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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)

a) What Cupido is:

Cupido contains clopidogrel and belongs to a group of medicines called antiplatelet medicinal products. Platelets are very small structures in the blood which clump together during blood clotting. By preventing this clumping, antiplatelet medicinal products reduce the chances of blood clots forming (a process called thrombosis).

 

b) What it is taken for:

Cupido is taken by adults to prevent blood clots (thrombi) forming in hardened blood vessels (arteries), a process known as atherothrombosis, which can lead to atherothrombotic events (such as stroke, heart attack, or death). You have been prescribed Cupido to help prevent blood clots and reduce the risk of these severe events because:

  • You have a condition of hardening of arteries (also known as atherosclerosis), and
  • You have previously experienced a heart attack, stroke or have a condition known as peripheral arterial disease, or
  • You have experienced a severe type of chest pain known as ‘unstable angina’ or ‘myocardial infarction’ (heart attack). For the treatment of this condition your doctor may have placed a stent in the blocked or narrowed artery to restore effective blood flow. You should also be given acetylsalicylic acid (a substance present in many medicines used to relieve pain and lower fever as well as to prevent blood clotting) by your doctor.
  • You have an irregular heartbeat, a condition called ‘atrial fibrillation’, and you cannot take medicines known as ‘oral anticoagulants’ (vitamin K antagonists) which prevent new clots from forming and prevent existing clots from growing. You should have been told that ‘oral anticoagulants’ are more effective than acetylsalicylic acid or the combined use of Cupido and acetylsalicylic acid for this condition. Your doctor should have prescribed Cupido plus acetylsalicylic acid if you cannot take ‘oral anticoagulants’ and you do not have a risk of major bleeding.

a) Do not take Cupido if you:

  • If you are allergic (hypersensitive) to clopidogrel or any of the other ingredients of this medicine (listed in section 6).
  • If you have a medical condition that is currently causing bleeding such as a stomach ulcer or bleeding within the brain.
  • If you suffer from severe liver disease.

If you think any of these apply to you, or if you are in any doubt at all, consult your doctor before taking Cupido

 

b) Warnings and precaution:

If any of the situations mentioned below apply to you, you should tell your doctor before taking Cupido:

  • if you have a risk of bleeding such as
    • a medical condition that puts you at risk of internal bleeding (such as a stomach ulcer).
    • a blood disorder that makes you prone to internal bleeding (bleeding inside any tissues, organs or joints of your body).
    • a recent serious injury.
    • a recent surgery (including dental).
    • a planned surgery (including dental) in the next seven days.
  • if you have had a clot in an artery of your brain (ischemic stroke) which occurred within the last seven days.
  •  if you have kidney or liver disease.
  • if you have had an allergy or reaction to any medicine used to treat your disease.

 

c) While you are taking Cupido:

  • You should tell your doctor if a surgery (including dental) is planned.
  • You should also tell your doctor immediately if you develop a medical condition (also known as Thrombotic Thrombocytopenic Purpura or TTP) that includes fever and bruising under the skin that may appear as red pinpoint dots, with or without unexplained extreme tiredness, confusion, yellowing of the skin or eyes (jaundice) (see section 4 ‘Possible side effects’).
  • If you cut or injure yourself, it may take longer than usual for bleeding to stop. This is linked to the way your medicine works as it prevents the ability of blood clots to form. For minor cuts and injuries e.g., cutting yourself, shaving, this is usually of no concern. However, if you are concerned by your bleeding, you should contact your doctor straightaway (see section 4 ‘Possible side effects’).
  • Your doctor may order blood tests.

 

d) Children and adolescents:

Do not give this medicine to children because it does not work.

 

e) Taking Cupido with other medicines, herbal or dietary supplements:

Tell your doctor or pharmacist if you are taking, have recently taken or might take any other medicines, including medicines obtained without a prescription.

Some other medicines may influence the use of Cupido or vice versa.

 

You should specifically tell your doctor if you take:

  • medicines that may increase your risk of bleeding such as:
    • oral anticoagulants, medicines used to reduce blood clotting,
    • a non‐steroidal anti‐inflammatory medicine, usually used to treat painful and/or inflammatory conditions of muscle or joints,
    • heparin or any other injectable medicine used to reduce blood clotting,
    • ticlopidine, other antiplatelet agent,
    • a selective serotonin reuptake inhibitor (including but not restricted to fluoxetine or fluvoxamine), medicines usually used to treat depression,
  • omeprazole or esomeprazole, medicines to treat upset stomach,
  • fluconazole or voriconazole, medicines to treat fungal infections,
  • efavirenz, a medicine to treat HIV (human immunodeficiency virus) infections,
  • carbamazepine, a medicine to treat some forms of epilepsy,
  • moclobemide, medicine to treat depression,
  • repaglinide, medicine to treat diabetes,
  • paclitaxel, medicine to treat cancer.

If you have experienced severe chest pain (unstable angina or heart attack), you may be prescribed Cupido in combination with acetylsalicylic acid, a substance present in many medicines used to relieve pain and lower fever. An occasional use of acetylsalicylic acid (no more than 1,000 mg in any 24 hour period) should generally not cause a problem, but prolonged use in other circumstances should be discussed with your doctor.

 

f) Cupido with food and drink:

Cupido may be taken with or without food.

 

g) Pregnancy and breast‐feeding:

It is preferable not to take this product during pregnancy.

If you are pregnant or suspect that you are pregnant, you should tell your doctor or your pharmacist before taking Cupido. If you become pregnant while taking Cupido, consult your doctor immediately as it is recommended not to take clopidogrel while you are pregnant.

You should not breast‐feed while taking this medicine.

If you are breast‐feeding or planning to breast‐feed, talk to your doctor before taking this medicine.

Ask your doctor or pharmacist for advice before taking any medicine.

 

h) Driving and using machines:

Cupido is unlikely to affect your ability to drive or to use machines.

 

Cupido contains lactose

If you have been told by your doctor that you have an intolerance to some sugars (e.g. lactose),

contact your doctor before taking this medicine.

 

Cupido contains hydrogenated castor oil

This may cause stomach upset or diarrhea


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

 

a) How much Cupido to take:

The recommended dose, including for patients with a condition called ‘atrial fibrillation’ (an irregular heartbeat), is one 75 mg tablet of Cupido per day to be taken orally with or without food, and at the same time each day.

If you have experienced severe chest pain (unstable angina or heart attack), your doctor may give you 300 mg of Cupido (1 tablet of 300 mg or 4 tablets of 75 mg) once at the start of treatment. Then, the recommended dose is one 75 mg tablet of Cupido per day as described above.

You should take Cupido for as long as your doctor continues to prescribe it.

 

b) If you take more Cupido than should (overdose):

Contact your doctor or the nearest hospital emergency department because of the increased risk of bleeding.

 

c) If you forget to take Cupido:

If you forget to take a dose of Cupido, but remember within 12 hours of your usual time, take your tablet straightaway and then take your next tablet at the usual time.

If you forget for more than 12 hours, simply take the next single dose at the usual time. Do not take a double dose to make up for a forgotten tablet.

For the 7, 14, 28 and 84 tablets pack sizes, you can check the day on which you last took a tablet of Cupido by referring to the calendar printed on the blister.

 

d)  If you stop taking Cupido:

Do not stop the treatment unless your doctor tells you so. Contact your doctor or pharmacist before stopping.

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.

Contact your doctor immediately if you experience:

  • fever, signs of infection or extreme tiredness. These may be due to rare decrease of some blood cells.
  • signs of liver problems such as yellowing of the skin and/or the eyes (jaundice), whether or not associated with bleeding which appears under the skin as red pinpoint dots and/or confusion (see section 2 ‘Warnings and precautions’).
  • swelling in the mouth or skin disorders such as rashes and itching, blisters of the skin. These may be the signs of an allergic reaction.

 

The most common side effect reported with Cupido is bleeding.

Bleeding may occur as bleeding in the stomach or bowels, bruising, hematoma (unusual bleeding or bruising under the skin), nose bleed, blood in the urine. In a small number of cases, bleeding in the eye, inside the head, the lung or the joints has also been reported.

 

If you experience prolonged bleeding when taking Cupido

If you cut or injure yourself, it may take longer than usual for bleeding to stop. This is linked to the way your medicine works as it prevents the ability of blood clots to form. For minor cuts and injuries e.g., cutting yourself, shaving, this is usually of no concern. However, if you are concerned by your bleeding, you should contact your doctor straightaway (see section 2 ‘Warnings and precautions’).

 

Other side effects include:

Common side effects (may affect up to 1 in 10 people):

Diarrhea, abdominal pain, indigestion or heartburn.

 

Uncommon side effects (may affect up to 1 in 100 people):

Headache, stomach ulcer, vomiting, nausea, constipation, excessive gas in stomach or intestines, rashes, itching, dizziness, sensation of tingling and numbness.

 

Rare side effect (may affect up to 1 in 1000 people):

Vertigo, enlarged breasts in males.

 

Very rare side effects (may affect up to 1 in 10,000 people):

Jaundice; severe abdominal pain with or without back pain; fever, breathing difficulties sometimes associated with cough; generalized allergic reactions (for example, overall sensation of heat with sudden general discomfort until fainting); swelling in the mouth; blisters of the skin; skin allergy; sore mouth (stomatitis); decrease in blood pressure; confusion; hallucinations; joint pain; muscular pain; changes in taste or loss of taste of food.

 

Side effects with frequency not known (frequency cannot be estimated from the available data): Hypersensitivity reactions with chest or abdominal pain, persistent low blood sugar symptoms. Insulin Autoimmune Syndrome, which can lead to severe hypoglycemia, particularly in patients with HLA DRA4 subtype (more frequent in the Japanese population).

 

In addition, your doctor may identify changes in your blood or urine test results.


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 carton and on the blister, after EXP . The expiry date refers to the last day of that month.

Store below 30°C.

Do not use this medicine if you notice any visible sign of deterioration.

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


a) What the medicinal ingredient is:

The active substance is clopidogrel. Each tablet contains 75 mg of clopidogrel (as hydrogen sulphate).

 

b) What the non-medicinal ingredients are:

The other ingredients are (see section 2 ‘Cupido contains lactose’ and ‘Cupido contains hydrogenated castor oil’):

  • Tablet core: mannitol (E421), hydrogenated castor oil, microcrystalline cellulose, macrogol 6000 and low‐substituted hydroxypropylcellulose,
  • Tablet coating: lactose monohydrate (milk sugar), hypromellose (E464), triacetin (E1518), red iron oxide (E172) and titanium dioxide (E171),
  • Polishing agent: carnauba wax.

Cupido 75 mg: Each pink, round, biconvex, film-coated tablet engraved with “CL” over "75" on one side and "APO" on the other side contains clopidogrel bisulfate equivalent to 75 mg clopidogrel. Available in blisters of 30 tablets.

Apotex Incorporated

150 Signet Drive Toronto, Ontario Canada, M9L 1T9

Tel: 1-800-268-4623, Fax: 1-800-609-9444

www.apotex.com


This leaflet was last revised on 03/2019
  نشرة الدواء تحت مراجعة الهيئة العامة للغذاء والدواء (اقرأ هذه النشرة بعناية قبل البدء في استخدام هذا المنتج لأنه يحتوي على معلومات مهمة لك)

أ- ما هو كيوبيدو؟

يحتوي كيوبيدو على كلوبيدوجريل، وينتمي إلى مجموعة من الأدوية تسمى المنتجات الدوائية المضادة للصفيحات. الصفائح الدموية هي
هياكل صغيرة جدًّا في الدم تتجمع معًا من خلال تخثر الدم. وعن طريق منع هذا التكتل، تعمل المنتجات الدوائية المضادة للصفيحات على التقليل من فرص تشكيل جلطات الدم، وهي عملية تسمى تخثر الدم.

 

ب- فيم يُستخدم؟

يتناول البالغون كيوبيدو لمنع تكون جلطات الدم (تخثر الدم) في الأوعية الدموية (الشرايين) المتصلبة، التي قد ينتج عنها تجلط الأوعية الدموية (مثل السكتة الدماغية، والنوبات القلبية، أو الموت). لقد وصف لك كوبيدو
للمساعدة على منع تخثر الدم وللتقليل من خطر هذه الحالات الخطيرة لأنك:

  • تعاني من وجود شرايين متصلبة.
  • عانيت في السابق من نوبة قلبية أو سكتة دماغية، أو تعاني من حالة تعرف باسم مرض الشرايين الطرفية.
  • عانيت من نوع خطير من ألم الصدر يُعرف بإسم الذبحة الصدرية غير المستقرة  أو احتشاء عضلة القلب (نوبة قلبية). لعلاج هذه الحالة، قد يضع طبيبك دعامة في الشريان المسدود أو الضيق لاستعادة تدفق الدم الفعال. ينبغي على الطبيب إعطاؤك حمض خلي الصفصافي «أسبرين» (مادة موجودة في العديد من الأدوية المستخدمة لتخفيف الألم وخفض الحمى، وكذلك لمنع تخثر الدم).
  • تعاني من عدم انتظام ضربات القلب، وهي حالة تسمى بالرجفان الأذيني، ولا يمكنك تناول الأدوية المعروفة بإسم مضادات التخثر الفموية» (مضادات فيتامين ك)، أو التي تمنع تشكل جلطات جديدة، كما تمنع نمو الجلطات الموجودة. وينبغي إبلاغك أن «مضادات التخثر الفموية» تُعد أكثر فعالية من حمض خلي الصفصافي أو الجمع بين استخدام كيوبيدو و حمض خلي الصفصافي لهذه الحالة. ينبغي أن يصف لك الطبيب كيوبيدو بالإضافة إلى حمض خلي الصفصافي، إذا كنت لا تستطيع تناول ‹مضادات التخثر الشفوية› ولم تكن مُعرضًا لخطر النزيف الحاد.
     

أ- لا تتناول كيوبيدو:

  • إذا كان لديك حساسية (فرط التحسس) من كلوبيدوجريل، أو أي من المكونات الأخرى لهذا الدواء المحددة في القسم 6.
  • إذا كنت تعاني من حالة صحية تسبب لك نزيف في الوقت الحالي مثل قرحة المعدة أو نزيف في الدماغ.
  • إذا كنت تعاني من مرض حاد في الكبد.
  • إذا كنت تعتقد أن أي من هذه الحالات تنطبق عليك، أو كان لديك أي شك على الإطلاق، فاستشر الطبيب قبل تناول كيوبيدو.

 

ب- الاحتياطات والتحذيرات:

إذا كانت أي من الحالات المذكورة أدناه تنطبق عليك، فيجب عليك أن تخبر الطبيب قبل تناول كيوبيدو:

  • إذا كنت معرضًا لخطر نزيف، مثل:
    • حالة طبية تُعرضك لخطر النزيف الداخلي (مثل قرحة المعدة).
    • اضطراب في الدم يجعلك عرضة لنزيف داخلي (نزيف داخل أي أنسجة أو أعضاء أو مفاصل الجسم).
    • التعرض لإصابة خطيرة مؤخراً.
    • الخضوع لعملية جراحية مؤخراً (بما في ذلك جراحة الأسنان). 
    • خططت للخضوع لعملية جراحية (بما في ذلك جراحة الأسنان) في الأيام السبعة المقبلة.
  • إذا كان لديك تجلط في شريان الدماغ (السكتة الإقفارية) حدثت خلال الأيام السبعة الماضية.
  • إذا كان لديك مرض في الكلى أو الكبد.
  • إذا كان لديك حساسية أو رد فعل عكسي ضد أي دواء يُستخدم لعلاج مرضك.

 

ج- أثناء تناولك لدواء كيوبيدو:

  • ينبغي إخبار الطبيب إذا تم التخطيط لعملية جراحية (بما في ذلك جراحة الأسنان).
  • كما ينبغي عليك إخبار الطبيب على الفور إذا عانيت من حالة صحية تُعرف أيضاً بإسم فرفرية نقص الصفيحات التخثرية (TTP) التي تشمل الحمى وكدمات تحت الجلد التي قد تظهر كنقاط حمراء، مع أو بدون تعب شديد غير مبرر، والارتباك، واصفرار الجلد أو العينين (اليرقان). (انظر القسم 4 «الآثار الجانبية المحتملة»).
  • إذا جرحت نفسك، قد يستغرق النزيف وقتاً أطول من المعتاد حتى يتوقف. وهذا يرتبط بطريقة عمل أدويتك، حيث إنها تمنع تشكل الجلطات الدموية. بالنسبة للجروح والإصابات البسيطة، مثل جرح نفسك، أو الحلاقة، هذا عادة لا يشكل مصدر للقلق. ومع ذلك، إذا كنت تشعر بالقلق إزاء النزيف، ينبغي عليك الاتصال بطبيبك فوراً (انظر القسم 4 «الأثار الجانبية المحتملة»).
  • قد يطلب الطبيب منك إجراء فحوصات للدم.

 

د- الأطفال والمراهقون:

لا تعطِ هذه الأدوية للأطفال نظراً لأنها لا تعطي أي نتيجة مع الأطفال.

 

هـ- تناول كيوبيدو مع الأدوية الأخرى والمكملات الغذائية أو العشبية:

ينبغي عليك إخبار طبيبك أو الصيدلي إذا كنت تتناول، أو قد تناولت في الآونة الأخيرة أو قد تتناول أي أدوية أخرى، بما في ذلك الأدوية التي تم الحصول عليها دون وصفة طبية. قد تؤثر بعض الأدوية الأخرى على استخدام كيوبيدو أو العكس صحيح.

ينبغي عليك إخبار الطبيب خصيصًا إذا كنت تتناول:

  • أدوية قد تزيد من خطر إصابتك بنزيف، مثل:
    • مضادات التخثر الفموية، والأدوية المستخدمة لتقليل تخثر الدم.
    • مضادات الالتهاب اللاستيرويدية، عادة ما تُستخدم لعلاج حالات الالتهاب و/ أو الآلام في العضلات أو المفاصل.
    • الهيبارين أو أي أدوية أخرى عن طريق الحقن تُستخدم للحد من تخثر الدم.
    • تيكلوبيدين، عناصر مضادات الصفائح الأخرى. 
    • مثبط استرجاع السيروتونين الانتقائي (بما في ذلك ولكن لا يقتصر على فلوكسيتين أو فلوفوكسامين)، وهي أدوية عادة ما تُستخدم لعلاج الاكتئاب.
  • أوميبرازول أو إيسوميبرازول، وهي أدوية لعلاج اضطرابات المعدة.
  • فلوكونازول أو فوريكونازول، وهي أدوية لعلاج الالتهابات الفطرية.
  • إيفافيرنز، وهو دواء لعلاج التهابات فيروس نقص المناعة البشرية (الإيدز).
  • كاربامازيبين، وهو دواء لعلاج بعض أنواع الصرع.
  • موكلوبيميد ، وهو دواء لعلاج الاكتئاب.
  • ريباغلينيد ، وهو دواء لعلاج مرض السكري.
  • باكليتاكسيل، وهو دواء لعلاج السرطان.

إذا عانيت من آلام شديدة في الصدر (الذبحة الصدرية غير المستقرة أو النوبة القلبية)، قد يصف لك الطبيب كيوبيدو بالاقتران مع حمض خلي الصفصافي، وهي مادة موجودة في العديد من الأدوية المستخدمة لتخفيف الألم وخفض الحمى. إن الاستخدام العرضي لحمض خلي الصفصافي (بما لا يزيد عن 1000 ملجم كل 24 ساعة) ينبغي ألا يسبب مشكلة بشكل عام، ولكن ينبغي مناقشة طبيبك بخصوص الاستعمال المط ول لها في ظروف أخرى.

 

و- تناول كيوبيدو مع الطعام والشراب:

يُسمح بتناول كيوبيدو مع أو بدون طعام.

 

ز- الحمل والرضاعة الطبيعية:

من الأفضل عدم تناول هذا المنتج خلال فترة الحمل.

إذا كنتِ حاملًا أو تظنين أنكِ حامل ، ينبغي عليكِ إخبار طبيبك أو الصيدلي قبل تناول كيوبيدو. إذا أصبحتِ حاملًا أثناء تناول كيوبيدو، فاستشيري طبيبكِ فوراً، كما ينصح بعدم تناول كلوبيدوجريل عندما تكونين حاملًا.

لا ينبغي تناول الدواء عندم قيامكِ بالرضاعة الطبيعية.
إذا كنت تقومين بالرضاعة الطبيعية أو تخططين للقيام بالرضاعة الطبيعية، ينبغي عليكِ مناقشة الأمر مع طبيبكِ قبل تناول هذا الدواء.

اسألي طبيبكِ أو الصيدلي للحصول على المشورة، قبل تناول أي دواء.

 

ح- قيادة السيارات واستخدام الآلات:

من غير المحتمل أن يؤثر كيوبيدو على قدرتك على القيادة أو استخدام الآلات.

 

يحتوي كيوبيدو على اللاكتوز:
إذا أخبرك الطبيب أن لديك حساسية تجاه بعض السكريات (مثل اللاكتوز)، اتصل بطبيبك قبل تناول هذا الدواء.

 

يحتوى كيوبيدو على زيت الخروع المهدرج 

وهذا قد يسبب اضطراب في المعدة أو الإسهال.

https://localhost:44358/Dashboard

ينبغي دائمًا تناول هذا الدواء تمامًا بحسب تعليمات طبيبك أو الصيدلي. استشر طبيبك أو الصيدلي إذا لم تكن متأكدًا.

 

أ- ما هي الجرعة المقررة لك من كيوبيدو؟

إن الجرعة الموصى بها، بما في ذلك المرضى الذين يعانون من حالة تسمى بالرجفان الأذيني (عدم انتظام ضربات القلب)، هي قرص 75 ملجم واحد من كيوبيدو يوميًّا، ويؤخذ عن طريق الفم مع أو بدون الطعام، وفي نفس التوقيت كل يوم.

إذا واجهت آلام شديدة في الصدر (الذبحة الصدرية غير المستقرة أو النوبة القلبية)، قد يعطيك طبيبك كيوبيدو 300 ملجم من كيوبيدو (قرص واحد 300 ملجم أو 4 أقراص 75 ملجم) مرة واحدة في بداية العلاج. بعد ذلك، سيتم إعطاؤك الجرعة الموصى بها وهي قرص 75 ملجم واحد من كيوبيدو يوميًّا كما هو موضح أعلاه.

ينبغي عليك الاستمرار في تناول كيوبيدو طالما أن الطبيب مستمر في وصفه لك.

 

ب- إذا تناولت كيوبيدو بأكثر من الجرعة من المقررة لك (جرعة زائدة):

اتصل بطبيبك أو بأقرب قسم طوارئ بالمستشفى بسبب زيادة خطر حدوث نزيف.

 

ج- إذا نسيت تناول جرعة كيوبيدو:

إذا كنت قد نسيت تناول جرعة كيوبيدو، ولكن تذكرتها في غضون 12 ساعة من الوقت المعتاد، ينبغي عليك تناولها فوراً ومن ثم تناول القرص القادم في الوقت المعتاد. إذا كنت قد نسيت تناول الجرعة لأكثر من 12 ساعة، ما عليك إلا تناول الجرعة القادمة في الوقت المعتاد. ولا تتناول جرعة مزدوجة لتعويض القرص المنسي.

بالنسبة للعلب المحتوية على 7 و 14 و 28 و 84 قرص، يمكنك التحقق من آخر يوم تناولت فيه قرص كيوبيدو، وذلك بالرجوع إلى التقويم المطبوع على الشريط.

 

د- إذا توقفت عن تناول كيوبيدو:

لا تتوقف عن تناول العلاج ما لم يخبرك طبيبك بذلك. اتصل بالطيبب أو الصيدلي الخاص بك قبل أن تتوقف عن تناوله.

إذا كانت لديك أسئلة أخرى، اطلب المزيد من المعلومات من طبيبك أو الصيدلي.

مثل جميع الأدوية، يمكن أن يسبب هذا الدواء آثا راً جانبية، على الرغم من أنها لا تصيب الجميع.

 

أخبر طبيبك على الفور إذا ظهرت لديك أيا من الآثار الجانبية التالية:

  • الحمى، وعلامات العدوى أو التعب الشديد، وقد يرجع ذلك إلى الانخفاض النادر لبعض خلايا الدم.
  • - علامات على وجود مشاكل في الكبد مثل اصفرار الجلد أو العينين (اليرقان)، سواء أكان ذلك مرتبط أو غير مرتبط بالنزيف الذي يظهر تحت الجلد كنقاط حمراء و/ أو الشعور بالارتباك (انظر القسم 2 «الاحتياطات والتحذيرات»).
  • تورم في الفم أو اضطرابات الجلد مثل الطفح الجلدي والحكة، وظهور بثور في الجلد. قد تكون هذه علامات الحساسية.

 

من الأثار الجانبية الأكثر شيوعًا المُبلَّغ عنها مع العلاج بكيوبيدو هي النزيف
قد يحدث النزيف بصورة نزيف في المعدة أو الأمعاء، أو كدمات، أو ورم دموي (نزيف غير عادي أو كدمات تحت الجلد)، أو نزيف الأنف، أو دم في البول. في عدد قليل من الحالات، تم الإبلاغ عن حدوث نزيف في العين، داخل الرأس، أو في الرئة أو المفاصل.

 

إذا عانيت من نزيف لمدة طويلة عند تناول كيوبيدو:

إذا آذيت أو جرحت نفسك، قد يستغرق النزيف وقتًا أطول من المعتاد حتى يتوقف. وهذا يرتبط بطريقة عمل أدويتك، حيث إنها تمنع تشكل الجلطات الدموية. بالنسبة للجروح والإصابات البسيطة، مثل جرح نفسك، أو الحلاقة، هذا عادة لا يشكل مصدر للقلق. ومع ذلك، إذا كنت تشعر بالقلق إزاء النزيف، ينبغي عليك الاتصال بطبيبك فوراً (انظر القسم 2 «الاحتياطات والتحذيرات»).

 

تشمل الآثار الجانبية الأخرى:

الأثار الجانبية الشائعة (التي قد تحدث لشخص واحد من بين كل 10 أشخاص):

الإسهال، أو آلام في البطن، أو عسر الهضم أو الحرقة.

 

الأثار الجانبية غير الشائعة (التي قد تحدث لشخص واحد من بين كل 100 شخص):

الصداع، أو قرحة المعدة، أو القيء، أو الغثيان، أو الإمساك، أو الغازات المفرطة في المعدة أو الأمعاء، أو الطفح الجلدي، أو الحكة، أو
الدوخة، أو الإحساس بالوخز والخدر.

 

الأثار الجانبية النادرة (التي قد تحدث لشخص واحد من بين كل 1000 شخص):

الدوار، أو تضخم الثديين في الذكور.

 

الأثار الجانبية النادرة جدًّا (التي قد تحدث لشخص واحد من بين كل 10,000 شخص):

اليرقان؛ ألم شديد في البطن مع أو بدون آلام الظهر؛ الحمى، وصعوبات في التنفس مقترنة أحيا نا بالسعال؛ وحالة عامة من ردود الفعل
التحسسية (على سبيل المثال، الإحساس العام بالحرارة مع الشعور العام بعدم الارتياح المفاجئ حتى الإغماء)؛ التورم في الفم؛ بثور في
الجلد؛ حساسية الجلد؛ قرحة الفم (التهاب الفم)؛ انخفاض في ضغط الدم؛ الشعور بالارتباك؛ الهلوسة؛ ألم المفاصل؛ ألم عضلي؛ تغييرات
في مذاق الطعام أو فقدان القدرة على تذوق

 

الأثار الجانبية غير معروفة (لا يمكن تقدير تكرارها من البيانات المتاحة):

ردود فعل الحساسية المفرطة في الصدر أو ألم في البطن، أو استمرار أعراض انخفاض السكر في الدم. متلازمة المناعة الذاتية الخاصة بالأنسولين، والتي يمكن أن تؤدي إلى نقص شديد في سكر الدم، وخاصة في المرضى الذين يعانون من النوع الفرعي 4 HLA DRA (الأكثر تكراراً عند الشعب الياباني.) 

بالإضافة إلى ذلك، قد يتبين الطبيب وجود تغييرات في نتائج فحوصات الدم أو البول.

  • ابقِ الدواء بعيدًا عن متناول ومرأى الأطفال.
  • لا تستخدم هذا الدواء بعد تاريخ انتهاء الصلاحية المُدوَّن على العلبة والشريط بعد كلمة «تاريخ انتهاء الصلاحية». تاريخ انتهاء الصلاحية يشير إلى اليوم الأخير من الشهر.
  • يتم تخزينه في درجة حرارة أقل من 30 درجة مئوية.
  • لا تستخدم هذا الدواء إذا لاحظت أية علامة واضحة على تلفه.
  • ينبغي عدم التخلص من الأدوية في مياه الصرف الصحي أو النفايات المنزلية. إسأل الصيدلي الخاص بك عن كيفية التخلص من الأدوية التي لم تعد لازمة. ستساعد هذه التدابير في حماية البيئة.
     

أ- ما هو المكون الطبي؟

المادة الفعالة هي كلوبيدوجريل، ويحتوي كل قرص على 75 ملجم من كلوبيدوجريل (كبريتيد الهيدروجين).

 

ب- ما هي المكونات غير الطبية؟

المكونات الأخرى هي (انظر القسم 2 « يحتوى كيوبيدو على اللاكتوز» و «يحتوى كيوبيدو على زيت الخروع المهدرج»):

نواة القرص: المانيتول (E421) وزيت الخروع المهدرج، السليلوز فائق التبلور، ماكروغول 6000 وهيدروكسي بروبيل السيليلوز منخفض الاستبدال.

غلاف القرص: مونوهيدرات اللاكتوز (سكر الحليب)، هيدروكسي بروبيل ميثيل سيللوز (E464)، ثلاثي الأستين (E1518)، أكسيد الحديد الاحمر
 (E172) وثاني أكسيد التيتانيوم (E171).

عامل الصقل: الشمع الكرنوبي
 

كيوبيدو 75 ملجم
كل قرص وردي مُغلف بيضاوي الشكل ومحد ب الوجهين، مطبوع عليه أحرف «CL» على «75» على أحد الجانبين وأحرف «APO» على الجانب الآخر، يحتوي على كلوبيدوجرل بيسلفات ما يعادل 75 ملجم من كلوبيدوجرل.

متوفر في عبوات ذات أشرطة تحتوي على 30 قرص.

شركة ابوتاكس إنك
150 سيجنيت درايف
تورونتو ، أونتاريو
M9L 1T9، كندا  
هاتف: 4623-268-800-1 
فاكس: 9444-609-800-1
www.apotex.com

تمت مراجعة هذه النشرة آخر مرة في 03/2019.
 Read this leaflet carefully before you start using this product as it contains important information for you

Trade Name in the GCC States: Cupido Trade Name in the Country of Origin: Apo- Clopidogrel Generic Name: Clopidogrel

Route of Administration: Oral Dosage form/strength: 75mg Tablet Nonmedicinal Ingredients: Anhydrous lactose, colloidal silicon dioxide, crospovidone, ferric oxide red, hydroxypropyl cellulose, hydroxypropyl methylcellulose, methylcellulose, polyethylene glycol, titanium dioxide and zinc stearate.

Cupido 75mg Tablets: Each pink, round, biconvex, film-coated tablet engraved with “CL” over "75" on one side and "APO" on the other side contains clopidogrel bisulfate equivalent to 75 mg clopidogrel.

Secondary prevention of atherothrombotic events Clopidogrel is indicated in:

  • Adult patients suffering from myocardial infarction (from a few days until less than 35 days), ischemic stroke (from 7 days until less than 6 months) or established peripheral arterial disease.
  • Adult patients suffering from acute coronary syndrome:
    • Non-ST segment elevation acute coronary syndrome (unstable angina or non-Q-wave myocardial infarction), including patients undergoing a stent placement following percutaneous coronary intervention, in combination with acetylsalicylic acid (ASA).
    • ST segment elevation acute myocardial infarction, in combination with ASA in medically treated patients eligible for thrombolytic therapy.

 

Prevention of atherothrombotic and thromboembolic events in atrial fibrillation

In adult patients with atrial fibrillation who have at least one risk factor for vascular events, are not suitable for treatment with Vitamin K antagonists (VKA) and who have a low bleeding risk, clopidogrel is indicated in combination with ASA for the prevention of atherothrombotic and thromboembolic events, including stroke.

For further information please refer to section 5.1


Posology

Adults and elderly

Cupido 75 mg film-coated tablets

Clopidogrel should be given as a single daily dose of 75 mg.

In patients suffering from acute coronary syndrome:

  • Non-ST segment elevation acute coronary syndrome (unstable angina or non-Q-wave myocardial infarction): clopidogrel treatment should be initiated with a single 300-mg loading dose and then continued at 75 mg once a day (with acetylsalicylic acid (ASA) 75 mg-325 mg daily). Since higher doses of ASA were associated with higher bleeding risk it is recommended that the dose of ASA should not be higher than 100 mg. The optimal duration of treatment has not been formally established. Clinical trial data support use up to 12 months, and the maximum benefit was seen at 3 months (see section 5.1).
  • ST segment elevation acute myocardial infarction: clopidogrel should be given as a single daily dose of 75 mg initiated with a 300-mg loading dose in combination with ASA and with or without thrombolytics. For patients over 75 years of age clopidogrel should be initiated without a loading dose. Combined therapy should be started as early as possible after symptoms start and continued for at least four weeks. The benefit of the combination of clopidogrel with ASA beyond four weeks has not been studied in this setting (see section 5.1).

 

In patients with atrial fibrillation, clopidogrel should be given as a single daily dose of 75 mg. ASA (75-100 mg daily) should be initiated and continued in combination with clopidogrel (see section 5.1).

 

If a dose is missed:

  • Within less than 12 hours after regular scheduled time: patients should take the dose immediately and then take the next dose at the regular scheduled time.
  • For more than 12 hours: patients should take the next dose at the regular scheduled time and should not double the dose.

 

Pediatric population

Clopidogrel should not be used in children because of efficacy concerns (see section 5.1).

 

Renal impairment

Therapeutic experience is limited in patients with renal impairment (see section 4.4).

 

Hepatic impairment

Therapeutic experience is limited in patients with moderate hepatic disease who may have bleeding diatheses (see section 4.4).

 

Method of administration

For oral use

It may be given with or without food


• Hypersensitivity to the active substance or to any of the excipients listed in section 2 or section 6.1. • Severe hepatic impairment. • Active pathological bleeding such as peptic ulcer or intracranial hemorrhage.

Bleeding and haematological disorders

Due to the risk of bleeding and haematological adverse reactions, blood cell count determination and/or other appropriate testing should be promptly considered whenever clinical symptoms suggestive of bleeding arise during the course of treatment (see section 4.8). As with other antiplatelet agents, clopidogrel should be used with caution in patients who may be at risk of increased bleeding from trauma, surgery or other pathological conditions and in patients receiving treatment with ASA, heparin, glycoprotein IIb/IIIa inhibitors or non-steroidal anti-inflammatory drugs (NSAIDs) including Cox-2 inhibitors, or selective serotonin reuptake inhibitors (SSRIs), or other medicinal products associated with bleeding risk such as pentoxifylline (see section 4.5).

Patients should be followed carefully for any signs of bleeding including occult bleeding, especially during the first weeks of treatment and/or after invasive cardiac procedures or surgery. The concomitant administration of clopidogrel with oral anticoagulants is not recommended since it may increase the intensity of bleedings (see section 4.5).

If a patient is to undergo elective surgery and antiplatelet effect is temporarily not desirable, clopidogrel should be discontinued 7 days prior to surgery. Patients should inform physicians and dentists that they are taking clopidogrel before any surgery is scheduled and before any new medicinal product is taken. Clopidogrel prolongs bleeding time and should be used with caution in patients who have lesions with a propensity to bleed (particularly gastrointestinal and intraocular).

Patients should be told that it might take longer than usual to stop bleeding when they take clopidogrel (alone or in combination with ASA), and that they should report any unusual bleeding (site or duration) to their physician.

 

Thrombotic Thrombocytopenic Purpura (TTP)

Thrombotic Thrombocytopenic Purpura (TTP) has been reported very rarely following the use of clopidogrel, sometimes after a short exposure. It is characterized by thrombocytopenia and microangiopathic hemolytic anemia associated with either neurological findings, renal dysfunction or fever. TTP is a potentially fatal condition requiring prompt treatment including plasmapheresis.

 

Acquired hemophilia

Acquired hemophilia has been reported following use of clopidogrel. In cases of confirmed isolated activated Partial Thromboplastin Time (aPTT) prolongation with or without bleeding, acquired hemophilia should be considered. Patients with a confirmed diagnosis of acquired hemophilia should be managed and treated by specialists, and clopidogrel should be discontinued.

 

Recent ischemic stroke

In view of the lack of data, clopidogrel cannot be recommended during the first 7 days after acute ischemic stroke.

 

Cytochrome P450 2C19 (CYP2C19)

Pharmacogenetics: In patients who are poor CYP2C19 metabolizers, clopidogrel at recommended doses forms less of the active metabolite of clopidogrel and has a smaller effect on platelet function. Tests are available to identify a patient's CYP2C19 genotype.

 

Since clopidogrel is metabolized to its active metabolite partly by CYP2C19, use of medicinal products that inhibit the activity of this enzyme would be expected to result in reduced drug levels of the active metabolite of clopidogrel. The clinical relevance of this interaction is uncertain. As a precaution concomitant use of strong or moderate CYP2C19 inhibitors should be discouraged (see section 4.5 for a list of CYP2C19 inhibitors, see also section 5.2).

 

CYP2C8 substrates

Caution is required in patients treated concomitantly with clopidogrel and CYP2C8 substrate medicinal products (see section 4.5).

 

Cross-reactions among thienopyridines

Patients should be evaluated for history of hypersensitivity to thienopyridines (such as clopidogrel, ticlopidine, prasugrel) since cross-reactivity among thienopyridines has been reported (see section 4.8). Thienopyridines may cause mild to severe allergic reactions such as rash, angioedema, or hematological cross-reactions such as thrombocytopenia and neutropenia. Patients who had developed a previous allergic reaction and/or hematological reaction to one thienopyridine may have an increased risk of developing the same or another reaction to another thienopyridine. Monitoring for signs of hypersensitivity in patients with a known allergy to thienopyridines is advised.

 

Renal impairment

Therapeutic experience with clopidogrel is limited in patients with renal impairment. Therefore clopidogrel should be used with caution in these patients (see section 4.2).

 

Hepatic impairment

Experience is limited in patients with moderate hepatic disease who may have bleeding diatheses. Clopidogrel should therefore be used with caution in this population (see section 4.2).

 

Excipients

Cupido contains lactose. Patients with rare hereditary problems of galactose intolerance, the Lapp lactase deficiency or glucose-galactose malabsorption should not take this medicinal product.

This medicinal product contains hydrogenated castor oil which may cause stomach upset and diarrhea.


Medicinal products associated with bleeding risk: There is an increased risk of bleeding due to the potential additive effect. The concomitant administration of medicinal products associated with bleeding risk should be undertaken with caution (see section 4.4).

 

Oral anticoagulants: the concomitant administration of clopidogrel with oral anticoagulants is not recommended since it may increase the intensity of bleedings (see section 4.4). Although the administration of clopidogrel 75 mg/day did not modify the pharmacokinetics of S-warfarin or International Normalized Ratio (INR) in patients receiving long-term warfarin therapy, coadministration of clopidogrel with warfarin increases the risk of bleeding because of independent effects on hemostasis.

 

Glycoprotein IIb/IIIa inhibitors: clopidogrel should be used with caution in patients who receive concomitant glycoprotein IIb/IIIa inhibitors (see section 4.4).

 

Acetylsalicylic acid (ASA): ASA did not modify the clopidogrel-mediated inhibition of ADP- induced platelet aggregation, but clopidogrel potentiated the effect of ASA on collagen-induced platelet aggregation. However, concomitant administration of 500 mg of ASA twice a day for one day did not significantly increase the prolongation of bleeding time induced by clopidogrel intake. A pharmacodynamic interaction between clopidogrel and acetylsalicylic acid is possible, leading to increased risk of bleeding. Therefore, concomitant use should be undertaken with caution (see section 4.4). However, clopidogrel and ASA have been administered together for up to one year (see section 5.1).

 

Heparin: in a clinical study conducted in healthy subjects, clopidogrel did not necessitate modification of the heparin dose or alter the effect of heparin on coagulation. Co-administration of heparin had no effect on the inhibition of platelet aggregation induced by clopidogrel. A pharmacodynamic interaction between clopidogrel and heparin is possible, leading to increased risk of bleeding. Therefore, concomitant use should be undertaken with caution (see section 4.4).

 

Thrombolytics: the safety of the concomitant administration of clopidogrel, fibrin or non-fibrin specific thrombolytic agents and heparins was assessed in patients with acute myocardial infarction. The incidence of clinically significant bleeding was similar to that observed when thrombolytic agents and heparin are co-administered with ASA (see section 4.8)

 

NSAIDs: in a clinical study conducted in healthy volunteers, the concomitant administration of clopidogrel and naproxen increased occult gastrointestinal blood loss. However, due to the lack of interaction studies with other NSAIDs it is presently unclear whether there is an increased risk of gastrointestinal bleeding with all NSAIDs. Consequently, NSAIDs including Cox-2 inhibitors and clopidogrel should be co-administered with caution (see section 4.4).

 

SSRIs: since SSRIs affect platelet activation and increase the risk of bleeding, the concomitant administration of SSRIs with clopidogrel should be undertaken with caution.

 

Other concomitant therapy: Since clopidogrel is metabolised to its active metabolite partly by CYP2C19, use of medicinal products that inhibit the activity of this enzyme would be expected to result in reduced drug levels of the active metabolite of clopidogrel. The clinical relevance of this interaction is uncertain. As a precaution concomitant use of strong or moderate CYP2C19 inhibitors should be discouraged (see sections 4.4 and 5.2).

Medicinal products that are strong or moderate CYP2C19 inhibitors include, for example, omeprazole and esomeprazole, fluvoxamine, fluoxetine, moclobemide, voriconazole, fluconazole, ticlopidine, carbamazepine, and efavirenz.

 

Proton Pump Inhibitors (PPI): Omeprazole 80 mg once daily administered either at the same time as clopidogrel or with 12 hours between the administrations of the two drugs decreased the exposure of the active metabolite by 45% (loading dose) and 40% (maintenance dose). The decrease was associated with a 39% (loading dose) and 21% (maintenance dose) reduction of inhibition of platelet aggregation. Esomeprazole is expected to give a similar interaction with clopidogrel.

Inconsistent data on the clinical implications of this pharmacokinetic (PK)/pharmacodynamic (PD) interaction in terms of major cardiovascular events have been reported from both observational and clinical studies. As a precaution, concomitant use of omeprazole or esomeprazole should be discouraged (see section 4.4).

Less pronounced reductions of metabolite exposure has been observed with pantoprazole or lansoprazole.

The plasma concentrations of the active metabolite was 20% reduced (loading dose) and 14% reduced (maintenance dose) during concomitant treatment with pantoprazole 80 mg once daily. This was associated with a reduction of the mean inhibition of platelet aggregation by 15% and 11%, respectively. These results indicate that clopidogrel can be administered with pantoprazole.

There is no evidence that other medicinal products that reduce stomach acid such as H2 blockers or antacids interfere with antiplatelet activity of clopidogrel.

 

Other medicinal products: A number of other clinical studies have been conducted with clopidogrel and other concomitant medicinal products to investigate the potential for pharmacodynamic and pharmacokinetic interactions. No clinically significant pharmacodynamic interactions were observed when clopidogrel was co-administered with atenolol, nifedipine, or both atenolol and nifedipine. Furthermore, the pharmacodynamic activity of clopidogrel was not significantly influenced by the co-administration of phenobarbital or estrogen.

The pharmacokinetics of digoxin or theophylline were not modified by the co-administration of clopidogrel. Antacids did not modify the extent of clopidogrel absorption.

Data from the CAPRIE study indicate that phenytoin and tolbutamide which are metabolized by CYP2C9 can be safely co-administered with clopidogrel.

 

CYP2C8 substrate medicinal products: Clopidogrel has been shown to increase repaglinide exposure in healthy volunteers. In vitro studies have shown the increase in repaglinide exposure is due to inhibition of CYP2C8 by the glucuronide metabolite of clopidogrel. Due to the risk of increased plasma concentrations, concomitant administration of clopidogrel and drugs primarily cleared by CYP2C8 metabolism (e.g., repaglinide, paclitaxel) should be undertaken with caution (see section 4.4).

Apart from the specific medicinal product interaction information described above, interaction studies with clopidogrel and some medicinal products commonly administered in patients with atherothrombotic disease have not been performed. However, patients entered into clinical trials with clopidogrel received a variety of concomitant medicinal products including diuretics, beta blockers, ACEI, calcium antagonists, cholesterol lowering agents, coronary vasodilators, antidiabetic agents (including insulin), antiepileptic agents and GPIIb/IIIa antagonists without evidence of clinically significant adverse interactions.


Pregnancy

As no clinical data on exposure to clopidogrel during pregnancy are available, it is preferable not to use clopidogrel during pregnancy as a precautionary measure.

Animal studies do not indicate direct or indirect harmful effects with respect to pregnancy, embryonal/foetal development, parturition or postnatal development (see section 5.3).

 

Breast-feeding

It is unknown whether clopidogrel is excreted in human breast milk. Animal studies have shown excretion of clopidogrel in breast milk. As a precautionary measure, breast-feeding should not be continued during treatment with Cupido.

 

Fertility

Clopidogrel was not shown to alter fertility in animal studies.


Clopidogrel has no or negligible influence on the ability to drive and use machines.


Summary of the safety profile

Clopidogrel has been evaluated for safety in more than 44,000 patients who have participated in clinical studies, including over 12,000 patients treated for 1 year or more. Overall, clopidogrel 75 mg/day was comparable to ASA 325 mg/day in CAPRIE regardless of age, gender and race. The clinically relevant adverse reactions observed in the CAPRIE, CURE, CLARITY, COMMIT and ACTIVE-A studies are discussed below. In addition to clinical studies experience, adverse reactions have been spontaneously reported.

Bleeding is the most common reaction reported both in clinical studies as well as in post-marketing experience where it was mostly reported during the first month of treatment.

 

In CAPRIE, in patients treated with either clopidogrel or ASA, the overall incidence of any bleeding was 9.3%. The incidence of severe cases was similar for clopidogrel and ASA.

 

In CURE, there was no excess in major bleeds with clopidogrel plus ASA within 7 days after coronary bypass graft surgery in patients who stopped therapy more than five days prior to surgery. In patients who remained on therapy within five days of bypass graft surgery, the event rate was 9.6% for clopidogrel plus ASA, and 6.3% for placebo plus ASA.

 

In CLARITY, there was an overall increase in bleeding in the clopidogrel plus ASA group vs. the placebo plus ASA group .The incidence of major bleeding was similar between groups. This was consistent across subgroups of patients defined by baseline characteristics, and type of fibrinolytic or heparin therapy.

 

In COMMIT, the overall rate of noncerebral major bleeding or cerebral bleeding was low and similar in both groups.

 

In ACTIVE-A, the rate of major bleeding was greater in the clopidogrel + ASA group than in the placebo + ASA group (6.7% versus 4.3%). Major bleeding was mostly of extracranial origin in both groups (5.3% in the clopidogrel + ASA group; 3.5% in the placebo +ASA group), mainly from the gastrointestinal tract (3.5% vs. 1.8%). There was an excess of intracranial bleeding in the clopidogrel

+ ASA treatment group compared to the placebo + ASA group (1.4% versus 0.8%, respectively). There was no statistically significant difference in the rates of fatal bleeding (1.1% in the clopidogrel

+ ASA group and 0.7% in the placebo +ASA group) and haemorrhagic stroke (0.8% and 0.6%, respectively) between groups.

 

Tabulated list of adverse reactions

Adverse reactions that occurred either during clinical studies or that were spontaneously reported are presented in the table below. Their frequency is defined using the following conventions: 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). Within each system organ class, adverse reactions are presented in order of decreasing seriousness.

 

System Organ Class

Common

Uncommon

Rare

Very Rare, not known*

Blood and the lymphatic system disorders

 

Thrombocytopenia, leucopenia, eosinophilia

Neutropenia, including severe neutropenia

Thrombotic thrombocytopenic purpura (TTP) (see section 4.4), aplastic anemia, pancytopenia, agranulocytosis, severe thrombocytopenia, acquired hemophilia

A, granulocytopenia, anemia

Cardiac disorders

 

 

 

Kounis syndrome (vasospastic allergic angina / allergic myocardial infarction) in the context of a hypersensitivity reaction due to clopidogrel*

Immune system disorders

 

 

 

Serum sickness, anaphylactoid reactions, cross- reactive drug hypersensitivity among thienopyridines (such as ticlopidine, prasugrel) (see section 4.4), insulin autoimmune

syndrome, which can lead to severe hypoglycemia, particularly in patients with HLA DRA4 subtype (more frequent in the Japanese population)*

Psychiatric disorders

 

 

 

Hallucinations, confusion

Nervous system disorders

 

Intracranial bleeding (some cases were reported with fatal

outcome), headache, paraesthesia, dizziness

 

Taste disturbances, ageusia

System Organ Class

Common

Uncommon

Rare

Very Rare, not known*

Eye disorders

 

Eye bleeding (conjunctival, ocular, retinal)

 

 

Ear and labyrinth disorders

 

 

Vertigo

 

Vascular disorders

Hematoma

 

 

Serious hemorrhage, hemorrhage of operative wound, vasculitis, hypotension

Respiratory, thoracic and mediastinal disorders

Epistaxis

 

 

Respiratory tract bleeding (haemoptysis, pulmonary hemorrhage), bronchospasm, interstitial

pneumonitis, eosinophilic pneumonia

Gastrointestinal disorders

Gastrointestinal hemorrhage, diarrhea, abdominal

pain, dyspepsia

Gastric ulcer and duodenal ulcer, gastritis, vomiting, nausea, constipation, flatulence

Retroperitoneal hemorrhage

Gastrointestinal and retroperitoneal hemorrhage with fatal outcome, pancreatitis, colitis (including ulcerative or lymphocytic colitis), stomatitis

Hepato-biliary disorders

 

 

 

Acute liver failure, hepatitis, abnormal liver function test

Skin and subcutaneous tissue disorders

Bruising

Rash, pruritus, skin bleeding (purpura)

 

Bullous dermatitis (toxic epidermal necrolysis, Stevens Johnson Syndrome, erythema multiforme, acute generalized exanthematous pustulosis (AGEP)), angioedema, drug- induced hypersensitivity syndrome, drug rash with eosinophilia and systemic symptoms (DRESS), rash erythematous or exfoliative, urticaria, eczema, lichen planus

Reproductive systems and breast disorders

 

 

Gynaecomastia

 

Musculoskeletal, connective tissue and bone disorders

 

 

 

Musculo-skeletal bleeding (haemarthrosis), arthritis, arthralgia, myalgia

Renal and urinary disorders

 

Haematuria

 

Glomerulonephritis, blood creatinine increased

General disorders and administration site conditions

Bleeding at puncture site

 

 

Fever

Investigations

 

Bleeding time prolonged, neutrophil count decreased, platelet count decreased

 

 

* Information related to clopidogrel with frequency “not known”.

Reporting of suspected adverse reactions

Reporting suspected adverse reactions after authorization of the medicinal product is important. It allows continued monitoring of the benefit/risk balance of the medicinal product. Healthcare professionals are asked to report any suspected adverse reactions via Yellow Card Scheme at: www.mhra.gov.uk/yellowcard or search for MHRA Yellow Card in the Google Play or Apple App Store.

 

To report any side effects:

Saudi Arabia:

The National Pharmacovigilance and Drug Safety Centre (NPC)

  • Fax: +966‐11‐205‐7662
  • Call NPC at +966‐11‐2038222, Exts: 2317‐2356‐2340.
  • Reporting Hotline: 19999
  • E‐mail: npc.drug@sfda.gov.sa
  • Website: www.sfda.gov.sa/npc

 

United Arab Emirates

Pharmacovigilance & Medical Device section

  • P.O.Box: 1853
  • Tel: 80011111
  • Email : pv@moh.gov.ae

Drug Department

Ministry of Health & Prevention Dubai

 

Other GCC States:

Please contact the relevant competent authority.

 


Overdose following clopidogrel administration may lead to prolonged bleeding time and subsequent bleeding complications. Appropriate therapy should be considered if bleedings are observed.

No antidote to the pharmacological activity of clopidogrel has been found. If prompt correction of prolonged bleeding time is required, platelet transfusion may reverse the effects of clopidogrel.


Pharmacotherapeutic group: platelet aggregation inhibitors excl. heparin, ATC Code: B01AC-04.

 

Clopidogrel is a prodrug, one of whose metabolites is an inhibitor of platelet aggregation. Clopidogrel must be metabolized by CYP450 enzymes to produce the active metabolite that inhibits platelet aggregation. The active metabolite of clopidogrel selectively inhibits the binding of adenosine diphosphate (ADP) to its platelet P2Y12 receptor and the subsequent ADP-mediated activation of the glycoprotein GPIIb/IIIa complex, thereby inhibiting platelet aggregation. Due to the irreversible binding, platelets exposed are affected for the remainder of their lifespan (approximately 7-10 days) and recovery of normal platelet function occurs at a rate consistent with platelet turnover. Platelet aggregation induced by agonists other than ADP is also inhibited by blocking the amplification of platelet activation by released ADP.

 

Because the active metabolite is formed by CYP450 enzymes, some of which are polymorphic or subject to inhibition by other medicinal products, not all patients will have adequate platelet inhibition.

 

Repeated doses of 75 mg per day produced substantial inhibition of ADP-induced platelet aggregation from the first day; this increased progressively and reached steady state between Day 3 and Day 7. At steady state, the average inhibition level observed with a dose of 75 mg per day was

 

between 40% and 60%. Platelet aggregation and bleeding time gradually returned to baseline values, generally within 5 days after treatment was discontinued.

 

Clinical efficacy and safety

The safety and efficacy of clopidogrel have been evaluated in 5 double-blind studies involving over 88,000 patients: the CAPRIE study, a comparison of clopidogrel to ASA, and the CURE, CLARITY, COMMIT and ACTIVE-A studies comparing clopidogrel to placebo, both medicinal products given in combination with ASA and other standard therapy.

 

Recent myocardial infarction (MI), recent stroke or established peripheral arterial disease

The CAPRIE study included 19,185 patients with atherothrombosis as manifested by recent myocardial infarction (<35 days), recent ischemic stroke (between 7 days and 6 months) or established peripheral arterial disease (PAD). Patients were randomized to clopidogrel 75 mg/day or ASA 325 mg/day, and were followed for 1 to 3 years. In the myocardial infarction subgroup, most of the patients received ASA for the first few days following the acute myocardial infarction.

 

Clopidogrel significantly reduced the incidence of new ischemic events (combined end point of myocardial infarction, ischemic stroke and vascular death) when compared to ASA. In the intention to treat analysis, 939 events were observed in the clopidogrel group and 1,020 events with ASA (relative risk reduction (RRR) 8.7%, [95% CI: 0.2 to 16.4]; p=0.045), which corresponds, for every 1,000 patients treated for 2 years, to 10 [CI: 0 to 20] additional patients being prevented from experiencing a new ischemic event. Analysis of total mortality as a secondary endpoint did not show any significant difference between clopidogrel (5.8%) and ASA (6.0%).

 

In a subgroup analysis by qualifying condition (myocardial infarction, ischemic stroke, and PAD) the benefit appeared to be strongest (achieving statistical significance at p=0.003) in patients enrolled due to PAD (especially those who also had a history of myocardial infarction) (RRR = 23.7%; CI: 8.9 to 36.2) and weaker (not significantly different from ASA) in stroke patients (RRR = 7.3%; CI: -5.7 to 18.7 [p=0.258]). In patients who were enrolled in the trial on the sole basis of a

recent myocardial infarction, clopidogrel was numerically inferior, but not statistically different from ASA (RRR = -4.0%; CI: -22.5 to 11.7 [p=0.639]). In addition, a subgroup analysis by age suggested that the benefit of clopidogrel in patients over 75 years was less than that observed in patients ≤75 years.

 

Since the CAPRIE trial was not powered to evaluate efficacy of individual subgroups, it is not clear whether the differences in relative risk reduction across qualifying conditions are real, or a result of chance.

 

Acute coronary syndrome

The CURE study included 12,562 patients with non-ST segment elevation acute coronary syndrome (unstable angina or non-Q-wave myocardial infarction), and presenting within 24 hours of onset of the most recent episode of chest pain or symptoms consistent with ischemia. Patients were required to have either ECG changes compatible with new ischemia or elevated cardiac enzymes or troponin I or T to at least twice the upper limit of normal. Patients were randomized to clopidogrel (300 mg loading dose followed by 75 mg/day, N=6,259) or placebo (N=6,303), both given in combination

 

with ASA (75-325 mg once daily) and other standard therapies. Patients were treated for up to one year. In CURE, 823 (6.6%) patients received concomitant GPIIb/IIIa receptor antagonist therapy. Heparins were administered in more than 90% of the patients and the relative rate of bleeding between clopidogrel and placebo was not significantly affected by the concomitant heparin therapy.

 

The number of patients experiencing the primary endpoint [cardiovascular (CV) death, myocardial infarction (MI), or stroke] was 582 (9.3%) in the clopidogrel-treated group and 719 (11.4%) in the placebo-treated group, a 20% relative risk reduction (95% CI of 10%-28%; p=0.00009) for the clopidogrel-treated group (17% relative risk reduction when patients were treated conservatively, 29% when they underwent percutaneous transluminal coronary angioplasty (PTCA) with or without stent and 10% when they underwent coronary artery bypass graft (CABG)). New cardiovascular events (primary endpoint) were prevented, with relative risk reductions of 22% (CI: 8.6, 33.4), 32% (CI: 12.8, 46.4), 4% (CI: -26.9, 26.7), 6% (CI: -33.5, 34.3) and 14% (CI: -31.6, 44.2), during the 0-1,

1-3, 3-6, 6-9 and 9-12 month study intervals, respectively. Thus, beyond 3 months of treatment, the benefit observed in the clopidogrel + ASA group was not further increased, whereas the risk of hemorrhage persisted (see section 4.4).

 

The use of clopidogrel in CURE was associated with a decrease in the need of thrombolytic therapy (RRR = 43.3%; CI: 24.3%, 57.5%) and GPIIb/IIIa inhibitors (RRR = 18.2%; CI: 6.5%, 28.3%).

 

The number of patients experiencing the co-primary endpoint (CV death, MI, stroke or refractory ischemia) was 1,035 (16.5%) in the clopidogrel-treated group and 1,187 (18.8%) in the placebo- treated group, a 14% relative risk reduction (95% CI of 6%-21%, p=0.0005) for the clopidogrel- treated group. This benefit was mostly driven by the statistically significant reduction in the incidence of MI [287 (4.6%) in the clopidogrel treated group and 363 (5.8%) in the placebo treated group]. There was no observed effect on the rate of rehospitalization for unstable angina.

 

The results obtained in populations with different characteristics (e.g. unstable angina or non-Q- wave MI, low to high risk levels, diabetes, need for revascularization, age, gender, etc.) were consistent with the results of the primary analysis. In particular, in a post-hoc analysis in 2,172 patients (17% of the total CURE population) who underwent stent placement (Stent-CURE), the data showed that clopidogrel compared to placebo, demonstrated a significant RRR of 26.2% favoring clopidogrel for the co-primary endpoint (CV death, MI, stroke) and also a significant RRR of 23.9% for the second co-primary endpoint (CV death, MI, stroke or refractory ischemia). Moreover, the safety profile of clopidogrel in this subgroup of patients did not raise any particular concern. Thus, the results from this subset are in line with the overall trial results.

 

The benefits observed with clopidogrel were independent of other acute and long-term cardiovascular therapies (such as heparin/LMWH, GPIIb/IIIa antagonists, lipid lowering medicinal products, beta blockers, and ACE-inhibitors). The efficacy of clopidogrel was observed independently of the dose of ASA (75-325 mg once daily).

In patients with acute ST-segment elevation MI, safety and efficacy of clopidogrel have been evaluated in 2 randomized, placebo-controlled, double-blind studies, CLARITY and COMMIT.

 

The CLARITY trial included 3,491 patients presenting within 12 hours of the onset of a ST elevation MI and planned for thrombolytic therapy. Patients received clopidogrel (300 mg loading

dose, followed by 75 mg/day, n=1,752) or placebo (n=1,739), both in combination with ASA (150 to 325 mg as a loading dose, followed by 75 to 162 mg/day), a fibrinolytic agent and, when appropriate, heparin. The patients were followed for 30 days. The primary endpoint was the occurrence of the composite of an occluded infarct-related artery on the predischarge angiogram, or death or recurrent MI before coronary angiography. For patients who did not undergo angiography, the primary endpoint was death or recurrent myocardial infarction by Day 8 or by hospital discharge. The patient population included 19.7% women and 29.2% patients ≥ 65 years. A total of 99.7% of patients received fibrinolytics (fibrin specific: 68.7%, non-fibrin specific: 31.1%), 89.5% heparin, 78.7% beta blockers, 54.7% ACE inhibitors and 63% statins.

 

Fifteen percent (15.0%) of patients in the clopidogrel group and 21.7% in the placebo group reached the primary endpoint, representing an absolute reduction of 6.7% and a 36 % odds reduction in favor of clopidogrel (95% CI: 24, 47%; p < 0.001), mainly related to a reduction in occluded infarct- related arteries. This benefit was consistent across all prespecified subgroups including patients' age and gender, infarct location, and type of fibrinolytic or heparin used.

 

The 2x2 factorial design COMMIT trial included 45,852 patients presenting within 24 hours of the onset of the symptoms of suspected MI with supporting ECG abnormalities (i.e. ST elevation, ST depression or left bundle-branch block). Patients received clopidogrel (75 mg/day, n=22,961) or placebo (n=22,891), in combination with ASA (162 mg/day), for 28 days or until hospital discharge. The co-primary endpoints were death from any cause and the first occurrence of re-infarction, stroke or death. The population included 27.8% women, 58.4% patients ≥ 60 years (26% ≥ 70 years) and 54.5% patients who received fibrinolytics.

 

Clopidogrel significantly reduced the relative risk of death from any cause by 7% (p=0.029), and the relative risk of the combination of re-infarction, stroke or death by 9% (p=0.002), representing an absolute reduction of 0.5% and 0.9%, respectively. This benefit was consistent across age, gender and with or without fibrinolytics, and was observed as early as 24 hours.

 

De-escalation of P2Y12 Inhibitor Agents in ACS

 

Switching from a more potent P2Y12 receptor inhibitor to clopidogrel in association with aspirin after acute phase in ACS has been evaluated in two randomized investigator-sponsored studies (ISS) - TOPIC and TROPICAL-ACS - with clinical outcome data.

 

The clinical benefit provided by the more potent P2Y12 inhibitors, ticagrelor and prasugrel, in their pivotal studies is related to a significant reduction in recurrent ischemic events (including acute and subacute stent thrombosis (ST), myocardial infarction (MI), and urgent revascularization). Although the ischemic benefit was consistent throughout the first year, greater reduction in ischemic recurrence after ACS was observed during the initial days following the treatment initiation. In contrast, post-hoc analyses demonstrated statistically significant increases in the bleeding risk with the more potent P2Y12 inhibitors, occurring predominantly during the maintenance phase, after the first month post-ACS. TOPIC and TROPICAL-ACS were designed to study how to mitigate the bleeding events while maintaining efficacy.

 

TOPIC (Timing Of Platelet Inhibition after acute Coronary syndrome)

 

This randomized, open-label trial included ACS patients requiring PCI. Patients on aspirin and a more potent P2Y12 blocker and without adverse event at one month were assigned to switch to fixed-dose aspirin plus clopidogrel (de-escalated dual antiplatelet therapy (DAPT)) or continuation of their drug regimen (unchanged DAPT).

 

Overall, 645 of 646 patients with STEMI or NSTEMI or unstable angina were analyzed (de- escalated DAPT (n=322); unchanged DAPT (n=323)). Follow-up at one year was performed for 316 patients (98.1%) in the de-escalated DAPT group and 318 patients (98.5%) in the unchanged DAPT group. The median follow-up for both groups was 359 days. The characteristics of the studied cohort were similar in the 2 groups.

 

The primary outcome, a composite of cardiovascular death, stroke, urgent revascularization, and BARC (Bleeding Academic Research Consortium) bleeding ≥2 at 1 year post ACS, occurred in 43 patients (13.4%) in the de-escalated DAPT group and in 85 patients (26.3%) in the unchanged DAPT group (p<0.01). This statistically significant difference was mainly driven by fewer bleeding events, with no difference reported in ischaemic endpoints (p=0.36), while BARC ≥2 bleeding occurred less frequently in the de-escalated DAPT group (4.0%) versus 14.9% in the unchanged DAPT group (p<0.01). Bleeding events defined as all BARC occurred in 30 patients (9.3%) in the de-escalated DAPT group and in 76 patients (23.5%) in the unchanged DAPT group (p<0.01).

 

TROPICAL-ACS (Testing Responsiveness to Platelet Inhibition on Chronic Antiplatelet Treatment for Acute Coronary Syndromes)

 

This randomized, open-label trial included 2,610 biomarker-positive ACS patients after successful PCI. Patients were randomized to receive either prasugrel 5 or 10 mg/d (Days 0-14) (n=1309), or prasugrel 5 or 10 mg/d (Days 0-7) then de-escalated to clopidogrel 75 mg/d (Days 8-14) (n=1309), in combination with ASA (<100 mg/day). At Day 14, platelet function testing (PFT) was performed. The prasugrel-only patients were continued on prasugrel for 11.5 months.

 

The de-escalated patients underwent high platelet reactivity (HPR) testing. If HPR≥46 units, the patients were escalated back to prasugrel 5 or 10 mg/d for 11.5 months; if HPR<46 units, the patients continued on clopidogrel 75 mg/d for 11.5 months. Therefore, the guided de-escalation arm had patients on either prasugrel (40%) or clopidogrel (60%). All patients were continued on aspirin and were followed for one year.

 

The primary endpoint (the combined incidence of CV death, MI, stroke and BARC bleeding grade ≥2 at 12 months) was met showing non-inferiority. Ninety five patients (7%) in the guided de- escalation group and 118 patients (9%) in the control group (p non-inferiority=0.0004) had an event. The guided de-escalation did not result in an increased combined risk of ischemic events (2.5% in the de-escalation group vs 3.2% in the control group; p non-inferiority=0.0115), nor in the key secondary endpoint of BARC bleeding ≥2 ((5%) in the de-escalation group versus 6% in the control group (p=0.23)). The cumulative incidence of all bleeding events (BARC class 1 to 5) was 9% (114 events) in the guided de-escalation group versus 11% (137 events) in the control group (p=0.14) Atrial fibrillation

 

The ACTIVE-W and ACTIVE-A studies, separate trials in the ACTIVE program, included patients with atrial fibrillation (AF) who had at least one risk factor for vascular events. Based on enrollment criteria, physicians enrolled patients in ACTIVE-W if they were candidates for vitamin K antagonist (VKA) therapy (such as warfarin). The ACTIVE-A study included patients who could not receive VKA therapy because they were unable or unwilling to receive the treatment.

 

The ACTIVE-W study demonstrated that anticoagulant treatment with vitamin K antagonists was more effective than with clopidogrel and ASA.

 

The ACTIVE-A study (N=7,554) was a multicenter, randomized, double-blind, placebo-controlled study which compared clopidogrel 75 mg/day + ASA (N=3,772) to placebo + ASA (N=3,782). The recommended dose for ASA was 75 to 100 mg/day. Patients were treated for up to 5 years.

Patients randomized in the ACTIVE program were those presenting with documented AF, i.e., either permanent AF or at least 2 episodes of intermittent AF in the past 6 months, and had at least one of the following risk factors: age ≥75 years or age 55 to 74 years and either diabetes mellitus requiring drug therapy, or documented previous MI or documented coronary artery disease; treated for systemic hypertension; prior stroke, transient ischemic attack (TIA), or non-CNS systemic embolus; left ventricular dysfunction with left ventricular ejection fraction <45%; or documented peripheral vascular disease. The mean CHADS2 score was 2.0 (range 0-6).

 

The major exclusion criteria for patients were documented peptic ulcer disease within the previous months; prior intracerebral hemorrhage; significant thrombocytopenia (platelet count < 50 x 109/l); requirement for clopidogrel or oral anticoagulants (OAC); or intolerance to any of the two compounds.

 

Seventy-three percent (73%) of patients enrolled into the ACTIVE-A study were unable to take VKA due to physician assessment, inability to comply with INR (international normalized ratio) monitoring, predisposition to falling or head trauma, or specific risk of bleeding; for 26% of the patients, the physician's decision was based on the patient's unwillingness to take VKA.

 

The patient population included 41.8 % women. The mean age was 71 years, 41.6% of patients were ≥75 years. A total of 23.0% of patients received anti-arrhythmic, 52.1% beta-blockers, 54.6% ACE inhibitors, and 25.4% statins.

 

The number of patients who reached the primary endpoint (time to first occurrence of stroke, MI, non-CNS systemic embolism or vascular death) was 832 (22.1%) in the group treated with clopidogrel + ASA and 924 (24.4%) in the placebo + ASA group (relative risk reduction of 11.1%; 95% CI of 2.4% to 19.1%; p=0.013), primarily due to a large reduction in the incidence of strokes. Strokes occurred in 296 (7.8%) patients receiving clopidogrel + ASA and 408 (10.8%) patients receiving placebo + ASA (relative risk reduction, 28.4%; 95% CI, 16.8% to 38.3%; p=0.00001).

 

Pediatric population

In a dose escalation study of 86 neonates or infants up to 24 months of age at risk for thrombosis (PICOLO), clopidogrel was evaluated at consecutive doses of 0.01, 0.1 and 0.2 mg/kg in neonates and infants and 0.15 mg/kg only in neonates. The dose of 0.2 mg/kg achieved the mean percent inhibition of 49.3% (5 µM ADP-induced platelet aggregation) which was comparable to that of adults taking Cupido 75 mg/day.

 

In a randomized, double-blind, parallel-group study (CLARINET), 906 pediatric patients (neonates and infants) with cyanotic congenital heart disease palliated with a systemic-to-pulmonary arterial shunt were randomized to receive clopidogrel 0.2 mg/kg (n=467) or placebo (n=439) along with concomitant background therapy up to the time of second stage surgery. The mean time between shunt palliation and first administration of study medicinal product was 20 days. Approximately 88% of patients received concomitant ASA (range of 1 to 23 mg/kg/day). There was no significant difference between groups in the primary composite endpoint of death, shunt thrombosis or cardiac- related intervention prior to 120 days of age following an event considered of thrombotic nature (89 [19.1%] for the clopidogrel group and 90 [20.5%] for the placebo group) (see section 4.2). Bleeding was the most frequently reported adverse reaction in both clopidogrel and placebo groups; however, there was no significant difference in the bleeding rate between groups. In the long-term safety follow-up of this study, 26 patients with the shunt still in place at one year of age received clopidogrel up to 18 months of age. No new safety concerns were noted during this long-term follow-up.

 

The CLARINET and the PICOLO trials were conducted using a constituted solution of clopidogrel. In a relative bioavailability study in adults, the constituted solution of clopidogrel showed a similar extent and slightly higher rate of absorption of the main circulating (inactive) metabolite compared to the authorized tablet.


Absorption

After single and repeated oral doses of 75 mg per day, clopidogrel is rapidly absorbed. Mean peak plasma levels of unchanged clopidogrel (approximately 2.2-2.5 ng/ml after a single 75 mg oral dose) occurred approximately 45 minutes after dosing. Absorption is at least 50%, based on urinary excretion of clopidogrel metabolites.

 

Distribution

Clopidogrel and the main circulating (inactive) metabolite bind reversibly in vitro to human plasma proteins (98% and 94% respectively). The binding is non-saturable in vitro over a wide concentration range.

 

Biotransformation

Clopidogrel is extensively metabolized by the liver. In vitro and in vivo, clopidogrel is metabolized according to two main metabolic pathways: one mediated by esterases and leading to hydrolysis into its inactive carboxylic acid derivative (85% of circulating metabolites), and one mediated by multiple cytochromes P450. Clopidogrel is first metabolized to a 2-oxo-clopidogrel intermediate metabolite. Subsequent metabolism of the 2-oxo-clopidogrel intermediate metabolite results in formation of the active metabolite, a thiol derivative of clopidogrel. The active metabolite is formed mostly by CYP2C19 with contributions from several other CYP enzymes, including CYP1A2, CYP2B6 and CYP3A4. The active thiol metabolite which has been isolated in vitro, binds rapidly and irreversibly to platelet receptors, thus inhibiting platelet aggregation.

 

The Cmax of the active metabolite is twice as high following a single 300-mg clopidogrel loading dose as it is after four days of 75-mg maintenance dose. Cmax occurs approximately 30 to 60 minutes after dosing.

 

Elimination

Following an oral dose of 14C-labelled clopidogrel in man, approximately 50% was excreted in the urine and approximately 46% in the faeces in the 120-hour interval after dosing. After a single oral dose of 75 mg, clopidogrel has a half-life of approximately 6 hours. The elimination half-life of the main circulating (inactive) metabolite was 8 hours after single and repeated administration.

 

Pharmacogenetics

CYP2C19 is involved in the formation of both the active metabolite and the 2-oxo-clopidogrel intermediate metabolite. Clopidogrel active metabolite pharmacokinetics and antiplatelet effects, as measured by ex vivo platelet aggregation assays, differ according to CYP2C19 genotype.

 

The CYP2C19*1 allele corresponds to fully functional metabolism while the CYP2C19*2 and CYP2C19*3 alleles are nonfunctional. The CYP2C19*2 and CYP2C19*3 alleles account for the majority of reduced function alleles in Caucasian (85%) and Asian (99%) poor metabolizers. Other alleles associated with absent or reduced metabolism are less frequent and include CYP2C19*4, *5,

*6, *7, and *8. A patient with poor metabolizer status will possess two loss-of-function alleles as defined above. Published frequencies for the poor CYP2C19 metabolizer genotypes are approximately 2% for Caucasians, 4% for Blacks and 14% for Chinese. Tests are available to determine a patient's CYP2C19 genotype.

 

A crossover study in 40 healthy subjects, 10 each in the four CYP2C19 metabolizer groups (ultrarapid, extensive, intermediate and poor), evaluated pharmacokinetic and antiplatelet responses using 300 mg followed by 75 mg/day and 600 mg followed by 150 mg/day, each for a total of 5 days (steady state). No substantial differences in active metabolite exposure and mean inhibition of platelet aggregation (IPA) were observed between ultrarapid, extensive and intermediate metabolizers. In poor metabolizers, active metabolite exposure was decreased by 63-71% compared to extensive metabolizers. After the 300 mg/75 mg dose regimen, antiplatelet responses were decreased in the poor metabolizers with mean IPA (5 μM ADP) of 24% (24 hours) and 37% (Day 5) as compared to IPA of 39% (24 hours) and 58% (Day 5) in the extensive metabolizers and 37% (24 hours) and 60% (Day 5) in the intermediate metabolizers. When poor metabolizers received the 600 mg/150 mg regimen, active metabolite exposure was greater than with the 300 mg/75 mg regimen.

In addition, IPA was 32% (24 hours) and 61% (Day 5), which were greater than in the poor metabolizers receiving the 300 mg/75 mg regimen, and were similar to the other CYP2C19 metabolizer groups receiving the 300 mg/75 mg regimen. An appropriate dose regimen for this patient population has not been established in clinical outcome trials.

 

Consistent with the above results, in a meta-analysis including 6 studies of 335 clopidogrel-treated subjects at steady state, it was shown that active metabolite exposure was decreased by 28% for intermediate metabolizers, and 72% for poor metabolizers while platelet aggregation inhibition (5 μM ADP) was decreased with differences in IPA of 5.9% and 21.4%, respectively, when compared to extensive metabolizers.

 

The influence of CYP2C19 genotype on clinical outcomes in patients treated with clopidogrel has not been evaluated in prospective, randomized, controlled trials. There have been a number of retrospective analyses, however, to evaluate this effect in patients treated with clopidogrel for whom there are genotyping results: CURE (n=2721), CHARISMA (n=2428), CLARITY-TIMI 28 (n=227), TRITON-TIMI 38 (n=1477), and ACTIVE-A (n=601), as well as a number of published cohort studies.

 

In TRITON-TIMI 38 and 3 of the cohort studies (Collet, Sibbing, Giusti) the combined group of patients with either intermediate or poor metabolizer status had a higher rate of cardiovascular events (death, myocardial infarction, and stroke) or stent thrombosis compared to extensive metabolizers.

 

In CHARISMA and one cohort study (Simon), an increased event rate was observed only in poor metabolizers when compared to extensive metabolizers.

 

In CURE, CLARITY, ACTIVE-A and one of the cohort studies (Trenk), no increased event rate was observed based on metabolizer status.

None of these analyses were adequately sized to detect differences in outcome in poor metabolizers.

 

Special populations

The pharmacokinetics of the active metabolite of clopidogrel is not known in these special populations.

 

Renal impairment

After repeated doses of 75 mg clopidogrel per day in subjects with severe renal disease (creatinine clearance from 5 to 15 ml/min), inhibition of ADP-induced platelet aggregation was lower (25%) than that observed in healthy subjects, however, the prolongation of bleeding time was similar to that seen in healthy subjects receiving 75 mg of clopidogrel per day. In addition, clinical tolerance was good in all patients.

 

Hepatic impairment

After repeated doses of 75 mg clopidogrel per day for 10 days in patients with severe hepatic impairment, inhibition of ADP-induced platelet aggregation was similar to that observed in healthy subjects. The mean bleeding time prolongation was also similar in the two groups.

 

Race

The prevalence of CYP2C19 alleles that result in intermediate and poor CYP2C19 metabolism differs according to race/ethnicity (see Pharmacogenetics). From literature, limited data in Asian populations are available to assess the clinical implication of genotyping of this CYP on clinical outcome events.


During non-clinical studies in rat and baboon, the most frequently observed effects were liver changes. These occurred at doses representing at least 25 times the exposure seen in humans receiving the clinical dose of 75 mg/day and were a consequence of an effect on hepatic metabolizing enzymes. No effect on hepatic metabolizing enzymes was observed in humans receiving clopidogrel at the therapeutic dose.

 

At very high doses, a poor gastric tolerability (gastritis, gastric erosions and/or vomiting) of clopidogrel was also reported in rat and baboon.

 

There was no evidence of carcinogenic effect when clopidogrel was administered for 78 weeks to mice and 104 weeks to rats when given at doses up to 77 mg/kg per day (representing at least 25 times the exposure seen in humans receiving the clinical dose of 75 mg/day).

 

Clopidogrel has been tested in a range of in vitro and in vivo genotoxicity studies, and showed no genotoxic activity.

 

Clopidogrel was found to have no effect on the fertility of male and female rats and was not teratogenic in either rats or rabbits. When given to lactating rats, clopidogrel caused a slight delay in the development of the offspring. Specific pharmacokinetic studies performed with radiolabeled clopidogrel have shown that the parent compound or its metabolites are excreted in the milk.

Consequently, a direct effect (slight toxicity), or an indirect effect (low palatability) cannot be excluded.


Core:

Mannitol (E421) Macrogol 6000

Microcrystalline cellulose Hydrogenated castor oil

Low substituted hydroxypropylcellulose

 

Coating:

Hypromellose (E464)

Lactose monohydrate

Triacetin (E1518)

Titanium dioxide (E171)

Red iron oxide (E172)

 

Polishing agent:

Carnauba wax


None Applicable


18 months

Store below 30°C.


 

Strength

Unit Count or Fill Size

 

Container Size(s)

 

Description

 

75 mg

 

30’s (3

Blisters containing 10 tablets each)

 

Blisters

Foil Silver Plain 205 MM 25 urn

Dull silver on one side, shiny silver on other.

Rolled material approximately 205 mm wide.

Cold Formable Foil 205 MM

Dull silver on one side, shiny silver on other.

Rolled material approximately 205 mm wide.


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


Apotex Incorporated 150 Signet Drive, Toronto, Ontario Canada, M9L 1T9 Tel: 1‐800‐268‐4623, Fax: 1‐800‐609‐9444 www.apotex.com

03/2019
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