Search Results
| نشرة الممارس الصحي | نشرة معلومات المريض بالعربية | نشرة معلومات المريض بالانجليزية | صور الدواء | بيانات الدواء |
|---|
What Brevie is
Brevie contains the active substance brivaracetam. It belongs to a group of medicines called ‘anti-epileptics’. These medicines are used to treat epilepsy.
What Brevie is used for
· Brevie is used in adults, adolescents and children from 2 years of age.
· It is used to treat a type of epilepsy that has partial seizures with or without a secondary generalisation.
· Partial seizures are fits that start by only affecting one side of the brain. These partial seizures can spread and extend to larger areas on both sides of the brain – this is called a ‘secondary generalisation’.
· You have been given this medicine to lower the number of fits (seizures) you have.
· Brevie is used together with other medicines for epilepsy.
Do not use Brevie if:
· You are allergic to brivaracetam, other similar chemical compounds as levetiracetam or piracetam or any of the other ingredients of this medicine (listed in section 6). If you are not sure, talk to your doctor or pharmacist before taking Brevie.
Warnings and precautions
Talk to your doctor or pharmacist before using Brevie if:
· You have thoughts of harming or killing yourself. A small number of people being treated with anti-epileptic medicines such as brivaracetam have had thoughts of harming or killing themselves. If you have any of these thoughts at any time, contact your doctor immediately.
· You have liver problems - your doctor may need to adjust your dose.
Children
Brevie is not recommended for use in children under 2 years of age.
Other medicines and Brevie
Tell your doctor or pharmacist if you are taking, have recently taken or might take any other medicines.
In particular, tell your doctor if you are taking any of the following medicines – this is because your doctor may need to adjust your Brevie dose:
· Rifampicin - a medicine used to treat bacterial infections.
· St John’s wort (also known as Hypericum perforatum) - a herbal medicine used to treat depression and anxiety as well as other conditions.
Brevie with alcohol
· Combining this medicine with alcohol is not recommended.
· If you drink alcohol while taking Brevie the negative effects of alcohol may be increased.
Pregnancy and breast-feeding
Fertile women should discuss the use of contraceptives with the doctor.
If you are pregnant or breast-feeding, think you may be pregnant or planning to have a baby, ask your doctor or pharmacist for advice before taking this medicine.
It is not recommended to take Brevie if you are pregnant, as the effects of brivaracetam on pregnancy and the unborn baby are not known.
It is not recommended to breast-feed your baby while taking Brevie, as brivaracetam passes into breast milk.
Do not stop treatment without talking to your doctor first. Stopping treatment could increase your seizures and harm your baby.
Driving and using machines
· You may feel sleepy, dizzy or tired while taking Brevie.
· These effects are more likely at the start of the treatment or after a dose increase.
· Do not drive, cycle or use any tools or machines until you know how the medicine affects you.
Brevie contains sodium
BrevieThis medicine contains 21.18 mg sodium (main component of cooking/table salt) in each vial. This is equivalent to 1% of the recommended maximum daily dietary intake of sodium for an adult.
Always use this medicine exactly as your doctor has told you. Check with your doctor or pharmacist if you are not sure.
You will use Brevie together with other medicines for epilepsy.
· When you start taking this medicine you will take it either orally (as tablets or an oral solution) or be given it as an injection or infusion.
· Brevie solution for injection/infusion is used for a short amount of time when you cannot take brivaracetam orally.
· You can switch between taking brivaracetam orally to the solution for injection/infusion, and the other way around.
How much you will be given
Your doctor will work out the right daily dose for you. Take the daily dose in two equally divided doses, approximately 12 hours apart.
Adolescents and children weighing 50 kg or more, and adults
· The recommended dose is from 25 mg to 100 mg taken twice a day. Your doctor may then decide to adjust your dose to find the best dose for you.
Adolescents and children weighing from 20 kg to less than 50 kg
· Your doctor may prescribe the injection only for a few days if you cannot take your medicine by mouth.
· The recommended dose is from 0.5 mg to 2 mg for each kg of bodyweight, taken twice a day. Your doctor may then decide to adjust your dose to find the best dose for you.
Children weighing from 10 kg to less than 20 kg
· Your child’s doctor may prescribe the injection only for a few days if your child cannot take the medicine by mouth.
· The recommended dose is from 0.5 mg to 2.5 mg for each kg of bodyweight, taken twice a day. Your child’s doctor may then decide to adjust the dose to find the best dose for your child.
People with liver problems
If you have problems in the liver:
· As an adolescent or child weighing 50 kg or more, or as an adult, the maximum dose you will take is 75 mg twice a day.
· As an adolescent or child weighing from 20 kg to less than 50 kg, the maximum dose you will take is 1.5 mg for each kg of bodyweight twice a day.
· As a child weighing from 10 kg to less than 20 kg, the maximum dose your child will take is 2 mg for each kg of bodyweight twice a day.
How Brevie is given
Brevie is administered as an injection or infusion into a vein by a doctor or a nurse. The medicine is injected slowly into your vein or given as an infusion (drip) over 15 minutes.
How long to use Brevie for
· Your doctor will decide for how many days you will be given the injections or infusion.
· For the long term treatment with Brevie, your doctor will ask to you to take brivaracetam tablets or oral solution.
If you have more Brevie than you should
If you think you have been given too much Brevie, tell your doctor straight away.
If you stop using Brevie
· Do not stop taking this medicine unless your doctor tells you to. This is because stopping treatment could increase the number of fits you have.
· If your doctor asks you to stop taking this medicine they will lower your dose gradually. This helps to stop your fits coming back or getting worse.
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.
Very common: may affect more than 1 in 10 people
· Feeling sleepy or dizzy
Common: may affect up to 1 in 10 people
· Flu
· Feeling very tired (fatigue)
· Convulsion, a feeling of ‘spinning’ (vertigo)
· Feeling and being sick, constipation
· Pain or discomfort at the injection or infusion site
· Depression, anxiety, not being able to sleep (insomnia), irritability
· Infections of the nose and throat (such as the ‘common cold’), cough
· Decreased appetite
Uncommon: may affect up to 1 in 100 people
· Allergic reactions
· Abnormal thinking and/or loss of touch with reality (psychotic disorder), being aggressive, nervous excitement (agitation)
· Thoughts or attempts of harming or killing yourself: tell your doctor straight away
· A decrease in white blood cells (called ‘neutropenia’) - shown in blood tests
Additional side effects in children
Common: may affect up to 1 in 10 people
· Restlessness and hyperactivity (psychomotor hyperactivity)
Reporting of side effects
If any of the side effects gets serious, or if you notice any side effects not listed in this leaflet, please tell your <doctor, health care provider> <or> <pharmacist>.
To report any side effect(s):
If you get any side effects, talk to your doctor, pharmacist or nurse. This includes any possible side effects not listed in this leaflet. You can also report side effects directly via below. By reporting side effects you can help provide more information on the safety of this medicine.
· Saudi Arabia:
The National Pharmacovigilance Centre (NPC):
SFDA Call Center: 19999
E-mail: npc.drug@sfda.gov.sa
Website: https://ade.sfda.gov.sa
· UAE:
Pharmacovigilance & Medical Device section
P.O.Box: 1853
Tel: 80011111
Email : pv@mohap.gov.ae
Drug Department
Ministry of Health & Prevention
Dubai
· Other GCC States:
Please contact the relevant competent authority.
………………………………………………………………………………………
The following information is intended for medical or healthcare professionals only
Brevie solution for injection/infusion can be administered as a bolus injection or as an infusion:
· Intravenous bolus: may be administered directly without dilution
· Intravenous infusion: may be administered over 15 minutes in a compatible diluent
Brevie may be diluted with the following solutions: 9 mg/ml (0.9%) sodium chloride, 50 mg/ml (5%) glucose solution for injection or lactated Ringer’s solution.
Each vial of Brevie solution for injection/infusion must be used only once (single use). Any unused solution should be discarded (see section 3).
This is a Medicament · Medicament is a product which affects your health and its consumption contrary to instructions is dangerous for you. · Follow strictly the doctor’s prescription, the method of use and the instructions of the pharmacist who sold the medicament. · The doctor and the pharmacist are the experts in medicines, their benefits and risks. · Do not by yourself interrupt the period of treatment prescribed for you. · Do not repeat the same prescription without consulting your doctor. · Keep all medicaments out of reach of children. |
Council of Arab Health Ministers
Union of Arab Pharmacists
Keep this medicine out of the sight and reach of children.
Do not store above 30˚C.
Brevie may be diluted before it is injected by your doctor or nurse. In such cases, it should be used straight after dilution.
This medicinal product does not require any special storage conditions.
Each vial of Brevie solution for injection/infusion must be used only once (single use). Any unused solution should be discarded.
Only clear solution free from particles and discoloration should be used.
Do not use this medicine after the expiry date which is stated on the carton after EXP. The expiry date refers to the last day of that month.
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 protect the environment.
The active substance is brivaracetam.
Each ml of Brevie 50 mg/5 ml Solution for Injection/Infusion contains 10 mg brivaracetam.
The other ingredients are sodium chloride, sodium acetate trihydrate, glacial acetic acid, water for injection and nitrogen.
Marketing Authorization Holder and Manufacturer
Marketing Authorization Holder
Sudair Pharma Company (SPC)
King Fahad Road – King Fahad District, Building no. 7639
P.O. Box 12262 Riyadh, Saudi Arabia
Tel: +966-11-920001432
Fax: +966-11-4668195
Email: info@sudairpharma.com
Manufacturer
MSN Laboratories Private Limited,
Formulations Division, Unit-II,
Sy. No. 1277 & 1319 to 1324,
Nandigama (Village & Mandal),
Rangareddy District, Pin Code. 509228,
Telangana, India
يحتوي بريفي على المادة الفعالة بريفاراسيتام. ينتمي إلى مجموعة من الأدوية تدعى ’الأدوية المضادة للصرع‘. تستخدم هذه الأدوية لعلاج الصرع.
دواعي استخدام بريفي
• يستخدم بريفي لدى البالغين، المراهقين والأطفال بعمر عامين و أكثر.
• يستخدم لعلاج نوع من الصرع الذي يحدث فيه تشنجات جزئية مع أو بدون تعيمم ثانوي.
• تشنجات الصرع الجزئية هي نوبات تبدأ من خلال التأثير على جهة واحدة فقط من المخ. يمكن أن تنتشر هذه التشنجات الجزئية وتمتد إلى مناطق أكبر في كلا جانبي المخ- يسمى هذا ’التعميم الثانوي‘.
• تم إعطاؤك هذا الدواء لخفص عدد النوبات (التشنجات) التي تحدث لك.
• يستخدم بريفي بالتزامن مع أدوية أخرى لعلاج الصرع.
لا تستخدم بريفي إذا:
• كان لديك حساسية من بريفاراسيتام أو أي مركبات كيميائية مشابهة مثل ليفيتيراسيتام أو بيراسيتام أو أي مكون آخر من مكونات هذا الدواء (المدرجة في القسم 6). إذا لم تكن متأكداً، تحدث مع طبيبك أو الصيدلي قبل أخذ بريفاراسيتام.
الاحتياطات والتحذيرات
تحدث إلى طبيبك أو الصيدلي قبل استخدام بريفي إذا:
• كان لديك أفكار لإيذاء نفسك أو قتلها. حيث ظهرت لدى عدد قليل من الأشخاص الذين يعالجون بالأدوية المضادة للصرع مثل بريفاراسيتام أفكار لإيذاء أو قتل أنفسهم. إذا كانت لديك أي من هذه الأفكار في أي وقت، فتواصل مع طبيبك فوراً.
• كان لديك مشاكل في الكبد حيث قد يحتاج طبيبك إلى تعديل جرعتك.
الأطفال
لا ينصح باستخدام بريفي لدى الأطفال بعمر أقل من عامين.
الأدوية الأخرى وبريفي
أخبر طبيبك أو الصيدلي إذا كنت تأخذ، أخذت مؤخرًا أو قد تأخذ أي أدوية أخرى.
بشكل خاص، أخبر طبيبك إذا كنت تتناول أي من الأدوية التالية – لأن طبيبك قد يحتاج إلى تعديل جرعة بريفي الخاصة بك:
• ريفامبيسين – دواء يستخدم لعلاج العدوى البكتيرية.
• عشبة القديس يوحنا (المعروفة أيضاً بـهايبيريكوم بيرفوراتم) و هى عبارة عن دواء عشبي يستخدم لعلاج الاكتئاب والقلق بالإضافة لحالات أخرى.
استخدام بريفي مع الكحول
• لا ينصح بدمج هذا الدواء مع الكحول.
• إذا كنت تشرب الكحول أثناء أخذ بريفي فقد تزداد الآثار السلبية للكحول لديك.
الحمل والرضاعة
يجب على النساء في سن الإنجاب مناقشة استخدام موانع الحمل مع الطبيب.
إذا كنت حاملاً أو تمارسين الرضاعة الطبيعية ، تعتقدين أنك حامل أو تخططين لإنجاب طفل، استشيري طبيبك أو الصيدلي قبل أخذ هذا الدواء.
لا ينصح بأخذ بريفي إذا كنت حاملاً، حيث أن تأثيرات بريفاراسيتام على الحمل والجنين غير معروفة.
لا ينصح بإرضاع طفلك طبيعيًا أثناء أخذ بريفي، حيث أن بريفاراسيتام يعبر في حليب الثدي.
لا تتوقفى عن العلاج دون التحدث مع طبيبك أولاً. قد يؤدي إيقاف العلاج إلى زيادة تشنجاتك وإلحاق الضرر بالرضيع.
القيادة واستخدام الآلات
• قد تشعر بالنعاس، الدوخة أو التعب أثناء أخذ بريفي.
• تزداد احتمالية حدوث هذه التأثيرات في بداية العلاج أو بعد زيادة الجرعة.
• لا تقم بالقيادة، ركوب الدراجة أو استخدام أي أدوات أو آلات حتى تعرف كيف يؤثر الدواء عليك.
يحتوي بريفي على الصوديوم
يحتوي بريفي على الصوديوم. يحتوي هذا الدواء على 21.18 ملغم صوديوم (المكون الرئيسي لملح الطبخ/الطعام) في كل قارورة. هذا يكافئ 1% من الكمية الغذائية اليومية القصوى من الصوديوم الموصى بها للبالغين.
احرص دائمًا على استخدام هذا الدواء تمامًا كما أخبرك طبيبك. استشر طبيبك أو الصيدلي إذا لم تكن متأكدًا.
سوف تستخدم بريفي مع أدوية أخرى لعلاج الصرع.
• عندما تبدأ بأخذ هذا الدواء سوف تأخذ بريڨاراسيتام إما عن طريق الفم (على شكل أقراص أو محلول فموي) أو سوف يعطى لك على شكل حقنة أو تنقيط وريدى.
• يستخدم محلول بريفي للحقن/للتنقيط الوريدى لمدة قصيرة من الزمن عندما لا تستطيع أخذ بريفاراسيتام عن طريق الفم.
• يمكنك الانتقال من أخذ بريفاراسيتام عن طريق الفم إلى المحلول المخصص للحقن/للتنقيط الوريدى، وبالعكس.
الكمية التي سوف تعطى لك
سيحدد طبيبك الجرعة اليومية المناسبة لك. خذ الجرعة اليومية مقسمة على جرعتين متساويتين، بفاصل 12 ساعة تقريبًا.
المراهقون والأطفال الذين يزنون 50 كلغم فأكثر، والبالغون
• الجرعة الموصى بها هي من 25 ملغم إلى 100 ملغم تؤخذ مرتين في اليوم. قد يقرر طبيبك بعد ذلك تعديل جرعتك للعثور على أفضل جرعة لك.
المراهقون والأطفال الذين يتراوح وزنهم بين 20 كلغم إلى أقل من 50 كلغم
• قد يصف لك طبيبك الحقنة فقط لأيام قليلة إذا لم تستطع أخذ الدواء عن طريق الفم.
• الجرعة الموصى بها هي من 0,5 ملغم إلى 2 ملغم لكل كلغم من وزن الجسم تؤخذ مرتين في اليوم. قد يقرر طبيبك بعد ذلك تعديل جرعتك للعثور على أفضل جرعة لك.
الأطفال الذين يتراوح وزنهم بين 10 كلغم إلى أقل من 20 كلغم
• قد يصف طبيب طفلك الحقنة فقط لأيام قليلة إذا لم يستطع طفلك أخذ الدواء عن طريق الفم.
• الجرعة الموصى بها هي من 0,5 ملغم إلى 2,5 ملغم لكل كلغم من وزن الجسم تؤخذ مرتين في اليوم. قد يقرر طبيب طفلك بعد ذلك تعديل الجرعة للعثور على أفضل جرعة لطفلك.
الأشخاص الذين يعانون من مشاكل في الكبد
إذا كان هناك مشاكل في الكبد:
• كمراهق أو كطفل يزن 50 كلغم أو أكثر، أو كشخص بالغ، فإن الحد الأقصى للجرعة التي ستأخذها هو 75 ملغم مرتين في اليوم.
• كمراهق أو كطفل يزن من 20 كلغم إلى أقل من 50 كلغم، فإن الحد الأقصى للجرعة التي ستأخذها هو 1,5 ملغم لكل كلغم من وزن الجسم مرتين في اليوم.
• كطفل يزن من 10 كلغم إلى أقل من 20 كلغم، فإن الحد الأقصى للجرعة التي سيأخذها طفلك هو 2 ملغم لكل كلغم من وزن الجسم مرتين في اليوم.
كيفية إعطاء بريفي
يتم إعطاء بريفي كحقنة أو تنقيط في الوريد بواسطة طبيب أو ممرض. يتم حقن الدواء ببطء في وريدك أو يتم تنقيطه (بالتنقيط) على فترة 15 دقيقة.
مدة استخدام بريفي
• سيقرر طبيبك عدد الأيام التي سيتم فيها إعطاؤك الحقن أو التنقيط الوريدى.
• بالنسبة للعلاج طويل الأمد ببريفي، سيطلب منك طبيبك أخذ أقراص بريفاراسيتام أو المحلول الفموي.
إذا أخذت بريفي أكثر مما ينبغي
إذا اعتقدت أنه قد تم إعطاؤك بريفي أكثر مما ينبغي، أخبر طبيبك فوراً.
إذا توقفت عن استخدام بريفي
• لا تتوقف عن أخذ هذا الدواء إلا إذا أخبرك طبيبك بذلك. وذلك لأن التوقف عن العلاج قد يزيد من عدد النوبات التي تعاني منها.
• إذا طلب منك طبيبك التوقف عن أخذ هذا الدواء، فسيقوم بتخفيض جرعتك تدريجياً. هذا يساعد على منع نوباتك من العودة أو أن تزداد سوءًا.
إذا كان لديك أي أسئلة إضافية عن استخدام هذا الدواء، استشر طبيبك أو الصيدلي.
كما هو الحال في كل الأدوية، هذا الدواء يمكن أن يتسبب بأعراض جانبية، بالرغم من أنها قد لا تحدث للجميع.
شائعة جدًا: قد تصيب أكثر من شخص واحد من كل 10 أشخاص
• الشعور بالنعاس أو الدوخة
شائعة: قد تصيب ما يصل إلى شخص واحد من كل 10 أشخاص
• أنفلونزا
• الشعور بالتعب الشديد (الإرهاق)
• تشنج، شعور ’بالدوار‘ (الدوران)
• الغثيان والقيء، الإمساك
• الألم أو الشعور بعدم الارتياح في موضع الحقن أو التنقيط الوريدى
• الاكتئاب، القلق، عدم القدرة على النوم (الأرق)، التهيج
• التهابات الأنف والحنجرة (مثل ’نزلات البرد‘)، السعال
• انخفاض الشهية
غير شائعة: (قد تصيب ما يصل إلى شخص واحد من كل 100 شخص)
• ردود الفعل التحسسية (حساسية)
• التفكير غير الطبيعي و/أو فقدان الاتصال بالواقع (اضطراب ذهاني)، العدوانية، إثارة عصبية (التهيج)
• أفكار أو محاولات لإيذاء نفسك أو قتلها: أخبر طبيبك على الفور
• انخفاض في خلايا الدم البيضاء (تسمى ’قلة العدلات‘) - يظهر في اختبارات الدم
آثار جانبية إضافية في الأطفال
شائعة: قد تصيب ما يصل إلى شخص واحد من كل 10 أشخاص
• التململ وفرط النشاط (فرط النشاط الحركي الذهني)
الإبلاغ عن الآثار الجانبية
إن كان لديك أعراض جانبية أو لاحظت أعراض جانبية غير مذكورة في هذه النشرة، فضلًا ابلغ <طبيبك، أو مقدم الرعاية الصحية> <أو> <الصيدلي>.
الإبلاغ عن الآثار الجانبية
إذا أصبت بأي آثار جانبية، تحدث إلى طبيبك، الصيدلي أو الممرض. يشمل هذا أي آثار جانبية محتملة لم يتم ذكرها في هذه النشرة. يمكنك أيضاً الإبلاغ عن الآثار الجانبية مباشرة من خلال المذكور أدناه. من خلال الإبلاغ عن الآثار الجانبية يمكنك المساعدة في توفير المزيد من المعلومات حول سلامة هذا الدواء.
• المملكة العربية السعودية:
المركز الوطني للتيقظ الدوائي :
مركز الاتصال الموحد: 19999
البريد الإلكتروني: npc.drug@sfda.gov.sa
الموقع الإلكتروني: https://ade.sfda.gov.sa
• الإمارات العربية المتحدة:
قطاع اليقظة الدوائية والجهاز الطبي
صندوق بريد 1853
هاتف: 80011111
البريد الإلكتروني: pv@mohap.gov.ae
قسم الدواء
وزارة الصحة والوقاية
دبي
• دول الخليج العربي الأخرى:
الرجاء الاتصال بالجهات الوطنية في كل دولة.
.........................................................................................
المعلومات التالية مقدمة لمتخصصي الرعاية الطبية أوالصحية فقط
يمكن إعطاء محلول بريفي للحقن/للتنقيط الوريدى كحقنة كاملة أو عن طريق التنقيط الوريدى:
• حقنة كاملة في الوريد: يمكن إعطاؤها مباشرة دون تخفيف
• التنقيط في الوريد: يمكن إعطاؤه على فترة 15 دقيقة في مادة مخففة متوافقة
يمكن تخفيف بريفي بالمحاليل التالية: محلول كلوريد الصوديوم بتركيز 9 ملغم/مللتر (0,9٪) ، محلول جلوكوز للحقن برؤكيز 50 ملغم/مللتر (5٪) أو محلول رينجر اللاكتاتي.
يجب استخدام كل قارورة من محلول بريفي للحقن/للتنقيط الوريدى مرة واحدة فقط (استخدام واحد). يجب التخلص من أي محلول غير مستخدم (راجع القسم 3).
هذا مستحضر دوائي • الدواء مستحضر يؤثر على صحتك واستهلاكه خلافًا للتعليمات يعرضك للخطر. • اتبع بدقة وصفة الطبيب، وطريقة الاستعمال المنصوص عليها، وتعليمات الصيدلي الذي صرفها لك. • الطبيب والصيدلي هما الخبيران في الدواء، وفي نفعه وضرره. • لا تقطع مدة العلاج المحددة لك من تلقاء نفسك. • لا تكرر صرف الدواء بدون استشارة الطبيب المختص. • لا تترك الأدوية في متناول الاطفال. |
مجلس وزراء الصحة العرب
واتحاد الصيادلة العرب
احفظ هذا الدواء بعيداً عن مرأى ومتناول الأطفال.
لا يحفظ عند درجة حرارة أعلى من 30° مئوية.
قد يتم تخفيف دواء بريفي قبل حقنه من قبل طبيبك أو الممرض. في مثل هذه الحالات، يجب استخدامه مباشرة بعد التخفيف.
لا يتطلب هذا المستحضر الدوائي أي شروط تخزين خاصة.
يجب استخدام كل قارورة من محلول بريفي للحقن/للتنقيط الوريدى مرة واحدة فقط (استخدام واحد). يجب التخلص من أي محلول غير مستخدم.
يجب فقط استخدام المحلول الصافي الخالي من الجزيئات وتغير اللون.
لا تستخدم هذا الدواء بعد تاريخ انتهاء الصلاحية المذكور على العبوة الكرتونية بعد EXP. يشير تاريخ انتهاء الصلاحية إلى اليوم الأخير من ذلك الشهر.
لا تتخلص من اي أدوية عن طريق مياه الصرف الصحي أو النفايات المنزلية. اسأل الصيدلي عن طريقة التخلص من الأدوية التي لم تعد تستخدمها. هذه الإجراءات ستساعد في الحفاظ على سلامة البيئة.
المادة الفعالة هي بريفاراسيتام.
يحتوي كل مللتر من بريفي 50 ملغم/5 مللتر محلول للحقن/للتنقيط الوريدى على 10 ملغم بريفاراسيتام.
المواد الأخرى هي: كلوريد الصوديوم، أسيتات الصوديوم ثلاثي الماء، حمض الأسيتيك الجليدي، ماء معد للحقن ونيتروجين.
بريفي 50 ملغم/5 مللتر محلول للحقن/للتنقيط الوريدى هو محلول صافي عديم اللون خالي من الجزيئات المرئية معبأ في زجاجات بحجم 10 مللتر من النوع رقم واحد شفافة عديمة اللون مع أغطية مطاطية بحجم 20 مم ومحكمة الإغلاق بسدادات من الألمنيوم بحجم 20 مم لها أقراص من متعدد البروبيلين زرقاء اللون.
حجم العبوة: قارورة واحدة(5 مللتر).
مالك رخصة التسويق والشركة المصنّعة:
مالك رخصة التسويق
شركة سدير فارما،
طريق الملك فهد – مقاطعة الملك فهد، بناية رقم 7639،
صندوق بريد 12262 الرياض، السعودية
هاتف: 920001432-11-966+
فاكس: 4668195-11-966+
البريد الإلكتروني: info@sudairpharma.com
الشركة المصنّعة
مختبرات إم إس إن الخاصة المحدودة،
قسم التطوير، وحدةII ،
سي رقم 1277 و1319 إلى 1324،
نانديغاما (قرية وماندال)،
مقاطعة رانجاريدي، الرمز 509228،
تيلانغانا، الهند
Solution for Injection/Infusion.
Brevie 50 mg/5 ml Solution for Injection/Infusion is a clear colorless solution free from visible particles.
Posology
Brivaracetam solution for injection/infusion is an alternative route of administration for patients when oral administration is temporarily not feasible. There is no experience with twice daily intravenous administration of brivaracetam for a period longer than 4 days.
The recommended posology for adults, adolescents and children from 2 years of age is summarised in the following table. The dose should be administered in two equally divided doses, approximately 12 hours apart.
Recommended starting dose | Recommended maintenance dose | Therapeutic dose range* |
Adolescents and children weighing 50 kg or more, and adults | ||
50 mg/day (or 100 mg/day)** | 100 mg/day | 50 - 200 mg/day |
Adolescents and children weighing from 20 kg to less than 50 kg | ||
1 mg/kg/day (up to 2 mg/kg/day)** | 2 mg/kg/day | 1 – 4 mg/kg/day |
Children weighing from 10 kg to less than 20 kg | ||
1 mg/kg/day (up to 2.5 mg/kg/day)** | 2.5 mg/kg/day | 1 – 5 mg/kg/day |
* Based on individual patient response, the dose may be adjusted within this effective dose range.
** Based on physician's assessment of need for seizure control
Adults
Brivaracetam may be initiated with either intravenous or oral administration. When converting from oral to intravenous administration or vice versa, the total daily dose and frequency of administration should be maintained.
The recommended starting dose is either 50 mg/day or 100 mg/day based on physician's assessment of required seizure reduction versus potential side effects. Based on individual patient response and tolerability, the dose may be adjusted in the effective dose range of 50 mg/day to 200 mg/day.
Adolescents and children weighing 50 kg or more
The recommended starting dose is 50 mg/day. Brivaracetam may also be initiated at 100 mg/day based on physician's assessment of need for seizure control. The recommended maintenance dose is 100 mg/day. Based on individual patient response, the dose may be adjusted in the effective dose range of 50 mg/day to 200 mg/day.
Adolescents and children weighing from 20 kg to less than 50 kg
The recommended starting dose is 1 mg/kg/day. Brivaracetam may also be initiated at doses up to 2 mg/kg/day based on physician's assessment of need for seizure control. The recommended maintenance dose is 2 mg/kg/day. Based on individual patient response, the dose may be adjusted in the effective dose range of 1 mg/kg/day to 4 mg/kg/day.
Children weighing from 10 kg to less than 20 kg
The recommended starting dose is 1 mg/kg/day. Brivaracetam may also be initiated at doses up to 2.5 mg/kg/day based on physician's assessment of need for seizure control. The recommended maintenance dose is 2.5 mg/kg/day. Based on individual patient response, the dose may be adjusted in the effective dose range of 1 mg/kg/day to 5 mg/kg/day.
Missed doses
If patients missed one dose or more, it is recommended that they take a single dose as soon as they remember and take the following dose at the usual morning or evening time. This may avoid the brivaracetam plasma concentration falling below the efficacy level and prevent breakthrough seizures from occurring.
Discontinuation
For patients from 16 years of age, if brivaracetam has to be discontinued, it is recommended that the dose is reduced gradually by 50 mg/day on a weekly basis.
For patients below the age of 16 years, if brivaracetam has to be discontinued, it is recommended that the dose is reduced by a maximum of half the dose every week until a dose of 1 mg/kg/day (for patients with a body weight less than 50 kg) or 50 mg/day (for patients with body weight of 50 kg or more) is reached.
After 1 week of treatment at 50 mg/day, a final week of treatment at the dose of 20 mg/day is recommended.
Special populations
Elderly (65 years of age and above)
No dose adjustment is needed in elderly patients (see section 5.2).
The clinical experience in patients ≥ 65 years is limited.
Renal impairment
No dose adjustment is needed in patients with impaired renal function (see section 5.2). Brivaracetam is not recommended in end-stage renal disease patients undergoing dialysis due to lack of data.
Based on data in adults, no dose adjustment is necessary in paediatric patients with impaired renal function. No clinical data are available in paediatric patients with renal impairment.
Hepatic impairment
Exposure to brivaracetam was increased in adult patients with chronic liver disease.
In patients with hepatic impairment, the following adjusted doses, administered in 2 divided doses, approximately 12 hours apart, are recommended for all stages of hepatic impairment (see sections 4.4 and 5.2). No clinical data are available in paediatric patients with hepatic impairment.
Age and body weight | Recommended starting dose | Recommended maximum daily dose |
Adolescents and children weighing 50 kg or more, and adults | 50 mg/day | 150 mg/day |
Adolescents and children weighing from 20 kg to less than 50 kg | 1 mg/kg/day | 3 mg/kg/day |
Children weighing from 10 kg to less than 20 kg | 1 mg/kg/day | 4 mg/kg/day |
Paediatric patients less than 2 years of age
The efficacy of brivaracetam in paediatric patients aged less than 2 years has not yet been established.
Currently available data are described in section 4.8, 5.1, and 5.2 but no recommendation on a posology can be made.
Method of administration
· Intravenous bolus: brivaracetam may be administered as an intravenous bolus without dilution.
· Intravenous infusion: brivaracetam may be diluted in a compatible diluent and administered as a 15-minute intravenous infusion (see section 6.6). This medicinal product must not be mixed with other medicinal products.
Brivaracetam bolus injection or intravenous infusion has not been studied in acute conditions; e.g. status epilepticus and is therefore not recommended for such conditions.
Suicidal ideation and behaviour
Suicidal ideation and behaviour have been reported in patients treated with anti-epileptic drugs (AEDs), including brivaracetam, in several indications. A meta-analysis of randomized placebo-controlled clinical studies of AEDs has also shown a small increased risk of suicidal ideation and behaviour. The mechanism of this risk is not known and the available data do not exclude the possibility of an increased risk for brivaracetam.
Patients should be monitored for signs of suicidal ideation and behaviours and appropriate treatment should be considered. Patients (and caregivers of patients) should be advised to seek medical advice should any signs of suicidal ideation or behaviour emerge. See also section 4.8, paediatric data.
Hepatic impairment
There are limited clinical data on the use of brivaracetam in patients with pre-existing hepatic impairment. Dose adjustments are recommended for patients with hepatic impairment (see section 4.2).
Brevie contains sodium
This medicinal product contains 21.18 mg sodium per vial, equivalent to 1% of the WHO recommended maximum daily intake of 2 g sodium for an adult.
Formal interaction studies have only been performed in adults.
Pharmacodynamic interactions
Concomitant treatment with levetiracetam
In the clinical studies, although the numbers were limited, there was no observed benefit of brivaracetam versus placebo in patients taking levetiracetam concurrently. No additional safety or tolerability concern was observed (see section 5.1).
Interaction with alcohol
In a pharmacokinetic and pharmacodynamic interaction study between brivaracetam 200 mg single dose and ethanol 0.6 g/L continuous infusion in healthy subjects, there was no pharmacokinetic interaction, but brivaracetam approximately doubled the effect of alcohol on psychomotor function, attention and memory. Intake of brivaracetam with alcohol is not recommended.
Pharmacokinetic interactions
Effects of other medicinal products on the pharmacokinetics of brivaracetam
In vitro data suggest that brivaracetam has a low interaction potential. The main disposition pathway of brivaracetam is by CYP-independent hydrolysis. A second disposition pathway involves hydroxylation mediated by CYP2C19 (see section 5.2).
Brivaracetam plasma concentrations may increase when coadministered with CYP2C19 strong inhibitors (e.g. fluconazole, fluvoxamine), but the risk of a clinically relevant CYP2C19-mediated interaction is considered to be low. Limited clinical data are available implying that coadministration of cannabidiol may increase the plasma exposure of brivaracetam, possibly through CYP2C19 inhibition, but the clinical relevance is uncertain.
Rifampicin
In healthy subjects, coadministration with the strong enzyme inducer rifampicin (600 mg/day for 5 days), decreased brivaracetam area under the plasma concentration curve (AUC) by 45 %. Prescribers should consider adjusting the brivaracetam dose in patients starting or ending treatment with rifampicin.
Strong enzyme inducing AEDs
Brivaracetam plasma concentrations are decreased when coadministered with strong enzyme inducing AEDs (carbamazepine, phenobarbital, phenytoin) but no dose adjustment is required (see table 1).
Other enzyme inducers
Other strong enzyme inducers (such as St John´s wort (Hypericum perforatum)) may also decrease the systemic exposure of brivaracetam. Therefore, starting or ending treatment with St John's wort should be done with caution.
Effects of brivaracetam on other medicinal products
Brivaracetam given 50 or 150 mg/day did not affect the AUC of midazolam (metabolised by CYP3A4). The risk of clinically relevant CYP3A4 interactions is considered to be low.
In vitro studies have shown that brivaracetam exhibits little or no inhibition of CYP450 isoforms except for CYP2C19. Brivaracetam may increase plasma concentrations of medicinal products metabolised by CYP2C19 (e.g. lanzoprazole, omeprazole, diazepam). When tested in vitro brivaracetam did not induce CYP1A1/2 but induced CYP3A4 and CYP2B6. No CYP3A4 induction was found in vivo (see midazolam above). CYP2B6 induction has not been investigated in vivo and brivaracetam may decrease plasma concentrations of medicinal products metabolised by CYP2B6 (e.g. efavirenz). In vitro interaction studies to determine the potential inhibitory effects on transporters concluded that there were no clinically relevant effects, except for OAT3. In vitro, Brivaracetam inhibits OAT3 with a half maximal inhibitory concentration 42-fold higher than the Cmax at the highest clinical dose. Brivaracetam 200mg/day may increase plasma concentrations of medicinal products transported by OAT3.
Antiepileptic drugs
Potential interactions between brivaracetam (50 mg/day to 200 mg/day) and other AEDs were investigated in a pooled analysis of plasma drug concentrations from all phase 2-3 studies, in a population pharmacokinetic analysis of placebo-controlled phase 2-3 clinical studies, and in dedicated drug-drug interaction studies (for the following AEDs: carbamazepine, lamotrigine, phenytoin and topiramate). The effect of the interactions on the plasma concentration is summarised in table 1 (increase is indicated as “↑” and decrease as “↓”, area under the plasma concentration versus time curve as “AUC”, maximum observed concentration as Cmax).
Table 1: Pharmacokinetic interactions between brivaracetam and other AEDs
AED coadministered | Influence of AED on brivaracetam plasma concentration | Influence of brivaracetam on AED plasma concentration |
Carbamazepine | AUC 29 % ↓ Cmax 13 % ↓ No dose adjustment required | Carbamazepine - None Carbamazepine-epoxide ↑ (See below) No dose adjustment required. |
Clobazam | No data available | None |
Clonazepam | No data available | None |
Lacosamide | No data available | None |
Lamotrigine | None | None |
Levetiracetam | None | None |
Oxcarbazepine | None | None (monohydroxy derivative, MHD) |
Phenobarbital | AUC 19 % ↓ No dose adjustment required | None |
Phenytoin | AUC 21 % ↓ No dose adjustment required | None a AUC 20% ↑ a Cmax 20% ↑ |
Pregabalin | No data available | None |
Topiramate | None | None |
Valproic acid | None | None |
Zonisamide | No data available | None |
a Based on a study involving the administration of a supratherapeutic dose of 400 mg/day brivaracetam.
Carbamazepine
Brivaracetam is a moderate reversible inhibitor of epoxide hydrolase resulting in an increased concentration of carbamazepine epoxide, an active metabolite of carbamazepine. In controlled clinical studies, the carbamazepine epoxide plasma concentration increased by a mean of 37 %, 62 % and 98 % with little variability at brivaracetam doses of 50 mg/day, 100 mg/day and 200 mg/day respectively. No safety risks were observed. There was no additive effect of brivaracetam and valproate on the AUC of carbamazepine epoxide.
Oral contraceptives
Co-administration of brivaracetam (100 mg/day) with an oral contraceptive containing ethinylestradiol (0.03 mg) and levonorgestrel (0.15 mg) did not influence the pharmacokinetics of either substance. When brivaracetam was coadministered at a dose of 400 mg/day (twice the recommended maximum daily dose) with an oral contraceptive containing ethinylestradiol (0.03 mg) and levonorgestrel (0.15 mg), a reduction in oestrogen and progestin AUCs of 27 % and 23 %, respectively, was observed without impact on suppression of ovulation. There was generally no change in the concentration-time profiles of the endogenous markers estradiol, progesterone, luteinizing hormone (LH), follicle stimulating hormone (FSH), and sex hormone binding globulin (SHBG).
Women of childbearing potential
Physicians should discuss family planning and contraception with women of childbearing potential taking brivaracetam (see Pregnancy).
If a woman decides to become pregnant, the use of brivaracetam should be carefully re-evaluated.
Pregnancy
Risk related to epilepsy and antiepileptic medicinal products in general
For all anti-epileptic drugs, it has been shown that in the offspring of treated women with epilepsy, the prevalence of malformations is two to three times greater than the rate of approximately 3 % in the general population. In the treated population, an increase in malformations has been noted with polytherapy; however, the extent to which the treatment and/or the underlying condition is responsible has not been elucidated. Discontinuation of anti-epileptic treatments may result in exacerbation of the disease which could be harmful to the mother and the foetus.
Risk related to brivaracetam
There is a limited amount of data from the use of brivaracetam in pregnant women. There is no data on placental transfer in humans, but brivaracetam was shown to readily cross the placenta in rats (see section 5.3). The potential risk for humans is unknown. Animal studies did not detect any teratogenic potential of brivaracetam (see section 5.3).
In clinical studies, brivaracetam was used as adjunctive therapy and when it was used with carbamazepine, it induced a dose-related increase in the concentration of the active metabolite, carbamazepine-epoxide (see section 4.5). There is insufficient data to determine the clinical significance of this effect in pregnancy.
As a precautionary measure, brivaracetam should not be used during pregnancy unless clinically necessary i.e. (if the benefit to the mother clearly outweighs the potential risk to the foetus).
Breast-feeding
Brivaracetam is excreted in human breast milk. A decision should be made whether to discontinue breastfeeding or to discontinue brivaracetam, taking into account the benefit of the medicinal product to the mother. In case of co-administration of brivaracetam and carbamazepine, the amount of carbamazepine-epoxide excreted in breast milk could increase. There is insufficient data to determine the clinical significance.
Fertility
No human data on the effect of brivaracetam on fertility are available. In rats, there was no effect on fertility with brivaracetam (see section 5.3).
Brivaracetam has minor or moderate influence on the ability to drive and use machines.
Due to possible differences in individual sensitivity some patients might experience somnolence, dizziness, and other central nervous system (CNS) related symptoms. Patients should be advised not to drive a car or to operate other potentially hazardous machines until they are familiar with the effects of brivaracetam on their ability to perform such activities.
Summary of the safety profile
The most frequently reported adverse reactions (>10 %) with brivaracetam treatment were: somnolence (14.3 %) and dizziness (11.0 %). They were usually mild to moderate in intensity. Somnolence and fatigue were reported at a higher incidence with increasing dose.
The discontinuation rate due to adverse reactions was 3.5 %, 3.4 % and 4.0 % for patients randomized to brivaracetam at respectively the dose of 50 mg/day, 100 mg/day and 200 mg/day and 1.7 % for patients randomized to placebo. The adverse reactions most frequently resulting in discontinuation of brivaracetam therapy were dizziness (0.8 %) and convulsion (0.8 %).
Tabulated list of adverse reactions
In the table below, adverse reactions, which were identified based on review of the three placebo-controlled, fixed-dose studies safety database in subjects ≥ 16 years of age, are listed by System Organ Class and frequency.
The frequencies are defined as follows: very common (≥ 1/10), common (≥ 1/100 to < 1/10), uncommon (≥ 1/1,000 to < 1/100). Within each frequency grouping, undesirable effects are presented in order of decreasing seriousness.
System organ class | Frequency | Adverse reactions from clinical studies |
Infections and infestations | Common | Influenza |
Blood and lymphatic system disorders | Uncommon | Neutropenia |
Immune system disorders | Uncommon | Type I hypersensitivity |
Metabolism and nutrition disorders | Common | Decreased appetite |
Psychiatric disorders | Common | Depression, anxiety, insomnia, irritability |
Uncommon | Suicidal ideation, psychotic disorder, aggression, agitation | |
Nervous system disorders | Very common | Dizziness, somnolence |
Common | Convulsion, vertigo | |
Respiratory, thoracic and mediastinal disorders | Common | Upper respiratory tract infections, cough |
Gastrointestinal disorders | Common | Nausea, vomiting, constipation |
General disorders and administration site conditions | Common | Fatigue |
Description of selected adverse reactions
Neutropenia has been reported in 0.5 % (6/1099) brivaracetam patients and 0 % (0/459) placebo patients. Four of these subjects had decreased neutrophil counts at baseline, and experienced additional decrease in neutrophil counts after initiation of brivaracetam treatment. None of the 6 cases of neutropenia were severe, required any specific treatment or led to discontinuation of brivaracetam and none had associated infections.
Suicidal ideation has been reported in 0.3 % (3/1099) brivaracetam patients and 0.7 % (3/459) placebo patients. In the short-term clinical studies of brivaracetam in epilepsy patients, there were no cases of completed suicide and suicide attempt, however both have been reported in open-label extension studies (see section 4.4).
Reactions suggestive of immediate (Type I) hypersensitivity have been reported in a small number of brivaracetam patients (9/3022) during clinical development.
Adverse reactions with intravenous administration generally appeared to be similar to those observed with oral administration. Intravenous administration was associated with infusion site pain in 2.8 % of the patients.
Paediatric population
The safety profile of brivaracetam observed in children from 1 month of age was consistent with the safety profile observed in adults. In the open label, uncontrolled, long-term studies suicidal ideation was reported in 4.7 % of paediatric patients assessed from 6 years onwards (more common in adolescents) compared with 2.4 % of adults and behavioural disorders were reported in 24.8 % of paediatric patients compared with 15.1 % of adults. The majority of events were mild or moderate in intensity, were non-serious, and did not lead to discontinuation of study drug. An additional adverse reaction reported in children was psychomotor hyperactivity (4.7 %).
No specific pattern of adverse event (AE) was identified in children from 1 month to < 4 years of age when compared to older paediatric age groups. No significant safety information was identified indicating the increasing incidence of a particular AE in this age group. As data available in children younger than 2 years of age is limited, brivaracetam is not indicated in this age range. Limited clinical data are available in neonates.
Elderly
Of the 130 elderly subjects enrolled in the brivaracetam phase 2/3 development program (44 with epilepsy), 100 were 65-74 years of age and 30 were 75-84 years of age. The safety profile in elderly patients appears to be similar to that observed in younger adult patients.
To reports any side effect(s):
Saudi Arabia:
· The National Pharmacovigilance Centre (NPC):
- SFDA Call Center: 19999
- E-mail: npc.drug@sfda.gov.sa
- Website: https://ade.sfda.gov.sa/
Other GCC States:
- Please contact the relevant competent authority
Symptoms
There is limited clinical experience with brivaracetam overdose in humans. Somnolence and dizziness have been reported in a healthy subject taking a single dose of 1,400 mg of brivaracetam.
The following adverse reactions were reported with brivaracetam overdose: nausea, vertigo, balance disorder, anxiety, fatigue, irritability, aggression, insomnia, depression, and suicidal ideation in the post-marketing experience. In general, the adverse reactions associated with brivaracetam overdose were consistent with the known adverse reactions.
Management of overdose
There is no specific antidote for overdose with brivaracetam. Treatment of an overdose should include general supportive measures. Since less than 10 % of brivaracetam is excreted in urine, haemodialysis is not expected to significantly enhance brivaracetam clearance (see section 5.2).
Pharmacotherapeutic group: antiepileptics, other antiepileptics, ATC code: N03AX23.
Mechanism of action
Brivaracetam displays a high and selective affinity for synaptic vesicle protein 2A (SV2A), a transmembrane glycoprotein found at presynaptic level in neurons and in endocrine cells. Although the exact role of this protein remains to be elucidated it has been shown to modulate exocytosis of neurotransmitters. Binding to SV2A is believed to be the primary mechanism for brivaracetam anticonvulsant activity.
Clinical efficacy and safety
The efficacy of brivaracetam for the adjunctive therapy of partial onset seizures (POS) was established in 3 randomized, double-blind, placebo-controlled, fixed-dose, multi-center clinical studies in subjects 16 years of age and older. The daily dose of brivaracetam ranged from 5 to 200 mg/day across these studies. All studies had an 8-week baseline period followed by a 12-week treatment period with no up-titration. 1,558 patients received study drug of which 1,099 received brivaracetam. Study enrollment criteria required that patients have uncontrolled POS despite treatment with either 1 or 2 concomitant AEDs. Patients were required to have at least 8 POS during the baseline period. The primary endpoints in the phase 3 studies were the percent reduction in POS frequency over placebo and the 50 % responder rate based on 50 % reduction in POS frequency from baseline.
The most commonly taken AEDs at the time of study entry were carbamazepine (40.6 %), lamotrigine (25.2 %), valproate (20.5 %), oxcarbazepine (16.0 %), topiramate (13.5 %), phenytoin (10.2 %) and levetiracetam (9.8 %). The median baseline seizure frequency across the 3 studies was 9 seizures per 28 days. Patients had a mean duration of epilepsy of approximately 23 years.
The efficacy outcomes are summarized in Table 2. Overall, brivaracetam was efficacious for the adjunctive treatment of partial onset seizures in patients 16 years of age and older between 50 mg/day and 200 mg/day.
Table 2: Key Efficacy Outcomes for Partial Onset Seizure Frequency per 28 Days
Study | Placebo | Brivaracetam * Statistically significant (p-value) | ||
50 mg/day | 100 mg/day | 200 mg/day | ||
Study N01253(1) | ||||
n= 96 | n= 101 | |||
50 % Responder rate | 16.7 | 32.7* (p=0.008) | ~ | ~ |
Percent reduction over placebo (%) | NA | 22.0* (p=0.004) | ~ | ~ |
Study N01252(1) | ||||
n = 100 | n = 99 | n = 100 | ||
50 % Responder rate | 20.0 | 27.3 (p=0.372) | 36.0(2) (p=0.023) | ~ |
Percent reduction over placebo (%) | NA | 9.2 (p=0.274) | 20.5(2) (p=0.010) | ~ |
Study N01358 | ||||
n = 259 | n = 252 | n = 249 | ||
50% Responder rate | 21.6 | ~ | 38.9* (p<0.001) | 37.8* (p<0.001) |
Percent reduction over placebo (%) | NA | ~ | 22.8* (p<0.001) | 23.2* (p<0.001) |
n = randomised patients who received at least 1 dose of study medication
~ Dose not studied
* Statistically significant
(1) Approximately 20 % of the patients were on concomitant levetiracetam
(2) The primary outcome for N01252 did not achieve statistical significance based on the sequential testing procedure. The 100 mg/day dose was nominally significant.
In clinical studies, a reduction in seizure frequency over placebo was higher with the dose of 100 mg/day than with 50 mg/day. Apart from dose-dependent increases in incidences of somnolence and fatigue, brivaracetam 50 mg/day and 100 mg/day had a similar safety profile including CNS-related AEs and with long-term use.
Figure 1 shows the percentage of patients (excluding patients with concomitant levetiracetam) by category of reduction from baseline in POS frequency per 28 days in all 3 studies. Patients with more than a 25 % increase in POS are shown at left as “worse”. Patients with an improvement in percent reduction in baseline POS frequency are shown in the 4 right-most categories. The percentages of patients with at least a 50 % reduction in seizure frequency were 20.3 %, 34.2 %, 39.5 %, and 37.8 % for placebo, 50 mg/day, 100 mg/day, and 200 mg/day, respectively.
Figure 1: Proportion of patients by category of seizure response for brivaracetam and placebo over 12 weeks across all three double-blind pivotal clinical trials
In a pooled analysis of the three pivotal clinical studies, no differences in efficacy (measured as 50 % responder rate) was observed within the dose range of 50 mg/day to 200 mg/day when brivaracetam is combined with inducing or non-inducing AEDs. In clinical studies 2.5 % (4/161), 5.1 % (17/332) and 4.0% (10/249) of the patients on brivaracetam 50 mg/day, 100 mg/day and 200 mg/day respectively became seizure free during the 12-week treatment period compared with 0.5 % (2/418) on placebo.
Improvement in the median percent reduction in seizure frequency per 28 days has been observed in patients with type IC seizure (secondary generalized tonic-clonic seizures) at baseline treated with brivaracetam (66.6 % (n=62), 61.2 % (n=100) and 82.1 % (n=75) of the patients on brivaracetam 50 mg/day, 100 mg/day and 200 mg/day respectively as compared to placebo 33.3 % (n=115)).
The efficacy of brivaracetam in monotherapy has not been established. Brivaracetam is not recommended for use in monotherapy.
Treatment with levetiracetam
In two phase 3 randomised placebo-controlled clinical studies, levetiracetam was administered as concomitant AED in about 20 % of the patients. Although the number of subjects is limited, there was no observed benefit of brivaracetam versus placebo in patients taking levetiracetam concurrently which may reflect competition at the SV2A binding site. No additional safety or tolerability concerns were observed.
In a third study, a pre-specified analysis demonstrated efficacy over placebo for 100 mg/day and 200 mg/day in patients with prior exposure to levetiracetam. The lower efficacy observed in these patients compared to the leveticacetam-naïve patients was likely due to the higher number of prior AEDs used and higher baseline seizure frequency.
Elderly (65 years of age and above)
The three pivotal double-blind placebo-controlled clinical studies included 38 elderly patients aged between 65 and 80 years. Although data are limited, the efficacy was comparable to younger subjects.
Open label extension studies
Across all studies, 81.7 % of the patients who completed randomized studies were enrolled in the long-term open-label extension studies. From entry into the randomized studies, 5.3 % of the subjects exposed to brivaracetam for 6 months (n=1,500) were seizure free compared to 4.6 % and 3.7 % for subjects exposed for 12 months (n=1,188) and 24 months (n=847), respectively. However, as a high proportion of subjects (26%) discontinued from the open-label studies due to lack of efficacy, a selection bias may have occurred, as the subjects who stayed in the study responded better than those who have terminated prematurely.
In patients who were followed up in the open-label extension studies for up to 8 years, the safety profile was similar to that observed in the short-term, placebo-controlled studies.
Paediatric population
In children aged 2 years and older, partial onset seizures have a similar pathophysiology to those in adolescents and adults. Experience with epilepsy medicines suggests that the results of efficacy studies performed in adults can be extrapolated to children down to the age of 2 years provided the paediatric dose adaptations are established and safety has been demonstrated (see sections 5.2 and 4.8). Doses in patients from 2 years of age were defined by weight-based dose adaptations which have been established to achieve similar plasma concentrations to the ones observed in adults taking efficacious doses (section 5.2).
A long-term, uncontrolled, open-label safety study included children (from 1 month of age to less than 16 years) who continued treatment after completing the PK study (see section 5.2), children who continued treatment after completing the i.v. (intravenous) safety study and children directly enrolled into the safety study. Children who directly enrolled received a brivaracetam starting dose of 1 mg/kg/day and depending on response and tolerability, the dose was increased up to 5 mg/kg/day by doubling the dose at weekly intervals. No child received a dose greater than 200 mg/day. For children weighing 50 kg or greater the brivaracetam starting dose was 50 mg/day and depending on response and tolerability, the dose was increased up to a maximum of 200 mg/day by weekly increments of 50 mg/day.
From the pooled open-label safety and PK studies in adjunctive therapy, 186 children with POS in the age range of 1 month < 16 years of age have received brivaracetam, of whom 149 have been treated for ≥ 3 months, 138 for ≥ 6 months, 123 for ≥ 12 months, 107 for ≥ 24 months, and 90 for ≥ 36 months.
Brivaracetam film-coated tablets, oral solution and solution for intravenous injection show the same AUC, while the maximum plasma concentration is slightly higher after intravenous administration. Brivaracetam exhibits linear and time-independent pharmacokinetics with low intra- and inter-subject variability, and features complete absorption, very low protein binding, renal excretion following extensive biotransformation, and pharmacologically inactive metabolites.
Absorption
Brivaracetam is rapidly and completely absorbed after oral administration and the absolute bioavailablity is approximately 100 %. The median tmax for tablets taken without food is 1 hour (tmax range is 0.25 to 3 h).
Coadministration with a high-fat meal slowed down the absorption rate (median tmax 3 h) and decreased the maximum plasma concentration (37 % lower) of brivaracetam, while the extent of absorption remained unchanged.
Distribution
Brivaracetam is weakly bound (≤ 20 %) to plasma proteins. The volume of distribution is 0.5 L/kg, a value close to that of the total body water.
Due to its lipophylicity (Log P) brivaracetam has high cell membrane permeability.
Biotransformation
Brivaracetam is primarily metabolized by hydrolysis of the amide moiety to form the corresponding carboxylic acid (approximately 60 % the elimination), and secondarily by hydroxylation on the propyl side chain (approximately 30 % the elimination). The hydrolysis of the amide moiety leading to the carboxylic acid metabolite (34 % of the dose in urine) is supported by hepatic and extra-hepatic amidase. In vitro, the hydroxylation of brivaracetam is mediated primarily by CYP2C19. Both metabolites, are further metabolised forming a common hydroxylated acid formed predominantly by hydroxylation of the propyl side chain on the carboxylic acid metabolite (mainly by CYP2C9). In vivo, in human subjects possessing ineffective mutations of CYP2C19, production of the hydroxy metabolite is decreased 10-fold while brivaracetam itself is increased by 22 % or 42 % in individuals with one or both mutated alleles. The three metabolites are not pharmacologically active.
Elimination
Brivaracetam is eliminated primarily by metabolism and by excretion in the urine. More than 95 % of the dose, including metabolites, is excreted in the urine within 72 hours after intake. Less than 1 % of the dose is excreted in faeces and less than 10 % of brivaracetam is excreted unchanged in urine. The terminal plasma half-life (t1/2) is approximately 9 hours. The total plasma clearance in patients was estimated to 3.6 L/h.
Linearity
Pharmacokinetics is dose-proportional from 10 to at least 600 mg.
Interactions with medicinal products
Brivaracetam is cleared by multiple pathways including renal excretion, non-CYP-mediated hydrolysis and CYP-mediated oxidations. In vitro, brivaracetam is not a substrate of human P-glycoprotein (P-gp), multidrug resistance proteins (MRP) 1 and 2, and likely not organic anion transporter polypeptide 1B1 (OATP1B1) and OATP1B3.
In vitro assays showed that brivaracetam disposition should not be significantly affected by CYP (eg. CYP1A, CYP2C8, CYP2C9, CYP2D6 and CYP3A4) inhibitors.
In vitro, brivaracetam was not an inhibitor of the CYP1A2, CYP2A6, CYP2B6, CYP2C8, CYP2C9, CYP2D6, CYP3A4, or the transporters P-gp, BCRP, BSEP MRP2, MATE-K, MATE-1, OATP1B1, OATP1B3, OAT1 and OCT1 at clinically relevant concentrations. In vitro, brivaracetam did not induce CYP1A2.
Pharmacokinetics in special patient groups
Elderly (65 years of age and above)
In a study in elderly subjects (65 to79 years old; with creatinine clearance 53 to 98 ml/min/1.73 m²) receiving brivaracetam 400 mg/day in bid administration, the plasma half-life of brivaracetam was 7.9 hours and 9.3 hours in the 65 to 75 and >75 years groups, respectively. The steady-state plasma clearance of brivaracetam was similar (0.76 ml/min/kg) to young healthy male subjects (0.83 ml/min/kg) (see section 4.2).
Renal impairment
A study in subjects with severe renal impairment (creatinine clearance < 30 ml/min/1.73 m² and not requiring dialysis) revealed that the plasma AUC of brivaracetam was moderately increased (+21 %) relative to healthy controls, while the AUC of the acid, hydroxy and hydroxyacid metabolites were increased 3-, 4-, and 21-fold, respectively. The renal clearance of these non active metabolites was decreased 10-fold. The hydroxyacid metabolite did not reveal any safety concerns in non clinical studies. Brivaracetam has not been studied in patients undergoing hemodialysis (see section 4.2).
Hepatic impairment
A pharmacokinetic study in subjects with hepatic cirrhosis (Child-Pugh classes A, B, and C) showed similar increases in exposure to brivaracetam irrespective of disease severity (50 %, 57 % and 59 %), relative to matched healthy controls. (see section 4.2).
Body weight
A 40 % decrease in steady-state plasma concentration has been estimated across a body weight range from 46 kg to 115 kg. However, this is not considered to be a clinically relevant difference.
Gender
There are no clinically relevant differences in the pharmacokinetics of brivaracetam by gender.
Race
The pharmacokinetics of brivaracetam was not significantly affected by race (Caucasian, Asian) in a population pharmacokinetic modeling from epilepsy patients. The number of patients with other ethnic background was limited.
Pharmacokinetic/pharmacodynamics relationship
The EC50 (brivaracetam plasma concentration corresponding to 50 % of the maximum effect) was estimated to be 0.57 mg/L. This plasma concentration is slightly above the median exposure obtained after brivaracetam doses of 50 mg/day. Further seizure frequency reduction is obtained by increasing the dose to 100 mg/day and reaches a plateau at 200 mg/day.
Paediatric population
In a pharmacokinetic study with a 3-week evaluation period and weekly fixed 3-step up-titration using the brivaracetam oral solution, 99 subjects aged 1 month to < 16 years were evaluated. Brivaracetam was administered at weekly increasing doses of approximately 1 mg/kg/day, 2 mg/kg/day, and 4 mg/kg/day. All doses were adjusted by body weight, and did not exceed a maximum of 50 mg/day, 100 mg/day, and 200 mg/day. At the end of the evaluation period, subjects may have been eligible for entry into a long-term follow-up study continuing on their last received dose (see section 4.8). Plasma concentrations were shown to be dose-proportional in all age groups. Population pharmacokinetics modeling was performed based on sparse plasma concentration data collected in the 3-week PK study and the ongoing long-term follow-up study. 232 paediatric patients with epilepsy, aged 2 months to 17 years, were included in the analysis. The analysis indicated that doses of 5.0 (body weights 10-20 kg) and 4.0 mg/kg/day (body weights 20-50 kg) provide the same steady-state average plasma concentration as in adults receiving 200 mg/day. The estimated plasma clearance was 0.96 L/h, 1.61 L/h, 2.18 L/h and 3.19 L/h for children weighing 10 kg, 20 kg, 30 kg and 50 kg, respectively. In comparison, plasma clearance was estimated at 3.58 L/h in adult patients (70 kg body weight).
Currently, no clinical data are available in neonates.
In safety pharmacology studies, the predominant effects were CNS related (mainly transient CNS depression and decreased spontaneous locomotor activity) seen at multiples (greater than 50 fold) of the pharmacologically active dose of brivaracetam, 2 mg/kg. Learning and memory function were not affected.
Findings not observed in clinical studies, but seen in the repeated-dose toxicology dog studies at exposure similar to the clinical plasma AUC, were hepatotoxic effects (mainly porphyria). However, toxicological data accumulated on brivaracetam and on a structurally-related compound indicate that the dog liver changes have developed through mechanisms not relevant for humans. No adverse liver changes were seen in rats and monkeys following chronic administration of brivaracetam at 5- and 42-fold the clinical AUC exposure. In monkeys, CNS signs (prostrate, loss of balance, clumsy movements) occurred at 64 fold the clinical Cmax, these effects being less apparent over time.
Genotoxicity studies have not detected any mutagenic or clastogenic activity. Carcinogenicity studies did not indicate any oncogenic potential in rats, whereas increased incidences of hepatocellular tumors in male mice are considered to result of a non-genotoxic, mode of action linked to a phenobarbitone-like liver enzyme induction, which is a known rodent specific phenomenon.
Brivaracetam did not affect male or female fertility and has demonstrated no teratogenic potential in either rat or rabbit. Embryotoxicity was observed in rabbits at a maternal toxic dose of brivaracetam with an exposure level 8-fold the clinical AUC exposure at the maximum recommended dose. In rats, brivaracetam was shown to readily cross the placenta and to be excreted in milk of lactating rats with concentrations similar to maternal plasma levels.
Brivaracetam did not show any dependence potential in rats.
Juvenile animals studies
In juvenile rats, brivaracetam exposure levels 6- to 15-fold the clinical AUC exposure at the maximum recommended dose induced developmental adverse effects (i.e. mortality, clinical signs, decreased body weight and lower brain weight). There were no adverse effects on CNS function, neuropathological and brain histopathological examination. In juvenile dogs, the brivaracetam-induced changes at the exposure level 6- fold the clinical AUC were similar to those observed in adult animals. There were no adverse effects in any of the standard developmental or maturation endpoints.
- Sodium chloride
- Sodium acetate trihydrate
- Glacial acetic acid
- Water for injection
- Nitrogen
This medicinal product must not be mixed with other medicinal products.
Do not store above 30°C. Keep out of the sight and reach of children.
This medicinal product does not require any special storage conditions.
For storage conditions after dilution of the medicinal product, see section 6.3.
Brevie 50 mg/5 ml Solution for Injection/Infusion is packed in 10 ml type-I clear colorless glass vials with 20 mm rubber stoppers and sealed with 20 mm aluminum seals having blue color polypropylene discs.
Pack size : 1 Vial (5 ml)
This medicinal product is for single use only, any unused solution should be discarded. Product with particulate matter or discoloration should not be used.
Brivaracetam solution for injection/infusion is physically compatible and chemically stable when mixed with the following diluents
Diluents
· 9 mg/ml (0.9 %) Sodium chloride solution for injection
· 50 mg/ml (5 %) Glucose solution for injection
· Lactated Ringer's solution for injection.
Any unused medicinal product or waste material should be disposed of in accordance with local requirements.
