Consumer medicine information

Tobi Podhaler

Tobramycin

BRAND INFORMATION

Brand name

Tobi, Tobi Podhaler

Active ingredient

Tobramycin

Schedule

SUMMARY CMI

TOBI^® Podhaler^®

Consumer Medicine Information (CMI) summary

The full CMI on the next page has more details. If you are worried about using this medicine, speak to your doctor or pharmacist.

1. Why am I using TOBI Podhaler?

TOBI Podhaler contains the active ingredient tobramycin. TOBI Podhaler is used to treat lung infections caused by a bacterium called Pseudomonas aeruginosa, in patients who have cystic fibrosis.

For more information, see Section 1. Why am I using TOBI Podhaler? in the full CMI.

2. What should I know before I use TOBI Podhaler?

Do not use if you have ever had an allergic reaction to tobramycin or any of the ingredients listed at the end of the CMI.

Talk to your doctor if you have any other medical conditions, take any other medicines, or are pregnant or plan to become pregnant or are breastfeeding.

For more information, see Section 2. What should I know before I use TOBI Podhaler? in the full CMI.

3. What if I am taking other medicines?

Some medicines may interfere with TOBI Podhaler and affect how it works.

A list of these medicines is in Section 3. What if I am taking other medicines? in the full CMI.

4. How do I use TOBI Podhaler?

The usual dose for all patients aged 6 years and older is 4 capsules for inhalation taken every 12 hours (each morning and evening).
Do not exceed the recommended dose.

More instructions can be found in Section 4. How do I use TOBI Podhaler? in the full CMI.

5. What should I know while using TOBI Podhaler?

Things you should do	Remind any doctor, dentist or pharmacist you visit that you are using TOBI Podhaler. Once removed from the blister strip, use the capsule immediately. Use a new Podhaler device after 7 days. Discard the old one. Tell your doctor if you become pregnant while using TOBI Podhaler. Keep all of your doctor's appointments so that your progress can be checked. If you are about to be started on any new medicine, remind your doctor and pharmacist that you are using TOBI Podhaler.
Things you should not do	Do not swallow the capsules. The powder in the capsules are taken by inhalation only, using a Podhaler device that is provided in the pack. Do not use other capsules or powders in the Podhaler device. Do not wash the Podhaler device. Do not change or lower the dosage, without checking with your doctor.
Driving or using machines	TOBI Podhaler should not affect your ability to drive and use machines.
Looking after your medicine	Store this medicine in a cool, dry place, where the temperature stays below 30°C.

For more information, see Section 5. What should I know while using TOBI Podhaler? in the full CMI.

6. Are there any side effects?

For more information, including what to do if you have any side effects, see Section 6. Are there any side effects? in the full CMI.

FULL CMI

TOBI^® Podhaler^®

Active ingredient(s): tobramycin

Consumer Medicine Information (CMI)

This leaflet provides important information about using TOBI Podhaler. You should also speak to your doctor or pharmacist if you would like further information or if you have any concerns or questions about using TOBI Podhaler.

Where to find information in this leaflet:

1. Why am I using TOBI Podhaler?
2. What should I know before I use TOBI Podhaler?
3. What if I am taking other medicines?
4. How do I use TOBI Podhaler?
5. What should I know while using TOBI Podhaler?
6. Are there any side effects?
7. Product details

1. Why am I using TOBI Podhaler?

TOBI Podhaler contains the active ingredient tobramycin in a powdered form. TOBI Podhaler is a class of medicines called aminoglycoside antibiotics.

Pseudomonas aeruginosa is a very common bacterium that infects the lung of nearly everyone with cystic fibrosis, at some time during their lives. Some people do not get this infection until later on in their lives, while others get it very young. This infection is one of the most damaging bacteria for people with cystic fibrosis. If it is not properly fought, it will continue to damage your lungs causing further problems to your breathing.

TOBI Podhaler capsules are for oral inhalation only. The powder from the capsule is inhaled (breathed into the lungs), using the TOBI Podhaler inhalation device provided with the medicine. When you inhale the powder, tobramycin gets directly into your lungs, to fight against the Pseudomonas aeruginosa bacteria causing the infection.

TOBI Podhaler is used to TOBI Podhaler is used to treat lung infections caused by a bacterium called pseudomonas aeruginosa, in patients who have cystic fibrosis.

TOBI Podhaler is only available with a doctor's prescription. It is not addictive. This medicine can be used in children aged 6 years or over, adolescents, and adults.

2. What should I know before I use TOBI Podhaler?

Warnings

Do not use TOBI Podhaler if:

you are allergic to tobramycin, any type of aminoglycoside antibiotic, or any of the ingredients listed at the end of this leaflet. See symptoms of an allergic reaction under Section 6. Are there any side effects?.

Always check the ingredients to make sure you can use this medicine.

Do not give TOBI Podhaler to a child below the age of 6, unless directed to by the child's doctor or pharmacist.

Check with your doctor if you:

have allergies to any other medicines or any other substances, such as foods, preservatives or dyes. See symptoms of an allergic reaction under Section 6. Are there any side effects?.
aged 65 years or older, your doctor may perform additional tests to decide if TOBI Podhaler is right for you. Your doctor will supervise your first dose of this medicine and check your lung function before and after dosing.
are taking any other medicines
have hearing problems (including noises in the ears and dizziness)
have Kidney problems
have unusual difficulty in breathing with wheezing or coughing, chest tightness
blood in your sputum (the substance you cough up)
have muscle weakness that lasts or becomes worse in time, a symptom mostly related to conditions such as myasthenia or Parkinson's disease.

During treatment, you may be at risk of developing certain side effects. It is important you understand these risks and how to monitor for them. See additional information under Section 6. Are there any side effects?

Pregnancy and breastfeeding

Check with your doctor if you are pregnant or intend to become pregnant.

TOBI Podhaler may affect your developing baby if you use it during pregnancy. Your doctor or pharmacist will discuss the possible risks and benefits of using TOBI Podhaler during pregnancy.

Talk to your doctor if you are breastfeeding or intend to breastfeed.

Your baby may absorb this medicine from breast milk and therefore there is a possibility of harm to the baby. Your doctor or pharmacist will discuss the risks and benefits of using TOBI Podhaler during breastfeeding.

3. What if I am taking other medicines?

Tell your doctor or pharmacist if you are taking any other medicines, including any medicines, vitamins or supplements that you buy without a prescription from your pharmacy, supermarket or health food shop.

Some medicines may interfere with TOBI Podhaler and affect how it works.

diuretics (fluid tablets), especially those that contain furosemide (frusemide), etacrynic acid, urea or intravenous mannitol
tobramycin or another aminoglycoside antibiotic by injection (eg. amikacin, gentamicin, neomycin, streptomycin

Medicines that may increase the effect of TOBI Podhaler include:

Amphotericin B (amphotericin) (an antifungal medicine)
Cefalotin or polymyxins (antibiotic medicines)
Ciclosporin or tacrolimus (medicines that help to control your body's immune system)
Carboplatin, cisplatin, or other platinum compounds (usually used in the treatment of various cancer types)
Anticholinesterase medicines, such as neostigmine and pyridostigmine
Botulinum toxin (a medicine used to relax muscles)

Check with your doctor or pharmacist if you are not sure about what medicines, vitamins or supplements you are taking and if these affect TOBI Podhaler.

4. How do I use TOBI Podhaler?

How much to use

The usual dose for all patients aged 6 years and older is 4 capsules for inhalation taken every 12 hours (each morning and evening).
Do not exceed the recommended dose.
Follow the instructions provided when TOBI Podhaler was prescribed, including the number of days it should be taken.
Always use TOBI Podhaler exactly as your doctor has told you.
Your doctor may ask you to use other medicines before using TOBI Podhaler.
You should check with your doctor if you are not sure.
Children 6 years and over should use this medicine with the help of an adult.
When initiating children on Podhaler treatment, caregivers should particularly provide assistance to those aged 10 years or younger, and should continue to supervise them until they are able to use the Podhaler inhaler properly without help. If you are not sure how to use the medicine and Podhaler device, which are provided in the pack, ask your doctor or pharmacist.

When to use TOBI Podhaler

TOBI Podhaler should be used twice a day (morning and evening) at about the same time each day. You must leave as close as possible to 12 hours between doses.
Using your medicine at the same time each day will help you remember when to take it. TOBI Podhaler is taken in a 28 day cycle.
After taking the medicine for 28 days, you will have a 28-day break, during which you do not inhale any TOBI Podhaler. You then start another course.
Please check the order of medications with your doctor.
If you are taking several different inhaled treatments and performing therapies for cystic fibrosis, you should use TOBI Podhaler last.

How to use TOBI Podhaler

USE A NEW PODHALER INHALATION DEVICE EVERY WEEK

Wash and fully dry hands.

Just before use, remove the Podhaler device from its case by holding the base and twisting off the top of the case in a counter-clockwise direction. Set the top of the case aside. Briefly inspect the inhaler to make sure it is not damaged or dirty, and then stand it in the base of the case.

Holding the body of the inhaler, unscrew and remove the mouth piece from the inhaler body. Set the mouth piece aside on a clean, dry surface.

Separate the morning and evening doses from the capsule card. Peel back the foil from the capsule card to reveal one capsule and remove it from the card.

Immediately insert the capsule into the inhaler chamber. Replace the mouth piece and screw it on firmly until it stops. Do not over tighten.

The medication is now ready for inhalation.

Fully exhale away from the inhaler

Position the inhaler with the mouth piece facing towards you. Place mouth over the mouth piece creating a tight seal. Inhale the powder deeply with a single continuous inhalation.

Remove inhaler from mouth, and hold breath for a count of approximately 5 seconds then exhale normally away from the inhaler.

After a few normal breaths, perform a second inhalation from the same capsule, repeating steps 7, 8 and 9.

Unscrew mouth piece and remove the capsule from the chamber. Inspect the used capsule. It should appear punctured and empty .

If the capsule is punctured but still contains some powder, place it back into the chamber with the punctured side of the capsule inserted first, replace the mouth piece and take another two inhalations from the capsule (repeat step 5, then steps 7 to 11). Reinspect capsule.

If the capsule appears to be unpunctured, place it back into the chamber, replace the mouth piece, press the button firmly as far as it goes and take another two inhalations from the capsule (repeat steps 5 to 11). If the capsule is still full and appears to be unpunctured, replace the inhaler with the reserve inhaler and try again (repeat steps 2, 3, and 5 to 11). Discard the empty capsule.

Repeat, starting at step 4, for the remaining 3 capsules of the dose.

Replace the mouth piece and screw it on firmly until it stops. When the full dose (4 capsules) has been inhaled, wipe the mouthpiece with a clean, dry cloth.

Place inhaler back in storage case and close tightly. The inhaler should never be washed with water.

Continue to take TOBI Podhaler, in the cycling pattern, for as long as your doctor tells you.

It is important that you keep using the product twice each day during your 28 days on treatment and that you keep to the 28-day on and 28-day off cycle. Continue to take TOBI, in the cycling pattern, for as long as your doctor tells you.

If you forget to use TOBI Podhaler

TOBI Podhaler should be used should be used twice a day (morning and evening) at about the same time each day. You must leave as close as possible to 12 hours between doses. If you miss your dose at the usual time, take your dose as soon as you remember if there are at least 6 hours to your next dose. Then go back to using your medicine as you would normally.

If it is almost time for your next dose, skip the dose you missed and take your next dose when you are meant to.

Do not take a double dose to make up for the dose you missed.

This may increase the chance of you getting an unwanted side effect.

Use your medicine at the same time each day. This will help you remember to take your medicine dose.
If you have trouble remembering when to use your medicine, ask your doctor or pharmacist for some hints.

If you use too much TOBI Podhaler

If you think that you have used too much TOBI Podhaler, you may need urgent medical attention.

You should immediately:

phone the Poisons Information Centre (Australia telephone 13 11 26) for advice, or
contact your doctor, or
go to the Emergency Department at your nearest hospital.

You should do this even if there are no signs of discomfort or poisoning.

If you use too much of this medicine, you may feel:

dizziness
ringing in the ears
loss of hearing
difficulty or decreased breathing
weakness

5. What should I know while using TOBI Podhaler?

Things you should do

Once removed from the blister strip, use the capsule immediately.
Avoid using the product in a very humid environment, for example in tropical regions or in bathrooms.
Use a new Podhaler device after 7 days. Discard the old one.
Keep all of your doctor's appointments so that your progress can be checked. Over time, strains of Pseudomonas can become resistant to the treatment of an antibiotic. This may mean that TOBI Podhaler may not work as well as it should over time.

Call your doctor straight away if you:

become pregnant.
are about to be started on any new medicine.
experience a persistent cough and it is worrying you. Inhaling medicines can also cause cough and this may happen when using this medicine. Inhaling medicines can cause chest tightness and wheezing. This may happen immediately after inhaling this medicine.
are taking tobramycin or another aminoglycoside antibiotic by injection, it may sometimes cause hearing loss, dizziness, and kidney damage, and may harm an unborn child.

Remind any doctor, dentist or pharmacist you visit that you are using TOBI Podhaler.

Things you should not do

Do not swallow the capsules. The powder in the capsules are taken by inhalation only, using a Podhaler device that is provided in the pack. If you have swallowed the capsules in error, tell your doctor as soon as possible. When swallowed, the capsules will not harm you, but this medicine will not work against your lung infection, as it is meant to.
Do not give this medicine to anyone else, even if they have the same condition as you.
Do not use other capsules or powders in the Podhaler device.
Do not wash the Podhaler device.
Do not change or lower the dosage, without checking with your doctor.

Driving or using machines

Be careful before you drive or use any machines or tools until you know how TOBI Podhaler affects you.

TOBI Podhaler should not affect your ability to drive and use machines.

Looking after your medicine

Clean the Podhaler after each use by wiping it with a clean dry cloth or tissue.

It is important to keep your Podhaler clean and dry. It may not work as well if it gets dirty or wet.

Keep your medicine in the original container until it is time to use it.

Keep the Podhaler in its tightly closed case when not in use.

Follow the instructions in the carton on how to take care of your medicine properly.

Store it in a cool dry place away from moisture, heat or sunlight; for example, do not store it:

in the bathroom or near a sink, or
in the car or on window sills.

Keep it where young children cannot reach it.

When to discard your medicine (as relevant)

Discard your medicine when your doctor stops your treatment with TOBI Podhaler or you find that it has passed the expiry date.

Getting rid of any unwanted medicine

If you no longer need to use this medicine or it is out of date, take it to any pharmacy for safe disposal.

Do not use this medicine after the expiry date.

6. Are there any side effects?

All medicines can have side effects. If you do experience any side effects, most of them are minor and temporary. However, some side effects may need medical attention.

See the information below and, if you need to, ask your doctor or pharmacist if you have any further questions about side effects.

Less serious side effects

Less serious side effects

What to do

Respiratory system:

Shortness of breath
Cough or a productive cough
Voice alteration (hoarseness)
Loss of your voice
Sore throat
Headache
Fever
Wheezing, crackles
Chest discomfort, chest pain from muscles and/or skeleton origins
Decreased results for the tests of lung function
High level of sugar (glucose) in the blood
Blocked nose
Nosebleed
Vomiting, nausea
Diarrhoea
Rash
Disturbed sense of taste

Speak to your doctor if you have any of these less serious side effects and they worry you.

Serious side effects

Serious side effects	What to do
Unusual difficulty in breathing, with wheezing or coughing or chest tightness Worsening of your underlying lung disease Coughing up blood Decreasing hearing (ringing in the ears is a potential warning sign of hearing loss) Noises (such as hissing) in the ears Generally feeling unwell Discoloration of the substance you cough up (sputum)	Call your doctor straight away, or go straight to the Emergency Department at your nearest hospital if you notice any of these serious side effects.

Allergic reactions

Severe rash, itching or hives on the skin
Swelling of the face, lips, tongue which may cause difficulty in swallowing or breathing, or swelling of any other parts of the body
Fast heart beat, dizziness, vertigo, unsteadiness, and light headedness
Wheezing or shortness of breath

Tell your doctor or pharmacist asap if you notice anything that is making you feel unwell.

Tell your doctor or pharmacist if you notice anything else that may be making you feel unwell.

Other side effects not listed here may occur in some people.

Reporting side effects

After you have received medical advice for any side affects you experience, you can report side effects to the Therapeutic Goods Administration online at www.tga.gov.au/reporting-problems. By reporting side effects, you can help provide more information on the safety of this medicine.

Always make sure you speak to your doctor or pharmacist before you decide to stop taking any of your medicines.

7. Product details

This medicine is only available with a doctor's prescription.

What TOBI Podhaler contains

Active ingredient (main ingredient)	Tobramycin
Other ingredients (inactive ingredients)	Distearoylphosphatidylcholine Calcium chloride dihydrate Sulfuric acid (for pH adjustment) The capsule shell contains: Hypromellose (E464) Potassium chloride (E508) Carrageenan (E407) Carnauba wax (E903) Indigo carmine aluminium lake Isopropyl alcohol Propylene glycol Purified water Shellac Titanium dioxide
Potential allergens	Do not contain potential allergens

Each hard capsule contains tobramycin 28 mg inhalation powder.

Do not take this medicine if you are allergic to any of these ingredients.

What TOBI Podhaler looks like

TOBI Podhaler is Clear, colourless capsules, containing a white to almost white powder. The capsules have "MYL TPH" in blue radial imprinted on one part of the capsule, and the Mylan logo in blue radial imprinted on the other part of the capsule.

Each sealed foil pack contains a capsule card. The card contains a daily dose of 8 capsules (combined morning and evening doses).

A carton contains 224 capsules and 5 plastic podhaler devices (AUST R 182302).

The capsules must be administered specifically with a Podhaler^® device provided in the same pack.

Who distributes TOBI Podhaler

Viatris Pty Ltd
Level 1, 30 The Bond
30-34 Hickson Road
Millers Point NSW 2000
www.viatris.com.au
Phone: 1800 274 276

TOBI^® and Podhaler^® are a Viatris company trade mark.

This leaflet was prepared in November 2021.

TOBI Podhaler_cmi\Nov21/00

Published by MIMS March 2022

BRAND INFORMATION

Brand name

Tobi, Tobi Podhaler

Active ingredient

Tobramycin

Schedule

1 Name of Medicine

Tobramycin.

2 Qualitative and Quantitative Composition

Tobi solution for inhalation (Tobi solution) and Tobi Podhaler capsules for inhalation (Tobi Podhaler) are two different formulations of tobramycin specifically developed for administration by inhalation.

Tobi solution for inhalation.

Each Tobi solution single-use 5 mL ampoule contains 300 mg tobramycin and 11.25 mg sodium chloride in sterile water for injections. Sulfuric acid and sodium hydroxide are added to adjust the pH to 6.0. Nitrogen is used for sparging. All ingredients meet USP requirements. The formulation contains no preservatives.

Tobi Podhaler.

Each Tobi Podhaler capsule contains tobramycin 28 mg, distearoylphosphatidylcholine, calcium chloride dihydrate, and sulfuric acid. The hard capsule shell contains hypromellose, potassium chloride, carrageenan, carnauba wax, butan-1-ol, indigo carmine aluminium lake, isopropyl alcohol, propylene glycol, purified water, shellac, titanium dioxide.

3 Pharmaceutical Form

Tobi solution for inhalation ampoule.

Tobi solution is a sterile, clear, slightly yellow, non-pyrogenic, aqueous solution with the pH and salinity adjusted specifically for administration by a compressed air driven reusable nebuliser.

Tobi Podhaler capsules for inhalation.

Tobi Podhaler includes clear, colorless hypromellose capsules containing a white to almost-white powder for inhalation. The capsules have "MYL TPH" in blue radial imprint on one part of the capsule and the Mylan logo in blue radial imprint on the other part of the capsule. The capsules must be administered specifically with a Podhaler device provided in the same pack.

4 Clinical Particulars

4.1 Therapeutic Indications

Tobi solution and Tobi Podhaler are indicated for the management of cystic fibrosis patients with P. aeruginosa infections.
Safety and efficacy have not been demonstrated in patients under the age of 6 years, patients with FEV₁ < 25% or > 80% predicted at screening, or patients colonized with Burkholderia cepacia (see Section 5.1, Clinical trials).

4.2 Dose and Method of Administration

Dosage.

Dosage is not adjusted by age or weight. The doses should be taken as close to 12 hours apart as possible; they should not be taken less than six hours apart. In case of a missed dose with at least 6 hours until the next dose, the patient should take the dose as soon as possible. Otherwise, the patient should wait for the next dose and not inhale more medication to make up for the missed dose.
Tobi solution or Tobi Podhaler are administered twice daily in alternating periods of 28 days. After 28 days of therapy, patients should stop therapy for the next 28 days, and then resume therapy for the next 28 day on/28 day off cycle.
Therapy should be initiated by a physician experienced in the management of cystic fibrosis. Treatment with Tobi should be continued on a cyclical basis for as long as the physician considers that the patient is gaining clinical benefit from the inclusion of Tobi solution or Tobi Podhaler in their treatment regimen. If clinical deterioration of pulmonary status is evident, additional anti-pseudomonal therapy should be considered.
Tobi solution.

Adults and paediatric patients 6 years of age and older.

The recommended dosage for both adults and paediatric patients 6 years of age and older is one single-use ampoule (300 mg) administered twice daily for 28 days.
Tobi Podhaler.

Adults and paediatric patients 6 years of age and older.

The recommended dosage is four capsules (4 x 28 mg = 112 mg tobramycin) administered twice daily for 28 days.
Dosing in special populations.

Paediatric population below 6 years.

Tobi solution and Tobi Podhaler are not indicated for use in paediatric patients less than 6 years of age.

Elderly patients (≥ 65 years).

There are insufficient data in this population to support a recommendation for or against dose adjustment. Renal function in elderly patients should be taken into account while using Tobi solution and Tobi Podhaler (see Section 4.4 Special Warnings and Precautions for Use).

Patients with renal impairment.

Patients with serum creatinine 176.8 micromoles per litre (0.18 mmol/L) or more and blood urea nitrogen (BUN) 14 mmol/L or more have not been included in clinical studies and there are no data in this population to support a recommendation for or against dose adjustment with Tobi. Also see Section 4.4 Special Warnings and Precautions for Use.

Patients with hepatic impairment.

No studies have been performed on patients with hepatic impairment. As tobramycin is not metabolized, an effect of hepatic impairment on the exposure to tobramycin is not expected.

Patients after organ transplantation.

Adequate data do not exist for the use in patients after organ transplantation.

Administration.

Where patients are receiving several different inhaled medications and performing chest physiotherapy, it is recommended that Tobi is taken last.
Tobi solution. Tobi solution is supplied as a single-use, ready to use ampoule and is administered by inhalation, over an approximately 15 minute period, using a hand-held nebuliser and compressor. See Section 4.4 Special Warnings and Precautions for Use.
Tobi solution should be inhaled whilst the patient is sitting or standing upright and breathing normally through the mouthpiece of the nebulizer. Nose clips may be used to help the patient breathe through the mouth.
Tobi should not be diluted or mixed with dornase alfa or other medications in the nebuliser. See Section 4.5 Interactions with Other Medicines and Other Forms of Interactions.
During clinical studies, patients on multiple therapies were instructed to take them first, followed by Tobi.
Detailed instructions for use are provided in the patient package insert supplied with Tobi.
Tobi Podhaler. Tobi Podhaler capsules are for oral inhalation route only using a Podhaler device. The capsules must not be administered by any other route.
To ensure proper administration of the medicine, the physician or other healthcare professional should show the patient how to operate the Podhaler device. In addition, any caregivers must be advised to provide assistance to children starting Tobi Podhaler treatment, particularly those aged 10 years or younger, and that they should continue to supervise them until they are able to use the Podhaler device without help.
Studies under high humidity conditions (25°C/75% relative humidity) during product use showed some accumulation of powder (drug) in the inhaler. Patients should be made aware of the need to store the product in the original package when not in use and to avoid using the product in humid environments (see Section 6.4 Special Precautions for Storage).

Basic instructions for Tobi Podhaler use.

1. Wash and fully dry hands.
2. Just before use, remove the Podhaler device from its case by holding the base and twisting off the top of the case in a counter-clockwise direction. Set the top of the case aside. Briefly inspect the inhaler to make sure it is not damaged or dirty, and then stand it in the base of the case.
3. Holding the body of the inhaler, unscrew and remove the mouthpiece from the inhaler body. Set the mouthpiece aside on a clean, dry surface.
4. Separate the morning and evening doses from the capsule card.
5. Peel back the foil from the capsule card to reveal one Tobi Podhaler capsule and remove it from the card.
6. Immediately insert the capsule into the inhaler chamber. Replace the mouthpiece and screw it on firmly until it stops. Do not over tighten.
7. To puncture the capsule, hold the inhaler with the mouthpiece down, press the button firmly with your thumb as far as it will go, then release the button. The medication is now ready for inhalation.
8. Fully exhale away from the inhaler.
9. Position the inhaler with the mouthpiece facing towards you. Place mouth over the mouthpiece creating a tight seal. Inhale the powder deeply with a single continuous inhalation.
10. Remove inhaler from mouth, and hold breath for a count of approximately 5 seconds, then exhale normally away from the inhaler.
11. After a few normal breaths away from the inhaler, perform a second inhalation from the same capsule, repeating steps 8 - 10.
12. Unscrew mouthpiece and remove the capsule from the chamber. Inspect the used capsule. It should appear punctured and empty.
13. If the capsule is punctured but still contains some powder, place it back into the chamber with the punctured side of the capsule inserted first, replace the mouthpiece and take another two inhalations from the capsule (repeat step 6, then steps 8-12). Reinspect the capsule.
14. If the capsule appears to be unpunctured, place it back into the chamber, replace the mouthpiece, press the button firmly as far as it goes and take another two inhalations from the capsule (repeat steps 6-12). If the capsule is still full and appears to be unpunctured, replace the inhaler with the reserve inhaler and try again (repeat steps 2, 3, and 6-12).
15. Discard the empty capsule.
16. Repeat, starting at step 5, for the remaining 3 capsules of the dose.
17. Replace the mouthpiece and screw it on firmly until it stops. When the full dose (4 capsules) has been inhaled, wipe the mouthpiece with a clean, dry cloth.
18. Place inhaler back in storage case and close tightly. The inhaler should never be washed with water.
19. Tobi Podhaler should be kept out of sight and reach of children, except when administered therapeutically under appropriate adult supervision.
20. Caregivers should provide assistance to children starting Tobi Podhaler treatment, particularly those aged 10 years or younger, and should continue to supervise them until they are able to use the Podhaler inhaler properly without help.

4.3 Contraindications

Tobi is contraindicated in patients with a known hypersensitivity to any aminoglycoside.

4.4 Special Warnings and Precautions for Use

Tobi solution and Tobi Podhaler are for oral inhalation only.
Tobi solution is not for subcutaneous, intravenous or intrathecal administration.
Tobi Podhaler capsules must not be swallowed.
The use of Tobi solution with nebulisers other than the Pari LC Plus reusable nebuliser or Pari Pro-neb system with a DeVilbiss Pulmo-Aide compressor has not been adequately studied.
Caution should be exercised when prescribing Tobi solution or Tobi Podhaler to patients with known or suspected renal, auditory, vestibular, or neuromuscular dysfunction. Patients receiving concomitant parenteral aminoglycoside therapy should be monitored as clinically appropriate.
Aminoglycosides can cause foetal harm when administered to a pregnant woman. Aminoglycosides cross the placenta, and streptomycin has been associated with several reports of total, irreversible, bilateral congenital deafness in paediatric patients exposed in utero. Patients who use Tobi solution or Tobi Podhaler during pregnancy, or become pregnant while taking one of these products should be apprised of the potential hazard to the foetus.

Ototoxicity.

In clinical studies, 4 patients (1%) reported mild to moderate hearing loss in clinical studies of up to 9 treatment cycles of Tobi solution. Hearing loss was transient for 3 patients and ongoing at the end of study for one patient. Three of these patients had received IV aminoglycosides concomitantly to receiving Tobi solution.
Hearing loss and tinnitus were reported by patients in the Tobi Podhaler clinical trials (see Section 4.8 Adverse Effects (Undesirable Effects)).
In postmarketing experience, some patients receiving Tobi solution and extensive previous or concomitant parenteral aminoglycosides have reported hearing loss. Some of these reports occurred in patients with previous or concomitant treatment with systemic aminoglycosides. Patients with hearing loss frequently reported tinnitus. Tinnitus is a sentinel symptom of ototoxicity, and therefore the onset of this symptom warrants caution (see Section 4.8 Adverse Effects (Undesirable Effects)). Ototoxicity, manifested as both auditory and vestibular toxicity, has been reported with parenteral aminoglycosides. Vestibular toxicity may be manifested by vertigo, ataxia or dizziness.
Caution should be exercised when prescribing Tobi solution or Tobi Podhaler to patients with known or suspected auditory or vestibular dysfunction. Physicians should consider an audiogram before initiating Tobi therapy for patients who show any evidence of auditory dysfunction, or who are at increased risk for auditory dysfunction.
If a patient reports tinnitus or hearing loss during Tobi solution or Tobi Podhaler therapy, the physician should refer them for audiological assessment.
If ototoxicity occurs in a patient receiving Tobi solution or Tobi Podhaler, tobramycin therapy should be discontinued until tobramycin serum concentrations fall below 2 microgram/mL.

Risk of ototoxicity due to mitochondrial DNA variants.

Cases of ototoxicity with aminoglycosides have been observed in patients with certain variants in the mitochondrially encoded 12S rRNA gene (MT-RNR1), particularly the m.1555A>G variant. Ototoxicity occurred in some patients even when their aminoglycoside serum levels were within the recommended range. Mitochondrial DNA variants are present in less than 1% of the general US population, and the proportion of the variant carriers who may develop ototoxicity as well as the severity of ototoxicity is unknown. In case of known maternal history of ototoxicity due to aminoglycoside use or a known mitochondrial DNA variant in the patient, consider alternative treatments other than aminoglycosides unless the increased risk of permanent hearing loss is outweighed by the severity of infection and lack of safe and effective alternative therapies.

Nephrotoxicity.

Nephrotoxicity was not seen during Tobi solution or Tobi Podhaler clinical studies but has been associated with aminoglycosides as a class. Nephrotoxicity has been reported with the use of parenteral aminoglycosides. Caution should be exercised when prescribing Tobi solution or Tobi Podhaler to patients with known or suspected renal dysfunction.
If nephrotoxicity occurs in a patient receiving Tobi solution or Tobi Podhaler, tobramycin therapy should be discontinued until tobramycin serum concentrations fall below 2 microgram/mL. Also see Section 4.4 Special Warnings and Precautions for Use.
Laboratory tests of renal function should be monitored as clinically appropriate. Urea and creatinine levels should be reassessed after every 6 complete cycles of therapy.

Neuromuscular dysfunction.

Tobi solution or Tobi Podhaler should be used cautiously in patients with muscular disorders, such as myasthenia gravis or Parkinson's disease, since aminoglycosides may aggravate muscle weakness because of a potential curare-like effect on neuromuscular function.

Bronchospasm.

Bronchospasm can occur with inhalation of medicinal products and has been reported with Tobi solution or Tobi Podhaler. Bronchospasm should be treated as medically appropriate. If an allergic response is suspected, Tobi solution or Tobi Podhaler should be discontinued.
In clinical studies of Tobi, changes in FEV₁ measured after the inhaled doses were similar in the Tobi and placebo groups.
The first dose of Tobi Podhaler should be given under supervision. FEV₁ should be measured before and after inhalation of the first dose of Tobi Podhaler. If there is evidence of therapy-induced bronchospasm, the physician should carefully evaluate whether the benefits of continued use of Tobi Podhaler outweigh the risks to the patient.

Cough.

Cough was the most commonly reported adverse event considered treatment related for both Tobi solution and Tobi Podhaler, but was reported more frequently in patients treated with Tobi Podhaler. If there is evidence of continued therapy-induced cough, the physician should consider the use of alternative therapeutic options.

Haemoptysis.

Haemoptysis is a complication in cystic fibrosis and is more frequent in adults. Patients with clinically significant haemoptysis (> 60 mL) were excluded from the clinical studies so no data exist on the use of Tobi solution or Tobi Podhaler in these patients. The use of Tobi solution or Tobi Podhaler in such patients should be undertaken only if the benefits of treatment are considered to outweigh the risks of inducing further haemorrhage.

Concomitant antibiotic therapy.

Serum concentrations of tobramycin should be monitored in patients receiving concomitant parenteral aminoglycoside therapy (or other medications that can affect renal excretion). These patients should be monitored as clinically appropriate, taking into account the risk of cumulative toxicity. See Section 4.4 Special Warnings and Precautions for Use.

Decrease in susceptibility to tobramycin.

In clinical studies, some patients on Tobi Podhaler therapy showed an increase in aminoglycoside MICs for P. aeruginosa isolates tested. There is a theoretical risk that patients being treated with Tobi Podhaler may develop P. aeruginosa isolates resistant to tobramycin. The in vitro antimicrobial susceptibility test methods used for parenteral tobramycin therapy can be used to monitor the susceptibility of P. aeruginosa isolated from CF patients. Also see Section 5.1 Pharmacodynamic Properties.

Clostridium difficile-associated disease.

Antibiotic associated pseudomembranous colitis has been reported with many antibiotics including tobramycin. A toxin produced with Clostridium difficile appears to be the primary cause. The severity of the colitis may range from mild to life threatening. It is important to consider this diagnosis in patients who develop diarrhoea or colitis in association with antibiotic use (this may occur up to several weeks after cessation of antibiotic therapy). Mild cases usually respond to drug discontinuation alone. However, in moderate to severe cases appropriate therapy with a suitable oral antibacterial agent effective against Clostridium difficile should be considered. Fluids, electrolytes and protein replacement should be provided when indicated.

Use in hepatic impairment.

No studies have been performed on patients with hepatic impairment. As tobramycin is not metabolized, an effect of hepatic impairment on the exposure to tobramycin is not expected.

Use in renal impairment.

Tobramycin is primarily excreted unchanged in the urine and renal function is expected to affect the exposure to tobramycin. See Section 4.4 Special Warnings and Precautions for Use.

Use in the elderly.

See Section 5.2, Pharmacokinetics in special patient groups, Elderly patients.

Paediatric use.

The safety and efficacy of Tobi have not been demonstrated in paediatric patients under 6 years of age.

Effects on laboratory tests.

Audiograms.

Tinnitus may be a sentinel symptom of ototoxicity, and therefore the onset of this symptom warrants caution. Physicians should consider an audiogram for patients who show any evidence of auditory dysfunction, or who are at increased risk for auditory dysfunction.

Serum concentrations.

In patients with normal renal function treated with Tobi solution or Tobi Podhaler, serum tobramycin concentrations are approximately 1 microgram/mL one hour after dose administration and do not require routine monitoring.
Serum concentrations of tobramycin should be monitored in patients receiving concomitant parenteral aminoglycoside therapy (or other medications that can affect renal excretion). These patients should be monitored as clinically appropriate, taking into account the risk of cumulative toxicity.
Serum concentrations of tobramycin should be monitored in patients with known or suspected auditory or renal dysfunction. Patients treated with concomitant parenteral tobramycin should be monitored at the discretion of the treating physician.
The serum concentration of tobramycin should only be monitored through venipuncture and not finger prick blood sampling. Contamination of the skin of the fingers with tobramycin may lead to falsely increased measurements of serum levels of the drug. This contamination cannot be completely avoided by hand washing before testing.

Renal function.

The clinical studies with Tobi solution and Tobi Podhaler did not reveal any imbalance in the percentage of patients in the Tobi and placebo groups who experienced at least a 50% rise in serum creatinine from baseline (see Section 4.8 Adverse Effects (Undesirable Effects)). Laboratory tests of urine and renal function should be conducted at the discretion of the treating physician.

4.5 Interactions with Other Medicines and Other Forms of Interactions

No clinical drug interaction studies have been performed with Tobi solution or Tobi Podhaler.
Some diuretics can enhance aminoglycoside toxicity by altering antibiotic concentrations in serum and tissue. Tobi should not be administered concomitantly with etacrynic acid, furosemide (frusemide), urea, or intravenous mannitol.
Based on the interaction profile for tobramycin following intravenous and aerosolized administration, concurrent and/or sequential use of Tobi with other drugs with neurotoxic, nephrotoxic, or ototoxic potential should be avoided.
In patients with a predisposing risk due to previous prolonged, systemic aminoglycoside therapy, it may be necessary to consider renal and audiological assessment before initiating Tobi therapy.
Other medicinal products that have been reported to increase the potential toxicity of parenterally administered aminoglycosides include: amphotericin B (amphotericin), cefalotin, ciclosporin, tacrolimus, polymyxins (risk of increased nephrotoxicity); platinum compounds (risk of increased nephrotoxicity and ototoxicity); anticholinesterases, and botulinum toxin (neuromuscular effects).
Aminoglycosides may aggravate muscle weakness because of a potential curare-like effect on neuromuscular function.

Absence of interactions.

In clinical studies of Tobi solution, patients taking Tobi solution concomitantly with dornase alfa, β₂-agonists, inhaled corticosteroids, other anti-pseudomonal antibiotics, or parenteral aminoglycosides demonstrated adverse experience profiles similar to the study population as a whole.
In a clinical study with Tobi Podhaler, similar proportions of patients receiving Tobi Podhaler and Tobi solution continued to take dornase alfa, bronchodilators, inhaled corticosteroids and macrolides.

4.6 Fertility, Pregnancy and Lactation

Effects on fertility.

No reproduction toxicology studies have been conducted with Tobi administered by inhalation.
Subcutaneous administration of up to 600 mg/m²/day of tobramycin did not affect mating behaviour or cause impairment of fertility in male or female rats, although fertility of the offspring was not examined.
(Category D)
There are no adequate data from the use of tobramycin administered by inhalation in pregnant women.
Subcutaneous administration of tobramycin at doses of 600 or 220 mg/m²/day during organogenesis was not teratogenic in rats or rabbits, respectively. Doses of tobramycin ≥ 440 mg/m²/day were severely maternally toxic to rabbits and precluded the evaluation of teratogenicity.
Aminoglycosides can cause foetal harm (e.g. congenital deafness) when administered to a pregnant woman and high systemic concentrations are achieved. Ototoxicity was not evaluated in offspring during nonclinical reproduction toxicity studies with tobramycin.
Treatment with Tobi during pregnancy should be undertaken only if the benefits to the mother outweigh the risks to the foetus or baby. If Tobi is used during pregnancy, or if the patient becomes pregnant while taking Tobi, the patient should be apprised of the potential hazard to the foetus.
Aminoglycosides can cross the placenta. There is evidence of selective uptake of aminoglycosides by foetal kidney resulting in damage (probably reversible) to immature nephrons. Eighth cranial nerve damage has also been reported following in utero exposure to some of the aminoglycosides. Because of their chemical similarity, all aminoglycosides must be considered potentially nephrotoxic and ototoxic to the foetus. It should also be noted that therapeutic blood concentrations in the mother do not equate with safety to the foetus.
It is not known if Tobi will reach sufficient concentrations after administration by inhalation to be excreted in human breast milk. Because of the potential for ototoxicity and nephrotoxicity in infants, a decision should be made whether to terminate nursing or discontinue treatment with Tobi, taking into account the importance of the drug to the mother.

4.7 Effects on Ability to Drive and Use Machines

The effects of this medicine on a person's ability to drive and use machines were not assessed as part of its registration.

4.8 Adverse Effects (Undesirable Effects)

Adverse events in clinical trials.

Tobi solution.

Tobi solution was generally well tolerated during two placebo-controlled clinical studies in 258 cystic fibrosis patients ranging in age from 6 to 48 years. Patients received Tobi solution in alternating periods of 28 days on and 28 days off drug in addition to their standard cystic fibrosis therapy for a total of 24 weeks.
Voice alteration and tinnitus were the only adverse experiences reported by significantly more Tobi solution-treated patients. Thirty-three patients (13%) treated with Tobi solution complained of voice alteration compared to 17 (7%) placebo patients. Voice alteration was more common in the on-drug periods.
Eight patients from the Tobi solution group (3%) reported tinnitus compared to no placebo patients. All episodes were transient, resolved without discontinuation of the Tobi solution treatment regimen, and were not associated with loss of hearing in audiograms. Tinnitus is one of the sentinel symptoms of cochlear toxicity, and patients with this symptom should be carefully monitored for high frequency hearing loss. The numbers of patients reporting vestibular adverse experiences such as dizziness were similar in the Tobi solution and placebo groups.
Nine (3%) patients in the Tobi solution group and nine (3%) patients in the placebo group had increases in serum creatinine of at least 50% over baseline. In all nine patients in the Tobi group, creatinine decreased at the next visit.
Table 1 lists the percent of patients with treatment-emergent adverse experiences that occurred in 25% of patients during the 48 weeks of the open label extension. The table also presents the corresponding data from the 24-week placebo-controlled studies, where one group of patients received placebo and the other group received Tobi solution during the first three cycles of therapy.

Tobi Podhaler.

Tobi Podhaler has been evaluated for safety in 395 CF patients exposed to at least one dose of Tobi Podhaler, including 273 who were exposed across three cycles (6 months) of treatment. Each cycle consisted of 28 days on-treatment (with 112 mg administered twice daily) and 28 days off treatment. The majority of patients evaluated for safety were entered into Study C2302 which included an active-treatment control group administered Tobi solution. The Tobi Podhaler group included 308 patients; the Tobi solution group numbered 209 patients (see Section 5.1, Clinical trials).
The primary safety population, randomized in a planned 3:2 ratio, consisted of the 308 patients treated with Podhaler capsules and 209 patients treated with Tobi solution (300 mg/5 mL tobramycin nebulizer solution) in Study C2302, an open-label study comparing Podhaler capsules with Tobi solution over 3 treatment cycles. For both treatment groups, mean exposure to medication for each cycle was 28-29 days.
The supportive safety population considered an additional 87 patients treated with Podhaler capsules and 49 treated with placebo in Study C2301, which was double-blind for the first treatment cycle, followed by all patients receiving Podhaler capsules for 2 additional cycles. At these exposures, Podhaler capsules were generally well tolerated.
In Study C2302, the most frequently occurring adverse drug reactions (ADRs) related to the respiratory, thoracic and mediastinal system organ class. The most commonly occurring ADRs (by preferred term) were cough and lung disorder in both the Podhaler capsules and Tobi solution treatment groups.
During the placebo-controlled cycle of Study C2301, the overall incidence of ADRs was lower in the Podhaler treatment group than in the placebo group, with the exceptions of pharyngolaryngeal pain, dysphonia, and dysgeusia.
In Study C2301, no patients reported adverse events related to hearing loss. Two patients were found during planned audiology testing to have significant decreases in hearing (defined as 10-15 dB in at least two consecutive frequencies, or 20 dB or more at a single frequency). In Study C2302, hearing complaints such as tinnitus were reported in approximately 2% of patients overall. Of a subset of patients in Study C2302 who received serial audiology testing, 25.6% (Podhaler capsules) and 15.6% (Tobi solution) showed decreases from baseline at any visit (80% of the subset had normal hearing assessments at baseline). However, the majority of such changes was transient and had resolved by the end of the study. Four patients in the Podhaler capsules treatment group experienced significant decreases in hearing which were transient in three patients and persistent in one case. Less than 3% of patients in either group showed evidence of significant hearing loss. Using the criteria for either ear of 10 dB loss at 3 consecutive frequencies, 15 dB loss at two consecutive frequencies and 20 dB loss at any frequency, three Podhaler capsules patients and two Tobi solution patients (matching the randomization ratio) were judged to have ototoxicity.
Adverse drug reactions reported in Study C2302 regardless of relationship to study medication are listed in Table 2. Adverse reactions considered at least possibly related to study medication are summarized below. Overall the most frequently reported adverse event was cough which was reported in 48% of the Tobi Podhaler group compared with 31% of the Tobi solution group. Discontinuations due to cough were reported by 3.9% of the Tobi Podhaler group and 1.0% of the Tobi solution group. Adverse drug reactions from Study C2302 are listed according to MedDRA system organ class in Table 2. Within each system organ class, the adverse reactions are ranked by frequency, with the most frequent reactions first, and by database. Within each frequency grouping, adverse reactions are presented in order of decreasing seriousness. In addition, the corresponding frequency category using the following convention (CIOMS III) is also provided for each adverse reaction: Very common (≥ 1/10); common (≥ 1/100, < 1/10); uncommon (≥ 1/1,000, < 1/100); rare (≥ 1/10,000, < 1/1,000); very rare (< 1/10,000), including isolated reports.
Bronchospasm was reported for 1.6% of the Tobi Podhaler group and 0.5% of the Tobi solution group.
In Study C2302, hearing complaints such as tinnitus were reported in 1.9% of patients overall. Of the subsets of patients in this study who underwent serial audiology testing, 25.6% of the Tobi Podhaler group and 15.6% of the Tobi solution group showed decreases from baseline at any visit; however, the majority of such changes were transient. Using the criteria of 10 dB loss at 3 consecutive frequencies, 15 dB loss at two consecutive frequencies and 20 dB loss at any one frequency for either ear, three Tobi capsule patients and two Tobi solution patients were judged to have ototoxicity. Deafness including deafness unilateral (reported as mild to moderate hearing loss or increased hearing loss) was reported in 1.0% of patients receiving Tobi Podhaler and 0.5% of patients receiving Tobi solution. Aphonia was reported in 1.0% of the Tobi Podhaler group and 0% of the Tobi solution group.
In the placebo-controlled Cycle 1 of Study C2301, which included 46 Tobi Podhaler patients and 49 placebo patients, ADRs included: pharyngolaryngeal pain (10.9% Tobi Podhaler vs. 0% placebo, very common) and dysphonia (4.3% Tobi Podhaler vs. 0% placebo, common) in the System Organ Class (SOC) Respiratory, Thoracic, and Mediastinal Disorders; and dysgeusia (6.5% Tobi Podhaler vs. 2.0% placebo, common) in the SOC Gastrointestinal Disorders.

Post-marketing surveillance.

Some patients receiving Tobi solution and extensive previous or concomitant parenteral aminoglycosides have reported hearing loss during postmarketing surveillance (see Section 4.4 Special Warnings and Precautions for Use).
Adverse drug reactions derived from spontaneous reports for Tobi solution. The following adverse drug reactions have been derived from postmarketing experience with Tobi via spontaneous case reports and literature cases. Because these reactions are reported voluntarily from a population of uncertain size, it is not possible to reliably estimate their frequency which is therefore categorized as not known. Adverse drug reactions are listed according to system organ classes in MedDRA. Within each system organ class, ADRs are presented in order of decreasing seriousness.

Ear and labyrinth disorders.

Hearing loss.

Skin and subcutaneous tissue disorders.

Hypersensitivity, pruritus, urticaria, rash.

Nervous system disorders.

Aphonia, dysgeusia.

Respiratory, thoracic, and mediastinal disorders.

Bronchospasm, oropharyngeal pain, sputum increased, chest pain.

General disorders and administration site conditions.

Decreased appetite.
Adverse drug reactions from spontaneous reports and literature cases for Tobi Podhaler (frequency not known). The following adverse drug reactions have been derived from postmarketing experience with Tobi Podhaler via spontaneous case reports and literature cases. Because these reactions are reported voluntarily from a population of uncertain size, it is not possible to reliably estimate their frequency which is therefore categorized as not known.
Malaise.
Sputum discolored.
Reporting suspected adverse reactions after registration of the medicinal product is important. It allows continued monitoring of the benefit-risk balance of the medicinal product. Healthcare professionals are asked to report any suspected adverse reactions at www.tga.gov.au/reporting-problems.

4.9 Overdose

Signs and symptoms.

In the event of inadvertent administration of tobramycin by the IV route, signs and symptoms of parenteral toxicity from overdosage may occur that include dizziness, tinnitus, vertigo, loss of high-tone hearing acuity, respiratory distress or failure, renal impairment, and neuromuscular blockade. Administration by inhalation results in low systemic bioavailability of tobramycin.
In the event of accidental oral ingestion, systemic toxicity is unlikely as tobramycin is poorly absorbed from an intact gastrointestinal tract.
The maximum tolerated daily dose of Tobi solution or Tobi Podhaler has not been established. Tobramycin serum concentrations may be helpful in monitoring overdose.

Treatment.

In all cases of suspected overdosage, physicians should contact the Poison Information Centre on 13 11 26 (Australia) for advice on management. In the case of any overdosage, the possibility of drug interactions with alterations in drug disposition should be considered.
Acute toxicity should be treated with immediate withdrawal of Tobi, and baseline tests of renal function should be undertaken.
Haemodialysis may be helpful in removing tobramycin from the body.

5 Pharmacological Properties

5.1 Pharmacodynamic Properties

Pharmacotherapeutic group: Aminoglycoside antibacterials; ATC Code: J01GB01.

Mechanism of action.

Tobramycin is an aminoglycoside antibiotic produced by Streptomyces tenebrarius. It acts primarily by disrupting protein synthesis, leading to altered cell membrane permeability, progressive disruption of the cell envelope, and eventual cell death. Tobramycin has in vitro activity against a wide range of gram-negative organisms including Pseudomonas aeruginosa (P. aeruginosa). It is bactericidal at concentrations equal to or slightly greater than inhibitory concentrations.

Susceptibility testing.

A single sputum sample from a cystic fibrosis (CF) patient may contain multiple morphotypes of P. aeruginosa and each morphotype may have a different level of in vitro susceptibility to tobramycin. Treatment for 6 months with Tobi Podhaler in two clinical studies did not affect the susceptibility of the majority of P. aeruginosa isolates tested; however, increased MICs were noted in some patients. The clinical significance of this information has not been clearly established in the treatment of P. aeruginosa in CF patients.
The in vitro antimicrobial susceptibility test methods used for parenteral tobramycin therapy can be used to monitor the susceptibility of P. aeruginosa isolated from CF patients. If decreased susceptibility is noted, the results should be reported to the clinician.
Susceptibility breakpoints established for parenteral administration of tobramycin do not apply to inhaled administration of Tobi. The relationship between in vitro susceptibility test results and clinical outcome with Tobi therapy is not clear.

Clinical trials.

Placebo-controlled studies.

Tobi solution.

Management of pulmonary Pseudomonas aeruginosa infection.

Two identically designed, double-blind, randomised, placebo-controlled, parallel group, 24-week clinical studies were conducted in 520 cystic fibrosis patients aged ≥ 6 years who had baseline FEV₁ % predicted between 25% and 75% and were positive for P. aeruginosa. Patients with a baseline creatinine of > 0.18 mmol/L or who had Burkholderia cepacia isolated from sputum were excluded. A cyclical treatment regimen consisting of 28 days on therapy followed by 28 days off therapy was used in these studies. This cycle was repeated twice for a total of three cycles. Patients received either Tobi solution (300 mg) or placebo (saline with 1.25 mg quinine) twice daily, delivered by aerosol using a hand-held Pari LC Plus Reusable Nebuliser with a DeVilbiss Pulmo-Aide Compressor.
All patients received study drug in addition to standard treatment recommended for cystic fibrosis patients, which included oral and parenteral anti-pseudomonal therapy, β₂-agonists, sodium cromoglycate, inhaled steroids, and airway clearance techniques. In addition, approximately 77% of patients were concurrently treated with dornase alfa.
The randomised clinical studies were followed by a 48-week open label extension where all patients who chose to continue received up to 6 cycles of treatment with Tobi solution following the same regimen of 28 days on and 28 days off. Thus, patients who continued into the open label extension received a total exposure of either up to 9 cycles or up to 6 cycles, depending on their original assignment in the controlled studies.
In each of the two placebo-controlled studies, Tobi solution-treated patients experienced significant improvement in pulmonary function. Improvement was demonstrated in the Tobi solution group in Study 1 by an average increase in FEV₁ % predicted of about 11% relative to baseline (Week 0) during 24 weeks compared to no average change in placebo patients. In Study 2, Tobi solution treated patients had an average increase of about 7% compared to an average decrease of about 1% in placebo patients. Figure 1 shows the average relative change in FEV₁ % predicted over 24 weeks for both studies.

Three hundred ninety-six (396) patients from the controlled studies participated in the open label extension. Of these, a total of 192 patients received up to 9 cycles of Tobi solution, 3 cycles during the controlled studies and 6 cycles during the open label extension. At the end of cycle 9, in these patients FEV₁ % predicted was 1.7% above baseline (measured at the start of the controlled trials). A total of 204 patients received placebo for 3 cycles followed by 6 cycles of Tobi solution. Whilst on placebo, these patients experienced a mean 2.9% decrease in FEV₁ % predicted from baseline. After 6 cycles of Tobi solution, FEV₁ % predicted had improved to 1% below baseline (see Figure 2).

P. aeruginosa density in sputum was measured during the 24-week placebo-controlled studies. Treatment with Tobi solution resulted in a significant reduction in the number of P. aeruginosa colony forming units (CFUs) in sputum during the on-drug periods. Sputum bacterial density returned to baseline during the off drug periods. Reductions in sputum bacterial density were smaller in each successive cycle see Figure 3. P. aeruginosa density in sputum was not measured during the open label extension.
During the 24 weeks of the placebo-controlled studies, patients treated with Tobi solution were hospitalised for an average of 5.1 days compared to 8.1 days for placebo patients. Patients treated with Tobi solution required an average of 9.7 days of parenteral anti-pseudomonal antibiotic treatment compared to 14.1 days for placebo patients. During the 24 weeks of treatment, 40% of Tobi solution patients and 53% of placebo patients were treated with parenteral anti-pseudomonal antibiotics. Over the subsequent 48 weeks of the open label extension, patients were hospitalised for a mean of 11.1 days. Patients were treated with parenteral anti-pseudomonal antibiotics for a mean of 22.4 days and 60.6% of patients were treated with parenteral anti-pseudomonal antibiotics.

The relationship between in vitro susceptibility test results and clinical outcome with Tobi therapy is not clear. However, four Tobi solution patients who began the clinical trial with P. aeruginosa isolates having MIC values ≥ 128 microgram/mL did not experience an improvement in FEV₁ or a decrease in sputum bacterial density during the first 24 weeks of therapy.
For patients given 9 cycles of active treatment, the proportion of patients with isolates of P. aeruginosa with an MIC ≥ 16 microgram/mL increased from 13.7% at baseline to 29.8% at the end of cycle 9. The proportion of patients with isolates of P. aeruginosa with MIC ≥ 128 microgram/mL increased from 2.1% at baseline to 9.2% at the end of cycle 9.
During the open-label extension, susceptibility testing of other aminoglycosides (amikacin and gentamicin) indicated a shift toward increasing MIC values similar in magnitude to that seen for tobramycin. The MIC values for ciprofloxacin, aztreonam, ceftazidime and ticarcillin remained unchanged.
As noted in Figure 4, treatment for 18 months (9 cycles) with Tobi solution in clinical studies demonstrated a trend to decreasing in vitro susceptibility of P. aeruginosa isolates. The clinical significance of changes in Minimum inhibitory concentrations (MICs) for P. aeruginosa has not been clearly established in the treatment of CF patients.

Paediatric clinical study.

In a double-blind, randomized, placebo-controlled trial, 51 patients aged 3 months to less than 7 years with a confirmed diagnosis of CF and an early colonization with P. aeruginosa (defined as: either first positive culture overall or first positive culture after at least a 1-year history of negative cultures) were treated with Tobi 300 mg/5 mL or placebo, both inhaled via a nebulizer (Pari LC Plus) twice daily for 28 days. Patients who were treated with anti-pseudomonal therapy in the previous year were excluded.
This was a crossover trial in which 26 patients were allocated to the group receiving Tobi in the first treatment period and placebo in the crossover treatment period, and 25 patients were allocated to the group receiving placebo in the first treatment period and Tobi in the crossover treatment period.
The primary outcome was the proportion of patients free from P. aeruginosa colonization assessed by sputum/throat swab culture after completion of a 28-day treatment period which was 84.6% and 24% (p < 0.001) for the Tobi and placebo groups, respectively.
The safety and efficacy of Tobi in children < 6 years of age is not established. Tobi is not indicated for use in paediatric patients less than 6 years of age.
Tobi Podhaler (study C2301). Tobi Podhaler was studied in a randomized, placebo-controlled, multicentre, three-cycle, two treatment group trial in CF patients, aged between 6 and 21 years (mean age 13.3 years), with FEV₁ values from 25% to 80% (inclusive) predicted, who were infected with P. aeruginosa. Patients had no exposure to inhaled anti-pseudomonal antibiotics within 4 months prior to screening. The first cycle of this trial was conducted as a double-blind, randomized, placebo-controlled, parallel group trial. During the second and third cycles, all subjects were treated with Tobi Podhaler. Four capsules (112 mg tobramycin) were administered twice daily (each morning and evening), for three cycles of 28 days on-treatment and 28 days off-treatment (a total treatment period of 24 weeks).
Tobi Podhaler significantly improved lung function compared with placebo, as shown by the results for the primary endpoint: relative increase in percent predicted FEV₁ after 28 days of treatment (Table 3 and Figure 5). An analysis of covariance was employed for the efficacy analysis, with factors for treatment groups and regions and two continuous covariates (baseline FEV₁ % predicted and age). The sequential boundaries and stopping rules for the interim analysis were based on the Lan-DeMets procedure with an alpha-spending function that resembles the O'Brien-Fleming boundaries, to ensured control of the overall Type I error at the 0.5 level. A blinded review of the acceptability of spirometry data was conducted prior to study termination (recommended by an external Data Monitoring Committee) at the time of the interim analysis; all efficacy results below are derived from the sensitivity interim analysis after exclusion of technically unreliable spirometry data.
The improvements in lung function achieved during the first treatment cycle were maintained during the subsequent cycles of treatment with capsules. When patients in the placebo treatment group were switched from placebo to capsules at the start of the second treatment cycle, the relative change from baseline in percent predicted FEV₁ was the same as that seen during the first treatment cycle in the Tobi Podhaler treatment group and the improvements were also maintained over time during the third treatment cycle.
The distribution of tobramycin MICs of P. aeruginosa isolates was characterized by biotype: mucoid, dry, small colony variants, and overall. Sputum assessments in this study showed that at baseline, 91% of Tobi Podhaler patients had P. aeruginosa isolates with an MIC at least 20 times lower than the mean sputum concentration observed within 30 minutes of dosing. At the end of the third 28 day dosing cycle, 86% of Tobi Podhaler patients had P. aeruginosa with an MIC at least 30 times lower and 89% of Tobi Podhaler patients had P. aeruginosa with a MIC at least 15 times lower than mean sputum concentration observed within 30 minutes of dosing. The sub-group of patients with MIC values > 8 microgram/mL at baseline had an improvement in FEV₁ % predicted measurements after 3 cycles of treatment when treated with Tobi Podhaler.

Active-controlled studies.

Tobi Podhaler and Tobi solution (study C2302).

Tobi Podhaler and Tobi solution were studied in a randomized, open-label, multicentre, three-cycle, parallel-arm trial in 553 CF patients, aged between 6 and 66 years (mean age 25.6 years), with FEV₁ values from 25% to 75% (inclusive) predicted, who were infected with P. aeruginosa. Patients with no exposure to inhaled anti-pseudomonal antibiotics within 28 days prior to study drug administration were randomized in a 3:2 ratio to receive either Tobi Podhaler 112 mg (four 28 mg capsules) or Tobi solution 300 mg (one 300 mg/5 mL ampoule). The study medications were administered twice daily, at the same time each morning and evening, approximately 12 hours (but not less than 6 hours) apart, for three cycles of 28 days on-treatment and 28 days off-treatment (a total treatment period of 24 weeks). Blinding was not possible due to differences in study drug administration. Baseline demographics, disease characteristics and use of concomitant medications were similar between the two treatment groups.
The primary objective of the study was to assess the safety of Tobi Podhaler compared to Tobi solution. The main secondary objective was to assess the efficacy of Tobi Podhaler compared to Tobi solution, the key efficacy variable was the relative change in FEV₁ percent predicted at the end of Cycle 3 compared to baseline. A formal analysis of non-inferiority of Tobi Podhaler relative to Tobi solution was conducted based on a one-sided 85% confidence interval calculated from an analysis of covariance (ANCOVA) of relative change in FEV₁ % predicted from baseline to pre-dose Day 28 of Cycle 3. The non-inferiority margin of Delta = 6% was pre-defined. Treatment with both Tobi Podhaler and Tobi solution resulted in relative increases from baseline to Day 28 of the third treatment cycle in percent predicted FEV₁ of 5.8% and 4.7% respectively (Figure 6).

In Study C2302, at the end of the third active treatment period, there was a greater decrease in the mean change from baseline in log₁₀ CFUs in both the Tobi Podhaler treatment group (-1.61 log₁₀ CFUs) and Tobi solution treatment group (-0.77 log₁₀ CFUs) especially during the third treatment cycle (a mean change of -1.61 log₁₀ CFUs in the Podhaler capsule treatment group compared with -0.77 log₁₀ CFUs in the Tobi solution treatment group. As in the previous study, there was a partial recovery of P. aeruginosa density at the end of the 28 day off-treatment phase in both treatment groups, but this was reversed during the on-treatment phase of each treatment cycle.
The mean time to administer a nebulised dose of Tobi solution was approximately 20 minutes, compared with 6 minutes to administer a dose of Tobi Podhaler through the dry powder inhaler. This time excludes any set up and breakdown time for the nebuliser used with Tobi solution.
In Study C2302, patients' satisfaction with treatment was assessed using a modified Treatment Satisfaction Questionnaire for Medication (TSQM) as part of the secondary objective. Patients consistently reported higher levels of satisfaction with treatment with Tobi Podhaler compared with Tobi solution, particularly for assessments of effectiveness, convenience and overall satisfaction.
In study C2302, the proportions of patients in the Tobi Podhaler and Tobi solution treatment groups requiring hospitalization for respiratory events was 24.4% and 22.0% respectively. The duration of hospitalizations was 15.6 days and 15.3 days respectively.

5.2 Pharmacokinetic Properties

Absorption.

Tobi solution and Tobi Podhaler contain tobramycin, a cationic polar molecule that does not readily cross epithelial membranes. Following inhalation of tobramycin, it is concentrated primarily in the airways. The systemic exposure to tobramycin after inhalation is expected to result from pulmonary absorption of the dose fraction delivered to the lungs as tobramycin is not absorbed to any appreciable extent when administered via the oral route.
The bioavailability of Tobi solution may vary because of individual differences in nebuliser performance and airway pathology.
Sputum concentrations.

Tobi solution.

Ten minutes after inhalation of the first 300 mg dose, the average concentration of tobramycin was 1237 microgram/g (ranging from 35 to 7414 microgram/g) in sputum. Tobramycin does not accumulate in sputum; after 20 weeks of therapy with the Tobi solution regimen, the average concentration of tobramycin at ten minutes after inhalation was 1154 micromol/g (ranging from 39 to 8085 micromol/g) in sputum. High variability of tobramycin concentration in sputum was observed. Two hours after inhalation, sputum concentrations declined to approximately 14% of tobramycin levels at ten minutes after inhalation.

Tobi Podhaler.

After inhalation of a single 112 mg dose (4 x 28 mg Tobi Podhaler capsules) in CF patients, sputum C_max of tobramycin was 1048 ± 1080 microgram/g (mean ± SD). The variability in pharmacokinetic parameters was higher in sputum as compared to serum.
Serum concentrations.

Tobi solution.

The average serum concentration of tobramycin one hour after inhalation of a single 300 mg dose of Tobi solution by CF patients was 0.95 microgram/mL. After 20 weeks of therapy on the Tobi solution regimen, the average serum tobramycin concentration one hour after dosing was 1.05 microgram/mL.

Tobi Podhaler.

After inhalation of a single 112 mg dose (4 capsules of 28 mg each) in CF patients, the maximum serum concentration (C_max) of tobramycin was 1.02 ± 0.53 microgram/mL (mean ± SD) and the median time to reach the peak concentration (T_max) was one hour. At the end of a 4 week dosing cycle of Tobi Podhaler (112 mg twice daily), maximum average serum concentrations of tobramycin 1 hour after dosing was 1.99 ± 0.59 microgram/mL.

Distribution.

A population pharmacokinetic analysis for Tobi Podhaler in CF patients estimated the apparent volume of distribution of tobramycin in the central compartment to be 84.1 L for a typical CF patient. While the volume was shown to vary with body mass index (BMI) and lung function (as FEV₁ % predicted), model-based simulations showed that peak (C_max) and trough (C_trough) concentrations were not impacted markedly with changes in BMI or lung function. Binding of tobramycin to serum proteins is negligible.

Metabolism.

Tobramycin is not metabolized and is primarily excreted unchanged in the urine.

Excretion.

The elimination half-life of tobramycin from serum is approximately 2 hours after intravenous (IV) administration. The apparent terminal half-life of tobramycin in serum after inhalation of a single 300 mg dose of Tobi solution or a single 112 mg dose of Tobi Podhaler was approximately 3 hours in CF patients in both dosage forms.
Assuming tobramycin absorbed following inhalation behaves similarly to tobramycin following IV administration; systemically absorbed tobramycin is eliminated principally by glomerular filtration. Unabsorbed tobramycin, following Tobi solution or Tobi Podhaler administration, is probably eliminated primarily in expectorated sputum.
A population pharmacokinetic analysis for Tobi Podhaler in CF patients aged 6 to 66 years estimated the apparent serum clearance of tobramycin to be 14 L/h. This analysis did not show gender- or age-related pharmacokinetic differences.

Effect of food.

Assessments of food-effect were not performed as Tobi solution and Tobi Podhaler are administered by oral inhalation.

Pharmacokinetics in special patient groups.

Renal impairment.

Tobramycin is primarily excreted unchanged in the urine and renal function is expected to affect the exposure to tobramycin. Patients with serum creatinine 176.8 micromoles per litre (0.18 mmol/L) or more and blood urea nitrogen (BUN) 14 mmol/L or more have not been included in clinical studies and there are no data in this population to support a recommendation for or against dose adjustment with Tobi solution or Tobi Podhaler. See Section 4.4 Special Warnings and Precautions for Use; Section 4.2 Dose and Method of Administration.

Hepatic impairment.

No studies have been performed on patients with hepatic impairment. As tobramycin is not metabolized, an effect of hepatic impairment on the exposure to tobramycin is not expected.

Patients after organ transplantation.

Adequate data do not exist for the use of Tobi solution or Tobi Podhaler in these patients.

Elderly patients.

Renal function in elderly patients should be taken into account as systemically absorbed tobramycin is primarily excreted unchanged in the urine. See Section 4.4 Special Warnings and Precautions for Use; Section 4.2 Dose and Method of Administration.

Paediatric population below 6 years.

No pharmacokinetic studies have been conducted in children below 6 years of age. Children 6 years and older have been included in clinical studies in which there was no dose adjustment made based on age or weight.

Race.

Ethnic sensitivity studies have not been conducted. Since tobramycin is not metabolized, it is not expected that ethnic origin would influence exposure.

5.3 Preclinical Safety Data

Animal toxicology.

Bronchoepithelial hyperplasia and chronic interstitial inflammation around terminal bronchioles occurred in studies in rats after daily inhalational exposures to Tobi for 6 months.

Genotoxicity.

Tobi has been evaluated for genotoxicity in a battery of assays for gene mutations and chromosomal damage. Tobramycin was negative in the bacterial reverse mutation and the mouse lymphoma forward mutation assays. Tobramycin did not induce chromosomal aberrations in Chinese hamster ovary cells and was negative in the mouse micronucleus test.

Carcinogenicity.

A two-year rat inhalation toxicology study to assess the carcinogenic potential of Tobi has been completed. Rats were exposed to tobramycin for up to 1.5 h/day for 95 weeks. Serum levels of tobramycin of up to 35 microgram/mL were measured in rats, in contrast to the maximum 1.99 ± 0.59 microgram/mL level observed in CF patients in clinical trials. At the highest doses in rats, the estimated dose of tobramycin deposited in the lungs and adjusted for body surface area, was similar to the human clinical dose. There was no drug-related increase in the incidence of any variety of tumour.

6 Pharmaceutical Particulars

6.1 List of Excipients

See Section 2 Qualitative and Quantitative Composition.

6.2 Incompatibilities

Incompatibilities were either not assessed or not identified as part of the registration of this medicine.

6.3 Shelf Life

In Australia, information on the shelf life can be found on the public summary of the Australian Register of Therapeutic Goods (ARTG). The expiry date can be found on the packaging.

6.4 Special Precautions for Storage

Tobi solution.

Tobi solution should be stored under refrigeration at 2°C-8°C. Upon removal from the refrigerator, or if refrigeration is unavailable, Tobi pouches (opened or unopened) may be stored at room temperature (up to 25°C) for up to 28 days.
Tobi solution should not be used beyond the expiration date stamped on the ampoule when stored under refrigeration (2°C-8°C) or beyond 28 days when stored at room temperature (up to 25°C). Tobi solution should not be used if it is cloudy or if there are particles in the solution.
Tobi solution ampoules should not be exposed to intense light. The solution in the ampoule is slightly yellow, but may darken with age if not stored in the refrigerator; however, the colour change does not indicate any change in the quality of the product as long as it is stored within the recommended storage conditions.
The contents of the whole ampoule should be used directly after opening; opened ampoules should never be stored for re-use.

Tobi Podhaler.

Do not store above 30°C. Protect from moisture. Store capsules in their original packaging and remove immediately before use only.

Podhaler device.

Store the Podhaler device in its tightly closed case when not in use. Discard each Podhaler device after seven days use.

6.5 Nature and Contents of Container

Tobi solution.

Tobi solution for inhalation is supplied in single-use, low-density polyethylene plastic 5 mL ampoules, containing 300 mg tobramycin. Tobi solution is packaged in laminated foil over-pouches, each containing 4 ampoules. Packs of 4*, 8*, or 56 ampoules.

Tobi Podhaler.

Each Tobi Podhaler capsule contains a white to almost white powder in a clear, colourless capsule with "MYL TPH" in blue radial imprint on one part of the capsule and the Mylan logo in blue radial imprint on the other part of the capsule. Capsules are packed in blister strips, with each blister strip containing a daily dose of 8 capsules; 4 capsules taken in the morning and 4 capsules taken in the evening.
The Podhaler is a plastic inhalation device, used to puncture the capsules and deliver a tobramycin aerosol into the lungs. Each Podhaler device is housed in a sealed plastic case, which is used to protect the device during transport, storage, and the in-use period.
Tobi Podhaler is supplied in a monthly pack of 224 capsules with 5 Podhalers (4 boxes of 56 capsules with 1 Podhaler plus 1 spare Podhaler). The sample pack is supplied in a pack of 8 capsules with 1 Podhaler.

6.6 Special Precautions for Disposal

In Australia, any unused medicine or waste material should be disposed of by taking to your local pharmacy.

6.7 Physicochemical Properties

Chemical structure.

C₁₈H₃₇N₅O₉.

CAS number.

32986-56-4.
Chemical name: O-3-amino-3-deoxy-α-D-glucopyranosyl-(l→4)-O-[2,6-diamino-2,3,6-trideoxy-α-D-ribo-hexopyranosyl-(l→6)]-2-deoxy-L-streptamine.
Molecular weight: 467.52.

7 Medicine Schedule (Poisons Standard)

Schedule 4 - Prescription Only Medicine.

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