Unimed Products

[Guest guest]

Hi all,

Last night I was at Tom Inclendon's office and we pulled up info on the

new T gel that Unimed products is coming out with. Below is there data.

Take care,

Dale

http://www.unimed.com/proddisc2.html

AndroGel

(testosterone gel) 1% CIII

DESCRIPTION

AndroGel (testosterone gel) is a clear, colorless hydroalcoholic gel containing 1%

testosterone. AndroGel provides continuous transdermal delivery of testosterone,

the primary circulating endogenous androgen, for 24 hours following a single application

to intact, clean, dry skin of the shoulders, upper arms and/or abdomen.

A daily application of AndroGel 5 G, 7.5 G, or 10 G delivers 50 mg, 75 mg, or 100

mg of testosterone, respectively, per day, to the skin's surface. Approximately 10%

of the applied testosterone dose is absorbed across skin of average permeability during

a 24-hour period.

The active pharmacologic ingredient in AndroGel is testosterone. Testosterone USP

is a white to practically white crystalline powder chemically described as 17-beta

hydroxyandrost-4-en-3-one.

Inactive ingredients in AndroGel are ethanol 68.9%, purified water, sodium hydroxide,

Carbomer 940 and isopropyl myristate; these ingredients are not pharmacologically

active.

CLINICAL PHARMACOLOGY

AndroGel (testosterone gel) delivers physiologic amounts of testosterone, producing

circulating testosterone concentrations that approximate normal levels (2981043 ng/dL)

seen in healthy men.

Testosterone--General Androgen Effects:

Endogenous androgens, including testosterone and dihydrotestosterone (DHT), are responsible

for the normal growth and development of the male sex organs and for maintenance of

secondary sex characteristics. These effects include the growth and maturation of

prostate, seminal vesicles, penis, and scrotum; the development of male hair distribution,

such as facial, pubic, chest, and axillary hair; laryngeal enlargement, vocal cord

thickening, alterations in body musculature, and fat distribution. Testosterone and

DHT are necessary for the normal development of secondary sex characteristics. Male

hypogonadism results from insufficient secretion of testosterone and is characterized

by low serum testosterone concentrations. Symptoms associated with male hypogonadism

include impotence and decreased sexual desire, fatigue and loss of energy, mood depression,

regression of secondary sexual characteristics and osteoporosis. Hypogonadism is a

risk factor for osteoporosis in men.

Drugs in the androgen class also promote retention of nitrogen, sodium, potassium,

phosphorus, and decreased urinary excretion of calcium. Androgens have been reported

to increase protein anabolism and decrease protein catabolism. Nitrogen balance is

improved only when there is sufficient intake of calories and protein.

Androgens are responsible for the growth spurt of adolescence and for the eventual

termination of linear growth brought about by fusion of the epiphyseal growth centers.

In children, exogenous androgens accelerate linear growth rates but may cause a disproportionate

advancement in bone maturation. Use over long periods may result in fusion of the

epiphyseal growth centers and termination of the growth process. Androgens have been

reported to stimulate the production of red blood cells by enhancing erythropoietin

production.

During exogenous administration of androgens, endogenous testosterone release may

be inhibited through feedback inhibition of pituitary luteinizing hormone (LH). At

large doses of exogenous androgens, spermatogenesis may also be suppressed through

feedback inhibition of pituitary follicle-stimulating hormone (FSH).

There is a lack of substantial evidence that androgens are effective in accelerating

fracture healing or in shortening post-surgical convalescence.

Pharmacokinetics

Absorption

AndroGel is a hydroalcoholic formulation that dries quickly when applied to the skin

surface. The skin serves as a reservoir for the sustained release of testosterone

into the systemic circulation. In a study with the 10 G dose (to deliver 100 mg testosterone),

all patients showed an increase in serum testosterone within 30 minutes, and eight

of nine patients had a serum testosterone concentration within the normal range by

4 hours after the initial application. Absorption of testosterone into the blood continues

for the entire 24-hour dosing interval. Serum concentrations approximate the steady

state level by the end of the first 24 hours and are at steady state by the second

or third day of dosing.

With single daily applications of AndroGel, follow-up measurements 30, 90 and 180

days after starting treatment have confirmed that serum testosterone concentrations

are generally maintained within the eugonadal range. Figure 1 summarizes the 24-hour

pharmacokinetic profiles of testosterone for patients maintained on 5 G or 10 G of

AndroGel (to deliver 50 or 100 mg of testosterone, respectively) for 30 days. The

average (±SD) daily testosterone concentration produced by AndroGel 10 G on Day 30

was 792 (±294) ng/dL and by AndroGel 5 G 566 (±262) ng/dL.

When AndroGel treatment is discontinued after achieving steady state, serum testosterone

levels remain in the normal range for 24 to 48 hours but return to their pretreatment

levels by the fifth day after the last application.

Distribution

Circulating testosterone is chiefly bound in the serum to sex hormone-binding globulin

(SHBG) and albumin. The albumin-bound fraction of testosterone easily dissociates

from albumin and is presumed to be bioactive. The portion of testosterone bound to

SHBG is not considered biologically active. The amount of SHBG in the serum and the

total testosterone level will determine the distribution of bioactive and nonbioactive

androgen. SHBG-binding capacity is high in prepubertal children, declines during puberty

and adulthood, and increases again during the later decades of life. Approximately

40% of testosterone in plasma is bound to SHBG, 2% remains unbound (free) and the

rest is bound to albumin and other proteins.

Metabolism

There is considerable variation in the half-life of testosterone as reported in the

literature, ranging from ten to 100 minutes.

Testosterone is metabolized to various 17-keto steroids through two different pathways.

The major active metabolites of testosterone are estradiol and DHT. DHT binds with

greater affinity to SHBG than does testosterone. In many tissues, the activity of

testosterone depends on its reduction to DHT, which binds to cytosol receptor proteins.

The steroid-receptor complex is transported to the nucleus where it initiates transcription

and cellular changes related to androgen action. In reproductive tissues, DHT is further

metabolized to 3-alpha and 3-ß androstanediol.

DHT concentrations increased in parallel with testosterone concentrations during AndroGel

treatment. After 180 days of treatment, mean DHT concentrations were within the normal

range with 5 G AndroGel and were about 7% above the normal range after a 10 G dose.

The mean steady state DHT/T ratio during 180 days of AndroGel treatment remained

within normal limits (as determined by the analytical laboratory involved with this

clinical trial) and ranged from 0.23 to 0.29 (5 G/day) and from 0.27 to 0.33 (10 G/day).

Excretion

About 90% of a dose of testosterone given intramuscularly is excreted in the urine

as glucuronic and sulfuric acid conjugates of testosterone and its metabolites; about

6% of a dose is excreted in the feces, mostly in the unconjugated form. Inactivation

of testosterone occurs primarily in the liver.

Special Populations

In patients treated with AndroGel, there are no observed differences in the average

daily serum testosterone concentration at steady-state based on age, cause of hypogonadism

or body mass index. No formal studies were conducted involving patients with renal

or hepatic insufficiencies.

Clinical Studies

AndroGel 1% was evaluated in a multicenter, randomized, parallel-group, active-controlled,

180-day trial in 227 hypogonadal men. The study was conducted in 2 phases. During

the Initial Treatment Period (Days 1-90), 73 patients were randomized to AndroGel

5 G daily (to deliver 50 mg testosterone), 78 patients to AndroGel 10 G daily (to

deliver 100 mg testosterone), and 76 patients to a non-scrotal testosterone transdermal

system (5 mg daily). The study was double-blind for dose of AndroGel but open-label

for active control. Patients who were originally randomized to AndroGel and who had

single-sample serum testosterone levels above or below the normal range on Day 60

were titrated to 7.5 G daily (to deliver 75 mg testosterone) on Day 91. During the

Extended Treatment Period (Days 91-180), 51 patients continued on AndroGel 5 G daily,

52 patients continued on AndroGel 10 G daily, 41 patients continued on a non-scrotal

testosterone transdermal system (5 mg daily), and 40 patients received AndroGel 7.5

G daily.

Mean peak, trough and average serum testosterone concentrations within the normal

range (298-1043 ng/dL) were achieved on the first day of treatment with doses of 5

G and 10 G. In patients continuing on AndroGel 5 G and 10 G, these mean testosterone

levels were maintained within the normal range for the 180-day duration of the study.

Figure 2 summarizes the 24-hour pharmacokinetic profiles of testosterone administered

as AndroGel for 30, 90 and 180 days. Testosterone concentrations were maintained

as long as the patient continued to properly apply the prescribed AndroGel treatment.

Table 1 summarizes the mean testosterone concentrations on Treatment Day 180 for patients

receiving 5 G, 7.5 G, or 10 G of AndroGel. The 7.5 G dose produced mean concentrations

intermediate to those produced by 5 G and 10 G of AndroGel.

Of 129 hypogonadal men who were appropriately titrated with AndroGel and who had

sufficient data for analysis, 87% achieved an average serum testosterone level within

the normal range on Treatment Day 180.

AndroGel 5 G/day and 10 G/day resulted in significant increases over time in total

body mass and total body lean mass, while total body fat mass and the percent body

fat decreased significantly. These changes were maintained for 180 days of treatment.

Changes in the 7.5 G dose group were similar. Bone mineral density in both hip and

spine increased significantly from Baseline to Day 180 with 10 G AndroGel.

AndroGel treatment at 5 G/day and 10 G/day for 90 days produced significant improvement

in libido (measured by sexual motivation, sexual activity and enjoyment of sexual

activity as assessed by patient responses to a questionnaire). The degree of penile

erection as subjectively estimated by the patients, increased with AndroGel treatment,

as did the subjective score for satisfactory duration of erection. AndroGel treatment

at 5 G/day and 10 G/day produced positive effects on mood and fatigue. Similar changes

were seen after 180 days of treatment and in the group treated with the 7.5 G dose.

DHT concentrations increased in parallel with testosterone concentrations at AndroGel

doses of 5 G/day and 10 G/day, but the DHT/T ratio stayed within the normal range,

indicating enhanced availability of the major physiologically active androgen. Serum

estradiol (E2) concentrations increased significantly within 30 days of starting treatment

with AndroGel 5 or 10 G/day and remained elevated throughout the treatment period

but remained within the normal range for eugonadal men. Serum levels of SHBG decreased

very slightly (1 to 11%) during AndroGel treatment. In men with hypergonadotropic

hypogonadism, serum levels of LH and FSH fell in a dose- and time-dependent manner

during treatment with AndroGel.

Potential for testosterone transfer:

The potential for dermal testosterone transfer following AndroGel use was evaluated

in a clinical study between males dosed with AndroGel and their untreated female

partners. Two to 12 hours after AndroGel (10 G) application by the male subjects,

the couples (N=38 couples) engaged in daily, 15-minute sessions of vigorous skin-to-skin

contact so that the female partners gained maximum exposure to the AndroGel application

sites. Under these study conditions, all unprotected female partners had a serum testosterone

concentration >2 times the baseline value at some time during the study. When a shirt

covered the application site(s), the transfer of testosterone from the males to the

female partners was completely prevented.

INDICATIONS AND USAGE

AndroGel is indicated for replacement therapy in males for conditions associated

with a deficiency or absence of endogenous testosterone:

1. Primary hypogonadism (congenital or acquired)--testicular failure due to cryptorchidism,

bilateral torsion, orchitis, vanishing testis syndrome, orchiectomy, Klinefelter's

syndrome, chemotherapy, or toxic damage from alcohol or heavy metals. These men usually

have low serum testosterone levels and gonadotropins (FSH, LH) above the normal range.

2. Hypogonadotropic hypogonadism (congenital or acquired)--idiopathic gonadotropin

or luteinizing hormone-releasing hormone (LHRH) deficiency or pituitary-hypothalamic

injury from tumors, trauma, or radiation. These men have low testosterone serum levels

but have gonadotropins in the normal or low range.

AndroGel has not been clinically evaluated in males under 18 years of age.

CONTRAINDICATIONS

Androgens are contraindicated in men with carcinoma of the breast or known or suspected

carcinoma of the prostate.

AndroGel is not indicated for use in women, has not been evaluated in women, and

must not be used in women.

Pregnant women should avoid skin contact with AndroGel application sites in men.

Testosterone may cause fetal harm. In the event that unwashed or unclothed skin to

which AndroGel has been applied does come in direct contact with the skin of a pregnant

woman, the general area of contact on the woman should be washed with soap and water

as soon as possible. In vitro studies show that residual testosterone is removed from the skin surface by washing

with soap and water.

AndroGel should not be used in patients with known hypersensitivity to any of its

ingredients.

WARNINGS

1. Prolonged use of high doses of orally active 17-alpha-alkyl androgens (e.g., methyltestosterone)

has been associated with serious hepatic adverse effects (peliosis hepatitis, hepatic

neoplasms, cholestatic hepatitis, and jaundice). Peliosis hepatitis can be a life-threatening

or fatal complication. Long-term therapy with testosterone enanthate, which elevates

blood levels for prolonged periods, has produced multiple hepatic adenomas. Testosterone

is not known to produce these adverse effects.

2. Geriatric patients treated with androgens may be at an increased risk for the development

of prostatic hyperplasia and prostatic carcinoma.

3. Geriatric patients and other patients with clinical or demographic characteristics

that are recognized to be associated with an increased risk of prostate cancer should

be evaluated for the presence of prostate cancer prior to initiation of testosterone

replacement therapy. In men receiving testosterone replacement therapy, surveillance

for prostate cancer should be consistent with current practices for eugonadal men

(see PRECAUTIONS: Carcinogenesis, Mutagenesis, Impairment of Fertility and Laboratory

Tests).

4. Edema with or without congestive heart failure may be a serious complication in

patients with preexisting cardiac, renal, or hepatic disease. In addition to discontinuation

of the drug, diuretic therapy may be required.

5. Gynecomastia frequently develops and occasionally persists in patients being treated

for hypogonadism.

6. The treatment of hypogonadal men with testosterone esters may potentiate sleep

apnea in some patients, especially those with risk factors such as obesity or chronic

lung diseases.

PRECAUTIONS

Transfer of testosterone to another person can occur when vigorous skin-to-skin contact

is made with the application site (see Clinical Studies). The following precautions

are recommended to minimize potential transfer of testosterone from AndroGel-treated

skin to another person:

Patients should wash their hands immediately with soap and water after application

of AndroGel.

Patients should cover the application site(s) with clothing after the gel has dried

(e.g. a shirt).

In the event that unwashed or unclothed skin to which AndroGel has been applied does

come in direct contact with the skin of another person, the general area of contact

on the other person should be washed with soap and water as soon as possible. In vitro studies show that residual testosterone is removed from the skin surface by washing

with soap and water.

Changes in body hair distribution, significant increase in acne, or other signs of

virilization of the female partner should be brought to the attention of a physician.

General

The physician should instruct patients to report any of the following:

Too frequent or persistent erections of the penis.

Any nausea, vomiting, changes in skin color, or ankle swelling.

Breathing disturbances, including those associated with sleep.

Information for Patients

Advise patients to carefully read the information brochure that accompanies each carton

of 30 AndroGel single-use packets.

Advise patients of the following:

AndroGel should not be applied to the scrotum.

AndroGel should be applied once daily to clean dry skin.

After application of AndroGel, it is currently unknown for how long showering or

swimming should be delayed. For optimal absorption of testosterone, it appears reasonable

to wait at least 5-6 hours after application prior to showering or swimming. Nevertheless,

showering or swimming after just 1 hour should have a minimal effect on the amount

of AndroGel absorbed if done very infrequently.

Laboratory Tests

1. Hemoglobin and hematocrit levels should be checked periodically (to detect polycythemia)

in patients on long-term androgen therapy.

2. Liver function, prostatic specific antigen, cholesterol, and high-density lipoprotein

should be checked periodically.

3. To ensure proper dosing, serum testosterone concentrations should be measured (see

DOSAGE AND ADMINISTRATION).

Drug Interactions

Oxyphenbutazone: Concurrent administration of oxyphenbutazone and androgens may result

in elevated serum levels of oxyphenbutazone.

Insulin: In diabetic patients, the metabolic effects of androgens may decrease blood

glucose and, therefore, insulin requirements.

Propranolol: In a published pharmacokinetic study of an injectable testosterone product,

administration of testosterone cypionate led to an increased clearance of propranolol

in the majority of men tested.

Corticosteroids: The concurrent administration of testosterone with ACTH or corticosteroids

may enhance edema formation; thus these drugs should be administered cautiously, particularly

in patients with cardiac or hepatic disease.

Drug/Laboratory Test Interactions

Androgens may decrease levels of thyroxin-binding globulin, resulting in decreased

total T4 serum levels and increased resin uptake of T3 and T4. Free thyroid hormone

levels remain unchanged, however, and there is no clinical evidence of thyroid dysfunction.

Carcinogenesis, Mutagenesis, Impairment of Fertility

Animal Data: Testosterone has been tested by subcutaneous injection and implantation

in mice and rats. In mice, the implant induced cervical-uterine tumors, which metastasized

in some cases. There is suggestive evidence that injection of testosterone into some

strains of female mice increases their susceptibility to hepatoma. Testosterone is

also known to increase the number of tumors and decrease the degree of differentiation

of chemically induced carcinomas of the liver in rats.

Human Data: There are rare reports of hepatocellular carcinoma in patients receiving

long-term oral therapy with androgens in high doses. Withdrawal of the drugs did not

lead to regression of the tumors in all cases.

Geriatric patients treated with androgens may be at an increased risk for the development

of prostatic hyperplasia and prostatic carcinoma.

Geriatric patients and other patients with clinical or demographic characteristics

that are recognized to be associated with an increased risk of prostate cancer should

be evaluated for the presence of prostate cancer prior to initiation of testosterone

replacement therapy.

In men receiving testosterone replacement therapy, surveillance for prostate cancer

should be consistent with current practices for eugonadal men.

Pregnancy Category X (see Contraindications)--Teratogenic Effects: AndroGel is not

indicated for women and must not be used in women.

Nursing Mothers: AndroGel is not indicated for women and must not be used in women.

Pediatric Use: Safety and efficacy of AndroGel in pediatric patients have not been

established.

ADVERSE REACTIONS

In a controlled clinical study, 154 patients were treated with AndroGel for up to

6 months (see Clinical Studies). Adverse Events possibly, probably or definitely related

to the use of AndroGel and reported by >1% of the patients are listed in Table 2.

*Lab test abnormal occurred in nine patients with one or more of the following events: elevated hemoglobin

or hematocrit, hyperlipidemia, elevated triglycerides, hypokalemia, decreased HDL,

elevated glucose, elevated creatinine, or elevated total bilirubin.

**Prostate disorders included five patients with enlarged prostate, one patient with BPH, and one patient

with elevated PSA results.

The following adverse events possibly related to the use of AndroGel occurred in

fewer than 1% of patients: amnesia, anxiety, discolored hair, dizziness, dry skin,

hirsutism, hostility, impaired urination, paresthesia, penis disorder, peripheral

edema, sweating, and vasodilation.

In this clinical trial of AndroGel, skin reactions at the site of application were

occasionally reported with AndroGel, but none was severe enough to require treatment

or discontinuation of drug.

Six (4%) patients in this trial had adverse events that led to discontinuation of

AndroGel. These events included the following: cerebral hemorrhage, convulsion (neither

of which were considered related to AndroGel administration), depression, sadness,

memory loss, elevated prostate specific antigen and hypertension. No AndroGel patients

discontinued due to skin reactions.

In an uncontrolled pharmacokinetic study of 10 patients, two had adverse events associated

with AndroGel; these were asthenia and depression in one patient and increased libido

and hyperkinesia in the other. Among 17 patients in foreign clinical studies there

was 1 instance each of acne, erythema and benign prostate adenoma associated with

a 2.5% testosterone gel formulation applied dermally.

One hundred six (106) patients have received AndroGel for up to 12 months in a long-term

follow-up study for patients who completed the controlled clinical trial. The preliminary

safety results from this study are consistent with those reported for the controlled

clinical trial. Table 3 summarizes those adverse events possibly, probably or definitely

related to the use of AndroGel and reported by at least 1% of the total number of

patients during long-term exposure to AndroGel.

*Lab test abnormal included one patient each with elevated GGTP, elevated hematocrit and hemoglobin,

increased total bilirubin, worsened hyperlipidemia, decreased HDL, and hypokalemia.

**Prostate disorders included enlarged prostate, elevated PSA results, and in one patient, a new diagnosis

of prostate cancer; three patients (one taking 7.5 G daily and two taking 10 G daily)

discontinued AndroGel treatment during the long-term study because of such disorders.

DRUG ABUSE AND DEPENDENCE

AndroGel contains testosterone, a Schedule III controlled substance as defined by

the Anabolic Steroids Control Act.

Oral ingestion of AndroGel will not result in clinically significant serum testosterone

concentrations due to extensive first-pass metabolism.

OVERDOSAGE

There is one report of acute overdosage by injection of testosterone enanthate: testosterone

levels of up to 11,400 ng/dL were implicated in a cerebrovascular accident.

DOSAGE AND ADMINISTRATION

The recommended starting dose of AndroGel 1% is 5 G (to deliver 50 mg of testosterone)

applied once daily (preferably in the morning) to clean, dry, intact skin of the shoulders

and upper arms and/or abdomen. Upon opening the packet(s), the entire contents should

be squeezed into the palm of the hand and immediately applied to the application sites.

Application sites should be allowed to dry for a few minutes prior to dressing. Hands

should be washed with soap and water after AndroGel has been applied.

Do not apply AndroGel to the genitals.

Serum testosterone levels should be measured approximately 14 days after initiation

of therapy to ensure proper dosing. If the serum testosterone concentration is below

the normal range, or if the desired clinical response is not achieved, the daily AndroGel

1% dose may be increased from 5 G to 7.5 G and from 7.5 G to 10 G as instructed by

the physician.

HOW SUPPLIED

AndroGel contains testosterone, a Schedule III controlled substance as defined by

the Anabolic Steroids Control Act.

AndroGel is supplied in unit-dose aluminum foil packets in cartons of 30. Each packet

contains 2.5 G or 5.0 G of gel to deliver 25 mg or 50 mg of testosterone, respectively,

and is supplied as follows:

NDC Number

Strength

Package Size

0051-8425-30

1% (25 mg)

30 packets: 2.5 G per packet

0051-8450-30

1% (50 mg)

30 packets: 5 G per packet

Storage

Store at controlled room temperature 20-25°C (68-77°F) [see USP].

Disposal

Used AndroGel packets should be discarded in household trash in a manner that prevents

accidental application or ingestion by children or pets.

Rx Only

Manufactured by Laboratoires Besins Iscovesco

Montrouge, France

For:

Unimed Pharmaceuticals, Inc.

Buffalo Grove, IL 60089-1864, USA

2/28/00