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نشرة الممارس الصحي نشرة معلومات المريض بالعربية نشرة معلومات المريض بالانجليزية صور الدواء بيانات الدواء
  SFDA PIL (Patient Information Leaflet (PIL) are under review by Saudi Food and Drug Authority)

What Brilinta is

Brilinta contains an active substance called ticagrelor. This belongs to a group of medicines called antiplatelet medicines.

 

What Brilinta is used for

Brilinta in combination with acetylsalicylic acid (another antiplatelet agent) is to be used in adults only. You have been given this medicine because you have had:

·     a heart attack, or

·     unstable angina (angina or chest pain that is not well controlled).

It reduces the chances of you having another heart attack, stroke or dying from a disease related to your heart or blood vessels.

 

How Brilinta works

Brilinta affects cells called ‘platelets’ (also called thrombocytes). These very small blood cells help stop bleeding by clumping together to plug tiny holes in blood vessels that are cut or damaged.

 

However, platelets can also form clots inside diseased blood vessels in the heart and brain. This can be very dangerous because:

·     the clot can cut off the blood supply completely; this can cause a heart attack (myocardial infarction) or stroke, or

·     the clot can partly block the blood vessels to the heart; this reduces the blood flow to the heart and can cause chest pain which comes and goes (called ‘unstable angina’).

 

Brilinta helps stop the clumping of platelets. This reduces the chance of a blood clot forming that can reduce blood flow.

 


Do not take Brilinta if:

·   You are allergic to ticagrelor or any of the other ingredients of this medicine (listed in section 6).

·     You are bleeding now.

·     You have had a stroke caused by bleeding in the brain.

·     You have severe liver disease.

·     You are taking any of the following medicines:

-  ketoconazole (used to treat fungal infections)

-  clarithromycin (used to treat bacterial infections)

-  nefazodone (an antidepressant)

-  ritonavir and atazanavir (used to treat HIV infection and AIDS)

Do not take Brilinta if any of the above applies to you. If you are not sure, talk to your doctor or pharmacist before taking this medicine.

 

Warnings and precautions

Talk to your doctor or pharmacist before taking Brilinta if:

·     You have an increased risk of bleeding because of:

-  a recent serious injury

-  recent surgery (including dental work, ask your dentist about this)

-  you have a condition that affects blood clotting

-  recent bleeding from your stomach or gut (such as a stomach ulcer or colon ‘polyps’)

·     You are due to have surgery (including dental work) at any time while taking Brilinta. This is because of the increased risk of bleeding. Your doctor may want you to stop taking this medicine 5 days prior to surgery.

·    Your heart rate is abnormally low (usually lower than 60 beats per minute) and you do not already have in place a device that paces your heart (pacemaker).

·    You have asthma or other lung problems or breathing difficulties.

·    You develop irregular breathing patterns such as speeding up, slowing down or short pauses in breathing. Your doctor will decide if you need further evaluation.

·    You have had any problems with your liver or have previously had any disease which may have affected your liver.

·    You have had a blood test that showed more than the usual amount of uric acid.

If any of the above apply to you (or you are not sure), talk to your doctor or pharmacist before taking this medicine.

 

If you are taking both Brilinta and heparin:

·    Your doctor may require a sample of your blood for diagnostic tests if they suspect a rare platelet disorder caused by heparin. It is important that you inform your doctor that you are taking both Brilinta and heparin, as Brilinta may affect the diagnostic test.

 

Children and adolescents

Brilinta is not recommended for children and adolescents under 18 years.

 

Other medicines and Brilinta

Please tell your doctor or pharmacist if you are taking, have recently taken or might take any other medicines. This is because Brilinta can affect the way some medicines work and some medicines can have an effect on Brilinta.

 

Tell your doctor or pharmacist if you are taking any of the following medicines:

·     more than 40 mg daily of either simvastatin or lovastatin (medicines used to treat high cholesterol)

·     rifampicin (an antibiotic)

·     phenytoin, carbamazepine and phenobarbital (used to control seizures)

·     digoxin (used to treat heart failure)

·     cyclosporine (used to lessen your body’s defenses)

·     quinidine and diltiazem (used to treat abnormal heart rhythms)

·     beta blockers and verapamil (used to treat high blood pressure)

·     morphine and other opioids (used to treat severe pain)

 

In particular, tell your doctor or pharmacist if you are taking any of the following medicines that increase your risk of bleeding:

·     ‘oral anticoagulants’ often referred to as ‘blood thinners’ which include warfarin.

·     Non‑Steroidal Anti‑Inflammatory Drugs (abbreviated as NSAIDs) often taken as painkillers such as ibuprofen and naproxen.

·     Selective Serotonin Reuptake Inhibitors (abbreviated as SSRIs) taken as antidepressants such as paroxetine, sertraline and citalopram.

·     other medicines such as ketoconazole (used to treat fungal infections), clarithromycin (used to treat bacterial infections), nefazodone (an antidepressant), ritonavir and atazanavir (used to treat HIV infection and AIDS), cisapride (used to treat heartburn), ergot alkaloids (used to treat migraines and headaches).

 

Also tell your doctor that because you are taking Brilinta, you may have an increased risk of bleeding if your doctor gives you fibrinolytics, often called ‘clot dissolvers’, such as streptokinase or alteplase.

 

 

Pregnancy and breast‑feeding

It is not recommended to use Brilinta if you are pregnant or may become pregnant. Women should use appropriate contraceptive measures to avoid pregnancy while taking this medicine.

 

Talk to your doctor before taking this medicine if you are breast‑feeding. Your doctor will discuss with you the benefits and risks of taking Brilinta during this time.

 

If you are pregnant or breast‑feeding, think you may be pregnant or are planning to have a baby, ask your doctor or pharmacist for advice before taking this medicine.

 

Driving and using machines

Brilinta is not likely to affect your ability to drive or use machines. If you feel dizzy or confused while taking this medicine, be careful while driving or using machines.

 

Sodium content

This medicine contains less than 1 mmol sodium (23 mg) per dose, that is to say it is essentially ‘sodium‑free’.

 


Always take this medicine exactly as your doctor has told you. Check with your doctor or pharmacist if you are not sure.

 

How much to take

·     The starting dose is two tablets at the same time (loading dose of 180 mg). This dose will usually be given to you in the hospital.

·     After this starting dose, the usual dose is one tablet of 90 mg twice a day for up to 12 months unless your doctor tells you differently.

·     Take this medicine around the same time every day (for example, one tablet in the morning and one in the evening).

 

Taking Brilinta with other medicines for blood clotting

Your doctor will usually also tell you to take acetylsalicylic acid. This is a substance present in many medicines used to prevent blood clotting. Your doctor will tell you how much to take (usually between 75‑150 mg daily).

 

How to take Brilinta

·     You can take the tablet with or without food.

·     You can check when you last took a tablet of Brilinta by looking on the blister. There is a sun (for the morning) and a moon (for the evening). This will tell you whether you have taken the dose.

 

If you have trouble swallowing the tablet

If you have trouble swallowing the tablet you can crush it and mix with water as follows:

·     Crush the tablet to a fine powder.

·     Pour the powder into half a glass of water.

·     Stir and drink immediately.

·     To make sure there is no medicine left, rinse the empty glass with another half a glass of water and drink it.

If you are in the hospital you may be given this tablet mixed with some water and given through a tube via the nose (nasogastric tube). 

 

If you take more Brilinta than you should

If you take more Brilinta than you should, talk to a doctor or go to hospital straight away. Take the medicine pack with you. You may be at increased risk of bleeding.

 

If you forget to take Brilinta

·     If you forget to take a dose, just take your next dose as normal.

·     Do not take a double dose (two doses at the same time) to make up for the forgotten dose.

 

If you stop taking Brilinta

Do not stop taking Brilinta without talking to your doctor. Take this medicine on a regular basis and for as long as your doctor keeps prescribing it. If you stop taking Brilinta, it may increase your chances of having another heart attack or stroke or dying from a disease related to your heart or blood vessels.

 

If you have any further questions on the use of this medicine, ask your doctor or pharmacist.

 


Like all medicines, this medicine can cause side effects, although not everybody gets them. The following side effects may happen with this medicine:

 

Brilinta affects blood clotting, so most side effects are related to bleeding. Bleeding may occur in any part of the body. Some bleeding is common (like bruising and nosebleeds). Severe bleeding is uncommon but can be life threatening.

 

See a doctor straight away if you notice any of the following – you may need urgent medical treatment:

·     Bleeding into the brain or inside the skull is an uncommon side effect, and may cause signs of a stroke such as:

-  sudden numbness or weakness of your arm, leg or face, especially if only on one side of the body

-  sudden confusion, difficulty speaking or understanding others

-  sudden difficulty in walking or loss of balance or co‑ordination

-  suddenly feeling dizzy or sudden severe headache with no known cause

 

·     Signs of bleeding such as:

-  bleeding that is severe or that you cannot control

-  unexpected bleeding or bleeding that lasts a long time

-  pink, red or brown urine

-  vomiting red blood or your vomit looks like ‘coffee grounds’

-  red or black stools (look like tar)

-  coughing up or vomiting blood clots

 

·     Fainting (syncope)

-  a temporary loss of consciousness due to sudden drop in blood flow to the brain (common)

 

·     Signs of a blood clotting problem called Thrombotic Thrombocytopenic Purpura (TTP) such as:

-  fever and purplish spots (called purpura) on the skin or in the mouth, with or without yellowing of the skin or eyes (jaundice), unexplained extreme tiredness or confusion

 

 

Discuss with your doctor if you notice any of the following:

·     Feeling short of breath ‑ this is very common. It might be due to your heart disease or another cause, or it might be a side effect of Brilinta. Brilinta ‑related breathlessness is generally mild and characterised as a sudden, unexpected hunger for air usually occurring at rest and may appear in the first weeks of therapy and for many may disappear. If your feeling of shortness of breath gets worse or lasts a long time, tell your doctor. Your doctor will decide if it needs treatment or further investigations.

 

Other possible side effects

 

Very common (may affect more than 1 in 10 people)

·     High level of uric acid in your blood (as seen in tests)

·     Bleeding caused by blood disorders

 

Common (may affect up to 1 in 10 people)

·     Bruising

·     Headache

·     Feeling dizzy or like the room is spinning

·     Diarrhoea or indigestion

·     Feeling sick (nausea)

·     Constipation

·     Rash

·     Itching

·     Severe pain and swelling in your joints – these are signs of gout

·     Feeling dizzy or light‑headed, or having blurred vision – these are signs of low blood pressure

·     Nosebleed

·     Bleeding after surgery or from cuts (for example while shaving) and wounds more than is normal

·     Bleeding from your stomach lining (ulcer)

·     Bleeding gums

 

Uncommon (may affect up to 1 in 100 people)

·     Allergic reaction – a rash, itching or a swollen face or swollen lips/tongue may be signs of an allergic reaction

·     Confusion

·     Visual problems caused by blood in your eye

·     Vaginal bleeding that is heavier, or happens at different times, than your normal period (menstrual) bleeding

·     Bleeding into your joints and muscles causing painful swelling

·     Blood in your ear

·     Internal bleeding, this may cause dizziness or light‑headedness

 

Not known (frequency cannot be estimated from the available data)

·     Abnormally Low heart rate (usually lower than 60 beats per minute)

 


Keep this medicine out of the sight and reach of children.

Do not use this medicine after the expiry date which is stated on the blister and carton after EXP. The expiry date refers to the last day of that month.

This medicine does not require any special storage conditions.

Do not throw away any medicines via wastewater or household waste. Ask your pharmacist how to throw away medicines you no longer use. These measures will help to protect the environment.

 


What Brilinta contains

·     The active substance is ticagrelor. Each film‑coated tablet contains 90 mg of ticagrelor.

 

·     The other ingredients are:

Tablet core: mannitol (E421), calcium hydrogen phosphate dihydrate, sodium starch glycolate type A, hydroxypropylcellulose (E463), magnesium stearate (E470b).

 

Tablet film‑coating: hypromellose (E464), titanium dioxide (E171), talc, macrogol 400, iron oxide yellow (E172).

 


What Brilinta looks like and contents of the pack Film coated tablet (tablet): The tablets are round, biconvex, yellow, film coated marked with a “90” above “T” on one side. Brilinta is available in: • standard blisters (with sun/moon symbols) in cartons of 60 and 180 tablets • calendar blisters (with sun/moon symbols) in cartons of 14, 56 and 168 tablets • perforated unit dosed blisters in a carton of 100x1 tablets Not all pack sizes may be marketed.

Marketing Authorisation Holder:

AstraZeneca AB

SE‑151 85 Södertälje

Sweden

 

Manufacturer:

AstraZeneca AB

Gärtunavägen

SE-152 57 Södertälje

Sweden


July 2023
  نشرة الدواء تحت مراجعة الهيئة العامة للغذاء والدواء (اقرأ هذه النشرة بعناية قبل البدء في استخدام هذا المنتج لأنه يحتوي على معلومات مهمة لك)

ما هو عقار بريلينتا

يحتوي عقار بريلينتا على مادة فعالة يُطلق عليها اسم تيكاجريلور. تنتمي هذا المادة إلى مجموعة من الأدوية يُطلق عليها الأدوية المضادة للصفيحات.

 

ما هي دواعي استعمال عقار بريلينتا

يُستخدم عقار بريلينتا في توليفة مع حمض أسيتيل ساليسيليك (عامل آخر مضاد للصفيحات) للبالغين فقط. لقد تم وصف هذا الدواء لك لأنك عانيت مما يلي:

·     نوبة قلبية، قبل أكثر من عام.

يقلل هذا العقار من احتمالات إصابتك بنوبة قلبية أو سكتة دماغية أخرى أو الوفاة من جراء الإصابة بمرض متعلق بالقلب أو الأوعية الدموية.

 

طريقة عمل عقار بريلينتا

يؤثر عقار بريلينتا على الخلايا التي يُطلق عليها "الصفيحات" (يُطلق عليها أيضًا اسم الصفيحات الدموية). تساعد خلايا الدم الصغيرة جدًا هذه على إيقاف النزف عن طريق التكدس جنبًا إلى جنب من أجل سد الفتحات الدقيقة في الأوعية الدموية التي تعرضت لجرح أو تلف.

 

مع ذلك، يمكن للصفيحات أيضًا تكوين الجلطات داخل الأوعية الدموية المريضة في القلب والمخ. وقد يشكّل ذلك خطورة بالغة نتيجة ما يلي:

·     يمكن للجلطة قطع تدفق الدم تمامًا - وقد يسبب ذلك نوبة قلبية (احتشاء عضلة القلب) أو سكتة دماغية، أو

·     يمكن للجلطة أن تسد الطريق على الأوعية الدموية الموصلة إلى القلب بشكل جزئي - يؤدي ذلك إلى تقليل تدفق الدم إلى القلب، كما يمكن أن يسبب ألمًا في الصدر كل حين والأخر (ويُسمى "الذبحة الصدرية غير المستقرة").

 

يساعد عقار بريلينتا على إيقاف تكدس الصفيحات. يؤدي ذلك إلى تقليل فرصة تكوّن الجلطات الدموية التي قد تقلل من تدفق الدم.

لا تتلقى عقار بريلينتا إذا:

·     كانت لديك حساسية تجاه تيكاجريلور أو أي من المكونات الأخرى لهذا الدواء (المذكورة في القسم 6).

·     كنت تعاني من نزف في الوقت الحالي.

·     كنت قد أصِبت بسكتة دماغية من جراء حدوث نزف في المخ.

·     كنت تعاني من مرض شديد في الكبد.

·     كنت تتلقى أيًا من الأدوية التالية:

-    كيتوكونازول (المستخدم في علاج العدوى الفطرية)

-    كلاريثرومايسين (المستخدم في علاج العدوى البكتيرية)

-    نيفازودون (المستخدم في علاج الاكتئاب)

-    ريتونافير وأتازانافير (المستخدمان في علاج العدوى بفيروس نقص المناعة البشرية المكتسب والإيدز).

لا تتلقى عقار بريلينتا في حال انطبق عليك أيٌّ مما سبق. إذا لم تكن متأكدًا، فتحدث إلى طبيبك أو الصيدلي قبل تلقي هذا العقار.

 

تحذيرات واحتياطات

تحدث إلى طبيبك أو الصيدلي قبل تلقي عقار بريلينتا إذا:

·     كنت معرضًا لخطر متزايد للإصابة بنزف لأنك:

-    أصبت إصابة بالغة مؤخرًا

-    خضعت مؤخرًا لعملية جراحية (يشمل ذلك جراحات الأسنان، استشر طبيب الأسنان المتابع لك في هذا الشأن)

-    تعاني من حالة تؤثر على تجلط الدم

-    أصبت مؤخرًا بنزف من معدتك أو أمعائك (مثل قرحة المعدة أو "سلائل" القولون)

·     كنت بصدد الخضوع لجراحة (بما في ذلك جراحات الأسنان) في أي وقت أثناء تلقي عقار بريلينتا. وذلك بسبب زيادة خطر الإصابة بنزف. قد يطلب منك طبيبك إيقاف تلقي هذا الدواء لمدة 5 أيام قبل الخضوع للجراحة.

·    كانت سرعة ضربات قلبك منخفضة بشكل غير طبيعي (عادةً أقل من 60 نبضة في الدقيقة) ولم يكن لديك بالفعل جهاز ينظم سرعة ضربات قلبك (منظم ضربات القلب).

·    كنت تعاني من مرض الربو أو مشاكل أخرى في الرئة أو صعوبات في التنفس.

·    كنت تعاني من أنماط تنفس غير منتظمة مثل سرعة التنفس، أو بطء التنفس، أو توقف التنفس لفترة قصيرة. سيقرر طبيبك ما إذا كنت بحاجة إلى مزيد من الفحص.

·    كنت تعاني من أي مشكلات في الكبد أو إذا كنت قد أصبت في الماضي بأي مرض ربما أثر على الكبد لديك.

·    خضعت لاختبار دم أظهر قدرًا من حمض اليوريك أكثر من القدر المعتاد.

في حال ما انطبق عليك أيٌّ مما سبق (أو إن لم تكن متأكدًا)، فتحدّث إلى طبيبك أو الصيدلي قبل تلقي هذا العقار.

 

إذا كنت تتلقى كلاً من عقار بريلينتا والهيبارين:

·    قد يطلب طبيبك عينة من دمك لإجراء اختبارات تشخيصية إذا اشتبه في إصابتك باضطراب نادر في الصفائح الدموية بسبب الهيبارين. من المهم أن تخبر طبيبك بأنك تتلقى كلاً من عقار بريلينتا والهيبارين، لأن عقار بريلينتا قد يؤثر على نتائج الاختبارات التشخيصية.

 

الأطفال والمراهقون

لا يُوصى باستخدام عقار بريلينتا مع الأطفال والمراهقين أقل من 18 عامًا.

 

الأدوية الأخرى وعقار بريلينتا

يُرجى إخبار طبيبك أو الصيدلي بما إذا كنت تتلقى حاليًا أو تلقيت مؤخرًا أو قد تتلقى أي أدوية أخرى. ويعود ذلك إلى أنّ عقار بريلينتا قد يؤثر على طريقة عمل بعض الأدوية كما قد يكون لبعض الأدوية تأثير على عقار بريلينتا.

 

أخبر طبيبك أو الصيدلي إذا كنت تتناول أي من الأدوية التالية:

·     روزيوفاستاتين (دواء لعلاج ارتفاع الكوليستيرول)

·     أكثر من 40 مجم يوميًا إما من سيمفاستاتين أو لوفاستاتين (دواءان مستخدمان لعلاج ارتفاع الكوليستيرول)

·     ريفامبيسين (مضاد حيوي)

·     فنيتوين أو كَرْبامازِيبين أو فينوباربيتال (تُستخدم لعلاج النوبات التشنجية)

·     ديجوكسين (يُستخدم لعلاج فشل القلب)

·     سايكلوسبورين (يُستخدم لتثبيط الجهاز المناعي بجسمك)

·     كينيدين وديلتيازيم (يُستخدمان لعلاج اضطرابات نظم القلب)

·     حاصرات البيتا وفيراباميل (يُستخدمان لعلاج ارتفاع ضغط الدم)

·     مورفين والأفيونات الأخرى (تُستخدم لعلاج الألم الشديد)

 

على وجه الخصوص، تحدث إلى طبيبك أو الصيدلي إذا كنت تتلقى أيًا من الأدوية التالية التي تزيد خطر الإصابة بنزف:

·     "مضادات التخثر الفموية" والتي يُشار إليها غالبًا باسم "مرققات الدم"، والتي تشمل وارفارين.

·     في كثير من الأحيان، يتم تلقي الأدوية غير الستيرويدية المضادة للالتهاب (التي يُشار إليها بالاختصار NSAID) كمسكّنات ألم مثل إيبوبروفين ونابروكسين.

·     "مثبطات استرجاع السيروتونين الانتقائية" (يُشار إليها بالاختصار SSRI) والتي تُستخدم كمضادات للاكتئاب مثل باروكستين وسيرترالين وسيتالوبرام.

·     الأدوية الأخرى مثل كيتوكونازول (المستخدم لعلاج العدوى الفطرية)، وكلاريثرومايسين (المستخدم لعلاج العدوى البكتيرية)، ونيفازودون (دواء مضاد للاكتئاب)، وريتونافير وأتازانافير (المستخدمان لعلاج عدوى فيروس نقص المناعة البشرية المكتسب ومرض الإيدز)، وسيسابرايد (المستخدم لعلاج حرقة المعدة)، وقلوانيَّات الإِرغوت (المستخدمة لعلاج داء الشقيقة وحالات الصداع).

 

كما ينبغي عليك أن تخبر طبيبك بذلك لأن تلقيك عقار بريلينتا قد يتسبب لك في زيادة خطر الإصابة بنزف إذا كان طبيبك قد وصف لك مواد مضادة للفبرين، والتي يُطلق عليها غالبًا "مذيبات الجلطات"، مثل ستربتوكيناز أو ألتيبليز.

 

الحمل والرضاعة الطبيعية

لا يُنصح باستخدام عقار بريلينتا إذا كنتِ حاملاً أو من المحتمل أن تحملي. يجب على النساء استعمال وسائل منع حمل مناسبة لتجنب حدوث الحمل أثناء فترة تلقي هذا الدواء.

 

تحدثي مع طبيبكِ قبل تلقي هذا الدواء إذا كنتِ تُرضعين طبيعيًا. سيتناقش معكِ طبيبكِ حول الفوائد والمخاطر الناجمة عن تلقي عقار بريلينتا في هذه الفترة.

 

إذا كنتِ حاملًا أو ترضعين طبيعيًا، أو تعتقدين أنكِ حاملًا، أو تخططين لإنجاب طفل، فاطلبي المشورة من طبيبك أو الصيدلي قبل تناول هذا الدواء.

 

القيادة واستخدام الآلات

من غير المحتمل أن يؤثّر عقار بريلينتا على قدرتك على القيادة أو استعمال الآلات. إذا شعرت بالدوخة أو الارتباك أثناء تلقي هذا الدواء، فتوخ الحذر أثناء القيادة أو استخدام الآلات.

 

محتوى الصوديوم

يحتوي هذا الدواء على أقل من 1 مليمول صوديوم (23 مجم) للجرعة، أي أنه يكاد يكون "خاليًا من الصوديوم".

 

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احرص دائمًا على تناول هذا الدواء تمامًا وفقًا لتوجيهات طبيبك. استشر طبيبك أو الصيدلي إذا لم تكن متأكدًا من طريقة تناوله.

 

عدد الأقراص الواجب تناولها

·     الجرعة العادية هي قرص واحد بجرعة 60 مجم مرتين يوميًا. استمر في تلقي عقار بريلينتا طوال المدة التي يوصي بها طبيبك.

·     احرص على تلقي هذا الدواء في الوقت نفسه من كل يوم تقريبًا (على سبيل المثال، قرص واحد صباحًا وقرص مساءً).

 

تلقي عقار بريلينتا مع أدوية أخرى مضادة لتجلط الدم

عادةً ما سيطلب منك طبيبك أيضًا تلقي حمض الأسيتيل ساليساليك. وهو مادة موجودة في الكثير من الأدوية المستخدمة لمنع تجلط الدم. سيخبرك طبيبك بالكمية التي يتعين عليك تلقيها (عادةً ما تكون بين 75 و150 مجم يوميًا).

 

كيفية تلقي عقار بريلينتا

·     يمكنك تلقي الأقراص مع الطعام أو بدونه.

·     يمكنك التحقق من آخر مرة تلقيت فيها قرص بريلينتا عن طريق فحص الشريط. ستجد علامة الشمس (للصباح) وعلامة القمر (للمساء). ستتمكن من خلال هاتين العلامتين من معرفة ما إذا كنت قد تلقيت الجرعة أم لا.

 

إذا عانيت من مشكلات عند ابتلاع القرص

إذا عانيت من مشكلات عند ابتلاع القرص، فيمكنك سحقه وخلطه مع الماء كما يلي:

·     اسحق القرص إلى مسحوق دقيق.

·     اسكب المسحوق في نصف كوب من الماء.

·     حّركه واشربه على الفور.

·     لضمان عدم وجود دواء متبقي، اشطف الكوب الفارغ بنصف كوب آخر من الماء واشربه.

إذا كنت متواجدًا في مستشفى، فقد تُعطى هذا القرص ممزوجًا ببعض الماء ومن خلال أنبوب عبر الأنف (أنبوب أنفي مَعِدي).

 

إذا تلقيت جرعة من عقار بريلينتا أكثر مما ينبغي

إذا تلقيت جرعة من عقار بريلينتا أكثر مما ينبغي، فتحدث إلى طبيبك أو توجّه إلى المستشفى على الفور. احتفظ بعلبة الدواء معك. فقد يزداد خطر الإصابة بنزف.

 

إذا نسيت تلقي عقار بريلينتا

·     إذا نسيت تلقي إحدى الجرعات، فما عليك سوى تلقي جرعتك التالية كالمعتاد.

·     لا تتلقى جرعة مضاعفة (جرعتين في نفس الوقت) بغرض تعويض الجرعة الفائتة.

 

إذا توقفت عن تلقي عقار بريلينتا

لا تتوقف عن تلقي عقار بريلينتا دون التحدث إلى طبيبك. احرص على تلقي هذا الدواء بشكل منتظم وطوال الفترة التي حدد لك الطبيب تلقيها فيها. إذا توقفت عن تلقي عقار بريلينتا، فقد تزداد احتمالات إصابتك بنوبة قلبية أخرى أو سكتة دماغية أو الوفاة من جراء الإصابة بمرض متعلق بقلبك أو أوعيتك الدموية.

 

إذا كانت لديك أي أسئلة أخرى بشأن استخدام هذا الدواء، ينبغي استشارة طبيبك أو الصيدلي.

 

 

4.     الآثار الجانبية المحتملة

قد يُسبِّب هذا الدواء، شأنه شأن جميع الأدوية، آثارًا جانبية، على الرغم من أنها لا تصيب الجميع. قد تحدث الآثار الجانبية التالية عند تلقي هذا الدواء:

 

يؤثر عقار بريلينتا على تجلط الدم، وبالتالي ترتبط غالبية أثاره الجانبية بالنزف. يمكن أن يحدث النزف في أي جزء من أجزاء الجسم. قد تحدث بعض أنواع النزف الشائعة (مثل الكدمات أو الرعاف). من غير الشائع حدوث نزف شديد، إلا أن هذا النزف قد يمثل مصدر تهديد للحياة في حال حدوثه.

 

استشر طبيبًا فورًا إذا لاحظت أيًا مما يلي - قد تحتاج إلى علاج طبي طارئ:

·     يُعد النزف في المخ أو داخل الجمجمة من الأعراض الجانبية غير الشائعة لهذا العقار، وقد يسبب في حال حدوثه أعراض السكتة الدماغية، مثل:

-    تنميل مفاجئ أو ضعف في ذراعك أو ساقك أو وجهك، خصوصًا إذا حدث هذا في جانب واحد فقط من الجسم

-    ارتباك مفاجئ أو صعوبة في التحدث إلى الآخرين أو فهمهم

-    صعوبة مفاجئة في المشي أو فقدان التوازن أو التوافق الحركي

-    شعور مفاجئ بالدوّار أو صداع شديد مفاجئ من دون سبب معروف

 

·     علامات تدل على الإصابة بالنزف، مثل:

-    نزف شديد أو يتعذر إيقافه

-    نزف غير متوقع أو نزف يستمر لفترة طويلة

-    تحول لون البول إلى اللون الوردي أو الأحمر أو البني

-    تقيؤ دم أحمر أو قيء يشبه "مسحوق القهوة"

-    براز أحمر أو أسود (يبدو أشبه بالقطران)

-    خروج خثرات دموية مع السعال أو القيء

 

·     الإغماء (الغشي)

-    فقدان مؤقت للوعي ناتج عن انخفاض مفاجئ في تدفق الدم للمخ (شائع)

 

·     علامات تدل على وجود مشكلة في تجلط الدم تُسمى الفرفرية القليلة الصفيحات الخثارية (TTP) مثل:

-    حمى وبقع أرجوانية (تُسمى الفرفرية) على الجلد أو في الفم، مصحوبة أو غير مصحوبة باصفرار الجلد أو العينين (اليرقان)، أو تعب شديد بدون سبب معروف أو ارتباك

 

تناقش مع طبيبك إذا لاحظت أيًا مما يلي:

·     الشعور بضيق في التنفس هذا شائع جدًا. قد ينجم ذلك عن إصابتك بمرض قلبي أو لسبب آخر، أو قد يكون أحد الآثار الجانبية لتلقي عقار بريلينتا. يتصف ضيق التنفس المرتبط بعقار بريلينتا بشكل عام بكونه خفيفًا ويتسم بأنه حالة مفاجئة وغير متوقعة من الحاجة المُلحة للهواء، تحدث عادةً وقت الراحة، وقد تظهر في الأسابيع الأولى من العلاج وقد تزول لدى الكثيرين. ابلغ طبيبك بما إذا شعرت بأن ضيق التنفس يزداد سوءًا أو استمر لفترة طويلة. سيقرر طبيبك ما إذا كنت بحاجة إلى علاج أو إجراء مزيد من الفحوصات.
 

الآثار الجانبية المحتملة الأخرى

 

شائعة جدًا (قد تصيب أكثر من شخص واحد من بين كل 10 أشخاص)

·     ارتفاع مستوى حمض اليوريك في دمك (يظهر في الاختبارات)

·     نزف ناتج عن الاضطرابات الدموية

 

شائعة (قد تصيب ما يصل إلى شخص واحد من بين كل 10 أشخاص)

·     التكدم

·     الصداع

·     الشعور بالدوخة أو الدوار وكأن الغرفة تدور

·     إسهال أو عسر هضم

·     الشعور بالغثيان

·     إمساك

·     الطفح الجلدي

·     حكة

·     آلام شديدة وتورم في مفاصلك – هاتان علامتان على النقرس

·     الشعور بالدوخة أو الدوار، أو تشوش الرؤية – هذه علامات على انخفاض ضغط الدم

·     رعاف

·     نزف بعد إجراء جراحة أو بسبب جروح (أثناء الحلاقة على سبيل المثال) والإصابة بالجروح أكثر من المعتاد

·     نزف بطانة معدتك (القرحة)

·     نزف اللثة

 

غير شائعة (قد تصيب ما يصل إلى شخص واحد من بين كل 100 شخص)

·     ردود فعل تحسسية – قد يكون الطفح الجلدي، أو الحكة، أو تورم الوجه أو الشفتين/اللسان علامات على وجود رد فعل تحسسي

·     الارتباك

·     مشكلات في الرؤية يسببها وجود دم في عينك

·     نزف مهبلي أكثر شدة من نزف الدورة الشهرية المعتاد أو يحدث في مواعيد مختلفة عن موعد الدورة الشهرية (الحيض)

·     نزف في مفاصلك أو عضلاتك يؤدي إلى تورم مؤلم

·     دم في أذنك

·     نزف داخلي، قد يؤدي هذا إلى الدوخة أو الدوار

 

غير معروفة (لا يمكن تقدير معدّل الحدوث من البيانات المتاحة)

·     انخفاض معدل ضربات القلب بشكل غير طبيعي (عادةً أقل من 60 نبضة في الدقيقة)

 

 

قد يُسبِّب هذا الدواء، شأنه شأن جميع الأدوية، آثارًا جانبية، على الرغم من أنها لا تصيب الجميع. قد تحدث الآثار الجانبية التالية عند تلقي هذا الدواء:

 

يؤثر عقار بريلينتا على تجلط الدم، وبالتالي ترتبط غالبية أثاره الجانبية بالنزف. يمكن أن يحدث النزف في أي جزء من أجزاء الجسم. قد تحدث بعض أنواع النزف الشائعة (مثل الكدمات أو الرعاف). من غير الشائع حدوث نزف شديد، إلا أن هذا النزف قد يمثل مصدر تهديد للحياة في حال حدوثه.

 

استشر طبيبًا فورًا إذا لاحظت أيًا مما يلي - قد تحتاج إلى علاج طبي طارئ:

·     يُعد النزف في المخ أو داخل الجمجمة من الأعراض الجانبية غير الشائعة لهذا العقار، وقد يسبب في حال حدوثه أعراض السكتة الدماغية، مثل:

-    تنميل مفاجئ أو ضعف في ذراعك أو ساقك أو وجهك، خصوصًا إذا حدث هذا في جانب واحد فقط من الجسم

-    ارتباك مفاجئ أو صعوبة في التحدث إلى الآخرين أو فهمهم

-    صعوبة مفاجئة في المشي أو فقدان التوازن أو التوافق الحركي

-    شعور مفاجئ بالدوّار أو صداع شديد مفاجئ من دون سبب معروف

 

·     علامات تدل على الإصابة بالنزف، مثل:

-    نزف شديد أو يتعذر إيقافه

-    نزف غير متوقع أو نزف يستمر لفترة طويلة

-    تحول لون البول إلى اللون الوردي أو الأحمر أو البني

-    تقيؤ دم أحمر أو قيء يشبه "مسحوق القهوة"

-    براز أحمر أو أسود (يبدو أشبه بالقطران)

-    خروج خثرات دموية مع السعال أو القيء

 

·     الإغماء (الغشي)

-    فقدان مؤقت للوعي ناتج عن انخفاض مفاجئ في تدفق الدم للمخ (شائع)

 

·     علامات تدل على وجود مشكلة في تجلط الدم تُسمى الفرفرية القليلة الصفيحات الخثارية (TTP) مثل:

-    حمى وبقع أرجوانية (تُسمى الفرفرية) على الجلد أو في الفم، مصحوبة أو غير مصحوبة باصفرار الجلد أو العينين (اليرقان)، أو تعب شديد بدون سبب معروف أو ارتباك

 

تناقش مع طبيبك إذا لاحظت أيًا مما يلي:

·     الشعور بضيق في التنفس هذا شائع جدًا. قد ينجم ذلك عن إصابتك بمرض قلبي أو لسبب آخر، أو قد يكون أحد الآثار الجانبية لتلقي عقار بريلينتا. يتصف ضيق التنفس المرتبط بعقار بريلينتا بشكل عام بكونه خفيفًا ويتسم بأنه حالة مفاجئة وغير متوقعة من الحاجة المُلحة للهواء، تحدث عادةً وقت الراحة، وقد تظهر في الأسابيع الأولى من العلاج وقد تزول لدى الكثيرين. ابلغ طبيبك بما إذا شعرت بأن ضيق التنفس يزداد سوءًا أو استمر لفترة طويلة. سيقرر طبيبك ما إذا كنت بحاجة إلى علاج أو إجراء مزيد من الفحوصات.
 

الآثار الجانبية المحتملة الأخرى

 

شائعة جدًا (قد تصيب أكثر من شخص واحد من بين كل 10 أشخاص)

·     ارتفاع مستوى حمض اليوريك في دمك (يظهر في الاختبارات)

·     نزف ناتج عن الاضطرابات الدموية

 

شائعة (قد تصيب ما يصل إلى شخص واحد من بين كل 10 أشخاص)

·     التكدم

·     الصداع

·     الشعور بالدوخة أو الدوار وكأن الغرفة تدور

·     إسهال أو عسر هضم

·     الشعور بالغثيان

·     إمساك

·     الطفح الجلدي

·     حكة

·     آلام شديدة وتورم في مفاصلك – هاتان علامتان على النقرس

·     الشعور بالدوخة أو الدوار، أو تشوش الرؤية – هذه علامات على انخفاض ضغط الدم

·     رعاف

·     نزف بعد إجراء جراحة أو بسبب جروح (أثناء الحلاقة على سبيل المثال) والإصابة بالجروح أكثر من المعتاد

·     نزف بطانة معدتك (القرحة)

·     نزف اللثة

 

غير شائعة (قد تصيب ما يصل إلى شخص واحد من بين كل 100 شخص)

·     ردود فعل تحسسية – قد يكون الطفح الجلدي، أو الحكة، أو تورم الوجه أو الشفتين/اللسان علامات على وجود رد فعل تحسسي

·     الارتباك

·     مشكلات في الرؤية يسببها وجود دم في عينك

·     نزف مهبلي أكثر شدة من نزف الدورة الشهرية المعتاد أو يحدث في مواعيد مختلفة عن موعد الدورة الشهرية (الحيض)

·     نزف في مفاصلك أو عضلاتك يؤدي إلى تورم مؤلم

·     دم في أذنك

·     نزف داخلي، قد يؤدي هذا إلى الدوخة أو الدوار

 

غير معروفة (لا يمكن تقدير معدّل الحدوث من البيانات المتاحة)

·     انخفاض معدل ضربات القلب بشكل غير طبيعي (عادةً أقل من 60 نبضة في الدقيقة)

 

 

لا تُخزّنه في درجة حرارة أعلى من 30 درجة مئوية

احفظ هذا الدواء بعيدًا عن مرأى الأطفال ومتناولهم.

لا تستخدم هذا الدواء بعد تاريخ انتهاء الصلاحية المطبوع على الشريط البلاستيكي والعلبة الكرتونية بعد كلمة "EXP". يشير تاريخ انتهاء الصلاحية إلى آخر يوم في هذا الشهر.

لا يستلزم هذا الدواء أي شروط تخزين خاصة.

لا تتخلص من الأدوية في مياه الصرف الصحي أو مكب النفايات المنزلية. اسأل الصيدلي عن كيفية التخلص من الأدوية التي لم تعد تستخدمها. ستُساعد هذه الإجراءات في حماية البيئة.

 

المواد التي يحتوي عليها عقار بريلينتا

·     المادة الفعالة هي تيكاجريلور. يحتوي كل قرص مغلف على ٦٠ مجم من تيكاجريلور.

 

·     المكونات الأخرى هي:

مكونات القرص: مانِّيتول (E421)، ثنائي هيدرات فوسفات هيدروجين الكالسيوم، غليكولات نشاء الصوديوم من النوع A، هيدروكسي بروبيل السيليلوز (E463)، ستيرات المغنسيوم (E470b).

 

غلاف القرص: هايبروميلوز (E464)، ثاني أكسيد التيتانيوم (E171)، ماكروغول 400، أكسيد الحديد الأسود (E172) وأكسيد الحديد الأحمر (E172).

 

يتوفر عقار بريلينتا في:

·     أشرطة بلاستيكية (تحتوي على رمزيّ الشمس/القمر) في علب كرتون تحتوي على 60 و180 قرصًا

·     أشرطة مرتبة بالتقويم (تحتوي على رمزيّ الشمس/القمر) في علب كرتون تحتوي على 14، و56، و168 قرصًا

قد لا يتم تسويق جميع أحجام العبوات.

 

 

حامل ترخيص التسويق:

AstraZeneca AB

SE‑151 85 Södertälje

السويد

 

الشركة المصنعة:

AstraZeneca AB

Gärtunavägen

SE‑152 57 Södertälje

السويد

 

 

يوليو 2023
 Read this leaflet carefully before you start using this product as it contains important information for you

Brilinta 90 mg film-coated tablets

Each film coated tablet contains 90 mg ticagrelor. For the full list of excipients, see section 6.1.

Film coated tablet (tablet). Round, biconvex, yellow tablets marked with ‘90’ above ‘T’ on one side and plain on the other.

Brilinta, co‑administered with acetylsalicylic acid (ASA), is indicated for the prevention of atherothrombotic events in adult patients with

-      acute coronary syndromes (ACS) or

-      a history of myocardial infarction (MI) and a high risk of developing an atherothrombotic event (see sections 4.2 and 5.1).

 


Posology

 

Patients taking Brilinta should also take a daily low maintenance dose of ASA 75‑150 mg, unless specifically contraindicated.

 

Acute coronary syndromes

Brilinta treatment should be initiated with a single 180 mg loading dose (two tablets of 90 mg) and then continued at 90 mg twice daily.Treatment with Brilinta 90 mg twice daily is recommended for 12 months in ACS patients unless discontinuation is clinically indicated (see section 5.1).  

 

Discontinuation of ASA may be considered after 3 months in patients with ACS who have undergone a percutaneous coronary intervention (PCI) procedure and have an increased risk of bleeding. In that case, ticagrelor as single antiplatelet therapy should be continued for 9 months (see section 4.4).

 

History of myocardial infarction

Brilinta 60 mg twice daily is the recommended dose when an extended treatment is required for patients with a history of MI of at least one year and a high risk of an atherothrombotic event (see section 5.1). Treatment may be started without interruption as continuation therapy after the initial one‑year treatment with Brilinta 90 mg or other adenosine diphosphate (ADP) receptor inhibitor therapy in ACS patients with a high risk of an atherothrombotic event. Treatment can also be initiated up to 2 years from the MI, or within one year after stopping previous ADP receptor inhibitor treatment. There are limited data on the efficacy and safety of ticagrelor beyond 3 years of extended treatment.

 

If a switch is needed, the first dose of Brilinta should be administered 24 hours following the last dose of the other antiplatelet medication.

 

Missed dose

Lapses in therapy should also be avoided. A patient who misses a dose of Brilinta should take only one tablet (their next dose) at its scheduled time.

 

Special populations

Elderly

No dose adjustment is required in elderly (see section 5.2).

 

Renal impairment

No dose adjustment is necessary for patients with renal impairment (see section 5.2).

 

Hepatic impairment

Ticagrelor has not been studied in patients with severe hepatic impairment and its use in these patients is therefore contraindicated (see section 4.3). Only limited information is available in patients with moderate hepatic impairment. Dose adjustment is not recommended, but ticagrelor should be used with caution (see sections 4.4 and 5.2). No dose adjustment is necessary for patients with mild hepatic impairment (see section 5.2).

 

Paediatric population

The safety and efficacy of ticagrelor in children below the age of 18 years have not been established. There is no relevant use of ticagrelor in children with sickle cell disease (see sections 5.1 and 5.2).

 

Method of administration

For oral use.

Brilinta can be administered with or without food.

For patients who are unable to swallow the tablet(s) whole, the tablets can be crushed to a fine powder and mixed in half a glass of water and drunk immediately. The glass should be rinsed with a further half glass of water and the contents drunk. The mixture can also be administered via a nasogastric tube (CH8 or greater). It is important to flush the nasogastric tube through with water after administration of the mixture.

 


• Hypersensitivity to the active substance or to any of the excipients listed in section 6.1 (see section 4.8). • Active pathological bleeding. • History of intracranial haemorrhage (see section 4.8). • Severe hepatic impairment (see sections 4.2, 4.4 and 5.2). • Co administration of ticagrelor with strong CYP3A4 inhibitors (e.g. ketoconazole, clarithromycin, nefazodone, ritonavir and atazanavir), as co administration may lead to a substantial increase in exposure to ticagrelor (see section 4.5).

Bleeding risk

The use of ticagrelor in patients at known increased risk for bleeding should be balanced against the benefit in terms of prevention of atherothrombotic events (see sections 4.8 and 5.1). If clinically indicated, ticagrelor should be used with caution in the following patient groups:

·     Patients with a propensity to bleed (e.g. due to recent trauma, recent surgery, coagulation disorders, active or recent gastrointestinal bleeding) or who are at increased risk of trauma. The use of ticagrelor is contraindicated in patients with active pathological bleeding, in those with a history of intracranial haemorrhage, and in patients with severe hepatic impairment (see section 4.3).

·     Patients with concomitant administration of medicinal products that may increase the risk of bleeding (e.g. non‑steroidal anti‑inflammatory drugs (NSAIDs), oral anticoagulants and/or fibrinolytics) within 24 hours of ticagrelor dosing.

In two randomised controlled studies (TICO and TWILIGHT) in patients with ACS who have undergone a PCI procedure with a drug-eluting stent, discontinuing ASA after 3 months dual antiplatelet therapy with ticagrelor and ASA (DAPT), and continuing with ticagrelor as single antiplatelet therapy (SAPT) for 9 and 12 months, respectively, has been shown to decrease the risk of bleeding with no observed increase in risk of major adverse cardiovascular events (MACE) compared with continued DAPT. The decision to discontinue ASA after 3 months and continue with ticagrelor as single antiplatelet therapy for 9 months in patients with an increased risk of bleeding should be based on clinical judgment considering the risk of bleeding versus the risk of thrombotic events (see section 4.2).

 

Platelet transfusion did not reverse the antiplatelet effect of ticagrelor in healthy volunteers and is unlikely to be of clinical benefit in patients with bleeding. Since co‑administration of ticagrelor with desmopressin did not decrease template‑bleeding time, desmopressin is unlikely to be effective in managing clinical bleeding events (see section 4.5).

 

Antifibrinolytic therapy (aminocaproic acid or tranexamic acid) and/or recombinant factor VIIa therapy may increase haemostasis. Ticagrelor may be resumed after the cause of bleeding has been identified and controlled.

 

Surgery

Patients should be advised to inform physicians and dentists that they are taking ticagrelor before any surgery is scheduled and before any new medicinal product is taken.

 

In PLATO patients undergoing coronary artery bypass grafting (CABG), ticagrelor had more bleeding than clopidogrel when stopped within 1 day prior to surgery but a similar rate of major bleeds compared to clopidogrel after stopping therapy 2 or more days before surgery (see section 4.8). If a patient is to undergo elective surgery and antiplatelet effect is not desired, ticagrelor should be discontinued 5 days prior to surgery (see section 5.1).

 

Patients with prior ischaemic stroke

ACS patients with prior ischaemic stroke can be treated with ticagrelor for up to 12 months (PLATO study).

 

In PEGASUS, patients with history of MI with prior ischaemic stroke were not included. Therefore, in the absence of data, treatment beyond one year is not recommended in these patients.

 

Hepatic impairment

Use of ticagrelor is contraindicated in patients with severe hepatic impairment (see sections 4.2 and 4.3). There is limited experience with ticagrelor in patients with moderate hepatic impairment, therefore, caution is advised in these patients (see sections 4.2 and 5.2).

 

Patients at risk for bradycardic events

Holter ECG monitoring has shown an increased frequency of mostly asymptomatic ventricular pauses during treatment with ticagrelor compared with clopidogrel. Patients with an increased risk of bradycardic events (e.g. patients without a pacemaker who have sick sinus syndrome, 2nd or 3rd degree AV block or bradycardic‑related syncope) have been excluded from the main studies evaluating the safety and efficacy of ticagrelor. Therefore, due to the limited clinical experience, ticagrelor should be used with caution in these patients (see section 5.1).

 

In addition, caution should be exercised when administering ticagrelor concomitantly with medicinal products known to induce bradycardia. However, no evidence of clinically significant adverse reactions was observed in the PLATO trial after concomitant administration with one or more medicinal products known to induce bradycardia (e.g. 96% beta blockers, 33% calcium channel blockers diltiazem and verapamil and 4% digoxin) (see section 4.5).

 

During the Holter substudy in PLATO, more patients had ventricular pauses >3 seconds with ticagrelor than with clopidogrel during the acute phase of their ACS. The increase in Holter‑detected ventricular pauses with ticagrelor was higher in patients with chronic heart failure (CHF) than in the overall study population during the acute phase of ACS, but not at one month with ticagrelor or compared to clopidogrel. There were no adverse clinical consequences associated with this imbalance (including syncope or pacemaker insertion) in this patient population (see section 5.1).

Bradyarrhythmic events and AV blocks have been reported in the post-marketing setting in patients taking ticagrelor (see section 4.8), primarily in patients with ACS, where cardiac ischemia and concomitant drugs reducing the heart rate or affecting cardiac conduction are potential confounders. The patient’s clinical condition and concomitant medication should be assessed as potential causes prior to adjusting treatment.

 

Dyspnoea

Dyspnoea was reported in patients treated with ticagrelor. Dyspnoea is usually mild to moderate in intensity and often resolves without need for treatment discontinuation. Patients with asthma/chronic obstructive pulmonary disease (COPD) may have an increased absolute risk of experiencing dyspnoea with ticagrelor. Ticagrelor should be used with caution in patients with history of asthma and/or COPD. The mechanism has not been elucidated. If a patient reports new, prolonged or worsened dyspnoea this should be investigated fully and if not tolerated, treatment with ticagrelor should be stopped. For further details see section 4.8.

 

Central sleep apnoea

Central sleep apnoea including Cheyne-Stokes respiration has been reported in the post-marketing

setting in patients taking ticagrelor. If central sleep apnoea is suspected, further clinical assessment

should be considered.

 

Creatinine elevations

Creatinine levels may increase during treatment with ticagrelor. The mechanism has not been elucidated. Renal function should be checked according to routine medical practice. In patients with ACS, it is recommended that renal function is also checked one month after initiating the treatment with ticagrelor, paying special attention to patients ≥75 years, patients with moderate/severe renal impairment and those receiving concomitant treatment with an angiotensin receptor blocker (ARB).

 

Uric acid increase

Hyperuricaemia may occur during treatment with ticagrelor (see section 4.8). Caution is advised in patients with history of hyperuricaemia or gouty arthritis. As a precautionary measure, the use of ticagrelor in patients with uric acid nephropathy is discouraged.

 

Thrombotic Thrombocytopenic Purpura (TTP)

Thrombotic Thrombocytopenic Purpura (TTP) has been reported very rarely with the use of ticagrelor. It is characterised by thrombocytopenia and microangiopathic haemolytic anaemia associated with either neurological findings, renal dysfunction or fever. TTP is a potentially fatal condition requiring prompt treatment including plasmapheresis.

 

Interference with platelet function tests to diagnose heparin induced thrombocytopenia (HIT)

In the heparin induced platelet activation (HIPA) test used to diagnose HIT, anti-platelet factor 4/heparin antibodies in patient serum activate platelets of healthy donors in the presence of heparin.
False negative results in a platelet function test (to include, but may not be limited to the HIPA test) for HIT have been reported in patients administered ticagrelor. This is related to inhibition of the P2Y12-receptor on the healthy donor platelets in the test by ticagrelor in the patient’s sera/plasma. Information on concomitant treatment with ticagrelor is required for interpretation of HIT platelet function tests.

In patients who have developed HIT, the benefit-risk of continued treatment with ticagrelor should be assessed, taking both the prothrombotic state of HIT and the increased risk of bleeding with concomitant anticoagulant and ticagrelor treatment into consideration.

 

Other

Based on a relationship observed in PLATO between maintenance ASA dose and relative efficacy of ticagrelor compared to clopidogrel, co‑administration of ticagrelor and high maintenance dose ASA (>300 mg) is not recommended (see section 5.1).

 

Premature discontinuation
Premature discontinuation with any antiplatelet therapy, including Brilinta, could result in an increased risk of cardiovascular (CV) death, MI or stroke due to the patient’s underlying disease. Therefore, premature discontinuation of treatment should be avoided.

 

Sodium

Brilinta contains less than 1 mmol sodium (23 mg) per dose, i.e. is essentially ‘sodium‑free’.

 


Ticagrelor is primarily a CYP3A4 substrate and a mild inhibitor of CYP3A4. Ticagrelor is also a P‑glycoprotein (P‑gp) substrate and a weak P‑gp inhibitor and may increase the exposure of P‑gp substrates.

 

Effects of medicinal and other products on ticagrelor

 

CYP3A4 inhibitors

·     Strong CYP3A4 inhibitors – Co‑administration of ketoconazole with ticagrelor increased the ticagrelor Cmax and AUC equal to 2.4‑fold and 7.3‑fold, respectively. The Cmax and AUC of the active metabolite were reduced by 89% and 56%, respectively. Other strong inhibitors of CYP3A4 (clarithromycin, nefazodone, ritonavir and atazanavir) would be expected to have similar effects and therefore concomitant use of strong CYP3A4 inhibitors with ticagrelor is contraindicated (see section 4.3).

·     Moderate CYP3A4 inhibitors – Co‑administration of diltiazem with ticagrelor increased the ticagrelor Cmax by 69% and AUC to 2.7‑fold and decreased the active metabolite Cmax by 38% and AUC was unchanged. There was no effect of ticagrelor on diltiazem plasma levels. Other moderate CYP3A4 inhibitors (e.g. amprenavir, aprepitant, erythromycin and fluconazole) would be expected to have a similar effect and can as well be co‑administered with ticagrelor.

·     A 2‑fold increase of ticagrelor exposure was observed after daily consumption of large quantities of grapefruit juice (3x200 ml). This magnitude of increased exposure is not expected to be clinically relevant to most patients.

CYP3A inducers

Co‑administration of rifampicin with ticagrelor decreased ticagrelor Cmax and AUC by 73% and 86%, respectively. The Cmax of the active metabolite was unchanged and the AUC was decreased by 46%, respectively. Other CYP3A inducers (e.g. phenytoin, carbamazepine and phenobarbital) would be expected to decrease the exposure to ticagrelor as well. Co‑administration of ticagrelor with potent CYP3A inducers may decrease exposure and efficacy of ticagrelor, therefore, their concomitant use with ticagrelor is discouraged.

 

Cyclosporine (P‑gp and CYP3A inhibitor)

Co‑administration of cyclosporine (600 mg) with ticagrelor increased ticagrelor Cmax and AUC equal to 2.3‑fold and 2.8‑fold, respectively. The AUC of the active metabolite was increased by 32% and Cmax was decreased by 15% in the presence of cyclosporine.

 

No data are available on concomitant use of ticagrelor with other active substances that also are potent P‑gp inhibitors and moderate CYP3A4 inhibitors (e.g. verapamil, quinidine) that also may increase ticagrelor exposure. If the association cannot be avoided, their concomitant use should be made with caution.

 

Others

Clinical pharmacology interaction studies showed that co‑administration of ticagrelor with heparin, enoxaparin and ASA or desmopressin did not have any effect on the pharmacokinetics of ticagrelor or the active metabolite or on ADP‑induced platelet aggregation compared with ticagrelor alone. If clinically indicated, medicinal products that alter haemostasis should be used with caution in combination with ticagrelor.

 

A delayed and decreased exposure to oral P2Y12 inhibitors, including ticagrelor and its active metabolite, has been observed in patients with ACS treated with morphine (35% reduction in ticagrelor exposure). This interaction may be related to reduced gastrointestinal motility and apply to other opioids. The clinical relevance is unknown, but data indicate the potential for reduced ticagrelor efficacy in patients co-administered ticagrelor and morphine. In patients with ACS, in whom morphine cannot be withheld and fast P2Y12 inhibition is deemed crucial, the use of a parenteral P2Y12 inhibitor may be considered.

 

Effects of ticagrelor on other medicinal products

 

Medicinal products metabolised by CYP3A4

·     Simvastatin – Co‑administration of ticagrelor with simvastatin increased simvastatin Cmax by 81% and AUC by 56% and increased simvastatin acid Cmax by 64% and AUC by 52% with some individual increases equal to 2‑ to 3‑fold. Co‑administration of ticagrelor with doses of simvastatin exceeding 40 mg daily could cause adverse reactions of simvastatin and should be weighed against potential benefits. There was no effect of simvastatin on ticagrelor plasma levels. Ticagrelor may have similar effect on lovastatin. The concomitant use of ticagrelor with doses of simvastatin or lovastatin greater than 40 mg is not recommended.

·     Atorvastatin – Co‑administration of atorvastatin and ticagrelor increased atorvastatin acid Cmax by 23% and AUC by 36%. Similar increases in AUC and Cmax were observed for all atorvastatin acid metabolites. These increases are not considered clinically significant.

·     A similar effect on other statins metabolised by CYP3A4 cannot be excluded. Patients in PLATO receiving ticagrelor took a variety of statins, with no concern of an association with statin safety among the 93% of the PLATO cohort taking these medicinal products.

 

Ticagrelor is a mild CYP3A4 inhibitor. Co‑administration of ticagrelor and CYP3A4 substrates with narrow therapeutic indices (i.e. cisapride or ergot alkaloids) is not recommended, as ticagrelor may increase the exposure to these medicinal products.

 

P‑gp substrates (including digoxin, cyclosporine)

Concomitant administration of ticagrelor increased the digoxin Cmax by 75% and AUC by 28%. The mean trough digoxin levels were increased about 30% with ticagrelor co‑administration with some individual maximum increases to 2‑fold. In the presence of digoxin, the Cmax and AUC of ticagrelor and its active metabolite were not affected. Therefore, appropriate clinical and/or laboratory monitoring is recommended when giving narrow therapeutic index P‑gp dependent medicinal products like digoxin concomitantly with ticagrelor.

 

There was no effect of ticagrelor on cyclosporine blood levels. Effect of ticagrelor on other P‑gp substrates has not been studied.

 

Medicinal products metabolised by CYP2C9

Co‑administration of ticagrelor with tolbutamide resulted in no change in the plasma levels of either medicinal product, which suggests that ticagrelor is not a CYP2C9 inhibitor and unlikely to alter the CYP2C9 mediated metabolism of medicinal products like warfarin and tolbutamide.

 

 

 

Oral contraceptives

Co‑administration of ticagrelor and levonorgestrel and ethinyl estradiol increased ethinyl estradiol exposure approximately 20% but did not alter the pharmacokinetics of levonorgestrel. No clinically relevant effect on oral contraceptive efficacy is expected when levonorgestrel and ethinyl estradiol are co‑administered with ticagrelor.

 

Medicinal products known to induce bradycardia

Due to observations of mostly asymptomatic ventricular pauses and bradycardia, caution should be exercised when administering ticagrelor concomitantly with medicinal products known to induce bradycardia (see section 4.4). However, no evidence of clinically significant adverse reactions was observed in the PLATO trial after concomitant administration with one or more medicinal products known to induce bradycardia (e.g. 96% beta blockers, 33% calcium channel blockers diltiazem and verapamil and 4% digoxin).

 

Other concomitant therapy

In clinical studies, ticagrelor was commonly administered with ASA, proton pump inhibitors, statins, beta‑blockers, angiotensin converting enzyme (ACE) inhibitors and angiotensin receptor blockers as needed for concomitant conditions for long‑term and also heparin, low molecular weight heparin and intravenous GpIIb/IIIa inhibitors for short durations (see section 5.1). No evidence of clinically significant adverse interactions with these medicinal products was observed.

 

Co‑administration of ticagrelor with heparin, enoxaparin or desmopressin had no effect on activated partial thromboplastin time (aPTT), activated coagulation time (ACT) or factor Xa assays. However, due to potential pharmacodynamic interactions, caution should be exercised with the concomitant administration of ticagrelor with medicinal products known to alter haemostasis.

 

Due to reports of cutaneous bleeding abnormalities with SSRIs (e.g. paroxetine, sertraline and citalopram), caution is advised when administering SSRIs with ticagrelor as this may increase the risk of bleeding.

 

 


Women of childbearing potential

Women of childbearing potential should use appropriate contraceptive measures to avoid pregnancy during ticagrelor therapy.

 

Pregnancy

There are no or limited amount of data from the use of ticagrelor in pregnant women. Studies in animals have shown reproductive toxicity (see section 5.3). Ticagrelor is not recommended during pregnancy.

 

Breast‑feeding

Available pharmacodynamic/toxicological data in animals have shown excretion of ticagrelor and its active metabolites in milk (see section 5.3). A risk to newborns/infants cannot be excluded. A decision must be made whether to discontinue breast‑feeding or to discontinue/abstain from ticagrelor therapy taking into account the benefit of breast‑feeding for the child and the benefit of therapy for the woman.

 

Fertility

Ticagrelor had no effect on male or female fertility in animals (see section 5.3).

 


Ticagrelor has no or negligible influence on the ability to drive and use machines. During treatment with ticagrelor, dizziness and confusion have been reported. Therefore, patients who experience these symptoms should be cautious while driving or using machines.

 


Summary of the safety profile

The safety profile of ticagrelor has been evaluated in two large phase 3 outcome trials (PLATO and PEGASUS) including more than 39,000 patients (see section 5.1).

 

In PLATO, patients on ticagrelor had a higher incidence of discontinuation due to adverse events than clopidogrel (7.4% vs. 5.4%). In PEGASUS, patients on ticagrelor had a higher incidence of discontinuation due to adverse events compared to ASA therapy alone (16.1% for ticagrelor 60 mg with ASA vs. 8.5% for ASA therapy alone). The most commonly reported adverse reactions in patients treated with ticagrelor were bleeding and dyspnoea (see section 4.4).

 

Tabulated list of adverse reactions

The following adverse reactions have been identified following studies or have been reported in

post‑marketing experience with ticagrelor (Table 1).

 

Adverse reactions are listed by MedDRA System Organ Class (SOC). Within each SOC the adverse reactions are ranked by frequency category. Frequency categories are defined according to the following conventions: Very common (≥1/10), common (≥1/100 to <1/10), uncommon (≥1/1,000 to <1/100), rare (≥1/10,000 to <1/1,000), very rare (<1/10,000), not known (cannot be estimated from the available data).

 

Table 1 – Adverse reactions by frequency and system organ class (SOC)

 

SOC

Very common

 

Common

 

Uncommon

 

Not known

Neoplasms benign, malignant and unspecified (including cysts and polyps)

 

 

Tumour bleedingsa

 

Blood and lymphatic system disorders

Blood disorder bleedingsb

 

 

Thrombotic Thrombocytopenic Purpurac

Immune system disorders

 

 

Hypersensitivity including angioedemac

 

Metabolism and nutrition disorders

Hyperuricaemiad

Gout/Gouty Arthritis

 

 

Psychiatric disorders

 

 

Confusion

 

Nervous system disorders

 

Dizziness,
Syncope, Headache

Intracranial haemorrhagem

 

Eye disorders

 

 

Eye haemorrhagee

 

Ear and labyrinth disorders

 

Vertigo

Ear haemorrhage

 

Cardiac disorders

 

 

 

Bradyarrhythmia, AV blockc

Vascular disorders

 

Hypotension

 

 

Respiratory, thoracic and mediastinal disorders

Dyspnoea

Respiratory system bleedingsf

 

 

 

Gastrointestinal disorders

 

Gastrointestinal haemorrhageg,
Diarrhoea, Nausea, Dyspepsia, Constipation

Retroperitoneal haemorrhage

 

Skin and subcutaneous tissue disorders

 

Subcutaneous or dermal bleedingh, Rash, Pruritus

 

 

Musculoskeletal connective tissue and bone

 

 

Muscular bleedingsi

 

 

Renal and urinary disorders

 

Urinary tract bleedingj

 

 

Reproductive system and breast disorders

 

 

Reproductive system bleedingsk

 

Investigations

 

Blood creatinine increasedd

 

 

Injury, poisoning and procedural complications

 

Post procedural haemorrhage, Traumatic bleedingsl

 

 

a e.g. bleeding from bladder cancer, gastric cancer, colon cancer

b e.g. increased tendency to bruise, spontaneous haematoma, haemorrhagic diathesis

c Identified in post‑marketing experience

d Frequencies derived from lab observations (Uric acid increases to >upper limit of normal from baseline below or within reference range. Creatinine increases of >50% from baseline.) and not crude adverse event report frequency.

e e.g. conjunctival, retinal, intraocular bleeding

f e.g. epistaxis, haemoptysis

g e.g. gingival bleeding, rectal haemorrhage, gastric ulcer haemorrhage

h e.g. ecchymosis, skin haemorrhage, petechiae

i e.g. haemarthrosis, muscle haemorrhage

j e.g. haematuria, cystitis haemorrhagic

k e.g. vaginal haemorrhage, haematospermia, postmenopausal haemorrhage

l e.g. contusion, traumatic haematoma, traumatic haemorrhage

m i.e. spontaneous, procedure related or traumatic intracranial haemorrhage

 

Description of selected adverse reactions

 

Bleeding

Bleeding findings in PLATO

Overall outcome of bleeding rates in the PLATO study are shown in Table 2.

 

Table 2 – Analysis of overall bleeding events, Kaplan‑Meier estimates at 12 months (PLATO)

 

 

Ticagrelor 90 mg
twice daily

N=9235

Clopidogrel

N=9186

 

p‑value*

PLATO Total Major

11.6

11.2

0.4336

PLATO Major Fatal/Life-Threatening

5.8

5.8

0.6988

Non-CABG PLATO Major

4.5

3.8

0.0264

Non-Procedural PLATO Major

3.1

2.3

0.0058

PLATO Total Major + Minor

16.1

14.6

0.0084

Non-Procedural PLATO Major + Minor

5.9

4.3

<0.0001

TIMI-defined Major

7.9

7.7

0.5669

TIMI-defined Major + Minor

11.4

10.9

0.3272

Bleeding category definitions:

Major Fatal/Life-threatening Bleed: Clinically apparent with >50 g/L decrease in haemoglobin or ≥4 red cell units transfused; or fatal; or intracranial; or intrapericardial with cardiac tamponade; or with hypovolaemic shock or severe hypotension requiring pressors or surgery.

Major Other: Clinically apparent with 30‑50 g/L decrease in haemoglobin or 2‑3 red cell units transfused; or significantly disabling.

Minor Bleed: Requires medical intervention to stop or treat bleeding.

TIMI Major Bleed: Clinically apparent with >50 g/L decrease in haemoglobin or intracranial haemorrhage.

TIMI Minor Bleed: Clinically apparent with 30‑50 g/L decrease in haemoglobin.

*p-value calculated from Cox proportional hazards model with treatment group as the only explanatory variable.

 

Ticagrelor and clopidogrel did not differ in rates of PLATO Major Fatal/Life-threatening bleeding, PLATO total Major bleeding, TIMI Major bleeding, or TIMI Minor bleeding (Table 2). However, more PLATO combined Major + Minor bleeding occurred with ticagrelor compared with clopidogrel. Few patients in PLATO had fatal bleeds: 20 (0.2%) for ticagrelor and 23 (0.3%) for clopidogrel (see section 4.4).

 

Age, sex, weight, race, geographic region, concurrent conditions, concomitant therapy and medical history, including a previous stroke or transient ischaemic attack, all did not predict either overall or non-procedural PLATO Major bleeding. Thus, no particular group was identified at risk for any subset of bleeding.

 

CABG-related bleeding:

In PLATO, 42% of the 1584 patients (12% of cohort) who underwent coronary artery bypass graft (CABG) surgery had a PLATO Major Fatal/Life-threatening bleeding with no difference between treatment groups. Fatal CABG bleeding occurred in 6 patients in each treatment group (see section 4.4).

 

Non-CABG related bleeding and non-procedural related bleeding:

Ticagrelor and clopidogrel did not differ in non-CABG PLATO-defined Major Fatal/Life-threatening bleeding, but PLATO-defined Total Major, TIMI Major, and TIMI Major + Minor bleeding were more common with ticagrelor. Similarly, when removing all procedure related bleeds, more bleeding occurred with ticagrelor than with clopidogrel (Table 2). Discontinuation of treatment due to non-procedural bleeding was more common for ticagrelor (2.9%) than for clopidogrel (1.2%; p<0.001).

 

Intracranial bleeding:

There were more intracranial non-procedural bleeds with ticagrelor (n=27 bleeds in 26 patients, 0.3%) than with clopidogrel (n=14 bleeds, 0.2%), of which 11 bleeds with ticagrelor and 1 with clopidogrel were fatal. There was no difference in overall fatal bleeds.

 

Bleeding findings in PEGASUS

Overall outcome of bleeding events in the PEGASUS study are shown in Table 3.

 

Table 3 – Analysis of overall bleeding events, Kaplan‑Meier estimates at 36 months (PEGASUS)

 

 

Ticagrelor 60 mg twice daily + ASA

N=6958

ASA alone

N=6996

 

Safety Endpoints

KM%

Hazard Ratio

(95% CI)

KM%

p‑value

TIMI‑defined bleeding categories

TIMI    Major

2.3

2.32

(1.68, 3.21)

1.1

<0.0001

            Fatal

0.3

1.00

(0.44, 2.27)

0.3

1.0000

            ICH

0.6

1.33

(0.77, 2.31)

0.5

0.3130

            Other TIMI Major

1.6

3.61

(2.31, 5.65)

0.5

<0.0001

TIMI Major or Minor

3.4

2.54

(1.93, 3.35)

1.4

<0.0001

TIMI Major or Minor or Requiring medical attention

16.6

2.64

(2.35, 2.97)

7.0

<0.0001

PLATO‑defined bleeding categories

PLATO Major

3.5

2.57

(1.95, 3.37)

1.4

<0.0001

             Fatal/Life‑threatening

2.4

2.38

(1.73, 3.26)

1.1

<0.0001

             Other PLATO Major

1.1

3.37

(1.95, 5.83)

0.3

<0.0001

PLATO Major or Minor

15.2

2.71

(2.40, 3.08)

6.2

<0.0001

Bleeding category definitions:
TIMI Major: Fatal bleeding, OR any intracranial bleeding, OR clinically overt signs of haemorrhage associated with a drop in haemoglobin (Hgb) of ≥50 g/L, or when Hgb is not available, a fall in haematocrit (Hct) of 15%.

Fatal: A bleeding event that directly led to death within 7 days.

ICH: Intracranial haemorrhage.

Other TIMI Major: Non‑fatal non‑ICH TIMI Major bleeding.

TIMI Minor: Clinically apparent with 30‑50 g/L decrease in haemoglobin.

TIMI Requiring medical attention: Requiring intervention, OR leading to hospitalisation, OR prompting evaluation.

PLATO Major Fatal/life‑threatening: Fatal bleeding, OR any intracranial bleeding, OR intrapericardial with cardiac tamponade, OR with hypovolaemic shock or severe hypotension requiring pressors/inotropes or surgery OR clinically apparent with >50 g/L decrease in haemoglobin or ≥4 red cell units transfused.

PLATO Major Other: Significantly disabling, OR clinically apparent with 30‑50 g/L decrease in haemoglobin, OR 2‑3 red cell units transfused.

PLATO Minor: Requires medical intervention to stop or treat bleeding.

 

In PEGASUS, TIMI Major bleeding for ticagrelor 60 mg twice daily was higher than for ASA alone. No increased bleeding risk was seen for fatal bleeding and only a minor increase was observed in intracranial haemorrhages, as compared to ASA therapy alone. There were few fatal bleeding events in the study, 11 (0.3%) for ticagrelor 60 mg and 12 (0.3%) for ASA therapy alone. The observed increased risk of TIMI Major bleeding with ticagrelor 60 mg was primarily due to a higher frequency of Other TIMI Major bleedings driven by events in the gastrointestinal SOC.

 

Increased bleeding patterns similar to TIMI Major were seen for TIMI Major or Minor and PLATO Major and PLATO Major or Minor bleeding categories (see Table 3). Discontinuation of treatment due to bleeding was more common with ticagrelor 60 mg compared to ASA therapy alone (6.2% and 1.5%, respectively). The majority of these bleedings were of less severity (classified as TIMI Requiring medical attention), e.g. epistaxis, bruising and haematomas.

 

The bleeding profile of ticagrelor 60 mg was consistent across multiple pre‑defined subgroups (e.g. by age, gender, weight, race, geographic region, concurrent conditions, concomitant therapy and medical history) for TIMI Major, TIMI Major or Minor and PLATO Major bleeding events.

 

Intracranial bleeding:

Spontaneous ICHs were reported in similar rates for ticagrelor 60 mg and ASA therapy alone (n=13, 0.2% in both treatment groups). Traumatic and procedural ICHs showed a minor increase with ticagrelor 60 mg treatment, (n=15, 0.2%) compared with ASA therapy alone (n=10, 0.1%). There were 6 fatal ICHs with ticagrelor 60 mg and 5 fatal ICHs with ASA therapy alone. The incidence of intracranial bleeding was low in both treatment groups given the significant comorbidity and CV risk factors of the population under study.

 

Dyspnoea

Dyspnoea, a sensation of breathlessness, is reported by patients treated with ticagrelor. In PLATO, dyspnoea adverse events (AEs) (dyspnoea, dyspnoea at rest, dyspnoea exertional, dyspnoea paroxysmal nocturnal and nocturnal dyspnoea), when combined, was reported by 13.8% of patients treated with ticagrelor and by 7.8% of patients treated with clopidogrel. In 2.2% of patients taking ticagrelor and by 0.6% taking clopidogrel investigators considered the dyspnoea causally related to treatment in the PLATO study and few were serious (0.14% ticagrelor; 0.02% clopidogrel), (see section 4.4). Most reported symptoms of dyspnoea were mild to moderate in intensity, and most were reported as a single episode early after starting treatment.

 

Compared with clopidogrel, patients with asthma/COPD treated with ticagrelor may have an increased risk of experiencing non‑serious dyspnoea (3.29% ticagrelor versus 0.53% clopidogrel) and serious dyspnoea (0.38% ticagrelor versus 0.00% clopidogrel). In absolute terms, this risk was higher than in the overall PLATO population. Ticagrelor should be used with caution in patients with history of asthma and/or COPD (see section 4.4).

 

About 30% of episodes resolved within 7 days. PLATO included patients with baseline congestive heart failure, COPD or asthma; these patients, and the elderly, were more likely to report dyspnoea. For ticagrelor, 0.9% of patients discontinued study drug because of dyspnoea compared with 0.1% taking clopidogrel. The higher incidence of dyspnoea with ticagrelor is not associated with new or worsening heart or lung disease (see section 4.4). Ticagrelor does not affect tests of pulmonary function.

 

In PEGASUS, dyspnoea was reported in 14.2% of patients taking ticagrelor 60 mg twice daily and in 5.5% of patients taking ASA alone. As in PLATO, most reported dyspnoea was mild to moderate in intensity (see section 4.4). Patients who reported dyspnoea tended to be older and more frequently had dyspnoea, COPD or asthma at baseline.

 

Investigations

Uric acid elevations: In PLATO, serum uric acid increased to more than upper limit of normal in 22% of patients receiving ticagrelor compared to 13% of patients receiving clopidogrel. The corresponding numbers in PEGASUS were 9.1%, 8.8% and 5.5% for ticagrelor 90 mg, 60 mg and placebo, respectively. Mean serum uric acid increased approximately 15% with ticagrelor compared to approximately 7.5% with clopidogrel and after treatment was stopped, decreased to approximately 7% on ticagrelor but with no decrease observed for clopidogrel. In PEGASUS, a reversible increase in mean serum uric acid levels of 6.3% and 5.6% was found for ticagrelor 90 mg and 60 mg, respectively, compared to a 1.5% decrease in the placebo group. In PLATO, the frequency of gouty arthritis was 0.2% for ticagrelor vs. 0.1% for clopidogrel. The corresponding numbers for gout/gouty arthritis in PEGASUS were 1.6%, 1.5% and 1.1% for ticagrelor 90 mg, 60 mg and placebo, respectively.

 

 

To report any side effect(s):

  • Saudi Arabia:

 

 

- The National Pharmacovigilance Centre (NPC)

  • Toll free phone: 19999
  • E-mail: npc.drug@sfda.gov.sa  
  • Website: https://ade.sfda.gov.sa/

 

 

  • Other GCC States:

 

-       Please contact the relevant competent authority.

 

 

 


Ticagrelor is well tolerated in single doses up to 900 mg. Gastrointestinal toxicity was dose‑limiting in a single ascending dose study. Other clinically meaningful adverse reactions which may occur with overdose include dyspnoea and ventricular pauses (see section 4.8).

 

In the event of an overdose, the above potential adverse reactions could occur and ECG monitoring should be considered.

 

There is currently no known antidote to reverse the effects of ticagrelor, and ticagrelor is not dialysable (see section 5.2). Treatment of overdose should follow local standard medical practice. The expected effect of excessive ticagrelor dosing is prolonged duration of bleeding risk associated with platelet inhibition. Platelet transfusion is unlikely to be of clinical benefit in patients with bleeding (see section 4.4). If bleeding occurs other appropriate supportive measures should be taken.

 


Pharmacotherapeutic group: Platelet aggregation inhibitors excluding heparin, ATC code: B01AC24

 

Mechanism of action

Brilinta contains ticagrelor, a member of the chemical class cyclopentyltriazolopyrimidines (CPTP), which is an oral, direct acting, selective and reversibly binding P2Y12 receptor antagonist that prevents ADP‑mediated P2Y12 dependent platelet activation and aggregation. Ticagrelor does not prevent ADP binding but when bound to the P2Y12 receptor prevents ADP‑induced signal transduction. Since platelets participate in the initiation and/or evolution of thrombotic complications of atherosclerotic disease, inhibition of platelet function has been shown to reduce the risk of CV events such as death, MI or stroke.

 

Ticagrelor also increases local endogenous adenosine levels by inhibiting the equilibrative nucleoside transporter‑1 (ENT‑1).

 

Ticagrelor has been documented to augment the following adenosine‑induced effects in healthy subjects and in patients with ACS: vasodilation (measured by coronary blood flow increases in healthy volunteers and ACS patients; headache), inhibition of platelet function (in human whole blood in vitro) and dyspnoea. However, a link between the observed increases in adenosine and clinical outcomes (e.g. morbidity‑mortality) has not been clearly elucidated.

 

Pharmacodynamic effects

Onset of action

In patients with stable coronary artery disease (CAD) on ASA, ticagrelor demonstrates a rapid onset of pharmacological effect as demonstrated by a mean inhibition of platelet aggregation (IPA) for ticagrelor at 0.5 hours after 180 mg loading dose of about 41%, with the maximum IPA effect of 89% by 2‑4 hours post dose, and maintained between 2‑8 hours. 90% of patients had final extent IPA>70% by 2 hours post dose.

 

Offset of action

If a CABG procedure is planned, ticagrelor bleeding risk is increased compared to clopidogrel when discontinued within less than 96 hours prior to procedure.

 

Switching data

Switching from clopidogrel 75 mg to ticagrelor 90 mg twice daily results in an absolute IPA increase of 26.4% and switching from ticagrelor to clopidogrel results in an absolute IPA decrease of 24.5%. Patients can be switched from clopidogrel to ticagrelor without any interruption of antiplatelet effect (see section 4.2).

 

Clinical efficacy and safety

The clinical evidence for the efficacy and safety of ticagrelor is derived from two phase 3 trials:

 

·     The PLATO [PLATelet Inhibition and Patient Outcomes] study, a comparison of ticagrelor to clopidogrel, both given in combination with ASA and other standard therapy.

·     The PEGASUS TIMI‑54 [PrEvention with TicaGrelor of SecondAry Thrombotic Events in High‑RiSk AcUte Coronary Syndrome Patients] study, a comparison of ticagrelor combined with ASA to ASA therapy alone.

 

 

 

 

PLATO study (Acute Coronary Syndromes)

 

The PLATO study included 18,624 patients who presented within 24 hours of onset of symptoms of unstable angina (UA), non‑ST elevation myocardial infarction (NSTEMI) or ST elevation myocardial infarction (STEMI), and were initially managed medically, or with percutaneous coronary intervention (PCI), or with CABG.

 

Clinical efficacy

On a background of daily ASA, ticagrelor 90 mg twice daily showed superiority to 75 mg daily clopidogrel in preventing the composite endpoint of CV death, MI or stroke, with the difference driven by CV death and MI. Patients received a 300 mg loading dose of clopidogrel (600 mg possible if having PCI) or 180 mg of ticagrelor.

 

The result appeared early (absolute risk reduction [ARR] 0.6% and relative risk reduction [RRR] of 12% at 30 days), with a constant treatment effect over the entire 12‑month period, yielding ARR 1.9% per year with RRR of 16%. This suggests it is appropriate to treat patients with ticagrelor 90 mg twice daily for 12 months (see section 4.2). Treating 54 ACS patients with ticagrelor instead of clopidogrel will prevent 1 atherothrombotic event; treating 91 will prevent 1 CV death (see Figure 1 and Table 4).

 

The treatment effect of ticagrelor over clopidogrel appears consistent across many subgroups, including weight; sex; medical history of diabetes mellitus, transient ischaemic attack or non‑haemorrhagic stroke, or revascularisation; concomitant therapies including heparins, GpIIb/IIIa inhibitors and proton pump inhibitors (see section 4.5); final index event diagnosis (STEMI, NSTEMI or UA); and treatment pathway intended at randomisation (invasive or medical).

 

A weakly significant treatment interaction was observed with region whereby the hazard ratio (HR) for the primary endpoint favours ticagrelor in the rest of world but favours clopidogrel in North America, which represented approximately 10% of the overall population studied (interaction p‑value=0.045). Exploratory analyses suggest a possible association with ASA dose such that reduced efficacy was observed with ticagrelor with increasing ASA doses. Chronic daily ASA doses to accompany ticagrelor should be 75‑150 mg (see sections 4.2 and 4.4).

 

Figure 1 shows the estimate of the risk to the first occurrence of any event in the composite efficacy endpoint.

 

Figure 1 – Analysis of primary clinical composite endpoint of CV death, MI and stroke (PLATO)

 

Ticagrelor reduced the occurrence of the primary composite endpoint compared to clopidogrel in both the UA/NSTEMI and STEMI population (Table 4). Thus, Brilinta 90 mg twice daily together with low‑dose ASA can be used in patients with ACS (unstable angina, non‑ST elevation Myocardial Infarction [NSTEMI] or ST elevation Myocardial Infarction [STEMI]); including patients managed medically, and those who are managed with percutaneous coronary intervention (PCI) or coronary artery by‑pass grafting (CABG).

 

Table 4 ‑ Analysis of primary and secondary efficacy endpoints (PLATO)

 

 

Ticagrelor 90 mg

twice daily

(% patients with event)

N=9333

Clopidogrel 75 mg
once daily

(% patients with event)

N=9291

ARRa

(%/yr)

RRRa (%)
(95% CI)

p‑value

CV death, MI (excl. silent MI) or stroke

9.3

10.9

1.9

16 (8, 23)

0.0003

Invasive intent

8.5

10.0

1.7

16 (6, 25)

0.0025

Medical intent

11.3

13.2

2.3

15 (0.3, 27)

0.0444d

CV death

3.8

4.8

1.1

21 (9, 31)

0.0013

MI (excl. silent MI)b

5.4

6.4

1.1

16 (5, 25)

0.0045

Stroke

1.3

1.1

‑0.2

‑17 (‑52, 9)

0.2249

All‑cause mortality, MI (excl. silent MI) or stroke

9.7

11.5

2.1

16 (8, 23)

0.0001

CV death, total MI, stroke, SRI, RI, TIA or other ATEc

13.8

15.7

2.1

12 (5, 19)

0.0006

All‑cause mortality

4.3

5.4

1.4

22 (11, 31)

0.0003d

Definite stent thrombosis

1.2

1.7

0.6

32 (8, 49)

0.0123d

a ARR = absolute risk reduction; RRR = relative risk reduction = (1‑Hazard ratio) x 100%. A negative RRR indicates a relative risk increase.

b Excluding silent MI.

c SRI = serious recurrent ischaemia; RI = recurrent ischaemia; TIA = transient ischaemic attack; ATE = arterial thrombotic event. Total MI includes silent MI, with date of event set to date when discovered.

d Nominal significance value; all others are formally statistically significant by pre‑defined hierarchical testing.

 

PLATO genetic substudy

CYP2C19 and ABCB1 genotyping of 10,285 patients in PLATO provided associations of genotype groups with PLATO outcomes. The superiority of ticagrelor over clopidogrel in reducing major CV events was not significantly affected by patient CYP2C19 or ABCB1 genotype. Similar to the overall PLATO study, total PLATO Major bleeding did not differ between ticagrelor and clopidogrel, regardless of CYP2C19 or ABCB1 genotype. Non‑CABG PLATO Major bleeding was increased with ticagrelor compared clopidogrel in patients with one or more CYP2C19 loss of function alleles, but similar to clopidogrel in patients with no loss of function allele.

 

Combined efficacy and safety composite

A combined efficacy and safety composite (CV death, MI, stroke or PLATO‑defined ‘Total Major’ bleeding) indicates that the benefit in efficacy of ticagrelor compared to clopidogrel is not offset by the major bleeding events (ARR 1.4%, RRR 8%, HR 0.92; p=0.0257) over 12 months after ACS.

 

Clinical safety

 

Holter sub-study:

To study the occurrence of ventricular pauses and other arrhythmic episodes during PLATO, investigators performed Holter monitoring in a subset of nearly 3000 patients, of whom approximately 2000 had recordings both in the acute phase of their ACS and after one month. The primary variable of interest was the occurrence of ventricular pauses ≥3 seconds. More patients had ventricular pauses with ticagrelor (6.0%) than with clopidogrel (3.5%) in the acute phase; and 2.2% and 1.6%, respectively, after 1 month (see section 4.4). The increase in ventricular pauses in the acute phase of ACS was more pronounced in ticagrelor patients with history of CHF (9.2% versus 5.4% in patients without CHF history; for clopidogrel patients, 4.0% in those with versus 3.6% in those without CHF history). This imbalance did not occur at one month: 2.0% versus 2.1% for ticagrelor patients with and without CHF history, respectively; and 3.8% versus 1.4% with clopidogrel. There were no adverse clinical consequences associated with this imbalance (including pacemaker insertions) in this population of patients.

 

PEGASUS study (History of Myocardial Infarction)

 

The PEGASUS TIMI‑54 study was a 21,162 patient, event‑driven, randomized, double‑blind, placebo‑controlled, parallel group, international multicenter study to assess the prevention of atherothrombotic events with ticagrelor given at 2 doses (either 90 mg twice daily or 60 mg twice daily) combined with low dose ASA (75‑150 mg), compared to ASA therapy alone in patients with history of MI and additional risk factors for atherothrombosis.

 

Patients were eligible to participate if they were aged 50 years or over, with a history of MI (1 to 3 years prior to randomization) and had at least one of the following risk factors for atherothrombosis: age ≥65 years, diabetes mellitus requiring medication, a second prior MI, evidence of multivessel CAD or chronic non‑end‑stage renal dysfunction.

 

Patients were ineligible if there was planned use of a P2Y12 receptor antagonist, dipyridamole, cilostazol, or anticoagulant therapy during the study period; if they had a bleeding disorder or a history of an ischemic stroke or intracranial bleeding, a central nervous system tumour or an intracranial vascular abnormality; if they had had gastrointestinal bleeding within the previous 6 months or major surgery within the previous 30 days.

 

Clinical efficacy

Figure 2 ‑ Analysis of primary clinical composite endpoint of CV death, MI and stroke (PEGASUS)

Table 5 ‑ Analysis of primary and secondary efficacy endpoints (PEGASUS)

 

 

Ticagrelor 60 mg twice daily +ASA
N = 7045

ASA alone
N = 7067

p‑value

Characteristic

Patients with events

KM %

HR
(95% CI)

Patients with events

KM %

Primary endpoint

Composite of CV Death/MI/Stroke

487 (6.9%)

7.8%

0.84
(0.74, 0.95)

578 (8.2%)

9.0%

0.0043 (s)

CV death

174 (2.5%)

2.9%

0.83
(0.68, 1.01)

210 (3.0%)

3.4%

0.0676

MI

285 (4.0%)

4.5%

0.84
(0.72, 0.98)

338 (4.8%)

5.2%

0.0314

Stroke

91 (1.3%)

1.5%

0.75
(0.57, 0.98)

122 (1.7%)

1.9%

0.0337

Secondary endpoint

CV death

174 (2.5%)

2.9%

0.83
(0.68, 1.01)

210 (3.0%)

3.4%

All‑cause mortality

289 (4.1%)

4.7%

0.89

(0.76, 1.04)

326 (4.6%)

5.2%

Hazard ratio and p‑values are calculated separately for ticagrelor vs. ASA therapy alone from Cox proportional hazards model with treatment group as the only explanatory variable.

KM percentage calculated at 36 months.

Note: the number of first events for the component’s CV death, MI and stroke are the actual number of first events for each component and do not add up to the number of events in the composite endpoint

(s) Indicates statistical significance.

CI = Confidence interval; CV = Cardiovascular; HR = Hazard ratio; KM = Kaplan‑Meier; MI = Myocardial infarction; N = Number of patients.

 

Both 60 mg twice daily and 90 mg twice daily regimens of ticagrelor in combination with ASA were superior to ASA alone in the prevention of atherothrombotic events (composite endpoint: CV death, MI and stroke), with a consistent treatment effect over the entire study period, yielding a 16% RRR and 1.27% ARR for ticagrelor 60 mg and a 15% RRR and 1.19% ARR for ticagrelor 90 mg.

 

Although the efficacy profile of 90 mg and 60 mg were similar, there is evidence that the lower dose has a better tolerability and safety profile in relation to risk of the bleeding and dyspnoea. Therefore, only Brilinta 60 mg twice daily co‑administered with ASA is recommended for the prevention atherothrombotic events (CV death, MI and stroke) in patients with a history of MI and a high risk of developing an atherothrombotic event.

 

Relative to ASA alone, ticagrelor 60 mg twice daily significantly reduced the primary composite endpoint of CV death, MI and stroke. Each of the components contributed to the reduction in the primary composite endpoint (CV death 17% RRR, MI 16% RRR and stroke 25% RRR).

 

The RRR for the composite endpoint from 1 to 360 days (17% RRR) and from 361 days and onwards (16% RRR) was similar. There are limited data on the efficacy and safety of ticagrelor beyond 3 years of extended treatment.

 

There was no evidence of benefit (no reduction in the primary composite endpoint of CV death, MI and stroke, but an increase in major bleeding) when ticagrelor 60 mg twice daily was introduced in clinically stable patients >2 years from the MI, or more than one year after stopping previous ADP receptor inhibitor treatment (see also section 4.2).

 

Clinical safety

The rate of discontinuations with ticagrelor 60 mg due to bleeding and dyspnoea was higher in patients >75 years (42%) than in younger patients (range: 23‑31%), with a difference versus placebo higher than 10% (42% vs. 29%) in patients >75 years.

 

Paediatric population

In a randomised, double-blind, parallel-group Phase III study (HESTIA 3), 193 paediatric patients (ages 2 to less than 18 years) with sickle cell disease were randomised to receive either placebo or ticagrelor at doses of 15 mg to 45 mg twice daily depending on body weight. Ticagrelor resulted in a median platelet inhibition of 35% at pre-dose and 56% at 2 hours post-dose at steady state.

 

Compared to placebo, there was no treatment benefit of ticagrelor on the rate of vaso-occlusive crises.

 

The European Medicines Agency has waived the obligation to submit the results of studies with Brilinta in all subsets of the paediatric population in acute coronary syndromes (ACS) and history of myocardial infarction (MI) (see section 4.2 for information on paediatric use).

 


Ticagrelor demonstrates linear pharmacokinetics and exposure to ticagrelor and the active metabolite (AR‑C124910XX) are approximately dose proportional up to 1260 mg.

 

Absorption

Absorption of ticagrelor is rapid with a median tmax of approximately 1.5 hours. The formation of the major circulating metabolite AR‑C124910XX (also active) from ticagrelor is rapid with a median tmax of approximately 2.5 hours. Following an oral ticagrelor 90 mg single dose under fasted conditions in healthy subjects, Cmax is 529 ng/ml and AUC is 3451 ng*h/ml. The metabolite parent ratios are 0.28 for Cmax and 0.42 for AUC. The pharmacokinetics of ticagrelor and AR‑C124910XX in patients with a history of MI were generally similar to that in the ACS population. Based on a population pharmacokinetic analysis of the PEGASUS study the median ticagrelor Cmax was 391 ng/ml and AUC were 3801 ng*h/ml at steady state for ticagrelor 60 mg. For ticagrelor 90 mg Cmax was 627 ng/ml and AUC were 6255 ng*h/ml at steady state.

 

The mean absolute bioavailability of ticagrelor was estimated to be 36%. Ingestion of a high‑fat meal resulted in a 21% increase in ticagrelor AUC and 22% decrease in the active metabolite Cmax but had no effect on ticagrelor Cmax or the AUC of the active metabolite. These small changes are considered of minimal clinical significance; therefore, ticagrelor can be given with or without food. Ticagrelor as well as the active metabolite are P‑gp substrates.

 

Ticagrelor as crushed tablets mixed in water, given orally or administered through a nasogastric tube into the stomach, has a comparable bioavailability to whole tablets with regards to AUC and Cmax for ticagrelor and the active metabolite. Initial exposure (0.5- and 1-hour post‑dose) from crushed ticagrelor tablets mixed in water was higher compared to whole tablets, with a generally identical concentration profile thereafter (2 to 48 hours).

 

Distribution

The steady state volume of distribution of ticagrelor is 87.5 l. Ticagrelor and the active metabolite is extensively bound to human plasma protein (>99.0%).

 

Biotransformation

CYP3A4 is the major enzyme responsible for ticagrelor metabolism and the formation of the active metabolite and their interactions with other CYP3A substrates ranges from activation through to inhibition.

 

The major metabolite of ticagrelor is AR‑C124910XX, which is also active as assessed by in vitro binding to the platelet P2Y12 ADP‑receptor. The systemic exposure to the active metabolite is approximately 30‑40% of that obtained for ticagrelor.

 

Elimination

The primary route of ticagrelor elimination is via hepatic metabolism. When radiolabelled ticagrelor is administered, the mean recovery of radioactivity is approximately 84% (57.8% in faeces, 26.5% in urine). Recoveries of ticagrelor and the active metabolite in urine were both less than 1% of the dose. The primary route of elimination for the active metabolite is most likely via biliary secretion. The mean t1/2 was approximately 7 hours for ticagrelor and 8.5 hours for the active metabolite.

 

Special populations

 

Elderly

Higher exposures to ticagrelor (approximately 25% for both Cmax and AUC) and the active metabolite were observed in elderly (≥75years) ACS patients compared to younger patients by the population pharmacokinetic analysis. These differences are not considered clinically significant (see section 4.2).

 

Paediatric population

Limited data are available in children with sickle cell disease (see sections 4.2 and 5.1).

 

In the HESTIA 3 study, patients aged 2 to less than 18 years weighing ≥ 12 to ≤ 24 kg, > 24 to ≤ 48 kg and > 48 kg, were administered ticagrelor as paediatric dispersible 15 mg tablets at doses of respectively 15, 30 and 45 mg twice daily. Based on population pharmacokinetic analysis, the mean AUC ranged from 1095 ng*h/mL to 1458 ng*h/mL and the mean Cmax ranged from 143 ng/mL to 206 ng/mL at steady state.

 

Gender

Higher exposures to ticagrelor and the active metabolite were observed in women compared to men. These differences are not considered clinically significant.

 

Renal impairment

Exposure to ticagrelor was approximately 20% lower and exposure to the active metabolite was approximately 17% higher in patients with severe renal impairment (creatinine clearance <30 ml/min) compared to subjects with normal renal function.

 

In patients with end stage renal disease on haemodialysis AUC and Cmax of ticagrelor 90 mg administered on a day without dialysis were 38% and 51% higher compared to subjects with normal renal function. A similar increase in exposure was observed when ticagrelor was administered immediately prior to dialysis (49% and 61%, respectively) showing that ticagrelor is not dialysable. Exposure of the active metabolite increased to a lesser extent (AUC 13‑14% and Cmax 17‑36%). The inhibition of platelet (IPA) effect of  ticagrelor was independent of dialysis in patients with end stage renal disease and similar to subjects with normal renal function (see section 4.2).

 

Hepatic impairment

Cmax and AUC for ticagrelor were 12% and 23% higher in patients with mild hepatic impairment compared to matched healthy subjects, respectively, however, the IPA effect of ticagrelor was similar between the two groups. No dose adjustment is needed for patients with mild hepatic impairment. Ticagrelor has not been studied in patients with severe hepatic impairment and there is no pharmacokinetic information in patients with moderate hepatic impairment. In patients that had moderate or severe elevation in one or more liver function tests at baseline, ticagrelor plasma concentrations were on average similar or slightly higher as compared to those without baseline elevations. No dose adjustment is recommended in patients with moderate hepatic impairment (see sections 4.2 and 4.4).

 

Ethnicity

Patients of Asian descent have a 39% higher mean bioavailability compared to Caucasian patients. Patients’ self‑identified as black had an 18% lower bioavailability of ticagrelor compared to Caucasian patients, in clinical pharmacology studies, the exposure (Cmax and AUC) to ticagrelor in Japanese subjects was approximately 40% (20% after adjusting for body weight) higher compared to that in Caucasians. The exposure in patient’s self‑identified as Hispanic or Latino was similar to that in Caucasians.

 


Preclinical data for ticagrelor and its major metabolite have not demonstrated unacceptable risk for adverse effects for humans based on conventional studies of safety pharmacology, single and repeated dose toxicity and genotoxic potential.

 

Gastrointestinal irritation was observed in several animal species at clinical relevant exposure levels (see section 4.8).

 

In female rats, ticagrelor at high dose showed an increased incidence of uterine tumours (adenocarcinomas) and an increased incidence of hepatic adenomas. The mechanism for uterine tumours is likely hormonal imbalance which can lead to tumours in rats. The mechanism for the hepatic adenomas is likely due to a rodent‑specific enzyme induction in the liver. Thus, the carcinogenicity findings are considered unlikely to be relevant for humans.

 

In rats, minor developmental anomalies were seen at a maternal toxic dose (safety margin of 5.1). In rabbits, a slight delay in hepatic maturity and skeletal development was seen in foetuses from dams at high dose without showing maternal toxicity (safety margin of 4.5).

 

Studies in rats and rabbits have shown reproductive toxicity, with slightly reduced maternal body weight gain and reduced neonatal viability and birth weight, with delayed growth. Ticagrelor produced irregular cycles (mostly extended cycles) in female rats, but did not affect overall fertility in male and female rats. Pharmacokinetic studies performed with radiolabelled ticagrelor have shown that the parent compound and its metabolites are excreted in the milk of rats (see section 4.6).

 


Mannitol 126 mg

Magnesium stearate  3 mg

Sodium starch glycolate 9 mg

Hydroxypropylcellulose (E463) 9 mg

Talc 1 mg

Titanium dioxide (E171) 1.7 mg

Ferric oxide yellow 0.1 mg 

Polyethylene glycol 400 (0.6 mg)

HydroxyPropyl MethylCellulose 5.6 mg

Dibasic calcium phosphate 63 mg


Not applicable.


3 years

This medicinal product does not require any special storage conditions.


 

·       PVC‑PVDC/Al transparent blister (with sun/moon symbols) of 10 tablets; cartons of 60 tablets (6 blisters) and 180 tablets (18 blisters).

·       PVC‑PVDC/Al transparent calendar blister (with sun/moon symbols) of 14 tablets; cartons of 14 tablets (1 blister), 56 tablets (4 blisters) and 168 tablets (12 blisters).

·       PVC‑PVDC/Al perforated unit dose transparent blister of 10 tablets; cartons of 100x1 tablets (10 blisters).

 

Not all pack sizes may be marketed.

 

 


Any unused medicinal product or waste material should be disposed of in accordance with local requirements.

 


AstraZeneca AB SE 151 85 Södertälje, Sweden

March 2024
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