Consumer medicine information

Prograf and Advagraf XL

Tacrolimus

BRAND INFORMATION

Brand name

Prograf

Active ingredient

Tacrolimus

Schedule

SUMMARY CMI

PROGRAF^® Capsules, Concentrated Injection; ADVAGRAF^® XL Prolonged-Release Capsules

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 PROGRAF or ADVAGRAF XL?

PROGRAF or ADVAGRAF XL contains the active ingredient tacrolimus. PROGRAF or ADVAGRAF XL is used so that your new liver, kidney, lung or heart will not be attacked or rejected by your body. For more information, see Section 1. Why am I using PROGRAF or ADVAGRAF XL? in the full CMI.

2. What should I know before I use PROGRAF or ADVAGRAF XL?

Do not use if you have ever had an allergic reaction to PROGRAF or ADVAGRAF XL, macrolide antibiotics, or any of the ingredients listed at the end of the CMI. ADVAGRAF XL and PROGRAF are not interchangeable.

For more information, see Section 2. What should I know before I use PROGRAF or ADVAGRAF XL? in the full CMI.

3. What if I am taking other medicines?

Some medicines may interfere with PROGRAF or ADVAGRAF XL and affect how it works.

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. See 3. What if I am taking other medicines? in the full CMI for more information.

4. How do I use PROGRAF or ADVAGRAF XL?

PROGRAF capsules should be taken in two doses (e.g. morning and evening) each day.
ADVAGRAF XL should be taken once a day in the morning.
PROGRAF or ADVAGRAF XL capsules should be taken at least 1 hour before or 2 to 3 hours after a meal preferably with water and not with grapefruit juice.

More instructions can be found in Section 4. How do I use PROGRAF or ADVAGRAF XL? in the full CMI.

5. What should I know while using PROGRAF or ADVAGRAF XL?

Things you should do	Tell your doctor if you become pregnant while taking PROGRAF or ADVAGRAF XL. PROGRAF or ADVAGRAF XL suppresses your immune system by lowering your body's immune defence system. This increases your risk of skin cancer and other cancers while taking PROGRAF or ADVAGRAF XL. You should always protect yourself from the sun, wear sunscreen, a hat and protective clothing.
Things you should not do	Do not take PROGRAF or ADVAGRAF XL to treat any other complaint unless your doctor says so. Do not give this medicine to anyone else, even if their symptoms are similar to yours.
Driving or using machines	PROGRAF or ADVAGRAF XL may cause visual or nervous disturbances. If affected, do not drive or operate machinery.
Looking after your medicine	Store PROGRAF capsules in a cool dry place where the temperature is below 30°C. Store ADVAGRAF XL capsules in a cool dry place where the temperature is below 25°C.

For more information, see Section 5. What should I know while using PROGRAF or ADVAGRAF XL? in the full CMI.

6. Are there any side effects?

There are a number of side effects associated with this medicine. It is important to be aware of them so that you can identify any symptoms if they occur (see the full CMI for more details). The serious side effects are: signs of allergy; fever; diabetes / increased blood sugar; swelling, numbness or tingling in your hands and feet; constant "flu-like" symptoms; unusual bleeding or bruising; high blood pressure; palpitations, abnormal heart rhythms, chest pain; new lumps or moles, or changes to existing moles; swelling of the eyelids, hands or feet due to excess fluid; a change in the amount of urine passed or in the number of times you urinate, pain on urinating, or other kidney problems; yellowing of the skin and/or eyes (jaundice); symptoms of anaemia; seizures (fits); buzzing or ringing in the ears, difficulty hearing. 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

PROGRAF^® Capsules, Concentrated Injection; ADVAGRAF^® XL Prolonged-Release Capsules

Active ingredient(s): tacrolimus

Consumer Medicine Information (CMI)

This leaflet provides important information about using PROGRAF capsules, ADVAGRAF XL Prolonged-Release capsules and PROGRAF Concentrated Injection. It does not contain all the available information. It does not take the place of talking to your doctor or pharmacist.

All medicines have risks and benefits. Your doctor has weighed the risks of you taking PROGRAF or ADVAGRAF XL against the benefits this medicine is expected to have for you.

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 PROGRAF or ADVAGRAF XL.

Keep this leaflet with your medicine. You may need to read it again.

Where to find information in this leaflet:

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

1. Why am I using PROGRAF or ADVAGRAF XL?

PROGRAF or ADVAGRAF XL contains the active ingredient tacrolimus, which is an immunosuppressive agent.

You have been given a new transplanted liver, kidney, lung or heart from another person because your own was no longer healthy. Your body recognises that this new organ is different from your other organs and will try to reject it by attacking it in the same way that it would attack germs that enter your body. This could make you become ill again. PROGRAF or ADVAGRAF XL stops this attack; it is very important to take PROGRAF or ADVAGRAF XL given to you by your doctor regularly so that your new liver, kidney, lung or heart will not be attacked or rejected.

If you have been taking other medicines for this purpose, but are still feeling unwell, your doctor may change your treatment and begin giving you PROGRAF or ADVAGRAF XL.

Your doctor may have prescribed PROGRAF or ADVAGRAF XL for another reason.

Ask your doctor if you have any questions about why this medicine has been prescribed for you.

2. What should I know before I use PROGRAF or ADVAGRAF XL?

Warnings

Do not use PROGRAF or ADVAGRAF XL if:

you are allergic to any medicine containing tacrolimus or other macrolides (these are antibiotics of the erythromycin family - trade names are Eryc, EES, Klacid, Zithromax, Rulide and Biaxsig), or any of the ingredients listed at the end of this leaflet.
Always check the ingredients to make sure you can use this medicine.

Some of the symptoms of an allergic reaction may include:

shortness of breath
wheezing or difficulty breathing
swelling of the face, lips, tongue or other parts of the body
rash, itching or hives on the skin

Do not use PROGRAF or ADVAGRAF XL if the packaging is torn or shows signs of tampering. Do not use PROGRAF or ADVAGRAF XL beyond the expiry date printed on the pack.

Check with your doctor if:

you are receiving cyclosporin immunosuppressive therapy.

If you have not told your doctor or pharmacist about any of the above, tell them before you start taking or are given PROGRAF or ADVAGRAF XL.

Your doctor will advise you whether or not to take PROGRAF or ADVAGRAF XL or if you need to adjust the dose or adapt your treatment.

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.

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

Check with your doctor if you are using oral contraceptives.

3. What if I am taking other medicines?

Some medicines may interfere with PROGRAF or ADVAGRAF XL and affect how it works.

In particular, you should tell your doctor if you are taking or have recently taken medicines like:

antifungal medicines and antibiotics, particularly so called macrolide antibiotics, used to treat infections e.g., ketoconazole, fluconazole, itraconazole, voriconazole, clotrimazole, miconazole, caspofungin, erythromycin, clarithromycin, josamycin, rifampicin, rifabutin and isoniazid
letermovir, used to prevent illness caused by CMV (human cytomegalovirus)
HIV protease inhibitors (e.g., ritonavir, nelfinavir, saquinavir), the booster medicine cobicistat, and combination tablets, or HIV non-nucleoside reverse transcriptase inhibitors (efavirenz, etravirine, nevirapine) used to treat HIV infection
HCV protease inhibitors (e.g., telaprevir, boceprevir, the combination ombitasvir/paritaprevir/ritonavir with or without dasabuvir, elbasvir/grazoprevir, and glecaprevir/pibrentasvir), used to treat hepatitis C infection
mycophenolic acid used to suppress the immune system to prevent transplant rejection
medicines for stomach ulcer and acid reflux (e.g., omeprazole, lansoprazole or cimetidine)
antiemetics, used to treat nausea and vomiting (e.g., metoclopramide)
cisapride or the antacid magnesium-aluminium hydroxide, used to treat heartburn
the contraceptive pill or other hormone treatments with ethinylestradiol, hormone treatments with danazol
medicines used to treat high blood pressure or heart problems (e.g., nifedipine, nicardipine, diltiazem and verapamil)
anti-arrhythmic drugs (amiodarone) used to control arrhythmia (uneven beating of the heart)
medicines known as “statins” used to treat elevated cholesterol and triglycerides
carbamazepine, phenytoin or phenobarbital, used to treat epilepsy
metamizole, used to treat pain and fever
the corticosteroids prednisolone and methylprednisolone, belonging to the class of corticosteroids used to treat inflammations or suppress the immune system (e.g., in transplant rejection)
nefazodone, used to treat depression
herbal preparations containing St. John's wort (Hypericum perforatum) or extracts of Schisandra sphenanthera
cannabidiol.

Tell your doctor if you are taking or need to take ibuprofen, amphotericin B, antibiotics (cotrimoxazole, vancomycin, or so-called aminoglycoside antibiotics such as gentamicin), or antivirals (e.g., acyclovir, ganciclovir, cidofovir, or foscarnet). These may worsen kidney or nervous system problems when taken together with PROGRAF or ADVAGRAF XL.

Your doctor also needs to know if you are taking potassium supplements or potassium-sparing diuretics (e.g., amiloride, triamterene, or spironolactone), or the antibiotics trimethoprim or cotrimoxazole that may increase levels of potassium in your blood, certain pain killers (so-called NSAIDs, e.g., ibuprofen), anticoagulants, or oral medication for diabetic treatment, while you receive PROGRAF or ADVAGRAF XL.

Your doctor or pharmacist can tell you what to do if you are taking any of these medicines.

4. How do I use PROGRAF or ADVAGRAF XL?

How much to take

You can only get PROGRAF or ADVAGRAF XL from your doctor. Your dose will be calculated according to your weight, age, and medical condition. As your health and the function of your new liver, kidney, lung or heart can be affected by how much medicine you take, it is normal that your doctor tests samples of your blood and urine at regular intervals. This is in order to test whether your medicine requires adjustment.

When to take PROGRAF or ADVAGRAF XL

PROGRAF should be taken in two doses (e.g. morning and evening) each day.
ADVAGRAF XL should be taken once a day in the morning.

How to take PROGRAF or ADVAGRAF XL?

Take the capsule from the blister pack and swallow it whole with plenty of water. Do not use grapefruit juice as it contains substances that interfere with the action of PROGRAF or ADVAGRAF XL.
PROGRAF or ADVAGRAF XL capsules should generally be taken on an empty stomach or at least 1 hour before or 2 to 3 hours after a meal.
If you receive PROGRAF Concentrated Injection by intravenous infusion, it will be added to a larger volume of diluent and infused over a prolonged period of time (usually 24 hours).
You must never change the dose yourself even if you are feeling better. It is very important that you keep taking this medicine so that your body will not reject your new liver, kidney, lung or heart.
If you accidentally take a larger dose than recommended, tell your doctor immediately.
If you do not understand the instructions provided with this medicine, ask your doctor or pharmacist for help.

If you forget to take PROGRAF or ADVAGRAF XL

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.

If you have missed more than one dose, or are not sure what to do, check with your doctor or pharmacist.

If you have trouble remembering when to take your medicine, ask your pharmacist for some hints.

If you take too much PROGRAF or ADVAGRAF XL

If you think that you have used too much PROGRAF or ADVAGRAF XL, you may need urgent medical attention.

You should immediately:

phone the Poisons Information Centre
(by calling 13 11 26), 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. You may need urgent medical attention.

5. What should I know while using PROGRAF or ADVAGRAF XL?

Things you should do

Always follow your doctor's instructions carefully.
Tell your doctor if you become pregnant while taking PROGRAF or ADVAGRAF XL.
If you are about to start taking a new medicine, tell your doctor and pharmacist that you are taking PROGRAF or ADVAGRAF XL.
PROGRAF or ADVAGRAF XL suppresses your immune system by lowering your body's immune defence system. This increases your risk of skin cancer and other cancers while taking PROGRAF or ADVAGRAF XL. You should always protect yourself from the sun, wear sunscreen, a hat and protective clothing.

Things you should not do

Do not take PROGRAF or ADVAGRAF XL to treat any other complaint unless your doctor says so.
Do not give this medicine to anyone else, even if their symptoms are similar to yours.

Driving or using machines

Be careful before you drive or use any machines or tools until you know how PROGRAF or ADVAGRAF XL affects you.

PROGRAF or ADVAGRAF XL may cause visual or nervous disturbances. If affected, do not drive or operate machinery.

Effects of food and alcohol

Food reduces the absorption of PROGRAF or ADVAGRAF XL. Therefore, the capsules should be taken at least 1 hour before or 2 to 3 hours after a meal.

Drinking alcohol

Tell your doctor if you drink alcohol.

Looking after your medicine

Use all the PROGRAF capsules within 3 months of opening the aluminium wrapper.

Use all the ADVAGRAF XL capsules within 12 months of opening the aluminium wrapper.

Keep PROGRAF or ADVAGRAF XL capsules in the blisters until it is time to take them.

Keep PROGRAF capsules in a cool dry place where the temperature is below 30°C.

Keep ADVAGRAF XL capsules in a cool dry place where the temperature is below 25°C.

Keep PROGRAF Concentrated Injection away from light and store below 25°C.

Keep your medicines where children cannot reach them. A locked cupboard at least one-and-a-half metres (1.5 m) above the ground is a good place to store medicines.

Do not store PROGRAF or ADVAGRAF XL, or any other medicine, in the bathroom or near a sink. Do not leave medicines in the car or on window sills. Heat and dampness can destroy some medicines.

Keep it where young children cannot reach it.

When to discard your medicine (as relevant)

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.

Do not be alarmed by this list of possible side effects. You may not experience any of them.

Ask your doctor or pharmacist to answer any questions you may have.

Less serious side effects

Less serious side effects	What to do
tiredness, lack of energy stomach upset, including nausea (feeling sick), vomiting, loss of appetite, diarrhoea, stomach cramps tremor (shaking) headache feeling depressed (sad) sleeping difficulties blurred vision or sensitive to light muscle cramps, tenderness or weakness	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

signs of allergy such as rash, itching or hives on the skin; swelling of the face, lips, tongue or other part of the body; shortness of breath, wheezing or troubled breathing
fever
diabetes / increased blood sugar
swelling, numbness or tingling (pins and needles) in your hands and feet
constant "flu-like" symptoms such as chills, sore throat, aching joints, swollen glands, or any other signs of infection
unusual bleeding or bruising
high blood pressure
palpitations, abnormal heart rhythms, chest pain
new lumps or moles, or changes to existing moles, anywhere on the body
swelling of the eyelids, hands or feet due to excess fluid
a change in the amount of urine passed or in the number of times you urinate, pain on urinating, or other kidney problems
yellowing of the skin and/or eyes (jaundice) often accompanied by generally feeling unwell (for example, tiredness, lack of energy, loss of appetite, nausea and vomiting, pain in the abdomen)
symptoms of anaemia, such as shortness of breath, tiredness or dizziness
seizures (fits)
buzzing or ringing in the ears, difficulty hearing
fever and bruising under the skin that may appear as red pinpoint dots, with or without unexplained extreme tiredness, confusion, yellowing of the skin or eyes (jaundice), with symptoms of acute renal failure (low or no urine output)

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.

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 effects 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 PROGRAF or ADVAGRAF XL contains

Active ingredient
(main ingredient)

tacrolimus

Other ingredients
(inactive ingredients)

PROGRAF capsules contain hypromellose, croscarmellose sodium, lactose monohydrate, and magnesium stearate. The capsule shell contains gelatin, titanium oxide, purified water (0.5 mg and 1 mg only), iron oxide yellow (0.5 mg capsules only) and iron oxide red (5 mg capsules only). The 0.5 mg and 1 mg capsules have a trace of printing ink: OPACODE monogramming ink S-1-15083 RED (ARTG PI No: 12388). The 5 mg capsules have a trace of printing ink: OPACODE monogramming ink S-1-18086 WHITE (ARTG PI No: 107579).
ADVAGRAF XL prolonged-release capsules contain hypromellose, ethylcellulose, lactose monohydrate and magnesium stearate. The capsule shells contain gelatin, titanium dioxide, iron oxide yellow, iron oxide red and sodium lauryl sulfate. The capsules also have a trace of printing ink, OPACODE monogramming ink S-1-15083 RED (ARTG PI NO: 12388).
PROGRAF Concentrated Injection contains polyoxyethylene (PEG-60) hydrogenated castor oil and ethanol.
Prograf and Advagraf XL capsules contain excipients with known effect: sugars as lactose and soya bean products.

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

What PROGRAF or ADVAGRAF XL looks like

PROGRAF

PROGRAF 0.5 mg capsules (AUST R 77280) are light yellow with "0.5 mg" and "[f]607" printed in red, packed in blister sheets of ten capsules and sealed in an aluminium wrapper (Pack size 100 capsules).
PROGRAF 1 mg capsules (AUST R 58930) are white with "1 mg" and "[f]617" printed in red, packed in blister sheets of ten capsules and sealed in an aluminium wrapper (Pack size 100 capsules).
PROGRAF 5 mg capsules (AUST R 58931) are greyish-red with "5 mg" and "[f]657" printed in white (Pack size 50 capsules).

ADVAGRAF XL

ADVAGRAF XL 0.5 mg prolonged-release capsules (AUST R 269212) are oblong capsules with a light yellow cap imprinted with "0.5 mg" and an orange body imprinted with "647" (Pack size 30 capsules).
ADVAGRAF XL 1 mg prolonged-release capsules (AUST R 269214) are oblong capsules with a white cap imprinted with "1 mg" and an orange body imprinted with "677" (Pack size 60 capsules).
ADVAGRAF XL 3 mg prolonged-release capsules (AUST R 306501) are oblong capsules with an orange cap imprinted with "3 mg" and an orange body imprinted with "637" (Pack size: 50 capsules).
ADVAGRAF XL 5 mg prolonged-release capsules (AUST R 269215) are oblong capsules with a greyish red cap imprinted with "5 mg" and an orange body imprinted with "687" (Pack size 30 capsules).

PROGRAF Concentrated Injection

PROGRAF Concentrated Injection ampoules (AUST R 58932) contain 5 mg tacrolimus in 1 mL (Pack size 10 ampoules).

Who distributes PROGRAF or ADVAGRAF XL

PROGRAF and ADVAGRAF XL are supplied in Australia by:

Astellas Pharma Australia Pty Ltd
Suite 2.01, 2 Banfield Road
Macquarie Park NSW 2113

Tel: 1800 751 755 (Medical Information)
Email: [email protected] (Medical Information)
Website: www.astellas.com/au

^® = Registered Trademark

This leaflet was prepared in Feb 2024.

Published by MIMS July 2024

BRAND INFORMATION

Brand name

Prograf

Active ingredient

Tacrolimus

Schedule

1 Name of Medicine

Tacrolimus.

2 Qualitative and Quantitative Composition

Prograf capsules.

Each 0.5 mg capsule contains 0.5 mg tacrolimus.
Each 1 mg capsule contains 1 mg tacrolimus.
Each 5 mg capsule contains 5 mg tacrolimus.

Excipients with known effect.

Sugars as lactose and soya bean products.
For the full list of excipients, see Section 6.1 List of Excipients.

Advagraf XL prolonged-release capsules.

Each 0.5 mg prolonged-release capsule contains 0.5 mg tacrolimus.
Each 1 mg prolonged-release capsule contains 1 mg tacrolimus.
Each 3 mg prolonged-release capsule contains 3 mg tacrolimus.
Each 5 mg prolonged-release capsule contains 5 mg tacrolimus.

Excipients with known effect.

Sugars as lactose and soya bean products.
For the full list of excipients, see Section 6.1 List of Excipients.

Prograf concentrated injection.

Each 1 mL of concentrated injection contains 5 mg tacrolimus.

Contains.

Contains alcohol as 95% v/v ethanol.
For the full list of excipients, see Section 6.1 List of Excipients.

3 Pharmaceutical Form

Prograf capsules.

Capsule.
Supplied as:
Prograf capsules 0.5 mg: light yellow hard gelatine capsules with '0.5 mg' and '[f]607' printed in red.
Prograf capsules 1 mg: white, hard gelatine capsules with '1 mg' and '[f]617' printed in red.
Prograf capsules 5 mg: greyish-red, hard gelatine capsules with '5 mg' and '[f]657' printed in white.

Advagraf XL prolonged-release capsules.

Prolonged release capsule.
Supplied as:
Advagraf XL 0.5 mg prolonged-release capsules: oblong capsules with a light yellow cap imprinted with "0.5 mg" and an orange body imprinted with "Astellas logo 647".
Advagraf XL 1 mg prolonged-release capsules: oblong capsules with a white cap imprinted with "1 mg" and an orange body imprinted with "Astellas logo 677".
Advagraf XL 3 mg prolonged-release capsules: oblong capsules with an orange cap imprinted with "3 mg" and an orange body imprinted with "Astellas logo 637".
Advagraf XL 5 mg prolonged-release capsules: oblong capsules with a greyish red cap imprinted with "5 mg" and an orange body imprinted with "Astellas logo 687".

Prograf concentrated injection.

Injection, concentrated.
Supplied as:
Prograf concentrated injection 5 mg/1 mL: colourless, clear, sterile liquid in transparent glass ampoules.

4 Clinical Particulars

4.1 Therapeutic Indications

Prograf and Advagraf XL are indicated for use as an adjunct to liver, kidney, lung or heart allograft transplantation in adults and children.

4.2 Dose and Method of Administration

The dosage recommendations given below for oral and intravenous administration should act as a guideline. Prograf and Advagraf XL doses should be adjusted according to individual patient requirements.
If allograft rejection or adverse events occur, alteration in the immunosuppressive regimen should be considered.

Method of administration.

It is recommended that the oral daily dose of Prograf be administered as two divided doses, in the morning and in the evening.
It is recommended that the oral daily dose of Advagraf XL be administered once daily in the morning.
Prograf and Advagraf XL capsules should generally be administered on an empty stomach or at least 1 hour before or 2 to 3 hours after a meal, to achieve maximum absorption (see Section 5.2 Pharmacokinetic Properties, Absorption).
Prograf and Advagraf XL capsules should be taken immediately following removal from the blister. The capsules should be swallowed with fluid (preferably water).
Oral administration of Prograf or Advagraf XL should commence as soon as practicable. In some transplantation patients, therapy has commenced orally by administering the Prograf capsule contents suspended in water via an intranasal gastric tube.
In patients unable to take oral capsules, therapy may be initiated with Prograf Concentrated Injection as a continuous IV infusion.
Prograf Concentrated Injection should be diluted in 5% glucose solution in polyethylene or glass bottles or in 0.9% sodium chloride injection solution in polyethylene bottles. The concentration of a solution for final infusion produced in this way should be in the range 0.004 - 0.1 mg/mL. The solution should not be given as a bolus.
If IV therapy is necessary, conversion from IV to oral tacrolimus is recommended as soon as oral therapy can be tolerated. This usually occurs within 2 - 3 days. In patients receiving an IV infusion, the first dose of oral therapy should be given 8 - 12 hours after discontinuing the IV infusion.

Instructions for use and handling.

Based on immunosuppressive effects of tacrolimus, inhalation or direct contact with skin or mucous membranes of injection solutions or powder contained in tacrolimus products should be avoided during preparation. If such contact occurs, wash the skin and eyes.

Liver transplantation.

Oral tacrolimus therapy should commence at 0.10 - 0.20 mg/kg/day administered as two divided doses for Prograf or as a total daily dose for Advagraf XL. Administration should start approximately 6 hours after the completion of liver transplant surgery. If the clinical condition of the patient does not allow for oral dosing then intravenous tacrolimus therapy should be initiated as a continuous 24 hour infusion, at 0.01 to 0.05 mg/kg/day.

Kidney transplantation.

Oral tacrolimus therapy should commence at 0.15 - 0.30 mg/kg/day administered as two divided doses for Prograf or as a total daily dose for Advagraf XL. Administration should start within 24 hours of kidney transplant surgery. If the clinical condition of the patient does not allow for oral dosing then intravenous tacrolimus therapy should be initiated as a continuous 24 hour infusion, at 0.04 to 0.06 mg/kg/day.

Lung transplantation.

Oral tacrolimus therapy should commence at 0.10-0.30 mg/kg/day administered as two divided doses for Prograf or as a total daily dose for Advagraf XL. Administration should start within 24 hours of lung transplant surgery. If the clinical condition of the patient does not allow for oral dosing then intravenous tacrolimus therapy should be initiated as a continuous 24 hour infusion, at 0.01 to 0.05 mg/kg/day.

Heart transplantation.

Oral tacrolimus therapy should commence at 0.075 mg/kg/day administered as two divided doses for Prograf or as a total daily dose for Advagraf XL. Administration should start within 24 hours of heart transplant surgery. If the clinical condition of the patient does not allow for oral dosing then intravenous tacrolimus therapy should be initiated as a continuous 24 hour infusion, at 0.01 to 0.02 mg/kg/day.

Further information for all indications follows.

Children.

Higher mg/kg doses may be required in children compared with adults to achieve the same tacrolimus blood concentration. It is recommended that the initial intravenous dose if needed should be 0.05 - 0.06 mg/kg/day. Initial oral doses should be 0.15 - 0.30 mg/kg/day as two divided doses.

Therapy dose levels for kidney, liver, lung or heart allograft rejection resistant to existing immunosuppressive regimens.

In patients experiencing rejection episodes, which are unresponsive to conventional immunosuppressive therapy, Prograf and Advagraf XL treatment should begin with the initial dose recommended for primary immunosuppression in that particular allograft.

Conversion.

Conversion of Prograf treated patients to Advagraf XL.

Allograft transplant patients maintained on twice daily Prograf capsules dosing requiring conversion to once daily Advagraf XL should be converted on a 1:1 (mg:mg) total daily dose basis. Advagraf XL should be administered in the morning. Following conversion, tacrolimus trough levels should be monitored and if necessary dose adjustments made to maintain similar systemic exposure.
In stable patients converted from Prograf (twice daily dosing) to Advagraf XL (once daily dosing) on a 1:1 (mg:mg) total daily dose basis, the systemic exposure to tacrolimus (AUC_0-24) for Advagraf XL was approximately 10% lower than that for Prograf. The relationship between tacrolimus trough levels (C₂₄) and systemic exposure (AUC_0-24) for Advagraf XL is similar to that of Prograf. When converting from Prograf capsules to Advagraf XL tacrolimus trough levels should be measured prior to conversion and within two weeks after conversion. Dose adjustments should be made to ensure that similar systemic exposure is maintained.
In de novo kidney and liver transplant patients AUC_0-24 of tacrolimus for Advagraf XL on day 1 was 30% and 50% lower respectively, when compared with that for Prograf at equivalent doses. By day 4, systemic exposure as measured by trough levels is similar for both kidney and liver transplant patients with both formulations. Careful and frequent monitoring of tacrolimus trough levels is recommended in the first two weeks post-transplant with Advagraf XL to ensure adequate drug exposure in the immediate post-transplant period. As tacrolimus is a substance with low clearance, adjustments to the Advagraf XL dose regimen may take several days before steady state is achieved.

Conversion from ciclosporin to Prograf or Advagraf XL.

Care should be taken when converting patients from ciclosporin-based to tacrolimus-based therapy (see Section 4.4 Special Warnings and Precautions for Use, Conversion between agents; Section 4.5 Interactions with Other Medicines and Other Forms of Interactions). Tacrolimus-based therapy should be initiated after considering ciclosporin blood concentrations and the clinical condition of the patient. Dosing should be delayed in the presence of elevated ciclosporin blood levels. In practice, tacrolimus-based therapy has been initiated 12 - 24 hours after discontinuation of ciclosporin. Monitoring of ciclosporin blood levels should be continued following conversion as the clearance of ciclosporin might be affected.

Conversion between tacrolimus formulations.

Differences between oral formulations of tacrolimus can lead to important differences in systemic exposure to tacrolimus. Inadvertent or unsupervised switching between formulations is unsafe and could lead to graft rejection or increased incidence of side effects. Therefore, it is appropriate to prescribe and dispense tacrolimus by trade name, taking care to specify appropriate daily dosing (e.g. Prograf - twice daily dosing, Advagraf XL - once daily dosing). Patients must only be switched from one tacrolimus formulation to another under the close supervision of a transplant specialist.

Dose adjustments in special populations.

Elderly.

Experience in the elderly is limited. There is no evidence presently available to suggest that doses should be altered in elderly patients.

Patients with renal impairment.

No dose adjustment is required. However, careful monitoring of renal function is recommended.

Patients with liver impairment.

Tacrolimus is extensively metabolised by the liver. In patients with liver impairment dose reduction is recommended.
Tacrolimus is normally administered together with other immunosuppressive drugs. In isolated cases, successful maintenance therapy with tacrolimus alone has been described. Tacrolimus should not be given concurrently with ciclosporin.

Race.

In comparison to Caucasians, black patients may require higher tacrolimus doses to achieve similar trough levels.

Gender.

There is no evidence that male and female patients require different doses to achieve similar trough levels.

Monitoring advice.

Monitoring of tacrolimus whole blood trough concentrations in conjunction with other laboratory and clinical parameters is considered an essential aid to patient management for the evaluation of rejection, toxicity, dose adjustments and compliance. Factors influencing frequency of monitoring include but are not limited to hepatic or renal dysfunction, the addition or discontinuation of potentially interacting drugs and the post-transplant time. Blood trough concentration monitoring is not a replacement for renal or liver function monitoring and tissue biopsies.
Various assays have been used to measure blood or plasma concentrations of tacrolimus. Comparison of the concentrations in published literature to patient concentrations should be made with care and knowledge of the assay methods employed.
Trough blood concentrations should be measured at 12 hours after a Prograf dose or 24 hours after an Advagraf XL dose. The majority of patients (adults and children) can be successfully managed if the trough blood concentrations are maintained within the following range:
Liver transplant: 5 - 20 nanogram/mL for the first 3 months, 5 - 15 nanogram/mL thereafter.
Kidney transplant: 10 - 20 nanogram/mL for the first 3 months, 5 - 15 nanogram/mL thereafter.
Heart transplant: 10 - 20 nanogram/mL for the first 3 months, 5 - 15 nanogram/mL thereafter.
Lung transplant: 10 - 20 nanogram/mL for the first month, then 5 - 15 nanogram/mL thereafter.
During the first months post-transplant, monitoring of the following parameters should be undertaken on a routine basis: blood pressure, ECG, visual status, blood glucose levels, electrolytes (particularly potassium), creatinine, BUN, urinary output, haematology parameters, coagulation values, and liver and renal function tests. If clinically relevant changes are seen, adjustment of the immunosuppressive regimen should be considered.
Post-transplant improvement in the condition of the patient may alter the pharmacokinetics of Prograf and Advagraf XL. This should be considered when deciding upon a maintenance regimen.

4.3 Contraindications

Prograf and Advagraf XL are contraindicated in patients hypersensitive to tacrolimus or other macrolides, or to other ingredients of the capsules.
Prograf Concentrated Injection should not be used in patients known to be hypersensitive to polyoxyethylene hydrogenated castor oils.

4.4 Special Warnings and Precautions for Use

Tacrolimus therapy requires careful monitoring in hospital units equipped and staffed with adequate laboratory and supportive medical resources. The drug should only be prescribed, and changes in immunosuppressive therapy should be initiated, by physicians experienced in immunosuppressive therapy and the management of transplant patients. The physician responsible for maintenance therapy should have complete information requisite for the follow-up of the patient.

Post-transplant diabetes mellitus (PTDM).

Post-transplant insulin dependent diabetes mellitus (PTDM - use of insulin for 30 or more consecutive days, with < 5 day gap, by patients without a prior history of insulin or non-insulin-dependent diabetes mellitus) was reported in 20% (30/151) and 6% (17/281) of tacrolimus treated kidney transplant patients in the US and European randomised trials respectively. The median time to onset of PTDM was 68 days. Insulin dependence was reversible in 15% of these patients at one year and in 50% at two years post-transplant. Black and Hispanic patients were found to be at increased risk of development of PTDM in the US trial. The risk/benefit ratio should be carefully considered before using tacrolimus in kidney transplant patients with a pre-transplant diabetic condition.
In liver transplantation PTDM was reported in 18% (42/239) and 11% (26/239) of Prograf treated patients and was reversible in 45% and 31% of these patients at one year post-transplant in the US and European randomised trials, respectively.
Insulin-dependent post-transplant diabetes mellitus was reported in 13% (10/75) and 22% (29/132) of tacrolimus-treated heart transplant patients receiving mycophenolate mofetil or azathioprine and was reversible in 30% and 17% of these patients at one year post transplant, in the US and European randomised studies, respectively.

Neurotoxicity.

Neurological and CNS disorders have been reported with tacrolimus therapy. Symptoms include tremor, headache, changes in motor function, sensory function or mental status, insomnia, seizures, coma and delirium. Patients experiencing such events should be carefully monitored. In cases of severe or worsening neurological disorder, adjustment of the immunosuppressive regimen should be considered.

Posterior reversible encephalopathy syndrome (PRES).

Patients treated with tacrolimus have been reported to develop posterior reversible encephalopathy syndrome (PRES). If patients taking tacrolimus present with symptoms indicating PRES such as headache, altered mental status, seizures, and visual disturbances, a radiological procedure (e.g. MRI) should be performed. If PRES is diagnosed, adequate blood pressure and seizure control and immediate discontinuation of systemic tacrolimus is advised. Most patients completely recover after appropriate measures are taken.

Pure red cell aplasia (PRCA).

Cases of pure red cell aplasia (PRCA) have been reported in patients treated with tacrolimus. All patients reported risk factors for PRCA such as parvovirus B19 infection, underlying disease or concomitant medications associated with PRCA.

Nephrotoxicity.

Tacrolimus can cause both acute and chronic renal function impairment. This can be seen in transplant patients due to its vasoconstrictive effect on renal vasculature, toxic tubulopathy and tubular-interstitial effects. Acute renal impairment can result in high serum creatinine, hyperkalaemia, decreased secretion of urea and hyperuricemia, and is usually reversible. Chronic renal impairment is characterized by progressive renal dysfunction, increased blood urea and proteinuria. These changes have been observed to be dose dependent and improvements have been associated with reduced dosing. The mechanism leading to these changes is not fully understood. Use of tacrolimus with sirolimus in heart transplantation patients in a US study was associated with increased risk of renal function impairment, and is not recommended. Patients with impaired renal function should be monitored closely to adjust the dosage of tacrolimus and may need transient reduction or discontinuation. Acute renal impairment without active intervention may progress to chronic renal impairment.
Care should be taken in using tacrolimus with other nephrotoxic drugs as it could result in potentiation of nephrotoxicity. When concurrent use of tacrolimus with other known nephrotoxic drugs is required, monitor renal function and tacrolimus blood concentrations frequently, and dose adjustments of both tacrolimus and/or concomitant medications should be considered upon initiation, throughout concurrent treatment and at discontinuation of such concomitant drugs. In particular, tacrolimus should not be used simultaneously with ciclosporin. Tacrolimus or ciclosporin should be discontinued at least 24 hours prior to initiating the other. In the presence of elevated tacrolimus or ciclosporin concentrations, dosing with the other drug usually should be further delayed.

Hyperkalaemia.

Mild to severe hyperkalaemia was reported in patients treated with tacrolimus, especially in patients with renal impairment. Patients may require treatment, and should avoid high dietary potassium intake. Serum potassium levels should be monitored and potassium-sparing diuretics should not be used during tacrolimus therapy.

Vaccinations.

As with other immunosuppressants, response to vaccination during treatment with tacrolimus may be less effective. The use of live attenuated vaccines should be avoided.

Gastrointestinal disorders.

Gastrointestinal perforation has been reported in patients treated with tacrolimus, although all cases were considered a complication of transplant surgery or accompanied by infection, diverticulum, or malignant neoplasm. As gastrointestinal perforation is a medically important event that may lead to a life-threatening or serious condition, adequate treatments including surgery should be considered immediately after a suspect symptom occurs.

Anaphylaxis with IV administration.

Prograf Concentrated Injection contains PEG-60 hydrogenated castor oil, which has been reported to cause anaphylactoid reactions. These reactions consist of flushing of the face and upper thorax, acute respiratory distress with dyspnoea and wheezing, blood pressure changes and tachycardia. Caution is therefore necessary in patients who have previously received, by intravenous injection or infusion, preparations containing PEG-60 hydrogenated castor oil and in patients with an allergenic predisposition. Studies in dogs have shown that the risk of anaphylaxis may be reduced by slow infusion of Prograf Concentrated Injection or by prior administration of an H₁ antihistamine. Prograf or Advagraf XL capsules 1 mg and 5 mg do not contain PEG-60 hydrogenated castor oil.

Potential interactions.

When substances with a potential for interaction (see Section 4.5 Interactions with Other Medicines and Other Forms of Interactions) - particularly strong inhibitors of CYP3A4 (such as telaprevir, boceprevir, ritonavir, ketoconazole, voriconazole, itraconazole or clarithromycin) or inducers of CYP3A4 (such as rifampin, rifabutin) - are being combined with tacrolimus, tacrolimus blood levels should be monitored to adjust the tacrolimus dose as appropriate in order to maintain similar tacrolimus exposure.
Early and frequent continued monitoring of tacrolimus blood levels within the first few days of co-administration, as well as monitoring for renal function, for QT prolongation with ECG, and for other side effects is strongly recommended when co-administered with CYP3A4 inhibitors (see Section 4.5 Interactions with Other Medicines and Other Forms of Interactions).

Malignancies.

As with other potent immunosuppressive compounds, patients treated with tacrolimus are at increased risk of developing lymphomas and other malignancies, particularly of the skin. The risk appears to be related to the intensity and duration of immunosuppression rather than to the use of any specific agent. Exposure to sunlight and ultraviolet (UV) light should be limited by wearing protective clothing and using a sunscreen with a high protection factor.
Lymphoproliferative disorder (LPD) related to Epstein-Barr Virus (EBV) infection has been reported in immunosuppressed organ transplant recipients. In patients switched to tacrolimus, this may be attributable to over-immunosuppression before commencing therapy with this agent. Very young (< 2 years), EBV-sero-negative children have been reported to have an increased risk of developing lymphoproliferative disorders. Therefore, in this patient group, EBV serology should be ascertained before starting treatment with tacrolimus. During treatment, careful monitoring is recommended.

Infections.

Like other immunosuppressants, tacrolimus predisposes patients to the development of a variety of bacterial, fungal, parasitic and viral infections. Oversuppression of the immune system can also increase susceptibility to opportunistic infections, sepsis and fatal infections, such as BK virus associated nephropathy, JC virus associated progressive multifocal leukoencephalopathy (PML) and CMV infection. These infections are often related to a high total immunosuppressive burden and may lead to serious or fatal conditions that physicians should consider in the differential diagnosis in immunosuppressed patients with deteriorating renal function or neurological symptoms.

Hypertension.

Hypertension is a common adverse effect of tacrolimus therapy. Antihypertensive therapy may be required; the control of blood pressure can be accomplished with any of the common antihypertensive agents. Since tacrolimus may cause hyperkalaemia, potassium-sparing diuretics should be avoided. While calcium-channel blocking agents can be effective in treating tacrolimus-associated hypertension, care should be taken since interference with tacrolimus metabolism may require a dosage reduction.

Myocardial hypertrophy.

Ventricular hypertrophy or hypertrophy of the septum, reported as cardiomyopathies have been observed in a few cases in association with administration of tacrolimus. Most of these have been reversible, occurring primarily in patients having tacrolimus blood trough levels higher than the recommended level. Mean tacrolimus whole blood trough concentrations during the period prior to diagnosis of myocardial hypertrophy in 20 patients with pre and post treatment echocardiograms ranged from 10.6 to 53.3 nanogram/mL in infants (N = 10, age 0.4 to 2 years), 4.0 to 45.7 nanogram/mL in children (N = 7, age 2 to 15 years) and 10.9 to 24.3 nanogram/mL in adults (N = 3, age 37 to 45 years). Other factors observed to increase the risk of these clinical conditions are, for example, previously existing heart diseases, corticosteroid usage, hypertension, renal or hepatic dysfunction, and fluid overload. Accordingly, high-risk patients should be monitored, e.g. with echocardiography or ECG. If abnormalities develop, dose reduction of tacrolimus therapy, or change of treatment to other immunosuppressive agent should be considered.

QT interval prolongation.

Tacrolimus may prolong the QT interval and may cause Torsades de pointes. Caution should be exercised in patients with known risk factors for QT prolongation (including, but not limited to, congenital or acquired QT prolongation, concomitant medications known to prolong the QT interval or known to increase tacrolimus exposure).

Thrombotic microangiopathy (TMA) (including haemolytic uraemic syndrome (HUS) and thrombotic thrombocytopenic purpura (TTP)).

Thrombotic microangiopathies may have a multifactorial etiology. Risk factors for TMA that can occur in transplant patients include, for example, severe infections, graft-versus-host disease (GVHD), Human Leukocyte Antigen (HLA) mismatch, the use of calcineurin inhibitors and mammalian target of rapamycin (mTOR) inhibitors. These risk factors may either alone or as a combination effect contribute to the risk of TMA.
Concurrent use of tacrolimus and mTOR inhibitors may contribute to the risk of TMA.

Conversion between agents.

Conversion between tacrolimus formulations.

Various formulations of tacrolimus are available. Medication errors have resulted in incorrect dosing or unsupervised switching between tacrolimus formulations. This has led to serious adverse events, including graft rejection, or other side effects which could be a consequence of either under exposure or over exposure to tacrolimus. Therefore, it is appropriate to prescribe and dispense tacrolimus by trade name, taking care to specify appropriate daily dosing (e.g. Prograf - twice daily dosing, Advagraf XL - once daily dosing). It should be emphasised that patients, once titrated to an effective dose of a particular formulation of tacrolimus, should not be changed to another formulation of tacrolimus without blood trough level monitoring, clinical assessment and re-titration (see Section 4.2 Dose and Method of Administration, Conversion).

Conversion with ciclosporin.

Tacrolimus should not be administered concurrently with ciclosporin as the half-life of the latter may be increased. Synergistic/additive nephrotoxic effects can also occur. Care should be taken when administering tacrolimus to patients who have previously received ciclosporin and when converting patients from ciclosporin- to tacrolimus-based therapy. It is recommended that ciclosporin blood levels are monitored prior to the administration of tacrolimus. The most appropriate time to initiate tacrolimus therapy should be based upon information on ciclosporin blood levels and the clinical condition of the patient. Dosing may be delayed in the presence of elevated ciclosporin levels. Monitoring of ciclosporin blood levels should be continued following conversion as the clearance of ciclosporin may be affected. A 24 hour interval between stopping ciclosporin and starting tacrolimus has been commonly used.
Patients switched to tacrolimus rescue therapy should not be given anti-lymphocyte treatment concomitantly.

Use in hepatic impairment.

Tacrolimus is extensively metabolised by the liver. In patients with liver impairment dose reduction is recommended (see Section 4.2 Dose and Method of Administration, Dose adjustments in special populations).

Use in renal impairment.

No dose adjustment is required. However, careful monitoring of renal function is recommended (see Section 4.2 Dose and Method of Administration, Dose adjustments in special populations).

Use in the elderly.

Experience in the elderly is limited. There is no evidence presently available to suggest that doses should be altered in elderly patients (see Section 4.2 Dose and Method of Administration, Dose adjustments in special populations).

Paediatric use.

Higher mg/kg doses may be required in children compared with adults to achieve the same tacrolimus blood concentration. It is recommended that the initial intravenous dose if needed should be 0.05 - 0.06 mg/kg/day: initial oral doses should be 0.15 - 0.30 mg/kg/day as two divided doses (see Section 4.2 Dose and Method of Administration).

Effects on laboratory tests.

No data available.

4.5 Interactions with Other Medicines and Other Forms of Interactions

Metabolic interactions.

Systemically available tacrolimus is metabolised by hepatic CYP3A4. There is also evidence of gastrointestinal metabolism by CYP3A4 in the intestinal wall. Concomitant use of drugs or herbal remedies known to inhibit or induce CYP3A4 may affect the metabolism of tacrolimus and thereby increase or decrease tacrolimus blood levels. Significant tacrolimus dose reductions and prolongation of dosing interval may be required in order to maintain similar tacrolimus exposure when co-administered with strong CYP3A4 inhibitors, particularly telaprevir. Rapid increase in tacrolimus level may occur when co-administered with CYP3A4 inhibitors. Cases have been reported in which a sharp rise in tacrolimus levels occurred very rapidly, as early as within 1-3 days after co-administration with a strong CYP3A4 inhibitor, clarithromycin, despite immediate reduction of tacrolimus dose. Therefore early, within the first few days of co-administration, and frequent continued monitoring of tacrolimus blood levels, as well as monitoring for renal function, for QT prolongation with ECG, and for other side effects is strongly recommended.

Inhibitors of metabolism.

Clinically the following substances have been shown to increase tacrolimus blood levels:
Strong interactions have been observed with antifungal agents such as ketoconazole, fluconazole, itraconazole and voriconazole, the macrolide antibiotics erythromycin and clarithromycin, HIV protease inhibitors (e.g. ritonavir, nelfinavir, saquinavir), HCV protease inhibitors (e.g. telaprevir, boceprevir), or the CMV antiviral letermovir and amiodarone. Concomitant use of these drugs may require decreased tacrolimus doses in nearly all patients.
Weaker interactions have been observed with clotrimazole, josamycin, nifedipine, nicardipine, diltiazem, verapamil, danazol, ethinylestradiol, omeprazole and nefazodone.
The herbal remedy Schisandra sphenanthera extract inhibits CYP3A4 and may increase the blood levels of tacrolimus.
In vitro the following substances have been shown to be potential inhibitors of tacrolimus metabolism: bromocriptine, cortisone, dapsone, ergotamine, gestodene, lidocaine, mephenytoin, miconazole, midazolam, nilvadipine, norethindrone, quinidine, tamoxifen, (triacetyl)oleandomycin.
Grapefruit juice has been reported to increase the blood level of tacrolimus and should therefore be avoided.
Lansoprazole and ciclosporin may potentially inhibit CYP3A4-mediated metabolism of tacrolimus and thereby increase tacrolimus whole blood concentrations.

Other interactions leading to increased tacrolimus blood levels.

There have been reports of increased tacrolimus blood levels during concomitant use of tacrolimus with cannabidiol. This may be due to inhibition of intestinal P-glycoprotein, leading to increased bioavailability of tacrolimus. Tacrolimus and cannabidiol should be co-administered with caution, closely monitoring for side effects. Monitor tacrolimus whole blood trough concentrations and reduce the tacrolimus dose as necessary.

Inducers of metabolism.

Clinically the following substances have been shown to decrease tacrolimus blood levels:
Strong interactions have been observed with rifampicin, phenytoin or St John's wort (Hypericum perforatum) which may require increased tacrolimus doses in almost all patients. Clinically significant interactions have also been observed with phenobarbital. Maintenance doses of corticosteroids have been shown to reduce tacrolimus blood levels.
High dose prednisolone or methylprednisolone administered for the treatment of acute rejection have the potential to increase or decrease tacrolimus blood levels.
Carbamazepine, metamizole and isoniazid have the potential to decrease tacrolimus concentrations.

Other interactions leading to decreased tacrolimus blood levels.

Caspofungin has been shown to decrease the blood levels of tacrolimus. Mechanism of interaction has not been confirmed.

Effect of tacrolimus on the metabolism of other drugs.

Tacrolimus is a known CYP3A4 inhibitor; thus concomitant use of tacrolimus with drugs known to be metabolised by CYP3A4 may affect the metabolism of such drugs.
The half-life of ciclosporin is prolonged when tacrolimus is given concomitantly. In addition, synergistic/additive nephrotoxic effects can occur. For these reasons, the combined administration of ciclosporin and tacrolimus is not recommended and care should be taken when administering tacrolimus to patients who have previously received ciclosporin.
Tacrolimus has been shown to increase the blood level of phenytoin.
As tacrolimus may reduce the clearance of steroid-based contraceptives leading to increased hormone exposure, particular care should be exercised when deciding upon contraceptive measures.
Limited knowledge of interactions between tacrolimus and statins is available. Available data suggests that the pharmacokinetics of statins are largely unaltered by the co-administration of tacrolimus.
Animal data have shown that tacrolimus could potentially decrease the clearance and increase the half-life of pentobarbital and antipyrine.
Other potential interactions that may increase systemic exposure of tacrolimus: prokinetic agents such as metoclopramide and cisapride; cimetidine; magnesium-aluminium hydroxide.

Other interactions which have led to clinically detrimental effects.

Concurrent use of tacrolimus with drugs known to have nephrotoxic or neurotoxic effects may increase these effects (e.g. aminoglycosides, gyrase inhibitors, vancomycin, cotrimoxazole, NSAIDs, ganciclovir or aciclovir).
Enhanced nephrotoxicity has been observed following the administration of amphotericin B and ibuprofen in conjunction with tacrolimus.
As tacrolimus treatment may be associated with hyperkalaemia, or may increase pre-existing hyperkalaemia, high potassium intake, or potassium-sparing diuretics (e.g. amiloride, triamterene or spironolactone) should be avoided.
Immunosuppressants may affect the response to vaccination and vaccination during treatment with tacrolimus may be less effective. The use of live attenuated vaccines should be avoided.

Protein binding considerations.

Tacrolimus is extensively bound to plasma proteins. Possible interactions with other drugs known to have high affinity for plasma proteins should be considered (e.g. NSAIDs, oral anticoagulants or oral antidiabetics).

Other considerations.

Combination therapy with mycophenolic acid (MPA) products: Caution should be exercised when switching combination therapy from ciclosporin to tacrolimus and vice versa. Exposure to MPA is higher with tacrolimus co-administration than with ciclosporin co-administration because ciclosporin interrupts the enterohepatic recirculation of MPA while tacrolimus does not. Therapeutic drug monitoring of MPA is recommended.
Impact of direct-acting antiviral (DAA) therapy: The pharmacokinetics of tacrolimus may be impacted by changes in liver function during DAA therapy, related to clearance of HCV virus. A close monitoring and potential dose adjustment of tacrolimus is warranted to ensure continued efficacy and safety.

4.6 Fertility, Pregnancy and Lactation

Effects on fertility.

Tacrolimus subcutaneously administered to male rats at doses of 2 or 3 mg/kg/day resulted in a dose-related decrease in sperm count.
(Category C)
In reproduction studies in rats and rabbits, adverse effects on the foetus were observed mainly at dose levels that were toxic to the dams.
Tacrolimus given orally at 1.0 mg/kg (0.8 to 2.2 times the clinical dose range based on body surface area) to male and female rats, prior to and during mating, as well as to dams during gestation and lactation, was associated with embryolethality and adverse effects on female reproduction which were indicated by a higher rate of post-implantation loss and increased numbers of undelivered and nonviable pups. When given at 3.2 mg/kg (2.6 to 6.9 times the clinical dose range based on body surface area), tacrolimus was associated with maternal and paternal toxicity as well as reproductive toxicity including marked adverse effects on estrous cycles, parturition, pup viability, and pup malformations.
Human data show that tacrolimus is able to cross the placenta.
There are no adequate and well-controlled studies in pregnant women. There is data from a voluntary pregnancy exposure registry (Transplantation Pregnancy Registry International (TPRI)) that monitors outcomes of pregnancy in female transplant recipients and those fathered by male transplant recipients exposed to immunosuppressants including tacrolimus.
Safety data from post-marketing surveillance and the TPRI suggest infants of organ transplant recipients using immunosuppressive medications including tacrolimus have an increased risk for miscarriage, pre-term delivery (< 37 weeks), low birth weight (< 2500 g), birth defects/congenital anomalies and foetal distress.
The use of tacrolimus during pregnancy has been associated with neonatal hyperkalaemia and renal dysfunction.
Tacrolimus use may also be associated with hyperglycemia or diabetes in pregnancy in the absence of pre-existing diabetes or gestational. Monitor maternal blood glucose levels regularly.
Tacrolimus may exacerbate hypertension in pregnant women and increase pre-eclampsia. Monitor and control blood pressure.
Females and males of reproductive potential should consider the use of appropriate contraception prior to starting treatment with tacrolimus.
Tacrolimus should be used during pregnancy only if the potential benefit to the mother justifies potential risk to the foetus.
Tacrolimus is excreted into breast milk. It is therefore recommended that mothers should not breast-feed while receiving tacrolimus.

4.7 Effects on Ability to Drive and Use Machines

Tacrolimus may cause visual and neurological disturbances. Patients treated with tacrolimus who are affected by such disorders should not drive a car or operate dangerous machinery.

4.8 Adverse Effects (Undesirable Effects)

The adverse drug reaction profile associated with immunosuppressive agents is often difficult to establish owing to the underlying disease and the concurrent use of multiple medications.
The most commonly reported adverse drug reactions (occurring in > 10% of patients) are tremor, renal impairment, hyperglycaemic conditions, diabetes mellitus, hyperkalaemia, infections, hypertension and insomnia.
Many of the adverse drug reactions stated below are reversible and/or respond to dose reduction. Oral administration appears to be associated with a lower incidence of adverse drug reactions compared with intravenous use. Adverse drug reactions are listed below in descending order by frequency of occurrence: 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).

Infections and infestations.

As is well known for other potent immunosuppressive agents, patients receiving tacrolimus are frequently at increased risk for infections (viral, bacterial, fungal, protozoal). The course of pre-existing infections may be aggravated. Both generalised and localised infections can occur.
Cases of CMV infection, BK virus associated nephropathy, as well as cases of JC virus associated progressive multifocal leukoencephalopathy (PML), have been reported in patients treated with immunosuppressants, including tacrolimus.

Neoplasms benign, malignant and unspecified.

Patients receiving immunosuppressive therapy are at increased risk of developing malignancies. Benign as well as malignant neoplasms including EBV-associated lymphoproliferative disorders and skin malignancies have been reported in association with tacrolimus treatment.

Blood and lymphatic system disorders.

Common: anaemia, leukopenia, thrombocytopenia, leukocytosis, red blood cell analyses abnormal. Uncommon: coagulopathies, coagulation and bleeding analyses abnormal, pancytopenia, neutropenia, thrombotic microangiopathy. Rare: thrombotic thrombocytopenic purpura, hypoprothrombinaemia.

Immune system disorders.

Allergic and anaphylactoid reactions have been observed in patients receiving tacrolimus.

Endocrine disorders.

Rare: hirsutism.

Metabolism and nutrition disorders.

Very common: hyperglycaemic conditions, diabetes mellitus, hyperkalaemia. Common: hypomagnesaemia, hypophosphataemia, hypokalaemia, hypocalcaemia, hyponatraemia, fluid overload, hyperuricaemia, appetite decreased, anorexia, metabolic acidoses, hyperlipidaemia, hypercholesterolaemia, hypertriglyceridaemia, other electrolyte abnormalities. Uncommon: dehydration, hypoproteinaemia, hyperphosphataemia, hypoglycaemia.

Psychiatric disorders.

Very common: insomnia. Common: anxiety symptoms, confusion and disorientation, depression, depressed mood, mood disorders and disturbances, nightmare, hallucination, mental disorders. Uncommon: psychotic disorder.

Nervous system disorders.

Very common: tremor, headache. Common: seizures, disturbances in consciousness, paraesthesias and dysaesthesias, peripheral neuropathies, dizziness, writing impaired, nervous system disorders. Uncommon: coma, central nervous system haemorrhages and cerebrovascular accidents, paralysis and paresis, encephalopathy, speech and language abnormalities, amnesia. Rare: hypertonia. Very rare: myasthenia.

Eye disorders.

Common: vision blurred, photophobia, eye disorders. Uncommon: cataract. Rare: blindness.

Ear and labyrinth disorders.

Common: tinnitus. Uncommon: hypoacusis. Rare: deafness neurosensory. Very rare: hearing impaired.

Cardiac disorders.

Common: ischaemic coronary artery disorders, tachycardia. Uncommon: ventricular arrhythmias and cardiac arrest, heart failures, cardiomyopathies, ventricular hypertrophy, supraventricular arrhythmias, palpitations, ECG investigations abnormal, heart rate and pulse investigations abnormal, QT prolongation, Torsades de Pointes. Rare: pericardial effusion. Very rare: echocardiogram abnormal.

Vascular disorders.

Very common: hypertension. Common: haemorrhage, thromboembolic and ischaemic events, peripheral vascular disorders, vascular hypotensive disorders. Uncommon: infarction, venous thrombosis deep limb, shock.

Respiratory, thoracic and mediastinal disorders.

Common: dyspnoea, parenchymal lung disorders, pleural effusion, pharyngitis, cough, nasal congestion and inflammations. Uncommon: respiratory failures, respiratory tract disorders, asthma. Rare: acute respiratory distress syndrome.

Gastrointestinal disorders.

Very common: diarrhoea, nausea. Common: gastrointestinal inflammatory conditions, gastrointestinal ulceration and perforation, gastrointestinal haemorrhages, stomatitis and ulceration, ascites, vomiting, gastrointestinal and abdominal pains, dyspeptic signs and symptoms, constipation, flatulence, bloating and distension, loose stools, gastrointestinal signs and symptoms. Uncommon: ileus paralytic, peritonitis, acute and chronic pancreatitis, blood amylase increased, gastro-oesophageal reflux disease, impaired gastric emptying. Rare: subileus, pancreatic pseudocyst.

Hepatobiliary disorders.

Very common: liver function test abnormal. Common: bile duct disorders, cholestasis and jaundice, hepatocellular damage and hepatitis. Rare: hepatic artery thrombosis, veno-occlusive liver disease. Very rare: hepatic failure.

Skin and subcutaneous disorders.

Common: pruritus, rash, alopecias, acne, sweating increased. Uncommon: dermatitis, photosensitivity. Rare: toxic epidermal necrolysis (Lyell's syndrome). Very rare: Stevens-Johnson syndrome.

Musculoskeletal and connective tissue disorders.

Common: arthralgia, muscle cramps, pain in limb*, back pain. Uncommon: joint disorders.

Renal and urinary disorders.

Very common: renal impairment. Common: renal failure, renal failure acute, oliguria, renal tubular necrosis, nephropathy toxic, urinary abnormalities, bladder and urethral symptoms. Uncommon: anuria, haemolytic uraemic syndrome. Very rare: nephropathy, cystitis haemorrhagic.

Reproductive system and breast disorders.

Uncommon: dysmenorrhoea and uterine bleeding.

General disorders and administration site conditions.

Common: asthenic conditions, febrile disorders, oedema, pain and discomfort, blood alkaline phosphatase increased, weight increased, body temperature perception disturbed. Uncommon: multi-organ failure, influenza like illness, temperature intolerance, chest pressure sensation, feeling jittery, feeling abnormal, blood lactate dehydrogenase increased, weight decreased. Rare: thirst, fall, chest tightness, mobility decreased, ulcer. Very rare: fat tissue increased.

Injury, poisoning and procedural complications.

Common: primary graft dysfunction.
*In isolated cases, pain in limb has been reported as part of Calcineurin-Inhibitor Induced Pain Syndrome (CIPS), which typically presents bilaterally and symmetrical, severe, ascending pain in the lower extremities.

Post marketing experience.

The following adverse events have been reported in association with tacrolimus use during worldwide post-marketing experience:

Blood and lymphatic system disorders.

Unknown frequency: agranulocytosis, haemolytic anaemia, pure red cell aplasia, febrile neutropenia.

Eye disorders.

Unknown frequency: optic neuropathy.

Nervous system disorders.

Unknown frequency: posterior reversible encephalopathy syndrome (PRES).

Musculoskeletal and connective tissue disorders.

Unknown frequency: Calcineurin-inhibitor induced pain syndrome (CIPS)*.
Medication errors, including inadvertent, unintentional or unsupervised substitution of immediate- or prolonged-release tacrolimus formulations, have been observed. A number of associated cases of transplant rejection have been reported (frequency cannot be estimated from available data).

Reporting suspected adverse effects.

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

Experience of overdosage is limited.
Early clinical experience (when initial induction doses were 2 - 3 times greater than those currently recommended) suggested that symptoms of overdosage may include glucose intolerance, renal, neurological and cardiac disorders, hyperkalaemia and hypertension. Over immunosuppression may increase risk of severe infections.
Liver function clearly influences all pre- and post-operative pharmacokinetic variables. Patients with failing liver grafts or those switched from other immunosuppressive therapy to Prograf or Advagraf XL should be monitored carefully to avoid overdosage.
No specific antidote to tacrolimus therapy is available. If overdosage occurs, general supportive measures and symptomatic treatment should be conducted.
Based on the poor aqueous solubility and extensive erythrocyte and plasma protein binding, it is anticipated that Prograf or Advagraf XL will not be dialysable. Data on haemoperfusion are not available. Activated charcoal may reduce absorption of the drug if given within one or two hours after ingestion. In patients who are not fully conscious or have impaired gag reflex, consideration should be given to administering activated charcoal via a nasogastric tube, once the airway is protected.
For information on the management of overdose, contact the Poisons Information Centre on 13 11 26 (Australia).

5 Pharmacological Properties

5.1 Pharmacodynamic Properties

Mechanism of action.

Tacrolimus is a macrolide lactone with potent in vitro and in vivo immunosuppressive activity. Studies suggest that tacrolimus inhibits the formation of cytotoxic lymphocytes which are regarded as being primarily responsible for graft rejection. Tacrolimus suppresses T-cell activation and T-helper-cell-dependent B-cell proliferation, as well as the formation of lymphokines such as interleukins-2 and -3 and gamma-interferon and the expression of the interleukin-2 receptor. At the molecular level, the effects of tacrolimus appear to be mediated by binding to a cytosolic protein (FKBP), which is responsible for the intracellular accumulation of the compound. A complex of tacrolimus-FKBP-12, calcium, calmodulin and calcineurin is formed and the phosphatase activity of calcineurin inhibited.
Studies in animals and man have shown that Prograf is able to prevent and treat graft rejection following transplantation of the liver, kidney, and other solid organs.

Clinical trials.

Prograf.

Liver.

The efficacy and safety of a Prograf based immunosuppressive regimen following orthotopic liver transplantation was assessed in two prospective, randomised, non-blinded multicentre trials. The active control groups were treated with a ciclosporin based regimen. In a European trial, patients received a tacrolimus-steroid based regimen (n = 264) or a ciclosporin-azathioprine-steroid (with or without anti-lymphocyte globulin) based regimen (n = 265).
Equivalent graft survival (77.5 vs. 72.69%) and patient survival (82.9 vs. 77.5%) was seen. Significant reductions were seen in the tacrolimus treated patients for incidence of acute rejection (40.5 vs. 49.8%), refractory acute rejection (0.8 vs. 5.3%) and chronic rejection (1.5 vs. 5.3%). In American trial patients received a tacrolimus-steroid regimen (n = 263) or a ciclosporin (mainly triple therapy) based regimen (n = 266). Equivalent graft survival (82 vs. 79%) and patient survival (88 vs. 88%) rates were observed. Tacrolimus was associated with significant reductions in the incidence of acute rejection (68 vs. 76%), steroid resistant rejection (19 vs. 36%) and refractory rejection (3 vs. 15%).

Kidney.

Two randomised, multicentre non-blinded comparative trials were performed in cadaveric kidney transplantation. In an American trial patients received a tacrolimus based (n = 205) or ciclosporin based (n = 207) regimen. All patients also received maintenance azathioprine and corticosteroids and an induction course of an antilymphocyte antibody preparation. Equivalent graft survival (91.2 vs. 87.9%) and patient survival (95.6 vs. 96.6%) was seen for the tacrolimus and ciclosporin treated patients, respectively. A significantly reduced one year incidence rate of biopsy confirmed acute rejection (30.7 vs. 46.4%), moderate to severe acute rejection (10.7 vs. 26.6%) and use of antilymphocyte antibody preparation for treatment of rejection (10.7 vs. 25.1%) was seen in the tacrolimus treated patients.
A European trial compared triple drug based immunosuppression with tacrolimus or ciclosporin centred regimens, with 303 and 145 patients randomised to the tacrolimus and ciclosporin arms respectively. Equivalent one year graft survival (82.5 vs. 86.2%) and one year patient survival (93.0 vs. 96.5%) rates were observed, but with significantly reduced one year acute rejection rate (32.3 vs. 54.5%), rate of corticosteroid sensitive rejections (24.4 vs. 42.1%) and rate of corticosteroid resistant rejections (10.2 vs. 20.7%).

Heart.

Two open-label, randomised, comparative studies evaluated the safety and efficacy of tacrolimus-based and ciclosporin-based immunosuppression in primary orthotopic heart transplantation. In a Phase 3 study conducted in Europe, 314 patients received a regimen of antibody induction, corticosteroids and azathioprine in combination with tacrolimus or ciclosporin modified for 18 months. In a 3-arm study conducted in the US, 331 patients received corticosteroids and tacrolimus plus sirolimus, tacrolimus plus mycophenolate mofetil (MMF) or ciclosporin modified plus MMF for 1 year.
In the European Phase 3 study, patient/ graft survival at 18 months post-transplant was similar between treatment arms, 91.7% in the tacrolimus group and 89.2% in the ciclosporin group. In the US study, patient and graft survival at 12 months was similar with 93.5% survival in the tacrolimus plus MMF group and 86.1% survival in the ciclosporin modified plus MMF group. In the European study, the ciclosporin trough concentrations were above the pre-defined target range (i.e. 100-200 nanogram/mL) at Day 122 and beyond in 32 - 68% of the patients in the ciclosporin treatment arm, whereas the tacrolimus trough concentrations were within the pre-defined target range (i.e. 5-15 nanogram/mL) in 74 - 86% of the patients in the tacrolimus treatment arm.
The US study contained a third arm of a combination regimen of sirolimus, 2 mg/day, and full-dose tacrolimus; however, this regimen was associated with increased risk of wound healing complications, renal function impairment, and insulin dependent post-transplant diabetes mellitus, and is not recommended in de novo heart transplant patients (see Section 4.4 Special Warnings and Precautions for Use).

Lung.

In a prospective, 2-centre, open-label randomised trial, 74 lung transplant patients (aged 20-66 years old) were randomised to tacrolimus-based (n = 37) and ciclosporin-based (n = 37) immunosuppression. The drugs were given in combination with mycophenolate mofetil and corticosteroids. Tacrolimus was started immediately after transplantation as continuous intravenous infusion at a dose of 0.015 mg/kg/day and oral tacrolimus was administered at a dose of 0.1 to 0.3 mg/kg/day with subsequent dose adjustments to target trough levels of 12 to 15 nanogram/mL in the first month and 9 to 12 nanogram/mL thereafter. The 6-months and 1-year patient survival data was similar in both groups (89% vs. 84% and 82% vs. 71%, ciclosporin vs. tacrolimus respectively). Freedom from acute rejection was comparable at 1 year, 35% in the ciclosporin group and 46% in the tacrolimus group.
Another prospective, randomised, open-label study included 66 patients on tacrolimus versus 67 patients on ciclosporin, aged 20 to 66 years old. The drugs were given in combination with azathioprine and corticosteroids. Tacrolimus was started 6 to 8 hours after transplantation as continuous intravenous infusion at a dose of 0.025 mg/kg/day and oral tacrolimus was administered at a dose of 0.15 mg/kg/day with subsequent dose adjustments to target trough levels of 10 to 20 nanogram/mL. The 1-year patient survival was 83% in the tacrolimus group and 71% in the ciclosporin group, the 2-year survival rates were 76% and 66%, respectively. The differences between groups were not statistically significant. Freedom from acute rejection after at least 37 weeks follow-up was also comparable (14% in the tacrolimus group and 11.5% in the ciclosporin group).
A number of published, open, uncontrolled studies have examined the use of tacrolimus in lung transplant patients who have developed refractory acute rejection or bronchiolitis obliterans syndrome while receiving ciclosporin-based immunosuppressive regimens. In these studies, conversion from ciclosporin to tacrolimus has been associated with improved clinical outcomes such as reduced frequency of further acute rejection episodes and stabilisation or improvement in declining FEV₁ values.
Advagraf XL. Three phase III non-inferiority studies have been conducted, confirming the safety and efficacy of Advagraf XL is comparable to Prograf in de novo kidney transplant patients aged 12 years and older (n = 638 and 667) and de novo liver transplant patients aged 18 years and older (n = 471). Patient survival and graft survival at 1 year post-transplant ranged from 91% to 99%. In these studies tacrolimus was used in combination with corticosteroids (liver transplant), with corticosteroids and mycophenolate mofetil (kidney), or with corticosteroids, mycophenolate mofetil and basiliximab (kidney).
The results of all conversion studies demonstrate that conversion from Prograf-based immunosuppression regimens to Advagraf XL-based immunosuppression regimens on 1:1 (mg:mg) basis has been performed in adult kidney, liver and heart transplant recipients without any increase in incidences of acute rejection, graft loss or effects on patient survival rates. Long-term following up of patients in the conversion studies (up to 2 years) confirm patient survival and graft survival with Advagraf XL were consistent across all conversion studies, ranging from 97% to 100%.

5.2 Pharmacokinetic Properties

Absorption.

In man tacrolimus has been shown to be able to be absorbed throughout the gastrointestinal tract. Available tacrolimus is generally rapidly absorbed.
Following oral administration of Prograf capsules peak concentrations (C_max) of tacrolimus in blood are achieved in approximately 1 - 3 hours. Advagraf XL is a prolonged-release formulation of tacrolimus resulting in an extended oral absorption profile with an average time to C_max of approximately 2 hours. In some patients, tacrolimus appears to be continuously absorbed over a prolonged period yielding a relatively flat absorption profile. The mean oral bioavailability of Prograf is in the range of 20% - 25%.
After oral administration (0.30 mg/kg/day) to liver transplant patients, steady-state concentrations of Prograf were achieved within 3 days in the majority of patients.
In healthy subjects, Prograf 0.5 mg, Prograf 1 mg and Prograf 5 mg capsules have been shown to be bioequivalent, when administered as equivalent dose.
The rate and extent of absorption of tacrolimus is greatest under fasted conditions. The presence of food decreases both the rate and extent of absorption of tacrolimus, the effect being most pronounced after a high-fat meal. The effect of a high-carbohydrate meal is less pronounced.
In stable liver transplant patients, the oral bioavailability of Prograf was reduced when it was administered after a meal of moderate fat (34% of calories) content. Decreases in AUC (27%) and C_max (50%), and an increase in t_max (173%) in whole blood were evident.
In a study of stable renal transplant patients who were administered Prograf immediately after a standard continental breakfast the effect on oral bioavailability was less pronounced. Decreases in AUC (2 to 12%) and C_max (15 to 38%), and an increase in t_max (38 to 80%) in whole blood were evident.
Bile flow does not influence the absorption of Prograf.
A strong correlation exists between AUC and whole blood trough levels at steady-state for Prograf and Advagraf XL. Monitoring of whole blood trough levels, therefore, provides a good estimate of systemic exposure.

Distribution.

In man, the disposition of tacrolimus after intravenous infusion may be described as biphasic.
In the systemic circulation, tacrolimus binds strongly to erythrocytes resulting in an approximate 20:1 distribution ratio of whole blood/plasma concentrations. In plasma, tacrolimus is highly bound (> 98.8%) to plasma proteins, mainly to serum albumin and α-1-acid glycoprotein.
Tacrolimus is extensively distributed in the body. The steady-state volume of distribution based on plasma concentrations is approximately 1300 L (healthy subjects). Corresponding data based on whole blood averaged 47.6 L.
Tacrolimus is a low-clearance substance. In healthy subjects, the average total body clearance (TBC) estimated from whole blood concentrations was 2.25 L/h. In adult liver, kidney and heart transplant patients, values of 4.1 L/h, 6.7 L/h and 3.9 L/h, respectively, have been observed. Paediatric liver transplant recipients have a TBC approximately twice that of adult liver transplant patients. Factors such as low haematocrit and protein levels, which result in an increase in the unbound fraction of tacrolimus, or corticosteroid-induced increased metabolism are considered to be responsible for the higher clearance rates observed following transplantation.
The half-life of tacrolimus is long and variable. In healthy subjects, the mean half-life in whole blood is approximately 43 hours. In adult and paediatric liver transplant patients, it averaged 11.7 hours and 12.4 hours, respectively, compared with 15.6 hours in adult kidney transplant recipients. Increased clearance rates contribute to the shorter half-life observed in transplant recipients.

Metabolism.

Tacrolimus is widely metabolised in the liver, primarily by the cytochrome P450-3A4 (CYP3A4) and the cytochrome P450-3A5 (CYP3A5). Tacrolimus is also considerably metabolised in the intestinal wall. There are several metabolites identified. Only one of these has been shown in vitro to have immunosuppressive activity similar to that of tacrolimus. The other metabolites have only weak or no immunosuppressive activity. In systemic circulation only one of the inactive metabolites is present at low concentrations. Therefore, metabolites do not contribute to pharmacological activity of tacrolimus.

Excretion.

Following intravenous and oral administration of ¹⁴C-labelled tacrolimus, most of the radioactivity was eliminated in the faeces. Approximately 2% of the radioactivity was eliminated in the urine. Less than 1% of unchanged tacrolimus was detected in the urine and faeces, indicating that tacrolimus is almost completely metabolised prior to elimination: bile being the principal route of elimination.

Pharmacokinetics in special populations.

The pharmacokinetics of tacrolimus in special populations have not been studied in detail. For dose adjustments in special populations (see Section 4.2 Dose and Method of Administration).

5.3 Preclinical Safety Data

Genotoxicity.

No evidence of genotoxicity was seen in a series of assays for gene mutations and clastogenicity. Tacrolimus did not cause unscheduled DNA synthesis in rodent hepatocytes but high concentrations of tacrolimus have been reported to increase the frequency of sister chromatid exchanges in human lymphocytes in vitro.

Carcinogenicity.

Tacrolimus did not show any tumourigenic effects in long term carcinogenicity studies using the mouse and rat. The maximum dose tested in the rat resulted in a blood exposure less than, and a plasma exposure 1.4 times, the exposure achieved after the maximum recommended clinical dose, 0.3 mg/kg, based on AUC. In mice the maximum dose was 0.8 times the recommended clinical dose based on body surface area.
Patients receiving long-term immunosuppressive therapy are at an increased risk of developing lymphomas and other malignancies (see Section 4.4 Special Warnings and Precautions for Use, Malignancies).

6 Pharmaceutical Particulars

6.1 List of Excipients

Prograf capsules.

Prograf capsules contain hypromellose, croscarmellose sodium, lactose monohydrate and magnesium stearate. The capsule shell contains gelatin, titanium oxide, purified water (0.5 mg and 1 mg only), iron oxide yellow (0.5 mg capsules only) and iron oxide red (5 mg capsules only). The 0.5 mg and 1 mg capsules have a trace of printing ink: Opacode monogramming ink S-1-15083 Red (ARTG PI No: 12388). The 5 mg capsules have a trace of printing ink: Opacode monogramming ink S-1-18086 White (ARTG PI No: 107579).

Advagraf XL prolonged-release capsules.

Advagraf XL prolonged-release capsules contain hypromellose, ethylcellulose, lactose monohydrate and magnesium stearate. The capsule shells contain gelatin, titanium dioxide, iron oxide yellow, iron oxide red and sodium lauryl sulfate. The capsules also have a trace of printing ink, Opacode monogramming ink S-1-15083 Red (ARTG PI No: 12388).

Prograf concentrated injection.

Prograf concentrated injection contains PEG-60 hydrogenated castor oil and ethanol.

6.2 Incompatibilities

Tacrolimus is incompatible with PVC plastics. Tubing, syringes, and other equipment used to administer Prograf Concentrated Injection should not contain PVC.
See Section 4.5 Interactions with Other Medicines and Other Forms of Interactions.

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

Prograf capsules should be stored below 30°C. After opening the aluminium wrapper, Prograf capsules should all be used within three months. The blister strips should be kept in a dry place and the capsules should be left in the blister until required for use.
Advagraf XL prolonged-release capsules should be stored below 25°C. After opening the aluminium wrapper, Advagraf XL prolonged-release capsules should all be used within twelve months. The blister strips should be kept in a dry place and the capsules should be left in the blister until required for use.
Prograf Concentrated Injection should be protected from light and stored below 25°C. Once an ampoule is opened, the contents should be used immediately. Following reconstitution in either 5% w/v glucose solution in polyethylene or glass containers or in 0.9% Sodium Chloride Injection in polyethylene containers, the resulting infusion mixture should be used immediately.

6.5 Nature and Contents of Container

Prograf capsules are supplied as PVC-PVDC/Al blister strips each containing 10 capsules packed within a protective aluminium wrapper.

Package quantities.

Prograf capsules 0.5 mg: Cartons of 100 capsules.
Prograf capsules 1 mg: Cartons of 100 capsules.
Prograf capsules 5 mg: Cartons of 50 capsules.
Advagraf XL prolonged-release capsules are supplied as PVC-PVDC/Al blister strips each containing 10 capsules packed within a protective aluminium wrapper.

Package quantities.

Advagraf XL prolonged-release capsules 0.5 mg: Cartons of 30 and 50* capsules.
Advagraf XL prolonged-release capsules 1 mg: Cartons of 30*, 50*, 60 and 100* capsules.
Advagraf XL prolonged-release capsules 3 mg: Cartons of 50 capsules.
Advagraf XL prolonged-release capsules 5 mg: Cartons of 30 and 50* capsules.
(* Not marketed in Australia.)
Prograf Concentrated Injection 5 mg/mL: colourless, clear, sterile liquid in transparent glass ampoules.

Package quantities.

Prograf concentrated injection 5 mg/mL: Cartons of 10 ampoules.

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

Tacrolimus appears as white crystals or a crystalline powder, very soluble in methanol, and chloroform, freely soluble in acetone and ethanol and practically insoluble in hexane and water. Tacrolimus is obtained by fermentation as a single enantiomer but exists in tautomeric equilibration in aqueous solution.

Chemical structure.

[3S-[3R*[E (1S*, 3S*, 4S*)], 4S*, 5R*, 8S*, 9E, 12R*, 14R*, 15S*, 16R*, 18S*, 19S*, 26aR*]]-5, 6, 8, 11, 12, 13, 14, 15, 16, 17, 18, 19, 24, 25, 26, 26a-hexadecahydro-5, 19-dihydroxy-3- [2-(4-hydroxy-3-methoxycyclohexyl) -1-methylethenyl] -14, 16-dimethoxy-4, 10, 12, 18-tetramethyl-8-(2-propenyl)-15, 19-epoxy-3H-pyrido [2,1-c] [1,4] oxaazacyclotricosine-1, 7, 20, 21 (4H, 23H)-tetrone, monohydrate.

Molecular formula: C₄₄H₆₉NO₁₂.H₂O.
Molecular weight: 822.03.

CAS number.

CAS 104987-11-3.

7 Medicine Schedule (Poisons Standard)

Schedule 4 - Prescription Only Medicine.

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Advagraf XL 1 mg Capsules

Advagraf XL 3 mg Prolonged release capsule

Advagraf XL 5 mg Capsules

Advagraf XL 500 mcg Capsules

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