Friday, 4 May 2012

Ventavis



iloprost

Dosage Form: inhalation solution
FULL PRESCRIBING INFORMATION

1. INDICATIONS AND USAGE



Pulmonary Arterial Hypertension


Ventavis is indicated for the treatment of pulmonary arterial hypertension (PAH) (WHO Group 1) to improve a composite endpoint consisting of exercise tolerance, symptoms (NYHA Class), and lack of deterioration. Studies establishing effectiveness included predominately patients with NYHA Functional Class III-IV symptoms and etiologies of idiopathic or heritable PAH (65%) or PAH associated with connective tissue diseases (23%) [see Clinical Studies (14)].



2. DOSAGE AND ADMINISTRATION



Recommended Dosing


Ventavis is intended to be inhaled using either of two pulmonary drug delivery devices: the I-neb® AAD® System or the Prodose® AAD® System. The first inhaled dose should be 2.5 mcg (as delivered at the mouthpiece). If this dose is well tolerated, dosing should be increased to 5.0 mcg and maintained at that dose; otherwise maintain the dose at 2.5 mcg. Ventavis should be taken 6 to 9 times per day (no more than once every 2 hours) during waking hours, according to individual need and tolerability. The maximum daily dose evaluated in clinical studies was 45 mcg (5 mcg 9 times per day).


Direct mixing of Ventavis with other medications in the I-neb® AAD® System or the Prodose® AAD® System has not been evaluated; do not mix with other medications. To avoid potential interruptions in drug delivery due to equipment malfunctions, the patient should have easy access to a back-up I-neb®AAD® System or Prodose® AAD® System.


Ventavis is supplied in 1 mL ampules in two concentrations: 10 mcg/mL and 20 mcg/mL.













Delivered dose from ampule of :
Nebulizer10 mcg/mL20 mcg/mL
I-neb® AAD®2.5 or 5 mcg from one ampule5 mcg from one ampule
Prodose® AAD®2.5 or 5 mcg from two ampulesN/A

The 20 mcg/mL concentration is intended for patients who are maintained at the 5 mcg dose and who have repeatedly experienced extended treatment times which could result in incomplete dosing. Transitioning patients to the 20 mcg/mL concentration using the I-neb® AAD® System will decrease treatment times to help maintain patient compliance.


For each inhalation session, the entire contents of each opened ampule of Ventavis should be transferred into either the I-neb® AAD® System or the Prodose® AAD® System medication chamber immediately before use [see Patient Counseling Information (17.1)]. After each inhalation session, any solution remaining in the medication chamber should be discarded. Use of the remaining solution will result in unpredictable dosing. Patients should follow the manufacturer's instructions for cleaning the I-neb® AAD® System or the Prodose® AAD® System components after each dose administration.



Monitoring


Vital signs should be monitored while initiating Ventavis. [see Warnings and Precautions (5.1)].



Use in patients with pre-existing Hepatic Impairment


Because iloprost elimination is reduced in patients with impaired liver function [see Special Populations (8.6)], consider increasing the dosing interval (e.g., 3-4 hours between doses depending on the patient's response at the end of the dose interval) in patients with Child Pugh Class B or C hepatic impairment.



Use in patients with pre-existing Renal Impairment


Dose adjustment is not required in patients who are not on dialysis. The effect of dialysis on iloprost is unknown [see Special Populations (8.7)].



3. DOSAGE FORMS AND STRENGTHS


1 mL ampules in two concentrations: 10 mcg/mL and 20 mcg/mL.



5. WARNINGS AND PRECAUTIONS


Ventavis solution should not be allowed to come into contact with the skin or eyes; oral ingestion of Ventavis solution should be avoided.



Risk of Syncope


Monitor vital signs while initiating Ventavis. Do not initiate Ventavis in patients with systolic blood pressure below 85 mmHg. Syncope can also occur in association with pulmonary arterial hypertension, particularly in association with physical exertion. The occurrence of exertional syncope may reflect a therapeutic gap or insufficient efficacy, and the need to adjust dose or change therapy should be considered.



Pulmonary venous hypertension


Should signs of pulmonary edema occur when inhaled Ventavis is administered in patients with pulmonary hypertension, stop treatment immediately, as this may be a sign of pulmonary venous hypertension.



Bronchospasm


Ventavis inhalation can induce bronchospasm. Bronchospasm may be more severe or frequent in patients with a history of hyperreactive airways. Ventavis has not been evaluated in patients with chronic obstructive pulmonary disease (COPD), severe asthma, or with acute pulmonary infections.



6. ADVERSE REACTIONS



Clinical Studies Experience


Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials of another drug and may not reflect the rates observed in practice.


Pre-marketing safety data on Ventavis were obtained from 215 patients with pulmonary arterial hypertension receiving iloprost in two 12-week clinical trials and two long-term extensions. Patients received inhaled Ventavis for periods of from 1 day to more than 3 years. The median number of weeks of exposure was 15. Forty patients completed 12 months of open-label treatment with iloprost.


The following table shows adverse events reported by at least 4 Ventavis patients and reported at least 3% more frequently for Ventavis patients than placebo patients in the 12-week placebo-controlled study.
















































































Table 1: Adverse Events in Phase 3 Clinical Trial
Adverse EventVentavis

n = 101
Placebo

n = 102
Placebo subtracted %
Vasodilation (flushing)27918
Cough increased392613
Headache302010
Trismus1239
Insomnia826
Nausea1385
Hypotension1165
Vomiting725
Alk phos increased615
Flu syndrome14104
Back pain734
Tongue pain404
Palpitations743
Syncope853
GGT increased633
Muscle cramps633
Hemoptysis523
Pneumonia413

Pre-marketing serious adverse events reported with the use of inhaled Ventavis and not shown in Table 1 include congestive heart failure, chest pain, supraventricular tachycardia, dyspnea, peripheral edema, and kidney failure.


In a small clinical trial (the STEP trial) [see Clinical Studies (14)], safety trends in patients receiving concomitant bosentan and Ventavis were consistent with those observed in the larger experience of the Phase 3 study in patients receiving only Ventavis or bosentan.



Adverse events with higher doses


In a study in healthy subjects (n=160), inhaled doses of iloprost solution were given every 2 hours, beginning with 5 mcg and increasing up to 20 mcg for a total of 6 dose inhalations (total cumulative dose of 70 mcg) or up to the highest dose tolerated in a subgroup of 40 subjects. There were 13 subjects (32%) who failed to reach the highest scheduled dose (20 mcg). Five were unable to increase the dose because of (mild to moderate) transient chest pain/discomfort/tightness, usually accompanied by headache, nausea, and dizziness. The remaining 8 subjects discontinued for other reasons.



Postmarketing Experience


The following adverse reactions have been identified during the postapproval use of Ventavis. Because these reactions 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.


Cases of bronchospasm and wheezing have been reported, particularly in patients with a history of hyperreactive airways [see Warnings and Precautions (5.3)]. Cases of epistaxis and gingival bleeding have been reported within one month of starting Ventavis treatment. Cases of dizziness, diarrhea, mouth and tongue irritation, dysgeusia, hypersensitivity, and rash have also been reported with the use of Ventavis.



7. DRUG INTERACTIONS


During clinical trials, iloprost was used concurrently with anticoagulants, diuretics, cardiac glycosides, calcium channel blockers, analgesics, antipyretics, nonsteroidal anti-inflammatory drugs, corticosteroids, and other medications. Intravenous infusion of iloprost had no effect on the pharmacokinetics of digoxin. Acetylsalicylic acid did not alter the clearance (pharmacokinetics) of iloprost.



Cytochrome P450


Although clinical studies have not been conducted with Ventavis (inhaled iloprost), in vitro studies of iloprost indicate that no relevant inhibition of cytochrome P450 drug metabolism would be expected.



Antihypertensives and Vasodilators


In studies in normal subjects, there was no pharmacodynamic interaction between intravenous iloprost and either nifedipine, diltiazem, or captopril. However, Ventavis has the potential to increase the hypotensive effect of vasodilators and antihypertensive agents.



Anticoagulants and Platelet Inhibitors


Since Ventavis inhibits platelet function, there is a potential for increased risk of bleeding, particularly in patients maintained on anticoagulants or platelet inhibitors.



8. USE IN SPECIFIC POPULATIONS



Pregnancy



Pregnancy Category C:


Ventavis has been shown to be teratogenic in rats as described below. There are no adequate and well controlled studies in pregnant women. Ventavis should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.


In developmental toxicity studies in pregnant Han-Wistar rats, continuous intravenous administration of iloprost at a dosage of 0.01 mg/kg daily (serum levels not available) led to shortened digits of the thoracic extremity in fetuses and pups. In comparable studies in pregnant Sprague-Dawley rats which received iloprost clathrate (13% iloprost by weight) orally at dosages of up to 50 mg/kg/day (Cmax of 90 ng/mL), in pregnant rabbits at intravenous dosages of up to 0.5 mg/kg/day (Cmax of 86 ng/mL), and in pregnant monkeys at dosages of up to 0.04 mg/kg/day (serum levels of 1 ng/mL), no such digital anomalies or other gross-structural abnormalities were observed in the fetuses/pups. However, in gravid Sprague-Dawley rats, iloprost clathrate (13% iloprost) significantly increased the number of non-viable fetuses at a maternally toxic oral dosage of 250 mg/kg/day and in Han-Wistar rats was found to be embryolethal in 15 of 44 litters at an intravenous dosage of 1 mg/kg/day.



Nursing mothers


It is not known whether Ventavis is excreted in human milk. In studies with Han-Wistar rats, higher mortality was observed in pups of lactating dams receiving iloprost intravenously at 1 mg/kg daily. In Sprague-Dawley rats, higher mortality was also observed in nursing pups at a maternally toxic oral dose of 250 mg/kg/day of iloprost clathrate (13% iloprost by weight). It is not known whether iloprost is excreted in human milk. Because many drugs are excreted in human milk and because of the potential for serious adverse reactions in nursing infants from Ventavis, a decision to discontinue nursing should be made, taking into account the importance of the drug to the mother.



Pediatric use


Safety and efficacy in pediatric patients have not been established.



Geriatric use


Clinical studies of Ventavis did not include sufficient numbers of subjects aged 65 and older to determine whether they respond differently than younger subjects. Other reported clinical experience has not identified differences in responses between elderly and younger patients. In general, dose selection for an elderly patient should be cautious, usually starting at the low end of the dosing range, reflecting the greater frequency of decreased hepatic, renal, or cardiac function and of concomitant disease or other drug therapy.



Hepatic Impairment


Ventavis has not been evaluated in subjects with impaired hepatic function. However, in an intravenous iloprost study in patients with liver cirrhosis, the mean clearance in Child Pugh Class B subjects (n=5) was approximately 10 mL/min/kg (half that of healthy subjects). Following oral administration, the mean AUC0-8h in Child Pugh Class B subjects (n=3) was 1725 pg*h/mL compared to 117 pg*h/mL in normal subjects (n=4) receiving the same oral iloprost dose. In Child Pugh Class A subjects (n=5), the mean AUC0-8h was 639 pg*h/mL. Although exposure increased with hepatic impairment, there was no effect on half-life.



Renal Impairment


Ventavis has not been evaluated in subjects with impaired renal function. However, in a study with intravenous infusion of iloprost in patients with end-stage renal failure requiring intermittent dialysis treatment (n=7), the mean AUC0-4h was 230 pg*h/mL compared to 54 pg*h/mL in patients with renal failure (n=8) not requiring intermittent dialysis and 48 pg*h/mL in normals. The half-life was similar in both groups. The effect of dialysis on iloprost exposure has not been evaluated.



10. OVERDOSAGE


In clinical trials of Ventavis, no case of overdose was reported. Signs and symptoms to be anticipated are extensions of the dose-limiting pharmacological effects, including hypotension, headache, flushing, nausea, vomiting, and diarrhea. A specific antidote is not known. Interruption of the inhalation session, monitoring, and symptomatic measures are recommended.



11. DESCRIPTION


Ventavis (iloprost) Inhalation Solution is a clear, colorless, sterile solution containing iloprost formulated for inhalation via either of two pulmonary drug delivery devices: the I-neb® AAD® (Adaptive Aerosol Delivery) System or the Prodose® AAD® System. Ventavis is supplied in 1 mL single-use glass ampules containing either 10 mcg/mL or 20 mcg/mL.


For the 10 mcg/mL solution, one mL of the solution contains 0.01 mg iloprost, 0.81 mg ethanol, 0.121 mg tromethamine, 9.0 mg sodium chloride, and approximately 0.51 mg hydrochloric acid (for pH adjustment to 8.1) in water for injection.


For the 20 mcg/mL solution, one mL of the solution contains 0.02 mg iloprost, 1.62 mg ethanol, 0.242 mg tromethamine, 9.0 mg sodium chloride, and approximately 0.76 mg hydrochloric acid (for pH adjustment to 8.4) in water for injection.


The solution contains no preservatives.


The chemical name for iloprost is (E)-(3aS, 4R, 5R, 6aS) - hexahydro - 5 - hydroxy - 4 - [(E) - (3S,4RS) - 3 - hydroxy - 4 - methyl - 1 - octen - 6 - ynyl] - Δ2(1H),Δ - pentalenevaleric acid. Iloprost consists of a mixture of the 4R and 4S diastereoisomers at a ratio of approximately 53:47. Iloprost is an oily substance, which is soluble in methanol, ethanol, ethyl acetate, acetone, and pH 7 buffer, sparingly soluble in buffer pH 9, and very slightly soluble in distilled water, buffer pH 3, and buffer pH 5. The molecular formula of iloprost is C22H32O4. Its relative molecular weight is 360.49. The structural formula is shown below:




12. CLINICAL PHARMACOLOGY



Mechanism of Action


Iloprost is a synthetic analog of prostacyclin PGI2. Iloprost dilates systemic and pulmonary arterial vascular beds. It also affects platelet aggregation but the relevance of this effect to the treatment of pulmonary hypertension is unknown. The two diastereo isomers of iloprost differ in their potency in dilating blood vessels, with the 4S isomer substantially more potent than the 4R isomer.



Pharmacokinetics



General: In pharmacokinetic studies in animals, there was no evidence of interconversion of the two diastereoisomers of iloprost. In human pharmacokinetic studies, the two diastereoisomers were not individually assayed.


Iloprost administered intravenously has linear pharmacokinetics over the dose range of 1 to 3 ng/kg/min. The half-life of iloprost is 20 to 30 minutes. Following inhalation of iloprost (5 mcg) patients with pulmonary hypertension have iloprost peak plasma levels of approximately 150 pg/mL. Iloprost was generally not detectable in plasma 30 minutes to 1 hour after inhalation.



Absorption and Distribution: The absolute bioavailability of inhaled iloprost has not been determined. Following intravenous infusion, the apparent steady-state volume of distribution was 0.7 to 0.8 L/kg in healthy subjects. Iloprost is approximately 60% protein-bound, mainly to albumin, and this ratio is concentration-independent in the range of 30 to 3000 pg/mL.



Metabolism and Excretion: In vitro studies reveal that cytochrome P450-dependent metabolism plays only a minor role in the biotransformation of iloprost. Iloprost is metabolized principally via β-oxidation of the carboxyl side chain. The main metabolite is tetranor-iloprost, which is found in the urine in free and conjugated form. In animal experiments, tetranor-iloprost was pharmacologically inactive.


Clearance in normal subjects was approximately 20 mL/min/kg.


A mass-balance study using intravenously and orally administered [3H]-iloprost in healthy subjects (n=8) showed recovery of 81% of total radioactivity over 14 hours post-dose, with 68% and 12% recoveries in urine and feces, respectively.



13. NONCLINICAL TOXICOLOGY



Carcinogenesis, Mutagenesis, Impairment of Fertility


Iloprost was not mutagenic in bacterial and mammalian cells in the presence or absence of extrinsic metabolic activation. Iloprost did not cause chromosomal aberrations in vitro in human lymphocytes and was not clastogenic in vivo in NMRI/SPF mice. There was no evidence of a tumorigenic effect of iloprost clathrate (13% iloprost by weight) in Sprague-Dawley rats dosed orally for up to 8 months at doses of up to 125 mg/kg/day (Cmax of 45 ng/mL serum), followed by 16 months at 100 mg/kg/day, or in Crl:CD-1®(ICR)BR albino mice dosed orally for up to 24 months at doses of up to 125 mg/kg/day (Cmax of 156 ng/mL serum). The recommended clinical dosage regimen for iloprost (5 mcg) affords a serum Cmax of 0.16 ng/mL. Fertility of males or females was not impaired in Han-Wistar rats at intravenous doses up to 1 mg/kg/day.



14. CLINICAL STUDIES


A randomized, double-blind, multi-center, placebo-controlled trial was conducted in 203 adult patients (inhaled iloprost: n=101; placebo: n=102) with NYHA Class III or IV pulmonary arterial hypertension (PAH, WHO Group 1; idiopathic in 53%, associated with connective tissue disease, including CREST and scleroderma, in 17%, or associated with anorexigen use in 2%) or PAH related to chronic thromboembolic disease (WHO Group 4; 28%). Inhaled iloprost (or placebo) was added to patients' current therapy, which could have included anticoagulants, vasodilators (e.g., calcium channel blockers), diuretics, oxygen, and digoxin, but not PGI2 (prostacyclin or its analogs) or endothelin receptor antagonists. Patients received 2.5 or 5.0 mcg of iloprost by repeated inhalations 6 to 9 times per day during waking hours. The mean age of the entire study population was 52 years and 68% of the patients were female. The majority of patients (59%) were NYHA Class III. The baseline 6-minute walk test values reflected a moderate exercise limitation (the mean was 332 meters for the iloprost group and 315 meters for the placebo group). In the iloprost group, the median daily inhaled dose was 30 mcg (range of 12.5 to 45 mcg/day). The mean number of inhalations per day was 7.3. Ninety percent of patients in the iloprost group never inhaled study medication during the nighttime.


The primary efficacy endpoint was clinical response at 12 weeks, a composite endpoint defined by: a) improvement in exercise ability (6-minute walk test) by at least 10% versus baseline evaluated 30 minutes after dosing, b) improvement by at least one NYHA class versus baseline, and c) no death or deterioration of pulmonary hypertension. Deterioration required two or more of the following criteria: 1) refractory systolic blood pressure < 85 mmHg, 2) worsening of right heart failure with cardiac edema, ascites, or pleural effusion despite adequate background therapy, 3) rapidly progressive cardiogenic hepatic failure (e.g., leading to an increase of GOT or GPT to > 100 U/L, or total bilirubin ≥ 5 mg/dL), 4) rapidly progressive cardiogenic renal failure (e.g., decrease of estimated creatinine clearance to ≤ 50% of baseline), 5) decrease in 6-minute walking distance by ≥ 30% of baseline value, 6) new long-term need for i.v. catecholamines or diuretics, 7) cardiac index ≤ 1.3 L/min/m2, 8) CVP ≥ 22 mmHg despite adequate diuretic therapy, and 9) SVO2 ≤ 45% despite nasal O2 therapy.


Although effectiveness was seen in the full population (response rates for the primary composite endpoint of 17% and 5%; p=0.007), there was inadequate evidence of benefit in patients with pulmonary hypertension associated with chronic thromboembolic disease (WHO Group 4); the results presented are therefore those related to patients with PAH (WHO Group 1). The response rate for the primary efficacy endpoint among PAH patients was 19% for the iloprost group, compared with 4% for the placebo group (p=0.0033). All three components of the composite endpoint favored iloprost (Figure 1).



The absolute change in 6-minute walk distance (Figure 2) measured (using all available data and no imputation) 30 minutes after inhalation among patients with PAH was greater in the iloprost group compared to the placebo group at all time points. At Week 12, the placebo-corrected difference was 40 meters (p<0.01). When walk distance was measured immediately prior to inhalation, the improvement compared to placebo was approximately 60% of the effect seen at 30 minutes after inhalation.


Figure 2: Change (Mean ± SEM) in 6-Minute Walk Distance 30 Minutes post Inhalation in PAH Patients (WHO Group 1).



The effect of Ventavis in various subgroups is shown in Table 2.











































































































Table 2: Treatment Effects by Subgroup among PAH Patients (WHO Group 1)
Composite Clinical Endpoint6-Minute Walk (m)*
nVentavis

n (%)
nPlacebo

n (%)
nVentavis

(mean ±SD)
nPlacebo

(mean ±SD)

*

Change from baseline to 12 Weeks with measurement 30 minutes after dosing, based on all available data.


etiologies of PAH, WHO Group 1 included idiopathic in 62% (n=90), associated with connective tissue disease, including CREST and scleroderma, in 17%, (n=25), associated with anorexigen use in 6% (n=9), heritable PAH in 3% (n=5), other PPH in 3% (n=5), SLE in 1% (n=2), post-partum in 1% (n=2), and overlap/other in 5% (n=8).

All Subjects with PAH6813 (19%)783 (4%)6431 ± 7665-9 ± 79
         
NYHA III407 (18%)472 (4%)3924 ± 7243-16 ± 86
NYHA IV
286 (21%)311 (3%)2543 ± 82226 ± 63
         
Male235 (22%)240 (0%)2137 ± 8121-22 ± 77
Female
458 (18%)543 (6%)4329 ± 7444-2 ± 81
         
Age ≤ 55416 (15%)402 (5%)3924 ± 7932-5 ± 78
Age > 55277 (26%)381 (3%)2542 ± 7133-13 ± 81

Hemodynamic assessments obtained at week 12 before inhalation in both groups (at least 2 hours after a previous dose, trough) and after inhalation in the iloprost group (approximately 15 minutes after a dose, peak), are shown in Table 3. The relationship between hemodynamic changes and clinical effects is unknown.











































Table 3 Hemodynamic Parameters Before and After Iloprost Inhalation: Change from Baseline to Week 12*
BaselineMean (± SD) change from baseline at Week 12
ParameterIloprostPlaceboIloprostPlacebo
Before InhalationAfter Inhalation

*

Patients of all etiologies of PAH, including CTEPH.



PVR (dyn∙s∙cm–5)
1029 ± 3901041 ± 493-9 ± 275

(n=76)
-239 ± 279

(n=70)
+96 ± 323

(n=77)


mPAP (mmHg)
53 ± 1254 ± 14-0.2 ± 7.3

(n=93)
-4.6 ± 9.3

(n=90)
-0.1 ± 6.9

(n=82)


CO (L/min)
3.8 ± 1.13.8 ± 0.9+0.1 ± 0.9

(n=91)
+0.5 ± 1.1

(n=89)
-0.2 ± 0.8

(n=80)
SVO2 (%)
60 ± 860±8-1.1 ± 7.6

(n=72)
+1.8 ± 8.3

(n=70)
-3.2 ± 6.7

(n=63)

In a small, randomized, double-blind, placebo-controlled study (the STEP trial), 34 patients treated with bosentan 125 mg bid for at least 16 weeks tolerated the addition of inhaled iloprost (up to 5 mcg 6 to 9 times per day during waking hours). The mean daily inhaled dose was 27 mcg and the mean number of inhalations per day was 5.6.



16. HOW SUPPLIED/STORAGE AND HANDLING


Ventavis (iloprost) Inhalation Solution is supplied in cartons of 30 × 1 mL clear glass single-use ampules as follows:


1 mL ampule containing iloprost 10 mcg per mL, carton of 30 (NDC 66215-302-30)


1 mL ampule containing iloprost 20 mcg per mL, carton of 30 (NDC 66215-303-30)



STORAGE


Store at 20 – 25°C (68 – 77°F)


Excursions permitted to 15 – 30°C (59 – 86°F)


[See USP Controlled Room Temperature]



17. PATIENT COUNSELING INFORMATION


Patients receiving Ventavis should be advised to use the drug only as prescribed with either of two pulmonary drug delivery devices: the I-neb® AAD® System or the Prodose® AAD® System, following the manufacturer's instructions. Patients should be trained in proper administration techniques including dosing frequency, ampule dispensing, I-neb® AAD® System or the Prodose® AAD® System operation, and equipment cleaning.


Advise patients that they may have a fall in blood pressure with Ventavis, so they may become dizzy or even faint. They should stand up slowly when they get out of a chair or bed. If fainting gets worse, patients should consult their physicians about dose adjustment.


Advise patients that Ventavis should be inhaled at intervals of not less than 2 hours and that the acute benefits of Ventavis may not last 2 hours. Thus patients may want to adjust times of administration to cover planned activities.



Preparation Instructions


Ventavis ampules may be opened with a rubber pad or with an ampule breaker.
















When using a rubber pad:When using an ampule breaker:
1. With one hand, hold the bottom of the ampule with the blue dot facing away from your body.
1. Align the blue dot on the Ventavis ampule with the dot on the ampule breaker, if available, and then insert the top of the ampule into the ampule breaker.
2. With the other hand, wrap the included rubber pad around the entire ampule.
2. Gently break open the neck of the ampule by levering away from the dot on the Ventavis ampule to snap off the ampule lid.
3. Using your thumbs, break open the neck of the ampule by snapping the top towards you and then carefully dispose of the top of the ampule into a sharps bin.
3. Carefully dispose of the top of the ampule into a sharps bin or appropriate storage container.

For either:


4. After opening the ampule, use the small tube (pipette) supplied with Ventavis, draw-up the entire amount of one ampule of Ventavis and transfer the entire contents of the ampule into the medication chamber of either the I-neb® AAD® System or the Prodose® AAD® System. If using the Prodose® AAD® System, two 10 mcg/mL ampules need to be added to the medication chamber.



5. Safely dispose of the open ampule and pipette as instructed by your healthcare practitioner. Keep ampules and pipettes out of the reach of children.




Manufactured for:


Actelion Pharmaceuticals US, Inc.

5000 Shoreline Court, Ste. 200

South San Francisco, CA 94080


©2011 Actelion Pharmaceuticals US, Inc.

ACT20110215



PATIENT INFORMATION


Ventavis (ven TAY vis)

(iloprost)

Inhalation Solution


Read the Patient Information that comes with Ventavis before you start using it and each time you get a refill. There may be new information. The leaflet does not take the place of talking with your doctor about your medical condition or your treatment.


What is Ventavis?


Ventavis is a prescription medicine used to treat adults with certain kinds of severe pulmonary arterial hypertension (PAH), a condition in which blood pressure is too high in the blood vessels between the heart and the lungs. Ventavis may improve your ability to exercise and your symptoms for a short time by lowering your blood pressure and opening up the blood vessels in your lungs.


Ventavis has not been studied in children younger than 18 years old.


What should I tell my doctor before taking Ventavis?


Ventavis may not be right for you. Before taking Ventavis, tell your doctor about all of your medical conditions, including if you:


  • have liver or kidney problems. Your doctor may need to give you a lower dose of Ventavis.

  • are pregnant, or plan to become pregnant. It is not known if Ventavis can harm your unborn baby. Ventavis should only be used during pregnancy if the benefit to you is worth the possible risk to your baby.

  • are breast-feeding. It is not known if Ventavis passes into your breast milk. You and your doctor should decide if you will take Ventavis or breast feed.

Tell your doctor about all the medicines you take, including prescription and nonprescription medicines, vitamins, and herbal supplements.


Ventavis and other medicines may affect each other causing side effects. Ventavis may affect the way other medicines work, and other medicines may affect how Ventavis works.


Especially tell your doctor if you take:


  • medicines used to treat high blood pressure or heart problems

  • medicines that lessen blood clotting (warfarin, Coumadin, Jantoven)

Know the medicines you take. Keep a list of your medicines and show it to your doctor and pharmacist when you get a new medicine.


How should I take Ventavis?


See the end of this leaflet for detailed instructions for using Ventavis.


  • Take Ventavis exactly as your doctor tells you to take it. Your doctor may change your dose if needed.

  • You should not take Ventavis more than every 2 hours. The benefits of Ventavis may not last 2 hours, so you may adjust the times that you use it to cover planned activities.

  • Do not drink Ventavis.

  • Do not let Ventavis solution come into contact with your skin or eyes. If it does, rinse your skin or eyes with water right away.

  • Do not allow other people to be exposed to Ventavis while you are breathing it, especially babies and pregnant women.

  • If you take too much Ventavis, you may have a headache, red face, dizziness, nausea, vomiting and diarrhea. If this happens stop taking Ventavis. If your symptoms do not go away, call your doctor or get emergency help right away.

What are the possible side effects of Ventavis?


Ventavis may cause side effects, including feeling dizzy, lightheaded and faint. If you have any of these side effects, you should stand up slowly when you get out of chairs or bed. Tell your doctor if your fainting gets worse during treatment with Ventavis. Your doctor may need to change your dose or your treatment.


Do not drive a car or operate any tools or machines if dizziness or fainting from low blood pressure is a problem for you.


You may have trouble breathing after taking Ventavis because it may cause the muscles around your airway to tighten (bronchospasm). Get emergency help right away if you have trouble breathing.


The most common side effects of Ventavis include:


  • red face (flushing)

  • increased cough

  • low blood pressure

  • headaches

  • nausea

  • spasm of your jaw muscles that makes it hard to open your mouth

  • fainting

Talk to your doctor if you have any side effect that bothers you or that does not go away.


These are not all the possible side effects of Ventavis. For more information, ask your doctor or pharmacist.


Call your doctor for medical advice about side effects. You may report side effects to the FDA at 1-800-FDA 1088.


How should I store Ventavis?


  • Store Ventavis between 68°F to 77°F (20°C to 25°C).

  • Safely throw away Ventavis that is out of date or no longer needed.

Keep Ventavis and all medicines out of the reach of children.


General Information about Ventavis


Medicines are sometimes prescribed for conditions that are not listed in the patient leaflet. Do not use Ventavis for a condition for which it was not prescribed. Do not give Ventavis to other people, even if they have the same symptoms you have. It may harm them.


This patient information leaflet summarizes the most important information about Ventavis. If you would like more information about Ventavis talk with your doctor. You can ask your doctor or pharmacist for information about Ventavis that is written for health professionals. For more information go to www. Ventavis.com or call 1-866-ACTELION (1-866-228-3546).


What are the ingredients in Ventavis?


Active ingredient: iloprost


Inactive ingredients: tromethamine, ethanol, sodium chloride, hydrochloric acid for pH adjustment, and water for injection.


Patient Instructions for Using Ventavis


To take Ventavis, you will need to use either the Prodose Adaptive Aerosol Delivery (AAD) System or the I-neb Adaptive Aerosol Delivery (AAD) System. These systems are used to give you the right dose of Ventavis. You should not use other systems to take Ventavis as other systems may not give you the amount of Ventavis you need.


Do not use Ventavis until your doctor has showed you how to use one of these systems the right way. Make sure you understand all the instructions or ask questions until you do.






I-neb AAD SystemProdose AAD System

If you are using the Prodose System, your doctor will give you 2 dosing discs for it.







     Prodose AAD System Dosing Discs

     


     The Prodose dosing discs are white with a red band (2.5 mcg) or purple band (5 mcg) across each disc.

These dosing discs will control the amount of Ventavis you use. Do not change the dosing disc in your Prodose System without talking to your doctor. Always use all of the contents of 2 ampules (10 microgram per 1 mL only) when using your Prodose System.






     Ventavis Ampule

     


If you use less than the 2 mL of liquid with the Prodose System it may not give you enough medicine.


If you are using the I-neb System, you will receive two

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