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  SFDA PIL (Patient Information Leaflet (PIL) are under review by Saudi Food and Drug Authority)

What Bimzelx is

Bimzelx contains the active substance bimekizumab.

 

What Bimzelx is used for

Bimzelx is used to treat the following inflammatory diseases:

• Plaque psoriasis

• Psoriatic arthritis

• Axial spondyloarthritis, including non-radiographic axial spondyloarthritis and ankylosing spondylitis (radiographic axial spondyloarthritis)

 

Plaque psoriasis

Bimzelx is used in adults to treat a skin condition called plaque psoriasis. Bimzelx reduces the symptoms, including pain, itching, and scaling of the skin.

 

Psoriatic arthritis

Bimzelx is used to treat adults with psoriatic arthritis. Psoriatic arthritis is a disease that causes inflamed joints, often accompanied by plaque psoriasis. If you have active psoriatic arthritis, you may first be given other medicines. If these medicines do not work well enough or in case of intolerance, you will be given Bimzelx either alone or in combination with another medicine called methotrexate.

 

Bimzelx reduces inflammation and can therefore help to reduce pain, stiffness, swelling in and around your joints, psoriatic skin rash, psoriatic nail damage and slow down the damage to the cartilage and bone of the joints involved in the disease. These effects can help you to control signs and symptoms of the disease, ease your normal daily activities, reduce tiredness, and improve your quality of life.

 

Axial spondyloarthritis, including non-radiographic axial spondyloarthritis and ankylosing spondylitis (radiographic axial spondyloarthritis)

Bimzelx is used to treat adults with an inflammatory disease primarily affecting the spine which causes inflammation of the spinal joints, called axial spondyloarthritis. If the condition is not visible using X-rays, it is referred to as “non-radiographic axial spondyloarthritis”; if it occurs in patients with visible signs on X-rays, it is referred to as “ankylosing spondylitis” or “radiographic axial spondyloarthritis”.

 

If you have axial spondyloarthritis you will first be given other medicines. If you do not respond well enough to these medicines, you will be given Bimzelx to reduce the signs and symptoms of the disease, reduce inflammation and improve your physical function. Bimzelx can help to reduce back pain, stiffness and tiredness, which can ease your normal daily activities and improve your quality of life.

 

How Bimzelx works

Bimekizumab, the active substance in Bimzelx, belongs to a group of medicines called interleukin (IL) inhibitors. Bimekizumab works by reducing the activity of two proteins called IL-17A and IL-17F, which are involved in causing inflammation. There are higher levels of these proteins in inflammatory diseases such as psoriasis, psoriatic arthritis and axial spondyloarthritis.


Do not use Bimzelx

·            if you are allergic to bimekizumab or any of the other ingredients of this medicine (listed in

 section 6).

·            if you have an infection, including tuberculosis (TB), which your doctor thinks is important.

 

Warnings and precautions

Talk to your doctor, pharmacist or nurse before using Bimzelx if:

·            you have an infection or an infection that keeps coming back.

·            you recently had or plan to have a vaccination. You should not be given certain types of vaccines (live vaccines) while using Bimzelx.

·            you have ever had tuberculosis (TB).

·            you have ever had inflammatory bowel disease (Crohn’s disease or ulcerative colitis).

 

Inflammatory bowel disease (Crohn’s disease or ulcerative colitis)

Stop using Bimzelx and tell your doctor or get medical help immediately if you notice blood in the stool, abdominal cramps, pain, diarrhoea or weight loss. These may be signs of new or worsening inflammatory bowel disease (Crohn’s disease or ulcerative colitis).

 

Look out for infections and allergic reactions

Bimzelx can rarely cause serious infections. Talk to your doctor or get medical help immediately if you notice any signs of a serious infection. Such signs are listed under “Serious side effects” in section 4.

 

Bimzelx can potentially cause serious allergic reactions. Talk to your doctor or get medical help immediately if you notice any signs of a serious allergic reaction. Such signs may include:

·            difficulty breathing or swallowing

·            low blood pressure, which can make you dizzy or light-headed

·            swelling of the face, lips, tongue or throat

·            severe itching of the skin, with a red rash or raised bumps.

 

Children and adolescents

Do not give this medicine to children and young people under 18 years of age. This is because it has not been studied in this age group.

 

Other medicines and Bimzelx

Tell your doctor or pharmacist if you are using, have recently used or might use any other medicines.

 

Pregnancy, breast-feeding and fertility

If you are pregnant, think you may be pregnant or are planning to have a baby, ask your doctor for advice before using this medicine. It is preferable to avoid the use of Bimzelx in pregnancy. This is because it is not known how this medicine will affect the baby.

 

If you are a woman who can become pregnant, you should use contraception while using this medicine and for at least 17 weeks after your last dose of Bimzelx.

 

If you are breast-feeding or are planning to breast-feed, talk to your doctor before using this medicine. You and your doctor should decide if you can breast-feed or use Bimzelx.

 

Driving and using machines

Bimzelx is unlikely to affect your ability to drive and use machines.

 

Bimzelx contains sodium

This medicine contains less than 1 mmol (23 mg) sodium 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.

 

How much Bimzelx is given and for how long

 

Plaque psoriasis

The recommended dose, given as injections under your skin (‘subcutaneous injections’) is as follows:

·            320 mg (given as two pre-filled pens, containing 160 mg each) at weeks 0, 4, 8, 12, 16.

·            From week 16, you will use 320 mg (two pre-filled pens, containing 160 mg each) every 8 weeks. If you weigh more than 120 kg, your doctor may decide to continue your injections every 4 weeks from week 16.

 

Psoriatic arthritis

The recommended dose, given as an injection under your skin (‘subcutaneous injections’) is as follows:

  • 160 mg (given as one pre-filled pen) every 4 weeks.
  • If you have psoriatic arthritis with coexistent moderate to severe plaque psoriasis, the recommended dose regimen is the same as for plaque psoriasis. After Week 16, your doctor may adapt your injections to 160 mg every 4 weeks, depending on your joint symptoms.

Axial spondyloarthritis, including non-radiographic axial spondyloarthritis and ankylosing spondylitis (radiographic axial spondyloarthritis)

The recommended dose, given as an injection under your skin (‘subcutaneous injections’) is 160 mg (given as one pre-filled pen) every 4 weeks.

You and your doctor or nurse will decide if you should inject this medicine yourself. Do not inject this medicine unless you have been trained by a healthcare professional. A caregiver may also give your injections after they have been trained.

Read the ‘Instructions for use’ at the end of this leaflet before injecting Bimzelx pre-filled pen yourself.

If you use more Bimzelx than you should

Tell your doctor if you have used more Bimzelx than you should or if you have injected your dose earlier than you should.

 

If you forget to use Bimzelx

Talk to your doctor if you have forgotten to inject a dose of Bimzelx.

 

If you stop using Bimzelx

Talk to your doctor before you stop using Bimzelx. If you stop treatment, your symptoms may come back.

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 or get medical help immediately if you get any of the following side effects:

 

Possible serious infection - the signs may include:

·            fever, flu-like symptoms, night sweats

·            feeling tired or short of breath, cough which will not go away

·            warm, red and painful skin, or a painful skin rash with blisters

 

Your doctor will decide if you can keep using Bimzelx.

 

Other side effects

Tell your doctor, pharmacist or nurse if you get any of the following side effects:

 

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

·            upper respiratory infections with symptoms such as sore throat and stuffy nose

 

 

Common (may affect up to 1 in 10 people)

·            thrush in the mouth or throat with symptoms such as white or yellow patches; red or sore mouth and pain with swallowing

·            fungal infection of the skin, such as athlete’s foot between the toes

·            ear infections

·            cold sores (herpes simplex infections)

·            stomach flu (gastroenteritis)

·            inflamed hair follicles which may look like pimples

·            headache

·            itchy, dry skin or an eczema-like rash sometimes with swollen and reddened skin (dermatitis)

·            acne

·            redness, pain or swelling at the site of injection

·            feeling tired

 

Uncommon (may affect up to 1 in 100 people)

·            lowered levels of white blood cells (neutropenia)

·            fungal infections of the skin and mucous membranes (including oesophageal candidiasis)

·            discharge from the eye with itching, redness and swelling (conjunctivitis)

·            blood in the stool, abdominal cramps and pain, diarrhoea or weight loss (signs of bowel problems)

 

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 label and carton.

Store in a refrigerator between 2°C and 8°C. Do not freeze.

Keep the pre-filled pens in the original carton in order to protect from light.

Bimzelx can be kept out of the refrigerator for up to 25 days. This must be in the outer carton, not above 25°C and away from direct light. Do not use the pre-filled pens after this time period. There is a space on the box so you can write the date it was taken out of the refrigerator.

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 bimekizumab. Each pre-filled pen contains 160 mg of bimekizumab in the 1 mL solution.

·            The other ingredients are glycine, sodium acetate trihydrate, glacial acetic acid, polysorbate 80 and water for injections.


Bimzelx is a clear to slightly opalescent liquid. Its colour may vary from colourless to pale brownish-yellow . It comes in a single use disposable pre-filled pen. Bimzelx is available in unit packs containing 2 pre-filled pen(s).

Marketing Authorisation Holder

UCB Pharma S.A.

Allée de la Recherche 60

B-1070 Bruxelles, Belgium

 

Manufactured by:

Vetter Pharma-Fertigung GmbH & Co. KG

SchutzenstraBe 87 and 99-101, 88212 Ravensburg, , Germany

 

Batch released by:

UCB Pharma S.A.

Chemin du Foriest B-1420 Braine l'Alleud,

Belgium

 


This leaflet was last revised in (06/2023).
  نشرة الدواء تحت مراجعة الهيئة العامة للغذاء والدواء (اقرأ هذه النشرة بعناية قبل البدء في استخدام هذا المنتج لأنه يحتوي على معلومات مهمة لك)

ما هو دَّواء بيمزلكس؟

يحتوي دَّواء بيمزلكس على المادة الفعَّالة بيميكيزوماب.

 

فيمَ يُستَخدَم دَّواء بيمزلكس؟

يُستخدم بيمزلكس لعلاج الأمراض الالتهابية التالية:

·                الصدفية اللويحية

·                التهاب المفاصل الصدفي

·                التهاب المفاصل الفقرية المحورية، بما في ذلك التهاب المفاصل الفقرية المحورية الذي لا يظهر في صور الأشعة، والتهاب الفقار المقسط (التهاب المفاصل الفقرية المحورية الذي يظهر في صور الأشعة)

الصدفية اللويحية

يُستَخدَم دَّواء بيمزلكس لعلاج البالغين من حالة جلدية تُدعى الصدفية اللويحية. يحد دَّواء بيمزلكس من الأعراض، بما في ذلك الألم والحكة وتقشُّر الجلد.

 

التهاب المفاصل الصدفي

يُستخدم بيمزلكس لعلاج البالغين المصابين بالتهاب المفاصل الصدفي. التهاب المفاصل الصدفي هو مرض يُسبب التهاب المفاصل، وكثيرًا ما يصاحب الصدفية اللويحية. إذا كنت مصابًا بالتهاب المفاصل الصدفي النشط، فقد يكون عليك أولًا تلقي أدوية أخرى. وإذا لم تُفلح تلك الأدوية بالقدر الكافي أو في حالة عدم تحملها، فستتلقى بيمزلكس، إما وحده أو مع دواء آخر يُسمى ميثوتريكسات.

 

يقلل بيمزلكس من الالتهاب، وبذلك يمكن أن يساعد في الحد من الألم والتيبس والتورم في مفاصلك وحولها، والطفح الجلدي الصدفي، وتلف الأظافر الصدفي، ويمكن أن يبطئ تلف الغضاريف والعظام بالمفاصل المصابة بالمرض. ويمكن أن تساعدك تلك التأثيرات على السيطرة على علامات المرض وأعراضه، وتسهيل أنشطتك اليومية الطبيعية، والحد من التعب، وتحسين جودة حياتك.

 

 

التهاب المفاصل الفقرية المحورية، بما في ذلك التهاب المفاصل الفقرية المحورية الذي لا يظهر في صور الأشعة، والتهاب الفقار المقسط (التهاب المفاصل الفقرية المحورية الذي يظهر في صور الأشعة)

يُستخدم بيمزلكس لعلاج البالغين المصابين بمرض التهابي يؤثر في المقام الأول على العمود الفقري، ويسبب التهاب المفاصل الفقرية، ويُسمى التهاب المفاصل الفقرية المحورية. إذا لم تكن الحالة ظاهرة باستخدام الأشعة السينية، يُسمى ذلك "التهاب المفاصل الفقرية المحورية الذي لا يظهر في صور الأشعة"، وإذا حدث في المرضى مع علامات ظاهرة في صور الأشعة السينية، يُسمى "التهاب الفقار المُقسط" أو "التهاب المفاصل الفقرية المحوري الذي يظهر في صور الأشعة".

إذا كنت مصابًا بالتهاب المفاصل الفقرية المحورية، فستتلقى أولًا أدوية أخرى. وإذا لم تستجب بالقدر الكافي لتلك الأدوية، فستتلقى بيمزلكس للحد من علامات المرض وأعراضه، والحد من الالتهاب،وتحسين أدائك البدني. ويمكن أن يساعد بيمزلكس على الحد من ألم الظهر والتيبس والتعب، مما يمكن أن يسهل أنشطتك اليومية الطبيعية ويحسن جودة حياتك.

 

كيف يعمل دَّواء بيمزلكس؟

·                ينتمي بيميكيزوماب، وهو المادة الفعَّالة في دَّواء بيمزلكس، إلى مجموعة من الأدوية تُسمى مثبطات الإنترلوكين. يعمل بيميكيزوماب من خلال الحد من نشاط بروتينين يُدعيان إنترلوكين-17أ وإنترلوكين-17و، اللذين لهما دور في التسبب في حدوث الالتهاب. ترتفع مستويات هذين البروتينين في حالة الإصابة بالأمراض الالتهابية مثل: الصدفية ، التهاب المفاصل الصدفي والتهاب المفاصل الفقرية المحورية

لا تستخدم دَّواء بيمزلكس في الحالتين الآتيتين:

·            إذا كنت تعاني من حساسية تجاه بيميكيزوماب أو تجاه أي مكون من المكونات الأخرى الموجودة بهذا الدَّواء (المدرجة في قسم: 6).

·            إذا كنت مُصابًا بعدوى، بما في ذلك مرض السُّل، يرى طبيبك أنه من المهم أخذها بعين الاعتبار.

 

تحذيرات واحتياطات

تحدَّث إلى طبيبك أو الصيدلي أو الممرض(ة) الخاص(ة) بك قبل استخدام دَّواء بيمزلكس في الحالات الآتية:

·            إذا كنت مُصابًا بعدوى أو كنت تُعاني من عدوى يتكرر حدوثها.

·            إذا تلقيت مؤخرًا لقاحًا أو كنت تخطط لتلقيه. ينبغي ألا يتم إعطاؤك أنواع معينة من اللقاحات (اللقاحات الحية) أثناء استخدامك دَّواء بيمزلكس.

·            إذا كنت قد أُصبت من قبل بمرض السُّل.

·            إذا كنت قد أصبت من قبل بمرض الأمعاء الالتهابي (مرض كرون أو التهاب القولون التقرُّحي).

 

مرض الأمعاء الالتهابي (مرض كرون أو التهاب القولون التقرُّحي)

توقف عن استخدام دَّواء بيمزلكس وأخبر طبيبك أو اطلب المساعدة الطبية فورًا إذا لاحظت وجود دم في البراز أو تقلصات في البطن أو ألمًا أو إسهالًا أو فقدانًا في الوزن. قد تكون تلك الأعراض علامات تشير إلى الإصابة بمرض التهابي جديد في الأمعاء أو تفاقم مرض الأمعاء الالتهابي (مرض كرون أو التهاب القولون التقرُّحي).

 

انتبه للعدوى وتفاعلات الحساسية

نادرًا ما قد يسبب دَّواء بيمزلكس عدوى خطيرة. تحدَّث إلى طبيبك أو اطلب المساعدة الطبية فورًا إذا لاحظت أيًّا من علامات الإصابة بعدوى خطيرة. تُدْرَج هذه العلامات تحت "الآثار الجانبية الخطيرة" في قسم: 4.

 

من الممكن أن يسبب دَّواء بيمزلكس تفاعلات حساسية خطيرة. تحدث إلى طبيبك أو اطلب المساعدة الطبية فورًا إذا لاحظت أيًّا من علامات الإصابة بإحدى تفاعلات الحساسية الخطيرة. قد تشمل هذه العلامات الآتي:

·            صعوبة في التَّنفس أو البلع.

·            انخفاض ضغط الدَّم؛ مما قد يتسبب في شعورك بالدوخة أو دوار الرأس.

·            تورُّم الوجه، أو الشفتين، أو اللسان، أو الحَلْق.

·            حكَّة شديدة بالجلد مصحوبة بطفح جلدي أحمر اللون أو نتوءات بارزة.

 

الأطفال والمراهقون

لا تُعْطِ هذا الدَّواء للأطفال والشباب الأقل من 18 عامًا. لأنه لم يتم دراسة استخدامه في هذه الفئة العمرية.

 

تناوُل أدوية أخرى مع دَّواء بيمزلكس

أخبر طبيبك أو الصيدلي الخاص بك إذا كنت تستخدم أو استخدمت مؤخرًا أو قد تستخدم أيَّة أدوية أخرى.

 

الحمل والرَّضاعة الطبيعية والخصوبة

إذا كنتِ حاملًا، أو تعتقدين أنكِ قد تكونين حاملًا أو تخططين للحمل، فاستشيري طبيبكِ قبل استخدام هذا الدَّواء. يُفضَّل تجنُّب استخدام دَّواء بيمزلكس أثناء الحمل. فمن غير المعروف كيف سيؤثر هذا الدَّواء على الطفل.

 

إذا كنتِ سيدة بإمكانها الحمل، ينبغي عليكِ استخدام وسيلة لمنع الحمل أثناء استخدام هذا الدَّواء وبعد تلقي آخر جرعة من دَّواء بيمزلكس لمدة 17 أسبوعًا على الأقل.

 

تحدَّثي إلى طبيبكِ قبل استخدام هذا الدَّواء إذا كنتِ تُرضعين طبيعيًّا أو تخططين للإرضاع طبيعيًّا. ينبغي أن تتخذي أنتِ وطبيبكِ قرارًا بما إذا كان بإمكانكِ الإرضاع طبيعيًّا أم استخدام دَّواء بيمزلكس.

 

القيادة واستخدام الآلات

من غير المرجح أن يُؤثر دَّواء بيمزلكس على قدرتك على القيادة واستخدام الآلات.

 

يحتوي دَّواء بيمزلكس على الصوديوم

يحتوي هذا الدَّواء على أقل من 1 مللي مول (23 مجم) من الصوديوم لكل جرعة؛ مما يعني أنه "خالٍ من الصوديوم" بشكل أساسي.

https://localhost:44358/Dashboard

استخدم هذا الدَّواء بالضبط كما أخبرك طبيبك أو الصيدلي الخاص بك. راجع طبيبك أو الصيدلي الخاص بك إذا لم تكن متأكدًا من كيفية الاستخدام.

 

ما الكمية التي ينبغي إعطاؤها من دَّواء بيمزلكس؟ وكم تبلغ المدة التي ينبغي إعطاؤه خلالها؟

 

الصدفية اللويحية

الجرعة المُوصى بها التي تُعْطَى على هيئة حُقَن تحت الجلد هي كالآتي:

·            320 مجم (تُعْطَى على هيئة قلمين مُعبأين مُسبقًا، يحتوي كل واحد منهما على 160 مجم) في الأسبوع 0، 4، 8، 12، 16.

·            بدءًا من الأسبوع 16، ستستخدم 320 مجم (قلمين مُعبأين مُسبقًا، يحتوي كل منهما على 160 مجم) كل 8 أسابيع. إذا كنت تزن أكثر من 120 كجم، فقد يقرر طبيبك مواصلة إعطائك الحُقَن كل 4 أسابيع بدءًا من الأسبوع 16.

 

 

التهاب المفاصل الصدفي

تبلغ الجرعة الموصى بها، والتي تُعطى بالحقن تحت الجلد ما يلي:

·       160 مجم (تُعطى في شكل قلم واحد مُعبأ مُسبقًا) كل 4 أسابيع.

·       إذا كنت مصابًا بالتهاب المفاصل الصدفي مع وجود الصدفية اللويحية المتوسطة إلى الشديدة بالتزامن مع ذلك، فسيكون نظام الجرعات الموصى به هو نفسه في حالة الصدفية اللويحية. وبعد الأسبوع 16، قد يعدل الطبيب جرعتك إلى 160 مجم كل 4 أسابيع، حسب أعراض المفاصل لديك.

 

التهاب المفاصل الفقرية المحورية، بما في ذلك التهاب المفاصل الفقرية المحورية الذي لا يظهر في صور الأشعة، والتهاب الفقار المقسط (التهاب المفاصل الفقرية المحورية الذي يظهر في صور الأشعة)

تبلغ الجرعة الموصى بها، والتي تُعطى بالحقن تحت الجلد 160 مجم (تُعطى في شكل قلم واحد مُعبأ مُسبقًا) كل 4 أسابيع.

 

ستقرر أنت وطبيبك أو الممرض(ة) الخاص(ة) بك ما إذا كان عليك حقن هذا الدَّواء بنفسك أم لا. لا تحقن هذا الدَّواء ما لم يدربك أحد أخصائيي الرعاية الصحية. قد يُعطيك أحد مقدمي الرعاية أيضًا الحُقَن بعد تلقيه التدريب.

 

اقرأ "تعليمات الاستخدام" الواردة في آخر هذه النَّشرة قبل أن تحقن نفسك بقلم دَّواء بيمزلكس المُعبأ مُسبقًا.

 

إذا استخدمت كمية أكثر مما يجب من دَّواء بيمزلكس

أخبر طبيبك إذا استخدمت كمية أكثر مما يجب من دَّواء بيمزلكس أو إذا حقنت جرعتك في وقت أبكر مما ينبغي.

 

إذا أغفلت استخدام دَّواء بيمزلكس

تحدَّث إلى طبيبك إذا أغفلت حَقْن جرعة من جرعات دَّواء بيمزلكس.

 

إذا توقفت عن استخدام دَّواء بيمزلكس

تحدَّث إلى طبيبك قبل التوقف عن استخدام دَّواء بيمزلكس. قد تعاود الأعراض ظهورها إذا أوقفت العلاج.

 

إذا كانت لديك أية أسئلة إضافية حول استخدام هذا الدَّواء، فاستشر طبيبك أو الصيدلي أو الممرض(ة) الخاص(ة) بك.

مثله مثل كافة الأدوية، قد يُسبب هذا الدَّواء آثارًا جانبية، على الرَّغم من عدم حدوثها لدى الجميع.

 

الآثار الجانبية الخطيرة

أخبر طبيبك أو اطلب المساعدة الطبية فورًا إذا تعرضت لأيٍّ من الآثار الجانبية التالية:

 

الإصابة بعدوى خطيرة مُحْتَمَلة - قد تشمل العلامات ما يلي:

·            حُمى، أعراضًا شبيهة بأعراض الإنفلونزا، تعرُّقًا ليليًّا.

·            شعورًا بالتَّعب أو ضيقًا في التَّنفس، سُعالًا لا يزول.

·            جلدًا دافئًا به احمرار وألم، أو طفحًا جلديًّا مؤلمًا مصحوبًا ببثور.

 

سيقرر طبيبك ما إذا كان بإمكانك الاستمرار في استخدام دَّواء بيمزلكس أم لا.

 

الآثار الجانبية الأخرى

أخبر طبيبك أو الصيدلي أو الممرض(ة) الخاص(ة) بك إذا أُصبت بأيٍّ من الآثار الجانبية التالية:

 

شائعة جدًّا (قد تُؤثر على أكثر من شخص واحد من بين كل 10 أشخاص)

·            عدوى بالجهاز التَّنفسي العلوي مصحوبة بأعراض؛ مثل: التهاب الحَلْق وانسداد الأنف.

 

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

·            سُلاق في الفم أو الحَلْق مصحوب بأعراض؛ مثل: ظهور بقع بيضاء أو صفراء، احمرار الفم أو التهابه وألم مع البلع.

·            عدوى فطرية تصيب الجلد، مثل: القدم الرياضي بين أصابع القدم.

·            عدوى بالأذن.

·            قُرَح باردة (عدوى الهربس البسيط).

·            إنفلونزا المعدة (التهاب المعدة والأمعاء).

·            التهاب جريبات الشعر التي قد تبدو كالبثور.

·            صداع.

·            حكة وجفاف بالجلد أو طفح جلدي شبيه بالأكزيما يكون مصحوبًا أحيانًا بتورُّم الجلد واحمراره (التهاب جلدي).

·            حب الشباب.

·            احمرار أو ألم أو تورُّم في موضع الحَقْن.

·            شعور بالتعب.

 

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

·            انخفاض مستويات خلايا الدَّم البيضاء (قلة خلايا العَدِلات).

·            عدوى فطرية تصيب الجلد والأغشية المخاطية (تشمل مرض المبيضات الذي يصيب المريء).

·            إفرازات من العين مصحوبة بحكة، واحمرار، وتورُّم (التهاب الملتحمة).

·            وجود دم في البراز أو تقلصات وألم في البطن أو إِسْهال أو فقدان الوزن (علامات تشير إلى وجود مشاكل في الأمعاء).

 

الإبلاغ عن الآثار الجانبية

إذا أُصبت بأية آثار جانبية، فتحدَّث إلى طبيبك أو الصيدلي أو الممرض(ة) الخاص(ة) بك. يشمل ذلك أية آثار جانبية مُحتمَلة، غير المُدرجة في هذه النَّشرة. بإبلاغك عن الآثار الجانبية، يمكنك المساعدة في توفير المزيد من المعلومات حول أمان استخدام هذا الدَّواء

يُحفظ هذا الدَّواء بعيدًا عن رؤية ومُتناوَل الأطفال.

 

لا تستخدم هذا الدَّواء بعد تاريخ انتهاء الصلاحية المدون على الملصق والعبوة الكرتونية.

 

يُحفظ في الثلاجة بين 2 و8 درجات مئوية. لا تعرضه للتجميد.

 

احتفظ بالأقلام المُعبأة مُسبقًا داخل العبوة الكرتونية الأصلية لحمايتها من الضَّوء.

 

يمكن أن يُحْفَظ دَّواء بيمزلكس خارج الثلاجة لمدة تصل إلى25  يومًا. يجب أن يتم ذلك داخل العبوة الكرتونية الخارجية، في درجة حرارة لا تتجاوز 25 درجة مئوية وبعيدًا عن الضوء المباشر. لا تستخدم الأقلام المُعبأة مُسبقًا بعد هذه الفترة الزمنية. تُوجد خانة على العبوة؛ كي تتمكن من كتابة التاريخ الذي أُخرجت فيه من الثلاجة.

 

لا تتخلص من أي أدوية عن طريق إلقائها في مياه الصَّرف أو مع المخلفات المنزلية. استشر الصيدلي الخاص بك عن كيفية التَّخلص من الأدوية التي لم تعد تستخدمها. ستساعد هذه الإجراءات في الحفاظ على البيئة.

·            المادة الفعَّالة هي بيميكيزوماب. يحتوي كل قلم مُعبأ مُسبقًا على 160 مجم من بيميكيزوماب في محلول بحجم مللي لتر واحد.

·            المكونات الأخرى هي جلايسين وأسيتات الصوديوم ثلاثي الهيدرات وحَمْض الخليك الثلجي وبوليسوربات 80 وماء للحقن.

ما هو شكل دَّواء بيمزلكس؟ وما هي محتويات العبوة؟

دَّواء بيمزلكس عبارة عن سائل صافٍ مائل للضبابي بعض الشيء. وقد يختلف لونه من عديم اللون إلى أصفر شاحب يميل إلى البني.  يتوافر في قلم مُعبأ مُسبقًا مُعَد للاستخدام مرة واحدة.

 

يتوافر دَّواء بيمزلكس في عبوات للجرعات المفردة تحتوي على قلمين مُعبأين مُسبقًا

حامل رخصة التسويق:

                                                           

UCB Pharma SA                                                                                

Allée de la Recherche 60                                                                   

B-1070 Bruxelles                                                                               

Belgium (بلجيكا)                                                                                              

 

الشركة المصنعة

Vetter Pharma-Fertigung GmbH & Co. KG

SchutzenstraBe 87 and 99-101, 88212 Ravensburg, Germany

 

Batch released by:

UCB Pharma S.A.

Chemin du Foriest B-1420 Braine l'Alleud,

Belgium

تمت آخر مراجعة لهذه النَّشرة في: {2023/06}
 Read this leaflet carefully before you start using this product as it contains important information for you

Bimzelx 160 mg solution for injection in pre-filled syringe Bimzelx 160 mg solution for injection in pre-filled pen

Bimzelx 160 mg solution for injection in pre-filled syringe Each pre-filled syringe contains 160 mg of bimekizumab in 1 mL. Bimzelx 160 mg solution for injection in pre-filled pen Each pre-filled pen contains 160 mg of bimekizumab in 1 mL. Bimekizumab is a humanised IgG1monoclonal antibody produced in a genetically engineered Chinese hamster ovary (CHO) cell line by recombinant DNA technology. For the full list of excipients, see section 6.1.

Solution for injection (injection) The solution is clear to slightly opalescent and, colourless to pale brownish-yellow

Plaque psoriasis

Bimzelx is indicated for the treatment of moderate to severe plaque psoriasis in adults who are candidates for systemic therapy.

Psoriatic arthritis

Bimzelx, alone or in combination with methotrexate, is indicated for the treatment of active psoriatic arthritis in adults who have had an inadequate response or who have been intolerant to one or more disease-modifying antirheumatic drugs (DMARDs).

Axial spondyloarthritis

Non-radiographic axial spondyloarthritis (nr-axSpA)

Bimzelx is indicated for the treatment of adults with active non-radiographic axial spondyloarthritis with objective signs of inflammation as indicated by elevated C-reactive protein (CRP) and/or magnetic resonance imaging (MRI) who have responded inadequately or are intolerant to non-steroidal anti-inflammatory drugs (NSAIDs).

Ankylosing spondylitis (AS, radiographic axial spondyloarthritis)

Bimzelx is indicated for the treatment of adults with active ankylosing spondylitis who have responded inadequately or are intolerant to conventional therapy.


Bimzelx is intended for use under the guidance and supervision of a physician experienced in the diagnosis and treatment of conditions for which Bimzelx is indicated.

 

 

Posology

 

Plaque psoriasis

The recommended dose for adult patients with plaque psoriasis is 320 mg (given as 2 subcutaneous injections of 160 mg each) at week 0, 4, 8, 12, 16 and every 8 weeks thereafter.

 

Psoriatic arthritis

 

The recommended dose for adult patients with active psoriatic arthritis is 160 mg (given as 1 subcutaneous injection of 160 mg) every 4 weeks.

For psoriatic arthritis patients with coexistent moderate to severe plaque psoriasis, the recommended dose is the same as for plaque psoriasis [320 mg (given as 2 subcutaneous injections of 160 mg each) at Week 0, 4, 8, 12, 16 and every 8 weeks thereafter]. After 16 weeks, regular assessment of efficacy is recommended and if a sufficient clinical response in joints cannot be maintained, a switch to 160 mg every 4 weeks can be considered.

 

Axial spondyloarthritis (nr-axSpA and AS)

 

The recommended dose for adult patients with axial spondyloarthritis is 160 mg (given as 1 subcutaneous injection) every 4 weeks.

 

 

For above indications, consideration should be given to discontinuing treatment in patients who have shown no improvement by 16 weeks of treatment.

 

 

Special populations

 

Overweight patients with plaque psoriasis

 

For some patients with plaque psoriasis (including psoriatic arthritis with coexistent moderate to severe psoriasis) and a body weight ≥ 120 kg who did not achieve complete skin clearance at week 16, 320 mg every 4 weeks after week 16 may further improve treatment response (see section 5.1).

 

Elderly ( ≥65 years)

 

No dose adjustment is required (see section 5.2).

 

Renal or hepatic impairment

 

Bimekizumab has not been studied in these patient populations. Dose adjustments are not considered necessary based on pharmacokinetics (see section 5.2).

 

Paediatric population

 

The safety and efficacy of bimekizumab in children and adolescents below the age of 18 years have not been established. No data are available.

 

Method of administration

 

This medicinal product is administered by subcutaneous injection.

 

Suitable areas for injection include thigh, abdomen and upper arm. Injection sites should be rotated and injections should not be given into psoriasis plaques or areas where the skin is tender, bruised, erythematous, or indurated.

The pre-filled syringe or pre-filled pen must not be shaken.

After proper training in subcutaneous injection technique, patients may self-inject Bimzelx with the pre-filled syringe or pre-filled pen if their physician determines that it is appropriate and with medical follow-up as necessary. Patients should be instructed to inject the full amount of Bimzelx according to the instructions for use provided in the package leaflet.


Hypersensitivity to the active substance or to any of the excipients listed in section 6.1. Clinically important active infections (e.g. active tuberculosis, see section 4.4).

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.

 

Infections

 

Bimekizumab may increase the risk of infections such as upper respiratory tract infections and oral candidiasis (see section 4.8).

 

Caution should be exercised when considering the use of bimekizumab in patients with a chronic infection or a history of recurrent infection. Treatment with bimekizumab must not be initiated in patients with any clinically important active infection until the infection resolves or is adequately treated (see section 4.3).

 

Patients treated with bimekizumab should be instructed to seek medical advice if signs or symptoms suggestive of an infection occur. If a patient develops an infection, the patient should becarefully monitored. If the infection becomes serious or is not responding to standard therapy, treatment should be discontinued until the infection resolves.

 

Pre-treatment evaluation for tuberculosis (TB)

 

Prior to initiating treatment with bimekizumab, patients should be evaluated for TB infection. Bimekizumab should not be given in patients with active TB (see section 4.3). Patients receiving bimekizumab should be monitored for signs and symptoms of active TB. Anti-TB therapy should be considered prior to initiating bimekizumab in patients with a past history of latent or active TB in whom an adequate course of treatment cannot be confirmed.

 

Inflammatory bowel disease

 

Cases of new or exacerbations of inflammatory bowel disease have been reported with bimekizumab (see section 4.8). Bimekizumab is not recommended in patients with inflammatory bowel disease. If a patient develops signs and symptoms of inflammatory bowel disease or experiences an exacerbation of pre-existing inflammatory bowel disease, bimekizumab should be discontinued and appropriate medical management should be initiated.

 

Hypersensitivity

 

Serious hypersensitivity reactions including anaphylactic reactions have been observed with IL-17 inhibitors. If a serious hypersensitivity reaction occurs, administration of bimekizumab should be discontinued immediately and appropriate therapy initiated.

 

Vaccinations

 

Prior to initiating therapy with bimekizumab, completion of all age appropriate immunizations according to current immunization guidelines should be considered.

 

Live vaccines should not be given in patients treated with bimekizumab.

 

Patients treated with bimekizumab may receive inactivated or non-live vaccinations. Healthy individuals who received a single 320 mg dose of bimekizumab two weeks prior to vaccination with an inactivated seasonal influenza vaccine had similar antibody responses compared to individuals who did not receive bimekizumab prior to vaccination.

 

Excipients

This medicinal product contains less than 1 mmol (23 mg) sodium per dose, that is to say essentially “sodium free”.


No interaction studies have been performed.

There is no direct evidence for the role of IL-17A or IL-17F in the expression of CYP450 enzymes. The formation of some CYP450 enzymes is suppressed by increased levels of cytokines during chronic inflammation. Thus, anti-inflammatory treatments, such as with the IL-17A and IL-17F inhibitor bimekizumab, may result in normalisation of CYP450 levels with accompanying lower exposure of CYP450-metabolised medicinal products. Therefore, a clinically relevant effect on CYP450 substrates with a narrow therapeutic index, in which the dose is individually adjusted (e.g. warfarin) cannot be excluded. On initiation of bimekizumab therapy in patients being treated with these types of medicinal products, therapeutic monitoring should be considered.

 

Population pharmacokinetic (PK) data analyses indicated that the clearance of bimekizumab was not impacted by concomitant administration of conventional disease modifying antirheumatic drugs (cDMARDs) including methotrexate, or by prior exposure to biologics.

 

Live vaccines should not be given concurrently with bimekizumab (see section 4.4).


Women of childbearing potential

 

Women of childbearing potential should use an effective method of contraception during treatment and for at least 17 weeks after treatment.

 

Pregnancy

 

There is a limited amount of data on the use of bimekizumab in pregnant women. Animal studies do not indicate direct or indirect harmful effects with respect to pregnancy, embryonic/foetal development, parturition or postnatal development (see section 5.3). As a precautionary measure, it is preferable to avoid the use of Bimzelx during pregnancy.

 

Breast-feeding

 

It is unknown whether bimekizumab is excreted in human milk. A risk to the newborn/infant cannot be excluded. A decision must be made whether to discontinue breast-feeding or to discontinue/abstain from Bimzelx therapy taking into account the benefit of breast-feeding for the child and the benefit of therapy for the woman.

 

Fertility

 

The effect of bimekizumab on human fertility has not been evaluated. Animal studies do not indicate direct or indirect harmful effects with respect to fertility (see section 5.3).


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


System Organ Class

Frequency

Adverse reaction

 

Infections and infestations

Very common

Upper respiratory tract infections

Common

Oral candidiasis,

Tinea infections,

Ear infections,

Herpes simplex infections,

Oropharyngeal candidiasis,

Gastroenteritis,

Folliculitis

Uncommon

Mucosal and cutaneous candidiasis (including oesophageal candidiasis),

Conjunctivitis

Blood and lymphatic system disorders

Uncommon

Neutropenia

Nervous System disorders

Common

Headache

Gastrointestinal disorders

Uncommon

Inflammatory bowel disease

Skin and subcutaneous tissue disorders

Common

Rash, dermatitis and eczema,

Acne

General disorders and administration site conditions 

Common

Injection site reactionsa,

Fatigue

a) Includes: injection site erythema, reaction, oedema, pain, swelling.

 

Description of selected adverse reactions

 

Infections

 

In the placebo-controlled period of Phase III clinical studies in plaque psoriasis, infections were reported in 36.0% of patients treated with bimekizumab for up to 16 weeks compared with 22.5% of patients treated with placebo. Serious infections occurred in 0.3% of patients treated with bimekizumab and 0% treated with placebo.

 

The majority of infections consisted of non-serious mild to moderate upper respiratory tract infections such as nasopharyngitis. There were higher rates of oral and oropharyngeal candidiasis in patients treated with bimekizumab consistent with the mechanism of action (7.3% and 1.2% respectively compared to 0% for placebo-treated patients). More than 98% of cases were non-serious, mild or moderate in severity, and did not require treatment discontinuation. A slightly higher incidence of oral candidiasis was reported in patients <70 kg (8.5% versus 7.0% in patients ≥70 kg).

 

Over the entire treatment period of Phase III studies in plaque psoriasis, infections were reported in 63.2% of patients treated with bimekizumab (120.4 per 100 patient-years). Serious infections were reported in 1.5% of patients treated with bimekizumab (1.6 per 100 patient-years) (see section 4.4).

 

Infection rates observed in PsA and axSpA (nr-axSpA and AS) Phase III clinical studies were similar to those observed in plaque psoriasis apart from oral and oropharyngeal candidiasis rates in patients treated with bimekizumab, which were lower at 2.3% and 0% respectively in PsA and 3.7% and 0.3% respectively in axSpA compared to 0% with placebo.

 

Neutropenia

 

Neutropenia was observed with bimekizumab in phase III clinical studies in plaque psoriasis. Over the entire treatment period of Phase III studies, neutropenia grade 3/4 were observed in 1% of patients treated with bimekizumab.

 

The frequency of neutropenia in PsA and axSpA (nr-axSpA and AS) clinical studies was similar to that observed in plaque psoriasis studies.

 

Most cases were transient and did not require treatment discontinuation. No serious infections were associated with neutropenia.

 

Hypersensitivity

 

Serious hypersensitivity reactions including anaphylactic reactions have been observed with IL-17 inhibitors.

 

Immunogenicity

 

Plaque psoriasis

 

Approximately 45% of plaque psoriasis patients treated with bimekizumab up to 56 weeks at the recommended dosing regimen (320 mg every 4 weeks up to week 16 and 320 mg every 8 weeks thereafter) developed anti-drug antibodies. Of the patients who developed anti-drug antibodies, approximately 34% (16% of all patients treated with bimekizumab) had antibodies that were classified as neutralising.

 

Psoriatic arthritis

 

Approximately 31% of patients with psoriatic arthritis treated with bimekizumab at the recommended dosing regimen (160 mg every 4 weeks) up to 16 weeks had anti-drug antibodies. Of the patients with anti-drug antibodies, about 33% (10% of all patients treated with bimekizumab) had antibodies that were classified as neutralizing. By week 52, approximately 47% of biologic disease-modifying anti-rheumatic drug (bDMARD) treatment naïve patients with psoriatic arthritis in the BE OPTIMAL study treated with bimekizumab at the recommended dosing regimen (160 mg every 4 weeks) had anti-drug antibodies. Of the patients with anti-drug antibodies, about 38% (18% of all patients in the BE OPTIMAL study treated with bimekizumab) had antibodies that were classified as neutralizing.

 

Axial spondyloarthritis (nr-axSpA and AS)

 

Approximately 57% of patients with nr-axSpA treated with bimekizumab up to 52 weeks at the recommended dosing regimen (160 mg every 4 weeks) had anti-drug antibodies. Of the patients with anti-drug antibodies, approximately 44% (25% of all patients treated with bimekizumab) had antibodies that were classified as neutralizing.

 

Approximately 44% of patients with AS treated with bimekizumab up to 52 weeks at the recommended dosing regimen (160 mg every 4 weeks) had anti-drug antibodies. Of the patients with anti-drug antibodies, approximately 44% (20% of all patients treated with bimekizumab) had antibodies that were classified as neutralizing.

 

 

Across indications, no clinically meaningful impact on clinical response was associated with anti-bimekizumab antibodies development and an association between immunogenicity and treatment emergent adverse events has not been clearly established.

 

Elderly patients (≥65 years)

Exposure is limited in elderly subjects.

 

Elderly patients may be more likely to experience certain adverse reactions such as oral candidiasis, dermatitis and eczema when using bimekizumab.

 

In the placebo-controlled period of Phase III clinical studies in plaque psoriasis, oral candidiasis was observed in 18.2% of patients ≥65 years versus 6.3 % in <65 years, dermatitis and eczema in 7.3% of patients ≥65 years versus 2.8% in <65 years.

 

In the placebo-controlled period of Phase III clinical studies in psoriatic arthritis, oral candidiasis was observed in 8.1% of patients ≥65 years versus 2.3% in <65 years, dermatitis and eczema in 4.2% of patients ≥65 years versus 0.4% in <65 years.

 

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 reporting system. Listed below.

 

Please report any side effect(s) to:

·    Saudi Arabia:

 

 

·       The National Pharmacovigilance Center (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.

 


Single doses of 640 mg intravenously or 640 mg subcutaneously, followed by 320 mg subcutaneously every two weeks for five doses have been administered in clinical studies without dose-limiting toxicity. In the event of overdose, it is recommended that the patient be monitored for any signs and symptoms of adverse reactions and appropriate symptomatic treatment be instituted immediately.


Pharmacotherapeutic group: Immunosuppressants, interleukin inhibitors, ATC code: L04AC21

 

Mechanism of action

 

Bimekizumab is a humanised IgG1/κ monoclonal antibody that selectively binds with high affinity to IL-17A, IL-17F and IL-17AF cytokines, blocking their interaction with the IL-17RA/IL-17RC receptor complex. Elevated concentrations of IL-17A and IL-17F have been implicated in the pathogenesis of several immune-mediated inflammatory diseases including plaque psoriasis, psoriatic arthritis and axial spondyloarthritis. IL-17A and IL-17F cooperate and/or synergize with other inflammatory cytokines to induce inflammation. IL17-F is produced in significant amount by innate immune cells. This production can be independent of IL-23. Bimekizumab inhibits the proinflammatory cytokines, resulting in the normalization of skin inflammation and substantial decrease of local and systemic inflammation, and as a consequence improvement in clinical signs and symptoms associated with psoriasis, psoriatic arthritis and axial spondyloarthritis.  From in vitro models, bimekizumab was shown to inhibit psoriasis-related gene expression and cytokine production, the migration of inflammatory cells and pathological osteogenesis to a greater extent than inhibition of IL-17A alone.

 

Clinical efficacy and safety

 

Plaque psoriasis

 

The safety and efficacy of bimekizumab was evaluated in 1,480 patients with moderate to severe plaque psoriasis in three Phase 3 multicenter, randomised, placebo and/or active comparator-controlled studies. Patients were at least 18 years of age, had a Psoriasis Area and Severity Index (PASI) score ≥12 and Body Surface Area (BSA) affected by psoriasis (PSO) ≥10%, an Investigators Global Assessment (IGA) score ≥3 on a 5-point scale and were candidates for systemic psoriasis therapy and/or phototherapy. The efficacy and safety of bimekizumab were evaluated versus placebo and ustekinumab (BE VIVID – PS0009), versus placebo (BE READY – PS0013) and versus adalimumab (BE SURE - PS0008).

 

The BE VIVID study evaluated 567 patients for 52 weeks where patients were randomised to receive either bimekizumab 320 mg every 4 weeks, ustekinumab (45 mg or 90 mg, depending on patient weight, at baseline and week 4 and then every 12 weeks), or placebo for an initial 16 weeks, followed by bimekizumab 320 mg every 4 weeks.

 

The BE READY study evaluated 435 patients for 56 weeks. Patients were randomised to receive bimekizumab 320 mg every 4 weeks or placebo. At week 16, patients who achieved a PASI 90 response entered the 40-week randomised withdrawal period. Patients initially randomised to bimekizumab 320 mg every 4 weeks were re-randomised to either bimekizumab 320 mg every 4 weeks or bimekizumab 320 mg every 8 weeks or placebo (i.e. withdrawal of bimekizumab). Patients initially randomised to placebo continued to receive placebo provided they were PASI 90 responders. Patients who did not achieve a PASI 90 response at week 16 entered an open-label escape arm and received bimekizumab 320 mg every 4 weeks for 12 weeks. Patients who relapsed (did not achieve PASI 75 response) during the randomised withdrawal period also entered the 12-week escape arm.

 

The BE SURE study evaluated 478 patients for 56 weeks. Patients were randomised to receive either bimekizumab 320 mg every 4 weeks through week 56, bimekizumab 320 mg every 4 weeks through week 16 followed by bimekizumab 320 mg every 8 weeks through week 56 or adalimumab as per labeling recommendation through Week 24 followed by bimekizumab 320 mg every 4 weeks through week 56.

 

Baseline characteristics were consistent across all 3 studies: patients were predominantly male (70.7%) and white (84.1%), with a mean age of 45.2 years (18 to 83 years), and 8.9% were ≥65 years of age. The median baseline BSA was 20%, the median baseline PASI score was 18 and the baseline IGA score was severe in 33% of patients. The median baseline scores for Patient Symptoms Diary (PSD) pain, itch and scaling items ranged between 6 and 7 on a 0-10 points scale and the median baseline Dermatology Life Quality Index (DLQI) total score was 9.

 

Across all 3 studies, 38% of patients had received a prior biologic therapy; 23% had received at least one anti-IL17 agent (primary anti-IL17 failures were excluded) and 13% had received at least one TNF-antagonist. Twenty-two percent were naïve to any systemic therapy (including non-biologic and biologic) and 39% of patients had received prior phototherapy or photochemotherapy.

 

The efficacy of bimekizumab was evaluated with respect to impact on skin disease overall, specific

body locations (scalp, nails, palms and soles), patient reported symptoms and impact on quality of life. The two co-primary endpoints in all 3 studies were the proportion of patients who achieved 1) a PASI 90 response and 2) an IGA “clear or almost clear” (IGA 0/1with at least two points improvement from baseline) response at week 16. PASI 100, IGA 0 response at week 16 and PASI 75 response at week 4 were secondary endpoints in all 3 studies.

Skin disease overall

 

Treatment with bimekizumab resulted in significant improvement across efficacy endpoints compared to placebo, ustekinumab or adalimumab at week 16. The main efficacy results are shown in Table 2.

 

Table 2: Summary of clinical responses in BE VIVID, BE READY and BE SURE

 

BE VIVID

BE READY

BE SURE

 

Placebo

 

(N= 83)

 

n (%)

Bimekizumab 320 mg Q4W

(N= 321)

 

n (%)

Ustekinumab

 

(N=163)

 

n (%)

Placebo

 

(N= 86)

 

n (%)

Bimekizumab 320 mg Q4W

(N= 349)

 

n (%)

Bimekizumab 320 mg Q4W

(N= 319)

 

n (%)

Adalimumab

 

(N= 159)

 

n (%)

PASI 100

Week 16

 

0 (0.0)

 

188 (58.6)a

 

34 (20.9)

 

1 (1.2)

 

238 (68.2)a

 

194 (60.8)a

 

38 (23.9)

PASI 90

Week 16

 

4 (4.8)

 

273 (85.0)a, b

 

81 (49.7)

 

1 (1.2)

 

317 (90.8)a

 

275 (86.2)a

 

75 (47.2)

PASI 75

Week 4

Week 16

 

2 (2.4)

6 (7.2)

 

247 (76.9)a, b

296 (92.2)

 

25 (15.3)

119 (73.0)

 

1 (1.2)

2 (2.3)

 

265 (75.9)a

333 (95.4)

 

244 (76.5)a

295 (92.5)

 

50 (31.4)

110 (69.2)

IGA 0

Week 16

 

0 (0.0)

 

188 (58.6)a

 

36 (22.1)

 

1 (1.2)

 

243 (69.6)a

 

197 (61.8)

 

39 (24.5)

IGA 0/1

Week 16

 

4 (4.8)

 

270 (84.1)a, b

 

87 (53.4)

 

1 (1.2)

 

323 (92.6)a

 

272 (85.3)a

 

91 (57.2)

Absolute PASI ≤ 2

Week 16

 

 

3 (3.6)

 

 

273 (85.0)

 

 

84 (51.5)

 

 

1 (1.2)

 

 

315 (90.3)

 

 

280 (87.8)

 

 

86 (54.1)

PSD Pain improvement ≥4  (N)

Week 16

(N=48)

 

 

5 (10.4)

(N=190)

 

 

140 (73.7)

(N=90)

 

 

54 (60.0)

(N=49)

 

 

0 (0.0)

(N=209)

 

 

148 (70.8)

(N=222)

 

 

143 (64.4)

(N=92)

 

 

43 (46.7)

PSD Itch improvement ≥4 (N)

Week 16

(N=53)

 

 

6 (11.3)

(N=222)

 

 

151 (68.0)

(N=104)

 

 

57 (54.8)

(N=60)

 

 

0 (0.0)

(N=244)

 

 

161 (66.0)

(N=248)

 

 

153 (61.7)

(N=107)

 

 

42 (39.3)

PSD Scaling improvement ≥4 (N)

Week 16

(N=56)

 

 

6 (10.7)

(N=225)

 

 

171 (76.0)

(N=104)

 

 

59 (56.7)

(N=65)

 

 

1 (1.5)

(N=262)

 

 

198 (75.6)

(N=251)

 

 

170 (67.7)

(N= 109)

 

 

42 (38.5)

Bimekizumab 320 mg Q4W= bimekizumab every 4 weeks. Non-Responder Imputation (NRI) is used.

IGA 0/1 response was defined as Clear (0) or Almost Clear (1) with at least a 2-category improvement from Baseline at week 16. IGA 0 response was defined as Clear (0) with at least a 2-category improvement from Baseline at week 16.

PSD is a Patient Symptoms Diary, also referred to as Psoriasis Symptoms and Impacts Measure (P-SIM), measuring psoriasis symptom severity on a scale from 0 (no symptoms) to 10 (very severe symptoms). Response is defined as a decrease ≥4 from baseline to week 16 for pain, itch and scaling on a scale from 0 to 10.

a) p<0.001 versus placebo (BE VIVID and BE READY), versus adalimumab (BE SURE), adjusted for multiplicity.

b) p<0.001 versus ustekinumab (BE VIVID), adjusted for multiplicity.

 

Bimekizumab was associated with a rapid onset of efficacy. In BE VIVID, at week 2 and week 4, PASI 90 response rates were significantly higher for bimekizumab-treated patients (12.1% and 43.6% respectively) compared to placebo (1.2% and 2.4% respectively) and ustekinumab (1.2% and 3.1% respectively).

 

In the BE VIVID study, at week 52, bimekizumab-treated patients (every 4 weeks) achieved significantly higher response rates than the ustekinumab-treated patients on the endpoints of PASI 90 (81.9% bimekizumab vs 55.8% ustekinumab, p<0.001), IGA 0/1 (78.2% bimekizumab vs 60.7% ustekinumab, p<0.001) and PASI 100 (64.5% bimekizumab vs 38.0% ustekinumab).

 

Figure 1: PASI 90 responder rates over time in BE VIVID

BKZ 320 mg Q4W=bimekizumab every 4 weeks; Uste=ustekinumab. NRI is used.

 

In the BE SURE study at week 24, a significantly higher percentage of patients treated with bimekizumab (Q4W/Q4W and Q4W/Q8W combined dosing arms) achieved PASI 90 and IGA 0/1 responses as compared with adalimumab (85.6% and 86.5% respectively vs 51.6% and 57.9% respectively, p<0.001). At week 56, 70.2% of patients treated with bimekizumab Q8W achieved a PASI 100 response. Among the 65 adalimumab non-responders at week 24 (< PASI 90), 78.5% achieved a PASI 90 response after 16 weeks of treatment with bimekizumab. The safety profile observed in patients who switched from adalimumab to bimekizumab without a wash-out period was similar to patients who initiated bimekizumab after wash out of prior systemic therapies.

 

Figure 2: PASI 90 responder rates over time in BE SURE

 

BKZ 320 mg Q4W = bimekizumab every 4 weeks; BKZ 320 mg Q8W = bimekizumab every 8 weeks; ADA= adalimumab.

Patients in the BKZ Q4W/Q8W group switched from Q4W to Q8W dosing at week 16. Patients in the ADA/BKZ 320 mg Q4W group switched from ADA to BKZ Q4W at week 24. NRI is used.

 

The efficacy of bimekizumab was demonstrated regardless of age, gender, race, disease duration, body weight, PASI baseline severity and previous treatment with a biologic. Bimekizumab was efficacious in prior biologic exposed patients, including anti-TNF / anti IL-17 and in systemic treatment-naïve patients. Efficacy in patients with primary failure to anti-IL17 has not been investigated.

 

Based on population PK/ PD analysis and supported by clinical data, patients with higher body weight (≥120 kg) who did not achieve complete skin clearance at week 16 benefited from continued bimekizumab 320 mg every four weeks (Q4W) after the initial 16 weeks of treatment. In the BE SURE study, patients received bimekizumab 320 mg Q4W through week 16, followed by either Q4W or every eight weeks (Q8W) dosing through week 56, regardless of responder status at week 16. Patients in the ≥120 kg group (N=37) on the Q4W maintenance regimen showed greater improvement in PASI100 between week 16 (23.5%) and week 56 (70.6%) compared to those on the Q8W maintenance regimen (week 16: 45.0% vs week 56: 60.0%).

 

Improvements were observed in psoriasis involving the scalp, nails, palms and soles in patients treated with bimekizumab at week 16 (see Table 3).

 

Table 3: Scalp, palmoplantar and nail responses in BE VIVID, BE READY and BE SURE at week 16

 

BE VIVID

BE READY

BE SURE

 

Placebo

 

Bimekizumab 320 mg Q4W

Ustekinumab

Placebo

Bimekizumab 320 mg Q4W

Bimekizumab 320 mg Q4W

Adalimumab

 

Scalp IGA (N)a

Scalp IGA 0/1, n (%)

 

(72)

 

11 (15.3)

 

(285)

 

240 (84.2)b

 

(146)

 

103 (70.5)

 

(74)

 

5 (6.8)

 

(310)

 

286 (92.3)b

 

(296)

 

256 (86.5)

 

(138)

 

93 (67.4)

pp-IGA (N)a

pp-IGA 0/1, n (%)

 

(29)

 

7 (24.1)

 

(105)

 

85 (81.0)

 

(47)

 

39 (83.0)

 

(31)

 

10 (32.3)

 

(97)

 

91 (93.8)

 

(90)

 

75 (83.3)

 

(34)

 

24 (70.6)

mNAPSI 100 (N)a

mNAPSI 100, n (%)

 

(51)

 

4 (7.8)

 

(194)

 

57 (29.4)

 

(109)

 

15 (13.8)

 

(50)

 

3 (6.0)

 

(210)

 

73 (34.8)

 

(181)

 

54 (29.8)

 

(95)

 

21 (22.1)

Bimekizumab 320 mg Q4W= bimekizumab every 4 weeks. Non responder imputation (NRI) is used.

Scalp IGA 0/1 and pp-IGA 0/1 responses were defined as Clear (0) or Almost Clear (1) with ≥2 category improvement relative to Baseline.

a) Include only patients with a scalp Investigator Global Assessment (IGA) of 2 or greater, a palmoplantar IGA of 2 or greater and a modified Nail Psoriasis and Severity Index (mNAPSI) score > 0 at baseline.

b) p<0.001 versus placebo, adjusted for multiplicity

 

Scalp IGA and palmoplantar IGA responses in bimekizumab-treated patients were maintained through week 52 / 56. Nail psoriasis continued to improve beyond week 16. In BE VIVID, at week 52, 60.3% of patients treated with bimekizumab 320 mg every 4 weeks achieved complete nail clearance (mNAPSI 100). In BE READY, at week 56, 67.7% and 69.8% of week 16 PASI 90 responders achieved complete nail clearance with bimekizumab 320 mg every 8 weeks and bimekizumab 320 mg every 4 weeks respectively.

 

Maintenance of response

 

Table 4: Maintenance of responses with bimekizumab at week 52 in PASI100, PASI90, IGA 0/1 and Absolute PASI ≤ 2 responders at week 16*

PASI 100

PASI 90

IGA 0/1

Absolute PASI ≤ 2

320mg Q4W
(N=355)

n (%)

320mg Q8W
(N=182)

n (%)

320mg Q4W
(N=516)

n (%)

320mg Q8W
(N=237)

n (%)

320mg Q4W
(N=511)

n (%)

320mg Q8W
(N=234)

n (%)

320mg Q4W
(N=511)

n (%)

320mg Q8W
(N= 238)

n (%)

295 (83.1)

161 (88.5)

464 (89.9)

214 (90.3)

447 (87.5)

214 (91.5)

460 (90.0)

215 (90.3)

* Integrated analysis of BE VIVID, BE READY and BE SURE. NRI is used.

320 mg Q4W: bimekizumab 320 mg every 4 weeks followed by bimekizumab 320 mg every 4 weeks from week 16.

320 mg Q8W: bimekizumab 320 mg every 4 weeks followed by bimekizumab 320 mg every 8 weeks from week 16.

 

Durability of response (after bimekizumab discontinuation)

 

Figure 3: PASI 90 responder rates over time for PASI 90 responders at week 16 – Randomized withdrawal period in BE READY

NRI is used.

At week 16, 105 study participants started the Randomized-Withdrawal Period in the bimekizumab 320 mg Q4W/placebo group, 100 in the bimekizumab 320 mg Q4W/Q8W group, and 106 in the bimekizumab 320 mg Q4W/Q4W group.

 

In BE READY, for PASI 90 responders at week 16 who were re-randomised to placebo and withdrawn from bimekizumab, the median time to relapse, defined as loss of PASI 75, was approximately 28 weeks (32 weeks after the last bimekizumab dose). Among these patients, 88.1% regained a PASI 90 response within 12 weeks of restarting treatment with bimekizumab 320 mg every 4 weeks.

 

Health-related Quality of Life / Patient reported outcomes

 

Across all 3 studies, a greater proportion of patients treated with bimekizumab experienced no impact of psoriasis on their quality of life as measured by the Dermatology Life Quality Index (DLQI) compared to placebo and active comparator-treated patients at week 16 (Table 5).

 

Table 5: Quality of life in study BE VIVID, BE READY and BE SURE

 

BE VIVID

BE READY

BE SURE

 

Placebo

 

(N= 83)

n (%)

Bimekizumab 320 mg Q4W

(N= 321)

n (%)

Ustekinumab

 

(N= 163)

n (%)

Placebo

 

(N= 86)

n (%)

Bimekizumab 320 mg Q4W

(N= 349)

n (%)

Bimekizumab 320 mg Q4W

(N= 319)

n (%)

Adalimumab

 

(N= 159)

n (%)

DLQI 0/1a Baseline

 

3 (3.6)

 

16 (5.0)

 

5 (3.1)

 

4 (4.7)

 

11 (3.2)

 

10 (3.1)

 

13 (8.2)

DLQI 0/1a

Week 16

 

10 (12.0)

 

216 (67.3)

 

69 (42.3)

 

5 (5.8)

 

264 (75.6)

 

201 (63.0)

 

74 (46.5)

a) DLQI absolute score of 0 or 1 indicates no impact of the disease on health-related quality of life. NRI is used.

 

DLQI 0/1 responses continued to increase beyond week 16 and then were maintained through week 52 / 56. In BE VIVID, DLQI 0/1 response rate at week 52 was 74.8% in patients treated with bimekizumab 320 mg every 4 weeks. In BE SURE at week 56, 78.9% and 74.1% of patients had a DLQI 0/1 with bimekizumab 320 mg every 8 weeks and bimekizumab 320 mg every 4 weeks, respectively.

 

Phase 3b direct comparative study versus secukinumab

 

The efficacy and safety of bimekizumab were also evaluated in a double-blind study compared with secukinumab, an IL-17A inhibitor, (BE RADIANT - PS0015). Patients were randomized to receive bimekizumab (N=373, 320mg at Week 0, 4, 8, 12 and 16 (Q4W) followed by 320mg every 4 weeks (Q4W/Q4W) or 320 mg every 8 weeks (Q4W/Q8W)) or secukinumab (N=370, 300 mg at Weeks 0,1, 2, 3, 4 followed by 300 mg every 4 weeks). Baseline characteristics were consistent with a population of moderate to severe plaque psoriasis patients with a median BSA of 19% and a median PASI score of 18.

 

Bimekizumab-treated patients achieved significantly higher response rates compared to secukinumab for the primary endpoint of PASI100 (complete skin clearance) at Week 16. Significantly higher response rates were also achieved with bimekizumab for the secondary endpoint of PASI 100 at Week 48 (for both Q4W/Q4W and Q4W/Q8W regimens). Comparative PASI response rates are presented in Table 6.

Differences in response rates between bimekizumab and secukinumab-treated patients were noted as early as week 1 for PASI 75 (7.2% and 1.4% respectively) and as early as Week 2 for PASI 90 (7.5% and 2.4% respectively).

 

Table 6: PASI response rates from BE RADIANT - bimekizumab versus secukinumab

 

Week 4

Week 16

Week 48a)

 

Bimekizumab 320 mg Q4W

Secukinumab

Bimekizumab 320 mg Q4W

Secukinumab

Bimekizumab 320 mg Q4W/Q4W

Bimekizumab 320 mg Q4W/Q8W

Secukinumab

 

(N=373)

n (%)

(N=370)

n (%)

(N=373)

n (%)

(N=370)

n (%)

(N=147)

n (%)

(N=215)

n (%)

(N=354)

n (%)

PASI 100

52 (13.9)

23 (6.2)

230 (61.7)*

181 (48.9)

108 (73.5)*

142 (66.0)*

171 (48.3)

PASI 90

134 (35.9)

65 (17.6)

319 (85.5)

275 (74.3)

126 (85.7)

186 (86.5)

261 (73.7)

PASI 75

265 (71.0)*

175 (47.3)

348 (93.3)

337 (91.1)

134 (91.2)

196 (91.2)

301 (85.0)

Absolute PASI<2

151 (40.5)

75 (20.3)

318 (85.3)

283 (76.5)

127 (86.4)

186 (86.5)

269 (76.0)

a) Data are from the Maintenance Set consisting of patients who received at least one dose of study treatment at Week 16 or later

*p<0.001 versus secukinumab, adjusted for multiplicity. NRI is used.

 

Bimekizumab and secukinumab PASI 100 response rates through Week 48 are presented in Figure 4.

 

Figure 4: PASI 100 response rate over time in BE RADIANT

NRI is used. Maintenance Set consisting of patients who received at least one dose of study treatment at Week 16 or later

 

The efficacy of bimekizumab in BE RADIANT was consistent with BE VIVID, BE READY and BE SURE.

 

Psoriatic arthritis (PsA)

 

The safety and efficacy of bimekizumab were evaluated in 1112 adult patients (at least 18 years of age) with active psoriatic arthritis (PsA) in two multicentre, randomized, double-blind, placebo-controlled studies (PA0010 - BE OPTIMAL and PA0011- BE COMPLETE). The BE OPTIMAL study included an active reference treatment arm (adalimumab) (N=140).

 

For both studies, patients had a diagnosis of active psoriatic arthritis for at least 6 months based on the Classification Criteria for Psoriatic Arthritis (CASPAR) and had active disease with tender joint count (TJC) ≥3 and swollen joint count (SJC) ≥3. Patients had a diagnosis of PsA for a median of 3.6 years in BE OPTIMAL and 6.8 years in BE COMPLETE. Patients with each subtype of PsA were enrolled in these studies, including polyarticular symmetric arthritis, oligoarticular asymmetric arthritis, distal interphalangeal joint predominant, spondylitis predominant and arthritis mutilans. At baseline, 55.9% of patients had ≥ 3% Body Surface Area (BSA) with active plaque psoriasis. 10.4% of patients had moderate to severe plaque psoriasis and 31.9% and 12.3% had enthesitis and dactylitis at baseline, respectively. The primary efficacy endpoint in both studies was the American College of Rheumatology (ACR) 50 response at Week 16.

 

The BE OPTIMAL study evaluated 852 patients not previously exposed to any biologic disease-modifying anti-rheumatic drug (bDMARD) for the treatment of psoriatic arthritis or psoriasis. Patients were randomized (3:2:1) to receive bimekizumab 160 mg every 4 weeks through Week 52 or placebo up to Week 16 followed by bimekizumab 160 mg every 4 weeks through Week 52 or an active reference treatment arm (adalimumab 40mg every 2 weeks) up to Week 52. In this study, 78.3% of patients had received prior treatment with ≥ 1 cDMARDs and 21.7 % of patients had no prior treatment with cDMARDs. At baseline, 58.2% of patients were receiving concomitant methotrexate (MTX), 11.3% were receiving concomitant cDMARDs other than MTX, and 30.5% were receiving no cDMARDs.

 

The BE COMPLETE study evaluated 400 patients with an inadequate response (lack of efficacy) or intolerance to treatment with 1 or 2 tumour necrosis factor alpha inhibitors (anti-TNFα – IR) for either psoriatic arthritis or psoriasis. Patients were randomized (2:1) to receive bimekizumab 160 mg every 4 weeks or placebo up to Week 16. At baseline, 42.5% of patients were receiving concomitant MTX, 8.0% were receiving concomitant cDMARDs other than MTX, and 49.5% were receiving no cDMARDs. In this study, 76.5% of participants had an inadequate response to 1 TNFα inhibitor, 11.3% had an inadequate response to 2 TNFα inhibitors and 12.3% were intolerant to TNFα inhibitors.

 

Signs and symptoms

In bDMARDs-naïve patients (BE OPTIMAL) and anti-TNFα IR patients (BE COMPLETE) treatment with bimekizumab resulted in significant improvement in signs and symptoms and measures of disease activity compared to placebo at Week 16, with similar response rates seen in both patient populations (see Table 7). Clinical responses were sustained up to Week 52 in BE OPTIMAL as assessed by ACR 20, ACR 50, ACR 70, MDA, PASI 90, PASI 100 and ACR 50 / PASI 100.

 

Table 7: Clinical response in study BE OPTIMAL and BE COMPLETE

 

BE OPTIMAL (bDMARD-naïve)

BE COMPLETE (anti TNFα-IR)

Placebo

(N=281)

n (%)

BKZ 160mg Q4W

(N=431)

n (%)

Difference from placebo (95% CI)(d)

Reference Arm(e) (Adalimumab)

(N=140)

n (%)

Placebo

(N=133)

n (%)

BKZ 160 mg Q4W

(N=267)

n (%)

Difference from placebo (95% CI)(d)

 

ACR 20

Week 16

Week 24

Week 52

 

67 (23.8)

-

 

268 (62.2)

282 (65.4)

307 (71.2)

 

38.3 (31.4, 45.3)

 

 

96 (68.6)

99 (70.7)

102 (72.9)

 

21 (15.8)

 

 

179 (67.0)

 

 

51.2 (42.1, 60.4)

 

ACR 50

Week 16

Week 24

Week 52

 

28 (10.0)

-

 

189 (43.9)*

196 (45.5)

235 (54.5)

 

33.9 (27.4, 40.4)

 

 

64 (45.7)

66 (47.1)

70 (50.0)

 

9 (6.8)

 

116 (43.4)*

 

36.7 (27.7, 45.7)

 

ACR 70

Week16

Week 24

Week 52

 

12 (4.3)

-

 

105 (24.4)

126 (29.2)

169 (39.2)

 

20.1 (14.7, 25.5)

 

 

39 (27.9)

42 (30.0)

53 (37.9)

 

1 (0.8)

 

71 (26.6)

 

25.8 (18.2, 33.5)

 

MDA(a)

Week 16

Week 24

Week 52

 

37 (13.2)

-

 

194 (45.0)*

209 (48.5)

237 (55.0)

 

31.8 (25.2, 38.5)

 

 

63 (45.0)

67 (47.9)

74 (52.9)

 

8 (6.0)

 

118 (44.2)*

 

38.2 (29.2, 47.2)

 

Patients with ≥3% BSA

(N=140)

(N=217)

 

(N=68)

(N=88)

(N=176)

 

 

PASI 90

Week 16

Week 24

Week 52

 

4 (2.9)

-

 

133 (61.3)*

158 (72.8)

155 (71.4)

 

58.4 (49.9, 66.9)

 

 

28 (41.2)

32 (47.1)

41 (60.3)

 

6 (6.8)

 

121 (68.8)*

 

61.9 (51.5, 72.4)

 

PASI 100

Week 16

Week 24

Week 52

 

3 (2.1)

-

 

103 (47.5)

122 (56.2)

132 (60.8)

 

45.3 (36.7, 54.0)

 

 

14 (20.6)

26 (38.2)

33 (48.5)

 

4 (4.5)

 

103 (58.5)

 

54.0 (43.1, 64.8)

 

ACR50/

PASI 100

Week 16

Week 24

Week 52

 

 

0

-

 

 

60 (27.6)

68 (31.3)

102 (47.0)

 

 

NC (NC, NC)

 

 

 

11 (16.2)

17 (25.0)

24 (35.3)

 

 

1 (1.1)

 

 

59 (33.5)

 

 

32.4 (22.3, 42.5)

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

Patients with LDI>0 (b)

(N=47)

(N=90)

 

 

 

Dactylitis free state (b)

Week 16

 

24 (51.1)

 

68 (75.6)***

 

24.5 (8.4, 40.6)

 

 

Patients with LEI>0 (c)

(N=106)

(N=249)

 

 

 

Enthesitis free state (c)

Week 16

 

37 (34.9)

 

124 (49.8)**

 

14.9 (3.7, 26.1)

 

 

ACR50/PASI100= composite ACR50 and PASI100 response. BKZ 160 mg Q4W= bimekizumab 160 mg every 4 weeks. CI= confidence interval. NC=Not calculable

(a) A patient was classified as achieving Minimal Disease Activity (MDA) when meeting 5 of the 7 following criteria: tender joint count ⩽1; swollen joint count ⩽1; Psoriasis Activity and Severity Index ⩽1 or body surface area ⩽3; patient pain visual analogue scale (VAS) ⩽15; patient global disease activity VAS ⩽20; Health Assessment Questionnaire Disability Index ⩽0.5; tender entheseal points ⩽1   

(b) Based on pooled data from BE OPTIMAL and BE COMPLETE studies for patients with baseline Leeds Dactylitis Index (LDI) >0. Dactylitis free state is LDI=0

(c) Based on pooled data from BE OPTIMAL and BE COMPLETE studies for patients with baseline Leeds Enthesitis Index (LEI) >0. Enthesitis free state is LEI =0

(d) Unadjusted differences are shown

(e) No statistical comparison to bimekizumab or placebo performed

* p<0.001 versus placebo adjusted for multiplicity. ** p=0.008 versus placebo adjusted for multiplicity. *** p=0.002 versus placebo adjusted for multiplicity. NRI is used. Other endpoints at Week 16 and all endpoints at Week 24 and Week 52 were not part of the sequential testing hierarchy and any comparisons are nominal.

 

 

Improvements from baseline were shown in all individual ACR components with bimekizumab at Week 16 and were sustained up to Week 52 in BE OPTIMAL.

 

Treatment responses on bimekizumab were significantly greater than those on placebo as early as Week 2 for ACR 20 (BE OPTIMAL, 27.1% versus 7.8%, nominal p<0.001) and Week 4 for ACR 50 (BE OPTIMAL, 17.6% versus 3.2%, nominal p<0.001 and BE COMPLETE, 16.1% versus 1.5%, nominal p<0.001).

 

 

 

 

 

 

 

 

 

 

Figure 5: ACR 50 response over time up to Week 52 in BE OPTIMAL (NRI)

 

Patients on placebo switched to bimekizumab 160 mg Q4W at Week 16.

 

Figure 6: ACR 50 response over time up to Week 16 in BE COMPLETE (NRI)

 

For the bimekizumab-treated patients who achieved an ACR 50 response at Week 16 in BE OPTIMAL, 87.2% maintained this response at Week 52.

 

The efficacy and safety of bimekizumab were demonstrated regardless of age, gender, race, baseline body weight, baseline psoriasis involvement, baseline CRP, disease duration and prior cDMARDs use. In both studies, similar responses were observed with bimekizumab regardless of whether patients were on concomitant cDMARDs, including MTX, or not.

 

The modified Psoriatic Arthritis Response Criteria (PsARC) is a specific composite responder index comprising of tender joint count, swollen joints count, patient and physician global assessment. The proportion of patients achieving modified PsARC at Week 16 was higher in the bimekizumab-treated patients compared to placebo (80.3% versus 40.2% respectively in BE OPTIMAL and 85.4% versus 30.8% respectively in BE COMPLETE). PsARC response was sustained up to Week 52 in BE OPTIMAL.

 

Radiographic response

In BE OPTIMAL, inhibition of progression of structural damage was assessed radiographically and expressed as the change from baseline in the Van der Heijde modified total Sharp Score (vdHmTSS) and its components, the Erosion Score (ES) and the Joint Space Narrowing score (JSN) at Week 16 (see Table 8).

 

Table 8: Change in vdHmTSS in BE OPTIMAL at Week 16

 

Placebo

 

BKZ 160mg Q4W

 

Difference from placebo (95% CI)a)

Population with elevated hs-CRP and/or at least 1 bone erosion at baseline

(N=227)

(N=361)

 

Mean change from baseline (SE)

0.36 (0.10)

0.04 (0.05)*

-0.32 ( -0.35, -0.30)

Overall population

(N=269)

(N=420)

 

Mean change from baseline (SE)

0.32 (0.09)

0.04 (0.04)*

-0.26 ( -0.29, -0.23)

*p =0.001 versus placebo. p-values are based on reference-based imputation using difference in LS Mean using an ANCOVA model with treatment, bone erosion at Baseline and region as fixed effects and Baseline score as a covariate.

Week 16 summary data is based on the first set of reads for the primary analysis.

a)Unadjusted differences are shown

 

Bimekizumab significantly inhibited the progression of joint damage at Week 16 in both the population with elevated hs-CRP and/or at least 1 bone erosion at baseline and the overall population compared to placebo. While reference-based imputation was specified as the missing data handling method in the statistical testing procedure comparing bimekizumab versus placebo, changes from baseline were also calculated using standard multiple imputation in both the population with elevated hs-CRP and/or at least 1 bone erosion at baseline and the overall population at Week 16 in the bimekizumab arm (mean change from baseline 0.01 and 0.01 respectively) and the adalimumab arm (mean change from baseline -0.05 and -0.03 respectively). Inhibition of the progression of joint damage was sustained in both the population with elevated hs-CRP and/or at least 1 bone erosion at baseline and the overall population to Week 52 in both the bimekizumab arm (mean change from baseline 0.10 and 0.10 respectively) and the adalimumab arm (mean change from baseline -0.17 and -0.12 respectively).

The observed percentage of patients with no radiographic joint damage progression (defined as a change from baseline in mTSS of ≤0.5) from randomization to Week 52 was 87.9% (N=276/314) for bimekizumab and 84.8% (N=168/198) for placebo study participants switching to bimekizumab and 94.1% (N=96/102) for adalimumab in the population with elevated hs-CRP and/or at least 1 bone erosion. Similar rates were observed in the overall population (89.3% (N=326/365) for bimekizumab and 87.3% (N=207/237) for placebo study participants switching to bimekizumab and 94.1% (N=111/118) for adalimumab).

 

Physical function and other health-related outcomes

 

Both bDMARD-naïve (BE OPTIMAL) and anti-TNFα-IR (BE COMPLETE) patients receiving bimekizumab showed significant improvement from baseline in physical function compared to placebo patients at Week 16 (p<0.001) as assessed by the HAQ-DI (LS Mean change from baseline: - 0.3 versus - 0.1 in BE OPTIMAL and - 0.3 versus 0 in BE COMPLETE, respectively). In both studies, a greater proportion of patients achieved a clinically meaningful reduction of at least 0.35 in HAQ-DI score from baseline in the bimekizumab group compared with placebo at Week 16.

 

Bimekizumab-treated patients reported significant improvement from baseline in the Short Form-36 item Health Survey Physical Component Summary (SF-36 PCS) score at Week 16 compared to placebo (LS Mean change from baseline: 6.3 versus 1.9, p<0.001 in BE OPTIMAL and 6.2 versus 0.1, p<0.001 in BE COMPLETE).

 

In both studies, bimekizumab-treated patients reported meaningful reduction from baseline in fatigue as measured by the Functional Assessment of Chronic Illness Therapy (FACIT)-Fatigue score at Week 16 compared to placebo. Meaningful improvement from baseline was also observed in the Psoriatic Arthritis Impact of Disease-12 (PsAID-12) score in the bimekizumab-treated group compared to the placebo group at Week 16.

Patients with axial involvement at baseline, approximately 74% of patients, (defined as a Bath Ankylosing Spondylitis Disease Activity Index (BASDAI) score ≥4) showed greater improvement from baseline in BASDAI compared with placebo at Week 16

Improvements achieved at Week 16 in all measures of physical function and other health-related outcomes mentioned above (HAQ-DI, SF-36 PCS, FACIT-Fatigue, PsAID-12 scores and BASDAI) were sustained up to Week 52 in BE OPTIMAL.

 

In BE OPTIMAL, at Week 52, 65.5% of patients treated with bimekizumab achieved complete nail clearance (mNAPSI resolution in patients with mNAPSI higher than 0 at Baseline).

 

Axial spondyloarthritis (nr-axSpA and AS)

 

The efficacy and safety of bimekizumab was evaluated in 586 adult patients (at least 18 years of age) with active axial spondyloarthritis (axSpA) in two multicenter, randomized, double-blind, placebo-controlled studies, one in non-radiographic axial spondyloarthritis (nr-axSpA) and one in ankylosing spondylitis (AS), also known as radiographic axSpA. The primary endpoint in both studies was the percentage of patients achieving an Assessment of SpondyloArthritis International Society (ASAS) 40 response at Week 16. Consistent results were seen across both patient populations.

 

The BE MOBILE 1 study (AS0010) evaluated 254 patients with active nr-axSpA. Patients had axSpA (age of symptoms onset < 45 years) meeting the ASAS classification criteria and had active disease as defined by a Bath Ankylosing Spondylitis Disease Activity Index (BASDAI) ≥4 and spinal pain ≥4 on a 0 to 10 numeric rating scale (NRS) (from BASDAI Item 2) and no evidence of radiographic changes in the sacroiliac joints that would meet the modified New York criteria for AS. Patients also had objective signs of inflammation as indicated by elevated C-reactive protein (CRP) level and/or evidence of sacroiliitis on Magnetic Resonance Imaging (MRI) as well as a history of inadequate response to 2 different non-steroidal anti-inflammatory drugs (NSAIDs) or intolerance or contraindication to NSAIDs. Patients were randomized (1:1) to receive bimekizumab 160 mg every 4 weeks up to Week 52 or placebo up to Week 16 followed by bimekizumab 160 mg every 4 weeks up to Week 52. At baseline, patients had symptoms of nr-axSpA for a mean of 9 years (median of 5.5 years). 10.6% of patients were previously treated with an anti-TNFα agent.

 

The BE MOBILE 2 study (AS0011) evaluated 332 patients with active AS determined by documented radiologic evidence (x-ray) fulfilling the Modified New York criteria for AS. Patients had active disease as defined by a BASDAI ≥4 and spinal pain ≥4 on a 0 to 10 numeric rating scale (NRS) (from BASDAI Item 2). Patients had to have a history of inadequate response to 2 different NSAIDs or intolerance or contraindication to NSAIDs. Patients were randomized (2:1) to receive bimekizumab 160 mg every 4 weeks up to Week 52 or placebo up to Week 16 followed by bimekizumab 160 mg every 4 weeks up to Week 52. At baseline, patients had symptoms of AS for a mean of 13.5 years (median of 11 years). 16.3% of patients were previously treated with an anti-TNFα agent.

 

 

Clinical response

 

Treatment with bimekizumab resulted in significant improvement in signs and symptoms and measures of disease activity compared to placebo at Week 16 in both nr-axSpA and AS patient populations (see Table 9). Clinical responses were sustained up to Week 52 in both patient populations as assessed by all the endpoints presented in Table 9.

Table 9: Clinical responses in BE MOBILE 1 and BE MOBILE 2

 

BE MOBILE 1 (nr-axSpA)

BE MOBILE 2 (AS)

 

Placebo

(N=126)

n (%)

BKZ 160 mg Q4W

(N=128)

n (%)

Difference from placebo (95% CI)a)

Placebo

(N=111)

n (%)

BKZ 160 mg Q4W

(N=221)

n (%)

Difference from placebo (95% CI)a)

ASAS 40

Week 16

Week 52

 

27 (21.4)

 

61 (47.7)*

78 (60.9)

 

26.2 (14.9, 37.5)

 

 

25 (22.5)

 

99 (44.8)*

129 (58.4)

 

22.3 (11.5, 33.0)

ASAS 40 in anti-TNFα naives

Week 16

Week 52

 

(N=109)

25 (22.9)

 

 

(N= 118)

55 (46.6)

73 (61.9)

 

 

24.8 (12.4, 37.1)

 

(N=94)

22 (23.4)

 

 

(N=184)

84 (45.7)*

108 (58.7)

 

 

22.3 (10.5, 34.0)

ASAS 20

Week 16

Week 52

 

48 (38.1)

 

88 (68.8)*

94 (73.4)

 

30.7 (19.0, 42.3)

 

48 (43.2)

 

146 (66.1)*

158 (71.5)

 

22.8 (11.8, 33.8)

ASAS-partial remission

Week 16

Week 52

 

9 (7.1)

 

 

33 (25.8)*

38 (29.7)

 

18.6 (9.7, 27.6)

 

8 (7.2)

 

53 (24.0)*

66 (29.9)

 

16.8 (8.1, 25.5)

ASDAS-major improvement

Week 16

Week 52

 

 

9 (7.1)

 

 

35 (27.3)*

47 (36.7)

 

 

20.2 (11.2, 29.3)

 

 

6 (5.4)

 

 

57 (25.8)*

71 (32.1)

 

 

20.4 (11.7, 29.1)

BASDAI-50

Week 16

Week 52

 

27 (21.4)

 

60 (46.9)

69 (53.9)

 

25.3 (14.0, 36.6)

 

29 (26.1)

 

103 (46.6)

119 (53.8)

 

20.5 (9.6, 31.4)

BKZ 160 mg Q4W = bimekizumab 160 mg every 4 weeks. ASDAS = Ankylosing Spondylitis Disease Activity Score.

NRI is used.

a) Unadjusted differences are shown.

*p<0.001 versus placebo, adjusted for multiplicity.

The proportion of patients in BE MOBILE 1 reaching ASDAS <2.1 (combining ASDAS-inactive disease (ID) and ASDAS-low disease (LD)) at Week 16 was 46.1% in the bimekizumab group versus 21.1% in the placebo group (multiple imputation). At Week 52, 61.6% of patients in the bimekizumab group achieved an ASDAS <2.1, including 25.2% in inactive disease state (ASDAS <1.3).

 

The proportion of patients in BE MOBILE 2 reaching ASDAS <2.1 (combining ASDAS-ID and ASDAS-LD) at Week 16 was 44.8% in the bimekizumab group versus 17.4% in placebo group (multiple imputation). At Week 52, 57.1% of patients in the bimekizumab group achieved an ASDAS <2.1, including 23.4 % in inactive disease state (ASDAS <1.3).

 

All four ASAS 40 components (total spinal pain, morning stiffness, Bath Ankylosing Spondylitis Functional Index [BASFI] and Patient’s Global Assessment of Disease Activity [PGADA]) were improved with bimekizumab treatment and contributed to the overall ASAS 40 response at week 16, and these improvements were sustained up to Week 52 in both patient populations.  

 

Improvements in other measures of efficacy are shown in Table 10.

 

Table 10: Other measures of efficacy in BE MOBILE 1 and BE MOBILE 2

 

BE MOBILE 1 (nr-axSpA)

BE MOBILE 2 (AS)

 

Placebo

(N= 126)

BKZ 160 mg Q4W

(N= 128)

Placebo

(N= 111)

BKZ 160 mg Q4W

(N=221)

Nocturnal spinal pain

Baseline

Mean change from baseline at Week 16

Mean change from baseline at Week 52

 

6.7

-1.7

 

6.9

-3.6*

-4.3

 

6.8

-1.9

 

6.6

-3.3*

-4.1

BASDAI

Baseline

Mean change from baseline at Week 16

Mean change from baseline at Week 52

 

6.7

-1.5

 

6.9

-3.1*

-3.9

 

6.5

-1.9

 

6.5

-2.9*

-3.6

BASMI

Baseline

Mean change from baseline at Week 16

Mean change from baseline at Week 52

 

3.0

-0.1

 

2.9

-0.4

-0.6

 

3.8

-0.2

 

3.9

-0.5**

-0.7

hs-CRP (mg/L)

Baseline (Geometric Mean)

Ratio to baseline at Week 16

Ratio to baseline at Week 52

 

5.0

0.8

 

4.6

0.4

0.4

 

6.7

0.9

 

6.5

0.4

0.3

BASMI = Bath Ankylosing Spondylitis Metrology Index. Hs-CRP = high sensitivity C-reactive protein

MI is used.

*p<0.001 reference-based imputation, versus placebo, adjusted for multiplicity. **p<0.01 reference-based imputation, versus placebo, adjusted for multiplicity.

 

Bimekizumab was associated with a rapid onset of efficacy in both nr-axSpA and AS patient population.

Treatment responses on bimekizumab-treated patients for ASAS 40 were greater than those on placebo as early as Week 1 in BE MOBILE 1 (16.4% vs. 1.6%, nominal p<0.001) and Week 2 in BE MOBILE 2 (16.7% vs. 7.2%, nominal p=0.019).

Bimekizumab was also associated with a rapid decrease in systemic inflammation as measured by hs-CRP levels as early as Week 2 in both nr-axSpA and AS patient populations, with nominal p-values <0.001 in both studies.

Figure 7: ASAS 40 response over time up to Week 52 in BE MOBILE 1 (NRI)

Patients on placebo switched to bimekizumab 160 mg Q4W at Week 16

 

Figure 8: ASAS 40 response over time up to Week 52 in BE MOBILE 2 (NRI)

Patients on placebo switched to Bimekizumab 160 mg Q4W at Week 16

 

In an integrated analysis of BE MOBILE 1 and BE MOBILE 2, of bimekizumab-treated patients who achieved an ASAS 40 response at Week 16, 82.1% maintained this response at Week 52.

 

The efficacy of bimekizumab was demonstrated regardless of age, gender, race, disease duration, baseline inflammation status, baseline ASDAS and concomitant cDMARDs.

 

Similar response in ASAS 40 was seen in patients regardless of prior anti-TNFα exposure.

 

At Week 16, among patients with enthesitis at baseline, the proportion of patients (NRI) with enthesitis resolution as assessed by the Maastricht Ankylosing Spondylitis Enthesitis (MASES) index was greater with bimekizumab compared to placebo (BE MOBILE 1: 51.1% versus 23.9% and BE MOBILE 2: 51.5% versus 32.8%). The resolution of enthesitis with bimekizumab was sustained up to Week 52 in both studies (BE MOBILE 1: 54.3% and BE MOBILE 2: 50.8%).

 

Reduction of inflammation

 

Bimekizumab reduced inflammation as measured by hs-CRP (see Table 10) and as assessed by MRI in an imaging sub-study. Signs of inflammation were assessed by MRI at baseline and Week 16 and expressed as change from baseline in Spondyloarthritis Research Consortium of Canada (SPARCC) score for sacroiliac joints and Ankylosing Spondylitis spine Magnetic Resonance Imagine-activity (ASspiMRI-a score in the Berlin modification) for the spine. Reduction of inflammatory signs in both sacroiliac joints and the spine was observed in patients treated with bimekizumab as compared with placebo (see Table 11). Reduction of inflammation as measured by hs-CRP and as assessed by MRI was sustained to Week 52.

Table 11: Reduction of inflammation as assessed by MRI in BE MOBILE 1 and BE MOBILE 2

 

BE MOBILE 1 (nr-axSpA)

BE MOBILE 2 (AS)

 

Placebo

BKZ 160 mg Q4W

Placebo

BKZ 160 mg Q4W

SPARCC score

Mean change from baseline a) at week 16

 

Mean change from baseline a) at week 52

 

-1.56

(N=62)

 

 

-6.15

(N=78)

-7.57

(N=67)

 

0.59

(N=46)

 

 

-4.51

(N=81)

-4.67

(N=78)

ASspiMRI-a (Berlin modifications) score

Mean change from baseline a) at week 16

 

Mean change from baseline a) at week 52

 

0.03

(N=60)

 

 

-0.36

(N=74)

-0.70

(N=65)

 

-0.34

(N=46)

 

 

-2.23

(N=81)

-2.38

(N=77)

a)      Change from baseline values are based on observed cases as assessed by central read of Week 52 dataset.

 

Physical function and other health-related outcomes

 Patients treated with bimekizumab showed significant improvement from baseline in physical function as assessed by the BASFI compared to placebo (LS Mean change from baseline at Week 16 in BE MOBILE 1: -2.4 versus -0.9, p<0.001 and in BE MOBILE 2: -2.0 versus -1.0, p<0.001). Patients treated with bimekizumab reported significant improvement from baseline compared to placebo-treated patients in SF-36 PCS score (LS Mean change from baseline at Week 16 in BE MOBILE 1: 9.3 versus 5.4, p<0.001 and in BE MOBILE 2: 8.5 versus 5.2, p<0.001).

 

Patients treated with bimekizumab reported significant improvement from baseline in health-related quality of life as measured by the AS Quality of Life Questionnaire (ASQoL) compared to placebo (LS Mean change from baseline at Week 16 in BE MOBILE 1: -4.9 versus -2.3, p<0.001 and in BE MOBILE 2: -4.6 versus -3.0, p<0.001) as well as meaningful reduction in fatigue as assessed by the FACIT-Fatigue score (Mean change from baseline at Week 16 in BE MOBILE 1: 8.5 for bimekizumab versus 3.9 for placebo and in BE MOBILE 2: 8.4 for bimekizumab versus 5.0 for placebo).

 

Improvements achieved at Week 16 in all measures of physical function and other health-related outcomes mentioned above (BASFI, SF-36 PCS, ASQoL and FACIT-Fatigue scores) were sustained up to Week 52 in both studies.    

 

Extra-articular manifestation

 

In pooled data from BE MOBILE 1 (nr-axSpA) and BE MOBILE 2 (AS), at Week 16, the proportion of patients developing a uveitis event was lower with bimekizumab (0.6%) compared to placebo (4.6%). The incidence of uveitis remained low with long-term treatment with bimekizumab (1.2/100 patient-years in the pooled phase 2/3 studies).

 

Paediatric population

 

The European Medicines Agency has deferred the obligation to submit the results of studies with Bimzelx in one or more subsets of the paediatric population in psoriasis and chronic idiopathic arthritis (see section 4.2 for information on paediatric use).


The pharmacokinetic (PK) properties of bimekizumab were similar in patients with plaque psoriasis, psoriatic arthritis and axial spondyloarthritis (nr-axSpA and AS).

 

 

Absorption

 

Based on population pharmacokinetic analysis, following a single subcutaneous dose of 320 mg in plaque psoriasis patients, bimekizumab reached a median (2.5th and 97.5th percentile) peak plasma concentration of 25 (12 -50) μg/mL, between 3 and 4 days post dose.

 

Population pharmacokinetic analysis showed that bimekizumab was absorbed with an average absolute bioavailability of 70.1% in healthy volunteers.

 

Based on simulated data, the median (2.5th and 97.5th percentile) peak and trough concentration at steady-state following subcutaneous administration of 320 mg every 4 weeks are 43 (20-91) µg/mL and 20 (7-50) µg/mL respectively and steady-state is reached after approximately 16 weeks with every 4 weeks dosing regimen. Compared with exposure after a single dose, the population pharmacokinetic analysis showed that patients exhibited a 1.74-fold increase in peak plasma concentrations and area under the curve (AUC) following repeated four weekly dosing.

 

After switching from the 320 mg every 4 weeks dosing regimen to 320 mg every 8 weeks dosing regimen at week 16, steady-state is achieved approximately 16 weeks after the switch. Median (2.5th and 97.5th percentile) peak and trough plasma concentrations are 30 (14 -60) μg/mL and 5 (1-16) μg/mL respectively.

 

Distribution

 

Based on population pharmacokinetic analyses, the median (coefficient of variation %) volume of distribution (V/F) at steady state was 11.2 (30.5%) L in plaque psoriasis patients.

 

Biotransformation

 

Bimekizumab is a monoclonal antibody and is expected to be degraded into small peptides and amino acids via catabolic pathways in the same manner as endogenous immunoglobulins.

 

Elimination

 

Based on population pharmacokinetic analyses, the median (coefficient of variation %) apparent clearance (CL/F) of bimekizumab was 0.337 L/day (32.7%) and the mean terminal elimination half-life of bimekizumab was 23 days in clinical studies in patients with plaque psoriasis.

 

Linearity/non-linearity

 

Bimekizumab exhibited dose-proportional pharmacokinetics in patients with plaque psoriasis over a dose range from 64 mg to 480 mg following multiple subcutaneous administrations, with apparent clearance (CL/F) being independent of dose.

 

Pharmacokinetic/Pharmacodynamic relationship

 

A population pharmacokinetic/pharmacodynamic model was developed using all available data in moderate to severe plaque psoriasis patients. The analysis showed that higher bimekizumab concentrations are related to better Psoriasis Area and Severity Index (PASI) and Investigators Global Assessment (IGA) response. A dose of 320 mg every 4 weeks was shown to be an appropriate dose for the initial treatment period and 320 mg every 8 weeks thereafter is appropriate for the maintenance period for the majority of moderate to severe plaque psoriasis patients (see Special Populations, Body weight).

 

Special populations

 

Body weight

Population pharmacokinetic modelling indicated that exposure decreased as body weight increased. The average plasma concentration in adult patients weighing ≥120 kg following a 320 mg subcutaneous injection was predicted to be at least 30% lower than in adult patients weighing 90 kg. Dose adjustment may be appropriate in some patients (see section 4.2).

 

Elderly

Based on population pharmacokinetic analysis with a limited number of elderly patients (n=337 for age ≥ 65 years and n= 45 for age ≥ 75 years), apparent clearance (CL/F) in elderly patients and patients less than 65 years of age was similar. No dose adjustment is required (see section 4.2).

 

Renal impairment or hepatic impairment

No specific studies have been conducted to determine the effect of renal or hepatic impairment on the pharmacokinetics of bimekizumab. The renal elimination of intact bimekizumab, an IgG monoclonal antibody, is expected to be low and of minor importance. Similarly, IgGs are mainly eliminated via intracellular catabolism and hepatic impairment is not expected to influence clearance of bimekizumab. Based on population pharmacokinetic analyses, hepatic function markers (ALT/bilirubin) did not have any impact on bimekizumab clearance in patients with plaque psoriasis.

 

Race

No clinically meaningful differences in bimekizumab exposure were observed in Japanese or Chinese subjects compared to Caucasian subjects in a clinical pharmacokinetic study. No dose adjustment is required.

 

Gender

Population pharmacokinetic modelling indicated females may have 10% faster apparent clearance (CL/F) compared to males and it is not clinically meaningful. No dose adjustment is required


Non-clinical data revealed no special hazard for humans based on tissue cross-reactivity testing, repeat-dose toxicity studies (including safety pharmacology endpoints and assessment of fertility-related endpoints) and evaluation of pre- and postnatal development in the cynomolgus monkey.

 

In cynomolgus monkeys, bimekizumab-related effects were limited to mucocutaneous changes consistent with pharmacologic modulation of commensal microflora.

 

No mutagenicity or carcinogenicity studies were conducted with bimekizumab. However monoclonal antibodies are not expected to damage DNA or chromosomes. In a 26-week chronic toxicology study in cynomolgus monkeys there were no pre-neoplastic or neoplastic lesions observed at a dose resulting in 109 times the human exposure at 320 mg every 4 weeks.

 

In a peri- and postnatal development study in the cynomolgus monkey, bimekizumab showed no effects on gestation, parturition, infant survival, foetal and postnatal development when administered throughout organogenesis until parturition at a dose resulting in 27 times the human exposure at 320 mg every 4 weeks based on AUC. At birth, serum bimekizumab concentrations in infant monkeys were comparable to those of mothers.


Glycine

Sodium acetate trihydrate

Glacial acetic acid

Polysorbate 80

Water for injections


In the absence of compatibility studies, this medicinal product must not be mixed with other medicinal products.


3 years

Bimzelx 160 mg solution for injection in pre-filled syringe

Store in a refrigerator (2°C – 8°C).

Do not freeze.

 

Keep the pre-filled syringe in the outer carton in order to protect from light.

 

The pre-filled syringe may be stored at room temperature (up to 25°C) for a single period of maximum 25 days with protection from light. Once removed from the refrigerator and stored under these conditions, discard after 25 days or by the expiry date printed on the container, whichever occurs first. A field for the date is provided on the carton to record the date removed from the refrigerator.

 

Bimzelx 160 mg solution for injection in pre-filled pen

 

Store in a refrigerator (2°C – 8°C).

Do not freeze.

 

Keep the pre-filled pen in the outer carton in order to protect from light.

 

The pre-filled pen may be stored at room temperature (up to 25°C) for a single period of maximum 25 days with protection from light. Once removed from the refrigerator and stored under these conditions, discard after 25 days or by the expiry date printed on the container, whichever occurs first. A field for the date is provided on the carton to record the date removed from the refrigerator.


Bimzelx 160 mg solution for injection in pre-filled syringe

 

One mL pre-filled syringe (type I glass) with a fluoropolymer-laminated bromobutyl rubber stopper, staked 27G, ½” thin wall needle, and a polypropylene rigid needle shield assembled in a passive safety device.

 

Pack size of 1 pre-filled syringe.

Pack size of 2 pre-filled syringes.

Multipack containing 3 (3 packs of 1) pre-filled syringes.

Multipack containing 4 (2 packs of 2) pre-filled syringes.

 

Not all pack sizes may be marketed.

 

Bimzelx 160 mg solution for injection in pre-filled pen

 

One mL pre-filled pen containing a pre-filled syringe (type I glass) with a fluoropolymer-laminated bromobutyl rubber stopper, staked 27G, ½” thin wall needle, and a polypropylene rigid needle shield.

 

Pack size of 1 pre-filled pen.

Pack size of 2 pre-filled pens.

Multipack containing 3 (3 packs of 1) pre-filled pens.

Multipack containing 4 (2 packs of 2) pre-filled pens.

 

Not all pack sizes may be marketed


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


UCB Pharma S.A. Allée de la Recherche 60 B-1070 Bruxelles Belgium 8. MARKETING AUTHORISATION NUMBER(S) Bimzelx 160 mg solution for injection in pre-filled syringe EU/1/21/1575/001 EU/1/21/1575/002 EU/1/21/1575/003 EU/1/21/1575/004 Bimzelx 160 mg solution for injection in pre-filled pen EU/1/21/1575/005 EU/1/21/1575/006 EU/1/21/1575/007 EU/1/21/1575/008

(06/23) Detailed information on this medicinal product is available on the website of the European Medicines Agency http://www.ema.europa.eu.
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