HUMATROPE- somatropin kit

HUMATROPE by

Drug Labeling and Warnings

HUMATROPE by is a Prescription medication manufactured, distributed, or labeled by Eli Lilly and Company. Drug facts, warnings, and ingredients follow.

Drug Details [pdf]

HIGHLIGHTS OF PRESCRIBING INFORMATION
These highlights do not include all the information needed to use HUMATROPE safely and effectively. See full prescribing information for HUMATROPE.
HUMATROPE® (somatropin) for injection, for subcutaneous use
Initial U.S. Approval: 1987

RECENT MAJOR CHANGES

Indications and Usage (1) 10/2019

Dosage and Administration (2) 10/2019

Contraindications (4) 10/2019

Warnings and Precautions (5) 10/2019
INDICATIONS AND USAGE
HUMATROPE is a recombinant human growth hormone indicated for:
- Pediatric Patients: growth failure due to inadequate secretion of endogenous growth hormone (GH); short stature associated with Turner syndrome; Idiopathic Short Stature (ISS), height standard deviation score (SDS) <-2.25, and associated with growth rates unlikely to permit attainment of adult height in the normal range; short stature or growth failure in short stature homeobox-containing gene (SHOX) deficiency; short stature born small for gestational age (SGA) with no catch-up growth by 2 years to 4 years of age.(1.1)
- Adult Patients: replacement of endogenous GH in adults with GH deficiency. (1.2)
DOSAGE AND ADMINISTRATION
- Administer by subcutaneous injection to the back of upper arm, abdomen, buttock, or thigh with regular rotation of injection sites. (2.1)
- Pediatric Dosage - divide the calculated weekly dosage into equal doses given either 6, or 7 days per week.
  
  GHD: 0.18 mg/kg/week to 0.3 mg/kg/week. (2.2)
  
  Turner Syndrome: Up to 0.375 mg/kg/week. (2.2)
  
  ISS: Up to 0.37 mg/kg/week. (2.2)
  
  SHOX Deficiency: 0.35 mg/kg/week. (2.2)
  
  SGA: Up to 0.47 mg/kg/week. (2.2)
- Adult Dosage - Either of the following two dosing regimens may be used:
  
  Non-weight based dosing: Initiate with a dose of approximately 0.2 mg/day (range, 0.15 mg/day-0.3 mg/day) and increase the dose every 1-2 months by increments of approximately 0.1 mg/day-0.2 mg/day, according to individual patient requirements (2.3)
  
  Weight-based dosing (Not recommended for obese patients): Initiate at 0.006 mg/kg daily and increase the dose according to individual patient requirements to a maximum of 0.0125 mg/kg daily (2.3)
- See Full Prescribing Information for reconstitution instructions. (2.4, 2.5)
DOSAGE FORMS AND STRENGTHS
HUMATROPE for injection available as:
- 5 mg vial and 5-mL vial of Diluent for HUMATROPE. (3)
- 6 mg, 12 mg, and 24 mg cartridge with prefilled syringe of Diluent for HUMATROPE. (3)
CONTRAINDICATIONS
- Acute critical illness. (4)
- Pediatric patients with Prader-Willi syndrome who are severely obese, have history of upper airway obstruction or sleep apnea, or have severe respiratory impairment due to risk of sudden death. (4)
- Active malignancy. (4)
- Hypersensitivity to somatropin or excipients. (4)
- Active proliferative or severe non-proliferative diabetic retinopathy. (4)
- Pediatric patients with closed epiphyses. (4)
WARNINGS AND PRECAUTIONS
- Increased Risk of Neoplasm: Second neoplasms have occurred in childhood cancer survivors. Monitor patients with preexisting tumors for progression or recurrence. (5.3)
- Glucose Intolerance and Diabetes Mellitus: HUMATROPE may decrease insulin sensitivity, particularly at higher doses. Monitor glucose levels periodically in all patients receiving HUMATROPE, especially in patients with existing diabetes mellitus or at risk for development. (5.4)
- Intracranial Hypertension (IH): Has been reported usually within 8 weeks of initiation. Perform fundoscopic examinations prior to initiation and periodically thereafter. If papilledema occurs, stop treatment. (5.5)
- Hypersensitivity: Serious hypersensitivity reactions may occur. In the event of an allergic reaction, seek prompt medical attention. (5.6)
- Fluid Retention: May occur in adults and may be dose dependent. (5.7)
- Hypoadrenalism: Monitor patients for reduced serum cortisol levels and/or need for glucocorticoid dose increases in those with known hypoadrenalism. (5.8)
- Hypothyroidism: Monitor thyroid function periodically as hypothyroidism may occur or worsen after initiation of somatropin. (5.9)
- Slipped Capital Femoral Epiphysis in Pediatric Patients: May occur; evaluate patients with onset of a limp or hip/knee pain. (5.10)
- Progression of Preexisting Scoliosis in Pediatric Patients: Monitor patients with scoliosis for progression. (5.11)
- Pancreatitis: Has been reported; consider pancreatitis in patients with abdominal pain, especially pediatric patients. (5.12)
ADVERSE REACTIONS

Common adverse reactions reported in adult and pediatric patients include: upper respiratory infection, fever, pharyngitis, headache, otitis media, edema, arthralgia, paresthesia, myalgia, carpal tunnel syndrome, peripheral edema, flu syndrome, hypothyroidism, hyperglycemia, and impaired glucose tolerance. (6)

To report SUSPECTED ADVERSE REACTIONS, contact Eli Lilly and Company at 1-800-LillyRx (1-800-545-5979) or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch.
DRUG INTERACTIONS
- Replacement Glucocorticoid Treatment: Patients treated with glucocorticoids for hypoadrenalism may require an increase in their maintenance or stress doses following initiation of HUMATROPE. (7)
- Non-Replacement Glucocorticoid Treament in Pediatric Patients: Adjust glucocorticoid dosing in pediatric patients receiving glucocorticoid treatment to avoid both hypoadrenalism and an inhibitory effect on growth. (7)
- Cytochrome P450-Metabolized Drugs: HUMATROPE may alter the clearance. Monitor carefully if used with HUMATROPE. (7)
- Oral Estrogen: Patients may require larger doses of HUMATROPE. (7)
- Insulin and/or Other Hypoglycemic Agents: Dose adjustment of insulin or hypoglycemic agent may be required. (5.4, 7)
See 17 for PATIENT COUNSELING INFORMATION.

Revised: 10/2019
Table of Contents

FULL PRESCRIBING INFORMATION: CONTENTS*

1 INDICATIONS AND USAGE

1.1 Pediatric Patients

1.2 Adult Patients

2 DOSAGE AND ADMINISTRATION

2.1 Administration and Use Instructions

2.2 Pediatric Dosage

2.3 Adult Dosage

2.4 Reconstitution of Vials

2.5 Reconstitution of Cartridges

3 DOSAGE FORMS AND STRENGTHS

4 CONTRAINDICATIONS

5 WARNINGS AND PRECAUTIONS

5.1 Acute Critical Illness

5.2 Sudden Death in Pediatric Patients with Prader-Willi Syndrome

5.3 Increased Risk of Neoplasms

5.4 Glucose Intolerance and Diabetes Mellitus

5.5 Intracranial Hypertension

5.6 Severe Hypersensitivity

5.7 Fluid Retention

5.8 Hypoadrenalism

5.9 Hypothyroidism

5.10 Slipped Capital Femoral Epiphysis in Pediatric Patients

5.11 Progression of Preexisting Scoliosis in Pediatric Patients

5.12 Pancreatitis

5.13 Lipoatrophy

5.14 Laboratory Tests

6 ADVERSE REACTIONS

6.1 Clinical Studies Experience

6.2 Immunogenicity

6.3 Postmarketing Experience

7 DRUG INTERACTIONS

8 USE IN SPECIFIC POPULATIONS

8.1 Pregnancy

8.2 Lactation

8.4 Pediatric Use

8.5 Geriatric Use

9 DRUG ABUSE AND DEPENDENCE

9.1 Controlled Substance

9.2 Abuse

9.3 Dependence

10 OVERDOSAGE

11 DESCRIPTION

12 CLINICAL PHARMACOLOGY

12.1 Mechanism of Action

12.2 Pharmacodynamics

12.3 Pharmacokinetics

13 NONCLINICAL TOXICOLOGY

13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

14 CLINICAL STUDIES

14.1 Pediatric Patients with Growth Failure Due to Inadequate Secretion of Endogenous Growth Hormone

14.2 Pediatric Patients with Short Stature Associated with Turner Syndrome

14.3 Pediatric Patients with Idiopathic Short Stature (ISS)

14.4 Pediatric Patients with Short Stature or Growth Failure in SHOX Deficiency

14.5 Pediatric Patients with Short Stature Born Small for Gestational Age (SGA) Who Fail to Demonstrate Catch-up Growth by Age 2 - 4 Years

14.6 Adult Patients with Growth Hormone Deficiency

16 HOW SUPPLIED/STORAGE AND HANDLING

16.1 How Supplied

16.2 Storage and Handling

17 PATIENT COUNSELING INFORMATION

* Sections or subsections omitted from the full prescribing information are not listed.

1 INDICATIONS AND USAGE

1.1 Pediatric Patients

HUMATROPE is indicated for the treatment of pediatric patients with:

growth failure due to inadequate secretion of endogenous growth hormone (GH),
short stature associated with Turner syndrome,
Idiopathic Short Stature (ISS), height standard deviation score (SDS) <-2.25, and associated with growth rates unlikely to permit attainment of adult height in the normal range,
short stature or growth failure in short stature homeobox-containing gene (SHOX) deficiency,
short stature born small for gestational age (SGA) with no catch-up growth by 2 years to 4 years of age.

1.2 Adult Patients

HUMATROPE is indicated for the replacement of endogenous GH in adults with GH deficiency.

2 DOSAGE AND ADMINISTRATION

2.1 Administration and Use Instructions

Therapy with HUMATROPE should be supervised by a physician who is experienced in the diagnosis and management of patients with the conditions for which HUMATROPE is indicated [see Indications and Usage (1)].
Fundoscopic examination should be performed routinely before initiating treatment with HUMATROPE to exclude preexisting papilledema, and periodically thereafter [see Warnings and Precautions (5.5)].
Leave HUMATROPE at room temperature for 10 minutes prior to administration.
Administer HUMATROPE by subcutaneous injection to the back of the upper arm, abdomen, buttock, or thigh with regular rotation of injection sites to avoid lipoatrophy.

2.2 Pediatric Dosage

Individualize dosage for each patient based on the growth response.
Divide the calculated weekly HUMATROPE dosage into equal doses given either 6 or 7 days per week.
The recommended weekly dose in milligrams (mg) per kilogram (kg) of body weight for pediatric patients is:
- Pediatric GH Deficiency: 0.18 mg/kg/week to 0.3 mg/kg/week (0.026 to 0.043 mg/kg/day)
- Turner Syndrome: Up to 0.375 mg/kg/week (up to.054 mg/kg/day)
- Idiopathic Short Stature: Up to 0.37 mg/kg/week (up to 0.053 mg/kg/day)
- SHOX Deficiency: 0.35 mg/kg/week (0.05 mg/kg/day)
- Small for Gestational Age (SGA): Up to 0.47 mg/kg/week (up to 0.067 mg/kg/day)
  - In very short pediatric patients, height SDS less than -3, and older pubertal pediatric patients consider initiating treatment with a larger dose of HUMATROPE (up to 0.067 mg/kg/day). Consider a gradual reduction in dosage if substantial catch-up growth is observed during the first few years of therapy. In pediatric patients less than 4 years of age with less severe short stature, baseline height SDS values between -2 and -3, consider initiating treatment at 0.033 mg/kg/day and titrate the dose as needed.
Assess compliance and evaluate other causes of poor growth such as hypothyroidism, under-nutrition, advanced bone age and antibodies to recombinant human GH if patients experience failure to increase height velocity, particularly during the first year of treatment.
Discontinue HUMATROPE for stimulation of linear growth once epiphyseal fusion has occurred [see Contraindications (4)].

2.3 Adult Dosage

Patients who were treated with somatropin for GH deficiency in childhood and whose epiphyses are closed should be reevaluated before continuation of somatropin for GH deficient adults.
Consider using a lower starting dose and smaller dose increment increases for geriatric patients as they may be at increased risk for adverse reactions with HUMATROPE than younger individuals [see Use in Specific Populations (8.5)].
Women may require higher doses and patients receiving oral estrogen may require higher doses [see Drug Interactions (7)].
Administer the prescribed dose daily.
Either of two HUMATROPE dosing regimens may be used:
- Non-weight based:
  - Initiate HUMATROPE with a dose of approximately 0.2 mg/day (range, 0.15 mg/day to 0.3 mg/day) and increase the dose every 1-2 months by increments of approximately 0.1 mg/day to 0.2 mg/day, according to individual patient requirements based on the clinical response and serum insulin-like growth factor 1 (IGF-1) concentrations.
  - Use the patient's clinical response, adverse reactions, and determination of age- and gender-adjusted serum IGF-1 concentrations as guidance in dose titration.
  - Maintenance dosages will vary considerably from person to person, and between male and female patients.
- Weight-based:
  - Initiate HUMATROPE at 0.006 mg/kg daily and increase the dose according to individual patient requirements to a maximum of 0.0125 mg/kg daily.
  - Use the patient's clinical response, adverse reactions, and determination of age- and gender-adjusted serum IGF-1 concentrations as guidance in dose titration.
  - Maintenance dosages will vary considerably from person to person, and between male and female patients
  - Not recommended for obese patients as they are more likely to experience adverse reactions with this regimen.

2.4 Reconstitution of Vials

Reconstitute the 5-mg vial of HUMATROPE with 1.5 to 5 mL of Diluent for HUMATROPE.
- Inject the diluent into the vial by aiming the stream of liquid gently against the vial wall. Swirl the vial (do not shake) with a gentle rotary motion until the powder is completely dissolved into liquid and the solution is clear.
- Inspect visually for particulate matter and discoloration. If the resulting solution is cloudy or contains particulate matter do not use.
Vials of HUMATROPE are stable for up to 14 days when reconstituted with Diluent for HUMATROPE and refrigerated at 36° to 46°F (2° to 8°C). Do not leave reconstituted vials at room temperature more than 30 minutes per day. Avoid freezing the reconstituted vial of HUMATROPE. Protect HUMATROPE from light during storage.
For patients with known hypersensitivity to the Diluent for HUMATROPE [see Warnings and Precautions (5.6)], reconstitute the vial with Sterile Water for Injection. Use only one dose per vial, use immediately and discard the unused portion.

2.5 Reconstitution of Cartridges

Each HUMATROPE cartridge is designed for use only with the appropriate corresponding HumatroPen®.
- Reconstitute each cartridge of HUMATROPE using only the diluent syringe that accompanies the cartridge. Do not shake. The reconstituted solution should be clear.
- Inspect visually for particulate matter and discoloration. If the resulting solution is cloudy or contains particulate matter do not use.
- The somatropin concentrations for the reconstituted HUMATROPE cartridges are as follows:
  
  Cartridge Somatropin Concentration
  
  6 mg 2.08 mg/mL
  
  12 mg 4.17 mg/mL
  
  24 mg 8.33 mg/mL
Reconstituted cartridges of HUMATROPE are stable for up to 28 days when refrigerated at 36° to 46°F (2° to 8°C). Do not leave at room temperature more than 30 minutes per day. Avoid freezing the reconstituted cartridge. Protect HUMATROPE from light during storage.
For patients with known hypersensitivity to the diluent supplied with the HUMATROPE cartridge [see Warnings and Precautions (5.6)], do not use HUMATROPE cartridge. Use the HUMATROPE vial and reconstitute with Sterile Water for Injection [see Dosage and Administration (2.4)].

3 DOSAGE FORMS AND STRENGTHS

HUMATROPE for injection is a white lyophilized powder available in the following vial and cartridge sizes:

5 mg vial and a 5-mL vial of Diluent for HUMATROPE
6 mg cartridge (gold) and a prefilled syringe of Diluent for HUMATROPE
12 mg cartridge (teal) and a prefilled syringe of Diluent for HUMATROPE
24 mg cartridge (purple) and a prefilled syringe of Diluent for HUMATROPE

4 CONTRAINDICATIONS

HUMATROPE is contraindicated in patients with:

Acute critical illness after open heart surgery, abdominal surgery or multiple accidental trauma, or those with acute respiratory failure due to the risk of increased mortality with use of pharmacologic doses of somatropin [see Warnings and Precautions (5.1)].
Pediatric patients with Prader-Willi syndrome who are severely obese, have a history of upper airway obstruction or sleep apnea, or have severe respiratory impairment due to the risk of sudden death [see Warnings and Precautions (5.2)].
Active malignancy [see Warnings and Precautions (5.3)].
Known hypersensitivity to somatropin or any of the excipients in HUMATROPE. Systemic hypersensitivity reactions have been reported with postmarketing use of somatropin products [see Warnings and Precautions (5.6)].
Active proliferative or severe non-proliferative diabetic retinopathy.
Pediatric patients with closed epiphyses.

5 WARNINGS AND PRECAUTIONS

5.1 Acute Critical Illness

Increased mortality in patients with acute critical illness due to complications following open heart surgery, abdominal surgery or multiple accidental trauma, or those with acute respiratory failure has been reported after treatment with pharmacologic doses of somatropin [see Contraindications (4)]. Two placebo-controlled clinical studies in non-GH deficient adult patients (n=522) with these conditions in intensive care units revealed a significant increase in mortality (42% vs. 19%) among somatropin-treated patients (doses 5.3-8.0 mg/day) compared to those receiving placebo. The safety of continuing HUMATROPE treatment in patients receiving replacement doses for approved indications who concurrently develop these illnesses has not been established. HUMATROPE is not indicated for the treatment of non-GH deficient adults.

5.2 Sudden Death in Pediatric Patients with Prader-Willi Syndrome

There have been reports of sudden death after initiating therapy with somatropin in pediatric patients with Prader-Willi syndrome who had one or more of the following risk factors: severe obesity, history of upper airway obstruction or sleep apnea, or unidentified respiratory infection. Male patients with one or more of these factors may be at greater risk than females. Patients with Prader-Willi syndrome should be evaluated for signs of upper airway obstruction and sleep apnea before initiation of treatment with somatropin. If, during treatment with somatropin, patients show signs of upper airway obstruction (including onset of, or increased, snoring) and/or new onset sleep apnea, treatment should be interrupted. All patients with Prader-Willi syndrome treated with somatropin should also have effective weight control and be monitored for signs of respiratory infection, which should be diagnosed as early as possible and treated aggressively [see Contraindications (4)]. HUMATROPE is not indicated for the treatment of pediatric patients who have growth failure due to Prader-Willi syndrome.

5.3 Increased Risk of Neoplasms

Active Malignancy

There is an increased risk of malignancy progression with somatropin treatment in patients with active malignancy [see Contraindications (4)]. Any preexisting malignancy should be inactive and its treatment complete prior to instituting therapy with HUMATROPE. Discontinue HUMATROPE if there is evidence of recurrent activity.

Risk of Second Neoplasm in Pediatric Patients

An increased risk of a second neoplasm in pediatric cancer survivors who were treated with radiation to the brain/head and who developed subsequent GH deficiency and were treated with somatropin has been reported. Intracranial tumors, in particular meningiomas, were the most common of these second neoplasms. In adults, it is unknown whether there is any relationship between somatropin replacement therapy and CNS tumor recurrence. Monitor all patients receiving HUMATROPE who have a history of GH deficiency secondary to an intracranial neoplasm for progression or recurrence of the tumor.

New Malignancy During Treatment

Because pediatric patients with certain rare genetic causes of short stature have an increased risk of developing malignancies, thoroughly consider the risks and benefits of starting HUMATROPE in these patients. If HUMATROPE is initiated, carefully monitor patients for development of neoplasms.

Monitor all patients receiving HUMATROPE carefully for increased growth, or potential malignant changes, of preexisting nevi. Advise patients/caregivers to report marked changes in behavior, onset of headaches, vision disturbances and/or changes in skin pigmentation or changes in the appearance of pre-existing nevi.

5.4 Glucose Intolerance and Diabetes Mellitus

Treatment with somatropin may decrease insulin sensitivity, particularly at higher doses. New onset type 2 diabetes mellitus has been reported in patients taking somatropin. Previously undiagnosed impaired glucose tolerance and overt diabetes mellitus may be unmasked. Monitor glucose levels periodically in all patients receiving HUMATROPE, especially in those with risk factors for diabetes mellitus, such as obesity, Turner syndrome, or a family history of diabetes mellitus. Patients with preexisting type 1 or type 2 diabetes mellitus or impaired glucose tolerance should be monitored closely. The doses of antidiabetic agents may require adjustment when HUMATROPE is initiated.

5.5 Intracranial Hypertension

Intracranial hypertension (IH) with papilledema, visual changes, headache, nausea, and/or vomiting has been reported in a small number of patients treated with somatropin products. Symptoms usually occurred within the first eight (8) weeks after the initiation of somatropin therapy. In all reported cases, IH-associated signs and symptoms rapidly resolved after cessation of therapy or a reduction of the somatropin dose. Fundoscopic examination should be performed routinely before initiating treatment with HUMATROPE to exclude preexisting papilledema, and periodically thereafter. If papilledema is observed by fundoscopy during somatropin treatment, treatment should be stopped. If somatropin-induced IH is diagnosed, treatment with HUMATROPE can be restarted at a lower dose after IH-associated signs and symptoms have resolved. Patients with Turner syndrome may be at increased risk for the development of IH.

5.6 Severe Hypersensitivity

Serious systemic hypersensitivity reactions including anaphylactic reactions and angioedema have been reported with postmarketing use of somatropin products. Patients and caregivers should be informed that such reactions are possible and that prompt medical attention should be sought if an allergic reaction occurs. Do not use HUMATROPE in patients with known hypersensitivity to somatropin or any of the excipients in HUMATROPE. Do not use HUMATROPE cartridges or the diluent supplied with HUMATROPE vials in patients with known hypersensitivity to metacresol or glycerin [see Dosage and Administration (2.4, 2.5), Contraindications (4)].

5.7 Fluid Retention

Fluid retention during somatropin replacement therapy may frequently occur. Clinical manifestations of fluid retention (e.g. edema, arthralgia, myalgia, nerve compression syndromes including carpal tunnel syndrome/paresthesia) are usually transient and dose dependent.

5.8 Hypoadrenalism

Patients receiving somatropin therapy who have or are at risk for pituitary hormone deficiency(s) may be at risk for reduced serum cortisol levels and/or unmasking of central (secondary) hypoadrenalism. In addition, patients treated with glucocorticoid replacement for previously diagnosed hypoadrenalism may require an increase in their maintenance or stress doses following initiation of HUMATROPE treatment. Monitor patients for reduced serum cortisol levels and/or need for glucocorticoid dose increases in those with known hypoadrenalism [see Drug Interactions (7)].

5.9 Hypothyroidism

Undiagnosed/untreated hypothyroidism may prevent an optimal response to HUMATROPE, in particular, the growth response in pediatric patients. Patients with Turner syndrome have an inherently increased risk of developing autoimmune thyroid disease and primary hypothyroidism. In patients with GH deficiency, central (secondary) hypothyroidism may first become evident or worsen during somatropin treatment. Therefore, patients treated with somatropin should have periodic thyroid function tests performed, and thyroid hormone replacement therapy should be initiated or appropriately adjusted when indicated.

5.10 Slipped Capital Femoral Epiphysis in Pediatric Patients

Slipped capital femoral epiphysis may occur more frequently in patients undergoing rapid growth. Evaluate pediatric patients with the onset of a limp or complaints of hip or knee pain.

5.11 Progression of Preexisting Scoliosis in Pediatric Patients

Somatropin increases the growth rate, and progression of existing scoliosis can occur in patients who experience rapid growth. Somatropin has not been shown to increase the occurrence of scoliosis. Monitor patients with a history of scoliosis for progression of scoliosis.

5.12 Pancreatitis

Cases of pancreatitis have been reported in pediatric patients and adults receiving somatropin products. The risk may be greater risk in pediatric patients compared with adults. Published literature indicates that girls who have Turner syndrome may be at greater risk than other pediatric patients receiving somatropin products. Pancreatitis should be considered in patients who develop abdominal pain.

5.13 Lipoatrophy

When somatropin products are administered subcutaneously at the same site over a long period of time, tissue atrophy may result. Rotate injection sites when administering HUMATROPE to reduce this risk [see Dosage and Administration (2.1)].

5.14 Laboratory Tests

Serum levels of inorganic phosphorus, alkaline phosphatase, parathyroid hormone and IGF-I may increase after HUMATROPE therapy.

6 ADVERSE REACTIONS

The following important adverse reactions are also described elsewhere in the labeling:

Increased mortality in patients with acute critical illness [see Warnings and Precautions (5.1)]
Fatalities in children with Prader-Willi syndrome [see Warnings and Precautions (5.2)]
Neoplasms [see Warnings and Precautions (5.3)]
Glucose intolerance and diabetes mellitus [see Warnings and Precautions (5.4)]
Intracranial hypertension [see Warnings and Precautions (5.5)]
Severe hypersensitivity [see Warnings and Precautions (5.6)]
Fluid retention [see Warnings and Precautions (5.7)]
Hypoadrenalism [see Warnings and Precautions (5.8)]
Hypothyroidism [see Warnings and Precautions (5.9)]
Slipped capital femoral epiphysis in pediatric patients [see Warnings and Precautions (5.10)]
Progression of preexisting scoliosis in pediatric patients [see Warnings and Precautions (5.11)]
Pancreatitis [see Warnings and Precautions (5.12)]
Lipoatrophy [see Warnings and Precautions (5.14)]

6.1 Clinical Studies Experience

Because clinical studies are conducted under varying conditions, adverse reaction rates observed during the clinical studies performed with one somatropin formulation cannot always be directly compared to the rates observed during the clinical studies performed with a different somatropin formulation, and may not reflect the adverse reaction rates observed in practice.

Pediatric Patients

Growth Failure Due to Inadequate Secretion of Endogenous Growth Hormone

In an uncontrolled open-label study, 314 treatment-naive children aged >2 years who had GH deficiency were treated with HUMATROPE (0.06 mg/kg 3 times per week) for up to 8 years. Adverse reactions of special interest are reported in Table 1.

Table 1: Adverse Reactions of Special Interest Occurring in Humatrope-Treated Patients with Growth Failure Due to Inadequate Secretion of Endogenous Growth Hormone in an Open-label Study for Up to 8 Years
a Dose=0.06 mg/kg 3 times per week for up to 8 years.
b n=1
Adverse Reaction	HUMATROPEa (n=314)
Hypothyroidism	25%
Allergic reaction	11%
Arthralgia	6%
Bone disorder	4%
Edema	4%
Injection site pain/reaction	4%
Neoplasm/tumor	2%
Cardiovascular disorders	1%
Thyroid disorders	1%
Intracranial hypertension	0%b

Short Stature Associated with Turner Syndrome

In a randomized, concurrent-controlled (untreated), open-label study until attainment of adult height, the adverse reactions of special interest occurring in 74 patients treated with Humatrope at dose 0.3 mg/kg/week (mean duration 4.1 years) and in 62 untreated patients (mean duration 3.7 years) are reported in Table 2. A similar increase in otitis media was observed in an 18-month placebo-controlled study.

Table 2: Adverse Reactions of Special Interest Occurring in Patients with Turner Syndrome in an Open-label Study Until Attainment of Adult Height
	Untreated (n=62)	HUMATROPE (n=74)
Surgical procedure	27%	45%
Otitis media	26%	43%
Ear disorders	5%	18%

Idiopathic Short Stature

Adverse reactions occurring in a randomized, placebo-controlled study of HUMATROPE treatment (0.22 mg/kg/week) until attainment of adult height (mean duration of HUMATROPE treatment 3.7 years, mean duration of placebo treatment 3.3 years) are reported in Table 3. Mean fasting serum insulin concentration increased by 10% in the HUMATROPE treatment group at the end of treatment relative to baseline, but remained within the normal reference range.

Table 3: Adverse Reactions Occurring in Patients with Idiopathic Short Stature Treated with HUMATROPE in a Randomized Placebo-controlled Study
	Placebo (n=31)	HUMATROPE (n=37)
Scoliosis	13%	19%
Otitis media	7%	16%
Hyperlipidemia	3%	8%
Gynecomastia	3%	5%
Hip pain	0	3%
Arthralgia	3%	11%
Arthrosis	7%	11%
Myalgia	13%	24%
Hypertension	0	3%

In a dose-response study (239 patients treated for 2 years), among HUMATROPE dose groups [0.24 mg/kg/week (n=78), 0.37 mg/kg/week (n=83), 0.24 mg/kg/week for the first year and 0.37 mg/kg/week thereafter (n=78)], mean fasting blood glucose, mean glycosylated hemoglobin, and the incidence of elevated fasting blood glucose concentrations were similar. One patient developed glucose intolerance and high serum HbA1c.

Short Stature or Growth Failure in SHOX Deficiency

Adverse reactions of special interest from a 2-year randomized, open-label study with HUMATROPE (0.35 mg/kg/wk) compared to no treatment are presented in Table 4. During the 2-year study period, the proportion of patients who had at least one IGF-I concentration greater than 2.0 SD above the age- and gender-appropriate mean was 10 of 27 (37%) for the HUMATROPE-treated group vs. 0 of 24 patients (0%) for the untreated group. The proportion of patients who had at least one IGFBP-3 concentration greater than 2.0 SD above the age and gender appropriate mean was 16 of 27 (59%) for the HUMATROPE treated group vs. 7 of 24 (29%) for the untreated group.

Table 4: Adverse Reactions of Special Interest Occurring in Patients with SHOX Deficiency By Treatment Group in an Open-label Study
a Percentage calculated for males only: Untreated (0/1), HUMATROPE (1/12)
	Untreated (n=25)	HUMATROPE (n=27)
Arthralgia	8%	11%
Gynecomastiaa	0%	8%
Excessive number of cutaneous nevi	0%	7%
Scoliosis	0%	47%

Small for Gestational Age (SGA) with No Catch-up Growth by Age 2-4 Years

In a 2-year, multicenter, randomized study, 193 pediatric patients were treated with 2 different HUMATROPE treatment regimens: a fixed dose of 0.067 mg/kg/day (FHD group) or an individually adjusted dose regimen (IAD group; starting dose 0.035 mg/kg/day which could be increased as early as Month 3 to 0.067 mg/kg/day based on a validated growth prediction model). Reported adverse reactions included: common childhood infectious diseases, otitis media, headaches, and slipped capital femoral epiphysis (n=1. Six patients (4 in the FHD group and 2 in the IAD group whose dose was increased from 0.035 mg/kg/day to 0.067 mg/kg/day [one at Month 3 and one at Year 1]) had impaired fasting glucose at Year 2. Two of 6 had impaired fasting glucose during the study, and one discontinued HUMATROPE at month 15 as a consequence. At study completion, 20-25% of patients had serum IGF-I SDS values > +2.

The following adverse reactions were reported from an observational study of 340 pediatric patients who received HUMATROPE with an average dosage of 0.041 mg/kg/day (maximum dose: 0.084 mg/kg/day) for an average of 3.0 years: type 2 diabetes mellitus (n=1), carpal tunnel syndrome (n=1) and an exacerbation of preexisting scoliosis (n=1).

Adult Patients

Adult-Onset GH Deficiency

In the first 6 months of controlled blinded studies during which patients received either HUMATROPE or placebo, patients who received HUMATROPE experienced an increase in edema (17% vs. 4%) and peripheral edema (12% vs. 0%). Edema, muscle pain, joint pain, and joint disorder were reported early in therapy and tended to be transient or responsive to dosage titration.

Two of 113 patients developed carpal tunnel syndrome after beginning maintenance therapy without a low dose (0.00625 mg/kg/day) lead-in phase. Symptoms abated in these patients after dosage reduction.

Adverse reactions with ≥5% overall occurrence rate during 12 or 18 months of replacement therapy with HUMATROPE are shown in Table 5 (adult-onset patients) and in Table 6 (childhood-onset patients).

Table 5: Adverse Reactions with ≥5% Overall Occurrence in Adult-Onset Growth Hormone-Deficient Patients Treated with HUMATROPE for 18 Months as Compared with 6-Month Placebo and 12-Month HUMATROPE Exposure
Adverse Reaction	18 Months Exposure [Placebo (6 Months)/Humatrope (12 Months)] (n=44)	18 Months Humatrope Exposure (n=52)
Edema	11%	21%
Arthralgia	14%	17%
Paresthesia	14%	17%
Myalgia	9%	14%
Pain	14%	14%
Peripheral edema	18%	12%
Headache	7%	8%
Hypertension	5%	8%
Joint disorder	2%	6%
Rhinitis	11%	13%
Back pain	9%	10%
Acne	0%	6%
Surgical procedure	2%	6%
Flu syndrome	7%	4%

Childhood-Onset GH Deficiency

Two double-blind, placebo-controlled studies were conducted in 67 adult patients who had received previous somatropin treatment during childhood. Patients were randomized to receive either placebo injections or HUMATROPE (0.00625 mg/kg/day for the first 4 weeks, then 0.0125 mg/kg/day thereafter) for the first 6 months, followed by open-label use of HUMATROPE for the next 12 months for all patients. During the placebo-controlled phase (first 6 months) of the study, elevations of serum glutamic oxaloacetic transferase were reported more for HUMATROPE-treated (13% vs. 0%) than placebo-treated patients.

Table 6: Adverse Reactions with ≥5% Overall Occurrence in Childhood-Onset Growth Hormone-Deficient Patients Treated with HUMATROPE for 18 Months as Compared with 6-Month Placebo and 12-Month HUMATROPE Exposure
a Abbreviations: ALT=alanine aminotransferase; AST=aspartate aminotransferase
Adverse Reaction	18 Months Exposure [Placebo (6 Months)/Humatrope (12 Months)] (n=30)	18 Months Humatrope Exposure (n=32)
AST a increased	7%	13%
Headache	7%	9%
Asthenia	3%	6%
Edema	10%	6%
Myalgia	7%	6%
Pain	10%	6%
ALT a increased	7%	6%
Flu syndrome	10%	16%
Cough increased	0%	6%
Hypesthesia	0%	6%
Rhinitis	7%	6%
Respiratory disorder	7%	3%
Gastritis	7%	0%
Pharyngitis	7%	3%

6.2 Immunogenicity

As with all therapeutic proteins, there is potential for immunogenicity. The detection of antibody formation is highly dependent on the sensitivity and specificity of the assay. Additionally, the observed incidence of antibody (including neutralizing antibody) positivity in an assay may be influenced by several factors including assay methodology, sample handling, timing of sample collection, concomitant medications, and underlying disease. For these reasons, comparison of the incidence of antibodies to HUMATROPE with the incidence of antibodies to other products may be misleading.

In a clinical study with HUMATROPE during the first 6 months of HUMATROPE therapy in 314 naive patients, 1.6% developed specific antibodies to HUMATROPE (binding capacity ≥0.02 mg/L). None had antibody concentrations which exceeded 2 mg/L. Throughout 8 years of this same study, two patients (0.6%) had binding capacity >2 mg/L. Neither patient demonstrated a decrease in growth velocity at or near the time of increased antibody production. It has been reported that growth attenuation from pituitary-derived GH may occur when antibody concentrations are >1.5 mg/L.

6.3 Postmarketing Experience

The following adverse reactions have been identified during post-approval use of HUMATROPE. Because these adverse events are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure.

Severe Hypersensitivity Reactions — Serious systemic hypersensitivity reactions including anaphylactic reactions and angioedema have been reported with postmarketing use of somatropin products

Neurologic — Headaches (common in pediatric patients and occasional in adults)

Skin — Increase in size or number of cutaneous nevi

Endocrine — Gynecomastia

Gastrointestinal — Pancreatitis

Metabolic — New-onset type 2 diabetes mellitus

Neoplasia — Leukemia has been reported in a small number of GH deficient pediatric patients treated with somatropin

7 DRUG INTERACTIONS

Table 7 includes a list of drugs with clinically important drug interactions when administered concomitantly with HUMATROPE and instructions for preventing or managing them.

Table 7: Clinically Important Drug Interactions with HUMATROPE
Replacement Glucocorticoid Treatment
Clinical Impact:	Microsomal enzyme 11β-hydroxysteroid dehydrogenase type 1 (11βHSD-1) is required for conversion of cortisone to its active metabolite, cortisol, in hepatic and adipose tissue. HUMATROPE inhibits 11βHSD-1. Consequently, individuals with untreated GH deficiency have relative increases in 11βHSD-1 and serum cortisol. Initiation of HUMATROPE may result in inhibition of 11βHSD-1 and reduced serum cortisol concentrations.
Intervention:	Patients treated with glucocorticoid replacement for hypoadrenalism may require an increase in their maintenance or stress doses following initiation of HUMATROPE [see Warnings and Precautions (5.8)].
Examples:	Cortisone acetate and prednisone may be effected more than others since conversion of these drugs to their biologically active metabolites is dependent on the activity of 11βHSD-1.
Non-Replacement Glucocorticoid Treatment in Pediatric Patients
Clinical Impact:	Non-replacement glucocorticoid treatment, including supraphysiologic glucocorticoid treatment, may attenuate the growth promoting effects of HUMATROPE in pediatric patients.
Intervention:	Carefully adjust glucocorticoid dosing in pediatric patients receiving glucocorticoid treatments to avoid both hypoadrenalism and an inhibitory effect on growth.
Cytochrome P450-Metabolized Drugs
Clinical Impact:	Limited published data indicate that somatropin treatment increases cytochrome P450 (CP450)-mediated antipyrine clearance. HUMATROPE may alter the clearance of compounds known to be metabolized by CP450 liver enzymes.
Intervention:	Careful monitoring is advisable when HUMATROPE is administered in combination with drugs metabolized by CP450 liver enzymes.
Oral Estrogen
Clinical Impact:	Oral estrogens may reduce the serum IGF-1 response to HUMATROPE.
Intervention:	Patients receiving oral estrogen may require greater HUMATROPE dosages [see Dosage and Administration (2.3)].
Insulin and/or Other Hypoglycemic Agents
Clinical Impact:	Treatment with HUMATROPE may decrease insulin sensitivity, particularly at higher doses.
Intervention:	Patients with diabetes mellitus may require adjustment of their doses of insulin and/or other hypoglycemic agents [see Warnings and Precautions (5.4)].

8 USE IN SPECIFIC POPULATIONS

8.1 Pregnancy

Risk Summary

Limited available data with somatropin use in pregnant women are insufficient to determine a drug-associated risk of adverse developmental outcomes. Animal reproduction studies have not been conducted with HUMATROPE.

The estimated background risk of major birth defects and miscarriage for the indicated population is unknown. In the U.S. general population, the estimated background risk of major birth defects and miscarriage in clinically recognized pregnancies is 2-4% and 15-20%, respectively.

8.2 Lactation

Risk Summary

There is no information regarding the presence of somatropin in human milk. Limited published data indicate that exogenous somatropin does not increase normal breastmilk concentrations of growth hormone. No adverse effects related to somatropin in the breastfed infant have been reported. The developmental and health benefits of breastfeeding should be considered along with the mother's clinical need for HUMATROPE and any potential adverse effects on the breastfed infant from HUMATROPE or from the underlying maternal condition.

8.4 Pediatric Use

Safety and effectiveness of HUMATROPE in pediatric patients have been established in growth failure due to inadequate secretion of endogenous growth hormone, short stature associated with Turner syndrome, idiopathic short stature (ISS), short stature or growth failure in SHOX deficiency, and short stature in children born small for gestational age (SGA) with no catch-up growth by 2 years to 4 years of age.

Growth Failure due to Inadequate Secretion of Endogenous Growth Hormone

Safety and effectiveness of HUMATROPE have been established in pediatric patients with growth failure due to growth hormone deficiency based on data from an open-label, uncontrolled, multicenter study with HUMATROPE in 314 pediatric patients conducted for up to 8 years [see Clinical Studies (14.1)].

Short Stature Associated with Turner Syndrome

Safety and effectiveness of HUMATROPE have been established in pediatric patients with short stature associated with Turner syndrome based on data from one long-term, randomized, open-label, multicenter, concurrently controlled study; two long-term, open-label multicenter, historically controlled US studies; and one long-term, randomized, US dose-response study with HUMATROPE in 181 pediatric patients [see Clinical Studies (14.2)].

Idiopathic Short Stature (ISS)

Safety and effectiveness of HUMATROPE have been established in pediatric patients with ISS based on data from two randomized, multicenter studies, one placebo-controlled study and one dose-response study with HUMATROPE in 310 pediatric patients [see Clinical Studies (14.3)].

Short Stature or Growth Failure in SHOX Deficiency

Safety and effectiveness of HUMATROPE have been established in pediatric patients with short stature or growth failure in SHOX deficiency based on data from a randomized, controlled, two-year, three-arm, open-label study with HUMATROPE in 52 pediatric patients [see Clinical Studies (14.4)].

Short Stature in Children Born Small for Gestational Age (SGA) with No Catch-up Growth by 2 Years to 4 Years of Age

Safety and effectiveness of HUMATROPE have been established in pediatric patients with short stature born SGA with no catch-up growth based on data from two clinical studies with HUMATROPE in 214 pediatric patients [see Clinical Studies (14.5)].

8.5 Geriatric Use

The safety and effectiveness of HUMATROPE in patients aged 65 years and over has not been evaluated in clinical studies. Elderly patients may be more sensitive to the action of somatropin, and therefore may be more prone to development of adverse reactions. A lower starting dose and smaller dose increments should be considered for older patients [see Dosage and Administration (2.3)].

9 DRUG ABUSE AND DEPENDENCE

9.1 Controlled Substance

HUMATROPE contains somatropin, which is not a controlled substance.

9.2 Abuse

Inappropriate use of somatropin may result in significant negative health consequences.

9.3 Dependence

Somatropin is not associated with drug related withdrawal adverse reactions.

10 OVERDOSAGE

Acute overdosage could lead initially to hypoglycemia and subsequently to hyperglycemia. Overdose with somatropin is likely to cause fluid retention. Long-term overdosage could result in signs and symptoms of gigantism and/or acromegaly consistent with the known effects of excess endogenous growth hormone.

11 DESCRIPTION

HUMATROPE (somatropin) for injection is a recombinant human growth hormone. It is a polypeptide of recombinant DNA origin and is synthesized in a strain of Escherichia coli that has been modified by the addition of the gene for human growth hormone. The peptide is comprised of 191 amino acid residues and has a molecular weight of about 22,125 daltons. The amino acid sequence of the peptide is identical to that of human GH of pituitary origin.

HUMATROPE is a sterile, white, lyophilized powder intended for subcutaneous injection after reconstitution to its liquid form. Phosphoric acid and/or sodium hydroxide may have been added to adjust the pH. Reconstituted solutions have a pH of approximately 7.5. This product is oxygen sensitive.

Vial — Each vial of HUMATROPE contains 5 mg somatropin (15 IU); 25 mg mannitol; 5 mg glycine; and 1.13 mg dibasic sodium phosphate. Each vial is supplied in a combination package with an accompanying 5-mL vial of diluting solution (diluent). The diluent contains Water for Injection with 0.3% metacresol as a preservative and 1.7% glycerin.

Cartridge — Cartridges of HUMATROPE contain either 6 mg (18 IU), 12 mg (36 IU), or 24 mg (72 IU) of somatropin. Each HUMATROPE cartridge contains the following:

Component	Cartridge
Component	6 mg (gold)	12 mg (teal)	24 mg (purple)
Somatropin	6 mg	12 mg	24 mg
Mannitol	18 mg	36 mg	72 mg
Glycine	6 mg	12 mg	24 mg
Dibasic sodium phosphate	1.36 mg	2.72 mg	5.43 mg

Each cartridge is supplied in a combination package with an accompanying syringe containing approximately 3 mL of diluting solution (diluent). The diluent contains Water for Injection; 0.3% metacresol as a preservative; and 1.7%, 0.29%, and 0.29% glycerin in the 6, 12, and 24 mg cartridges, respectively.

12 CLINICAL PHARMACOLOGY

12.1 Mechanism of Action

Somatropin binds to dimeric GH receptors located within the cell membranes of target tissue cells. This interaction results in intracellular signal transduction and subsequent induction of transcription and translation of GH-dependent proteins including IGF-1, IGF BP-3 and acid-labile subunit. Somatropin has direct tissue and metabolic effects or mediated indirectly by IGF-1, including stimulation of chondrocyte differentiation, and proliferation, stimulation of hepatic glucose output, protein synthesis and lipolysis.

Somatropin stimulates skeletal growth in pediatric patients with GHD as a result of effects on the growth plates (epiphyses) of long bones. The stimulation of skeletal growth increases linear growth rate (height velocity) in most somatropin-treated pediatric patients. Linear growth is facilitated in part by increased cellular protein synthesis.

12.2 Pharmacodynamics

Subcutaneous administration of a single dose of Humatrope (0.033 mg/kg body weight) in healthy volunteers (10 males, 10 females) resulted in an increased median IGF-1 level from 202 ng/mL (men) and 107 ng/mL (women) predose to maximal level of 362 ng/mL (men) and 234 ng/mL (women) after a median of 21 hours (men) and 14 hours (women).

12.3 Pharmacokinetics

Absorption

HUMATROPE has been studied following intramuscular, subcutaneous, and intravenous administration in healthy adult subjects. A single subcutaneous dose administration of HUMATROPE 0.1 mg/kg (0.27 IU/kg) in healthy subjects (n= 8) resulted in a mean (SD) Cmax of 63.3 (18.2) ng/mL at median Tmax of 4.0 (range 3 to 8) hours. The absolute bioavailability of somatropin is 75% after subcutaneous administration.

Distribution

The mean (SD) volume of distribution of somatropin after single dose subcutaneous injection of 0.1 mg/kg (0.27 IU/kg) in healthy subjects is about 0.96 (0.3) L/kg.

Elimination

Metabolism — Extensive metabolism studies have not been conducted. The metabolic fate of somatropin involves classical protein catabolism in both the liver and kidneys. In renal cells, at least a portion of the breakdown products of somatropin is returned to the systemic circulation.

Excretion — In healthy subjects, mean somatropin clearance is 0.18 (0.03) L/hr/kg following subcutaneous administration. The mean half-life of subcutaneous somatropin is 3.8 (1.4) hours. The long half-life observed after subcutaneous administration is due to slow absorption from the injection site. Urinary excretion of intact HUMATROPE has not been measured. Small amounts of somatropin have been detected in the urine of pediatric patients following replacement therapy.

Specific Populations

Geriatric patients — The pharmacokinetics of HUMATROPE have not been studied in patients greater than 65 years of age.

Pediatric patients — The pharmacokinetics of HUMATROPE in pediatric patients are similar to those of adults.

Male and Female Patients — No gender-specific pharmacokinetic studies have been performed with HUMATROPE. The available literature indicates that the pharmacokinetics of somatropin are similar in men and women.

Patients with Renal or hepatic impairment — No studies have been performed with HUMATROPE.

13 NONCLINICAL TOXICOLOGY

13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

Carcinogenicity, mutagenicity and impairment of fertility studies have not been conducted with HUMATROPE.

14 CLINICAL STUDIES

14.1 Pediatric Patients with Growth Failure Due to Inadequate Secretion of Endogenous Growth Hormone

An open-label, uncontrolled, multicenter study with Humatrope was conducted in, 314 treatment-naive children aged >2 years who had GH deficiency. Patients were treated with HUMATROPE (0.06 mg/kg 3 times per week) for up to 8 years. The efficacy of HUMTROPE was assessed by evaluating height velocity. Mean increase in height velocity from baseline of 3.6 ± 1.9 cm/year to 8.8 ± 2.3 cm/year was achieved by 1 year of treatment. Height velocity remained increased above baseline for a small subset of patients (n=12) who remained on-study up to 8 years during the long-term extension phase (6.3 ± 2.5 cm/year at year 8 of treatment).

14.2 Pediatric Patients with Short Stature Associated with Turner Syndrome

One long-term, randomized, open-label, Canadian multicenter, concurrently controlled study, two long-term, open-label multicenter, historically controlled US studies and one long-term, randomized, US dose-response study were conducted to evaluate the efficacy of HUMATROPE for treatment of short stature due to Turner syndrome.

The randomized, open-label, Canadian study compared near-adult height outcomes for HUMATROPE-treated patients to those of a concurrent control group who received no injections. The HUMATROPE-treated patients received a dosage of 0.3 mg/kg/week given in divided doses 6 times per week from a mean age of 11.7 years for a mean duration of 4.7 years. Puberty was induced with a standardized estrogen regimen initiated at 13 years of age for both treatment groups.

In two of the US studies, the effect of long-term treatment with Humatrope (0.375 mg/kg/week given in divided doses either 3 times per week or daily) on adult height was determined by comparing adult heights in the treated patients with those of age-matched historical controls with Turner syndrome who received no growth-promoting therapy. Puberty was induced with a standardized estrogen regimen initiated after 14 years of age in one study; in the second study patients treated early (before 11 years of age) were randomized to begin pubertal induction at either age 12 (n=26) or 15 (n=29) years (conjugated estrogens, 0.3 mg escalating to 0.625 mg daily); those whose treatment was initiated after 11 years of age began estrogen replacement after 1 year of treatment with HUMATROPE.

In the third US study, a randomized, blinded dose-response study, patients were treated from a mean age of 10.9 years for a mean duration of 5.5 years with a weekly HUMATROPE dosage of either 0.27 mg/kg or 0.36 mg/kg administered in divided doses 3 or 6 times weekly.

In summary, patients with Turner syndrome (total n=249 from the 4 studies above) treated to adult height achieved average height gains ranging from 5.0 to 8.3 cm. See Table 8.

Table 8: Height Gain Resultsa of Somatropin Studies in Patients with Turner Syndrome
a Data shown are mean values.
b RCT: randomized controlled trial; MHT: matched historical controlled trial; RDT: randomized dose-response trial.
c Analysis of covariance (ANCOVA) vs. controls: ANCOVA models with GH (0.27 or 0.36 mg/kg/wk) included covariates of baseline age (all studies), baseline height (all studies), study site (all studies), mid-parental height (all studies) and karyotype (US1 and US2 only), baseline bone age (US2 only) or estrogen (low dose or placebo for US3 only).
d Group A: GH age <11 yr, estrogen is initiated at age 15.
e Group B: GH age <11 yr, estrogen is initiated at age 12.
f Group C: GH age >11 yr, estrogen is initiated at after 12 month of treatment with HUMATROPE.
Study	Group	Study Designb	Somatropin Treated Number at Adult Height	GH Age (yr)	Estrogen Age (yr)	GH Duration (yr)	Adult Height Gain (cm)c
Canadian		RCT	27	11.7	13	4.7	5.4
US 1		MHT	17	9.1	15.2	7.6	7.4
US 2	Ad	MHT	29	9.4	15	6.1	8.3
	Be	MHT	26	9.6	12.3	5.6	5.9
	Cf	MHT	51	12.7	13.7	3.8	5
US 3		RDT	99	10.9	8-13.5	5.5	5.7

14.3 Pediatric Patients with Idiopathic Short Stature (ISS)

Two randomized, multicenter studies, one placebo-controlled and one dose-response, were conducted in pediatric patients with idiopathic short stature. The diagnosis of idiopathic short stature was made after excluding other known causes of short stature, as well as GH deficiency. The placebo-controlled study enrolled 71 pediatric patients (55 males, 16 females) 9 to 15 years old (mean age 12.4 ± 1.5 years), with short stature, 68 of whom received placebo (n=31) or HUMATROPE (n=37). Patients were predominately prepubertal (Tanner I, 45%) or in early puberty (Tanner II, 47%) at baseline. In this double-blind study, patients received subcutaneous injections of either HUMATROPE 0.222 mg/kg/week, or placebo given in divided doses 3 times per week until height velocity decreased to ≤1.5 cm/year (“final height”). Final height measurements were available for 33 subjects (22 treated with HUMATROPE, 11 treated with placebo) after a mean treatment duration of 4.4 years (range 0.1-9.1 years).

Results are presented in Table 9. The number of patients whose final height was above the 5th percentile of the general population height standard for age and sex was significantly greater in the HUMATROPE group than the placebo group (41% vs. 0%), as was the number of patients who gained at least 1 SDS unit in height across the duration of the study (50% vs. 0%).

Table 9: Baseline Height Characteristics and Effect of HUMATROPE on Final Height in Placebo-Controlled Studyab
a For final height population.
b Abbreviations: BPH=baseline predicted height; CI=confidence interval; FH=final height; NA=not applicable; SDS=standard deviation score.
c Assessed using a one-way analysis of variance (ANOVA) with effect for treatment.
d Placebo n=10 as one patient was missing BPH.
e Assessed using analysis of covariance (ANCOVA) with baseline predicted height SDS as the covariate.
	Placebo (n=11) Mean (SD)	HUMATROPE (n=22) Mean (SD)	Treatment Effect Mean (95%CIb)	p-value
Baseline height SDS	-2.8 (0.6)	-2.7 (0.6)	NAb	0.77c
BPH SDS	-2.3 (0.8)	-2.1 (0.7)	NA	0.53c,d
Final height SDS	-2.3 (0.6)	-1.8 (0.8)	0.51 (0.10, 0.92)	0.017e
FHb SDS - baseline height SDS	0.4 (0.2)	0.9 (0.7)	0.51 (0.04, 0.97)	0.034e
FH SDS - BPH SDS	-0.1 (0.6)	0.3 (0.6)	0.46 (0.02, 0.89)	0.043d,e

The dose-response study included 239 pediatric patients (158 males, 81 females), 5 to 15 years old, (mean age 9.8 ± 2.3 years). Mean ± SD baseline characteristics included: height SDS -3.21 ± 0.70, predicted adult height SDS -2.63 ± 1.08, and height velocity SDS -1.09 ± 1.15. All but 3 patients were prepubertal. Patients were randomized to one of three HUMATROPE treatment groups: 0.24 mg/kg/week (n=78); 0.24 mg/kg/week for 1 year, followed by 0.37 mg/kg/week (n=78); and 0.37 mg/kg/week (n=83). Height velocity was assessed in each treatment group during the first 2 years of therapy. After completing the initial 2-year dose-response phase of the study, 50 patients were followed to final height.

After 2 years of treatment, patients who received the HUMATROPE dosage of 0.37 mg/kg/week (n=71) had a significantly greater increase in mean height velocity than patients who received 0.24 mg/kg/week (n=68), (4.04 vs. 3.27 cm/year respectively (ANOVA p=0.003). A total of 12 patients who received 0.37 mg/kg/week and 10 patients who received 0.24 mg/kg/week treatment had missing 2 year treatment data. The mean difference between final height and baseline predicted height was 7.2 cm for patients who received Humatrope 0.37 mg/kg/week and 5.4 cm for patients who received 0.24 mg/kg/week. The results are presented in Table 10. While no patient had height above the 5th percentile in any dosage group at baseline, 82% (n=14) of the 17 patients who received 0.37 mg/kg/week and 47% (n=8) of the 17 patients who received 0.24 mg/kg/week achieved final heights above the 5th percentile of the general population height standards.

Table 10: Idiopathic Short Stature Study Results: Final Height Minus Baseline Predicted Heighta
a Abbreviations: FH=final height; PH=predicted height; CI=confidence interval; cm=centimeters.
	Placebo-controlled Study 3x per week dosing		Dose Response Study 6x per week dosing
	Placebo (n=10)	HUMATROPE 0.22 mg/kg (n=22)	HUMATROPE 0.24 mg/kg (n=13)	HUMATROPE 0.24/0.37 mg/kg (n=13)	HUMATROPE 0.37 mg/kg (n=13)
FH - Baseline PH Mean (95% CI), cm	-0.7 (-3.6, 2.3)	+2.2 (0.4, 3.9)	+5.4 (2.8, 7.9)	+6.7 (4.1, 9.2)	+7.2 (4.6, 9.8)

14.4 Pediatric Patients with Short Stature or Growth Failure in SHOX Deficiency

A randomized, controlled, two-year, three-arm, open-label study was conducted to evaluate the efficacy of HUMATROPE for treatment of short stature in pediatric patients with SHOX deficiency who were not GH–deficient. A total of 52 patients (24 male, 28 female) with SHOX deficiency, 3 to 12.3 years of age, were randomized to either a HUMATROPE-treated arm (27 patients; mean age 7.3 ± 2.1 years) or an untreated control arm (25 patients; mean age 7.5 ± 2.7 years). To determine the comparability of treatment effect between patients with SHOX deficiency and patients with Turner syndrome, the third study arm enrolled 26 patients with Turner syndrome, 4.5 to 11.8 years of age (mean age 7.5 ± 1.9 years) who received HUMATROPE treatment. All patients were prepubertal at study entry. Patients in the HUMATROPE-treated group(s) received daily subcutaneous injections of 0.05 mg/kg of HUMATROPE, equivalent to 0.35 mg/kg/week. Patients in the untreated group received no injections. One untreated patient discontinued the study during the first year. The results are presented in Table 11; the mean first-year height velocity of treated patients with SHOX deficiency was significantly greater than that of the untreated patients (mean between-group difference = 3.5 [95% CI: 2.8 – 4.2] cm/year, p<0.001).

Table 11: Summary of Results in Patients with SHOX deficiency and Turner Syndrome
a Positive values favor HUMATROPE
b p<0.001 (assessed using analysis of covariance [ANCOVA] with covariates of treatment Group, Léri-Weill syndrome, sex and baseline age).
c p<0.001 (assessed using ANCOVA with covariates of treatment group and baseline height [cm]).
d p<0.001 (assessed using ANCOVA with covariates of treatment group and baseline height SDS).
e p=0.003 calculated using Fisher's exact test.
	SHOX Deficiency			Turner Syndrome
	Untreated (n=24) Mean (SD)	HUMATROPE (n=27) Mean (SD)	Treatment Differencea Mean (95% CI)	HUMATROPE (n=26) Mean (SD)
Height Velocity (cm/yr)
1st Year	5.2 (1.1)	8.7 (1.6)b	+3.5 (2.8, 4.2)	8.9 (2.0)
2nd Year	5.4 (1.2)	7.3 (1.1)b	+2.0 (1.3, 2.6)	7.0 (1.1)

Height Gain (cm)
Baseline to 1st Year	5.4 (1.2)	9.1 (1.5)c	+3.7 (2.9, 4.5)	8.9 (1.9)
Baseline to 2nd Year	10.5 (1.9)	16.4 (2.0)c	+5.8 (4.6, 7.1)	15.7 (2.7)

Height SDS Gain
Baseline to 1st Year	0.1 (0.5)	0.7 (0.5)d	+0.5 (0.3, 0.8)	0.8 (0.5)
Baseline to 2nd Year	0.2 (0.5)	1.2 (0.7)d	+1.0 (0.7, 1.3)	1.2 (0.7)

Patients with height SDS > -2.0 at 2 years	1 (4%)	11 (41%)e	--	8 (31%)

14.5 Pediatric Patients with Short Stature Born Small for Gestational Age (SGA) Who Fail to Demonstrate Catch-up Growth by Age 2 - 4 Years

The height increases would be considered similar if the lower bound of the 95% confidence interval (CI) for the mean difference between the groups (IAD – FHD) was greater than -0.5 height SDS. A 2-year, open-label, multicenter, European study enrolled 193 prepubertal, non-GH deficient children with mean chronological age 6.8 ± 2.4 years (range: 3 to 12.3). Study entry criteria included birth weight <10th percentile and/or birth length SDS <-2 for gestational age, and height SDS for chronological age ≤-3. Exclusion criteria included syndromal conditions (e.g., Turner syndrome), chronic disease (e.g., diabetes mellitus), and active tumors. The primary objective was to compare the increase from baseline in height SDS after 1 year of treatment when HUMATROPE is administered according to an individually adjusted dose (IAD) regimen with a fixed high dose (FHD) regimen. Patients were randomized to either a FHD (0.067 mg/kg/day [0.47 mg/kg/week]; n=99) or an IAD treatment group (n=94). The initial HUMATROPE dosage in the IAD treatment group was 0.035 mg/kg/day (0.25 mg/kg/week). The dosage was increased to 0.067 mg/kg/day in those patients in the IAD group whose 1-year height gain predicted at Month 3 was <0.75 height SDS (n=40) or whose actual height gain measured at Year 1 was <0.75 height SDS (n=11).

The results are presented in Table 12, The increase from baseline in height SDS in the IAD group was non-inferior to that in the FHD group at Year 1 (mean between-group difference = -0.3 SDS [95% CI: -0.4, -0.2 SDS]). The results were similar when children who entered puberty during the study were removed from the analysis. Data is shown for the efficacy analysis population that included all patients who received at least 1 dose of HUMATROPE and had at least 1 post randomization height measurement. Approximately 85% of the randomized patients completed 2 years of therapy.

Table 12: Results for Height SDS and Change from Baseline in Height SDS at Year 1 and Year 2 After HUMATROPE Treatment of Short Children Born SGA Who Fail to Demonstrate Catch-up Growtha
a Abbreviations: IAD=individually adjusted dose; FHD=fixed high dose; SD=standard deviation; SDS=standard deviation score
b Least squares mean difference ± standard error and 95% confidence interval based on ANCOVA model with treatment and gender as fixed effects, and baseline height SDS, baseline chronological age, baseline bone age, and mid-parental target height SDS as covariates.
c Only children with actual height measurements were included in the Year 1 and Year 2 analyses.
	IAD Group 0.035 to 0.067 mg/kg/day Mean (SD)	FHD Group 0.067 mg/kg/day Mean (SD)	IAD – FHD GroupDifference± SE (95% CI) b
Baseline	(n=86) -3.9 (0.6)	(n=93) -3.9 (0.7)	-0.0 ± 0.1 (-0.2, 0.2)
Year 1 Height SDS Change from baseline	(n=86)c -3.0 (0.7) 0.9 (0.4)	(n=93)c -2.7 (0.7) 1.1 (0.4)	-0.3 ± 0.1 (-0.4, -0.2) p-value <0.001
Year 2 Height SDS Change from baseline	(n=82)c -2.5 (0.8) 1.4 (0.5)	(n=88)c -2.2 (0.7) 1.6 (0.5)	-0.3 ± 0.1 (-0.4, -0.1)

An open-label, multicenter, single arm study was conducted in France, during which 35 prepubertal, non-GH deficient children were treated for 2 years with HUMATROPE 0.067 mg/kg/day (0.47 mg/kg/week). Mean chronological age at baseline was 9.3 ± 0.9 years (range: 6.7 to 10.8). Additional study entry criteria included birth length SDS <-2 or <3rd percentile for gestational age, and height SDS for chronological age <-2. Exclusion criteria included syndromal conditions (e.g., Turner syndrome), and chronic disease (e.g., diabetes mellitus). All 35 patients completed the study. Mean height SDS increased from a baseline value of -2.7 (SD 0.5) to -1.5 (SD 0.6) after 2 years of HUMATROPE treatment.

14.6 Adult Patients with Growth Hormone Deficiency

Two multicenter studies in patients with adult-onset GH deficiency (n=98) and two studies in patients with childhood-onset GH deficiency (n=67) were designed to assess the effects of replacement therapy with HUMATROPE. Adult-onset patients and childhood-onset patients differed by diagnosis (organic vs. idiopathic pituitary disease), body size (average vs. small [mean height (171 cm vs 161 cm) and weight (85 kg vs 64 kg)]), and age (mean 44 vs. 29 years).Each study included a 6-month randomized, blinded, placebo-controlled phase, during which approximately half of the patients received placebo injections, while the other half received HUMATROPE injections. The HUMATROPE dosages for all studies were identical: 1 month of treatment at 0.00625 mg/kg/day followed by 0.0125 mg/kg/day for the next 5 months. The 6-month, double-blind phase was followed by 12 months of open-label HUMATROPE treatment for all patients. The primary efficacy measures were body composition (lean body mass and fat mass) and lipid parameters [Total cholesterol, high-density lipoprotein (HDL) and low-density lipoprotein (LDL)]. Lean body mass was determined by bioelectrical impedance analysis (BIA), validated with potassium 40. Body fat was assessed by BIA and sum of skinfold thickness. Lipid subfractions were analyzed by standard assay methods in a central laboratory.

In patients with adult-onset GH deficiency, HUMATROPE treatment (vs. placebo) resulted in an increase in mean lean body mass (2.59 vs. -0.22 kg, p<0.001) and a decrease in body fat (-3.27 vs. 0.56 kg, p<0.001). Similar changes were seen in childhood-onset GH deficient patients. These changes in lean body mass persisted throughout the 18-month period for both the adult-onset and childhood-onset groups; the changes in fat mass persisted in the childhood-onset group. Serum concentrations of HDL cholesterol which were low at baseline (mean, 31.0 mg/dL and 33.9 mg/dL in adult-onset (n=46) and childhood-onset (n=30) patients, respectively) had increased by the end of 18 months of HUMATROPE treatment (mean change of 13.7 and 11.1 mg/dL for the adult-onset (n=40) and childhood-onset (n=21) groups, respectively p<0.001; there was no adjustment for missing data). Total cholesterol and LDL did not show significant difference from baseline results by the end of 18 months of HUMATROPE treatment.

In an additional 2-year, open-label, randomized study, 149 patients with childhood-onset GH deficiency who had completed pediatric somatropin therapy, had attained final height (height velocity <1 cm/yr) and were confirmed to be GH-deficient as young adults, were randomized to receive HUMATROPE 0.0125 mg/kg/day (n=59), HUMATROPE 0.025 mg/kg/day (n=58), or no treatment (control) (n=32). Total bone mineral content (BMC) increased by 5.2% ± 3.9% in the control group (n=28 for those with BMC measurements), 7.0% ± 7.2% in the HUMATROPE 0.025 mg/kg/day group (n=51) and 8.0% ± 8.9% in the HUMATROPE 0.0125 mg/kg/day group (n=51). For the treatment effect versus control group, p=0.012 (ANOVA); there was no statistically significant difference between the 2 HUMATROPE dose groups. A significant overall treatment effect (ANOVA, p=0.037) was seen for the percentage change in lumbar spine BMC, but not for femoral neck or hip.

16 HOW SUPPLIED/STORAGE AND HANDLING

16.1 How Supplied

HUMATROPE for injection is a white lyophilized powder available in the following vial and cartridge sizes:

NDC	Kit	HUMATROPE	Diluent
NDC: 0002-7335-11	Vial Kit	5 mg vial	5-mL vial of Diluent for HUMATROPE
NDC: 0002-8147-01	Cartridge Kit	6 mg cartridge (gold)	prefilled syringe of Diluent for HUMATROPE
NDC: 0002-8148-01	Cartridge Kit	12 mg cartridge (teal)	prefilled syringe of Diluent for HUMATROPE
NDC: 0002-8149-01	Cartridge Kit	24 mg cartridge (purple)	prefilled syringe of Diluent for HUMATROPE

16.2 Storage and Handling

Vials

Refrigerate vials of HUMATROPE and Diluent for HUMATROPE at 36° to 46°F (2° to 8°C). Avoid freezing Diluent for HUMATROPE. Protect HUMATROPE from light during storage.

Cartridges

Refrigerate cartridges of HUMATROPE and Diluent for HUMATROPE at 36° to 46°F (2° to 8°C). Avoid freezing Diluent for HUMATROPE. Protect HUMATROPE from light during storage.

17 PATIENT COUNSELING INFORMATION

Advise the patient to read the FDA-approved patient labeling (Instructions for Use).

Neoplasms – Advise childhood cancer survivors/caregivers that individuals treated with brain/head radiation are at increased risk of secondary neoplasms and as a precaution need to be monitored for recurrence. Advise patients/caregivers to report marked changes in behavior, onset of headaches, vision disturbances and/or changes in skin pigmentation or changes in the appearance of pre-existing nevi.
Fluid Retention - Advise patients that fluid retention during HUMATROPE replacement therapy in adults may frequently occur. Inform patients of the clinical manifestations of fluid retention (e.g. edema, arthralgia, myalgia, nerve compression syndromes including carpal tunnel syndrome/paraesthesias) and to report to their healthcare provider any of these signs or symptoms that occur during treatment with HUMATROPE.
Pancreatitis - Advise patients/caregivers that pancreatitis may develop and to report to their healthcare provider any new onset of abdominal pain.
Hypoadrenalism - Advise patients/caregivers who have or who are at risk for pituitary hormone deficiency(s) that hypoadrenalism may develop and to report to their healthcare provider if they experience hyperpigmentation, extreme fatigue, dizziness, weakness, or weight loss.
Hypothyroidism - Advise patients/caregivers that undiagnosed/untreated hypothyroidism may prevent an optimal response to HUMATROPE. Advise patients/caregivers they may require periodic thyroid function tests.
Intracranial Hypertension - Advise patients/caregivers to report to their healthcare provider any visual changes, headache, and nausea and/or vomiting.
Hypersensitivity Reactions – Advise patients/caregivers that serious systemic hypersensitivity reactions (anaphylaxis and angioedema) are possible and that prompt medical attention should be sought if an allergic reaction occurs.
Glucose Intolerance/ Diabetes Mellitus – Advise patients/caregivers that new onset impaired glucose intolerance/diabetes mellitus or exacerbation of preexisting diabetes mellitus can occur and monitoring of blood glucose during treatment with HUMATROPE may be needed.
Administration – Counsel patients and parents that they should never share a HumatroPen with another person, even if the needle is changed. Sharing of the pen between patients may pose a risk of transmission of infection.

Marketed by: Lilly USA, LLC, Indianapolis, IN 46285, USA
Copyright © 1987, 2019, Eli Lilly and Company. All rights reserved.

HTR-0004-USPI-20191028

INSTRUCTIONS FOR USE

Instructions for Use

HUMATROPE® (HU-ma-trope)

(somatropin) for injection

Vial Kit

Read this Instructions for Use before you start using HUMATROPE and each time you get a new HUMATROPE vial. There may be new information. This information does not take the place of talking to your healthcare provider about your or your child's medical condition or treatment.

Your healthcare provider should show you how to prepare, mix, measure, and inject HUMATROPE the right way before you use it for the first time. Ask your healthcare provider if you have any questions.

Do not share your syringes or needles with anyone else, even if the needle has been changed. You may give other people a serious infection or get a serious infection from them.

HUMATROPE is not recommended for use by blind or visually impaired individuals without the help of a sighted individual trained on how to use it.

How should I store HUMATROPE?

Store HUMATROPE in the refrigerator between 36°F to 46°F (2°C to 8°C) before and after mixing.
Do not freeze.
Protect HUMATROPE from light during storage.
Do not leave the HUMATROPE vial out of the refrigerator for more than 30 minutes a day.
HUMATROPE that has been mixed with Sterile Diluent for Humatrope and is in liquid form, should be used within 14 days. Throw away any mixed HUMATROPE left over after 14 days.

You will need the following supplies to mix your HUMATROPE and give your injection (Figures A and B):

2 alcohol swabs
1 cotton swab or gauze pad
2 sterile syringes (as recommended by your healthcare provider)
2 sterile needles (as recommended by your healthcare provider)
1 Sterile Diluent for HUMATROPE vial (provided in Humatrope Kit)
1 HUMATROPE vial (provided in Humatrope Kit)
1 sharps container for throwing away used needles and syringes. See “Disposing of used needles and syringes” at the end of these instructions.

Before mixing your HUMATROPE, check the expiration date on the vial labels (See Figure A). Do not use any vial that has expired. Contact your healthcare provider or call Lilly at 1-800-545-5979 if either vial has expired.

Figure A

Figure B

Mixing the Vial of HUMATROPE:

Only mix HUMATROPE with the Diluent for HUMATROPE that comes in the package.
Do not use other solutions for mixing HUMATROPE unless instructed to do so by your healthcare provider.
Your healthcare provider will also tell you what size syringe and needle to use and how much Diluent to add to the vial of HUMATROPE.

Wash your hands with soap and water.

Step 1.

Remove and throw away (discard) plastic caps from the tops of the vials of HUMATROPE and Diluent for HUMATROPE. Wipe tops of both vials with an alcohol swab (See Figure C).

Figure C

Step 2.

Remove outer wrapping from 1 syringe (See Figure D).

Figure D

Step 3.

Remove outer wrapping from 1 needle. Place needle on top of syringe and turn until it is tight and firmly attached (See Figure E).


Figure E

Step 4.

Remove needle cover by pulling straight off (See Figure F).

Figure F

Step 5.

Pull back on the syringe plunger to draw up an amount of air equal to the amount of Diluent your healthcare provider has prescribed (See Figure G).

Figure G

Step 6.

Insert the needle in the center of the stopper of the Diluent for HUMATROPE vial (See Figure H). Push down on the syringe plunger to insert air into the vial.

Figure H

Step 7.

Hold the Diluent vial upside down, making sure the needle tip remains in solution.
Slowly pull back on the syringe plunger until the tip of the plunger reaches the line for the amount of Diluent your healthcare provider has prescribed (See Figure I).
If there are air bubbles, tap the syringe gently a few times to let any air bubbles rise to the top. Slowly push the plunger up to remove the air bubbles.
If you push the Diluent back into the vial to remove the air bubbles, slowly pull back on the plunger to draw the correct amount of Diluent your healthcare provider prescribed.

Figure I

Step 8.

Turn the vial back upright, while holding the barrel, and slowly pull the needle out of the Diluent vial (See Figure J).

Figure J

Step 9.

Insert the needle into the vial of HUMATROPE and gently aim the needle tip toward the wall of the vial.
Slowly push down on the syringe plunger to inject the Diluent by aiming the stream of liquid against the wall of the vial (See Figure K).
Do not aim the needle tip at the white powder at the bottom of the vial.

Figure K

Step 10.

Remove the needle from the vial.
Throw away the syringe with the needle attached. See “Disposing of used needles and syringes” at the end of these instructions.

Step 11.

Swirl the HUMATROPE vial in a gentle circular motion until the powder is completely dissolved into liquid (See Figure L).
Do not shake.

Figure L

Step 12.

Write the date that you mixed the HUMATROPE on the vial label, and throw away the unused Diluent. You will use the mixed vial of HUMATROPE for each injection.
Keep the mixed vial of HUMATROPE in the refrigerator.
Protect HUMATROPE from light during storage.
Throw away the mixed vial of HUMATROPE after 14 days even if there is still medicine in the vial.

Preparing to give your Injection:

Step 13.

After mixing and before each injection, check the liquid in the HUMATROPE vial. The liquid should look clear, colorless, and free of particles. Do not use mixed HUMATROPE if it is cloudy or contains particles. Contact your healthcare provider or call Lilly at 1-800-545-5979 or go to www.humatrope.com.
Take the vial of HUMATROPE out of the refrigerator and let it sit for 10 minutes before injecting to allow it to reach room temperature. Injecting medicine that is cold can cause discomfort.

Step 14.

Before each injection, clean the rubber stopper of the mixed HUMATROPE vial with an alcohol swab.

Step 15.

When you are ready to give your injection use a new sterile syringe.
Remove outer wrapping from 1 syringe.

Step 16.

Use a new sterile needle.
Remove outer wrapping from 1 needle. Your healthcare provider will tell you the right size needle to use. Place needle on top of the syringe and turn until it is tight and firmly attached.

Step 17.

Remove the needle cover.

Step 18.

Pull back on the syringe plunger to draw up an amount of air equal to the amount of HUMATROPE your healthcare provider has prescribed.

Step 19.

Insert the needle into your vial of mixed HUMATROPE and inject the air into the vial.

Step 20.

Hold the vial upside down making sure to keep the needle tip in the solution and withdraw your correct dose. Make sure that no air bubbles are in the syringe.

Injecting HUMATROPE:

Step 21.

Choose your injection site. Your healthcare provider should show you the best areas to give your injection. Choose a different injection site each day.
Injections can be given under the skin (subcutaneously) in the following areas (See Figure M):

- Abdomen: above, below, or either side of the belly button (navel)

- Front of the upper thighs

- Upper, outer buttocks

- Back of the arms above the elbow and below the shoulder

Figure M

Step 22.

Wipe the area well with an alcohol swab. Use a circular motion and work outward from the inside of the circle (See Figure N).

Figure N

Step 23.

With the thumb and forefinger of one hand, pinch up a fold of skin (See Figure O).

Figure O

Step 24.

Holding the syringe at a 90-degree angle to the injection site or as recommended by your healthcare provider, quickly insert the needle all the way into the pinched area of skin (See Figure P).

Figure P

Step 25.

After the needle is inserted, release the pinched skin. Slowly inject the solution by gently pressing the plunger all the way down until the syringe is empty (See Figure Q).

Figure Q

Step 26.

Remove the needle quickly, and apply pressure over the injection site with a dry gauze pad or cotton swab. Rub the injection site for several seconds.

Step 27.

Throw away used needles and syringes in a sharps container. See “Disposing of used needles and syringes” at the end of these instructions.

Step 28.

Return mixed vial of HUMATROPE to the refrigerator and use within 14 days.
Protect HUMATROPE from light during storage.

Disposing of used needles and syringes:

Put your used needles and syringes in a FDA-cleared sharps disposal container right away after use. Do not throw away (dispose of) loose needles and syringes in your household trash.
If you do not have a FDA-cleared sharps disposal container, you may use a household container that is:

- made of a heavy-duty plastic,

- can be closed with a tight-fitting, puncture-resistant lid, without sharps being able to come out,

- upright and stable during use,

- leak-resistant, and

- properly labeled to warn of hazardous waste inside the container.

When your sharps disposal container is almost full, you will need to follow your community guidelines for the right way to dispose of your sharps disposal container. There may be state or local laws about how you should throw away used needles and syringes. Do not reuse or share your needles or syringes with other people. For more information about safe sharps disposal, and for specific information about sharps disposal in the state that you live in, go to the FDA's website at: http://www.fda.gov/safesharpsdisposal.

Do not dispose of your used sharps disposal container in your household trash unless your community guidelines permit this. Do not recycle your used sharps disposal container.

This Instructions for Use has been approved by the U.S. Food and Drug Administration.

HUMATROPE® is a registered trademark of Eli Lilly and Company.

Revised October 2019

Marketed by: LILLY USA, LLC, INDIANAPOLIS, IN 46285, USA

HTRVL-0001-IFU-20191028

This Instructions for Use has been approved by the U.S. Food and Drug Administration.

HUMATROPE® and HumatroPen® are registered trademarks of Eli Lilly and Company.

Instructions for Use

HumatroPen® 6 mg

(HU-ma-tro-Pen 6 mg)

HUMATROPE® Delivery System Device

for use with

HUMATROPE (somatropin) 6 mg Cartridges

6 mg

Section 1: Read Section 1 completely before you move on to Section 2.

What you need to know about HumatroPen® 6 mg

Read this Instructions for Use including the “Commonly asked questions” section, at the end of this Instructions for Use, before you start using HumatroPen 6 mg and each time you get a new Pen. There may be new information. This information does not take the place of talking to your healthcare provider about your or your child's medical condition or treatment.

Your healthcare provider should show you how to use HumatroPen (Pen) the right way before you use it for the first time. Ask your healthcare provider if you have any questions. If you are having problems using the HumatroPen 6 mg, call Lilly at 1-800-545-5979 or go to www.humatrope.com.

Introduction

The HumatroPen 6 mg is an injection device used with HUMATROPE 6 mg Cartridges. Your healthcare provider will prescribe the HUMATROPE dose and Pen that is right for you or your child. Do not change your dose or use another type of pen unless your healthcare provider tells you to.
If your healthcare provider changes the prescribed cartridge strength from the 6 mg HUMATROPE Cartridge to the 12 mg or 24 mg HUMATROPE Cartridge, you will need to get a new HumatroPen to match the new cartridge strength.

Important information about HumatroPen 6 mg:

Do not use the Pen if any part of the Pen or Cartridge looks broken or damaged. Contact your healthcare provider.
Make sure that you have a 6 mg HUMATROPE Cartridge to match the HumatroPen 6 mg. If the strength on the label for the Cartridge and the Pen do not match, do not use them and contact your healthcare provider. It is important to use the correct Pen and Cartridge to make sure that you inject the correct dose of HUMATROPE.
Do not use the HUMATROPE Cartridge past the expiration date.
Follow the instructions in Section 2 only to set up a new Cartridge before you use it for the first time.
Follow the instructions in Section 3 of this Instructions for Use for every injection.
Do not transfer the contents of the HUMATROPE Cartridge to a syringe.
Do not share your HumatroPen 6 mg or needles with anyone else, even if the needle has been changed. You may give other people a serious infection or get a serious infection from them.
The HumatroPen 6 mg is not recommended for use by blind or visually impaired individuals without the help of a sighted individual trained on how to use it.

Information about needles used with HumatroPen 6 mg:

Pen needles are not included with HumatroPen. You may need a prescription to get the needles from your pharmacist.
Becton, Dickinson and Company pen needles are recommended for use with the HumatroPen 6 mg.
Ask your healthcare provider what size needle is best for you to use.
Use of the Hidden Needle Cover with your HumatroPen is optional. When using the Hidden Needle Cover with your HumatroPen, you must use a needle length of 5 mm or longer. Read the Hidden Needle Cover Instructions for Use.
Follow your healthcare provider's instructions about how to safely handle needles.
Always remove the Pen needle after each injection and use a new needle with each injection. This helps reduce the risk of infection, prevent leakage of HUMATROPE, reduce air bubbles, and reduce needle clogs.
For information on the right way to throw away (dispose of) used needles see “Disposing of used needles” at the end of this Instructions for Use.

How do I care for HumatroPen 6 mg?

Soiled parts including the Hidden Needle Cover can be cleaned with a damp cloth. Do not use alcohol or any other cleaning product.
Do not wash or soak the Pen in any kind of liquid.
Do not apply oil or any other lubricant.

How do I store HumatroPen 6 mg with an attached cartridge?

After attaching a prepared HUMATROPE cartridge to your HumatroPen 6 mg, store it in the storage case in the refrigerator between 36°F to 46°F (2°C to 8°C) until it is time for your next injection.
Before injecting a dose of HUMATROPE, take the Pen out of the refrigerator and let it sit for 10 minutes to allow it to reach room temperature. Injecting medicine that is cold can cause discomfort. Do not leave the HumatroPen 6mg and HUMATROPE cartridge out of the refrigerator for more than 30 minutes a day.
HUMATROPE Cartridges attached to a Pen can be stored in the refrigerator for up to 28 days. Do not use a prepared Cartridge after 28 days.
Do not freeze.
Do not store the Pen with the needle attached.
Protect HUMATROPE Cartridges attached to the Pen from light during storage.

When do I need to replace my HumatroPen?

Do not use your Pen for more than 3 years after first use or past the expiration date on the carton, whichever comes first.

Record the date the Pen was first used here: __ / __ / __.

Record the expiration date from your carton here: __ / __ / __.

Contact your healthcare provider if you need a new HumatroPen 6 mg, or when the Pen has been used for 3 years.

For more information, call Lilly at 1-800-545-5979 or go to www.humatrope.com.

HumatroPen 6 mg Parts

Pen Needle Parts (Pen needles not included)

Hidden Needle Cover (optional, included)

Storage Case

Section 2: Read Section 2 only after you have read Section 1.

Getting Started

Be sure to follow the mixing directions in the HUMATROPE Cartridge Kit.
Perform the New Cartridge Set-up only 1 time at the beginning of each new Cartridge preparation.
For daily use, do not repeat the 1 time only New Cartridge Set-up. If you repeat the 1 time only New Cartridge Set-up, you may run out of HUMATROPE early.

New Cartridge Set-up

Step 2A – Check the Pen and Cartridge
Front View Back View
Be sure to check the Cartridge: - For 6 mg on the Cartridge label - For the expiration date on the opposite side of the Cartridge - To see if the liquid is clear and free of particles Important Notes: Do not use the Cartridge past the expiration date. Do not use the Pen if any part of the Pen or Cartridge appears broken or damaged. Contact your healthcare provider.	Pull off the Pen cap.	Look at the injection button and the front housing to make sure it is a 6 mg Pen. Important Note: Check the number on the front housing to make sure that it matches the Cartridge strength on the Cartridge label. If the Pen and Cartridge do not match, contact your healthcare provider.

Step 2B – Attach the Cartridge

The screw may be in or out when you get the Pen. If the screw is out, use the white tip of the Cartridge to push the screw back.	Push the white tip of the mixed Cartridge into the Pen body. Screw the 6 mg Pen body onto the Cartridge until it is secure. Important Note: If the Cartridge is not completely attached, the screw may not move and cause you to inject the wrong dose.

Step 2C – Attach the needle

Remove the paper tab from the end of the outer cap.	Push the needle straight onto the 6 mg Cartridge and turn it until secure.	Pull off the outer cap and the inner cap. Keep the outer cap to remove the needle after the injection.

Step 2D – Remove air from new Cartridge

Turn the dose knob to dial 1.25 mg.	Point the needle straight up. Push the injection button and hold it for 5 seconds. Dial 0.05 mg and repeat these steps until liquid is seen at the needle tip.

Important Notes:

The Pen must be set-up before injecting the first dose from each new 6 mg Cartridge.
Setting up the new Cartridge is important to remove large air bubbles that may be present after mixing the HUMATROPE 6 mg Cartridge.
If liquid is not seen at the needle tip after you have tried several times to remove air from the new Cartridge as instructed in Step 2D, contact your healthcare provider or Lilly at 1-800-545-5979.

Step 2E – Continue on to Daily Use

Do not repeat the New Cartridge Set-up before each dose.
Leave the Cartridge attached and do not remove it until the Cartridge is empty.
If you are ready to inject the first dose and you have finished setting up your Pen with a new Cartridge, go to Section 3, Step 3C.
If you are using the Hidden Needle Cover with HumatroPen 6 mg, read the Hidden Needle Cover Instructions for Use.

Section 3: Now that you have done the 1 time only New Cartridge Set-up, follow Section 3 for each of your daily injections.

Remove the prepared Pen with the Cartridge attached from your refrigerator.
Let the Pen with Cartridge attached stand at room temperature for 10 minutes before injecting.

Daily Use

Before your injection: Take the Pen out of the refrigerator and let it sit for 10 minutes before injecting to allow it to reach room temperature. Injecting medicine that is cold can cause discomfort.

Step 3A – Check the Pen

Pull off the Pen cap.

Important Note:
Do not use the Pen if any part of the Pen or Cartridge appears broken or damaged. Contact your healthcare provider.

Be sure to check the Cartridge:

- For 6 mg Cartridge label

- For expiration date

- To see if the liquid is clear and free of particles

Important Note:
Do not use the Cartridge past the expiration date.

Look at the injection button and the front housing to make sure it is a 6 mg Pen.

Important Note:
Check the number on the front housing to make sure that it matches the Cartridge strength on the Cartridge label. If the Pen and Cartridge do not match, contact your healthcare provider.

Step 3B – Attach a new disposable pen needle for each injection.

Remove the paper tab from the end of the outer cap.	Push the needle straight onto the 6 mg Cartridge and turn it until secure.	Pull off the outer cap and the inner cap. Keep the outer cap to remove the needle after the injection.

Important Note: Talk to your healthcare provider about the right way to use the Pen, and the optional Hidden Needle Cover, the right sites to inject HUMATROPE, and how to rotate your injection sites. When using the Hidden Needle Cover with your HumatroPen, you must use a needle length of 5 mm or longer. Read the Hidden Needle Cover Instructions for Use.

Step 3C – Dial and inject the dose

Turn the dose knob to the prescribed dose.

Important Note:
Confirm the dose dialed matches the prescribed dose.
Your dose may be different than the dose shown in the figure above.

If you turn past the prescribed dose, you can correct the dose by turning down to the right dose.
The dose knob clicks as you turn it. Do not dial your dose by counting clicks because you may dial the wrong dose.

Injections can be given under the skin (subcutaneous) in the following areas:

- Abdomen: above, below, or either side of the belly button (navel)

- Front of the upper thighs

- Upper, outer buttocks

- Back of the arms above the elbow and below the shoulder

Talk to your healthcare provider about the right way to use HumatroPen, the right areas to give your injection, and injection site rotation.

Insert the needle at a 90 degree angle or as shown by your healthcare provider.
Place your thumb on the injection button, then slowly and firmly push the injection button until it stops moving.
Continue to hold the injection button for 5 seconds, then remove the needle from the skin.
Check to make sure you see a 0.00 in the dose window. This means that the complete dose was injected.

Important Note:
It is possible to set a dose larger than the amount of HUMATROPE left in the Cartridge.

At the end of the injection, the number in the dose window should be 0.00. If you see any number other than “0.00”, this is the amount of HUMATROPE you did not receive. Write this number down and follow the steps below to get the rest of your dose.
Remove the needle and empty Cartridge from the Pen.
Repeat Steps 2A through 2D.
Complete your dose by injecting only the amount you did not receive.
If you still do not think you received your full dose, do not take another dose. Call Lilly at 1-800-545-5979 or call your healthcare provider for assistance.

Step 3D – Remove and dispose of the needle


Carefully replace the outer cap as instructed by your healthcare provider. - You can use the scoop method: Scoop the outer cap back on the needle.	Remove the capped needle. Follow the instructions in the “Disposing of used needles” section at the end of this Instructions for Use to dispose of the needle.	Replace the Pen cap.

Important Note: Do not remove this Cartridge from the Pen until the Cartridge is empty or needs to be replaced to help prevent you from giving the wrong dose.

Step 3E – Store Pen and Cartridge for next use

See, “How do I store HumatroPen 6 mg?” in Section 1 of this Instructions for Use for more information.
When it is time for the next scheduled dose, go to Section 3, and repeat Steps 3A through 3D.
When using the Hidden Needle Cover with HumatroPen 6 mg, repeat steps 1 to 10 of the Hidden Needle Cover Instructions for Use.

Commonly asked questions:

Do I need to perform the New Cartridge Setup before every dose?
- No. You only need to perform the New Cartridge Set-up 1 time for each Cartridge, just before a new Cartridge is used for the first time.
- The purpose of the New Cartridge Set-up is to make sure the HumatroPen 6 mg with an attached HUMATROPE 6 mg Cartridge are ready to use.
- If you repeat the New Cartridge Set-up before each routine dose, you may run out of HUMATROPE early. The small amount of medicine used in the New Cartridge Set-up will not affect the amount of HUMATROPE in the Cartridge.
What should I do if the Cartridge label and Pen do not match?
- Do not use the Pen if the Cartridge strength on the HUMATROPE Cartridge label does not match the number on the Pen's front housing. This is important to make sure the correct dose of HUMATROPE is given.
- Contact your healthcare provider for a replacement.
What should I do if the HUMATROPE is not clear?
- Do not use the Pen if the liquid is cloudy or contains particles. Contact your healthcare provider or call Lilly at 1-800-545-5979 or go to www.humatrope.com.
Why are there air bubbles in the Cartridge?
- Air bubbles may remain in the Cartridge after mixing.
- If the Pen is stored with a needle attached, air bubbles may form in the Cartridge.
  Do not store the Pen with a needle attached.
- Follow the instructions in Section 2, Step 2D (Remove air from new Cartridge) to remove air bubbles from the Cartridge.
- It is normal to see small air bubbles. It will not cause any harm or affect the dose.
What should I do if the screw does not move out when there is no Cartridge attached to the Pen?
- The screw may not move out when you push the injection button unless there is a Cartridge in the Pen. This allows you to easily push the screw into the Pen body when replacing a Cartridge.
- After a Cartridge is attached, the screw will move out when the injection button is pushed.
What should I do if I cannot attach the Cartridge to the Pen body?
- Check that the Cartridge is not damaged or broken.
- Carefully line up the Cartridge with the Pen body and screw them together until secure. If the Cartridge and Pen cannot be screwed together, contact your healthcare provider.
Why is it hard to push the injection button when I try to inject the dose?
- The needle may be clogged. Try attaching a new needle.
- Pushing the injection button down quickly may make the injection button harder to push. Pushing the injection button more slowly may make it easier.
- Using a larger needle will make it easier to push the injection button during injection. Ask your healthcare provider which needle is best for you.
- The injection button may become harder to push if the inside of the Pen gets dirty with HUMATROPE, food, drink, or other materials.
What should I do if the dose knob does not go to zero (0) when I inject the dose?
- This can happen if the HUMATROPE Cartridge does not have enough HUMATROPE left in it for the full dose.
- At the end of the injection, the number in the dose window should be 0.00. If you see any number other than “0.00”, this is the amount of HUMATROPE you did not receive. Write this number down and follow the steps below to get the rest of your dose.
- To get the rest of your dose:
  
  - Remove the needle and empty Cartridge from the Pen.
  
  - Insert a new Cartridge, attach a new needle, and remove air from the new Cartridge (see Steps 2A through 2D).
  
  - Complete your dose by injecting only the amount you did not receive (see Step 3C).
  
  - If you still do not think you received your full dose, do not take another dose. Call Lilly at 1-800-545-5979 or your healthcare provider for assistance.
What should I do if I see HUMATROPE leaking from the needle after I have finished the injection?
- It is normal for a single drop to remain on the tip of the needle after the injection is complete. If you see more than 1 drop:
  
  - The full dose may not have been delivered. Do not inject another dose. Talk with your healthcare provider for assistance.
  
  - To prevent this, for the next dose, firmly push and hold the injection button in and slowly count to 5 (see Section 3, Step 3C).
How can I tell when the injection is complete?
- The injection is complete when:
  
  - You place your thumb on the injection button, then slowly and firmly push the injection button until it stops moving.
  
  - Continue to hold the injection button for 5 seconds, then remove the needle from the skin.
  
  - You will see 0.00 in the center of the dose window.

Disposing of used needles:

Put your used needles in a FDA-cleared sharps disposal container right away after use. Do not throw away (dispose of) loose needles in your household trash.
If you do not have a FDA-cleared sharps disposal container, you may use a household container that is:

- made of a heavy-duty plastic,

- can be closed with a tight-fitting, puncture-resistant lid, without sharps being able to come out,

- upright and stable during use,

- leak-resistant, and

- properly labeled to warn of hazardous waste inside the container.

This Instructions for Use has been approved by the U.S. Food and Drug Administration.

Manufacturer:
Eli Lilly and Company
Pharmaceutical Delivery Systems
Lilly Corporate Center
Indianapolis, IN 46285, USA

HUMATROPE® and HumatroPen® 6 mg are registered trademarks of Eli Lilly and Company.

This Instructions for Use has been approved by the U.S. Food and Drug Administration.

Manufacturer:
Eli Lilly and Company
Pharmaceutical Delivery Systems
Lilly Corporate Center
Indianapolis, IN 46285, USA

HUMATROPE® and HumatroPen® 12 mg are registered trademarks of Eli Lilly and Company.

This Instructions for Use has been approved by the U.S. Food and Drug Administration.

Manufacturer:
Eli Lilly and Company
Pharmaceutical Delivery Systems
Lilly Corporate Center
Indianapolis, IN 46285, USA

HUMATROPE® and HumatroPen® 24 mg are registered trademarks of Eli Lilly and Company.

Preparing Your New HUMATROPE Cartridge

Start by thoroughly washing your hands. Remove all contents from the tray. Note: The HUMATROPE Cartridge is made for left or right handed use so you may handle it the way that is most comfortable for you.	Hold the gray needle cover at the bottom of the Diluent Syringe.		Pull the needle cover straight down to remove from the Diluent Syringe and throw it away. Do not push the plunger yet. It is okay if a drop of Diluent is seen. You do not have to release air from the Diluent Syringe.

Hold the Cartridge, with the black triangles up toward the Diluent Syringe. Make sure the Cartridge and Diluent Syringe are facing each other in a straight line. Do not insert the Cartridge at an angle.	Push the Cartridge straight into the Diluent Syringe until it stops and the black triangles are covered inside the Diluent Syringe. You may hear or feel a click. Do not twist the Cartridge.		Hold the Diluent Syringe and the Cartridge together with both hands. Push and release the plunger 2 or 3 times until the Diluent is in the Cartridge.

Remove your thumb from the plunger and check that the Diluent Syringe is empty. It is normal for small drops of Diluent to remain in the Diluent Syringe.	With your thumb off the plunger, pull the Cartridge away from the Diluent Syringe.		Place the end cap on a hard, flat surface. Push the Diluent Syringe onto the end cap and throw away the Diluent Syringe right away as instructed by your healthcare provider.

Mix the medicine in the Cartridge by gently moving it in an up and down motion 10 times. Then let the Cartridge sit for 3 minutes. Do not shake.		Check the HUMATROPE liquid, it should be clear. If the liquid is clear, your Cartridge is now prepared and ready to be attached to your HumatroPen (See the Instructions for Use for HumatroPen 6 mg, 12 mg or 24 mg). If the liquid is cloudy or contains particles, gently mix the medicine in the Cartridge 10 more times. Let the Cartridge sit for 5 more minutes. If the liquid still remains cloudy or contains particles, do not use the Cartridge. Contact your healthcare provider or call Lilly at 1-800-545-5979 or go to www.humatrope.com. If you have questions about preparing your HUMATROPE Cartridge, you should contact your healthcare provider.

Indications and Usage (1)	10/2019
Dosage and Administration (2)	10/2019
Contraindications (4)	10/2019
Warnings and Precautions (5)	10/2019

Cartridge	Somatropin Concentration
6 mg	2.08 mg/mL
12 mg	4.17 mg/mL
24 mg	8.33 mg/mL

Step 2C – Attach the needle


Remove the paper tab from the end of the outer cap.	Push the needle straight onto the 12 mg Cartridge and turn it until secure.	Pull off the outer cap and the inner cap. Keep the outer cap to remove the needle after the injection.

Step 2D – Remove air from new Cartridge

Turn the dose knob to dial 2.50 mg.	Point the needle straight up. Push the injection button and hold it for 5 seconds. Dial 0.10 mg and repeat these steps until liquid is seen at the needle tip.

Step 3A – Check the Pen


Pull off the Pen cap. Important Note: Do not use the Pen if any part of the Pen or Cartridge appears broken or damaged. Contact your healthcare provider.	Be sure to check the Cartridge: - For 12 mg Cartridge label - For expiration date - To see if the liquid is clear and free of particles Important Note: Do not use the Cartridge past the expiration date.	Look at the injection button and the front housing to make sure it is a 12 mg Pen. Important Note: Check the number on the front housing to make sure that it matches the Cartridge strength on the Cartridge label. If the Pen and Cartridge do not match, contact your healthcare provider.

Step 2A – Check the Pen and Cartridge
Front View Back View


Be sure to check the Cartridge: - For 24 mg on the Cartridge label - For the expiration date on the opposite side of the Cartridge - To see if the liquid is clear and free of particles Important Notes: Do not use the Cartridge past the expiration date. Do not use the Pen if any part of the Pen or Cartridge appears broken or damaged. Contact your healthcare provider.	Pull off the Pen cap.	Look at the injection button and the front housing to make sure it is a 24 mg Pen. Important Note: Check the number on the front housing to make sure that it matches the Cartridge strength on the Cartridge label. If the Pen and Cartridge do not match, contact your healthcare provider.

Step 2C – Attach the needle


Remove the paper tab from the end of the outer cap.	Push the needle straight onto the 24 mg Cartridge and turn it until secure.	Pull off the outer cap and the inner cap. Keep the outer cap to remove the needle after the injection.

Step 2D – Remove air from new Cartridge

Turn the dose knob to dial 5.00 mg.	Point the needle straight up. Push the injection button and hold it for 5 seconds. Dial 0.20 mg and repeat these steps until liquid is seen at the needle tip.

Before your injection: Take the Pen out of the refrigerator and let it sit for 10 minutes before injecting to allow it to reach room temperature. Injecting medicine that is cold can cause discomfort. Step 3A – Check the Pen