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Pomalidomide SPC is used to treat adults with a type of cancer called ‘multiple myeloma’.
Pomalidomide SPC is either used with:
· two other medicines - called ‘bortezomib’ (a type of chemotherapy medicine) and ‘dexamethasone’ (an anti-inflammatory medicine) in people who have had at least one other treatment - including lenalidomide.
Or
· one other medicine - called ‘dexamethasone’ in people whose myeloma has become worse, despite having at least two other treatments - including lenalidomide and
bortezomib.
What is multiple myeloma
Multiple myeloma is a type of cancer which affects a certain type of white blood cell (called the ‘plasma cell’). These cells grow out of control and accumulate in the bone marrow. This results in damage to the bones and kidneys.
Multiple myeloma generally cannot be cured. However, treatment can reduce the signs and symptoms of the disease, or make them disappear for a period of time. When this happens, it is called ‘response’.
How Pomalidomide SPC works
Pomalidomide SPC works in a number of different ways:
• by stopping the myeloma cells developing
• by stimulating the immune system to attack the cancer cells
• by stopping the formation of blood vessels supplying the cancer cells.
The benefit of using Pomalidomide SPC with bortezomib and dexamethasone
When Pomalidomide SPC is used with bortezomib and dexamethasone, in people who have had at least one other treatment, it can stop multiple myeloma getting worse:
• On average, Pomalidomide SPC when used with bortezomib and dexamethasone stopped multiple myeloma from coming back for up to 11 months - compared with 7 months for those patients who only used bortezomib and dexamethasone.
The benefit of using Pomalidomide SPC with dexamethasone
When Pomalidomide SPC is used with dexamethasone, in people who have had at least two other treatments, it can stop multiple myeloma getting worse:
• On average, Pomalidomide SPC when used with dexamethasone stopped multiple myeloma from coming back for up to 4 months - compared with 2 months for those patients who used only dexamethasone.
1. Do not use Pomalidomide SPC
• if you are pregnant or think you may be pregnant or are planning to become pregnant – this is because Pomalidomide SPC is expected to be harmful to an unborn child. (Men and women taking this medicine must read the section “Pregnancy, contraception and breast- feeding –information for women and men” below).
• if you are able to become pregnant, unless you follow all the necessary measures to prevent you from becoming pregnant (see “Pregnancy, contraception and breast-feeding – information for women and men”). If you are able to become pregnant, your doctor will record with each prescription that the necessary measures have been taken and will provide you with this confirmation.
• if you are allergic to Pomalidomide SPC or any of the other ingredients of this medicine (listed in section 6). If you think you may be allergic, ask your doctor for advice.
If you are uncertain whether any of the conditions above apply to you, talk to your doctor, pharmacist or nurse before taking Pomalidomide SPC.
Warnings and precautions
Talk to your doctor, pharmacist or nurse before taking Pomalidomide SPC if:
• you have ever had blood clots in the past. During the treatment with Pomalidomide SPC you have an increased risk of getting blood clots in your veins and arteries. Your doctor may
recommend you take additional treatments (e.g. warfarin) or lower the dose of
Pomalidomide SPC to reduce the chance that you get blood clots.
• you have ever had an allergic reaction such as rash, itching, swelling, feeling dizzy or trouble breathing while taking related medicines called ‘thalidomide’ or ‘lenalidomide’.
• you have had a heart attack, have heart failure, have difficulty breathing, or if you smoke, have high blood pressure or high cholesterol levels.
• you have a high total amount of tumour throughout the body, including your bone marrow. This could lead to a condition where the tumours break down and cause unusual levels of chemicals in the blood which can lead to kidney failure. You may also experience an uneven heartbeat. This condition is called tumour lysis syndrome.
• you have or have had neuropathy (nerve damage causing tingling or pain in your hands or feet).
• you have or have ever had hepatitis B infection. Treatment with Pomalidomide SPC may cause the hepatitis B virus to become active again in patients who carry the virus, resulting in a recurrence of the infection. Your doctor should check whether you have ever had hepatitis B infection.
• you experience or have experienced in the past a combination of any of the following symptoms:
• rash on face or extended rash, red skin, high fever, flu-like symptoms, enlarged lymph nodes (signs of severe skin reaction called Drug Reaction with Eosinophilia and Systemic Symptoms (DRESS) or drug hypersensitivity syndrome, Toxic Epidermal Necrolysis (TEN) or Stevens-Johnson Syndrome (SJS). See also section 4 “Possible side effects”).
It is important to note that patients with multiple myeloma treated with Pomalidomide SPC may develop additional types of cancer, therefore your doctor should carefully evaluate the benefit and risk when you are prescribed this medicine.
At the end of the treatment you should return all unused capsules to the pharmacist.
Pregnancy, contraception and breast-feeding – information for women and men
The following must be followed as stated in the Pomalidomide SPC Pregnancy Prevention Programme.
Women and men taking Pomalidomide SPC must not become pregnant or father a child. This is because Pomalidomide SPC is expected to harm the unborn baby. You and your partner should use effective methods of contraception while taking this medicine.
Women
Do not take Pomalidomide SPC if you are pregnant, think you may be pregnant or are planning to become pregnant.
This is because this medicine is expected to harm the unborn baby. Before starting the treatment, you should tell your doctor if you are able to become pregnant, even if you think this is unlikely.
If you are able to become pregnant:
• you must use effective methods of contraception for at least 4 weeks before starting treatment, for the whole time you are taking treatment, and until at least 4 weeks after stopping treatment. Talk to your doctor about the best method of contraception for you.
• each time your doctor writes a prescription for you, he will ensure you understand the necessary measures that have to be taken to prevent pregnancy.
• your doctor will arrange pregnancy tests before treatment, at least every 4 weeks during treatment, and at least 4 weeks after the treatment has finished.
If you become pregnant despite the prevention measures:
• you must stop the treatment immediately and talk to your doctor straight away.
Breast-feeding
It is not known if Pomalidomide SPC passes into human breast milk. Tell your doctor if you are breast- feeding or intend to breast-feed. Your doctor will advise if you should stop or continue breast- feeding.
Men
Pomalidomide SPC passes into human semen.
• If your partner is pregnant or able to become pregnant, you must use condoms for the whole time you are taking treatment and for 7 days after the end of treatment.
• If your partner becomes pregnant while you are taking Pomalidomide SPC, tell your doctor straight away. Your partner should also tell her doctor straight away.
You should not donate semen or sperm during treatment and for 7 days after the end of treatment.
Blood donation and blood tests
You should not donate blood during treatment and for 7 days after the end of treatment.
Before and during the treatment with Pomalidomide SPC you will have regular blood tests. This is because your medicine may cause a fall in the number of blood cells that help fight infection (white cells) and in the number of cells that help to stop bleeding (platelets).
Your doctor should ask you to have a blood test:
• before treatment
• every week for the first 8 weeks of treatment
• at least every month after that for as long as you are taking Pomalidomide SPC.
As a result of these tests, your doctor may change your dose of Pomalidomide SPC or stop
your treatment. The doctor may also change the dose or stop the medicine because of your general health.
Children and adolescents
Pomalidomide SPC is not recommended for use in children and young people under 18 years.
Other medicines and Pomalidomide SPC
Tell your doctor, pharmacist or nurse if you are taking, have recently taken or might take any other medicines. This is because Pomalidomide SPC can affect the way some other medicines work. Also some other medicines can affect the way Pomalidomide SPC works.
In particular, tell your doctor, pharmacist or nurse before taking Pomalidomide SPC if you are taking any of the following medicines:
• some antifungals such as ketaconazole
• some antibiotics (for example ciprofloxacin, enoxacin)
• certain antidepressants such as fluvoxamine.
Driving and using machines
Some people feel tired, dizzy, faint, confused or less alert when taking Pomalidomide SPC. If this happens to you, do not drive or operate tools or machinery.
Pomalidomide SPC contains sodium
This medicine contains less than 1 mmol sodium (23 mg) per capsule, therefore it is considered essentially ‘sodium-free’.
Pomalidomide must be given to you by a doctor with experience in treating multiple myeloma.
Always take your medicines exactly as your doctor has told you. Check with your doctor, pharmacist or nurse if you are not sure.
When to take Pomalidomide SPC with other medicines
Pomalidomide SPC with bortezomib and dexamethasone
• See the leaflets that come with bortezomib and dexamethasone for further information on their use and effects.
• Pomalidomide SPC, bortezomib and dexamethasone are taken in ‘treatment cycles’. Each cycle lasts 21 days (3 weeks).
• Look at the chart below to see what to take on each day of the 3-week cycle:
o Each day, look down the chart and find the correct day to see which medicines to take.
o Some days, you take all 3 medicines, some days just 2 or 1 medicines, and some days none at all.
POM: Pomalidomide SPC; BOR: Bortezomib; DEX: Dexamethasone
· After completing each 3-week cycle, start a new one.
Pomalidomide SPC with dexamethasone only
• See the leaflet that comes with dexamethasone for further information on its use and effects.
• Pomalidomide SPC and dexamethasone are taken in ‘treatment cycles’. Each cycle lasts 28 days (4 weeks).
• Look at the chart below to see what to take on each day of the 4-week cycle:
o Each day, look down the chart and find the correct day to see which medicines to take.
o Some days, you take both medicines, some days just 1 medicine, and some days none at all.
POM: Pomalidomide SPC; DEX: Dexamethasone
• After completing each 4-week cycle, start a new one.
How much Pomalidomide SPC to take with other medicines Pomalidomide with bortezomib and
• The recommended starting dose of Pomalidomide SPC is 4 mg per day.
dexa•mTehthearseocnoemmended starting dose of bortezomib will be worked out by your doctor and based on your height and weight (1.3 mg/m2 body surface area).
• The recommended starting dose of dexamethasone is 20 mg per day. However, if you are over 75, the recommended starting dose is 10 mg per day.
Pomalidomide SPC with dexamethasone only
• The recommended dose of Pomalidomide SPC is 4 mg per day.
• The recommended starting dose of dexamethasone is 40 mg per day. However, if you are over 75, the recommended starting dose is 20 mg per day.
Your doctor may need to reduce the dose of Pomalidomide SPC, bortezomib or dexamethasone or stop one or more of these medicines based on the results of your blood tests, your general condition, other medicines you may be taking (e.g. ciprofloxacin, enoxacin and fluvoxamine) and if you experience side effects (especially rash or swelling) from treatment.
If you suffer from liver or kidney problems your doctor will check your condition very carefully whilst you are receiving this medicine.
How to take Pomalidomide SPC
• Do not break, open or chew the capsules. If powder from a broken Pomalidomide SPC capsule makes contact with the skin, wash the skin immediately and thoroughly with soap and water.
• Swallow the capsules whole, preferably with water.
• You can take the capsules either with or without food.
• Take Pomalidomide SPC at about the same time each day.
To remove the capsule from the blister, press only one end of the capsule out to push it through
the foil.
Do not apply pressure on the centre of the capsule as this can cause it to break.
Your doctor will advise you of how and when to take Pomalidomide SPC if you have kidney problems and are receiving dialysis treatment.
Duration of the treatment with Pomalidomide SPC
You should continue the cycles of treatment until your doctor tells you to stop.
If you take more Pomalidomide SPC than you should
If you take more Pomalidomide SPC than you should, talk to a doctor or go to a hospital straight away. Take the medicine pack with you.
If you forget to take Pomalidomide SPC
If you forget to take Pomalidomide SPC on a day when you should, take your next capsule as normal the next day. Do not increase the number of capsules you take to make up for not taking Pomalidomide SPC the previous day.
If you have any further questions on the use of this medicine, ask your doctor or pharmacist.
Like all medicines, this medicine can cause side effects, although not everybody gets them.
Serious side effects
• Stop taking Pomalidomide SPC and see a doctor straight away if you notice any of the following serious side effects – you may need urgent medical treatment:
Fever, chills, sore throat, cough, mouth ulcers or any other signs of infection (due to less white blood cells, which fight infection).
• Bleeding or bruising without a cause, including nosebleeds and bleeding from the bowels or stomach (due to effects on blood cells called ‘platelets’).
• Rapid breathing, rapid pulse, fever and chills, passing very little to no urine, nausea and vomiting, confusion, unconsciousness (due to infection of blood called sepsis or septic shock).
• Severe, persistent or bloody diarrhoea (possibly with stomach pain or fever) caused by bacteria called Clostridium difficile.
• Chest pain, or leg pain and swelling, especially in your lower leg or calves (caused by blood clots).
• Shortness of breath (from serious chest infection, inflammation of the lung, heart failure or
blood clot).
• Swelling of face, lips, tongue and throat, which may cause difficulty breathing (due to a serious type of allergic reaction called angioedema).
• Certain types of skin cancer (squamous cell carcinoma and basal cell carcinoma), which can cause changes in the appearance of your skin or growths on your skin. If you notice any changes to your skin whilst taking Pomalidomide SPC, tell your doctor as soon as possible.
• Recurrence of hepatitis B infection, which can cause yellowing of the skin and eyes, dark brown coloured urine, right-sided abdominal pain, fever and feeling nauseous or being sick. Tell your doctor straightaway if you notice any of these symptoms.
•
Stop taking Pomalidomide SPC and see a doctor straight away if you notice any of the serious side effects listed above – you may need urgent medical treatment.
Other side effects
Very common (may affect more than 1 in 10 people):
• Shortness of breath (dyspnoea).
• Infections of the lungs (pneumonia and bronchitis).
• Infections of the nose, sinuses and throat, caused by bacteria or viruses.
• Low red blood cells, which may cause anaemia leading to tiredness and weakness.
• Low blood levels of potassium (hypokalaemia), which may cause weakness, muscle cramps, muscle aches, palpitations, tingling or numbness, dyspnoea, mood changes.
• High blood levels of sugar.
• Loss of appetite.
• Constipation, diarrhoea or nausea.
• Being sick (vomiting).
• Lack of energy.
• Difficulty in falling asleep or staying asleep.
• Dizziness, tremor.
• Muscle spasm, muscle weakness.
• Bone pain, back pain.
• Numbness, tingling or burning sensation to the skin, pains in hands or feet (peripheral sensory neuropathy).
• Swelling of the body, including swelling of the arms or legs.
Common (may affect up to 1 in 10 people):
• Fall.
• Bleeding within the skull.
• Decreased ability to move or feel (sensation) in your hands, arms, feet and legs because of nerve damage (peripheral sensorimotor neuropathy).
• Numbness, itching, and a feeling of pins and needles on your skin (paraesthesia).
• A spinning feeling in your head, making it difficult to stand up and move normally.
• Swelling caused by fluid.
• Hives (urticaria).
• Rashes.
• Itchy skin.
• Shingles.
• A fast and irregular heartbeat (atrial fibrillation).
• Heart attack (chest pain spreading to the arms, neck, jaw, feeling sweaty and breathless, feeling sick or vomiting).
• Chest pain, chest infection.
• Increased blood pressure.
• A fall in the number of red and white blood cells and platelets at the same time (pancytopenia), which will make you more prone to bleeding and bruising. You may feel
tired and weak, and short of breath and you are also more likely to get infections.
• Decreased number of lymphocytes (one type of white blood cells) often caused by infection (lymphopenia).
• Low blood levels of magnesium (hypomagnesaemia), which may cause tiredness, generalised weakness, muscle cramps, irritability and may result in low blood levels of calcium (hypocalcaemia), which may cause numbness and, or tingling of hands, feet, or lips, muscle cramps, muscle weakness, light-headedness, confusion.
• Low blood level of phosphate (hypophosphataemia), which may cause muscle weakness and irritability or confusion.
• High blood level of calcium (hypercalcaemia), which may cause slowing reflexes and skeletal muscle weaknesses.
• High blood levels of potassium, which may cause abnormal heart rhythm.
• Low blood levels of sodium, which may cause tiredness and confusion, muscle twitching, fits (epileptic seizures) or coma.
• High blood levels of uric acid, which may cause a form of arthritis called gout.
• Low blood pressure, which may cause dizziness or fainting.
• Flu-like symptoms (influenza).
• Sore or dry mouth.
• Changes in the way things taste.
• Abdominal pain, swollen abdomen.
• Feeling confused.
• Feeling down (depressed mood).
• Loss of consciousness, fainting.
• Clouding of your eye (cataract).
• Damage to the kidney.
• Inability to pass urine.
• Abnormal liver test.
• Urinary tract infection, which may cause a burning sensation when passing urine, or a need to pass urine more often.
• Pain in the pelvis.
• Weight loss.
Uncommon (may affect up to 1 in 100 people):
• Stroke.
• Inflammation of the liver (hepatitis) which can cause itchy skin, yellowing of the skin and the whites of the eyes (jaundice), pale coloured stools, dark coloured urine and abdominal pain.
• The breakdown of cancer cells resulting in the release of toxic compounds into the bloodstream (tumour lysis syndrome). This can result in kidney problems.
Not known (frequency cannot be estimated from the available data):
• Widespread rash, high body temperature, enlarged lymph nodes and other body organs involvement (Drug Reaction with Eosinophilia and Systemic Symptoms which is also known as DRESS or drug hypersensitivity syndrome, Toxic Epidermal Necrolysis or Stevens-Johnson Syndrome). Stop using pomalidomide if you develop these symptoms and contact your doctor or seek medical attention immediately.
Reporting of side effects
• Reporting of side effects If you get any side effects, talk to your doctor or pharmacist. This includes any possible side effects not listed in this leaflet. You can also report side effects directly via submitting completed forms to: npc.drug@sfda.gov.sa. By reporting side effects you can help provide more information on the safety of this medicine.
Do not Store above 30°C.
Capsules are packaged in blisters and bottle.
MARKETING AUTHORIZATION HOLDER:
Sudair Pharma Company (SPC)
King Fahad road, Building 911- The First Round Riyadh, Saudi Arabia
Tel: +966-11-920001432
Fax: +966-11-4622230
Email: info@sudairpharma.com
Mailing: P.O. Box 19047 Riyadh, Saudi Arabia
Manufacturer:
Dr. Reddy’s Laboratories Ltd. Formulation Unit VII Plot No. P1 to P9, Phase III,
Duvvada, VSEZ, Visakhapatnam, Andhra Pradesh, INDIA - 530 046
يرتبط بوماليدوميد اس بي سي بـمادة ثاليدومايد وينتمي إلى مجموعة من الأدوية التي تؤثر على الجهاز المناعي (جهاز المناعة الطبيعي الذي يحمي الجسم من الأمراض).
ما هي دواعي استعمال بوماليدوميد اس بي سي؟
يستخدم بوماليدوميد اس بي سي لعلاج المرضى من البالغين الذين يعانون من نوع من السرطان يسمى "الورم النقوي المتعدد".
كما يمكن استخدام بوماليدوميد اس بي سي بمصاحبة أدوية أخرى:
· مع نوعين آخرين من الدواء، يعرفوا باسم "بورتيزوميب" (أحد أنواع أدوية العلاج الكيميائي) و"ديكساميثازون" (دواء مضاد للالتهابات) في المرضى الذين قد تلقوا علاجًا واحدًا آخر على الأقل - بما في ذلك ليناليدومايد.
أو
· مع دواء آخر – يُعرف باسم "ديكساميثازون" في المرضى الذين يعانون من تفاقم مرض الورم النقوي المتعدد على الرغم من تلقي نوعين آخرين على الأقل من الأدوية - بما في ذلك ليناليدومايد. وبورتيزوميب.
ما هو مرض الورم النقوي المتعدد؟
الورم النقوي المتعدد هو نوع من أنواع السرطانات الذي يصيب نوع معين من خلايا الدم البيضاء (تسمى خلايا البلازما). تتزايد هذه الخلايا بطريقة لا يمكن إيقافها وتتراكم في نخاع العظام. وقد يُؤدي ذلك إلى تلف العظام والكُلى.
لا يمكن الشفاء بصورة كاملة من الورم النقوي المتعدد. ومع ذلك، يمكن أن يقلل العلاج من علامات وأعراض المرض أو يقلل ظهورها لفترة من الوقت. عندما يحدث ذلك، فإنه يسمى"الاستجابة".
كيفية عمل بوماليدوميد اس بي سي؟
يعمل بوماليدوميد اس بي سي بعدة طرق مختلفة:
· عن طريق منع تكوُّن خلايا الوَرَمِ النِّقَوِي.
· عن طريق تحفيز الجهاز المناعي لمهاجمة الخلايا السرطانية.
· عن طريق إيقاف تكوين الأوعية الدموية التي تغذي الخلايا السرطانية.
فائدة استخدام بوماليدوميد اس بي سي مع أدوية بورتيزوميب وديكساميثازون
يمكن أن يؤدي تناول بوماليدوميد اس بي سي بالتزامن مع استخدام بورتيزوميب وديكساميثازون في المرضى الذين قد خضعوا لتلقي علاجًا واحدًا على الأقل إلى توقف تفاقم الورم النقوي المتعدد:
· في المتوسط، يؤدي الاستخدام المتزامن لكل من بوماليدوميد اس بي سي مع بورتيزوميب وديكساميثازون إلى منع رجوع الإصابة بالورم النقوي المتعدد مرة أخرى لمدة تصل إلى 11 شهر - مقارنة بمدة تصل إلى 7 أشهر بالنسبة لأولئك المرضى الذين يتلقوا العلاج فقط باستخدام بورتيزوميب وديكساميثازون.
فائدة تناول بوماليدوميد اس بي سي مع ديكساميثازون
يمكن أن يؤدي تناول بوماليدوميد اس بي سي بالتزامن مع ديكساميثازون، في المرضى الذين قد خضعوا مسبقًا لتلقي نوعين أخرين من الأدوية على الأقل، إلى توقف تفاقم الورم النقوي المتعدد:
· في المتوسط، يؤدي تناول بوماليدوميد اس بي سي بالتزامن مع ديكساميثازون إلى منع رجوع الإصابة بالورم النقوي المتعدد مرة أخرى لمدة تصل إلى 4 أشهر مقارنة بمدة تصل إلى شهرين بالنسبة لأولئك المرضى الذين يتلقوا العلاج فقط باستخدام ديكساميثازون.
يحظر تناول بوماليدوميد اس بي سي في الحالات التالية:
· إذا كنتِ حاملًا أو تعتقدين أنكِ قد تكوني حاملًا أو تخططين للحمل، فمن المتوقع أن يضر بوماليدوميد اس بي سي بالجنين. (يجب على المرضى من الرجال والسيدات الذين يتناولون هذا الدواء قراءة قسم "الحمل، وموانع الحمل والرضاعة الطبيعية، معلومات هامة للمرضى من السيدات والرجال") المذكور أدناه).
إذا كنتِ سيدة قادرة على الحمل، إلا إذا اتبعتِ كافة الوسائل اللازمة لمنع الحمل، (انظري قسم "الحمل وموانع الحمل والرضاعة الطبيعية – ومعلومات للمرضى من السيدات والرجال" الوارد أدناه). إذا كنتِ سيدة قادرة على الحمل، فسيسجل الطبيب المعالج لك مع كل وصفة طبية أنه قد قام باتخاذ الإجراءات اللازمة وسيؤكد لكِ ذلك.
· إذا كنت تعاني من حساسية تجاه بوماليدوميد اس بي سي أو أي مكون من المكونات الأخرى الداخلة في تركيب هذا الدواء (المدرجة في القسم رقم 6). استشر الطبيب المعالج لك للحصول على النصيحة، إذا كنت تعتقد أنك قد تكون مصابًا بحساسية.
إذا لم تكن متأكدًا مما إذا كان أيٌّ مما سبق ينطبق عليك أم لا، فيُرجى التَّحدُّث إلى الطبيب المعالج لك أو الصيدلي الخاص بك أو الممرض(ة) المتابعة(ة) لحالتك قبل تناوُل بوماليدوميد اس بي سي.
تحذيرات واحتياطات
تحدث إلى الطبيب المعالج لك أو الصيدلي الخاص بك أو الممرض(ة) المتابع (ة) لحالتك لك قبل تناوُل بوماليدوميد اس بي سي، في الحالات التالية:
· إذا كنت قد عانيت مسبقًا من جلطات دموية بالأوردة. ستكون أكثر عرضة للإصابة بجلطات دموية بالأوردة والشرايين أثناء فترة العلاج بوماليدوميد اس بي سي، قد يوصي الطبيب المعالج لك باستخدام أدوية أخرى (مثل وارفارين) أو خفض جرعة بوماليدوميد اس بي سي للحد من معدلات الإصابة بالجلطات الدموية.
· إذا كنت قد عانيت مسبقًا من تفاعلات الحساسية مثل طفح جلدي أو حكة أو تورم أو شعور بدوار أو صعوبة بالتنفس أثناء تناول الأدوية المماثلة المعروفة باسم "ثاليدومايد" أو "لينالدومايد".
· إذا كنت تعاني من أزمة قلبية أو قصور بالقلب أو صعوبة بالتنفس أو إذا كنت مدخنًا أو تعاني من ارتفاع ضغط الدم أو ارتفاع مستويات الكوليسترول في الدم.
· إذا كنت تعاني من ارتفاع الحجم الكلي للأورام في كافة أنحاء الجسم بما في ذلك نخاع العظام.
قد يؤدي ذلك إلى تفتت الأورام مسببًا اضطرابات في مستويات المواد الكيميائية في الدم والذي يمكن أن يؤدي إلى الفشل الكلوي. فقد تعاني أيضًا من اضطرابات في نظم القلب (ضربات القلب) وتسمى هذه الحالة بمتلازمة تحلل الورم.
· إذا كنت تعاني أو قد عانيت مسبقًا من الاعتلال العصبي (وخز أو ألم في اليدين أو القدمين ناتج عن تلف الأعصاب).
· إذا كنت تعاني أو قد عانيت مسبقًا من التهاب الكبد الوبائي بي. قد يؤدي العلاج باستخدام بوماليدوميد اس بي سي إلى تنشيط فيروس الكبد الوبائي بي مرة أخرى في المرضى الحاملين لفيروس بي، مما يؤدى إلى تكرر الإصابة بالعدوى. يجب على الطبيب المعالج لك التأكد مما إذا كنت قد أصبت بعدوى التهاب الكبد الوبائي بي من قبل أم لا.
· إذا كنت تعاني أو قد عانيت مسبقًا من بعض الأعراض التالية:
o طفح جلدي على الوجه أو طفح جلدي منتشر في الجسم، احمرار الجلد، حمى مصحوبة بارتفاع شديد في درجة الحرارة، أعراض تشبه عدوى الأنفلونزا، تضخم العقد الليمفاوية (علامات تفاعلات جلدية حاد تعرف باسم تفاعلات دوائية مع كَثْرَةُ اليُوزينِيَّات والأعراض الجهازية (DRESS) أو متلازمة فرط الحساسية الدوائية أو تَقَشُّرُ الأَنْسِجَةِ المُتَمَوِّتَةِ البَشْرَوِيَّةِ التَّسَمُّمِيّ (TEN) أو متلازمة ستيفنز جونسون (SJS)، انظر أيضًا القسم رقم 4 "الآثار الجانبية المُحتمَلة").
من المهم معرفة أن المرضى الذين يعانون من الورم النقوي المتعدد ويتم علاجهم باستخدام بوماليدوميد اس بي سي قد يصابون بأنواع أخرى من السرطان، لذلك يجب على الطبيب المعالج لك تقييم الفوائد المتوقعة والمخاطر المحتملة عند وصف هذا الدواء لك.
يجب إعادة جميع الكبسولات غير المستخدمة في نهاية فترة العلاج إلى الصيدلي الخاص بك.
الحمل وموانع الحمل والرضاعة الطبيعية – ومعلومات للمرضى من السيدات والرجال
يجب اتباع التالي كما هو مذكور في برنامج منع الحمل أثناء العلاج بوماليدوميد اس بي سي.
يحظر على المرضى من السيدات والرجال الذين يتم علاجهم بوماليدوميد اس بي سي الإنجاب أثناء تناول هذا الدواء. حيث أنه من المتوقع أن يضر بوماليدوميد اس بي سي بالجنين. لذلك ينبغي أن تستخدم أنت وزوجتك وسائل فعالة لمنع الحمل أثناء تناول هذا الدواء.
بالنسبة للمرضي من السيدات
يحظر تناول بوماليدوميد اس بي سي، إذا كنت حاملًا أو تعتقدين أنك حاملًا أو تخططين للحمل، حيث أنه من المتوقع أن يضر هذا الدواء بالجنين. يجب إبلاغ الطبيب المعالج لك قبل بدأ فترة العلاج بهذا الدواء، إذا كنت قادرة على الحمل حتى لو كنت تعتقدين أن ذلك مستبعد.
إذا كنتِ قادرة على الحمل يتعين عليك القيام بما يلي:
· يجب استخدام وسائل فعالة لمنع الحمل لمدة 4 أسابيع قبل بدء العلاج وأثناء الفترة الكلية لتلقي العلاج ولمدة تصل إلى 4 أسابيع على الأقل بعد التوقف عن تناول العلاج. تحدثي مع الطبيب المعالج لكِ حول أفضل وسيلة مناسبة لكِ لمنع الحمل.
· سيقوم الطبيب المعالج لك بالتأكد من معرفتك بالإجراءات الضرورية التي يجب اتخاذها لمنع الحمل في كل مرة قبل كتابة أي وصفة طبية لك.
· سيقوم الطبيب المعالج لكِ بإجراء اختبارات الحمل قبل بدء العلاج وعلى الأقل كل 4 أسابيع خلال العلاج وكل 4 أسابيع بعد التوقف عن تناول العلاج)
إذا أصبحت حاملاً بالرغم من استخدام وسائل لمنع الحمل:
· يجب إيقاف العلاج فورًا والتحدَّث مع الطبيب المعالج لك على الفور.
الرضاعة الطبيعية
من غير المعروف ما إذا كان بوماليدوميد اس بي سي يفرز في لبن الأم أم لا. أخبري الطبيب المعالج لكِ إذا كنتِ تُمارسين الرضاعة الطبيعة أو تنوين ممارسة الرضاعة الطبيعية. سينصحك الطبيب المعالج لك بضرورة التوقف عن ممارسة الرضاعة الطبيعية أو الاستمرار فيها.
بالنسبة للمرضى من الرجال:
يفرز ليناليدوميد في السائل المنوي البشري.
· ينبغي استخدام الواقي الذكري طوال الوقت الذي تتناول فيه العلاج ولمدة تصل إلى 7 أيام بعد انتهاء فترة العلاج إذا كانت زوجتك حاملًا أو قادرة على الإنجاب.
· ينبغي أخبار الطبيب المعالج لك فورًا إذا أصبحت زوجتك حاملًا خلال فترة العلاج باستخدام بوماليدوميد اس بي سي. كما يجب أن تبلغ زوجتك فورًا الطبيب المعالج لها بذلك.
يجب عدم التبرع بالسائل المنوي أو الحيوانات المنوية أثناء العلاج ولمدة تصل إلى 7 أيام بعد انتهاء فترة العلاج.
التبرع بالدم واختبارات الدم
يحظر التبرع بالدم أثناء العلاج ولمدة تصل إلى 7 أيام بعد انتهاء فترة العلاج.
ستخضع لاختبارات دم بانتظام قبل وأثناء العلاج باستخدام بوماليدوميد اس بي سي. حيث أن هذا الدواء الخاص بك قد يسبب انخفاضًا في عدد خلايا الدم التي تساعد في مقاومة العدوى (كرات الدم البيضاء) وفي عدد الخلايا التي تساعد على وقف النزيف (الصفائح الدموية).
سيطلب منك الطبيب المعالج لك إجراء اختبارات للدم في الأوقات التالية:
· قبل بدء العلاج.
· كل أسبوع لمدة الأسابيع الثماني الأولى من بدء العلاج.
· كل شهر على الأقل وبعد ذلك طوال فترة تناولك بوماليدوميد اس بي سي.
قد يقوم الطبيب المعالج لك بتغيير جرعة بوماليدوميد اس بي سي أو بإيقاف العلاج كنتيجة لهذه الاختبارات.
كما قد يقوم الطبيب المعالج لك أيضًا بتغيير الجرعة أو إيقاف الدواء حفاظًا على حالتك الصحية العامة.
الاستخدام في المرضى من الأطفال والمراهقين
لا ينصح باستخدام بوماليدوميد اس بي سي للمرضى من للأطفال والمراهقين الذين تقل أعمارهم عن 18 سنة.
استخدام أدوية أخرى مع بوماليدوميد اس بي سي
أخبر الطبيب المعالج لك أو الصيدلي الخاص بك أو الممرض(ة) المتابع(ة) لحالتك إذا كنت تتناول أو قد تناولت مؤخرًا أو قد تتناول أية أدوية أخرى. حيث يؤثر بوماليدوميد اس بي سي على آلية عمل بعض الأدوية الأخرى. وبالمثل، فقد تُؤثر بعض الأدوية الأخرى على آلية عمل بوماليدوميد اس بي سي.
وعلى وجه الخصوص، أخبر الطبيب المعالج لك أو الصيدلي الخاص بك أو الممرض(ة) المتابع(ة) لحالتك قبل تناول بوماليدوميد اس بي سي إذا كنت تتناول أي من الأدوية التالية:
· بعض مضادات الفطريات مثل كيتوكونازول.
· بعض المضادات الحيوية (مثل سيبروفلوكساسين، اينوكساسين).
· بعض مضادات الاكتئاب مثل فلوفوكسامين.
القيادة واستخدام الآلات
قد يشعر بعض المرضى بتعب أو دوار أو إغماء أو ارتباك أو عدم تركيز عند تناول بوماليدوميد اس بي سي. ينبغي عدم قيادة السيارات أو استخدام أية أدوات أو آلات، إذا شعرت بذلك.
يحتوي بوماليدوميد اس بي سي على الصوديوم
يحتوي هذا الدواء على أقل من 1 مللي مول (23 مجم) من الصوديوم في كل كبسولة، مما يعني أن هذا "خال من الصوديوم" بشكل أساسي.
يجب إعطائك بوماليدوميد اس بي سي تحت إشراف طبيب ذو خبرة في علاج الورم النقوي المتعدد.
تناوَل دائمًا هذا الدَّواء تمامًا كما أخبرك الطبيب المعالج لك. يُرجى مراجعة الطبيب المعالج لكِ أو الصيدلي الخاص بكِ أو الممرض(ة) المتابع(ة) لحالتك إذا لم تكن متأكدًا من كيفية التَّناوُل.
متى يمكن تناول بوماليدوميد اس بي سي مع أدوية أخرى
تناول بوماليدوميد اس بي سي مع بورتيزوميب وديكساميثازون
· انظر النشرة الدوائية التي تأتي مع بورتيزوميب وديكساميثازون لمعرفة المزيد من المعلومات عن استخدامه وآثاره.
· يُعطى بوماليدوميد اس بي سي وبورتيزوميب وديكساميثازون على شكل دورات علاجية. حيث تستمر كل دورة علاجية لمدة 21 يومًا (3 أسابيع).
· انظر الجدول التخطيطي الوارد أدناه لمعرفة ما يجب تناوله في كل يوم من أيام الدورة العلاجية التي تستمر لمدة ثلاثة أسابيع:
o انظر كل يوم إلى الجدول التخطيطي وابحث عن اليوم الصحيح لمعرفة الأدوية التي يجب تناولها فيه.
o قد تناول الأدوية الثلاثة جميعها في بعض الأيام أو دواءين منها أو دواءً واحدًا فقط في بعض الأيام أو قد لا تتناول أي منهم في بعض الأيام الأخرى.
POM يعني: بوماليدوميد اس بي سي BOR يعني: بورتيزوميب DEX يعني: ديكساميثازون
أ) بعد الانتهاء من كل دورة علاجية تستمر لمدة 3 أسابيع، ابدأ واحدة جديدة.
بوماليدوميد اس بي سي مع ديكساميثازون فقط
· انظر النشرة الدوائية التي تأتي مع ديكساميثازون لمعرفة المزيد من المعلومات عن استخدامه وفعاليته.
· يُعطى بوماليدوميد اس بي سي وديكساميثازون على شكل دورات علاجية. تستمر كل دورة علاجية لمدة 28 يومًا (4 أسابيع).
· انظر الجدول التخطيطي أدناه لمعرفة ما يجب تناوله في كل يوم من أيام الدورة العلاجية التي تستمر لمدة 4 أسابيع:
o انظر كل يوم إلى ا الجدول التخطيطي وابحث عن اليوم الصحيح لمعرفة الأدوية التي يجب تناولها فيه.
o قد تناول دواءين في بعض الأيام أو دواءً واحدًا فقط في بعض الأيام الأخرى وقد لا تتناول أيًا منهما في بعض الأيام الأخرى.
POM يعني: بوماليدوميد اس بي سي DEX يعني: ديكساميثازون
· بعد الانتهاء من كل دورة علاجية مدتها 4 أسابيع، ابدأ دورة علاجية جديدة.
ما هي الجرعة التي ينبغي تناوُلها من بوماليدوميد اس بي سي مع الأدوية الأخرى
تناول بوماليدوميد اس بي سي مع بورتيزوميب وديكساميثازون
· جرعة البدء الموصي بها من بوماليدوميد اس بي سي هي 4 مجم يوميًا.
· سيقوم الطبيب المعالج لك بتحديد جرعة البدء الموصى بها من بورتيزوميب بناءً على طولك ووزنك (مساحة سطح الجسم 1.3 مجم / م 2).
· جرعة البدء الموصي بها من ديكساميثازون هي 20 مجم يوميًا. ومع ذلك، إذا كان عمرك أكبر من 75 عامًا، فإن جرعة البدء الموصى بها تكون 10 مجم يوميًا
تناول بوماليدوميد اس بي سي مع ديكساميثازون فقط
· الجرعة الموصي بها من بوماليدوميد اس بي سي هي 4 مجم يوميًا.
· جرعة البدء الموصي بها من ديكساميثازون هي 40 مجم يوميًا. ومع ذلك، إذا كان عمرك أكبر من 75 عامًا، فإن جرعة البدء الموصى بها تكون 20 مجم يوميًا.
قد يحتاج الطبيب المعالج لك إلى تقليل جرعة بوماليدوميد اس بي سي أو بورتيزوميب أو ديكساميثازون أو إيقاف واحد أو أكثر من هذه الأدوية بناءً على نتائج فحوصات الدم وحالتك الصحية العامة والأدوية الأخرى التي تتناولها (مثل سيبروفلوكساسين ونيوكساسين وفلوفوكسامين) وإذا كنت تعاني من أية آثار جانبية (وخاصة طفح جلدي أو تورم) أثناء تناول العلاج.
سيتابع الطبيب المعالج لك حالتك الصحية بدقة شديدة، إذا كنت تعاني من مشاكل في الكبد أو الكلى أثناء تناول هذا الدواء.
كيفية تناول بوماليدوميد اس بي سي
· لا تكسر الكبسولة أو تفتحها أو تمضغها. إذا لمس مسحوق بوماليدوميد اس بي سي الخارج من كبسولة مفتوحة بشرتك، فاغسل الجلد فورًا وجيدًا بالماء والصابون.
· ابتلع الكبسولة بالكامل، يُفضَّل بلعها بكوب من الماء.
· يمكنك تناوُل الكبسولات مع الطعام أو بدونه.
· تناوُل بوماليدوميد اس بي سي في نفس الوقت تقريبًا كل يوم.
لإخراج الكبسولة من الشريط، اضغط على نهاية أحد أطراف الكبسولة فقط لإخراجه من الرقاقة التي تغلف الكبسولة.
لا تضغط على منتصف الكبسولة، لأن هذا يمكن أن يؤدي إلى فتحها.
سينصحك الطبيب المعالج لك بكيفية وموعد تناول بوماليدوميد اس بي سي، إذا كنت تعاني من مشاكل في الكلى وتخضع لغسيل الكلى.
مدة العلاج بوماليدوميد اس بي سي
يجب أن تستمر في اتباع الدورات العلاجية الخاصة بك حتى يخبرك الطبيب المعالج لك بإيقافها.
إذا تناولت كمية أكثر مما يجب من بوماليدوميد اس بي سي
تحدث مع الطبيب المعالج لك أو توجه إلى إحدى المستشفيات فورًا، إذا تناولت كمية أكثر مما يجب من بوماليدوميد اس بي سي. اصطحب معك عبوة الدواء.
إذا نسيت تناول بوماليدوميد اس بي سي
إذا نسيت تناول بوماليدوميد اس بي سي في اليوم المحدد لتناوله، فيجب أن تتناول الكبسولة التالية بشكل طبيعي في اليوم التالي. لا تُضاعف عدد الكبسولات التي تتناولها لتعويض جرعة أغفلتها في اليوم السابق من بوماليدوميد اس بي سي.
إذا كانت لديك أية أسئلة إضافية حول استخدام هذا الدواء، فاستشر طبيبك المعالج لك أو الصيدلي الخاص بك.
يمكن أن يُسبب هذا الدَّواء، مثله مثل كافة الأدوية، آثارًا جانبية على الرغم من عدم حدوثها لجميع المرضى.
آثار جانبية خطيرة
· إذا لاحظت أيًّا من الآثار الجانبية الخطيرة التَّالية؛ فتوقف عن تناوُل بوماليدوميد اس بي سي واذهب إلي الطبيب المعالج لك فورًا حيث قد تحتاج إلى علاج طبي عاجل:
o حمى أو قشعريرة أو التهاب الحلق أو سعال أو تقرحات الفم أو أي علامات أخرى للعدوى (بسبب انخفاض عدد خلايا الدم البيضاء التي تقاوم العدوى).
o نزيف أو كدمات بدون سبب، بما في ذلك نزيف من الأنف ونزيف من الأمعاء أو المعدة (نتيجة تأثير الدواء على خلايا الدم المعروفة باسم "الصفائح الدموية").
o سرعة بالتنفس، ارتفاع معدل نبضات القلب، حمى وقشعريرة، انخفاض في كمية البول أو انعدامه، غثيان وقيء وارتباك وإغماء (بسبب عدوى الدم المعروفة باسم تسمم الدم أو صدمة إنتانية (تعفن الدم).
o إسهال حاد أو مستمر أو مصحوب بدم (قد يصاحبه ألم في المعدة أو حمى) ناجم عن الإصابة بالبكتيريا المطثية العسيرة.
o ألم في الصدر أو ألم في الساق وتورم وعلى وجه الخصوص في أسفل الساق أو السمانة (بسبب جلطات الدم).
o ضيق بالتنفس (بسبب الإصابة بعدوى خطيرة في الصدر أو التهاب بالرئة أو قصور القلب أو تجلط الدم).
o تورم الوجه والشفتين واللسان والحلق مما قد يسبب صعوبة بالتنفس (نتيجة الإصابة بتفاعل حساسية خطير يسمى الوذمة الوعائية).
o أنواع معينة من سرطان الجلد (سرطان الخلايا الحرشفية وسرطان الخلايا القاعدية) مما يسبب تغيرات في مظهر البشرة أو نمو الجلد. إذا لاحظت أي تغييرات على البشرة أثناء تناول بوماليدوميد اس بي سي فأخبر الطبيب المعالج لك في أقرب وقت ممكن.
o تكرار الإصابة بالتهاب الكبد الوبائي "بي" مما يسبب اصفرار الجلد والعينين، تغير لون البول إلى اللون البني الداكن، ألم البطن من الجنب الأيمن، حمى، شعور بغثيان أو إعياء. أبلغ الطبيب المعالج لك فورًا إذا لاحظت أيًا من هذه الأعراض.
توقف عن تناوُل بوماليدوميد اس بي سي واذهب إلي الطبيب المعالج لك فورًا، إذا لاحظت أيًّا من الآثار الجانبية الخطيرة التَّالية المُدرجة أعلاه؛ فقد تحتاج إلى علاج طبي عاجل.
آثار جانبية أخرى
أثار جانبية شائعة جدًا (قد تُؤثر على أكثر من مريض واحد من بين كل 10 مرضى):
· ضيق التنفس (اختناق).
· عدوى بالرئة (الالتهاب الرئوي والتهاب الشعب الهوائية).
· عدوى بالأنف والجيوب الأنفية والحلق ناجمة عن الإصابة بالبكتيريا أو الفيروسات.
· انخفاض عدد خلايا الدَّم الحمراء الذي قد يسبب الإصابة بالأنيميا (فقر دم) مما يؤدى إلى الشعور بتعب وضعف
· انخفاض مستويات البوتاسيوم في الدم (نقص بوتاسيوم الدم) مما يسبب الشعور بضعف، تشنج بالعضلات، آلام بالعضلات، خفقان القلب، وخز أو تنميل، ضيق التنفس، تغيرات في الحالة المزاجية.
· ارتفاع مستوى السكر في الدم.
· فقدان الشهية.
· إمساك أو إسهال أو غثيان.
· شعور بإعياء (قيء).
· نقص الطاقة.
· صعوبة في النَّوم أو الاستمرار بالنوم.
· دوخة، رعشة.
· تشنج بالعضلات وهن بالعضلات.
· ألم بالعظم، ألم بالظهر.
· تنميل أو وخز أو حرقان في الجلد أو آلام في اليدين أو القدمين (الاعتلال العصبي الطرفي).
· تورم في الجسم بما في ذلك الذراعين أو الساقين.
آثار جانبية شائعة: (قد تُؤثر على ما يصل إلى مريض واحد من بين كل ١٠ مرضى):
· سقوط.
· نزيف في الجمجمة.
· انخفاض في القدرة على الحركة أو فقدان الشعور (الإحساس) في اليدين والذراعين والقدمين والساقين ناتج عن تلف الأعصاب (الاعتلال العصبي الحسي الحركي الطرفي).
· تنميل وحكة وشعور بوخز مثل وخز الدبابيس والإبر على الجلد (مذل).
· شعور بتنميل في الرأس مما يؤدي إلى شعور بصعوبة بالوقوف والحركة بشكل طبيعي.
· تورم ناتج عن السوائل.
· شرى (ارتكاريا).
· طفح جلدي.
· حكة بالجلد.
· هربس نطاقي (قوباء منطقية).
· عدم انتظام ضربات قلب وسرعة ضربات القلب (رجفان أذيني)،
· نوبة قلبية (ألم بالصدر ينتقل إلى الذراعين والرقبة والفك وزيادة التعرق وضيق التنفس شعور بإعياء أو قيء).
· ألم بالصدر، عدوى بالصدر.
· ارتفاع ضغط الدَّم.
· انخفاض عدد خلايا الدم الحمراء والبيضاء والصفائح الدموية في نفس الوقت (قلة في عدد الكريات) مما يجعلك أكثر عرضة للنزيف والكدمات.
· قد تشعر بالتعب والضعف وضيق التنفس مما يجعلك أكثر عرضة للإصابة بالعدوى.
· انخفاض عدد الخلايا اللمفاوية (أحد أنواع خلايا الدم البيضاء) غالبًا ما يكون ناتجًا عن الإصابة بعدوى (قلة اللمفاويات).
· انخفاض مستويات الماغنيسيوم في الدم (نقص ماغنيسيوم الدم) مما يسبب تعب وضعف عام وتشنج بالعضلات وسرعة الانفعال وقد يؤدي إلى انخفاض مستويات الكالسيوم في الدم (نقص كالسيوم الدم) الذي قد يؤدي إلى تنميل أو وخز في اليدين أو القدمين أو الشفاه وتشنج العضلات وضعف بالعضلات ودوار وارتباك.
· انخفاض مستوى الفوسفات في الدم (نقص فوسفات الدم) مما يؤدي إلى ضعف بالعضلات أو سرعة الانفعال أو ارتباك.
· ارتفاع مستوى الكالسيوم في الدم (فرط كالسيوم الدم) مما يؤدي إلى انخفاض في رد الفعل وضعف العضلات الهيكلية.
· ارتفاع مستويات البوتاسيوم في الدم مما يؤدي إلى عدم انتظام ضربات القلب.
· انخفاض مستويات الصوديوم في الدم مما يؤدي إلى تعب أو ارتباك أو رعشة بالعضلات أو نوبات تشنجية (نوبات الصرع) أو غيبوبة.
· ارتفاع مستويات حمض اليوريك في الدم مما يؤدي إلى الإصابة بأحد أنواع التهاب المفاصل مثل الإصابة بالنقرس.
· انخفاض ضغط الدم مما يؤدي إلى الشعور بالدوار أو الإغماء.
· أعراض شبيهة بأعراض الأنفلونزا (الأنفلونزا).
· قرحة أو جفاف الفم.
· تغييرات في طعم الأشياء.
· ألم في البطن، تورم بالبطن.
· شعور بارتباك.
· شعور بالإحباط (شعور بالاكتئاب).
· فقدان الوعي، إغماء.
· اعتام عدسة العين (كاتاراكت).
· تلف بالكلى.
· عدم القدرة على التبول.
· نتائج غير طبيعية في فحوصات الكبد.
· عدوى المسالك البولية والتي قد تسبب الشعور بحرقان عند التبول أو زيادة معدل التبول بشكل متكرر.
· ألم بالحوض.
· فقدان الوزن.
آثار جانبية غير شائعة (قد تُؤثر على ما يصل إلى مريض واحد من بين كل ١٠٠ مريض):
· سكتة دماغية.
· التهاب الكبد (التهاب الكبد الوبائي) الذي يمكن أن يسبب حكة بالجلد واصفرار الجلد واصفرار الجزء الأبيض بداخل العين (يرقان) تغير لون البراز إلى اللون الباهت وتغير لون البول إلى اللون الداكن وألم بالبطن.
· تفتت الخلايا السرطانية مما يؤدي إلى خروج جزئيات سامة إلى مجرى الدم (متلازمة تحلل الورم). وقد يُؤدي ذلك إلى اضطرابات بالكلى.
آثار جانبية غير معروف معدل تكرارها (لا يمكن تقدير معدل التّكرار من واقع البيانات المتاحة):
· طفح جلدي منتشر بالجسم أو ارتفاع درجة حرارة الجسم أو تضخم الغدد الليمفاوية أو أضرار بأعضاء الجسم الأخرى (تفاعلات دوائية مع كَثْرَةُ اليُوزينِيَّات وأعراض جهازية تعرف باسم متلازمة (DRESS) أو متلازمة فرط التحسس الدوائي أو تَقَشُّرُ الأَنْسِجَةِ المُتَمَوِّتَةِ البَشْرَوِيَّةِ التَّسَمُّمِيّ (TEN) أو متلازمة ستيفنز جونسون (SJS). قم بإيقاف بوماليدوميد اس بي سي، إذا عانيت من أي من هذه الأعراض واتصل بالطبيب المعالج لك أو احصل على عناية طبية فورًا.
الإبلاغ عن الآثار الجانبية
· تحدَّث إلى الطبيب المعالج لك أو الصيدلي الخاص بكِ، إذا عانيت من أية آثار جانبية. ويشمل هذا أية آثار جانبية مُحتمَلة غير مُدرجة ﻓﻲ ﻫﺫﻩ النشرة، يمكنك أيضًا الإبلاغ عن الآثار الجانبية بشكل مباشر عن طريق إرسال نماذج كاملة إلى البريد الإلكتروني التالي: npc.drug@sfda.gov.sa، يمكنك المساعدة في تقديم معلومات إضافية حول أمان استخدام هذا الدواء من خلال إبلاغك عن الآثار الجانبية.
لا یتم تخزینه في درجة حرارة اعلى من 30 درجة مئوية.
يتم تعبئة وتغليف الكبسولات في شرائط وعبوة.
NA
مالك التصريح بالتسويق:
شركة سدير فارما (SPC)
طريق الملك فهد، مبنى رقم 911- الدوران الأول، الرياض، المملكة العربية السعودية
هاتف: 4668193-11-966+
فاكس: 4668195-11-966+
البريد الإلكتروني: info@sudairpharma.com
عنوان المراسلة: صندوق بريد رقم: 19047، الرياض - المملكة العربية السعودية
الشركة المصنعة:
مختبرات دكتور ريدى، ليمتد- الوحدة السابعة الخاصة بالتصنيع، القطع من رقم P1 إلى P9، المرحلة الثالثة،
دوفادا، فيسز، فيساخاباثنام، أندرا براديش، الهند، 530046
Pomalidomide in combination with bortezomib and dexamethasone is indicated in the treatment of adult patients with multiple myeloma who have received at least one prior treatment regimen including lenalidomide.
Pomalidomide in combination with dexamethasone is indicated in the treatment of adult patients with relapsed and refractory multiple myeloma who have received at least two prior treatment regimens, including both lenalidomide and bortezomib, and have demonstrated disease progression on the last therapy.
Treatment must be initiated and monitored under the supervision of physicians experienced in the management of multiple myeloma.
Dosing is continued or modified based upon clinical and laboratory findings. Posology
• Pomalidomide in combination with bortezomib and dexamethasone
The recommended starting dose of Pomalidomide is 4 mg orally once daily on Days 1 to 14 of repeated 21-day cycles.
Pomalidomide is administered in combination with bortezomib and dexamethasone, as shown in Table 1.
The recommended starting dose of bortezomib is 1.3 mg/m2 intravenous or subcutaneous once daily, on the days shown in Table 1. The recommended dose of dexamethasone is 20 mg orally once daily, on the days shown in Table 1.
Treatment with pomalidomide combined with bortezomib and dexamethasone should be given until disease progression or until unacceptable toxicity occurs.
Table 1. Recommended dosing scheme for Pomalidomide in combination with bortezomib and dexamethasone
Cycle 1-8 | Day (of 21-day cycle) | ||||||||||||||||||||
| 1 | 2 | 3 | 4 | 5 | 6 | 7 | 8 | 9 | 10 | 11 | 12 | 13 | 14 | 15 | 16 | 17 | 18 | 19 | 20 | 21 |
Pomalidomide (4 mg) | • | • | • | • | • | • | • | • | • | • | • | • | • | • |
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Bortezomib (1.3 mg/m2) | • |
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| • |
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| • |
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| • |
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Dexamethasone (20 mg) * | • | • |
| • | • |
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| • | • |
| • | • |
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Cycle 9 onwards | Day (of 21-day cycle) | ||||||||||||||||||||
| 1 | 2 | 3 | 4 | 5 | 6 | 7 | 8 | 9 | 10 | 11 | 12 | 13 | 14 | 15 | 16 | 17 | 18 | 19 | 20 | 21 |
Pomalidomide (4 mg) | • | • | • | • | • | • | • | • | • | • | • | • | • | • |
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Bortezomib (1.3 mg/m2) | • |
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| • |
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Dexamethasone (20 mg) * | • | • |
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| • | • |
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* For patients > 75 years of age, see Special populations.
Pomalidomide dose modification or interruption
To initiate a new cycle of pomalidomide, the neutrophil count must be ≥ 1 x 109/l and the platelet
count must be ≥ 50 x 109/l.
Instructions on dose interruptions or reductions for pomalidomide related adverse reactions are outlined in the Table 2 and dose levels are defined in Table 3 below:
Table 2. Pomalidomide dose modification instructions∞
Toxicity | Dose modification |
Neutropenia * | |
ANC** < 0.5 x 109/l or febrile neutropenia (fever ≥38.5°C and ANC <1 x 109/l) | Interrupt pomalidomide treatment for remainder of cycle. Follow CBC*** weekly. |
ANC return to ≥ 1 x 109/l | Resume pomalidomide treatment at one dose level lower than previous dose. |
For each subsequent drop < 0.5 x 109/l | Interrupt pomalidomide treatment. |
ANC return to ≥ 1 x 109/l | Resume pomalidomide treatment at one dose level lower than the previous dose. |
Thrombocytopenia | |
Platelet count < 25 x 109/l | Interrupt pomalidomide treatment for remainder of cycle. Follow CBC*** weekly. |
Platelet count return to ≥ 50 x 109/l | Resume pomalidomide treatment at one dose level lower than previous dose. |
For each subsequent drop < 25 x 109/l | Interrupt pomalidomide treatment. |
Platelet count return to ≥ 50 x 109/l | Resume pomalidomide treatment at one dose level lower than the previous dose |
Rash | |
Rash = Grade 2-3 | Consider dose interruption or discontinuation of pomalidomide treatment. |
Rash = Grade 4 or blistering (including angioedema, exfoliative or bullous rash or if Stevens-Johnson syndrome (SJS), Toxic Epidermal Necrolysis (TEN) or Drug Reaction with Eosinophilia and Systemic Symptoms (DRESS) is suspected) | Permanently discontinue treatment |
Other | |
Other ≥ Grade 3 pomalidomide-related adverse events | Interrupt pomalidomide treatment for remainder of cycle. Resume at one dose level lower than previous dose at next cycle (adverse event must be resolved or improved to ≤ Grade 2 before restarting dosing). |
∞ Dose modification instructions in this table are applicable to pomalidomide in combination with bortezomib and dexamethasone and to pomalidomide in combination with dexamethasone.
*In case of neutropenia, the physician should consider the use of growth factors. **ANC – Absolute Neutrophil Count; ***CBC – Complete Blood Count. | |
Table 3. Pomalidomide dose reduction ∞
Dose level | Oral pomalidomide dose |
Starting dose | 4 mg |
Dose level -1 | 3 mg |
Dose level -2 | 2 mg |
Dose level -3 | 1 mg |
∞ Dose reduction in this table is applicable to pomalidomide in combination with bortezomib and dexamethasone and to pomalidomide in
combination with dexamethasone.
If adverse reactions occur after dose reductions to 1 mg, then the medicinal product should be discontinued.
Strong CYP1A2 inhibitors
If strong inhibitors of CYP1A2 (e.g. ciprofloxacin, enoxacin and fluvoxamine) are co- administered with pomalidomide, reduce the dose of pomalidomide by 50%.
Bortezomib dose modification or interruption
For instructions on dose interruptions or reductions for bortezomib related adverse reactions, physicians should refer to Summary of Product Characteristics (SmPC).
Dexamethasone dose modification or interruption
Instructions on dose interruptions or reductions for low-dose dexamethasone related adverse reactions are outlined in Tables 4 and 5 below. However, dose interruption or resumption decisions are at the physician's discretion per Summary of Product Characteristics (SmPC).
Table 4. Dexamethasone dose modification instructions
Toxicity | Dose Modification |
Dyspepsia = Grade 1-2 | Maintain dose and treat with histamine (H2) blockers or equivalent. Decrease by one dose level if symptoms persist. |
Dyspepsia ≥ Grade 3 | Interrupt dose until symptoms are controlled. Add H2blocker or equivalent and resume at one dose level lower than previous dose. |
Oedema ≥ Grade 3 | Use diuretics as needed and decrease dose by one dose level. |
Confusion or mood alteration ≥ Grade 2 | Interrupt dose until symptoms resolve. Resume at one dose level lower than previous dose. |
Muscle weakness ≥ Grade 2 | Interrupt dose until muscle weakness ≤ Grade 1. Resume at one dose level lower than previous dose. |
Hyperglycaemia ≥ Grade 3 | Decrease dose by one dose level. Treat with insulin or oral hypoglycaemic agents as needed. |
Acute pancreatitis | Discontinue dexamethasone from treatment regimen. |
Other ≥ Grade 3 dexamethasone-related adverse events | Stop dexamethasone dosing until the adverse event resolves to ≤ Grade 2. Resume at one dose level lower than previous dose. |
If recovery from toxicities is prolonged beyond 14 days, then the dose of dexamethasone will be resumed at one dose level lower than the previous dose.
Table 5. Dexamethasone dose reduction
Dose Level | ≤ 75 years old Dose (Cycle 1-8: Days 1, 2, 4, 5, 8, 9, 11, 12 of a 21-day cycle Cycle ≥ 9: Days 1, 2, 8, 9 of a 21-day cycle) | > 75 years old Dose (Cycle 1-8: Days 1, 2, 4, 5, 8, 9, 11, 12 of a 21-day cycle Cycle ≥ 9: Days 1, 2, 8, 9 of a 21-day cycle) |
Starting Dose | 20 mg | 10 mg |
Dose Level -1 | 12 mg | 6 mg |
Dose Level -2 | 8 mg | 4 mg |
Dexamethasone should be discontinued if the patient is unable to tolerate 8 mg if ≤ 75 years old
or 4 mg if > 75 years old.
In case of permanent discontinuation of any component of the treatment regimen, continuation of the remaining medicinal products is at the physician's discretion.
• Pomalidomide in combination with dexamethasone
The recommended starting dose of Pomalidomide is 4 mg orally once daily on Days 1 to 21 of repeated 28-day cycles.
The recommended dose of dexamethasone is 40 mg orally once daily on Days 1, 8, 15 and 22 of each 28-day treatment cycle.
Treatment with pomalidomide combined with dexamethasone should be given until disease progression or until unacceptable toxicity occurs.
Pomalidomide dose modification or interruption
Instructions for dose interruptions or reductions for pomalidomide related adverse reactions are outlined in Table 2 and 3.
Dexamethasone dose modification or interruption
Instructions for dose modification for dexamethasone related adverse reactions are outlined in Table 4. Instructions for dose reduction for dexamethasone related adverse reactions are outlined in Table 6 below. However, dose interruption / resumption decisions are at physician's discretion per the current Summary of Product Characteristics (SmPC).
Table 6. Dexamethasone dose reduction
Dose Level | ≤ 75 years old
Days 1, 8, 15 and 22 of each 28-day treatment cycle | > 75 years old
Days 1, 8, 15 and 22 of each 28-day treatment cycle |
Starting Dose | 40 mg | 20 mg |
Dose Level -1 | 20 mg | 12 mg |
Dose Level -2 | 10mg | 8 mg |
Dexamethasone should be discontinued if the patient is unable to tolerate 10 mg if ≤ 75 years old
or 8 mg if > 75 years old. Special populations Elderly
• Pomalidomide in combination with bortezomib and dexamethasone
No dose adjustment is required for pomalidomide.
For information on bortezomib given in combination with Pomalidomide, refer to the respective current SmPC.
For patients >75 years of age, the starting dose of dexamethasone is:
• For Cycles 1 to 8: 10 mg once daily on Days 1, 2, 4, 5, 8, 9, 11 and 12 of each 21-day cycle
• For Cycles 9 and onwards: 10 mg once daily on Days 1, 2, 8 and 9 of each 21-day cycle.
• Pomalidomide in combination with dexamethasone
No dose adjustment is required for pomalidomide.
For patients > 75 years of age, the starting dose of dexamethasone is:
• 20 mg once daily on days 1, 8, 15 and 22 of each 28-day treatment cycle.
Hepatic impairment
Patients with serum total bilirubin > 1.5 x ULN (upper limit of normal range) were excluded from clinical studies. Hepatic impairment has a modest effect on the pharmacokinetics of pomalidomide. No adjustment of the starting dose of pomalidomide is required for patients with hepatic impairment as defined by the Child-Pugh criteria. However, patients with hepatic impairment should be carefully monitored for adverse reactions and dose reduction or interruption of pomalidomide should be used as needed.
Renal impairment
No dose adjustment of pomalidomide is required for patients with renal impairment. On haemodialysis days, patients should take their pomalidomide dose following haemodialysis.
Paediatric population
There is no relevant use of pomalidomide in children aged 0-17 years for the indication of multiple myeloma.
Method of administration
Oral use.
Pomalidomide hard capsules should be taken orally at the same time each day. The capsules should not be opened, broken or chewed. The capsules should be swallowed whole, preferably with water,
with or without food. If the patient forgets to take a dose of pomalidomide on one day, then the patient should take the normal prescribed dose as scheduled on the next day. Patients should not adjust the dose to make up for a missing dose on previous days.
It is recommended to press only on one end of the capsule to remove it from the blister thereby reducing the risk of capsule deformation or breakage.
For information on other medicinal products given in combination with Pomalidomide, refer to the respective SmPC.
Teratogenicity
Pomalidomide must not be taken during pregnancy, since a teratogenic effect is expected. Pomalidomide is structurally related to thalidomide. Thalidomide is a known human teratogen that causes severe life-threatening birth defects. Pomalidomide was found to be teratogenic in both rats and rabbits when administered during the period of major organogenesis.
The conditions of the Pregnancy Prevention Programme must be fulfilled for all patients unless there is reliable evidence that the patient does not have childbearing potential.
Criteria for women of non-childbearing potential
A female patient or a female partner of a male patient is considered of non-childbearing potential if she meets at least one of the following criteria:
• Age ≥ 50 years and naturally amenorrhoeic for ≥ 1 year (amenorrhoea following cancer therapy
or during breast-feeding does not rule out childbearing potential)
• Premature ovarian failure confirmed by a specialist gynaecologist
• Previous bilateral salpingo-oophorectomy, or hysterectomy
• XY genotype, Turner syndrome, uterine agenesis. Counselling
For women of childbearing potential, pomalidomide is contraindicated unless all of the following are met:
• She understands the expected teratogenic risk to the unborn child
• She understands the need for effective contraception, without interruption, at least 4 weeks before starting treatment, throughout the entire duration of treatment, and at least 4 weeks after the end of treatment
• Even if a woman of childbearing potential has amenorrhoea she must follow all the advice on effective contraception
• She should be capable of complying with effective contraceptive measures
• She is informed and understands the potential consequences of pregnancy and the need to rapidly consult if there is a risk of pregnancy
• She understands the need to commence the treatment as soon as pomalidomide is dispensed following a negative pregnancy test
• She understands the need and accepts to undergo pregnancy testing at least every 4 weeks except in case of confirmed tubal sterilisation
• She acknowledges that she understands the hazards and necessary precautions associated with the use of pomalidomide.
The prescriber must ensure that for women of childbearing potential:
• The patient complies with the conditions of the Pregnancy Prevention Programme, including confirmation that she has an adequate level of understanding
• The patient has acknowledged the aforementioned conditions.
For male patients taking pomalidomide, pharmacokinetic data has demonstrated that pomalidomide is present in human semen during treatment. As a precaution, and taking into account special populations with potentially prolonged elimination time such as hepatic impairment, all male patients taking pomalidomide must meet the following conditions:
• He understands the expected teratogenic risk if engaged in sexual activity with a pregnant woman or a woman of childbearing potential
• He understands the need for the use of a condom if engaged in sexual activity with a pregnant woman or a woman of childbearing potential not using effective contraception, throughout treatment duration, during dose interruption and for 7 days after dose interruptions and/or cessation of treatment. This includes vasectomised males who should wear a condom if engaged in sexual activity with a pregnant woman or a woman of childbearing potential as seminal fluid may still contain pomalidomide in the absence of spermatozoa.
• He understands that if his female partner becomes pregnant whilst he is taking pomalidomide or 7 days after he has stopped taking pomalidomide, he should inform his treating physician immediately and that it is recommended to refer the female partner to a physician specialised or experienced in teratology for evaluation and advice.
Contraception
Women of childbearing potential must use at least one effective method of contraception for at least 4 weeks before therapy, during therapy, and until at least 4 weeks after pomalidomide therapy and even in case of dose interruption unless the patient commits to absolute and continuous abstinence confirmed on a monthly basis. If not established on effective contraception, the patient must be referred to an appropriately trained health care professional for contraceptive advice in order that contraception can be initiated.
The following can be considered to be examples of suitable methods of contraception:
• Implant
• Levonorgestrel-releasing intrauterine system
• Medroxyprogesterone acetate depot
• Tubal sterilisation
• Sexual intercourse with a vasectomised male partner only; vasectomy must be confirmed by two negative semen analyses
• Ovulation inhibitory progesterone-only pills (i.e. desogestrel)
Because of the increased risk of venous thromboembolism in patients with multiple myeloma taking pomalidomide and dexamethasone, combined oral contraceptive pills are not recommended. If a patient is currently using combined oral contraception the patient should switch to one of the effective methods listed above. The risk of venous thromboembolism continues for
4-6 weeks after discontinuing combined oral contraception. The efficacy of contraceptive steroids may be reduced during cotreatment with dexamethasone.
Implants and levonorgestrel-releasing intrauterine systems are associated with an increased risk of infection at the time of insertion and irregular vaginal bleeding. Prophylactic antibiotics should be considered particularly in patients with neutropenia.
Insertion of copper-releasing intrauterine devices is not recommended due to the potential risks of infection at the time of insertion and menstrual blood loss which may compromise patients with severe neutropenia or severe thrombocytopenia.
Pregnancy testing
According to local practice, medically supervised pregnancy tests with a minimum sensitivity of 25 mIU/mL must be performed for women of childbearing potential as outlined below. This requirement includes women of childbearing potential who practice absolute and continuous abstinence. Ideally, pregnancy testing, issuing a prescription and dispensing should occur on the same day. Dispensing of pomalidomide to women of childbearing potential should occur within 7 days of the prescription.
Prior to starting treatment
A medically supervised pregnancy test should be performed during the consultation, when pomalidomide is prescribed, or in the 3 days prior to the visit to the prescriber once the patient had been using effective contraception for at least 4 weeks. The test should ensure the patient is not pregnant when she starts treatment with pomalidomide.
Follow-up and end of treatment
A medically supervised pregnancy test should be repeated at least every 4 weeks, including at least 4 weeks after the end of treatment, except in the case of confirmed tubal sterilisation. These pregnancy tests should be performed on the day of the prescribing visit or in the 3 days prior to the visit to the prescriber.
Additional precautions
Patients should be instructed never to give this medicinal product to another person and to return any unused capsules to their pharmacist at the end of treatment.
Patients should not donate blood, semen or sperm during treatment (including during dose interruptions) and for 7 days following discontinuation of pomalidomide.
Educational materials, prescribing and dispensing restrictions
In order to assist patients in avoiding foetal exposure to pomalidomide, the Marketing Authorisation Holder will provide educational material to health care professionals to reinforce the warnings about the expected teratogenicity of pomalidomide, to provide advice on contraception before therapy is started, and to provide guidance on the need for pregnancy testing. The prescriber must inform the patient about the expected teratogenic risk and the strict pregnancy prevention measures as specified in the Pregnancy Prevention Programme and provide patients with appropriate patient educational brochure, patient card and/or equivalent tool in accordance with the national implemented patient card system. A national controlled distribution system has been implemented in collaboration with each National Competent Authority. The controlled distribution system includes the use of a patient card and/or equivalent tool for prescribing and /or dispensing controls, and the collection of detailed data relating to the indication in order to monitor the off-label use within the national territory. Ideally, pregnancy testing, issuing a prescription and dispensing should occur on the same day. Dispensing of pomalidomide to women of childbearing potential should occur within 7 days of the prescription and following a medically supervised negative pregnancy test result. Prescriptions for women of childbearing potential can be for a
maximum duration of 4 weeks, and prescriptions for all other patients can be for a maximum duration of 12 weeks.
Haematological events
Neutropenia was the most frequently reported Grade 3 or 4 haematological adverse reaction in patients with relapsed/refractory multiple myeloma, followed by anaemia and thrombocytopenia. Patients should be monitored for haematological adverse reactions, especially neutropenia. Patients should be advised to report febrile episodes promptly. Physicians should observe patients for signs of bleeding including epistaxes, especially with use of concomitant medicinal products known to increase the risk of bleeding. Complete blood counts should be monitored at baseline, weekly for the first 8 weeks and monthly thereafter. A dose modification may be required. Patients may require use of blood product support and /or growth factors.
Thromboembolic events
Patients receiving pomalidomide either in combination with bortezomib and dexamethasone or in combination with dexamethasone have developed venous thromboembolic events (predominantly deep vein thrombosis and pulmonary embolism) and arterial thrombotic events (myocardial infarction and cerebrovascular accident). Patients with known risk factors for thromboembolism – including prior thrombosis – should be closely monitored. Action should be taken to try to minimise all modifiable risk factors (e.g. smoking, hypertension, and hyperlipidaemia). Patients and physicians are advised to be observant for the signs and symptoms of thromboembolism. Patients should be instructed to seek medical care if they develop symptoms such as shortness of breath, chest pain, arm or leg swelling. Anti-coagulation therapy (unless contraindicated) is recommended, (such as acetylsalicylic acid, warfarin, heparin or clopidogrel), especially in patients with additional thrombotic risk factors. A decision to take prophylactic measures should be made after a careful assessment of the individual patient's underlying risk factors. In clinical studies, patients received prophylactic acetylsalicylic acid or alternative anti-thrombotic therapy. The use of erythropoietic agents carries a risk of thrombotic events including thromboembolism. Therefore, erythropoietic agents, as well as other agents that may increase the risk of thromboembolic events, should be used with caution.
Peripheral neuropathy
Patients with ongoing ≥ Grade 2 peripheral neuropathy were excluded from clinical studies with pomalidomide. Appropriate caution should be exercised when considering the treatment of such patients with pomalidomide.
Significant cardiac dysfunction
Patients with significant cardiac dysfunction (congestive heart failure [NY Heart Association Class III or IV]; myocardial infarction within 12 months of starting study; unstable or poorly controlled angina pectoris) were excluded from clinical studies with pomalidomide. Cardiac events, including congestive cardiac failure, pulmonary oedema and atrial fibrillation, have been reported, mainly in patients with pre-existing cardiac disease or cardiac risk factors. Appropriate caution should be exercised when considering the treatment of such patients with pomalidomide, including periodic monitoring for signs or symptoms of cardiac events.
Tumour lysis syndrome
Patients at greatest risk of tumour lysis syndrome are those with high tumour burden prior to treatment. These patients should be monitored closely and appropriate precautions taken.
Second primary malignancies
Second primary malignancies, such as non-melanoma skin cancer, have been reported in patients receiving pomalidomide. Physicians should carefully evaluate patients before and during treatment
using standard cancer screening for occurrence of second primary malignancies and institute treatment as indicated.
Allergic reactions and severe skin reactions
Angioedema and severe dermatologic reactions including SJS, TEN and DRESS have been reported with the use of pomalidomide. Patients should be advised of the signs and symptoms of these reactions by their prescribers and should be told to seek medical attention immediately if they develop these symptoms. Pomalidomide must be discontinued for exfoliative or bullous rash, or if SJS, TEN or DRESS is suspected, and should not be resumed following discontinuation for these reactions. Patients with a prior history of serious allergic reactions associated with thalidomide or lenalidomide were excluded from clinical studies. Such patients may be at higher risk of hypersensitivity reactions and should not receive pomalidomide. Pomalidomide interruption or discontinuation should be considered for Grade 2-3 skin rash. Pomalidomide must be discontinued permanently for angioedema.
Dizziness and confusion
Dizziness and confusional state have been reported with pomalidomide. Patients must avoid situations where dizziness or confusion may be a problem and not to take other medicinal products that may cause dizziness or confusion without first seeking medical advice.
Interstitial lung disease (ILD)
ILD and related events, including cases of pneumonitis, have been observed with pomalidomide. Careful assessment of patients with an acute onset or unexplained worsening of pulmonary symptoms should be performed to exclude ILD. Pomalidomide should be interrupted pending investigation of these symptoms and if ILD is confirmed, appropriate treatment should be initiated. Pomalidomide should only be resumed after a thorough evaluation of the benefits and the risks.
Hepatic disorders
Markedly elevated levels of alanine aminotransferase and bilirubin have been observed in patients treated with pomalidomide. There have also been cases of hepatitis that resulted in discontinuation of pomalidomide. Regular monitoring of liver function is recommended for the first 6 months of treatment with pomalidomide and as clinically indicated thereafter.
Infections
Reactivation of hepatitis B has been reported rarely in patients receiving pomalidomide in combination with dexamethasone who have previously been infected with the hepatitis B virus (HBV). Some of these cases have progressed to acute hepatic failure, resulting in discontinuation of pomalidomide. Hepatitis B virus status should be established before initiating treatment with pomalidomide. For patients who test positive for HBV infection, consultation with a physician with expertise in the treatment of hepatitis B is recommended. Caution should be exercised when pomalidomide in combination with dexamethasone is used in patients previously infected with HBV, including patients who are anti-HBc positive but HBsAg negative. These patients should be closely monitored for signs and symptoms of active HBV infection throughout therapy.
Sodium content
This medicinal product contains less than 1 mmol sodium (23 mg) per capsule, i.e. essentially 'sodium-free'.
For information on other medicinal products given in combination with pomalidomide, refer to the respective current SmPC.
Effect of pomalidomide on other medicinal products
Pomalidomide is not anticipated to cause clinically relevant pharmacokinetic drug-drug interactions due to P450 isoenzyme inhibition or induction or transporter inhibition when co- administered with substrates of these enzymes or transporters. The potential for such drug-drug interactions, including the potential impact of pomalidomide on the pharmacokinetics of combined oral contraceptives, has not been evaluated clinically.
Effect of other medicinal products on pomalidomide
Pomalidomide is partly metabolised by CYP1A2 and CYP3A4/5. It is also a substrate for P- glycoprotein. Co-administration of pomalidomide with the strong CYP3A4/5 and P-gp inhibitor ketoconazole, or the strong CYP3A4/5 inducer carbamazepine, had no clinically relevant effect on exposure to pomalidomide. Co-administration of the strong CYP1A2 inhibitor fluvoxamine with pomalidomide in the presence of ketoconazole, increased mean exposure to pomalidomide by 107% with a 90% confidence interval [91% to 124%] compared to pomalidomide plus ketoconazole. In a second study to evaluate the contribution of a CYP1A2 inhibitor alone to metabolism changes, co-administration of fluvoxamine alone with pomalidomide increased mean exposure to pomalidomide by 125% with a 90% confidence interval [98% to 157%] compared to pomalidomide alone. If strong inhibitors of CYP1A2 (e.g. ciprofloxacin, enoxacin and fluvoxamine) are co-administered with pomalidomide, reduce the dose of pomalidomide by 50%.
Dexamethasone
Co-administration of multiple doses of up to 4 mg pomalidomide with 20 mg to 40 mg dexamethasone (a weak to moderate inducer of several CYP enzymes including CYP3A) to patients with multiple myeloma had no effect on the pharmacokinetics of pomalidomide compared with pomalidomide administered alone.
The effect of dexamethasone on warfarin is unknown. Close monitoring of warfarin concentration is advised during treatment.
For information on other medicinal products given in combination with pomalidomide, refer to the respective current SmPC
Women of childbearing potential / Contraception in males and females
Women of childbearing potential should use effective method of contraception. If pregnancy occurs in a woman treated with pomalidomide, treatment must be stopped and the patient should be referred to a physician specialised or experienced in teratology for evaluation and advice. If pregnancy occurs in a partner of a male patient taking pomalidomide, it is recommended to refer the female partner to a physician specialised or experienced in teratology for evaluation and advice. Pomalidomide is present in human semen. As a precaution, all male patients taking pomalidomide should use condoms throughout treatment duration, during dose interruption and for 7 days after cessation of treatment if their partner is pregnant or of childbearing potential and has no contraception.
Pregnancy
A teratogenic effect of pomalidomide in humans is expected. Pomalidomide is contraindicated during pregnancy and in women of childbearing potential, except when all the conditions for pregnancy prevention have been met
Breast-feeding
It is unknown whether pomalidomide is excreted in human milk. Pomalidomide was detected in milk of lactating rats following administration to the mother. Because of the potential for adverse reactions in breastfed infants from pomalidomide, a decision must be made whether to discontinue
breast-feeding or to discontinue the medicinal product, taking into account the benefit of breast- feeding for the child and the benefit of the therapy for the woman.
Fertility
Pomalidomide was found to impact negatively on fertility and be teratogenic in animals. Pomalidomide crossed the placenta and was detected in foetal blood following administration to pregnant rabbits.
Pomalidomide has minor or moderate influence on the ability to drive and use machines. Fatigue, depressed level of consciousness, confusion, and dizziness have been reported with the use of pomalidomide. If affected, patients should be instructed not to drive cars, use machines or perform hazardous tasks while being treated with pomalidomide.
Summary of the safety profile
• Pomalidomide in combination with bortezomib and dexamethasone
The most commonly reported blood and lymphatic system disorders were neutropenia (46.8%), thrombocytopenia (36.7%) and anaemia (28.4%). The most frequently reported adverse reaction was peripheral sensory neuropathy (47.8%). The most commonly reported Grade 3 or 4 adverse reactions were blood and lymphatic system disorders including neutropenia (41.7%), thrombocytopenia (27.3%) and anaemia (14.0%). The most commonly reported serious adverse reaction was pneumonia (11.5%). Other serious adverse reactions reported included pyrexia (4.0%), lower respiratory tract infection (2.9%), pulmonary embolism (2.9%), influenza (2.9%), and acute kidney injury (2.9%).
• Pomalidomide in combination with dexamethasone
The most commonly reported adverse reactions in clinical studies have been blood and lymphatic system disorders including anaemia (45.7%), neutropenia (45.3%) and thrombocytopenia (27%); in general disorders and administration site conditions including fatigue (28.3%), pyrexia (21%) and oedema peripheral (13%); and in infections and infestations including pneumonia (10.7%). Peripheral neuropathy adverse reactions were reported in 12.3% of patients and venous embolic or thrombotic (VTE) adverse reactions were reported in 3.3% of patients. The most commonly reported Grade 3 or 4 adverse reactions were in the blood and lymphatic system disorders including neutropenia (41.7%), anaemia (27%) and thrombocytopenia (20.7%); in infections and infestations including pneumonia (9%); and in general disorders and administration site conditions including fatigue (4.7%), pyrexia (3%) and oedema peripheral (1.3%). The most commonly reported serious adverse reaction was pneumonia (9.3%). Other serious adverse reactions reported included febrile neutropenia (4.0%), neutropenia (2.0%), thrombocytopenia (1.7%) and VTE adverse reactions (1.7
%).
Adverse reactions tended to occur more frequently within the first 2 cycles of treatment with pomalidomide.
Tabulated list of adverse reactions
• Pomalidomide in combination with bortezomib and dexamethasone
In randomised study CC-4047-MM-007, 278 patients received pomalidomide, bortezomib and dexamethasone (Pom+Btz+Dex arm).
The adverse reactions observed in patients treated with pomalidomide in combination with bortezomib and dexamethasone are listed in Table 7 by system organ class (SOC) and frequency for all adverse reactions and for Grade 3 or 4 adverse reactions.
Frequencies for Pom+Btz+Dex (any grade) are defined in accordance with current guidance, as:
very common (≥1/10), common (≥1/100 to <1/10); and uncommon (≥1/1,000 to <1/100).
Table 7. All Adverse Reactions (ADRs) reported in clinical trial MM-007 in patients treated
with pomalidomide in combination with bortezomib and dexamethasone.
System Organ Class/ Preferred Term | All Adverse Reactions /Frequency | Grade 3−4 Adverse Reactions /Frequency |
Infections and infestations | Very Common Pneumonia Bronchitis Upper respiratory tract infection Viral upper respiratory tract infection Common Sepsis Septic shock Clostridium difficile colitis Respiratory tract infection Lower respiratory tract infection Lung infection Influenza Bronchiolitis Urinary tract infection | Very Common Pneumonia Common Sepsis Septic shock Clostridium difficile colitis Bronchitis Upper respiratory tract infection Respiratory tract infection Lower respiratory tract infection Lung infection Influenza Bronchiolitis Urinary tract infection |
Neoplasms benign, malignant and unspecified (incl cysts and polyps) | Common Basal cell carcinoma |
|
Blood and lymphatic system disorders | Very Common Neutropenia Thrombocytopenia Leucopenia Anaemia Common Febrile neutropenia Lymphopenia | Very Common Neutropenia Thrombocytopenia Anaemia Common Febrile neutropenia Leucopenia Lymphopenia |
Metabolism and nutrition disorders | Very Common Hypokalaemia Hyperglycaemia Common Hypomagnesaemia Hypocalcaemia Hypophosphataemia Hyperkalaemia Hypercalcaemia | Common Hypokalaemia Hyperglycaemia Hypomagnaesaemia Hypocalcaemia Hypophosphataemia Hyperkalaemia Hypercalcaemia |
Psychiatric disorders | Very Common Insomnia Common Depression | Common Depression Insomnia |
Nervous system disorders | Very Common Peripheral sensory neuropathy Dizziness Tremor Common Syncope Peripheral sensorimotor neuropathy Paraesthesia Dysgeusia | Common Syncope Peripheral sensory neuropathy Peripheral sensorimotor neuropathy Uncommon Dizziness Tremor |
Eye disorders | Common Cataract | Common Cataract |
Cardiac disorders | Common Atrial fibrillation | Common Atrial fibrillation |
Vascular disorders | Common | Common |
| Deep vein thrombosis Hypotension Hypertension | Hypotension Hypertension Uncommon Deep vein thrombosis |
Respiratory, thoracic and mediastinal disorders | Very Common Dyspnoea Cough Common Pulmonary embolism | Common Pulmonary embolism Dyspnoea |
Gastrointestinal disorders | Very Common Diarrhoea Vomiting Nausea Constipation Common Abdominal pain Abdominal pain upper Stomatitis Dry mouth Abdominal distension | Common Diarrhoea Vomiting Abdominal pain Constipation Uncommon Abdominal pain upper Stomatitis Nausea Abdominal distension |
Skin and subcutaneous tissue disorders | Common Rash | Common Rash |
Musculoskeletal and connective tissue disorders | Very Common Muscular weakness Back pain Common Bone pain Muscle spasms | Common Muscular weakness Back pain Uncommon Bone pain |
Renal and urinary disorders | Common Acute kidney injury Chronic kidney injury Urinary retention | Common Acute kidney injury Chronic kidney injury Urinary retention |
General disorders and administration site conditions | Very Common Fatigue Pyrexia Oedema peripheral Common Non-cardiac chest pain Oedema | Common Fatigue Pyrexia Non-cardiac chest pain Oedema peripheral Oedema |
Investigations | Common Alanine aminotransferase increased Weight decreased | Common Weight decreased Uncommon Alanine aminotransferase increased |
Injury, poisoning and procedural complications | Common Fall | Uncommon Fall |
Tabulated list of adverse reactions
• Pomalidomide in combination with dexamethasone
In randomised study CC-4047-MM-003, 302 patients with relapsed and refractory multiple myeloma were exposed to 4 mg pomalidomide administered once daily for 21 days of each 28– day cycle in combination with a weekly low dose of dexamethasone.
The adverse reactions observed in patients treated with pomalidomide plus dexamethasone are listed below in Table 8 by system organ class (SOC) and frequency for all adverse reactions (ADRs) and for Grade 3 or 4 adverse reactions.
The frequencies of adverse reactions are those reported in the pomalidomide plus dexamethasone arm of study CC-4047-MM-003 (n = 302). Within each SOC and frequency grouping, adverse reactions are presented in order of decreasing seriousness. Frequencies are defined in accordance
with current guidance, as: very common (≥ 1/10), common (≥ 1/100 to < 1/10); and uncommon (≥
1/1,000 to < 1/100).
Table 8. ADRs reported in clinical study MM-003 in patients treated with pomalidomide in combination with dexamethasone.
System Organ Class/ Preferred Term | All ADRs/Frequency | Grade 3−4 ADRs/Frequency |
Infections and infestations | Very Common Pneumonia (bacterial, viral and fungal infections, including opportunistic infections) Common Neutropenic sepsis Bronchopneumonia Bronchitis Respiratory tract infection Upper respiratory tract infection Nasopharyngitis Herpes zoster | Common Neutropenic sepsis Pneumonia (bacterial, viral and fungal infections, including opportunistic infections) Bronchopneumonia Respiratory tract infection Upper respiratory tract infection Uncommon Bronchitis Herpes zoster |
Neoplasms benign, malignant and unspecified (incl cysts and polyps) | Uncommon Basal cell carcinoma of the skin, Squamous cell carcinoma of the skin | Uncommon Basal cell carcinoma of the skin, Squamous cell carcinoma of the skin |
Blood and lymphatic system disorders | Very Common Neutropenia Thrombocytopenia Leucopenia Anaemia Common Febrile neutropenia | Very Common Neutropenia Thrombocytopenia Anaemia Common Febrile neutropenia Leucopenia |
Metabolism and nutrition disorders | Very Common Decreased appetite Common Hyperkalaemia Hyponatraemia | Common Hyperkalaemia Hyponatraemia Uncommon Decreased appetite |
Psychiatric disorders | Common Confusional state | Common Confusional state |
Nervous system disorders | Common Depressed level of consciousness Peripheral sensory neuropathy Dizziness Tremor | Common Depressed level of consciousness Uncommon Peripheral sensory neuropathy Dizziness Tremor |
Ear and labyrinth disorders | Common Vertigo | Common Vertigo |
Vascular disorders | Common Deep vein thrombosis | Uncommon Deep vein thrombosis |
Respiratory, thoracic and mediastinal disorders | Very Common Dyspnoea Cough Common Pulmonary embolism | Common Dyspnoea Uncommon Pulmonary embolism Cough |
Gastrointestinal disorders | Very Common Diarrhoea Nausea Constipation Common Vomiting Gastrointestinal haemorrhage | Common Diarrhoea Vomiting Constipation Uncommon Nausea Gastrointestinal haemorrhage |
Hepatobiliary disorders | Uncommon Hyperbilirubinaemia | Uncommon Hyperbilirubinaemia |
Skin and subcutaneous tissue disorders | Common Rash Pruritus | Common Rash |
Musculoskeletal and connective tissue disorders | Very Common Bone pain Muscle spasms | Common Bone pain Uncommon Muscle spasms |
Renal and urinary disorders | Common Renal failure Urinary retention | Common Renal failure Uncommon Urinary retention |
Reproductive system and breast disorders | Common Pelvic pain | Common Pelvic pain |
General disorders and administration site conditions | Very Common Fatigue Pyrexia Oedema peripheral | Common Fatigue Pyrexia Oedema peripheral |
Investigations | Common Neutrophil count decreased White blood cell count decreased Platelet count decreased Alanine aminotransferase increased | Common Neutrophil count decreased White blood cell count decreased Platelet count decreased Alanine aminotransferase increased |
Tabulated list of post-marketing adverse reactions
In addition to the above adverse reactions identified from the pivotal clinical trials, the following Table 9 is derived from data gathered from post-marketing surveillance.
Table 9. ADRs reported in post-marketing use in patients treated with pomalidomide.
System Organ Class/ Preferred Term | All Adverse Reactions /Frequency | Grade 3−4 Adverse Reactions /Frequency |
Infections and infestations | Not Known Hepatitis B reactivation | Not Known Hepatitis B reactivation |
Blood and lymphatic system disorders | Common Pancytopenia | Common Pancytopenia |
Metabolism and nutrition disorders | Common Hyperuricaemia Uncommon Tumour lysis syndrome | Common Hyperuricaemia Uncommon Tumour lysis syndrome |
Nervous system disorders | Common Intracranial haemorrhage Uncommon Cerebrovascular accident | Uncommon Cerebrovascular accident Intracranial haemorrhage |
Cardiac disorders | Common Cardiac failure Atrial fibrillation Myocardial infarction | Common Cardiac failure Atrial fibrillation Uncommon Myocardial infarction |
Immune system disorders | Common Angioedema Urticaria | Uncommon Angioedema Urticaria |
Respiratory, thoracic and mediastinal disorders | Common Epistaxis Interstitial lung disease | Uncommon Epistaxis Interstitial lung disease |
Hepatobiliary disorders | Uncommon Hepatitis |
|
Skin and subcutaneous tissue disorders | Not Known Drug Reaction with Eosinophilia and Systemic Symptoms Toxic Epidermal Necrolysis Stevens-Johnson Syndrome | Not Known Drug Reaction with Eosinophilia and Systemic Symptoms Toxic Epidermal Necrolysis Stevens-Johnson Syndrome |
Investigations | Common Blood uric acid increased | Uncommon Blood uric acid increased |
Description of selected adverse reactions
Teratogenicity
Pomalidomide is structurally related to thalidomide. Thalidomide is a known human teratogenic active substance that causes severe life-threatening birth defects. Pomalidomide was found to be teratogenic in both rats and rabbits when administered during the period of major organogenesis. If pomalidomide is taken during pregnancy, a teratogenic effect of pomalidomide in humans is expected.
Neutropenia and thrombocytopenia
In patients receiving combination therapy with pomalidomide in clinical studies, neutropenia occurred in up to 46.8% of patients (41.7% Grade 3 or 4). Neutropenia did not lead to pomalidomide discontinuation in any patient and was infrequently serious.
Febrile neutropenia (FN) was reported in 3.2-6.7% of patients and was serious in 1.8-4.0% of patients.
In patients receiving combination therapy with pomalidomide in clinical studies, thrombocytopenia occurred in 27.0-36.7% of patients. Thrombocytopenia was Grade 3 or 4 in 20.7-27.3% of patients, led to pomalidomide discontinuation in 0.7% of patients and was serious in 0.4-1.7% of patients.
Neutropenia and thrombocytopenia tended to occur more frequently within the first 2 cycles of treatment with pomalidomide.
Infection
Infection was the most common non-haematological toxicity.
In patients receiving combination therapy with pomalidomide in clinical studies, infection occurred in 55.0-80.2% of patients (24.0-30.9% Grade 3 or 4). Upper respiratory tract infection and pneumonia were the most frequently occurring infections. Fatal infections (Grade 5) occurred in 2.7-4.0% of patients. Infections led to pomalidomide discontinuation in 2.0-2.9% of patients.
Thromboembolic events
Prophylaxis with acetylsalicylic acid (and other anticoagulants in high risk patients) was mandatory for all patients in clinical studies. Anticoagulation therapy (unless contraindicated) is recommended.
In patients receiving combination therapy with pomalidomide in clinical studies, venous thromboembolic events (VTE) occurred in 3.3-11.5% of patients (1.3-5.4% Grade 3 or 4). VTE was reported as serious in 1.7-4.3% of patients, no fatal reactions were reported, and VTE was associated with pomalidomide discontinuation in up to 1.8% of patients.
Peripheral neuropathy
• Pomalidomide in combination with bortezomib and dexamethasone
Patients with ongoing peripheral neuropathy ≥ Grade 2 with pain within 14 days prior to randomisation were excluded from clinical trials. Peripheral neuropathy occurred in 55.4 % of patients (10.8% Grade 3; 0.7% Grade 4). Exposure-adjusted rates were comparable across treatment arms. Approximately 30% of the patients experiencing peripheral neuropathy had a history of neuropathy at baseline. Peripheral neuropathy led to discontinuation of bortezomib in approximately 12.9% of patients, pomalidomide in 1.8% and dexamethasone in 2.2 - 8.9% of patients, respectively. Refer also to the bortezomib SmPC.
• Pomalidomide in combination with dexamethasone
Patients with ongoing peripheral neuropathy ≥ Grade 2 were excluded from clinical studies. Peripheral neuropathy occurred in 12.3% of patients (1.0% Grade 3 or 4). No peripheral neuropathy reactions were reported as serious, and peripheral neuropathy led to dose discontinuation in 0.3% of patients
Haemorrhage
Haemorrhagic disorders have been reported with pomalidomide, especially in patients with risk factors such as concomitant medicinal products that increase susceptibility to bleeding. Haemorrhagic events have included epistaxis, intracranial haemorrhage and gastrointestinal haemorrhage.
Allergic reactions and severe skin reactions
Angioedema and severe cutaneous reactions including SJS, TEN and DRESS has been reported with the use of pomalidomide. Patients with a history of severe rash associated with lenalidomide
or thalidomide should not receive pomalidomide.
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 submitting completed forms to: npc.drug@sfda.gov.sa.
Pomalidomide doses as high as 50 mg as a single dose in healthy volunteers, and 10 mg as once- daily multiple doses in multiple myeloma patients have been studied without reported serious adverse reactions related to overdose. In studies, pomalidomide was found to be removed by haemodialysis.
In the event of overdose, supportive care is advised.
Pharmacotherapeutic group: Immunosuppressants, Other immunosuppressants, ATC code: L04AX06
Mechanism of Action
Pomalidomide has direct anti-myeloma tumoricidal activity, immunomodulatory activities and inhibits stromal cell support for multiple myeloma tumour cell growth. Specifically, pomalidomide inhibits proliferation and induces apoptosis of haematopoietic tumour cells. Additionally, pomalidomide inhibits the proliferation of lenalidomide-resistant multiple myeloma cell lines and synergises with dexamethasone in both lenalidomide-sensitive and lenalidomide-resistant cell lines to induce tumour cell apoptosis. Pomalidomide enhances T cell- and natural killer (NK) cell- mediated immunity and inhibits production of pro-inflammatory cytokines (e.g., TNF-α and IL-6) by monocytes. Pomalidomide also inhibits angiogenesis by blocking the migration and adhesion of endothelial cells.
Pharmacodynamics:
Pomalidomide binds directly to the protein cereblon (CRBN), which is part of an E3 ligase complex that includes deoxyribonucleic acid (DNA) damage-binding protein 1(DDB1), cullin 4 (CUL4), and regulator of cullins-1 (Roc1), and can inhibit the auto-ubiquitination of CRBN within the complex. E3 ubiquitin ligases are responsible for the poly-ubiquitination of a variety of substrate proteins, and may partially explain the pleiotropic cellular effects observed with pomalidomide treatment.
In the presence of pomalidomide in vitro, substrate proteins Aiolos and Ikaros are targeted for ubiquitination and subsequent degradation leading to direct cytotoxic and immunomodulatory effects. In vivo, pomalidomide therapy led to reduction in the levels of Ikaros in patients with relapsed lenalidomide-refractory multiple myeloma.
Clinical efficacy and safety
• Pomalidomide in combination with bortezomib and dexamethasone
The efficacy and safety of pomalidomide in combination with bortezomib and low-dose dexamethasone (Pom+Btz+LD-Dex) was compared with bortezomib and low-dose dexamethasone (Btz+LD-Dex) in a Phase III multi-centre, randomised, open-label study (CC- 4047-MM-007), in previously treated adult patients with multiple myeloma, who had received at least one prior regimen, including lenalidomide and have demonstrated disease progression on or after the last therapy. A total of 559 patients were enrolled and randomised in the study: 281 in the Pom+Btz+LD-Dex arm and 278 in the Btz+LD-Dex arm. 54% of patients were male with median age for the overall population of 68 years (min, max: 27, 89 years). Approximately 70% of patients were refractory to lenalidomide (71.2% in Pom+Btz+LD-Dex, 68.7 % in Btz+LD-Dex). Approximately 40% of patients were in 1st relapse and approximately 73% of patients received bortezomib as prior treatment.
Patients in the Pom+Btz+LD-Dex arm were administered 4 mg pomalidomide orally on Days 1 to 14 of each 21-day cycle. Bortezomib (1.3 mg/m2/dose) was administered to patients in both study arms on Days 1, 4, 8 and 11 of a 21-day cycle for Cycles 1 to 8; and on Days 1 and 8 of a 21-day cycle for Cycles 9 and onwards. Low-dose dexamethasone (20 mg/day [≤ 75 years old] or 10 mg/day [> 75 years old]) was administered to patients in both study arms on Days 1, 2, 4, 5, 8, 9,
11 and 12 of a 21-day cycle for Cycles 1 to 8; and on Days 1, 2, 8 and 9 of each subsequent 21- day cycle from Cycles 9 onwards. Doses were reduced and treatment was temporarily interrupted or stopped as needed to manage toxicity.
The primary efficacy endpoint was Progression Free Survival (PFS) assessed by an Independent Response Adjudication Committee (IRAC) according to the IMWG criteria using the intent to treat population (ITT). After a median follow-up of 15.9 months, median PFS time was 11.20 months (95% CI: 9.66, 13.73) in the Pom+Btz+LD-Dex arm. In the Btz+LD-Dex arm, median PFS time was 7.1 months (95% CI: 5.88, 8.48).
Summary of overall efficacy data are presented in Table 10 using a cut-off date of 26 Oct 2017. Kaplan-Meier curve for PFS for the ITT population is provided in Figure 1.
Table 10. Summary of overall efficacy data
| Pom+Btz+LD-Dex (N = 281) | Btz+LD-Dex (N = 278) |
PFS (months) |
| |
Mediana time (95% CI) b | 11.20 (9.66, 13.73) | 7.10 (5.88, 8.48) |
HR c (95% CI), p-valued | 0.61 (0.49, 0.77), <0.0001 | |
ORR, n (%) | 82.2 % | 50.0% |
sCR | 9 (3.2) | 2 (0.7) |
CR | 35 (12.5) | 9 (3.2) |
VGPR | 104 (37.0) | 40 (14.4) |
PR | 83 (29.5) | 88 (31.7) |
OR (95% CI) e, p-valuef | 5.02 (3.35, 7.52), <0.001 | |
DoR (months) |
| |
Mediana time (95% CI) b | 13.7 (10.94, 18.10) | 10.94 (8.11, 14.78) |
HRc (95% CI) | 0.76 (0.56, 1.02) | |
Btz = bortezomib; CI = Confidence interval; CR = Complete response; DoR = Duration of response; HR = Hazard Ratio; LD-Dex = low-dose dexamethasone; OR = Odds ratio; ORR = Overall response rate; PFS = Progression free survival; POM = pomalidomide; PR = Partial Response; sCR = Stringent complete response VGPR = Very good partial response.
a The median is based on the Kaplan-Meier estimate.
b 95% CI about the median.
c Based on Cox proportional hazards model.
d The p-value is based on a stratified log-rank test.
e Odds ratio is for Pom+Btz+LD-Dex:Btz+LD-Dex.
f The p-value is based on a CMH test, stratified by age (<=75 vs >75), Prior number of antimyeloma regimens (1 vs >1), and Beta-2 microglobulin at screening (< 3.5 mg/L versus ≥ 3.5 mg/L — ≤ 5.5 mg/L versus > 5.5 mg/L).
The median duration of treatment was 8.8 months (12 treatment cycles) in the Pom+Btz+LD-Dex arm and 4.9 months (7 treament cycles) in the Btz+LD-Dex arm.
The PFS advantage was more pronounced in patients who received only one prior line of therapy. In patients who received 1 prior antimyeloma line, median PFS time was 20.73 months (95% CI: 15.11, 27.99) in the Pom + Btz + LD-Dex arm and 11.63 months (95% CI: 7.52, 15.74) in the Btz
+ LD-Dex arm. A 46% risk reduction was observed with Pom + Btz + LD-Dex treatment (HR = 0.54, 95% CI: 0.36, 0.82).
Figure 1. Progression Free Survival Based on IRAC Review of Response by IMWG Criteria (Stratified Log Rank Test) (ITT Population).
As per an interim analysis for Overall Survival (OS), using a cut-off of 15 September 2018 (median follow-up period of 26.2 months), median OS time from Kaplan-Meier estimates was 40.5 months for the Pom + Btz + LD-Dex arm and 30.5 months for the Btz + LD-Dex arm; HR = 0.91, 95% CI: 0.70, 1.18, with an overall event rate of 43.3%.
• Pomalidomide in combination with dexamethasone
The efficacy and safety of pomalidomide in combination with dexamethasone were evaluated in a Phase III multi-centre, randomised, open-label study (CC-4047-MM-003), where pomalidomide plus low-dose dexamethasone therapy (Pom+LD-Dex) was compared to high-dose dexamethasone alone (HD-Dex) in previously treated adult patients with relapsed and refractory multiple myeloma, who have received at least two prior treatment regimens, including both lenalidomide and bortezomib, and have demonstrated disease progression on the last therapy. A total of 455 patients were enrolled in the study: 302 in the Pom+LD-Dex arm and 153 in the HD-Dex arm. The majority of patients were male (59%) and white (79%); the median age for the overall population was 64 years (min, max: 35, 87 years).
Patients in the Pom+LD-Dex arm were administered 4 mg pomalidomide orally on days 1 to 21 of each 28-day cycle. LD-Dex (40 mg) was administered once per day on days 1, 8, 15 and 22 of a 28-day cycle. For the HD-Dex arm, dexamethasone (40 mg) was administered once per day on days 1 through 4, 9 through 12, and 17 through 20 of a 28-day cycle. Patients > 75 years of age started treatment with 20 mg dexamethasone. Treatment continued until patients had disease progression.
The primary efficacy endpoint was progression free survival by International Myeloma Working Group (IMWG criteria). For the intention to treat (ITT) population, median PFS time by Independent Review Adjudication Committee (IRAC) review based on IMWG criteria was 15.7 weeks (95% CI: 13.0, 20.1) in the Pom + LD-Dex arm; the estimated 26-week event-free survival rate was 35.99% (±3.46%). In the HD-Dex arm, median PFS time was 8.0 weeks (95% CI: 7.0, 9.0); the estimated 26-week event-free survival rate was 12.15% (±3.63%).
PFS was evaluated in several relevant subgroups: gender, race, ECOG performance status, stratification factors (age, disease population, prior anti-myeloma therapies [2, > 2]), selected parameters of prognostic significance (baseline beta-2 microglobulin level, baseline albumin
levels, baseline renal impairment, and cytogenetic risk), and exposure and refractoriness to prior anti-myeloma therapies. Regardless of the subgroup evaluated, PFS was generally consistent with that observed in the ITT population for both treatment groups.
PFS is summarised in Table 11 for the ITT population. Kaplan-Meier curve for PFS for the ITT population is provided in Figure 2.
Table 11. Progression Free Survival Time by IRAC Review Based on IMWG Criteria (Stratified
Log Rank Test) (ITT Population)
| Pom+LD-Dex (N=302) | HD-Dex (N=153) |
Progression free survival (PFS), N | 302 (100.0) | 153 (100.0) |
Censored, n (%) | 138 (45.7) | 50 (32.7) |
Progressed/Died, n (%) | 164 (54.3) | 103 (67.3) |
Progression Free Survival Time (weeks) | ||
Mediana | 15.7 | 8.0 |
Two sided 95% CIb | [13.0, 20.1] | [7.0, 9.0] |
Hazard Ratio (Pom+LD-Dex:HD-Dex) 2-Sided 95% CI c | 0.45 [0.35,0.59] | |
Log-Rank Test Two sided P-Value d | <0.001 | |
Note: CI=Confidence interval; IRAC=Independent Review Adjudication Committee; NE = Not Estimable. a The median is based on Kaplan-Meier estimate. b 95% confidence interval about the median progression free survival time. c Based on Cox proportional hazards model comparing the hazard functions associated with treatment groups, stratified by age (≤75 vs >75),diseases population (refractory to both lenalidomide and bortezomib vs not refractory to both active substances), and prior number of anti myeloma therapy (=2 vs >2). d The p-value is based on a stratified log-rank test with the same stratification factors as the above Cox model. Data cutoff: 07 Sep 2012 | ||
Figure 2. Progression Free Survival Based on IRAC Review of Response by IMWG Criteria
(Stratified Log Rank Test) (ITT Population)
Overall Survival was the key secondary study endpoint. A total of 226 (74.8%) of the Pom + LD- Dex patients and 95 (62.1%) of the HD-Dex patients were alive as of the cutoff date (07 Sep 2012). Median OS time from Kaplan-Meier estimates has not been reached for the Pom + LD-Dex, but would be expected to be at least 48 weeks, which is the lower boundary of the 95% CI. Median OS time for the HD-Dex arm was 34 weeks (95% CI: 23.4, 39.9). The 1-year event free rate was 52.6% (± 5.72%) for the Pom + LD-Dex arm and 28.4% (± 7.51%) for the HD-Dex arm. The difference in OS between the two treatment arms was statistically significant (p < 0.001).
Overall survival is summarised in Table 12 for the ITT population. Kaplan-Meier curve for OS for the ITT population is provided in Figure 3.
Based on the results of both PFS and OS endpoints, the Data Monitoring Committee established for this study recommended that the study be completed and patients in the HD-Dex arm be crossed over to the Pom + LD-Dex arm.
Table 12. Overall Survival: ITT Population
| Statistics | Pom+LD-Dex (N=302) | HD-Dex (N=153) |
| N | 302 (100.0) | 153 (100.0) |
Censored | n (%) | 226 (74.8) | 95 (62.1) |
Died | n (%) | 76 (25.2) | 58 (37.9) |
Survival Time (weeks) | Mediana | NE | 34.0 |
| Two sided 95% CIb | [48.1, NE] | [23.4, 39.9] |
Hazard Ratio (Pom+LD-Dex:HD-Dex) [Two sided 95% CIc] | 0.53[0.37, 0.74] | ||
Log-Rank Test Two sided P-Valued | <0.001 | ||
Note: CI=Confidence interval. NE = Not Estimable.
a The median is based on Kaplan-Meier estimate.
b 95% confidence interval about the median overall survival time.
c Based on Cox proportional hazards model comparing the hazard functions associated with treatment groups.
d The p-value is based on an unstratified log-rank test.
Figure 3. Kaplan-Meier Curve of Overall Survival (ITT Population)
Absorption
Pomalidomide is absorbed with a maximum plasma concentration (Cmax) occurring between 2 and 3 hours and is at least 73% absorbed following administration of single oral dose. The systemic exposure (AUC) of pomalidomide increases in an approximately linear and dose proportional manner. Following multiple doses, pomalidomide has an accumulation ratio of 27 to 31% on AUC.
Coadministration with a high-fat and high-calorie meal slows the rate of absorption, decreasing mean plasma Cmax by approximately 27%, but has minimal effect on the overall extent of absorption with an 8% decrease in mean AUC. Therefore, pomalidomide can be administered without regard to food intake.
Distribution
Pomalidomide has a mean apparent volume of distribution (Vd/F) between 62 and 138 L at steady state. Pomalidomide is distributed in semen of healthy subjects at a concentration of approximately 67% of plasma level at 4 hours post-dose (approximately Tmax) after 4 days of once daily dosing at 2 mg. In vitro binding of pomalidomide enantiomers to proteins in human plasma ranges from 12% to 44% and is not concentration dependent.
Biotransformation
Pomalidomide is the major circulating component (approximately 70% of plasma radioactivity) in vivo in healthy subjects who received a single oral dose of [14C]-pomalidomide (2 mg). No metabolites were present at >10% relative to parent or total radioactivity in plasma.
The predominant metabolic pathways of excreted radioactivity are hydroxylation with subsequent glucuronidation, or hydrolysis. In vitro, CYP1A2 and CYP3A4 were identified as the primary enzymes involved in the CYP-mediated hydroxylation of pomalidomide, with additional minor contributions from CYP2C19 and CYP2D6. Pomalidomide is also a substrate of P-glycoprotein in vitro. Co-administration of pomalidomide with the strong CYP3A4/5 and P-gp inhibitor ketoconazole, or the strong CYP3A4/5 inducer carbamazepine, had no clinically relevant effect on
exposure to pomalidomide. Co-administration of the strong CYP1A2 inhibitor fluvoxamine with pomalidomide in the presence of ketoconazole, increased mean exposure to pomalidomide by 107% with a 90% confidence interval [91% to 124%] compared to pomalidomide plus ketoconazole. In a second study to evaluate the contribution of a CYP1A2 inhibitor alone to metabolism changes, co-administration of fluvoxamine alone with pomalidomide increased mean exposure to pomalidomide by 125% with a 90% confidence interval [98% to 157%] compared to pomalidomide alone. If strong inhibitors of CYP1A2 (e.g. ciprofloxacin, enoxacin and fluvoxamine) are co-administered with pomalidomide, reduce the dose of pomalidomide to 50%. Administration of pomalidomide in smokers, with smoking tobacco known to induce the CYP1A2 isoform, had no clinically relevant effect on exposure to pomalidomide compared to that exposure to pomalidomide observed in non-smokers.
Based on in vitro data, pomalidomide is not an inhibitor or inducer of cytochrome P-450 isoenzymes, and does not inhibit any drug transporters that were studied. Clinically relevant drug- drug interactions are not anticipated when pomalidomide is coadministered with substrates of these pathways.
Elimination
Pomalidomide is eliminated with a median plasma half-life of approximately 9.5 hours in healthy subjects and approximately 7.5 hours in patients with multiple myeloma. Pomalidomide has a mean total body clearance (CL/F) of approximately 7-10 L/hr.
Following a single oral administration of [14C] -pomalidomide (2 mg) to healthy subjects, approximately 73% and 15% of the radioactive dose was eliminated in urine and faeces, respectively, with approximately 2% and 8% of the dosed radiocarbon eliminated as pomalidomide in urine and faeces.
Pomalidomide is extensively metabolised prior to excretion, with the resulting metabolites eliminated primarily in the urine. The 3 predominant metabolites in urine (formed via hydrolysis or hydroxylation with subsequent glucuronidation) account for approximately 23%, 17%, and 12%, respectively, of the dose in the urine.
CYP dependent metabolites account for approximately 43% of the total excreted radioactivity, while non-CYP dependent hydrolytic metabolites account for 25%, and excretion of unchanged pomalidomide accounted for 10% (2% in urine and 8% in faeces).
Population Pharmacokinetics (PK)
Based on population PK analysis using a two-compartment model, healthy subjects and MM patients had comparable apparent clearance (CL/F) and apparent central volume of distribution (V2/F). In peripheral tissues, pomalidomide was preferentially taken up by tumors with apparent peripheral distribution clearance (Q/F) and apparent peripheral volume of distribution (V3/F) 3.7- fold and 8-fold higher, respectively, than that of healthy subjects.
Paediatric population
No data are available on administration of pomalidomide to paediatric patients (< 18 years of age). Elderly
Based on population pharmacokinetic analyses in healthy subjects and multiple myeloma patients, no significant influence of age (19-83 years) on oral clearance of pomalidomide was observed. In clinical studies, no dose adjustment was required in elderly (> 65 years) patients exposed to pomalidomide.
Renal impairment
Population pharmacokinetic analyses showed that the pomalidomide pharmacokinetic parameters were not remarkably affected in renally impaired patients (defined by creatinine clearance or
estimated glomerular filtration rate [eGFR]) compared to patients with normal renal function (CrCl
≥60 mL/minute). Mean normalized AUC exposure to pomalidomide was 98.2% with a 90% confidence interval [77.4% to 120.6%] in moderate renal impairment patients (eGFR ≥30 to ≤45 mL/minute/1.73 m2) compared to patients with normal renal function. Mean normalized AUC exposure to pomalidomide was 100.2% with a 90% confidence interval [79.7% to 127.0%] in severe renal impairment patients not requiring dialysis (CrCl <30 or eGFR <30 mL/minute/1.73 m2) compared to patients with normal renal function. Mean normalized AUC exposure to pomalidomide increased by 35.8% with a 90% CI [7.5% to 70.0%] in severe renal impairment patients requiring dialysis (CrCl <30mL/minute requiring dialysis) compared to patients with normal renal function. The mean changes in exposure to pomalidomide in each of these renal impairment groups are not of a magnitude that requires dosage adjustments.
Hepatic impairment
The pharmacokinetic parameters were modestly changed in hepatically impaired patients (defined by Child-Pugh criteria) compared to healthy subjects. Mean exposure to pomalidomide increased by 51% with a 90% confidence interval [9% to 110%] in mildly hepatically impaired patients compared to healthy subjects. Mean exposure to pomalidomide increased by 58% with a 90% confidence interval [13% to 119%] in moderately hepatically impaired patients compared to healthy subjects. Mean exposure to pomalidomide increased by 72% with a 90% confidence interval [24% to 138%] in severely hepatically impaired patients compared to healthy subjects. The mean increases in exposure to pomalidomide in each of these impairment groups are not of a magnitude for which adjustments in schedule or dose are required.
Repeat-dose toxicology studies
In rats, chronic administration of pomalidomide at doses of 50, 250, and 1000 mg/kg/day for 6 months was well tolerated. No adverse findings were noted up to 1000 mg/kg/day (175-fold exposure ratio relative to a 4 mg clinical dose).
In monkeys, pomalidomide was evaluated in repeat-dose studies of up to 9 months in duration. In these studies, monkeys exhibited greater sensitivity to pomalidomide effects than rats. The primary toxicities observed in monkeys were associated with the haematopoietic/lymphoreticular systems. In the 9-month study in monkeys with doses of 0.05, 0.1, and 1 mg/kg/day, morbidity and early euthanasia of 6 animals were observed at the dose of 1 mg/kg/day and were attributed to immunosuppressive effects (staphylococcal infection, decreased peripheral blood lymphocytes, chronic inflammation of the large intestine, histologic lymphoid depletion, and hypocellularity of bone marrow) at high exposures of pomalidomide (15-fold exposure ratio relative to a 4 mg clinical dose). These immunosuppressive effects resulted in early euthanasia of 4 monkeys due to poor health condition (watery stool, inappetence, reduced food intake, and weight loss); histopathologic evaluation of these animals showed chronic inflammation of the large intestine and villous atrophy of the small intestine. Staphylococcal infection was observed in 4 monkeys; 3 of these animals responded to antibiotic treatment and 1 died without treatment. In addition, findings consistent with acute myelogenous leukemia led to euthanasia of 1 monkey; clinical observations and clinical pathology and/or bone marrow alterations observed in this animal were consistent with immunosuppression. Minimal or mild bile duct proliferation with associated increases in ALP and GGT were also observed at 1 mg/kg/day. Evaluation of recovery animals indicated that all treatment-related findings were reversible after 8 weeks of dosing cessation, except for proliferation of intrahepatic bile ducts observed in 1 animal in the 1 mg/kg/day group. The No Observed Adverse Effect Level (NOAEL) was 0.1 mg/kg/day (0.5-fold exposure ratio relative to a 4 mg clinical dose).
Genotoxicity/carcinogenicity
Pomalidomide was not mutagenic in bacterial and mammalian mutation assays, and did not induce chromosomal aberrations in human peripheral blood lymphocytes or micronuclei formation in polychromatic erythrocytes in bone marrow of rats administered doses up to 2000 mg/kg/day. Carcinogenicity studies have not been conducted.
Fertility and early embryonic development
In a fertility and early embryonic development study in rats, pomalidomide was administered to males and females at dosages of 25, 250, and 1000 mg/kg/day. Uterine examination on Gestation Day 13 showed a decrease in mean number of viable embryos and an increase in postimplantation loss at all dosage levels. Therefore, the NOAEL for these observed effects was < 25 mg/kg/day (AUC 24h was 39960 ng•h/mL (nanogram•hour/millilitres) at this lowest dose tested, and the exposure ratio was 99-fold relative to a 4 mg clinical dose). When treated males on this study were mated with untreated females, all uterine parameters were comparable to the controls. Based on these results, the observed effects were attributed to the treatment of females.
Embryo-foetal development
Pomalidomide was found to be teratogenic in both rats and rabbits when administered during the period of major organogenesis. In the rat embryofoetal developmental toxicity study, malformations of absence of urinary bladder, absence of thyroid gland, and fusion and misalignment of lumbar and thoracic vertebral elements (central and/or neural arches) were observed at all dosage levels (25, 250, and 1000 mg/kg/day).
There was no maternal toxicity observed in this study. Therefore, the maternal NOAEL was 1000 mg/kg/day, and the NOAEL for developmental toxicity was < 25 mg/kg/day (AUC24h was 34340 ng•h/mL on Gestation Day 17 at this lowest dose tested, and the exposure ratio was 85-fold relative to a 4 mg clinical dose). In rabbits, pomalidomide at dosages ranging from 10 to 250 mg/kg produced embryo-foetal developmental malforma tions. Increased cardiac anomalies were seen at all doses with significant increases at 250 mg/kg/day. At 100 and 250 mg/kg/day, there were slight increases in post-implantation loss and slight decreases in fetal body weights. At 250 mg/kg/day, fetal malformations included limb anomalies (flexed and/or rotated fore- and/or hindlimbs, unattached or absent digit) and associated skeletal malformations (not ossified metacarpal, misaligned phalanx and metacarpal, absent digit, not ossified phalanx, and short not ossified or bent tibia); moderate dilation of the lateral ventricle in the brain; abnormal placement of the right subclavian artery; absent intermediate lobe in the lungs; low-set kidney; altered liver morphology; incompletely or not ossified pelvis; an increased average for supernumerary thoracic ribs and a reduced average for ossified tarsals. Slight reduction in maternal body weight gain, significant reduction in triglycerides, and significant decrease in absolute and relative spleen weights were observed at 100 and 250 mg/kg/day. The maternal NOAEL was 10 mg/kg/day, and the developmental NOAEL was <10 mg/kg/day (AUC24h was 418 ng•h/mL on Gestation Day 19 at this lowest dose tested, which was similar to that obtained from a 4 mg clinical dose).
Anhydrous lactose, Pregelatinised Starch Sodium stearyl fumarate
Not applicable
Do not Store above 30°C.
Capsules are packaged in blisters and bottle.
Capsules should not be opened or crushed. If powder from pomalidomide makes contact with the skin, the skin should be washed immediately and thoroughly with soap and water. If pomalidomide makes contact with the mucous membranes, they should be thoroughly flushed with water.
Any unused medicinal product or waste material should be disposed of in accordance with local requirements. Unused medicinal product should be returned to the pharmacist at the end of treatment.
