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1. What Entyvio is
Entyvio contains the active substance ‘vedolizumab’. Vedolizumab belongs to a group of biological medicines called monoclonal antibodies (MAbs).
How Entyvio works
Entyvio works by blocking a protein on the surface of white blood cells that cause the inflammation in ulcerative colitis and Crohn’s disease. This reduces the amount of inflammation.
What Entyvio is used for
Entyvio is used to treat the signs and symptoms in adults of:
· moderately to severely active ulcerative colitis
· moderately to severely active Crohn’s disease.
Ulcerative colitis
Ulcerative colitis is a disease that causes inflammation of the large bowel. If you have ulcerative colitis, you will first be given other medicines. If you do not respond well enough or cannot tolerate these medicines, your doctor may give you Entyvio to reduce the signs and symptoms of your disease.
Crohn’s disease
Crohn’s disease is a disease that causes inflammation of the digestive system. If you have Crohn’s disease you will first be given other medicines. If you do not respond well enough or cannot tolerate these medicines, your doctor may give you Entyvio to reduce the signs and symptoms of your disease.
Do not use Entyvio
· if you are allergic to vedolizumab or any of the other ingredients of this medicine (listed in section 6).
· if you have an active severe infection - such as TB (tuberculosis), blood poisoning, severe diarrhoea and vomiting (gastroenteritis), nervous system infection.
Warnings and precautions
Talk to your doctor, pharmacist or nurse before using Entyvio.
Tell your doctor, pharmacist or nurse immediately when you first use this medicine, during treatment, and between doses:
· if you experience blurred, loss of or double vision, difficulty speaking, weakness in an arm or a leg, a change in the way you walk or problems with your balance, persistent numbness, decreased sensation or loss of sensation, memory loss or confusion. These may all be symptoms of a serious and potentially fatal brain condition known as progressive multifocal leukoencephalopathy (PML).
· if you have an infection, or think you have an infection – signs include chills, shivering, persistent cough or a high fever. Some infections may become serious and possibly even life-threatening if left untreated.
· if you experience signs of an allergic reaction such as wheezing, difficulty breathing, hives, itching, swelling or dizziness. For more detailed information, see allergic reactions in section 4.
· if you are going to receive any vaccination or have recently had a vaccination. Entyvio may affect the way you respond to a vaccination.
· if you have cancer, tell your doctor. Your doctor will have to decide if you can still be given Entyvio.
· if you are not feeling any better as vedolizumab may take up to 14 weeks to work in some patients with very active Crohn’s disease.
Children and adolescents
Entyvio is not recommended for use in children or adolescents (under 18 years of age) due to the lack of information regarding the use of this medicine in this age group.
Other medicines and Entyvio
Tell your doctor, pharmacist or nurse if you are taking, have recently taken or might take any other medicines.
· Entyvio should not be given with other biologic medicines that suppress your immune system as the effect of this is not known.
Tell your doctor if you have previously taken:
· natalizumab (a medicine for multiple sclerosis) or
· rituximab (a medicine for certain types of cancer and rheumatoid arthritis). Your doctor will decide if you can be given Entyvio.
Pregnancy and breast-feeding
If you are pregnant or breast-feeding, think you may be pregnant or are planning to have a baby, ask your doctor for advice before taking this medicine.
Pregnancy
The effects of Entyvio in pregnant women are not known. Therefore, this medicine is not recommended for use during pregnancy. You and your doctor should decide if the benefit to you clearly outweighs the potential risk to yourself and your baby.
If you are a woman of childbearing potential, you are advised to avoid becoming pregnant while using Entyvio. You should use adequate contraception during treatment and for at least 4.5 months after the last treatment.
Breast-feeding
Tell your doctor if you are breast-feeding or planning to breast-feed. Entyvio passes into breast milk. There is not enough information on what effect this may have on your baby. A decision must be made whether to stop breast-feeding or to stop using Entyvio therapy taking into account the benefit of breast-feeding for your child and the benefit of therapy for you.
Driving and using machines
This medicine has a minor effect on your ability to drive or use tools or machines. A small number of patients have felt dizzy after receiving Entyvio. If you feel dizzy, do not drive or use tools or machines.
Entyvio 108 mg solution for injection contains sodium
This medicine contains less than 1 mmol sodium (23 mg) per dose, that is to say essentially ‘sodium-free’.
Always use this medicine exactly as your doctor or pharmacist has told you. Check with your doctor or pharmacist if you are not sure.
You or your caregiver will be given training on how to use Entyvio injections under the skin (subcutaneous injections).
How much Entyvio you will receive
Treatment with Entyvio is the same for ulcerative colitis and Crohn’s disease.
The recommended dose is 108 mg of Entyvio administered by subcutaneous injection once every 2 weeks.
· At the start of treatment, the doctor will give initial doses of Entyvio through a drip into a vein in your arm (intravenous infusion) over about 30 minutes.
· After at least 2 intravenous infusions, you can start receiving Entyvio by a subcutaneous injection. The first subcutaneous injection is given at the time of the next scheduled intravenous infusion, and every 2 weeks thereafter.
Injecting Entyvio
The subcutaneous injections can be given by yourself or a caregiver, after training on how to do it. Instructions are provided at the end of this leaflet.
If you forget to take or miss your Entyvio injection
If you forget or miss a dose, inject the next dose as soon as possible and then every 2 weeks thereafter.
If you stop using Entyvio
Do not stop using Entyvio without talking with your doctor first.
If you have any further questions on the use of this medicine, ask your doctor pharmacist or nurse.
Like all medicines, this medicine can cause side effects although not everybody gets them.
Serious side effects
Tell your doctor immediately if you notice any of the following:
· allergic reactions (may affect up to 1 in 100 people) - the signs may include: wheezing or difficulty breathing, hives, itching of the skin, swelling, feeling sick, redness of skin and
· infections (may affect up to 1 in 10 people) - the signs may include: chills or shivering, high fever or rash
Other side effects
Tell your doctor as soon as possible if you notice any of the following:
Very common side effects (may affect more than 1 in 10 people)
· common cold
· joint pain
· headache
Common side effects (may affect up to 1 in 10 people)
· fever
· chest infection
· tiredness
· cough
· flu (influenza)
· back pain
· throat pain
· sinus infection
· itching / itchiness
· rash and redness
· pain in the limb
· muscle cramps
· muscle weakness
· throat infection
· stomach flu
· anal infection
· anal sore
· hard faeces
· bloated stomach
· passing gas
· high blood pressure
· prickling or tingling
· heart burn
· haemorrhoids
· blocked nose
· eczema
· night sweats
· acne (pimples)
· injection site reactions (including pain, swelling, redness or itching)
Uncommon side effects (may affect up to 1 in 100 people)
· redness and tenderness of hair follicle
· throat and mouth yeast infection
· vaginal infection
· shingles (herpes zoster)
Very rare side effects (may affect up to 1 in 10,000 people)
· pneumonia
· blurred vision (loss of sharpness of eyesight)
· sudden, severe allergic reaction which can cause breathing difficulty, swelling, fast heartbeat, sweating, drop in blood pressure, light-headedness, loss of consciousness and collapse (anaphylactic reaction and anaphylactic shock)
Reporting of side effects
If you get any side effects, talk to your doctor, pharmacist or nurse. This includes any possible side effects not listed in this leaflet. By reporting side effects you can help provide more information on the safety of this medicine.
· 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 after “EXP”. The expiry date refers to the last day of that month.
· Entyvio is for single use only.
· Store in a refrigerator (2 °C-8 °C). Keep the pre-filled pen in the original carton in order to protect from light. If needed the pre-filled pen can be left out of the refrigerator in its original carton at room temperature (up to 25 oC) for up to 7 days. Do not use if left out of the refrigerator for more than 7 days.
· Do not freeze. Do not leave in direct sunlight.
· Do not use this medicine if you notice any particles in the liquid or discolouration (should be colourless to yellow) prior to administration.
· 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.
What Entyvio contains
· The active substance is vedolizumab. Each pre-filled pen contains 108 mg of vedolizumab.
· The other ingredients are citric acid monohydrate, sodium citrate dihydrate, L-histidine, L-histidine monohydrochloride, L-arginine hydrochloride, polysorbate 80 and water for injections.
Takeda Pharma A/S
Delta Park 45 2665 Vallensbaek Strand
Denmark
ما هو دواء إنتيڨيو
يحتوي دواء إنتيڨيو على المادة الفعالة ’ڨيدوليزوماب‘. تنتمي مادة الڨيدوليزوماب إلى مجموعة الأدوية البيولوجية والتي تعرف باسم الأجسام المضادة وحيدة النسيلة (MAbs) .
كيف يعمل دواء إنتيڨيو
يعمل دواء إنتيڨيو عن طريق منع عمل بروتين معين موجود على سطح خلايا الدم البيضاء التي تسبب الالتهاب في حالات التهاب القولون التقرحي مما يعمل على تقليل هذا الالتهاب.
ماهي استخدامات دواء إنتيڨيو
يستخدم دواء إنتيڨيو في علاج أعراض الحالات التالية لدى البالغين:
· حالات التهاب القولون التقرحي النشطة متوسطة إلى حادة الشدة
· حالات مرض كرون النشطة متوسطة إلى حادة الشدة
التهاب القولون التقرحي
التهاب القولون التقرحي هو مرض يسبب التهابات في الأمعاء الغليظة. إذا كنت تعاني من التهاب القولون التقرحي، فإنه سيتم إعطائك أنواع أدوية أخرى في البداية. وفي حالة كانت استجابة حالتك لهذه الأدوية غير كافية أو لا يمكنك تحمل هذه الأدوية، فإن طبيبك قد يقوم بوصف دواء إنتيڨيو لك للتقليل من أعراض المرض لديك.
مرض كرون
مرض كرون هو مرض يسبب التهابات في الجهاز الهضمي. إذا كنت تعاني من مرض كرون، فإنه سيتم إعطائك أنواع أدوية أخرى في البداية. وفي حالة كانت استجابة حالتك لهذه الأدوية غير كافية أو لا يمكنك تحمل هذه الأدوية، فإن طبيبك قد يقوم بوصف دواء إنتيڨيو لك للتقليل من أعراض المرض لديك.
لا تستخدم دواء إنتيڨيو
· إذا كنت تعاني من حساسية لمادة ڨيدوليزوماب أو لأي من المكونات الأخرى لهذا الدواء (مذكورة في الجزء رقم 6) .
· إذا كنت تعاني من عدوى حادة نشطة مثل مرض السل، أو تسمم بالدم، أو إسهال شديد وقيء (نزلة معوية)، أو عدوى في الجهاز العصبي.
التحذيرات والاحتياطات
تحدث مع طبيبك، أو الصيدلي، أو الممرض قبل تناولك لدواء إنتيڨيو :
أخبر طبيبك أو الصيدلي أو الممرض على الفورعند استخدامك لهذا الدواء للمرة الأولى، أو أثناء العلاج به، أو خلال الفترات ما بين الجرعات:
· إذا أُصبت بتشوش في الرؤية، فقدان أو ازدواج الرؤية، أو صعوبة في الكلام، أو ضعف في أحد الذراعين أو الساقين، أو تغيير في طريقة مشيتك، أو حدوث اضطراب في الاتزان، أو خدر مستمر، أو ضعف الإحساس أو فقدانه، أو فقدان في الذاكرة أو حدوث ارتباك لديك. قد تكون هذه أعراض حالة خطيرة في المخ والتي قد تكون مميتة تُعرف باسم الاعتلال المتزايد متعدد البؤر لمادة المخ البيضاء (PML) .
· إذا كنت تعاني من عدوى، أو تعتقد أنه لديك عدوى - وتشتمل أعراضها على قشعريرة، رجفان، سعال مستمر أو حمى شديدة. بعض أنواع العدوى قد تصبح خطيرة ومن الممكن أن تكون مميتة إذا تركت بدون علاج.
· إذا أُصبت بأعراض رد فعل تحسسي مثل حدوث تزييق في الصدر، صعوبة في التنفس، طفح جلدى، حكة في الجلد، تورم أو دوار. لمزيد من المعلومات المفصلة، انظر ردود الفعل التحسسية في الجزء رقم 4.
· إذا كنت تنوي تناول أي تطعيم أو تناولت بالفعل أي تطعيم مؤخرًا. لأن إنتيڨيو قد يؤثر على طريقة استجابتك للتطعيم.
· إذا كنت تعاني من السرطان، عليك أن تخبر طبيك. وعندها سيقرر الطبيب ما إذا كان يمكنك استخدام دواء إنتيڨيو .
· إذا لم تشعر بأي تحسن، حيث أن مادة الڨيدوليزوماب قد تستغرق حتى 14 أسبوع ليظهر تأثيرها في بعض المرضى الذين يعانون من مرض كرون النشط جدًا.
الأطفال والمراهقين
لا يوصى باستخدام إنتيڨيو للأطفال والمراهقين (ممن تقل أعمارهم عن 18 عام) بسبب عدم توفر معلومات كافية بشأن استخدام هذا الدواء في هذه الفئة العمرية.
إنتيڨيو والأدوية الأخرى
أخبر طبيبك أو الصيدلي أو الممرض إذا كنت تتناول أو تناولت مؤخرًا أو قد تتناول أي أدوية أخرى.
· لا يجب إعطاء دواء إنتيڨيو مع الأدوية البيولوجية الأخرى التي تثبط جهازك المناعي لأن تأثير ذلك غير معروف.
أخبر طبيبك إذا كنت قد تناولت من قبل:
· ناتاليزوماب (دواء يستخدم لعلاج حالات التصلب المتعدد) أو
· ريتوكسيماب (دواء يستخدم لعلاج بعض أنواع السرطان أو التهاب المفاصل الروماتيزمي) . وعندها سيقرر الطبيب ما إذا كان يمكن إعطائك دواء إنتيڨيو .
الحمل والرضاعة
إذا كنتِ حامل أو مرضعة، أو تعتقدين أنك قد تكونين حامل، أو تخططين لإنجاب طفل، استشيري طبيبك قبل استخدامك لهذا الدواء.
الحمل
إن تأثير دواء إنتيڨيو على المرأة الحامل غير معروف. لذلك، لا يوصى باستخدام هذا الدواء أثناء الحمل. يجب أن تقرري أنت وطبيبك ما إذا كانت الفوائد التي ستعود عليكِ تفوق بوضوح المخاطر المحتملة عليكِ وعلى طفلك.
إذا كنت سيدة في سن الإنجاب، فإنه يجب عليك تجنب حدوث حمل أثناء فترة استخدامك لدواء إنتيڨيو . يجب عليك استخدام وسائل منع حمل فعالة أثناء العلاج بإنتيڨيو وكذلك لمدة أربعة أشهر ونصف على الأقل بعد تناولك للجرعة الأخيرة منه.
الرضاعة
أخبري طبيبك إذا كنت ترضعين أو تخططين لإرضاع طفلك. لأن دواء إنتيڨيو يُفرز في اللبن. لكن لا توجد معلومات كافية حول تأثيره على طفلك. لذلك يجب أن تقرري إما أن توقفي الرضاعة الطبيعية أو توقفي استخدام دواء إنتيڨيو مع مراعاة فائدة الرضاعة لطفلك وفائدة العلاج لك.
القيادة واستخدام الآلات
إن لهذا الدواء تأثير طفيف على قدرتك على القيادة أو استخدام الأدوات والآلات. عدد قليل من المرضى شعروا بحدوث دوار بعد تناولهم لدواء إنتيڨيو . إذا كنت تشعر بدوار بعد تناولك لإنتيڨيو ، احرص على عدم القيادة أو استخدام الأدوات والآلات بعد تناولك له.
يحتوي إنتيڨيو 108 مجم محلول للحقن على صوديوم.
يحتوي هذا الدواء على أقل من 1 مليمول من الصوديوم (23 مجم) في الجرعة الواحدة، بما معناه أنه خالِ من الصوديوم.
يجب عليك أن تتناول هذا الدواء تمامًا كما أخبرك طبيبك أو الصيدلي. راجع طبيبك أو الصيدلي إذا كنت غير متأكدًا بشأن ذلك.
سيتم تدريبك أو تدريب مقدم الرعاية لك حول كيفية استخدام حقن إنتيڨيو تحت الجلد (الحقن تحت الجلد) .
ما مقدار جرعة إنتيڨيو التي ستتناولها
إن جرعات إنتيڨيو هي ذاتها في حالات التهاب القولون التقرحي ومرض كرون.
إن الجرعة الموصى بها من إنتيڨيو هي 108 مجم، ويتم إعطائها عن طريق الحقن تحت الجلد مرة واحدة كل أسبوعين.
· عند بداية العلاج، سيقوم طبيبك بإعطائك جرعات أولية من إنتيڨيو عن طريق التسريب الوريدي في أحد أوردة ذراعك (التسريب الوريدي) على مدار 30 دقيقة تقريبًا.
· بعدما يتم إعطائك على الأقل جرعتين من إنتيڨيو عن طريق التسريب الوريدي، يمكنك البدء بتلقّي دواء إنتيڨيو عن طريق الحقن تحت الجلد. وعندها سيتم إعطائك الجرعة الأولى من الحقن تحت الجلد عند الموعد المحدد للجرعة الوريدية التالية، ثم كل أسبوعين بعد ذلك.
طريقة حَقْن إنتيڨيو
يمكنك أخذ الحقن تحت الجلد بنفسك أو بواسطة مقدم الرعاية، وذلك بعد التدريب على كيفية القيام بذلك. التعليمات الخاصة بذلك موجودة في نهاية هذه النشرة.
ماذا تفعل إذا نسيت تناول جرعتك من إنتيڨيو .
إذا نسيت أو فاتتك جرعة إنتيڨيو ، قم بحقن الجرعة التالية في أقرب وقت ممكن ثم بعد ذلك تناول الجرعات كل أسبوعين.
إذا توقفت عن استخدام إنتيڨيو
لا تتوقف عن تناول جرعات إنتيڨيو قبل أن تتحدث مع طبيبك أولًا.
إذا كان لديك أي أسئلة أخرى حول استخدام هذا الدواء، أسأل طبيبك أو الصيدلي أو الممرض.
على غرار جميع الأدوية الأخرى، قد يؤدي هذا الدواء إلى حدوث آثار جانبية، رغم أنها لا تحدث لجميع الأشخاص.
الآثار الجانبية الخطيرة
أخبر طبيبك على الفور إذا لاحظت أي من الأعراض التالية:
· ردود فعل تحسسية (قد تصيب شخص واحد لكل 100 شخص) - وتشتمل أعراضها على: تزييق في الصدر أو صعوبة في التنفس، طفح جلدي، حكة في الجلد، تورم، الشعور بالإعياء، احمرار في الجلد و
· عدوى (قد تصيب شخص واحد لكل 10 أشخاص) – وتشتمل أعراضها على: قشعريرة أو رجفان، ارتفاع درجة الحرارة أو طفح جلدي.
الآثار الجانبية الأخرى
أخبر طبيبك في أقرب وقت ممكن إذا لاحظت أيًا من التالي:
آثار جانبية شائعة جدًا (قد تصيب أكثر من شخص لكل 10 أشخاص)
· نزلة برد
· ألم بالمفاصل
· صداع
آثار جانبية شائعة (قد تصيب شخص واحد لكل 10 أشخاص)
· حمى
· عدوى بالصدر
· تعب
· كحة
· انفلونزا
· ألم بالظهر
· ألم بالحلق
· عدوى بالجيوب الأنفية
· حكة بالجلد
· طفح أو احمرار بالجلد
· ألم بأحد الأطراف
· شد عضلي
· ضعف بالعضلات
· عدوى بالحلق
· ألم بالمعدة
· عدوى عند فتحة الشرج
· تقرحات عند فتحة الشرج
· براز صلب/ إمساك
· انتفاخ بالمعدة
· زيادة إخراج الغازات
· ارتفاع ضغط الدم
· وخز أو تنميل
· حرقة بالمعدة
· بواسير
· انسداد بالأنف
· إكزيما
· تعرق أثناء الليل
· حب الشباب (بثور)
· حدوث تغيرات عند موضع الحقن (تشتمل على ألم، تورم، احمرار أو حكة)
آثار جانبية غير شائعة (قد تصيب شخص واحد لكل 100 شخص)
· احمرار وألم في بصيلات الشعر
· عدوى فطرية في الفم والحلق
· عدوى مهبلية
· القوباء (الهربس النطاقي)
آثار جانبية نادرة جدًا (قد تصيب شخص واحد لكل 10000 شخص)
· التهاب رئوي
· تشوش الرؤية (فقدان حدة الإبصار)
· رد فعل تحسسي شديد ومفاجئ، والذي قد يسبب صعوبة في التنفس، تورم، زيادة ضربات القلب، تعرق، انخفاض في ضغط الدم، دوار، فقدان الوعي والانهيار (رد فعل تحسسي وصدمة تحسسية)
الإبلاغ عن الآثار الجانبية
إذا حدثت لديك أي آثار جانبية، تحدث مع طبيبك، أو الصيدلي أو الممرض. يشمل ذلك حدوث أي آثار جانبية محتملة لم يتم ذكرها بهذه النشرة. إبلاغك عن هذه الآثار الجانبية، يساعد على توفير المزيد من المعلومات حول سلامة هذا الدواء.
1. كيفية تخزين دواء إنتيڨيو
· احتفظ بهذا الدواء بعيدًا عن الضوء وعن متناول الأطفال.
· لا تستخدم هذا الدواء بعد مرور تاريخ انتهاء صلاحيته المُدرَج على العبوة الكرتونية بعد الاختصار ”EXP“. يشير تاريخ انتهاء الصلاحية إلى اليوم الأخير من الشهر المذكور.
· إنتيڨيو مخصص للاستخدام مرة واحدة فقط.
· احتفظ به في الثلاجة (في درجة حرارة تتراوح ما بين 2-8 درجة مئوية) . احتفظ بالقلم المعبأ مُسبقًا في العبوة الكرتونية الأصلية له لكي تحمي الدواء من تأثير الضوء. إذا لزم الأمر، يمكنك الاحتفاظ بالقلم المعبأ مُسبقًا خارج الثلاجة داخل العبوة الكرتونية الأصلية له، في درجة حرارة الغرفة (حتى 25 درجة مئوية) لمدة تصل إلى 7 أيام. لكن لا تستخدم هذا الدواء إذا تم تركه خارج الثلاجة لمدة تزيد عن 7 أيام.
· لا تجمد هذا الدواء. لا تتركه معرّض لضوء الشمس المباشر.
· لا تستخدم هذا الدواء إذا لاحظت وجود أي حبيبات في سائل الحقن أو تغيير في لونه (يجب أن يكون عديم اللون أو مائل للاصفرار) قبل الاستخدام.
· لا تتخلص من أي أدوية في مياه الصرف الصحي أو النفايات المنزلية. اسأل الصيدلي عن كيفية التخلص من الأدوية التي لم تعد تستخدمها. فهذه الإجراءات ستساعد على حماية البيئة.
ما هي محتويات إنتيڨيو
· المادة الفعالة هي ڨيدوليزوماب. يحتوي كل قلم معبأ مسبقًا على 108 مجم من ڨيدوليزوماب.
· المكونات الأخرى هي أحادي هيدرات حامض الستريك، ثنائي هيدرات سترات الصوديوم، ل-هيستيدين، ل- هيستيدين مونوهيدروكلوريد، ل-أرجنين هيدروكلوريد، بولي سوربات 80 و ماء للحقن.
كيف يبدو إنتيڨيو وماهي محتويات العبوة
· إنتيڨيو هو عبارة محلول عديم اللون أو مائل للاصفرار مخصص للحقن، يوجد في قلم زجاجي معبأ مسبقًا مزود بغطاء آلي للإبرة لكي يمتد ويغلق على الإبرة بمجرد إزالة الجهاز من موضع الحقن.
· يتوفر إنتيڨيو في صورة عبوة كرتونية تحتوي على قلم واحد مُعبأ مسبقًا وكذلك في صورة عبوات متعددة تحتوي على عدد 2 (2×1 قلم مُعبأ مسبقًا)، أو عدد 6 (6×1 قلم مُعبأ مسبقًا) . قد لا تكون جميع أحجام العبوات متوفرة في الأسواق.
صاحب تراخيص التسويق
تاكيدا فارما أيه/أس
دلتا بارك 45 2665 فالينسبيك ستراند الدنمارك
الشركة المُصنعة
شركة فيتر فارما فيرتيجينج جي أم بي أتش آند كو. كيه جي
موسويزين 2
88214 رافينسبورج
ألمانيا
Ulcerative colitis
Entyvio is indicated for the treatment of adult patients with moderately to severely active ulcerative colitis who have had an inadequate response with, lost response to, or were intolerant to either conventional therapy or a tumour necrosis factor-alpha (TNFα) antagonist.
Crohn’s disease
Entyvio is indicated for the treatment of adult patients with moderately to severely active Crohn’s disease who have had an inadequate response with, lost response to, or were intolerant to either conventional therapy or a tumour necrosis factor-alpha (TNFα) antagonist.
Treatment should be initiated and supervised by specialist healthcare professionals experienced in the diagnosis and treatment of ulcerative colitis or Crohn’s disease (see section 4.4). Patients should be given the package leaflet.
Posology
Ulcerative colitis and Crohn’s disease
The recommended dose regimen of subcutaneous vedolizumab as a maintenance treatment, following at least 2 intravenous infusions, is 108 mg administered by subcutaneous injection once every
2 weeks. The first subcutaneous dose should be administered in place of the next scheduled intravenous dose and every 2 weeks thereafter.
For the intravenous dose regimen, see section 4.2 of the Entyvio 300 mg powder for concentrate for solution for infusion SmPC.
Insufficient data are available to determine if patients who experience a decrease in response on maintenance treatment with subcutaneous vedolizumab would benefit from an increase in dosing frequency.
There are no data on transition of patients from subcutaneous vedolizumab to intravenous vedolizumab during maintenance treatment.
In patients who have responded to treatment with vedolizumab, corticosteroids may be reduced and/or discontinued in accordance with standard of care.
Retreatment and missed dose(s)
If treatment with subcutaneous vedolizumab is interrupted or if a patient misses a scheduled dose(s) of subcutaneous vedolizumab, patient should be advised to inject the next subcutaneous dose as soon as possible and then every 2 weeks thereafter. The treatment interruption period in clinical trials extended up to 46 weeks with no evident increase in adverse reactions or injection site reactions during
re-initiation of treatment with subcutaneous vedolizumab (see section 4.8). Special populations
Elderly patients
No dose adjustment is required in elderly patients. Population pharmacokinetic analyses showed no effect of age (see section 5.2).
Patients with renal or hepatic impairment
Vedolizumab has not been studied in these patient populations. No dose recommendations can be made.
Paediatric population
The safety and efficacy of vedolizumab in children aged 0 to 17 years old have not been established. No data are available.
Method of administration
Entyvio solution for injection (in a pre-filled syringe or a pre-filled pen) is for subcutaneous injection only.
After proper training on correct subcutaneous injection technique, a patient or caregiver may inject with subcutaneous vedolizumab if their physician determines it is appropriate. Comprehensive instructions for administration using the pre-filled syringe or the pre-filled pen are given in the respective package leaflet.
For further instructions on preparation and special precautions for handling, see section 6.6.
Traceability
In order to improve the traceability of biological medicinal products, the name and the batch number of the administered product should be clearly recorded.
Hypersensitivity reactions
In clinical studies, hypersensitivity reactions have been reported, with the majority being mild to moderate in severity (see section 4.8).
If an anaphylactic reaction, or other severe reaction occurs, administration of vedolizumab must be discontinued immediately and appropriate treatment initiated (see section 4.3).
Infections
Vedolizumab is a gut-selective integrin antagonist with no identified systemic immunosuppressive activity (see section 5.1).
Physicians should be aware of the potential increased risk of opportunistic infections or infections for which the gut is a defensive barrier (see section 4.8). Treatment is not to be initiated in patients with active, severe infections until the infections are controlled, and physicians should consider withholding treatment in patients who develop a severe infection while on chronic treatment with vedolizumab.
Caution should be exercised when considering the use of vedolizumab in patients with a controlled chronic severe infection or a history of recurring severe infections. Patients should be monitored closely for infections before, during and after treatment.
Vedolizumab is contraindicated in patients with active tuberculosis (see section 4.3). Before starting treatment with vedolizumab, patients must be screened for tuberculosis according to the local practice. If latent tuberculosis is diagnosed, appropriate treatment must be started with anti-tuberculosis treatment in accordance with local recommendations, before beginning vedolizumab. In patients diagnosed with TB whilst receiving vedolizumab therapy, then vedolizumab therapy should be discontinued until the TB infection has been resolved.
Some integrin antagonists and some systemic immunosuppressive agents have been associated with progressive multifocal leukoencephalopathy (PML), which is a rare and often fatal opportunistic infection caused by the John Cunningham (JC) virus. By binding to the α4β7 integrin expressed on gut-homing lymphocytes, vedolizumab exerts an immunosuppressive effect specific to the gut.
Although no systemic immunosuppressive effect was noted in healthy subjects the effects on systemic immune system function in patients with inflammatory bowel disease is not known.
Healthcare professionals should monitor patients on vedolizumab for any new onset or worsening of neurological signs and symptoms as outlined in physician education materials, and consider neurological referral if they occur. If PML is suspected, treatment with vedolizumab must be withheld; if confirmed, treatment must be permanently discontinued.
Malignancies
The risk of malignancy is increased in patients with ulcerative colitis and Crohn’s disease. Immunomodulatory medicinal products may increase the risk of malignancy (see section 4.8).
Prior and concurrent use of biological products
No vedolizumab clinical trial data are available for patients previously treated with natalizumab or rituximab. Caution should be exercised when considering the use of vedolizumab in these patients.
Patients previously exposed to natalizumab should normally wait a minimum of 12 weeks prior to initiating therapy with vedolizumab, unless otherwise indicated by the patient’s clinical condition. No clinical trial data for concomitant use of vedolizumab with biologic immunosuppressants are available. Therefore, the use of vedolizumab in such patients is not recommended.
Live and oral vaccines
In a placebo-controlled study of healthy volunteers, a single 750 mg dose of vedolizumab did not lower rates of protective immunity to hepatitis B virus in subjects who were vaccinated intramuscularly with 3 doses of recombinant hepatitis B surface antigen. Vedolizumab-exposed subjects had lower seroconversion rates after receiving a killed, oral cholera vaccine. The impact on other oral and nasal vaccines is unknown. It is recommended that all patients be brought up to date with all immunisations in agreement with current immunisation guidelines prior to initiating vedolizumab therapy. Patients receiving vedolizumab treatment may continue to receive non-live vaccines. There are no data on the secondary transmission of infection by live vaccines in patients receiving vedolizumab. Administration of the influenza vaccine should be by injection in line with routine clinical practice. Other live vaccines may be administered concurrently with vedolizumab only if the benefits clearly outweigh the risks.
Induction of remission in Crohn’s disease
Induction of remission in Crohn’s disease may take up to 14 weeks in some patients. The reasons for this are not fully known and are possibly related to the mechanism of action. This should be taken into consideration, particularly in patients with severe active disease at baseline not previously treated with TNFα antagonists (see also section 5.1.).
Exploratory subgroup analyses from the clinical trials in Crohn’s disease suggested that vedolizumab administered in patients without concomitant corticosteroid treatment may be less effective for induction of remission in Crohn’s disease than in those patients already receiving concomitant corticosteroids (regardless of use of concomitant immunomodulators; see section 5.1).
Sodium content
This medicine contains less than 1 mmol sodium (23 mg) per dose, that is to say essentially ‘sodium-free’.
No interaction studies have been performed.
Vedolizumab has been studied in adult ulcerative colitis and Crohn’s disease patients with concomitant administration of corticosteroids, immunomodulators (azathioprine, 6-mercaptopurine, and methotrexate), and aminosalicylates. Population pharmacokinetic analyses suggest that
co-administration of such agents did not have a clinically meaningful effect on vedolizumab pharmacokinetics. The effect of vedolizumab on the pharmacokinetics of commonly co-administered medicinal compounds has not been studied.
Vaccinations
Live vaccines, in particular live oral vaccines, should be used with caution concurrently with vedolizumab (see section 4.4).
Women of childbearing potential
Women of childbearing potential should use adequate contraception to prevent pregnancy and to continue its use for at least 18 weeks after the last treatment.
Pregnancy
There are limited amount of data from the use of vedolizumab in pregnant women.
Animal studies do not indicate direct or indirect harmful effects with respect to reproductive toxicity (see section 5.3).
As a precautionary measure, it is preferable to avoid the use of vedolizumab during pregnancy unless the benefits clearly outweigh any potential risk to both the mother and foetus.
Breast-feeding
Vedolizumab has been detected in human milk. The effect of vedolizumab on infants is unknown. The use of vedolizumab in lactating women should take into account the benefit of therapy to the mother and potential risks to the infant.
Fertility
There are no data on the effects of vedolizumab on human fertility. Effects on male and female fertility have not been formally evaluated in animal studies (see section 5.3).
Vedolizumab has minor influence on the ability to drive and use machines, as dizziness has been reported in a small number of patients.
Summary of the safety profile
The most commonly reported adverse reactions are infections (such as nasopharyngitis, upper respiratory tract infection, bronchitis, influenza and sinusitis), headache, nausea, pyrexia, fatigue, cough, arthralgia.
No clinically relevant differences in the overall safety profile and adverse reactions were observed in patients who received subcutaneous vedolizumab compared to the safety profile observed in clinical studies with intravenous vedolizumab with the exception of injection site reactions (with subcutaneous administration).
Tabulated list of adverse reactions
The following listing of adverse reactions is based on clinical trial and post marketing experience and is displayed by system organ class. Within the system organ classes, adverse reactions are listed under headings of the following frequency categories: very common (≥ 1/10), common (≥ 1/100 to < 1/10), uncommon (≥ 1/1,000 to < 1/100) and very rare (< 1/10,000). Within each frequency grouping, adverse reactions are presented in order of decreasing seriousness.
Table 1. Adverse reactions
System organ class | Frequency* | Adverse reaction(s) |
Infections and infestations | Very common | Nasopharyngitis |
Common | Bronchitis, Gastroenteritis, Upper respiratory tract infection, Influenza, Sinusitis, Pharyngitis | |
Uncommon | Respiratory tract infection, Vulvovaginal candidiasis, Oral candidiasis, Herpes zoster | |
Very rare | Pneumonia | |
Immune system disorders | Very rare | Anaphylactic reaction, Anaphylactic shock |
Nervous system disorders | Very common | Headache |
Common | Paraesthesia | |
Eye disorders | Very rare | Blurred vision |
Vascular disorders | Common | Hypertension |
Respiratory, thoracic and mediastinal disorders | Common | Oropharyngeal pain, Nasal congestion, Cough |
Gastrointestinal disorders | Common | Anal Abscess, Anal fissure, Nausea, Dyspepsia, Constipation, Abdominal distension, Flatulence, Haemorrhoids |
Skin and subcutaneous tissue disorders | Common | Rash, Pruritus, Eczema, Erythema, Night sweats, Acne |
Uncommon | Folliculitis | |
Musculoskeletal and connective tissue disorders | Very common | Arthralgia |
Common | Muscle spasms, Back pain, Muscular weakness, Fatigue, Pain in the extremity | |
General disorders and administration site conditions | Common | Pyrexia Injection site reactions# |
Uncommon | Infusion site reaction (including: Infusion site pain and Infusion site irritation), Infusion related reaction, Chills, Feeling cold |
*Frequency is based on clinical trial data with intravenous administration except where noted.
#Subcutaneous administration only.
Description of selected adverse reactions
Injection site reactions
Injection site reactions (including pain, oedema, erythema or pruritus) were reported in 5.1% of patients receiving subcutaneous vedolizumab (pooled safety analysis). None resulted in discontinuation of study treatment or changes to the dosing schedule. The majority of injection site reactions resolved within 1-4 days. There were no reports of anaphylaxis following subcutaneous vedolizumab administration.
Infections
In GEMINI 1 and 2 controlled studies with intravenous vedolizumab, the rate of infections was
0.85 per patient-year in the vedolizumab-treated patients and 0.70 per patient-year in the
placebo-treated patients. The infections consisted primarily of nasopharyngitis, upper respiratory tract infection, sinusitis, and urinary tract infections. Most patients continued on vedolizumab after the infection resolved.
In GEMINI 1 and 2 controlled studies with intravenous vedolizumab, the rate of serious infections was
0.07 per patient year in vedolizumab-treated patients and 0.06 per patient year in placebo-treated patients. Over time, there was no significant increase in the rate of serious infections.
In controlled and open-label studies in adults with intravenous vedolizumab, serious infections have been reported, which include tuberculosis, sepsis (some fatal), salmonella sepsis, listeria meningitis, and cytomegaloviral colitis.
In clinical studies with subcutaneous vedolizumab, the rate of infections was 0.26 per patient year in vedolizumab-treated patients. The most frequent infections were nasopharyngitis, upper respiratory tract infection, bronchitis and influenza.
In clinical studies with subcutaneous vedolizumab, the rate of serious infections was 0.02 per patient year in subcutaneous vedolizumab-treated patients.
In clinical studies with intravenous and subcutaneous vedolizumab, the rate of infections in vedolizumab-treated patients with BMI of 30 kg/m2 and above was higher than for those with BMI less than 30 kg/m2.
In clinical studies with intravenous and subcutaneous vedolizumab, a slightly higher incidence of serious infections was reported in vedolizumab-treated patients who had prior exposure to TNFα antagonist therapy compared to patients who were naïve to previous TNFα antagonist therapy.
Malignancy
Overall, results from the clinical program to date do not suggest an increased risk for malignancy with vedolizumab treatment; however, the number of malignancies was small and long-term exposure was limited. Long-term safety evaluations are ongoing.
Reporting of suspected adverse reactions
Reporting suspected adverse reactions after authorisation 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. the National Pharmacovigilance and Drug Safety Centre (NPC) listed below:
To report any side effect(s):
Saudi Arabia:
· Other GCC States:
- Please contact the relevant competent authority. |
Doses up to 10 mg/kg (approximately 2.5 times the recommended dose) have been administered intravenously in clinical trials. No dose-limiting toxicity was seen in clinical trials.
Pharmacotherapeutic group: immunosuppressants, selective immunosuppressants, ATC code: L04AA33.
Mechanism of action
Vedolizumab is a gut-selective immunosuppressive biologic. It is a humanised monoclonal antibody that binds specifically to the α4β7 integrin, which is preferentially expressed on gut homing T helper lymphocytes. By binding to α4β7 on certain lymphocytes, vedolizumab inhibits adhesion of these cells to mucosal addressin cell adhesion molecule-1 (MAdCAM-1), but not to vascular cell adhesion molecule-1 (VCAM-1). MAdCAM-1 is mainly expressed on gut endothelial cells and plays a critical role in the homing of T lymphocytes to tissues within the gastrointestinal tract. Vedolizumab does not bind to, nor inhibit function of, the α4β1 and αEβ7 integrins.
The α4β7 integrin is expressed on a discrete subset of memory T helper lymphocytes which preferentially migrate into the gastrointestinal (GI) tract and cause inflammation that is characteristic of ulcerative colitis and Crohn’s disease, both of which are chronic inflammatory immunologically mediated conditions of the GI tract. Vedolizumab reduces gastrointestinal inflammation in UC and CD patients. Inhibiting the interaction of α4β7 with MAdCAM-1 with vedolizumab prevents transmigration of gut-homing memory T helper lymphocytes across the vascular endothelium into parenchymal tissue in nonhuman primates and induced a reversible 3-fold elevation of these cells in peripheral blood. The murine precursor of vedolizumab alleviated gastrointestinal inflammation in colitic cotton-top tamarins, a model of ulcerative colitis.
In healthy subjects, ulcerative colitis patients, or Crohn’s disease patients, vedolizumab does not elevate neutrophils, basophils, eosinophils, B-helper and cytotoxic T lymphocytes, total memory T helper lymphocytes, monocytes or natural killer cells, in the peripheral blood with no leukocytosis observed.
Vedolizumab did not affect immune surveillance and inflammation of the central nervous system in Experimental Autoimmune Encephalomyelitis in non-human primates, a model of multiple sclerosis. Vedolizumab did not affect immune responses to antigenic challenge in the dermis and muscle (see section 4.4). In contrast, vedolizumab inhibited an immune response to a gastrointestinal antigenic challenge in healthy human volunteers (see section 4.4).
Immunogenicity
Antibodies to vedolizumab may develop during vedolizumab treatment most of which are neutralising. The formation of anti-vedolizumab antibodies is associated with increased clearance of vedolizumab and lower rates of clinical remission.
Pharmacodynamic effects
In clinical trials with intravenous vedolizumab at doses ranging from 2 to 10 mg/kg, > 95% saturation of α4β7 receptors on subsets of circulating lymphocytes involved in gut immune surveillance was observed in patients.
Clinical efficacy and safety
Ulcerative colitis - vedolizumab for intravenous administration
The efficacy and safety of intravenous vedolizumab for the treatment of adult patients with moderately to severely active ulcerative colitis (Mayo score 6 to 12 with endoscopic sub score ≥ 2) was demonstrated in a randomised, double-blind, placebo-controlled study evaluating efficacy endpoints at week 6 and week 52 (GEMINI 1). Enrolled patients had failed at least 1 conventional therapy, including corticosteroids, immunomodulators, and/or the TNFα antagonist infliximab (including primary non-responders). Concomitant stable doses of oral aminosalicylates, corticosteroids and/or immunomodulators were permitted.
For the evaluation of the week 6 endpoints, 374 patients were randomised in a double-blind fashion (3:2) to receive vedolizumab 300 mg or placebo at week 0 and week 2. Primary endpoint was the proportion of patients with clinical response (defined as reduction in complete Mayo score of
³ 3 points and ³ 30% from baseline with an accompanying decrease in rectal bleeding subscore of
³ 1 point or absolute rectal bleeding subscore of ≤ 1 point) at week 6. Table 2 shows the results from the primary and secondary endpoints evaluated.
Table 2. Week 6 efficacy results of GEMINI 1
| Placebo | Vedolizumab |
Endpoint | n = 149 | n = 225 |
Clinical response | 26% | 47%* |
Clinical remission§ | 5% | 17%† |
Mucosal healing¶ | 25% | 41%‡ |
*p < 0.0001 |
|
|
†p ≤ 0.001
‡p < 0.05
§Clinical remission: Complete Mayo score of ≤ 2 points and no individual subscore > 1 point
¶Mucosal healing: Mayo endoscopic subscore of ≤ 1 point
The beneficial effect of vedolizumab on clinical response, remission and mucosal healing was observed both in patients with no prior TNFa antagonist exposure as well as in those who had failed prior TNFa antagonist therapy.
In GEMINI 1, 2 cohorts of patients received vedolizumab at week 0 and week 2: cohort 1 patients were randomised to receive either vedolizumab 300 mg or placebo in a double-blind fashion, and cohort 2 patients were treated with open-label vedolizumab 300 mg. To evaluate efficacy at week 52, 373 patients from cohort 1 and 2 who were treated with vedolizumab and had achieved clinical response at week 6 were randomised in a double-blind fashion (1:1:1) to 1 of the following regimens beginning at week 6: vedolizumab 300 mg every 8 weeks, vedolizumab 300 mg every 4 weeks, or placebo every 4 weeks. Beginning at week 6, patients who had achieved clinical response and were receiving corticosteroids were required to begin a corticosteroid-tapering regimen. Primary endpoint was the proportion of patients in clinical remission at week 52. Table 3 shows the results from the primary and secondary endpoints evaluated.
Table 3. Week 52 efficacy results of GEMINI 1
|
Placebo | Vedolizumab IV every 8 weeks | Vedolizumab IV every 4 weeks |
Endpoint | n = 126* | n = 122 | n = 125 |
Clinical remission | 16% | 42%† | 45%† |
Durable clinical response¶ | 24% | 57%† | 52%† |
Mucosal healing | 20% | 52%† | 56%† |
Durable clinical remission# | 9% | 20%§ | 24%‡ |
Corticosteroid-free clinical remission♠ | 14% | 31%§ | 45%† |
*The placebo group includes those subjects who received vedolizumab at week 0 and week 2, and were randomised to receive placebo from week 6 through week 52.
†p < 0.0001
‡p < 0.001
§p < 0.05
¶Durable clinical response: Clinical response at weeks 6 and 52
#Durable clinical remission: Clinical remission at weeks 6 and 52
♠Corticosteroid-free clinical remission: Patients using oral corticosteroids at baseline who had discontinued corticosteroids beginning at week 6 and were in clinical remission at week 52. Patient numbers were n = 72 for placebo, n = 70 for vedolizumab every 8 weeks, and n = 73 for vedolizumab every 4 weeks
Exploratory analyses provide additional data on key subpopulations studied. Approximately one-third of patients had failed prior TNFa antagonist therapy. Among these patients, 37% receiving vedolizumab every 8 weeks, 35% receiving vedolizumab every 4 weeks, and 5% receiving placebo achieved clinical remission at week 52. Improvements in durable clinical response (47%, 43%, 16%), mucosal healing (42%, 48%, 8%), durable clinical remission (21%, 13%, 3%) and corticosteroid-free clinical remission (23%, 32%, 4%) were seen in the prior TNFα antagonist failure population treated with vedolizumab every 8 weeks, vedolizumab every 4 weeks and placebo, respectively.
Patients who failed to demonstrate response at week 6 remained in the study and received vedolizumab every 4 weeks. Clinical response using partial Mayo scores was achieved at week 10 and week 14 by greater proportions of vedolizumab patients (32% and 39%, respectively) compared with placebo patients (15% and 21%, respectively).
Patients who lost response to vedolizumab when treated every 8 weeks were allowed to enter an open-label extension study and receive vedolizumab every 4 weeks. In these patients, clinical remission was achieved in 25% of patients at week 28 and week 52.
Patients who achieved a clinical response after receiving vedolizumab at week 0 and 2 and were then randomised to placebo (for 6 to 52 weeks) and lost response were allowed to enter the open-label extension study and receive vedolizumab every 4 weeks. In these patients, clinical remission was achieved in 45% of patients by 28 weeks and 36% of patients by 52 weeks.
In this open-label extension study, the benefits of vedolizumab treatment as assessed by partial Mayo score, clinical remission, and clinical response were shown for up to 196 weeks.
Health-related quality of life (HRQOL) was assessed by Inflammatory Bowel Disease Questionnaire (IBDQ), a disease specific instrument, and SF-36 and EQ-5D, which are generic measures.
Exploratory analysis show clinically meaningful improvements were observed for vedolizumab groups, and the improvements were significantly greater as compared with the placebo group at week 6 and week 52 on EQ-5D and EQ-5D VAS scores, all subscales of IBDQ (bowel symptoms, systemic function, emotional function and social function), and all subscales of SF-36 including the Physical Component Summary (PCS) and Mental Component Summary (MCS).
Ulcerative colitis - vedolizumab for subcutaneous administration
The efficacy and safety of subcutaneous vedolizumab for the treatment of adult patients with moderately to severely active ulcerative colitis (Mayo score 6 to 12 with endoscopic sub score ≥ 2) was demonstrated in a randomised, double-blind, placebo-controlled study evaluating efficacy endpoints at week 52 (VISIBLE 1). In VISIBLE 1, enrolled patients (n = 383) had failed at least
1 conventional therapy, including corticosteroids, immunomodulators, and/or TNFα antagonists (including primary non responders). Concomitant stable doses of oral aminosalicylates, corticosteroids and/or immunomodulators were permitted.
Patients who achieved clinical response to open-label treatment with intravenous vedolizumab at week 6 were eligible to be randomised For the evaluation of the week 52 endpoints, 216 (56.4%) patients were randomised and treated in a double-blind fashion (2:1:1) to 1 of the following regimens:
subcutaneous vedolizumab 108 mg every 2 weeks, intravenous vedolizumab 300 mg every 8 weeks, or placebo.
The baseline demographics were similar for patients in vedolizumab and placebo groups. The baseline Mayo score was between 9 to 12 (severe ulcerative colitis) in about 62% and 6 to 8 (moderate ulcerative colitis) in about 38% of the overall study population.
Primary study endpoint clinical remission was defined as a complete Mayo score of ≤ 2 points and no individual subscore > 1 point at 52 weeks in patients who had achieved a clinical response at week 6 of intravenous vedolizumab induction treatment. Clinical response was defined as a reduction in complete Mayo score of ≥ 3 points and ≥ 30% from baseline with an accompanying decrease in rectal bleeding subscore of ≥ 1 point or absolute rectal bleeding subscore of ≤ 2 points and no individual subscore >1 point.
Table 4 shows the evaluated results from the primary and secondary endpoints.
Table 4. Week 52 efficacy results of VISIBLE I
|
Vedolizumab
Estimatec of
Endpointa Placebo n = 56
SC 108 mg
every 2 weeks
n = 106
300 mg
every 8 weeks
n = 54
difference (95% CI)
Vedolizumab SC vs. Placebo
P-valuec
Clinical remissiond 14.3% 46.2% 42.6% 32.3 (19.7, 45.0) p < 0.001
Mucosal healinge 21.4% 56.6% 53.7% 35.7 (22.1, 49.3) p < 0.001
Durable clinical responsef
Durable clinical remissiong
Corticosteroid-free remissionh
28.6% 64.2% 72.2% 36.1 (21.2, 50.9) p < 0.001
5.4% 15.1% 16.7% 9.7 (-6.6, 25.7) p = 0.076
(NS)
8.3% 28.9% 28.6% 20.6 (-4.5, 43.7) p = 0.067
(NS)
aEndpoints are presented in the order that fixed-sequence testing was performed for control of Type 1 error at 5% bThe placebo group includes those subjects who received intravenous vedolizumab at week 0 and week 2, and were randomised to receive placebo from week 6 through week 52.
cEstimate of treatment difference and the p-value for all endpoints is based on the Cochrane-Mantel-Haenszel method
dClinical remission: Complete Mayo score of ≤ 2 points and no individual subscore > 1 point at week 52
eMucosal healing: Mayo endoscopic subscore of ≤ 1 point fDurable clinical response: Clinical response at weeks 6 and 52 gDurable clinical remission: Clinical remission at weeks 6 and 52
hCorticosteroid-free clinical remission: Patients using oral corticosteroids at baseline who had discontinued corticosteroids and were in clinical remission at week 52. Patient numbers using oral corticosteroids at baseline were n = 24 for placebo, n = 45 for subcutaneous vedolizumab and n = 21 for intravenous vedolizumab
NS = non significant (2-tailed p-value > 0.05)
The primary and secondary endpoints were analysed in subgroups of patients who had failed prior TNFα antagonist therapy (37%; n = 80) and patients who were naïve to previous TNFα antagonist therapy (63%; n = 136). Results of study patients treated with placebo and subcutaneous vedolizumab in these subgroups are presented in Table 5.
Table 5. VISIBLE 1 Study results at week 52 analysed by response to prior previous TNFα antagonist therapy
Treatment once every 2 weeks
| Placebo | Vedolizumab SC 108 mg |
Failure prior TNFα antagonist therapy | n = 19 | n = 39 |
Clinical remission | 5.3% | 33.3% |
Mucosal healing | 5.3% | 46.2% |
Durable clinical response | 15.8% | 66.7% |
Durable clinical remission | 0% | 2.6% |
Corticosteroid free clinical remissiona | 8.3% | 27.3% |
Naive TNFα antagonist therapy |
n = 37 |
n = 67 |
Clinical remission | 18.9% | 53.7% |
Mucosal healing | 29.7% | 62.7% |
Durable clinical response | 35.1% | 62.7% |
Durable clinical remission | 8.1% | 22.4% |
Corticosteroid free clinical remissionb | 8.3% | 30.4% |
a Patients who had failed prior TNFα antagonist therapy and using oral corticosteroids at baseline were n = 12 for placebo and n = 22 for subcutaneous vedolizumab
b Patients who were naïve to prior TNFα antagonist therapy and using oral corticosteroids at baseline were n = 12 for placebo and n = 23 for subcutaneous vedolizumab
Health related quality of life (HRQOL) was assessed by Inflammatory Bowel Disease Questionnaire (IBDQ), a disease specific instrument, and EuroQol-5 Dimension (EQ-5D, including EQ 5D VAS), which is a generic measure. Work productivity was assessed by work productivity and activity impairment questionnaire (WPAI-UC). Patients treated with subcutaneous vedolizumab maintained improvements in IBDQ, EQ-5D and WPAI-UC scores at week 52 to a greater extent than patients who received placebo.
Patients who completed VISIBLE 1 were eligible to enrol in an ongoing, open-label extension study to evaluate long-term safety and efficacy of subcutaneous vedolizumab treatment in patients with ulcerative colitis or Crohn’s disease.
Patients in VISIBLE 1 who did not achieve clinical response at week 6 received a third dose of vedolizumab 300 mg by intravenous infusion at week 6. Of patients who received a third dose of vedolizumab 300 mg by intravenous infusion at week 6, 79.7% (114/143) achieved a clinical response at week 14. Patients who achieved a clinical response at week 14 were eligible to enter the open-label extension study and receive subcutaneous vedolizumab 108 mg every 2 weeks. Clinical remission as assessed by the partial Mayo score (a standardised measure that includes 3 of the 4 scored subscales of the complete Mayo score: stool frequency, rectal bleeding, and physician global assessment) was achieved by 39.2% (40/102) of these patients at week 40 after transitioning to subcutaneous vedolizumab in the open-label extension study.
Patients randomised to intravenous vedolizumab treatment group in VISIBLE 1 received vedolizumab 300 mg intravenously at weeks 0, 2, and 6 and every 8 weeks thereafter until week 52. At week 52, these patients entered the open-label extension study and received subcutaneous vedolizumab 108 mg every 2 weeks. Clinical remission as assessed by the partial Mayo score was maintained in 77% of
patients at 24 weeks after transitioning to subcutaneous vedolizumab in the open-label extension study.
Crohn’s disease – vedolizumab for intravenous administration
The efficacy and safety of intravenous vedolizumab for the treatment of adult patients with moderately to severely active Crohn’s disease (Crohn’s Disease Activity Index [CDAI] score of 220 to 450) were evaluated in 2 studies (GEMINI 2 and 3). Enrolled patients have failed at least 1 conventional therapy, including corticosteroids, immunomodulators, and/or TNFα antagonists (including primary
non-responders). Concomitant stable doses of oral corticosteroids, immunomodulators, and antibiotics were permitted.
The GEMINI 2 Study was a randomised, double-blind, placebo-controlled study evaluating efficacy endpoints at week 6 and week 52. Patients (n = 368) were randomised in a double-blind fashion (3:2) to receive 2 doses of vedolizumab 300 mg or placebo at week 0 and week 2. The 2 primary endpoints were the proportion of patients in clinical remission (defined as CDAI score ≤ 150 points) at week 6 and the proportion of patients with enhanced clinical response (defined as a ≥ 100-point decrease in CDAI score from baseline) at week 6 (see Table 6).
GEMINI 2 contained 2 cohorts of patients that received vedolizumab at weeks 0 and 2:
cohort 1 patients were randomised to receive either vedolizumab 300 mg or placebo in a double-blind fashion, and cohort 2 patients were treated with open-label vedolizumab 300 mg. To evaluate efficacy at week 52, 461 patients from cohorts 1 and 2, who were treated with vedolizumab and had achieved clinical response (defined as a ≥ 70-point decrease in CDAI score from baseline) at week 6, were randomised in a double-blind fashion (1:1:1) to 1 of the following regimens beginning at week 6: vedolizumab 300 mg every 8 weeks, vedolizumab 300 mg every 4 weeks, or placebo every 4 weeks. Patients showing clinical response at week 6 were required to begin corticosteroid tapering. Primary endpoint was the proportion of patients in clinical remission at week 52 (see Table 7).
The GEMINI 3 Study was a second randomised, double-blind, placebo-controlled study that evaluated efficacy at week 6 and week 10 in the subgroup of patients defined as having failed at least
1 conventional therapy and failed TNFa antagonist therapy (including primary non-responders) as well as the overall population, which also included patients who failed at least 1 conventional therapy and were naïve to TNFa antagonist therapy. Patients (n = 416), which included approximately 75% TNFa antagonist failures patients, were randomised in a double-blind fashion (1:1) to receive either vedolizumab 300 mg or placebo at weeks 0, 2, and 6. The primary endpoint was the proportion of patients in clinical remission at week 6 in the TNFa antagonist failure subpopulation. As noted in Table 6, although the primary endpoint was not met, exploratory analyses show that clinically meaningful results were observed.
Table 6. Efficacy results for GEMINI 2 and 3 studies at week 6 and week 10
Study Endpoint |
Placebo |
Vedolizumab IV |
GEMINI 2 Study |
|
|
Clinical remission, week 6 |
|
|
Overall | 7% (n = 148) | 15%* (n = 220) |
TNFα Antagonist(s) Failure | 4% (n = 70) | 11% (n = 105) |
TNFα Antagonist(s) Naïve | 9% (n = 76) | 17% (n = 109) |
Enhanced clinical response, week 6 |
|
|
Overall | 26% (n = 148) | 31%† (n = 220) |
TNFα Antagonist(s) Failure | 23% (n = 70) | 24% (n = 105) |
TNFα Antagonist(s) Naïve | 30% (n = 76) | 42% (n = 109) |
Serum CRP change from baseline to week 6, median (mcg/mL) |
|
|
Overall‡ | -0.5 (n = 147) | -0.9 (n = 220) |
GEMINI 3 Study
Clinical remission, week 6
Overall‡ TNFα Antagonist(s) Failure¶ TNFα Antagonist(s) Naïve Clinical remission, week 10 | 12% (n = 207) 12% (n = 157) 12% (n = 50) | 19% (n = 209) 15%§ (n = 158) 31% (n = 51) |
Overall | 13% (n = 207) | 29% (n = 209) |
TNFα Antagonist(s) Failure¶,‡ | 12% (n = 157) | 27% (n = 158) |
TNFα Antagonist(s) Naïve Sustained clinical remission#,¶ | 16% (n = 50) | 35% (n = 51) |
Overall | 8% (n = 207) | 15% (n = 209) |
TNFα Antagonist(s) Failure¶,‡ | 8% (n = 157) | 12% (n = 158) |
TNFα Antagonist(s) Naïve | 8% (n = 50) | 26% (n = 51) |
Enhanced clinical response, week 6 |
|
|
Overall^ | 23% (n = 207) | 39% (n = 209) |
TNFα Antagonist(s) Failure‡ | 22% (n = 157) | 39% (n = 158) |
TNFα Antagonist(s) Naïve^ | 24% (n = 50) | 39% (n = 51) |
*p < 0.05
†not statistically significant
‡secondary endpoint to be viewed as exploratory by pre-specified statistical testing procedure
§not statistically significant, the other endpoints were therefore not tested statistically
¶n = 157 for placebo and n = 158 for vedolizumab
#Sustained clinical remission: clinical remission at weeks 6 and 10
^Exploratory Endpoint
Table 7. Efficacy results for GEMINI 2 at week 52
|
Placebo | Vedolizumab IV every 8 weeks | Vedolizumab IV every 4 weeks |
n = 153* | n = 154 | n = 154 | |
Clinical remission | 22% | 39%† | 36%‡ |
Enhanced clinical response | 30% | 44%‡ | 45%‡ |
Corticosteroid-free clinical remission§ | 16% | 32%‡ | 29%‡ |
Durable clinical remission¶ | 14% | 21% | 16% |
*The placebo group includes those subjects who received vedolizumab at week 0 and week 2, and were randomised to receive placebo from week 6 through week 52.
†p < 0.001
‡p < 0.05
§Corticosteroid-free clinical remission: Patients using oral corticosteroids at baseline who had discontinued corticosteroids beginning at week 6 and were in clinical remission at week 52. Patient numbers were n = 82 for placebo, n = 82 for vedolizumab every 8 weeks, and n = 80 for vedolizumab every 4 weeks
¶Durable clinical remission: Clinical remission at ≥ 80% of study visits including final visit (week 52)
Exploratory analyses examined the effects of concomitant corticosteroids and immunomodulators on induction of remission with vedolizumab. Combination treatment, most notably with concomitant corticosteroids, appeared to be more effective in inducing remission in Crohn’s disease than vedolizumab alone or with concomitant immunomodulators, which showed a smaller difference from placebo in the rate of remission. Clinical remission rate in GEMINI 2 at week 6 was 10% (difference from placebo 2%, 95% CI: -6, 10) when administered without corticosteroids compared to 20%
(difference from placebo 14%, 95% CI: -1, 29) when administered with concomitant corticosteroids. In GEMINI 3 at week 6 and 10 the respective clinical remission rates were 18% (difference from placebo 3%, 95% CI: -7, 13) and 22% (difference from placebo 8%, 95% CI: -3, 19) when
administered without corticosteroids compared to 20% (difference from placebo 11%, 95% CI: 2, 20)
and 35% (difference from placebo 23%, 95% CI: 12, 33) respectively when administered with concomitant corticosteroids. These effects were seen whether or not immunomodulators were also concomitantly administered.
Exploratory analyses provide additional data on key subpopulations studied. In GEMINI 2, approximately half of patients had previously failed TNFα antagonist therapy. Among these patients, 28% receiving vedolizumab every 8 weeks, 27% receiving vedolizumab every 4 weeks, and 13% receiving placebo achieved clinical remission at week 52. Enhanced clinical response was achieved in 29%, 38%, 21%, respectively, and corticosteriod-free clinical remission was achieved in 24%, 16%, 0%, respectively.
Patients who failed to demonstrate response at week 6 in GEMINI 2 were retained in the study and received vedolizumab every 4 weeks. Enhanced clinical response was observed at week 10 and week 14 for greater proportions of vedolizumab patients 16% and 22%, respectively, compared with placebo patients 7% and 12%, respectively. There was no clinically meaningful difference in clinical remission between treatment groups at these time points. Analyses of week 52 clinical remission in patients who were non-responders at week 6 but achieved response at week 10 or week 14 indicate that non-responder CD patients may benefit from a dose of vedolizumab at week 10.
Patients who lost response to vedolizumab when treated every 8 weeks in GEMINI 2 were allowed to enter an open-label extension study and received vedolizumab every 4 weeks. In these patients, clinical remission was achieved in 23% of patients at week 28 and 32% of patients at week 52.
Patients who achieved a clinical response after receiving vedolizumab at week 0 and 2 and were then randomised to placebo (for 6 to 52 weeks) and lost response were allowed to enter the open-label extension study and receive vedolizumab every 4 weeks. In these patients, clinical remission was achieved in 46% of patients by 28 weeks and 41% of patients by 52 weeks.
In this open-label extension study, clinical remission and clinical response were observed in patients for up to 196 weeks.
Exploratory analysis showed clinically meaningful improvements were observed for the vedolizumab every 4 weeks and every 8 weeks groups in GEMINI 2 and the improvements were significantly greater as compared with the placebo group from baseline to week 52 on EQ-5D and EQ-5D VAS scores, total IBDQ score, and IBDQ subscales of bowel symptoms and systemic function.
Crohn’s disease - vedolizumab for subcutaneous administration
The efficacy and safety of subcutaneous vedolizumab for the treatment of adult patients with moderately to severely active Crohn’s disease (CDAI score of 220 to 450) was demonstrated in a randomised, double-blind, placebo-controlled study evaluating efficacy endpoints at
week 52 (VISIBLE 2). In VISIBLE 2, enrolled patients (n = 644) had inadequate response to, loss of response to, or intolerance to one conventional therapy, including corticosteroids, immunomodulators, and/or TNFα antagonists (including primary non-responders). Concomitant stable doses of oral aminosalicylates, corticosteroids and/or immunomodulators were permitted.
Patients who achieved clinical response to open-label treatment with intravenous vedolizumab at week 6 were eligible to be randomised. For the evaluation of the week 52 endpoints, 409 (64%) patients were randomised and treated in a double-blind fashion (2:1) to receive subcutaneous vedolizumab 108 mg (n = 275) or subcutaneous placebo (n = 134) every 2 weeks.
The baseline demographics were similar for patients in vedolizumab and placebo groups. The baseline CDAI was > 330 (severe Crohn’s disease) in about 41% and ≤ 330 (moderate Crohn’s disease) in about 59% of the overall study population.
Beginning at week 6, patients who had achieved clinical response (defined as a ≥ 70-point decrease in the CDAI score from baseline) and were receiving corticosteroids were required to begin a corticosteroid tapering regimen. Primary endpoint was the proportion of patients with clinical remission (CDAI score ≤ 150) at week 52. The secondary endpoints were the proportion of patients with enhanced clinical response ( ≥ 100 point decrease in CDAI score from baseline) at week 52, the proportion of patients with corticosteroid-free remission (patients using oral corticosteroids at baseline who had discontinued corticosteroids and were in clinical remission) at week 52, and the proportion of TNFα antagonist naïve patients who achieved clinical remission (CDAI score ≤ 150) at week 52.
Table 8 shows the evaluated results from the primary and secondary endpoints.
Table 8. Week 52 efficacy results of VISIBLE 2
Vedolizumab
Estimate‡ of
Endpoint
* Placebo†
n = 134
SC 108 mg
every 2 weeks
n = 275
treatment difference (95% CI)
Vedolizumab SC vs.
Placebo
P-value‡
Clinical remission§ 34.3% 48.0% 13.7 (3.8, 23.7) p = 0.008
|
Enhanced clinical response# 44.8% 52.0% 7.3 (-3.0, 17.5) p = 0.167
remission**
antagonist naïve patients††
*Endpoints are presented in the order that fixed-sequence testing was performed for control of Type 1 error at 5%
†The placebo group includes those subjects who received intravenous vedolizumab at week 0 and week 2, and were randomised to receive placebo from week 6 through week 52.
‡Estimate of treatment difference and the p-value for all endpoints is based on the Cochrane-Mantel-Haenszel method
§Clinical remission: CDAI score ≤ 150, at week 52
#Enhanced clinical response: ≥ 100-point decrease in CDAI score from baseline (week 0), at week 52
**Corticosteroid-free clinical remission: Patients using oral corticosteroids at baseline who had discontinued corticosteroids and were in clinical remission at week 52. Patient numbers using oral corticosteroids at baseline were n = 44 for placebo and n = 95 for subcutaneous vedolizumab.
†† Clinical remission (CDAI score ≤ 150, at week 52) in TNFα antagonist naïve patients (n = 63 placebo; n = 107 subcutaneous vedolizumab
‡‡ nominal p-value
NS = non significant (2-tailed p-value > 0.05)
The primary and secondary endpoints were analysed in subgroups of patients who were naïve to prior TNFα antagonist therapy (42%; n = 170), patients who had failed prior TNFα antagonist therapy (51%; n = 210), and patients who had exposure to prior TNFα antagonist therapy but did not experience treatment failure (7%; n = 29). Results of study patients treated with placebo and subcutaneous vedolizumab in these subgroups are presented in Tables 9 and 10.
Table 9. Week 52 efficacy results in TNFα antagonist naïve patients in VISIBLE 2
|
| Treatment difference | |
Vedolizumab SC 108 mg | (95% CI) | ||
| Placebo | every 2 weeks | Vedolizumab SC vs. |
Endpoint | n = 63 | n = 107 | Placebo |
Clinical remission | 42.9% | 48.6% | 4.3 (-11.6, 20.3) |
Enhanced clinical response | 47.6% | 54.2% | 4.4 (-11.6, 20.3) |
Corticosteroid-free remission** | 18.2% | 41.0% | 22.8 (-3.2, 46.8) |
** Patients who were naïve to prior TNFα antagonist therapy and using oral corticosteroids at baseline were n = 22 for placebo and n = 39 for subcutaneous vedolizumab
Table 10. Week 52 efficacy results in patients who failed TNFα antagonist therapy in VISIBLE 2
|
|
| Treatment difference |
|
| Vedolizumab SC 108 mg | (95% CI) |
| Placebo | every 2 weeks | Vedolizumab SC vs. |
Endpoint | n = 59 | n = 151 | Placebo |
Clinical remission | 28.8% | 46.4% | 17.6 (3.8, 31.4) |
Enhanced clinical response | 45.8% | 49.0% | 3.2 (-11.8, 18.2) |
Corticosteroid-free remission** | 15.0% | 46.2% | 31.2 (5.2, 54.5) |
** Patients who had failed prior TNFα antagonist therapy and using oral corticosteroids at baseline were n = 20 for placebo and n = 52 for subcutaneous vedolizumab
HRQOL was assessed by IBDQ, a disease specific instrument, and EQ-5D (including EQ-5D VAS), which is a generic measure. Work productivity was assessed by WPAI-CD. Patients treated with subcutaneous vedolizumab maintained improvements in IBDQ, EQ-5D and WPAI-CD scores at week 52 to a greater extent than patients who received placebo.
Patients who completed VISIBLE 2 were eligible to enrol in an ongoing, open-label extension study to evaluate long-term safety and efficacy of subcutaneous vedolizumab treatment in patients with ulcerative colitis or Crohn’s disease.
Paediatric population
The European Medicines Agency has deferred the obligation to submit the results of studies with vedolizumab in 1 or more subsets of the paediatric population in ulcerative colitis and Crohn’s disease (see section 4.2 for information on paediatric use).
The single and multiple dose pharmacokinetics of vedolizumab have been studied in healthy subjects and in patients with moderate to severely active ulcerative colitis or Crohn’s disease.
Absorption
In patients administered 300 mg intravenous vedolizumab as a 30-minute intravenous infusion on weeks 0 and 2, mean serum trough concentrations at week 6 were 27.9 mcg/mL (SD ± 15.51) in ulcerative colitis and 26.8 mcg/mL (SD ± 17.45) in Crohn’s disease. In studies with intravenous vedolizumab, starting at week 6, patients received 300 mg intravenous vedolizumab every 8 or
4 weeks. In patients with ulcerative colitis, mean steady-state serum trough concentrations were
11.2 mcg/mL (SD ± 7.24) and 38.3 mcg/mL (SD ± 24.43), respectively. In patients with Crohn's disease mean steady-state serum trough concentrations were 13.0 mcg/mL (SD ± 9.08)
and 34.8 mcg/mL (SD ± 22.55), respectively.
In studies in patients with ulcerative colitis or Crohn’s disease receiving subcutaneous vedolizumab, starting at week 6, patients received 108 mg subcutaneous vedolizumab every 2 weeks. The mean steady state serum trough concentrations were 35.8 mcg/mL (SD ± 15.2) in patients with ulcerative colitis and 31.4 mcg/mL (SD ± 14.7) in patients with Crohn’s disease. The bioavailability of vedolizumab following single-dose subcutaneous administration of 108 mg relative to single-dose intravenous administration was approximately 75%. The median time to reach maximum serum concentration (tmax) was 7 days (range 3 to 14 days), and the mean maximum serum concentration (Cmax) was 15.4 mcg/mL (SD ± 3.2).
Distribution
Population pharmacokinetic analyses indicate that the distribution volume of vedolizumab is approximately 5 litres. The plasma protein binding of vedolizumab has not been evaluated. Vedolizumab is a therapeutic monoclonal antibody and is not expected to bind to plasma proteins.
Vedolizumab does not pass the blood brain barrier after intravenous administration. Vedolizumab 450 mg administered intravenously was not detected in the cerebrospinal fluid of healthy subjects.
Elimination
Population pharmacokinetic analyses indicate that vedolizumab has a total body clearance of approximately 0.169 L/day and a serum half-life of 24 days. The exact elimination route of vedolizumab is not known. Population pharmacokinetic analyses suggest that while low albumin, higher body weight and prior treatment with anti-TNF drugs may increase vedolizumab clearance, the magnitude of their effects is not considered to be clinically relevant.
Linearity
Vedolizumab exhibited linear pharmacokinetics at serum concentrations greater than 1 mcg/mL. Special populations
Age does not impact the vedolizumab clearance in ulcerative colitis and Crohn’s disease patients based on the population pharmacokinetic analyses. No formal studies have been conducted to examine the effects of either renal or hepatic impairment on the pharmacokinetics of vedolizumab.
Non-clinical data reveal no special hazard for humans based on conventional studies of safety pharmacology, repeated dose toxicity, genotoxicity, carcinogenic potential, toxicity to reproduction and development.
Long-term animal studies with vedolizumab to assess its carcinogenic potential have not been conducted because pharmacologically responsive models to monoclonal antibodies do not exist. In a pharmacologically responsive species (cynomolgus monkeys), there was no evidence of cellular hyperplasia or systemic immunomodulation that could potentially be associated with oncogenesis in 13- and 26-week toxicology studies. Furthermore, no effects were found of vedolizumab on the proliferative rate or cytotoxicity of a human tumor cell line expressing the α4β7 integrin in vitro.
No specific fertility studies in animals have been performed with vedolizumab. No definitive conclusion can be drawn on the male reproductive organs in cynomolgus monkey repeated dose toxicity study. Given the lack of binding of vedolizumab to male reproductive tissue in monkey and human, and the intact male fertility observed in β7 integrin-knockout mice, it is not expected that vedolizumab will affect male fertility.
Administration of vedolizumab to pregnant cynomolgus monkeys during most of gestation resulted in no evidence of effects on teratogenicity, prenatal or postnatal development in infants up to 6 months of age. Low levels (< 300 mcg/L) of vedolizumab were detected on post-partum day 28 in the milk of 3 of 11 cynomolgus monkeys treated 100 mg/kg of vedolizumab dosed every 2 weeks and not in any animals that received 10 mg/kg.
Citric acid monohydrate
Sodium citrate dihydrate
L-histidine
L-histidine monohydrochloride
L-arginine hydrochloride
Polysorbate 80
Water for injections
In the absence of compatibility studies, this medicinal product must not be mixed with other medicinal products
Store in a refrigerator (2 °C-8 °C). Keep the pre-filled syringe or pre-filled pen in the outer carton in order to protect from light.
Do not freeze.
If needed, the pre-filled syringe and pre-filled pen can be left out of the refrigerator in its original carton at room temperature (up to 25 °C) for up to 7 days. Do not use the pre-filled syringe or pre-filled pen if left out of the refrigerator for more than 7 days.
Entyvio 108 mg solution for injection in pre-filled syringe
Solution for injection in a Type I glass 1 mL syringe with a fixed 27 gauge thin wall, 1.27 cm needle. The syringe has a rubber needle cover encased in a plastic shell and rubber stopper.
The subcutaneous vedolizumab pre-filled syringe is a single dose, disposable drug delivery system with manual injection operation. Each pre-filled syringe is equipped with a safety device that activates to extend and lock a guard over the needle once the injection is completed.
Packs of 1 pre-filled syringe, and multipacks of 2 (2 packs of 1) or 6 (6 packs of 1) pre-filled syringes. Entyvio 108 mg solution for injection in pre-filled pen
Solution for injection in a pre-filled pen in a Type I glass 1 mL syringe and a fixed 27 gauge thin wall,
1.27 cm needle. The syringe has a rubber needle cover encased in a plastic shell and rubber stopper. The subcutaneous vedolizumab pre-filled pen is a single dose, disposable drug delivery system with mechanical injection operation. Each pre-filled pen is equipped with an automated needle shield to extend and lock over the needle once the device is removed from the injection site.
Packs of 1 pre-filled pen, and multipacks of 2 (2 packs of 1) or 6 (6 packs of 1) pre-filled pens. Not all pack sizes may be marketed.
Instructions for administration
After removing the pre-filled syringe or pre-filled pen from the refrigerator, wait 30 minutes before injecting to allow the solution to reach room temperature.
Do not leave the pre-filled syringe or pre-filled pen in direct sunlight. Do not freeze. Do not use if it has been frozen.
Inspect the solution visually for particulate matter and discoloration prior to administration. The solution should be colorless to yellow. Do not use pre-filled syringe or pre-filled pen with visible particulate matter or discoloration.
Each pre-filled syringe or pre-filled pen is for single use only.
Any unused medicinal product or waste material should be disposed of in accordance with local requirements.