered to the dorsal suspensory ligand of the penis.
25. A method as defined in claim 1, wherein said vasodilator is
administered as an intracavernosal injection.
26. A method as defined in claim 21, wherein said vasodilator is
administered as an implantable sustained release drug or device.
27. A method as defined in claim 20, wherein said prostaglandin E1 is
administered at a dosage of 0.5 to 100 micrograms/kg body weight/day by
intracavernosal injection.
28. A method as defined in claim 20, wherein the prostaglandin E1 is
administered systemically at a dosage of 2 to 10,000 micrograms/kg body
weight/day by an implantable sustained release drug or device.
29. A method as defined in claim 1 further comprising administration of a
potentiator which potentiates the effect of the vasodilator.
30. A method as defined in claim 29, wherein the potentiator is
administered by direct injection to the cavernosal tissue, by needle,
auto-injector, slow sustained injection pump, high pressure injection
device, microinfusion pump, urethral suppository, or implantable
sustained release drug or device.
31. A method as defined in claim 29, wherein the potentiator is
systemically administered by oral, sublingual, or suppository
administration, intravenous administration by needle, auto-injector, slow
sustained injection pump, high pressure injection device, microinfusion
pump, or implantable sustained release drug or device, or topical
administration, such as through the use of creams, lotions or patches.
32. A method as defined in claim 29, wherein the potentiator is
administered to the dense connective tissue surrounding the erectile
tissue of the penis by a deep injection that is well below the dermis and
subcutaneous tissues.
33. A method as defined in claim 29, wherein the potentiator is
administered to the dorsal suspensory ligand of the penis.
34. A method as defined in claim 29, wherein the potentiator is
administered by intracavernosal injection.
35. A method as defined in claim 29, wherein the potentiator is
administered as an implantable sustained release drug or device.
36. A method as defined in claim 29, wherein the potentiator is
administered separately from the composition.
37. A method as defined in claim 29, wherein the potentiator is
administered concurrently with the composition.
38. A method as defined in claim 29, wherein the potentiator is
administered more than once during said treatment.
39. A method as defined in claim 29 wherein the potentiator is a hormone.
40. A method as defined in claim 39, wherein the hormone is an androgen
selected from the group consisting of the naturally occurring androgens
and derivatives thereof, or an agent that will stimulate the androgen
receptor directly or indirectly, including androsterone, androsterone
acetate, androsterone propionate, androsterone benzoate, androstenediol,
androstenediol-3-acetate, androstenediol-17-acetate,
androstenediol-3,17-diacetate, androstenediol-17-benzoate,
androstenediol-3-acetate-17-benzoate, androstenedione,
dehydroepiandrosterone (DHEA; also termed "prasterone"), sodium
dehydroepiandrosterone sulfate, 4-dihydrotestosterone (DHT; also termed
"stanolone"), 17.beta.-hydroxyandrost-4-en-3-one, 5.alpha.-dihydrotestost-
erone, dromostanolone, dromostanolone propionate, ethylestrenol,
nandrolone phenpropionate, nandrolone decanoate, nandrolone
furylpropionate, nandrolone cyclohexanepropionate, nandrolone benzoate,
nandrolone cyclohexanecarboxylate, oxandrolone, stanozolol and
testosterone, pharmaceutically acceptable esters of testosterone and
4-dihydrotestosterone, including esters formed from the hydroxyl group
present at the C-17 position, including, but not limited to, the
enanthate, propionate, cypionate, phenylacetate, acetate, isobutyrate,
buciclate, cyclopentylpropionate, isocarponate, heptanoate, decanoate,
undecanoate, caprate and isocaprate esters, pharmaceutically acceptable
derivatives of testosterone such as methyl testosterone, testolactone,
oxymetholone and fluoxymesterone; synthetic androgens, and
7-Methyl-Nortestosterone ("MENT'") and its acetate ester, and salts,
derivatives, precursors, pharmaceutically active sequences or regions,
peptidomimetics, mimetics, and mixtures thereof.
41. A method as defined in claim 40, wherein the androgen is testosterone.
42. A method as defined in claim 40, wherein the androgen is
dihydrotestosterone.
43. A method as defined in claim 29, wherein the potentiator promotes the
elongation of collagen.
44. A method as defined in claim 29, wherein the potentiator inhibits
collagen cross-linkage.
45. A method as defined in claim 29, wherein the potentiator is selected
from a group consisting of relaxin, insulin like growth factor, growth
hormone, metallo-porteinases or metallo-proteinase agonists or promoters
of collagenase activity, tissue inhibitors of matrix metalloprotenases
(TIMPS) other agents that increase collagen solubility, prostaglandins,
corticosteroids, potassium aminobenzoate, and dimethyl sulfoxide (DMSO),
D-penicillamnine, and salts, derivatives, precursors, pharmaceutically
active sequences or regions, peptidomimetics, mimetics, and mixtures
thereof.
46. A method as defined in claim 45, wherein the potentiator is relaxin.
47. A method as defined in claim 45, wherein the prostaglandin is selected
from prostaglandin F2 alpha and prostaglandin E2.
48. A method as defined in claim 45, wherein the potentiator is relaxin,
prostaglandin F2 alpha, or prostaglandin E2, or the biochemical mediator
that results in the desired changes in collagen or the connective tissue
that produces and remodels collagen and express the effects of relaxin,
prostaglandin F2 alpha, or prostaglandin E2.
49. A method as defined in claim 45, wherein the potentiator is potassium
aminobenzoate.
50. A method as defined in claim 45, wherein the potentiator is dimethyl
sulfoxide (DMSO).
51. A method as defined in claim 45, wherein relaxin is administered at a
dosage of 0.02 to 1 micrograms/kg body weight/day by intracaversonal
injection.
52. A method as defined in claim 45, wherein relaxin is topically
administered at a dosage of 25 to 400 micrograms/kg body weight/day.
53. A method as defined in claim 45, wherein relaxin is administered at a
dosage of 0.02 to 1 micrograms/kg body weight/day by injection into the
dense connective tissue of the erectile tissue surrounding the penis.
54. A method as defined in claim 1, comprising applying a device to
prolong the retention of the composition in the penis.
55. A method as defined in claim 54, comprising fitting said device in the
form of a ring around the base of the penis.
56. A kit comprising a vasodilator per se or a composition thereof in
admixture with a pharmaceutically-acceptable diluent or carrier, and
instructions for administering said vasodilator to a human male according
to a method as defined in claim 1.
57. A kit as defined in claim 56, wherein the instructions are provided in
written form.
58. A kit as defined in claim 56 for use wherein the instructions are
provided orally by a health professional.
59. A kit as defined in claim 56, wherein the instructions are provided in
video compact disc form.
60. A kit as defined in claim 56, further comprising a potentiator for
enhancing the effect of the vasodilator.
61. A kit as defined in claim 57, further comprising a potentiator for
enhancing the effect of the vasodilator.
62. A kit as defined in claim 58, further comprising a potentiator for
enhancing the effect of the vasodilator.
63. A kit as defined in claim 59, further comprising a potentiator for
enhancing the effect of the vasodilator.
Description
RELATED APPLICATIONS
[0001] This application claims priority from U.S. application No.
60/398,562, filed Jul. 26, 2002, and PCT/CA2003/001139, filed Jul. 25,
2003.
FIELD OF INVENTION
[0002] This invention is in the field of penis enlargement.
BACKGROUND OF INVENTION
[0003] There are various circumstances under which a male subject may
desire the permanent enlargement of the length and/or girth of his penis,
in both its flaccid and erect states. Penis enlargement may be desired
for medical reasons, for example, if a patient is unable to penetrate
during coitus due to an unusually small penis size; for cosmetic reasons;
or to improve a person's self-esteem.
[0004] There have been many attempts to create a safe and effective means
for achieving permanent penis enlargement, including the use of external
weights and suction devices. The use of external weights is cumbersome
and impractical and produces localized compressive forces that may cause
localized ischemia. Furthermore, use of weights often leads to a thinning
of the penis and may even impair penis function.
[0005] Suction devices are also cumbersome and impractical to wear on a
prolonged basis, have limited effectiveness, and pose a number of risks.
Suction devices produce localized compressive forces that may cause
localized ischemia. Vacuum seals with pressure over 20 mm Hg can obstruct
capillary flow and inhibit tissue perfusion. Suction devices often come
with warnings that the devices should not be used for periods exceeding
20-30 minutes, which may be insufficient to achieve the desired result.
Use of suction devices can also result in the thickening of the skin and
accumulation of fluid in the superficial layers of the skin and
subdermis. The skin of the penis is hypermobile, and only very loosely
connected to deeper connective tissues and structures that comprise the
erectile tissues of the penis. The skin of the penis can readily separate
from the fibrous connective tissue capsule which encloses the erectile
tissue of the penis when externally applied suction forces are applied to
the penis.
[0006] Also, any suction forces applied to the penis will have a
proportionately larger effect on the skin, and the forces on the deeper
structures diminish dramatically. The increase in the surface area of the
skin causes the suction forces to be applied mainly to the skin, not to
the erectile tissue and the surrounding capsule of the cavernosal tissue.
As a result, the skin can be thickened as fluid is extravasated and there
is typically no, or only a limited enlargement, of the underlying
erectile tissues of the penis. Use of suction devices may also cause the
separation of the skin from the subdermis and the formation of seromas or
blisters on the penis. The application of suction devices to the penis
causes the extravasation of red blood cells out of the vascular spaces
and into the extracellular compartments. If vacuum devices are applied
for extended periods of time, this may lead to a significant pigmentation
of the penis. Applying a suction device repeatedly may cause the
deposition of large amounts of iron and other hemoglobin degradation
products in the tissue of the penis causing hemosiderosis, which
ultimately results in fibrosis. Furthermore, erectile dysfunction may
result from prolonged use of these devices.
SUMMARY OF THE INVENTION
[0007] In a first aspect, this invention provides a pharmaceutical
vasodilator which induces a cumulative prolonged engorgement of a human
penis, optionally as a composition together with a
pharmaceutically-acceptable diluent or carrier, for use in causing a
permanent increase in size of the human penis. As explained in greater
detail below, the permanent increase in size is achieved by repeated use
of the vasodilator or composition thereof, say, once a day for a few days
a week over many weeks, possibly many months.
[0008] In accordance with another aspect of this invention, there is
provided a method of enhancing penis size by administering said
vasodilator or composition thereof so as to induce a cumulative prolonged
engorgement of the penis. According to the method, such an administration
lasts for a limited time during one day, and is repeated up to daily or a
few days a week over a period of several weeks.
[0009] Thus, in one aspect the invention provides a method for causing a
permanent increase in the length and girth of a male subject's penis,
said method comprising treatment comprising the step of a (a)
administering to said patient an effective amount of a vasodilator
selected from the group consisting of a vasodilator per se and
compositions thereof comprising a pharmaceutically-acceptable diluent or
carrier, to induce a cumulative prolonged engorgement of the subject's
penis; and (b) repeating step (a) as necessary to cause said increase
during said treatment.
[0010] Preferably, the composition includes a pharmaceutically acceptable
diluent or carrier, which can aid in the administration of the
vasodilator of the composition for inducing a prolonged engorgement of a
human penis, for use in causing a permanent enlargement of the penis.
[0011] Although it is known in the prior art that vasodilators can be
administered to a male to induce engorgement of the penis, the prior art
is silent on the period of engorgement. In contrast, the present
invention provides for a prolonged period of engorgement as defined
herein. Further, in accordance with the practise of the present
invention, a permanent increase as defined herein is the primary object
of the invention.
[0012] The prior art is both silent on the hereindefined period of
engorgement and on the resulting permanent increase in penis size. In
contrast to the disclosure and teachings of the prior art, in the present
invention, engorgement of the penis is not the final desired result, nor
in isolation is the required period of engorgement. The present invention
defines the nature of the compound and its function, i.e. a vasodilator
of use in the present invention, and how it provides the solution of the
problem by administration thereof to provide the essential prolonged
engorgement feature to effect permanent increase in penis size, through
one or more administrative treatments.
[0013] This invention provides the use of pharmacological vasodilators to
cause a permanent increase in the length and girth of a human penis. As
used herein, the term "permanent increase" refers to a long-term increase
and refers to an increase that lasts for several months or years, or
maybe even the life-time of the person.
[0014] The term "penis length" refers to the maximum length of the penis,
as measured along the dorsal surface of the penis from the symphysis
pubis to the tip or end of the glans penis when the glans penis is pulled
manually and put under tension. Preferably, the measurement is taken when
the penis is fully erect.
[0015] The term "penis girth" refers to the largest measured value
obtained for circumference of the erect penis, as measured in the
midshaft region (middle third). Preferably, the measurement is taken when
the penis is fully erect.
[0016] An engorgement is deemed "cumulative prolonged" when an erectile
response lasts for at least 3 hours over a 24 hours period. Typically, an
engorgement of the invention, one that is suitable to cause penis
enlargement, is repeatedly induced for a cumulative period of 3 to 6
hours, daily (or at least four days per week), for weeks or months, but
for at least 4 weeks.
[0017] Erectile responses may be categorized according to the following: a
100% response or engorgement is a maximal erection which is very hard,
firm and unbendable, a 75% response is the softest response considered.
hard enough for penetration, a 65-75% response would be partially
engorged but would not be sufficient for penetration and intercourse,
40-65% is not a usable erection for sexual intercourse but will have
therapeutic effect for enlargement according to the invention, and a
response of less than 40% is a slightly engorged, very soft penis wherein
the size of the penis is close to the non-erect dimension of flaccid
penis with no discernable significant firmness when it is manually
palpated by an experienced health professional, and is probably not
useful for penis enlargement. Therefore, a "cumulative prolonged
engorgement" would be an erectile response that is over 40% for a period
of at least 3 hours in a 24 hours period.
[0018] As used herein, a "full erection", or the term "fully erect",
refers to an erectile response of between 75-100%.
[0019] The engorgement of the invention is typically for a "cumulative
prolonged" period, as described further below. The engorgement period is
thus usually at least 3 hours, but may be 31/2 hours, 4 hours, 41/2
hours, 5 hours, 51/2 hours, even up to 6 hours, but heavy engorgement of
a penis, say 40% or more, is usually avoided for extended periods of
time, i.e., of more than 6 hours. The erectile response may, thus, be of
the 3-6 hours engorgement resulting from a single administration per 24
hours or as a result of a plurality of administrations in this 24 hours
period.
[0020] It is possible, thus, with some patients to obtain the required
engorgement for a suitable length of time by administering a single dose.
Other patients may require two doses, one at the beginning of a daily
treatment, and one or more later one during the same treatment so as to
maintain the engorgement, say above 40% engorgement. Multiple dosing also
may simply be a preferred method of obtaining and maintaining a suitable
degree of engorgement without inducing (or at least inducing for a
relatively short period of time) a heavy engorgement of say 75%, 90% or
100%, which the subject may simply want to avoid for personal or other
reasons.
[0021] Typically, the initial erectile response is at least 65%. Later
doses can be administered if the engorgement falls below 65%, or say 40
to 45%.
[0022] Administration may be two times a week for one month, more likely 3
or 4 or more days per week, and treatments may to on for several weeks or
months, often at least 3 months.
[0023] Sometimes an endpoint is chosen after a degree of enlargement is
obtained, say 5% (length, and/or girth).within 12 to 18 months, for
example. More typically, an increase of say 30% is sought, depending upon
the desire of the subject and the effectiveness of the treatment, which
can vary.
[0024] Accordingly, the daily engorgement can include a 75-100% erectile
response for at least 90% of the time of the prolonged engorgement. In
another embodiment, the engorgement includes a 75-100% erectile response
for 50-90% of the time of the prolonged engorgement time. Alternatively,
the engorgement can include a 75-100% erectile response for up to 50% of
the time of the prolonged engorgement. Also, engorgement can include a
40-75% erectile response for at least 3 hours.
[0025] The active ingredient is a compound which causes vasodilation,
e.g., a vasodilator. The vasodilator may be selected from the group
consisting of nitrovasodilators, ACE inhibitors, angiotensin receptor
antagonists, phosphodiesterase inhibitors, direct vasodilators,
adrenergic receptor antagonists, calcium channel blocking drugs, alpha
blockers, beta blockers, lymphthomimetics, vitamins, organic nitrates,
serotonin receptor-blocking agents, angina blocking agents, other
hypertensive agents, cardiac stimulating agents, agents which improve
renal, vascular function, sympathomimetic amine, and salts, derivatives,
precursors, pharmaceutically active sequences or regions,
peptidomimetics, mimetics, and mixtures thereof.
[0026] Preferably, the vasodilator is selected from the group consisting
of papaverine, chlorpromazine, atropine, phentolamine, and prostaglandin
E1, and mixtures thereof. A preferred vasodilator is prostaglandin E1.
[0027] Administration can be by direct injection to the cavernosal tissue,
by needle, auto-injector, slow sustained injection pump, high pressure
injection device, micro pump infustion, urethral suppository, or
implantable sustained release drug or device.
[0028] The composition can be formulated for systemic administration by
oral, sublingual, or suppository administration, intravenous
administration by needle, auto-injector, slow sustained injection pump,
micro pump infusion, high pressure injection device, or implantable
sustained release drug or device, or topical administration, such as
through the use of creams, lotions or patches.
[0029] The composition can be formulated for administration to the dense
connective tissue surrounding the erectile tissue of the penis by a deep
injection that goes below the dermis and subcutaneous tissues. The
composition can be formulated for administration to the dorsal suspensory
ligand of the penis.
[0030] A preferred embodiment includes a composition formulated for
intracavernosal injection, but the composition might also be formulated
for administration by an implantable sustained release drug or device.
[0031] Prostaglandin E1 could be administered in a dosage range of from
about 0.5 to about 100 micrograms by intracavernosal injection, or
systemically at a dosage of 2 to 10,000 micrograms by an implantable
sustained release drug or device. In another aspect of the invention, the
active agent is combined with a potentiator, either directly or in vivo.
[0032] The potentiator can thus be formulated for administration by direct
injection to the cavernosal tissue, by needle, auto-injector, slow
sustained injection pump, high pressure injection device, micro pump
infusion, urethral suppository, or implantable sustained release drug or
device, etc.
[0033] The composition can be formulated for systemic administration by
oral, sublingual, or suppository administration, intravenous
administration by needle, auto-injector, slow sustained injection pump,
high pressure injection device, micro pump infusion, or implantable
sustained release drug or device, or topical administration, such as
through the use of creams, lotions or patches.
[0034] The potentiator can be formulated for administration to the dense
connective tissue surrounding the erectile tissue of the penis by a deep
injection that goes below the dermis and subcutaneous tissues.
[0035] The potentiator can be formulated for administration to the dorsal
suspensory ligand of the penis, or for intracavernosal injection, or for
administration by an implantable sustained release drug or device.
[0036] The potentiator can be administered separately from the composition
or concurrently with the composition.
[0037] The pharmaceutical composition can be such that the potentiator is
for administration more than once both separately from and concurrently
with the composition.
[0038] The potentiator can be a hormone. The hormone can be an androgen
selected from the group consisting of, but not limited to, the naturally
occurring androgens and derivatives thereof, or any agent that will
stimulate the androgen receptor directly or indirectly, including
androsterone, androsterone acetate, androsterone propionate, androsterone
benzoate, androstenediol, androstenediol-3-acetate,
androstenediol-17-acetate, androstenediol-3, 17-diacetate,
androstenediol-17-benzoate, androstenediol-3-acetate-17-benzoate,
androstenedione, dehydroepiandrosterone (DHEA; also termed "prasterone"),
sodium dehydroepiandrosterone sulfate, 4-dihydrotestosterone. (DHT; also
termed "stanolone"), 17.beta.-hydroxyandrost-4-en-3-one,
5.alpha.-dihydrotestosterone, dromostanolone, dromostanolone propionate,
ethylestrenol, nandrolone phenpropionate, nandrolone decanoate,
nandrolone ftirylpropionate, nandrolone cyclohexanepropionate, nandrolone
benzoate, nandrolone cyclohexanecarboxylate, oxandrolone, stanozolol and
testosterone, pharmaceutically acceptable esters of testosterone and
4-dihydrotestosterone, including esters formed from the hydroxyl group
present at the C-17 position, including, but not limited to, the
enanthate, propionate, cypionate, phenylacetate, acetate, isobutyrate,
buciclate, cyclopentylpropionate, isocarponate, heptanoate, decanoate,
undecanoate, caprate and isocaprate esters, pharmaceutically acceptable
derivatives of testosterone such as methyl testosterone, testolactone,
oxymetholone and fluoxymesterone; synthetic androgens, and
7-Methyl-Nortestosterone ("MENT'") and its acetate ester, and salts,
derivatives, precursors, pharmaceutically active sequences or regions,
peptidomimetics, mimetics, and mixtures thereof.
[0039] A specific potentiator is the androgen testosterone. Another is
4-dihydrotestosterone.
[0040] The potentiator can be selected to promote the elongation of
collagen, or to inhibit collagen cross-linkage, or to increase collagen
solubility.
[0041] The potentiator can be selected from a group consisting of relaxin,
insulin like growth factors, growth hormone, metallo-proteinases or
metallo-proteinase agonists or promoters of collagenase activity, tissue
inhibitors of matrix metalloprotenases (TIMPS), other agents that
increase collagen solubility, prostaglandins, corticosteroids, potassium
aminobenzoate (Potaba.TM.), and dimethyl sulfoxide (DMSO),
D-penicillamine, and salts, derivatives, precursors, pharmaceutically
active sequences or regions, peptidomimetics, mimetics, and a mixture
thereof.
[0042] A particular potentiator is relaxin.
[0043] A prostaglandin potentiator can be prostaglandin F2 alpha or
prostaglandin E2. The potentiator might be relaxin, prostaglandin F2
alpha, or prostaglandin E2, or the biochemical mediators that result in
the desired changes in collagen or the connective tissue that produces
and remodels collagen and express the effects of relaxin, prostaglandin
F2 alpha, or prostaglandin E2.
[0044] Another potentiator is aminobenzoate potassium (Potaba.TM.), or
dimethyl sulfoxide (DMSO).
[0045] Relaxin can be administered at a dosage of 0.02 to 10 micrograms/kg
body weight/day by intracavernosal injection. Relaxin might be for
topical administration at a dosage of 25 to 400 micrograms/kg body
weight/day. The relaxin might be for administration at a dosage of 0.02
to 1 micrograms/kg body weight/day by injection into the dense connective
tissue surrounding the erectile tissue of the penis.
[0046] A device can be used to prolong the retention of the composition in
the penis. For example, a ring designed to fit around the base of the
penis might be used.
[0047] Thus, as hereinabove defined, the invention provides a method for
causing enlargement of a male subject's penis, comprising the steps of
(a) administering to the patient an effective amount of a pharmaceutical
vasodilator, optionally in admixture with a pharmaceutically acceptable
agent to induce a prolonged engorgement of the subject's penis; and (b)
repeating step (a) as necessary to cause said enlargement.
[0048] The invention includes a kit that include a composition of the
invention as disclosed herein, in combination with instructions for
administering the composition to a human male according to a method
disclosed herein for the purposes disclosed herein.
[0049] Typically, such instructions are provided in written form, but they
could be provided orally by a health professional, or in an electronic
form on a medium such as a video compact disc, laser-readable disk, video
tape, audio tape or disk, etc.
DETAILED DESCRIPTION OF THE INVENTION
[0050] In one embodiment of the invention, a pharmaceutical vasodilator
composition is administered to a male patient to cause a prolonged
engorgement of the penis in order to cause expansion of the erectile
tissue. The pharmaceutical composition comprises a pharmaceutically
acceptable vasodilator for causing a prolonged suitable engorgement of
the penis, together with a pharmaceutically acceptable diluent or
carrier. The vasodilator may be a drug typically used to treat erectile
dysfunction, but administered at a similar or higher dosage or
sequentially as two or more lesser doses to achieve a prolonged period of
engorgement followed by an additional period of lesser engorgement.
Optionally, the agent may be administered at a slow rate with a micro
infusion pump, time-release device or other self-injection technique or
device. During a treatment, the penis should be engorged for a minimum of
3 hours and typically there is one treatment per day, and at least four
treatments per week.
[0051] A very hard firm erection which is usually preferred for erectile
dysfunction will have more veno-occlusive obstruction of the circulation
and the reduced flow of fresh oxygenated blood into the erectile tissue
will limit the maximum duration that the erection can be safely
maintained. A softer less firm response can be safely and comfortably
maintained for a greater length of time than a full erection.
[0052] The vasodilator drug may be one which either directly or indirectly
causes vasodilation and may be classified, without limitation, in one of
the following categories, namely, nitrovasodilators, ACE inhibitors,
angiotensin receptor antagonists, phosphodiesterase inhibitors, direct
vasodilators, adrenergic receptor antagonists, calcium channel blocking
drugs, alpha blockers, beta blockers, lymphthomimetics, vitamins, organic
nitrates, serotonin receptor-blocking agents, angina blocking agents,
other hypertensive agents, cardiac stimulating agents, agents which
improve renal, vascular function, sympathomimetic amine and mixtures
thereof. For example, the drug may be any suitable vasodilator, such as
papaverine, chlorpromazine, atropine, phentolamine, and prostaglandin E1,
and salts, derivative, precursors, pharmaceutically active sequences or
regions, peptidomimetics, mimetics, and mixtures thereof. Other drugs
which may cause vasodilation include, without limitation, any of the
following: niacin, nitroglycerine, nilatrin hydrochloride,
pentoxyphylene, phenoxybenzamine, dichlophenac, hydralazine, hydrazaline,
hydrochlorothiazide, sodium nitroprusside, isoxaprine hydrochloride,
epoprostenol sodium, nylidrin hydrochloride, tolazoline hydrochloride,
nicotinyl alcohol, phentolamine mesylate, phentolamine hydrochloride,
yohimbine, thymoxamine imipramine, verapamil, isoxsuprine, naftidrofuryl,
tolazoline, hydroisosorbide, dibenamine dinitrate, captopril, enalapril,
enalaprilat, quinapril, lisinopril, ramipril, losartan, amrinone,
milrinone, vesnarinone, nicorandil, prazosin, labetalol, celiprolol,
carvedilol, bucindolol, nifedipine, dobutamine, minoxidil, nylidrin, and
salts, derivatives, precursors, and mixtures thereof. Preferably, the
vasodilator is prostaglandin E1, alone or with other vasodilators,
administered as one or more doses that are typically lower than what
would be used to treat erectile dysfunction. For example, the
prostaglandin E1 may be administered by intracavernosal injection in a
dosage range of 0.2 mcg to 500 mcg, more preferably in a dosage range of
0.5 mcg to 100 mcg. For example again, the prostaglandin E1 may be
administered by an implantable sustained release drug or device in a
dosage range of 0.5 mcg to 20,000 mcg, more preferably in a dosage range
of 2 to 10,000 mcg (mcg=microgram).
[0053] Optionally, the patient may be treated with an additional, second
pharmacological agent, to potentiate the effect of the composition which
causes a prolonged, engorgement of the penis. Here, the second agent is
called a "potentiator". The potentiator may be administered as part of
the composition, separately from the composition, or a combination of
both.
[0054] The potentiator may be a pharmacological agent or combination of
agents that promote cellular processes that result in biological and/or
mechanical creep and ultimately induce remodelling of the connective
tissues that help define the size and shape of the penis. In addition, an
agent which increases solubility of collagen may be used as a
potentiator. Agents with very specific mechanisms of action may be used,
or other agents with pleomorphic mechanisms of action, such as relaxin or
growth hormone which trigger diverse mechanisms to induce growth in the
penis may be used. For example, agents may be administered that
facilitate the elongation of collagen fibres and accelerate the turnover
remodelling rates of collagen through numerous mechanisms. For example,
D-penicillamine and dimethyl sulfoxide (DMSO), which promote the
elongation of collagen by inhibiting or interfering with inter- and
intramolecular collagen cross-linkage may be used. Other agents include,
but are not limited to, relaxin, insulin like growth factors, growth
hormone, metalloproteinases or metalloproteinases agonists or promoters
of collagenase activity, tissue inhibitors of matrix metalloprotenases
(TIMPs) other agents that increase collagen solubility, prostaglandins,
corticosteroids, or aminobenzoate potassium, a commercial brand being
known as Potaba.TM.. Preferred prostaglandins are prostaglandin F2 alpha
and prostaglandin E2. Also included are pharmaceutically active
sequences, peptidomimetics, or mimetics above the above-listed molecules.
[0055] Relaxin directly and indirectly triggers a cascade of complex
biochemical and cellular effects that can cause general morphological
changes to genitalia. Prostaglandins such as prostaglandin F2 alpha and
prostaglandin E2 have similar effects. This invention includes the
mediators of these cascades as potentiators.
[0056] Collagen is a component of the extracellular matrix (ECM), which is
a dynamic entity with many other components (e.g., proteoglycans,
fibronectin, elastin, laminin, etc.) that functions as a storage
reservoir for cytokines and enzymes and interacts intimately with
surrounding cells to provide a structural scaffold and an efficient
biochemical communication network within tissues. Enzymes primarily
responsible for ECM remodeling are the Matrix MetalloProteinases (MMPs),
which break down ECM components, and the Tissue Inhibitors of Matrix
MetalloProteinases (TIMPs). Maintenance of a balance of ECM synthesis and
MMP/TIMP activity in tissues is required for normal homeostasis;
imbalances will generally lead to diseases or developmental problems such
as scleroderma, periodontal disease, restenosis, osteoarthritis, liver
cirrhosis, glomerulonephritis, and ulceration.
[0057] Relaxin is a 6 kDa peptide hormone that is structurally similar to
insulin; the prohormone form consists of B-C-A chains (20 kDa), and the C
chain is proteolytically excised in `mature` relaxin. However, unlike
many other pro-hormones, pro-relaxin retains its biological activity. The
profile of conserved amino acid sequences among various species such as
pig, human, whale, porpoise, and shark suggests that relaxin is an
ancient hormone with a unique molecular evolutionary history. The most
recognized effect of relaxin on target cells is induction of MMP
expression and inhibition of collagen synthesis.
[0058] Historically, relaxin has been classified as a "pregnancy hormone"
that acts on reproductive tissues only during pregnancy, preparing the
female for parturition by "relaxing" the pelvic ligaments and tendons.
However, recent evidence suggests that relaxin may be classified as a
"master hormone" that also induces biochemical, changes in a number of
non-reproductive tissues. In addition to up-regulating MMP expression in
reproductive tissues such as the cervix and placenta relaxin up-regulates
expression of MMP-1 and MMP-3 in lung fibroblasts, skin fibroblasts, and
fibrocartilaginous cells. Relaxin receptors are found in the brain heart,
skin, nipples, small intestine, mammary gland, blood vessels, and testes.
The bioactivity of relaxin is unique when compared with other cytokines
that affect ECM remodeling.
[0059] The potentiator or potentiators may be administered as part of the
composition, separately from the primary composition, or a combination of
both. For example, the potentiator Potaba.TM. may be administered orally
and the composition administered intracavernosally. Optionally, the
potentiater may be administered locally into the cavernosal tissue,
externally but adjacent the cavernosal tissue by injection into the
surrounding connective tissue or the dorsal suspensory ligament of the
penis, or a combination. The potentiator may be an agent which activates
the androgen receptor, which is involved with male sexual development and
function. For example, the potentiator may be an androgen hormone such
as, but not limited to, the naturally occurring androgens and derivatives
thereof, including androsterone, androsterone acetate, androsterone
propionate, androsterone benzoate, androstenediol,
androstenediol-3-acetate, androstenediol-17-acetate, androstenediol-3,
17-diacetate, androstenediol-17-benzoate, androstenediol-3-acetate-17-ben-
zoate, androstenedione, dehydroepiandrosterone (DHEA; also termed
"prasterone"), sodium dehydroepiandrosterone sulfate,
4-dihydrotestosterone (DHT; also termed "stanolone"),
17.beta.-hydroxyandrost-4-en-3-one, 5.alpha.-dihydrotestosterone,
dromostanolone, dromostanolone propionate, ethylestrenol, nandrolone
phenpropionate, nandrolone decanoate, nandrolone furylpropionate,
nandrolone cyclohexanepropionate, nandrolone benzoate, nandrolone
cyclohexanecarboxylate, oxandrolone, stanozolol and testosterone;
pharmaceutically acceptable esters of testosterone and
4-dihydrotestosterone, typically esters formed from the hydroxyl group
present at the C-17 position, including, but not limited to, the
enanthate, propionate, cypionate, phenylacetate, acetate, isobutyrate,
buciclate, heptanoate, decanoate, undecanoate, caprate and isocaprate
esters; and pharmaceutically acceptable derivatives of testosterone such
as methyl testosterone, testolactone, oxymetholone and fluoxymesterone.
Testosterone and testosterone esters, such as testosterone enanthate,
testosterone propionate and testosterone cypionate, may be used. The
aforementioned testosterone esters are commercially available or may be
readily prepared using techniques known to those skilled in the art or
described in the pertinent literature.
[0060] The aforementioned androgenic agents are selected from the group
consisting of naturally occurring androgens, synthetic androgens, and
derivatives thereof, and any agent that will stimulate the androgen
receptor directly or indirectly. The active agents may be incorporated
into the present dosage units and thus administered in the form of a
pharmaceutically acceptable derivative, analog, ester, salt, or amide, or
the agents may be modified by appending one or more appropriate
functionalities to enhance selected biological properties such as
penetration through mucosal tissue. Preparation of esters, as noted in
the preceding section, involves functionalization of hydroxyl and/or
carboxyl groups that may be present, as will be appreciated by those
skilled in the arts of pharmaceutical chemistry and drug delivery. For
example, to prepare testosterone esters, the 17-hydroxyl group of the
testosterone molecule is generally caused to react with a suitable
organic acid under esterifying conditions, such conditions typically
involving the use of a strong acid such as sulfuric acid, hydrochloric
acid, or the like, and a temperature sufficient to allow the reaction to
proceed at reflux. Esters can be reconverted to the free acids, if
desired, by using conventional hydrogenolysis or hydrolysis procedures.
[0061] Testosterone is the principal steroid secreted by the testes and is
the primary circulating androgen found in the plasma of males.
Testosterone is converted to 4-dihydrotestosterone(DHT) by the enzyme 5
alpha-reductase in many peripheral tissues. DHT is thus thought to serve
as the intracellular mediator for most androgen actions (Zhou, et al.,
Molec. Endocrinol. 9:208-18 (1995)). Other steroidal androgens include
esters of testosterone, such as the cypionate, propionate,
phenylpropionate, cyclopentylpropionate, isocarporate, enanthate, and
decanoate esters, and other synthetic androgens such as
7-Methyl-Nortestosterone ("MENT'") and its acetate ester.
[0062] Optionally, a mechanical device such as a ring may be used at the
base of the penis to prolong retention of the composition within the
penis. The mechanical device may also be used to prolong retention of any
pharmacological agent used to potentiate the effect of the composition,
i.e., the potentiator.
[0063] The pharmaceutical composition is administered to the patient in a
pharmaceutically acceptable dosage and schedule of administration to
achieve engorgement which lasts for several hours. The treatment regimen
typically begins with the physician determining a first dosage amount to
try on a patient to determine that subject's erectile responsiveness to
the composition. The amount of the first dosage given will be determined,
among other things, by the route of intended administration, the age of
the man, the recent history of erectile function of the man, and
pre-existing health conditions of the man.
[0064] To achieve an erectile response, one or more doses may be
administered which are typically of similar or a higher amount than that
used to treat erectile dysfunction. This should produce a full erection.
Alternatively, two or more lesser doses may be administered to achieve a
prolonged engorgement of about 40-75% response. Optionally, a combination
of similar, higher, and lesser doses may be administered.
[0065] It is the duration of a full erection and the subsequent period of
engorgement that determines the starting dose. The penis may be visually
inspected and palpated to determine the extent of the response to the
composition.
[0066] A desirable first erectile response for the purposes of this
invention is considered to be at least a 45-100% response for a period of
at least two hours, but preferably 3-6 hours duration. For
intracavernosal injections, first dosage amounts may range from about 0.5
mcg to about 30 mcg of prostaglandin E1, and more preferably from 1 mcg
to 6 mcg. If a 70-100% erection is not achieved within 20 minutes of the
first test dosage amount administered by intracavernosal injection, a
second injection of less, the same or more of the composition as the
initial test injection, depending on if there was any response with the
first test dosage. For example, if there was a 55-70% response, a
"booster" shot of a lesser amount than the first dosage amount may be
administered. If there was no response, the same or more than the amount
of the first dosage amount may be administered. Other administrative
routes may take a longer or shorter time to achieve the initial response.
The dosage is gradually increased by an amount that is usually within 50%
to 200% the previously administered dosage until a satisfactory response
is achieved. Using these general guidelines a maximum of two injections
are administered per visit.
[0067] If an erection is not achieved with the first or second injection,
one or more additional appointment/visits on another day may be required
to establish the dose.
[0068] Once the correct response is achieved, it will be followed by one
or more confirmatory doses on subsequent visits. Once a starting dosage
amount of a single or a sequence of two or more injections is established
that provides a response of suitable duration, the dosage may be
titrated, for example, to provide the subject with an initial 70%-100%
engorgement followed by a further period of reduced engorgement of at
least 40% for at least 3-6 hours. The firmness of the penis generally
decreases over this period, but will be at least 40% engorged for at
least 3 and preferably up to 6 hours and less than 75% engorged for the
majority of the time.
[0069] Depending on the subject's response to the treatment, higher
dosages may be used as determined by the physician. However, it should be
noted that higher dosages may increase the risk of a very firm erection
that may cause ischemia. If the veno-occlusive mechanism closes to an
extent that it reduces the inflow of fresh oxygenated blood for a
sufficient period to cause pain and tissue damage it can cause a medical
condition called a priapism. The risk of priapism can be reduced by using
smaller multiple doses. The subject's condition should be monitored and
the dosage adjusted to ensure that the patient experiences a prolonged
period of engorgement, rather than a prolonged full erection, which may
lead to priapism and associated health complications.
[0070] Subjects should have careful instruction in the signs and symptoms
of priapism, and have access to 24 hour emergency medical treatment to
allow prompt treatment and eliminate any risks of ischemia to the penis.
[0071] A physician should closely monitor the subject's response to
medication, to determine signs of edema, tenderness, and other early
signs that the dose is excessive and needs adjusting.
[0072] If lumps or unexpected thickening of the penis occurs during
treatment, the patient may have to stop or suspend treatment for a period
of time. Once the appropriate dosage for a given patient has been
determined, the treatment may be self-administered under the close
supervision of a properly trained physician or health professional.
[0073] The treatment is repeated over a period of time sufficient to cause
a permanent increase in the length and girth of the patient's penis. The
treatment may comprise administration with the composition alone, or in
conjunction with potentiator. For example, the treatment may be repeated
daily or at least two times a week over a period of several weeks or at
least one month. More preferably, the treatment may be repeated at least
3-4 times a week for a period of at least 3 months. For treatment periods
of between 12 and 18 months, an increase of at least 5% may be achieved
in the length and girth of an erect penis, and increases of at least 30%
or even at least 50% in the length and girth of an erect penis may be
achieved. Active treatment for more extended periods, e.g. 24 months, may
yield greater results.
[0074] The subject may continue with normal sexual activities during the
course of treatment. In fact, due to the prolonged elevation in penile
blood flow, patients using this treatment will experience a very
significant increase in erectile function. During treatment, patients
will have dramatic improvements in the frequency, strength and duration
of their own naturally stimulated erections. Men using this treatment
will require much lower levels of sexual arousal and stimulation to
produce and maintain their own naturally induced erections.
[0075] The pharmaceutical composition and/or potentiator may be
administered using a variety of different methods known to those of skill
in the art, including administration by direct manual injection to the
cavernosal tissue by needle, auto-injector, slow sustained injection
pumps, high pressure injection devices, urethral suppository, implantable
sustained release drug or device, microinfusion pump or systemically by
oral administration, parenteral administration such, as subcutaneously or
intra muscularly, intravenous administration by needle, auto-injector,
slow sustained injection pump, high pressure injection device or
implantable sustained release drug device, or topical administration,
such as through the use of creams, lotions or patches with suitable
additives for transdermal delivery. Most conveniently, the treatment with
the vasodilators is administered by intracavernosal injection.
Optionally, the pharmaceutical composition and/or potentiator may be
administered by a deep injection that is well below the dermis and
subcutaneous tissues which is administered into the dense connective
tissue that surround the erectile tissue of the penis. This may be in the
form of a depot oil. The pharmaceutical composition and/or potentiator
may also be administered to the dorsal suspensory ligand of the penis.
[0076] For example, relaxin may be administered by intracavernosal
injection at a dosage ranging from 0.01 to 50 mcg/kg body weight/day,
more preferably at a dosage ranging from 0.02 to 10 mcg/kg body
weight/day, or topically at a dosage ranging from 5 to 1000 mcg/kg body
weight/day, more preferably at a dosage ranging of 25 to 400 mcg/kg body
weight/day, or by injection into the dense connective tissue surrounding
the erectile tissue of the penis at a dose ranging from 0.01 to 50 mcg/kg
body weight/day, more preferably at a dosage ranging from 0.02 to 10
mcg/kg body weight/day, and more preferably still, at a dosage ranging
from 0.02 to 1 mcg/kg body weight/day.
[0077] Kits of the composition are part of this invention. The kit may
include a pharmaceutical composition of the invention and written
instructions as to how and when to administer the composition in order to
achieve an enlarged penis by repeated treatments, over a period of weeks
or months. Optionally, the kit may include a pharmaceutical composition
of the invention with written and possibly videotaped/cd rom (compact
disc) video, instructional information and/or be accompanied by oral
instructions from a health professional as to how and when to administer
the composition in order to achieve an enlarged penis. Preferably, the
patient does not self-administer the composition without the supervision
of a health professional. Optionally, the kit may also include an agent
which will potentiate the effects of the pharmaceutical compositions of
this invention. In this case, written, video format instructions or oral
instructions will be included as to how to use the agent to potentiate
the effect of the composition.
[0078] Without binding itself to any particular theory, applicant believes
that this invention works by inducing biological creep (induction of
cellular processes for tissue remodelling and cellular growth) and, to a
lesser degree, biomechanical creep (mechanical microscopic tearing and
viscoelastic stretching of the connective tissue). The pharmaceutical
composition of the present invention induces prolonged penile
engorgement, which results in a significant increase in the arterial
blood flow through the penis. This increase in blood flow can safely
activate the veno-occlusive mechanism that then expands and pressurizes
the erectile tissue for several hours, while providing a constant flow of
fresh oxygenated blood flow into the penis. This avoids the complications
and health risks caused by priapism and ischemia and safely applies
prolonged, continuous stimulation of the cellular processes necessary to
induce maximal rates of biological and mechanical creep to enlarge the
penis with minimal distortions in the shape or architecture of the penis.
The potentiators may be co-comittently administered to accelerate the
rate of the cellular processes that remodel the tissues of the penis in
the growth/enlargement process.
[0079] In order that the invention may be better understood, preferred
embodiments will now be described in the following examples.
EXAMPLE 1
[0080] A male patient, age 41, was treated with intracavernosal injections
of a vasodilator, prostaglandin E1, on a regular basis (approximately
four to five times per week) over an 18 month treatment period. A
sufficient quantity was administered to maintain a prolonged engorgement
of an erectile response between 40-75% over a period of several hours,
generally 3 to 6 hours. The quantity of medication was adjusted from time
to time in accordance with the patient's response, which was monitored at
least weekly.
[0081] The size of the patient's fully erect penis increased from 5.8
inches to 8.6 inches in length (about an 48% increase) and 3.7 inches to
5.8 inches in girth (about an 56% increase) over the 18-month treatment
period. Following the discontinuation of this treatment, the erect penis
length remained stable for two years at over 81/2 inches. Treatment was
re-institued combining intracavernosal injections 3-4 times per week of a
mixture of testosterone (0.5 mg) and vasodilators with low dose oral
Potaba (500-1000 mg) 3-4 times per day. After a short treatment period of
21/2 months, the patient's erect penis was over 9 inches in length, which
means he has gained an additional 0.4-0.5 inches in length (about an 6%
increase). The total increase in length was therefore about 3.2 inches
(about an 55% increase) in length.
EXAMPLE 2
[0082] A male patient, age 30, was treated with intracavernosal injections
of the vasodilator on a regular basis (approximately four to five times
per week) over a 6-month treatment period. A sufficient quantity was
administered to maintain a prolonged engorgement over a period of about 3
to 6 hours. The quantity of medication was adjusted in accordance with
the patient's response. The potentiator potaba (aminobenzoate) (1000 mg/4
times per day) was administered orally to the patient for the last 60
days of treatment.
[0083] The patient's erect penis increased from 5.6 inches to 7.7 inches
(about an 38% increase) in length and 3.2 inches to 5.3 inches (about an
65% increase) in girth over the 6-month treatment period.
EXAMPLE 3
[0084] A male patient, age 52, was treated with separate intracavernosal
injections of vasodilators, Papavarine, phentolamine and prostaglandin
E1, on a regular basis, selected from treatments of 0 to 4 times per
week, over a 7 month treatment period along with daily subcutaneous
injections of a prostaglandin F analogue. A sufficient quantity of
vasodilator was administered to maintain a prolonged engorgement of an
erectile response greater than 70% for 3.5-5 hours duration. The quantity
of medication was adjusted from time to time in accordance with the
patient's response, which was monitored initially weekly then monthly
once the patient had mastered the IC technique and the responses were
consistently of the same duration.
[0085] The size of the patient's fully erect penis increased from 5.0
inches to 6.3 inches in length, i.e. about a 26% increase, over the
7-month treatment period. Following the discontinuation of this
treatment, the erect penis length remained stable.
EXAMPLE 4
[0086] A male patient, age 34, was treated with intracavernosal injections
of a triple mix of the vasodilators Atropine, Chlorpromazine and
Papavarine on a regular basis (approximately two to five times per week)
over a 4-month treatment period. A sufficient-quantity was administered
to maintain a prolonged engorgement of 60-90% over a period of about 3 to
4.5 hours. The quantity of medication was adjusted in accordance with the
patient's response. The potentiator, Potaba.TM.--potassium aminobenzoate
(1000 mg/3-4 times per day) was administered orally starting 1 month
before starting the IC injections of the vasodilators Atropine,
Chlorpromazine and Papavarine.
[0087] After 5 months of treatment the patient's erect penis increased
from 6.0 inches to 7.1 inches (about an 18% increase) in length.
EXAMPLE 5
[0088] A male patient, age 44, was treated with intracavernosal injections
of a quadruple mix of the vasodilators prostaglandin E1, Atropine,
Chlorpromazine and Papavarine on a regular basis (approximately two to
four times per week) over a 4-month treatment period. A sufficient
quantity was administered to maintain a prolonged engorgement over a
period of about 3 to 5 hours. The quantity of medication was adjusted in
accordance with the patient's response. The potentiator
dihydrotestosterone 5% ointment was administered orally starting two
weeks before starting the IC injections of the vasodilators Atropine,
Chlorpromazine and Papavarine and prostaglandin.
[0089] After 4 months of treatment the patient's erect penis increased
from 5.2 inches to 6.5 inches (about a 25% increase) in length.
EXAMPLE 6
[0090] A male patient, age 44, was treated with intracavernosal injections
of the vasodilator phentolamine on a regular basis (approximately two to
four times per week) over a 4-month treatment period. Phentolamine was
frequently combined with indirect vasodilating effects of oral Viagra to
produce and maintain a prolonged engorgement of 60-90% over a period of
about 3 to 5 hours. The quantity of medication was adjusted in accordance
with the patient's response. The potentiator dihydrotestosterone gel was
administered orally starting two weeks before starting the IC injections
of the vasodilators Atropine, Chlorpromazine and Papavarine and
prostaglandin.
[0091] After 4 months of treatment the patient's erect penis increased
from 5.2 inches to 6.5 inches (about a 25% increase) in length.
EXAMPLE 7
[0092] A male patient, age 72, was treated with intracavernosal injections
of the quadruple mix of the vasodilators prostaglandin E1, Atropine,
Chlorpromazine and Papavarine on a regular basis (approximately two to
four times per week) over a 3-month treatment. The indirect vasodilating
effects of oral Cialis and Levitra were sometimes added to the quadruple
mix of the vasodilators prostaglandin E1, Atropine, Chlorpromazine and
Papavarine to produce and maintain a prolonged engorgement of 60-85% over
a period of about 2.5 to 3 hours. The quantity of medication was adjusted
in accordance with the patient's response. The potentiators Potaba 1000
mg 4.times./day orally and prostaglandin F topically were also used with
the vasodilators. After 3 months of treatment the patient's erect penis
increased from 6.5 inches to 7.1 inches (about a 9% increase) in length.
EXAMPLE 8
[0093] A male patient, age 47, was treated with intracavernosal injections
of a triple mix of the vasodilators Atropine, Chlorpromazine and
Papavarine on a regular basis (approximately three to four times per
week) over a 6-month treatment period. A sufficient quantity was
administered to maintain a prolonged engorgement of an erectile response
between 60-95% over a period of several hours, generally 3 to 4.5 hours.
The quantity of medication was adjusted from time to time in accordance
with the patient's response, which was monitored initially weekly. After
2 months of treatment subcutaneous injections of testosterone 14-20 mg
into the penis were added as an accelerator.
[0094] The size of the patient's fully erect penis increased from 5.2
inches to 6.0 inches in length (about a 15% increase) over the 6 month
treatment period.
EXAMPLE 9
[0095] A male patient, age 52, was treated with intracavernosal injections
of the quadruple mix of the vasodilators prostaglandin E1, Atropine,
Phentolamine and Papavarine on a regular basis (using IC medications
approximately two to four days per week) over a 3-month treatment. Since
the maximum duration of the engorgement of the erection from a single
dose was only 45 to 80 minutes, the patient used two to three separate IC
injects spaced through out the treatment days to achieve a total i.e.
cumulative daily duration of 3 to 4 hours. The indirect vasodilating
effects of oral Cialis and Levitra were sometimes added to the quadruple
mix of the vasodilators prostaglandin E1, Atropine, Chlorpromazine and
phentolamine to produce and maintain a prolonged engorgement of 60-85%
over a period of about 3 to 4 hours. The quantity of medication was
adjusted in accordance with the patient's response. The potentiator
Potaba 1000 mg 4.times./day orally was used with the vasodilator. After 4
months of treatment the patient's erect penis increased from 5.4 inches
to 6.1 inches (about al 3% increase) in length and 4.4 to 5.1 inches in
circumference (about a 16% increase in circumference).
EXAMPLE 10
[0096] A male patient, age 27, was treated with intracavernosal injections
of a prostaglandin E1 on a regular basis (approximately two to five times
per week) over a 3-month treatment period. Due to a sensitivity to
Prostraglandin E1 causing aching and pain at higher doses, the maximum
tolerated dose which produced a comfortable erection was only lasting 90
to 120 minutes. The patient used two separate IC injects spaced
throughout the treatment days to achieve a total daily cumulative
engorgement duration of 3 to 4 hours. The quantity of medication was
adjusted in accordance with the patient's response. The 15 mg of the
potentiator Dihydrotestosterone was injected subcutaenously into the
penis daily throughout the treatment period. After 3 months of treatment
the patient's erect penis increased from 6.3 inches to 7.1 inches (about
an 13% increase) in length.
[0097] Although various examples of combined elements of the invention
have been described, it will also be understood that these are not
intended to be exhaustive and features of one embodiment may be combined
with those of another, and such other combinations are contemplated to be
within the scope of the invention disclosed herein.
[0098] All publications and other documents mentioned herein are hereby
incorporated by reference into this specification.
[0099] While preferred embodiments of the invention have been illustrated
and described, it will be appreciated that various changes and
modifications can be made therein without departing from the spirit and
scope of the invention as defined by the following claims.
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