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SFDA PIL
(Patient Information Leaflet (PIL) are under review by Saudi Food and Drug Authority)
Bendokey, Bendamustine hydrochloride 100mg Injection is a medicine which
is used for the treatment of certain types of cancer (cytotoxic medicine).
Bendokey is used alone (monotherapy) or in combination with other
medicines for the treatment of the following forms of cancer:
- chronic lymphocytic leukaemia in cases where fludarabine combination
chemotherapy is not appropriate for you,
- non-Hodgkin lymphomas, which had not, or only shortly, responded to
prior rituximab treatment,
- multiple myeloma in cases where thalidomide or bortezomib containing
therapy is not appropriate for you.
Do not use Bendokey
- if you are hypersensitive (allergic) to the active substance bendamustine
hydrochloride or any of the other ingredients of Bendokey;
- while breast-feeding;
- if you have severe liver dysfunction (damage to the functional cells of the
liver);
- if you have yellowing of the skin or whites of the eyes caused by liver or
blood problems (jaundice);
- if you have severely disturbed bone marrow function (bone marrow
depression) and serious changes in your number of white blood cells
and platelets in the blood (white blood cells and/or thrombocyte values
dropped to < 3,000/μl or < 75,000/μl, respectively.);
- if you have had major surgical operations less than 30 days before starting
treatment;
- if you have an infection, especially one accompanied by a reduction in
white blood cells (leucocytopenia);
- in combination with yellow fever vaccines.
Take special care with Bendokey
- in case of reduced capability of the bone marrow to replace blood cells.
You should have your number of white blood cells and platelets in the
blood checked before starting treatment with Bendokey, before each
subsequent course of treatment and in the intervals between courses of
treatment.
- in case of infections. You should contact your doctor if you have signs of
infection, including fever or lung symptoms.
- in case of reactions on your skin during treatment with Bendokey. The
reactions may increase in severity.
- in cases of existing heart disease (e.g. heart attack, chest pain, severely
disturbed heart rhythms).
- in case you notice any pain in your side, blood in your urine or reduced
amount of urine. When your disease is very severe, your body may not
be able to clear all the waste products from the dying cancer cells. This
is called tumour lysis syndrome and can cause kidney failure and heart
problems within 48 hours of the first dose of Bendokey. Your doctor will
be aware of this and may give you other medicines to help prevent it.
- in case of severe allergic or hypersensitivity reactions. You should pay
attention to infusion reactions after your first cycle of therapy.
Men receiving treatment with Bendokey are advised not to conceive a child
during treatment and for up to 6 months afterwards. Before starting treatment,
you should seek advice on storing sperm because of the possibility of
permanent infertility.
Unintentional injection into the tissue outside blood vessels (extravasal
injection) should be stopped immediately. The needle should be removed
after a short aspiration. Thereafter the affected area of tissue should be
cooled. The arm should be elevated. Additional treatments like the use of
corticosteroids are not of clear benefit (see section 4).
Using other medicines
Please tell your doctor or pharmacist if you are taking or have recently
taken other medicines, including medicines obtained without a prescription.
If Bendokey is used in combination with medicines which inhibit the formation
of blood in the bone marrow, the effect on the bone marrow may be intensified.
If Bendokey is used in combination with medicines which alter you immune
response, this effect may be intensified.
Cytostatic medicines may diminish the effectiveness of live-virus vaccination.
Additionally cytostatic medicines increase the risk of an infection after
vaccination with live vaccines (e.g. viral vaccination).
Pregnancy and breast-feeding
Pregnancy
Bendokey can cause fetal harm when administered to a pregnant woman.
Single intraperitoneal doses of bendamustine from 210 mg/m2 (70 mg/kg) in
mice administered during organogenesis caused an increase in resorptions,
skeletal and visceral malformations (exencephaly, cleft palates, accessory
rib, and spinal deformities) and decreased fetal body weights. This dose
did not appear to be maternally toxic and lower doses were not evaluated.
Repeat intraperitoneal dosing in mice on gestation days 7-11 resulted in an
increase in resorptions from 75 mg/m2 (25 mg/kg) and an increase in
abnormalities from 112.5 mg/m2 (37.5 mg/kg) similar to those seen after
a single intraperitoneal administration. Single intraperitoneal doses of
bendamustine from 120 mg/m2 (20 mg/kg) in rats administered on gestation
days 4, 7, 9, 11, or 13 caused embryo and fetal lethality as indicated by
increased resorptions and a decrease in live fetuses. A significant increase in
external [effect on tail, head, and herniation of external organs (exomphalos)]
and internal (hydronephrosis and hydrocephalus) malformations were seen
in dosed rats. There are no adequate and well-controlled studies in pregnant
women. If this drug is used during pregnancy, or if the patient becomes
pregnant while taking this drug, the patient should be apprised of the potential
hazard to the fetus.
Breast-feeding
Bendokey must not be administered during breast feeding. If treatment with
Bendokey is necessary during lactation you must discontinue breast-feeding.
Ask your doctor or pharmacist for advice before taking any medicine.
Driving and using machines
No studies on the effects on the ability to drive and to use machines have
been performed. Do not drive or operate machines if you experience side
effects, such as dizziness or lack of coordination.
Bendokey is administered into a vein over 30-60 minutes in various
dosages, either alone (monotherapy) or in combination with other medicines.
Treatment should not be started if your white blood cells (leukocytes) have
fallen to counts below 3,000 cells/μl and/or your blood platelets have fallen
to counts below 75,000 cells/μl.
Your doctor will determine these values at regular intervals.
Chronic lymphocytic leukaemia
on Days 1+2 | Bendokey 100 mg per square metre of your body surface |
| Repeat the cycle after 4 weeks up to 6 times |
Non-Hodgkin lymphomas
| on Days 1+2 | Bendokey 120 mg per square metre of your body surface area (based on your height and weight) |
| Repeat the cycle after 3 weeks at least 6 times |
Multiple myeloma
| on Days 1+2 | Bendokey 120 - 150 mg per square meter of your body surface area (based on your height and weight) |
| on Days 1 - 4 | Prednisone 60 mg per square metre of your body surface area (based on your height and weight) by injection |
| Repeat the cycle after 4 weeks at least 3 times |
Treatment should be terminated if white blood cell (leukocyte) and/or platelet
values dropped to < 3,000/μl or < 75,000/μl, respectively. Treatment can be
continued after white blood cell values have increased to > 4,000/μl and
platelet values to > 100,000/μl.
Impaired liver or kidney function
Dependent on the degree of impairment of your liver function it may be
necessary to adjust your dose (by 30% in case of moderate liver
dysfunction). No dose adjustment is necessary in case of impairment of
kidney function. Your attending doctor will decide whether a dosage
adjustment is necessary.
How it is administered
Treatment with Bendokey should be undertaken only by doctors experienced
in tumour therapy. Your doctor will give you the exact dose of Bendokey
and use the necessary precautions.
Your attending doctor will administer the solution for infusion after preparation
as prescribed. The solution is administered into a vein as a short-term
infusion over 30 - 60 minutes.
Duration of use
There is no time limit laid down as a general rule for treatment with Bendokey.
Duration of treatment depends on disease and response to treatment.
If you are at all worried or have any questions regarding treatment with
Bendokey, please speak to your doctor or nurse.
If you forget to use Bendokey
If a dose of Bendokey has been forgotten, your doctor will usually retain the
normal dosage schedule.
If you stop using of Bendokey
The doctor treating you will decide whether to interrupt the treatment or to
change over to a different preparation.
If you have any further questions on the use of this product, ask your doctor
or pharmacist.
Like all medicines, Bendokey can cause side-effects, although not everybody
gets them. The following definitions of frequency are used when assessing
side-effects:
| affects more than 1 user in 10 | Very common |
| affects 1 to 10 users in 100 | common |
| 1to 10 users in 1,000 | Uncommon affects |
| affects 1 to 10 users in 10,000 | Rare |
| affects less than 1 user in 10,000 | Very rare |
| frequency cannot be estimated from the available data | not known |
Tissue changes (necrosis) have been observed very rarely following
unintentional injection into the tissue outside blood vessels (extravascular).
A burning sensation where the infusion needle is inserted may be a sign
for administration outside the blood vessels. The consequence of
administration in this way can be pain and poorly healing skin defects.
The dose-limiting side-effect of Bendokey is impaired bone-marrow
function, which usually returns to normal after treatment. Suppressed bone
marrow function increases the risk of infection.
Very common:
• Low counts of white blood cells
(leukocytopenia)
• Decrease in the red pigment of
the blood (haemoglobin)
• Low counts of platelets
(thrombocytopenia)
• Infections
• Feeling sick
(nausea)
• Vomiting
• Mucosal
inflammation
• Increased blood
level of creatinine
• Increased blood
level of urea
• Fever
• Fatigue
Common:
• Bleeding (haemorrhage)
• Disturbed metabolism caused
by dying cancer cells releasing
their contents into the blood
stream
• Reduction in red blood cells
which can make the skin pale
and cause weakness or
breathlessness (anaemia)
• Low counts of neutrophils
(neutropenia)
• Hypersensitivity reactions such
as allergic inflammation of the
skin (dermatitis), nettle rash
(urticaria)
• A rise in liver enzymes AST/ALT
• A rise in the enzyme alkaline
phosphatase
• A rise in bile pigment
• Low potassium
blood levels
• Disturbed
function
(dysfunction) of
the heart
• Disturbed heart
rhythms
(arrhythmia)
• Low or high
blood pressure
(hypotension or
hypertension)
• Disturbed lung
function
• Diarrhoea
• Constipation
• Sore mouth
(Stomatitis)
• Loss of appetite
• Hair loss
• Skin changes
• Missed periods
(amenorrhoea)
• Pain
• Insomnia
• Chills
• Dehydration
Uncommon:
• Accumulation of fluid in the heart sac (escape of fluid into the pericardial
space)
Rare:
• Infection of the blood
(sepsis)
• Severe allergic
hypersensitivity
reactions
(anaphylactic
reactions)
• Signs similar to
anaphylactic
reactions
(anaphylactoid
reactions)
• Drowsiness
• Loss of voice
(aphonia)
• Acute circulatory
collapse
• Reddening of the
skin (erythema)
• Inflammation of the
skin (dermatitis)
• Itching (pruritus)
• Skin rash (macular
exanthema)
• Excessive sweating
(hyperhidrosis)
Very rare:
• Primary atypical
inflammation of the
lungs (pneumonia)
• Break-down of red
blood cell
• Rapid decrease in
blood pressure
sometimes with skin
reactions or rash
(anaphylactic shock)
• Disturbed sense of
taste
• Altered sensations
(paraesthesia)
• Malaise and pain in
the limbs (peripheral
neuropathy)
• Disease of the
nervous system
(anticholinergic
syndrome)
• Neurological
disorders
• Lack of coordination
(ataxia)
• Inflammation of the
brain (encephalitis)
• Increased heart rate
(tachycardia)
• Heart attack, chest
pain (myocardial
infarct)
• Heart failure
• Inflammation of the
veins (phlebitis)
• Formation of tissue
in the lungs (fibrosis
of the lungs)
• Bleeding
inflammation of the
gullet (haemorrhagic
oesophagitis)
• Bleeding of stomach
or gut
• Infertility
• Multiple organ failure
There have been reports of secondary tumours (myelodysplastic syndrome,
acute myeloid leukemia, bronchial carcinoma) following treatment with
Bendokey. No clear relationship with Bendokey could be determined.
A small number of cases of severe skin reactions (Stevens-Johnson
Syndrome and Toxic Epidermal Necrolysis) have been reported. The
relationship with Bendokey is unclear.
If any of the side effects gets serious, or if you notice any side effects not
listed in this leaflet, please tell your doctor.
Reporting of side effects:
If you get any side effects talk to your doctor or pharmacist. This includes
any side effects not listed in this leaflet.
Keep out of the reach and sight of children.
Store below 30°C.
Do not use Bendokey after the expiry date which is stated on the label and
the carton. The expiry date refers to the last day of that month.
Keep the container in the outer carton to protect the content from light.
Shelf life
24 months.
The powder should be reconstituted immediately after opening of the vial.
The reconstituted concentrate should be diluted immediately with 0.9%
sodium chloride solution.
Solution for infusion
After reconstitution and dilution, chemical and physical stability has been
demonstrated for 3.5 hours at 25°C and 60% RH and 48 hours at 2°C to
8°C in polyethylene bags.
From a microbiological point of view, the solution should be used
immediately. If not used immediately, in-use storage times and conditions
prior to use are the responsibility of the user.
The active substance is bendamustine hydrochloride.
1 vial contains 100 mg of bendamustine hydrochloride
After reconstitution 1 ml of the concentrate contains 2.5 mg bendamustine
hydrochloride.
The other ingredient is Mannitol.
Marketing Authorisation Holder
Eugia Pharma Specialities Limited
(a wholly owned subsidiary of Aurobindo Pharma Limited)
Plot No.: 2, Maitrivihar,
Ameerpet, Hyderabad-500 038,
Telangana State, India.
Manufacturer of the final product
Eugia Pharma Specialities Limited,
Survey No. 550, 551 & 552,
Kolthur Village, Shamirpet Mandal,
Medchal-Malkajgiri District,
Telangana, India.
بيندوكي هو دواء يستخدم لعلاج أنواع معينة من السرطان ) الطب السام للخلايا(.
يستخدم بيندوكي وحده ) العلاج الأحادي (أو بالاشتراك مع أدوية أخرى لعلاج الأشكال التالية من السرطان:
- سرطان الدم الليمفاوي المزمن في الحالات التي يكون فيها العلاج الكيميائي المركب من فلودارابين غير
مناسب لك،
- الأورام اللمفاوية غير هودجكين، التي لم، أو فقط بعد فترة وجيزة، استجابت لعلاج ريتوكسيماب السابقة.
- المايلوما المتعددة في الحالات التي يكون فيها الثاليدوميد أو البورتيزوميب الذي يحتوي على العلاج غير
مناسب لك.
1. لا تستخدم بيندوكي:
- إذا كنت مفرط الحساسية ) حساسية (للمادة الفعالة بينداموستين هيدروكلوريد أو أي من المكونات الأخرى
من بيندوكي.
- أثناء الرضاعة الطبيعية.
- إذا كان لديك خلل الكبد الحاد ) تلف في الخلايا الوظيفية للكبد(؛
- إذا كان لديك اصفرار الجلد أو بياض العينين الناجمة عن مشاكل في الكبد أو الدم ) اليرقان(؛
- إذا كنت تعاني من اضطراب شديد في وظيفة نخاع العظم ) اكتئاب نخاع العظم (والتغيرات الخطيرة في
عدد خلايا الدم البيضاء والصفائح الدموية في الدم ) انخفضت قيم خلايا الدم البيضاء و/أو الجلطات
الدموية إلى > 3000 /ميكرو لتر أو > 75000 /ميكرو لتر على التوالي(.
- إذا أجريت عمليات جراحية كبرى قبل أقل من 30 يوما من بدء العلاج؛
- إذا كان لديك عدوى، وخاصة واحدة يرافقه انخفاض في خلايا الدم البيضاء؛
- بالاشتراك مع لقاحات الحمى الصفراء.
اعتني بشكل خاص مع بيندوكي:
- في حالة انخفاض قدرة نخاع العظم على استبدال خلايا الدم. يجب فحص عدد خلايا الدم البيضاء
والصفائح الدموية في الدم قبل بدء العلاج بالبيندوكي، قبل كل دورة لاحقة من العلاج وفي الفترات
الفاصلة بين دورات العلاج.
- في حالة العدوى يجب عليك الاتصال بطبيبك إذا كانت لديك علامات العدوى، بما في ذلك الحمى أو
أعراض الرئة.
- في حالة حدوث ردود فعل على بشرتك أثناء العلاج مع بيندوكي. ردود الفعل قد تزيد في شدتها.
- في حالات أمراض القلب الموجودة ) مثل النوبات القلبية، ألم في الصدر، نبضات القلب المضطربة بشدة(.
- في حال لاحظت أي ألم في جانبك، الدم في البول أو انخفاض كمية البول. عندما يكون مرضك شديدا
جدا، قد لا يتمكن جسمك من إزالة جميع النفايات من الخلايا السرطانية المحتضرة. وهذا ما يسمى
متلازمة تحلل الورم ويمكن أن يسبب الفشل الكلوي ومشاكل في القلب في غضون 48 ساعة من الجرعة
الأولى من بيندوكي. سيدرك طبيبك ذلك وقد يعطيك أدوية أخرى للمساعدة في الوقاية منه.
- في حالة الحساسية الشديدة أو فرط الحساسية. يجب الانتباه إلى ردود الفعل التسريب بعد دورة العلاج الأولى.
ينصح الرجال الذين يتلقون العلاج مع بيندوكي بعدم إنجاب طفل أثناء العلاج ولفترة تصل إلى 6 أشهر بعد
ذلك. قبل بدء العلاج، يجب عليك طلب المشورة بشأن تخزين الحيوانات المنوية بسبب إمكانية العقم الدائم.
يجب إيقاف الحقن غير المتعمد في الأنسجة خارج الأوعية الدموية على الفور. يجب إزالة الإبرة بعد طموح
قصير. بعد ذلك يجب تبريد المنطقة المصابة من الأنسجة. يجب أن تكون الذراع مرتفعة. العلاجات الإضافية
.) مثل استخدام الكورتيكوستيرويدات ليست ذات فائدة واضحة ) انظر القسم 4
استخدام أدوية أخرى:
يرجى إخبار طبيبك أو الصيدلي إذا كنت تتناول أدوية أخرى أو تناولتها مؤخرا، بما في ذلك الأدوية التي تم
الحصول عليها دون وصفة طبية.
إذا تم استخدام بيندوكي في تركيبة مع الأدوية التي تمنع تكوين الدم في نخاع العظام، قد يتم تكثيف التأثير
على نخاع العظام.
إذا تم استخدام بيندوكي في تركيبة مع الأدوية التي تغير لك الاستجابة المناعية، قد يكون هذا التأثير قوي.
الأدوية الخلوية قد تقلل من فعالية التطعيم ضد الفيروسات الحية. بالإضافة إلى ذلك، تزيد الأدوية الخلوية من
خطر العدوى بعد التطعيم باللقاحات الحية ) مثل التطعيم الفيروسي(.
الحمل والرضاعة الطبيعية:
الحمل:
يمكن أن يسبب بيندوكي ضررا للجنين عندما يعطى لامرأة حامل. تسببت الجرعات الوحيدة داخل الصفاق
70 ملغم/كغ (في الفئران التي تدار أثناء تكوين الأعضاء في زيادة في ( من بينداموستين من 210 ملغم /م 2
الامتصاصات والتشوهات الهيكلية والحوشية ) الإكستفالي والحنك المشقوق والضلع الملحق وتشوهات العمود
الفقري (وانخفاض أوزان جسم الجنين. ولا يبدو أن هذه الجرعة سامة للأم ولم يتم تقييم الجرعات المنخفضة.
11 أدى إلى زيادة في الامتصاص من 75 ملغم - تكرار الزحف داخل الصفاق في الفئران في أيام الحمل 7
37.5 ملغم/كغ (مشابهة لتلك التي ( 25 ملغ / كجم (وزيادة في التشوهات من 112.5 ملغم/م 2 ( / م 2
شوهدت بعد إدارة واحدة داخل الصفاق. تسبب جرعات واحدة داخل الصفاق من بينداموستين من 120 ملغم
11 ، أو 13 الجنين والفتك الجنين كما هو ،9 ،7 ، 20 ملغ / كغ (في الفئران تدار في أيام الحمل 4 ( / م 2
مبين من زيادة الامتصاص وانخفاض في الأجنة الحية. وشوهدت زيادة كبيرة في التشوهات الخارجية
]التأثير على الذيل والرأس وفتق الأعضاء الخارجية[ والداخلية ) استسقاء الدماغ واستسقاء الرأس (في
الفئران الكمية. لا توجد دراسات كافية وخاضعة للرقابة الجيدة لدى النساء الحوامل. إذا تم استخدام هذا الدواء
أثناء الحمل، أو إذا أصبحت المريضة حاملا أثناء تناول هذا الدواء، فيجب أن يكون المريض على علم
بالمخاطر المحتملة على الجنين.
الرضاعة الطبيعية:
يجب ألا يعطى البيندوكي أثناء الرضاعة الطبيعية. إذا كان العلاج مع بيندوكي ضروري أثناء الرضاعة
يجب التوقف عن الرضاعة الطبيعية.
القيادة واستخدام الآلات
لم يتم إجراء أي دراسات حول الآثار على القدرة على القيادة واستخدام الآلات.
لا تقود أو تشغل الآلات إذا واجهت آثارا جانبية، مثل الدوخة أو عدم التنسيق.
تؤخذ بيندوكي في الوريد على مدى 30-60 دقيقه في جرعات مختلفة، إما وحدها ) العلاج الأحادي (أو بالاشتراك مع أدوية أخرى.
لا ينبغي أن يبدأ العلاج إذا انخفضت خلايا الدم البيضاء ) الكريات البيضاء (إلى أقل من 3000 خلية /
ميكرو لتر و / أو الصفائح الدموية الخاصة بك قد انخفضت إلى عدد أقل من 75،000 خلية / ميكرو لتر.
سيحدد طبيبك هذه القيم على فترات منتظمة.
سرطان الدم الليمفاوي المزمن:
| بيندوكي 100 ملغ لكل متر مربع من مساحة سطح الجسم ) بناء على طولك ووزنك( | في الأيام 1+2 |
| كرر الدورة بعد 4 أسابيع حتى 6 مرات |
الأورام اللمفاوية غير هودجكين
| بيندوكي 120 ملغ لكل متر مربع من مساحة سطح الجسم ) بناء على طولك ووزنك( | في الأيام 1+2 |
| كرر الدورة بعد 3 أسابيع حتى 6 مرات |
المايلوما المتعددة
| 150 ملغ لكل متر مربع من مساحة سطح الجسم ) على أساس - بيندوكي 120 طولك ووزنك( | في الأيام 1+2 |
| بريدنيزون 60 ملغ لكل متر مربع من مساحة سطح الجسم ) على أساس طولك ووزنك (عن طريق الحقن أو عن طريق الفم. | 4 - في الأيام 1 |
| كرر الدورة بعد 4 أسابيع على الأقل 3 مرات |
يجب إنهاء العلاج إذا انخفضت قيم خلايا الدم البيضاء ) الكريات البيض (و/أو الصفائح الدموية إلى
3000 /ميكرو لتر أو > 75000 /ميكرو لتر، على التوالي. يمكن أن يستمر العلاج بعد أن زادت قيم <
خلايا الدم البيضاء إلى < قيم 4000 /ميكرو لتر والصفائح الدموية إلى < 100000 /ميكرو لتر.
ضعف وظائف الكبد أو الكلى:
اعتمادا على درجة ضعف وظائف الكبد قد يكون من الضروري ضبط الجرعة ) بنسبة 30 ٪ في حالة ضعف
الكبد المعتدل(. لا يلزم تعديل الجرعة في حالة ضعف وظائف الكلى. الطبيب المعالج سيقرر ما إذا كان
تعديل الجرعة ضروري.
كيف يستعمل:
يجب أن يتم العلاج بالبيندوكي فقط من قبل الأطباء ذوي الخبرة في علاج الأورام. سيعطيك طبيبك الجرعة
الدقيقة من بيندوكي وسيستخدم الاحتياطات اللازمة.
سيقوم طبيبك المعالج بإعطاء محلول التسريب بعد التحضير كما هو مقرر. يتم إعطاء الحل في الوريد
60 دقيقة. - كتسريب قصير الأجل على مدى 30
مدة الاستخدام:
لا يوجد حد زمني محدد كقاعدة عامة للعلاج مع بيندوكي. تعتمد مدة العلاج على المرض والاستجابة للعلاج.
إذا كنت قلقا على الإطلاق أو لديك أي أسئلة تتعلق بالعلاج مع بيندوكي، يرجى التحدث إلى طبيبك أو
ممرضتك.
إذا نسيت استخدام بيندوكي:
إذا تم نسيان جرعة من بيندوكي، طبيبك عادة ما تحتفظ الجدول الزمني الجرعة العادية.
إذا توقفت عن استخدام بيندوكي:
سيقرر الطبيب الذي يعالجك ما إذا كان سيقطع العلاج أو يغير الى طريقة علاج اخرى.
إذا كان لديك أي أسئلة أخرى حول استخدام هذا المنتج، اسأل طبيبك أو الصيدلي.
مثل جميع الأدوية، يمكن أن يسبب بيندوكي آثارا جانبية، على الرغم من أن الجميع لا يحصل عليها.
تستخدم التعاريف التالية تقييم الآثار الجانبية:
- شائع جدا يؤثر على أكثر من مستخدم واحد في 10
- شائع يؤثر على 1 إلى 10 مستخدمين في 100
- غير المألوف يؤثر على 1 إلى 10 مستخدمين في 1000
- نادر يؤثر على 1 إلى 10 مستخدمين في 10,000
- نادرة جدا يؤثر على أقل من مستخدم واحد في 10,000
- غير معروف لا يمكن تقدير التردد من البيانات المتوفرة
وقد لوحظت تغيرات الأنسجة ) نخر (نادرا جدا بعد الحقن غير المتعمد في الأنسجة خارج الأوعية الدموية
)خارج الأوعية الدموية(. قد يكون الإحساس بالحرقة حيث يتم إدخال إبرة التسريب علامة للاستخدام خارج
الأوعية الدموية. يمكن أن تكون نتيجة الاستخدام بهذه الطريقة الألم وعيوب الجلد صعبة الشفاء.
الآثار الجانبية للحد من الجرعة من بيندوكي هو ضعف وظيفة نخاع العظام، التي عادة ما تعود إلى وضعها
الطبيعي بعد العلاج. الخلل في وظيفة نخاع العظم تزيد من خطر العدوى.
شائع جدا:
• انخفاض عدد خلايا الدم
البيضاء ) الكريات البيضاء(
• انخفاض في الصباغ الأحمر
للدم ) الهيموغلوبين(
• انخفاض عدد الصفائح الدموية
)الجلطات الدموية(
• العدوى
• الشعور بالمرض ) غثيان(
• القيء
• التهاب الاغشية المخاطية
• زيادة مستوى الكرياتينين في
الدم
• زيادة مستوى الدم من اليوريا
• الحمى
• التعب
شائع:
• نزيف ) نزيف(
• الأيض المضطرب الناجم عن
موت الخلايا السرطانية التي
تطلق محتوياتها في مجرى
الدم
• انخفاض في خلايا الدم
الحمراء التي يمكن أن تجعل
الجلد شاحب ويسبب الضعف
أو ضيق التنفس ) فقر الدم(
• انخفاض عدد العدلات
)العدلات(
• فرط الحساسية مثل التهاب
الحساسية في الجلد ) التهاب
الجلد(، طفح القراص
)الشرى(
• ارتفاع في إنزيمات الكبد
AST / ALT
• ارتفاع في الفوسفات القلوية
الإنزيم
• ارتفاع في صبغة الصفراء
• انخفاض مستويات الدم
البوتاسيوم
• وظيفة مضطربة ) خلل
وظيفي (في القلب
• اضطراب نظم القلب ) عدم
انتظام ضربات القلب(
• انخفاض أو ارتفاع ضغط الدم
)انخفاض ضغط الدم أو
ارتفاع ضغط الدم(
• اضطراب في وظائف الرئة
• الإسهال
• الإمساك
• التهاب الفم ) التهاب الفم(
• فقدان الشهية
• تساقط الشعر
• تغيرات الجلد
• فترات ضائعة ) انقطاع
الفترات(
• ألم
• الأرق
• قشعريرة
• الجفاف
غير شائع:
• تراكم السوائل في كيس القلب.
نادر:
• عدوى الدم ) الإنتان(.
• الحساسية الشديدة فرط
الحساسية ) الحساسية(.
• علامات مشابهة لردود الفعل
الحساسية ) ردود الفعل
الحساسية(.
• النعاس.
• فقدان الصوت.
• انهيار الدورة الدموية الحاد.
• احمرار الجلد ) الحمامية(.
• التهاب الجلد ) التهاب الجلد(.
• الحكة ) الحكة(.
• طفح جلدي ) انتفاخ اكسانثيما
البقعي(.
• التعرق المفرط ) فرط التعرق(.
نادر جدا:
• التهاب غير نمطي أولي في
الرئتين ) الالتهاب الرئوي(
• كسر خلايا الدم الحمراء
• انخفاض سريع في ضغط الدم
في بعض الأحيان مع ردود
فعل الجلد أو الطفح الجلدي
)صدمة الحساسية(
• الشعور المضطرب بالذوق
• الأحاسيس المتغيرة ) الشلل(
• الشعور بالضيق والألم في
الأطراف ) اعتلال الأعصاب
المحيطية(
• مرض الجهاز العصبي
)متلازمة مضادة للكولين(
• الاضطرابات العصبية
• عدم التنسيق ) ترنح(
• التهاب الدماغ ) التهاب
الدماغ(
• زيادة معدل ضربات القلب
)عدم دقات القلب(
• نوبة قلبية، ألم في الصدر
)احتشاء عضلة القلب(
• قصور القلب
• التهاب الأوردة ) التهاب
البلبلة(
• تكوين الأنسجة في الرئتين
)تليف الرئتين(
• نزيف التهاب في القناة
الهضمية ) التهاب المريء
النزفي(
• نزيف المعدة أو الأمعاء
• العقم
• فشل الجهاز متعددة
كانت هناك تقارير عن الأورام الثانوية ) متلازمة خلل التنسج النخاعي
العلاج مع بيندوكي. لا يمكن تحديد علاقة واضحة مع بيندوكي.
تم الإبلاغ عن عدد قليل من حالات ردود الفعل الجلدية الشديدة ) متلازمة ستيفنز جونسون وانحلال البشرة
السام(. العلاقة مع بيندوكي غير واضحة.
إذا كان أي من الآثار الجانبية يحصل خطيرة، أو إذا لاحظت أي آثار جانبية غير مدرجة في هذا المنشور، يرجى إخبار طبيبك.
الابتعاد عن متناول وبصر الأطفال. يخزن تحت 30 درجة مئوية.
لا تستخدم بيندوكي بعد تاريخ انتهاء الصلاحية الذي ورد على الملصق والكرتون. يشير تاريخ انتهاء
الصلاحية إلى اليوم الأخير من ذلك الشهر.
احتفظ بالحاوية في الكرتون الخارجي لحماية المحتوى من الضوء.
الصلاحية:
24 شهرا.
يجب إعادة تشكيل المسحوق مباشرة بعد فتح القارورة.
.٪ يجب تخفيف التركيز المعاد تشكيله على الفور بمحلول كلوريد الصوديوم بنسبة 0.9
حل للتسريب
بعد إعادة التشكيل والتخفيف، تم إثبات الاستقرار الكيميائي والمادي لمدة 3.5 ساعة عند 25 درجة مئوية
و 48 ساعة عند 2 درجة مئوية إلى 8 درجات مئوية في أكياس البولي إيثيلين. RH ٪ و 60
من وجهة نظر مكروبيولوجية، يجب استخدام الحل على الفور. إذا لم يتم استخدامها على الفور، فإن أوقات
التخزين في الاستخدام وشروطه قبل الاستخدام هي مسؤولية المستخدم.
المادة الفعالة هي هيدروكلوريد بينداموستين.
1 قارورة تحتوي على 25 ملغ من هيدروكلوريد بينداموستين 1 قارورة يحتوي على 100 ملغ من
هيدروكلوريد بينداموستين
بعد إعادة تشكيل 1 مل من التركيز يحتوي على 2.5 ملغ بينداموستين هيدروكلوريد.
العنصر الآخر هو مانيتول.
ب. كيف يبدو هذا المنتج ومحتويات الحزمة:
قارورة زجاجية بنية اللون مع سدادة مطاطية وغطاء من الألومنيوم. يبدو المسحوق أبيض وبلوري. بيندوكي
متاح في حزم تحتوي على 5 و 10 و 20 قنينة حقن مع 25 ملغ من هيدروكلوريد بينداموستين و 5 قنينات
حقن مع 100 ملغ من هيدروكلوريد بينداموستين. قد لا تتوفر كافة أحجام الحزم.
حامل تفويض التسويق
شركة يوجيا فارما للتخصصات المحدودة ) شركة تابعة مملوكة بالكامل لشركة أوروبيندو فارما المحدودة(
)شركة تابعة مملوكة بالكامل لشركة أوروبندو فارما المحدودة(،
المؤامرة رقم: 2، مايتريفيهار ،
،038 أميربيت، حيدر أباد- 500
ولاية تيلانغانا، الهند.
First-line treatment of chronic lymphocytic leukaemia (Binet stage B or C) in patients for whom fludarabine combination chemotherapy is not appropriate.
Indolent non-Hodgkin's lymphomas as monotherapy in patients who have progressed during or within 6 months following treatment with rituximab or a rituximab containing regimen.
Front line treatment of multiple myeloma (Durie-Salmon stage II with progress or stage III) in combination with prednisone for patients older than 65 years who are not eligible for autologous stem cell transplantation and who have clinical neuropathy at time of diagnosis precluding the use of thalidomide or bortezomib containing treatment.
Posology
Monotherapy for chronic lymphocytic leukaemia
100 mg/m² body surface area Bendamustine hydrochloride on days 1 and 2; every 4 weeks up to 6 times.
Monotherapy for indolent non-Hodgkin's lymphomas refractory to rituximab
120 mg/m² body surface area Bendamustine hydrochloride on days 1 and 2; every 3 weeks for at least 6 times.
Multiple myeloma
120 - 150 mg/m² body surface area Bendamustine hydrochloride on days 1 and 2, 60 mg/m² body surface area prednisone i.v. or per os on days 1 to 4; every 4 weeks for at least 3 times.
Hepatic impairment
On the basis of pharmacokinetic data, no dose adjustment is necessary in patients with mild hepatic impairment (serum bilirubin < 1.2mg/dl). A 30% dose reduction is recommended in patients with moderate hepatic impairment (serum bilirubin 1.2 - 3.0 mg/dl).
No data is available in patients with severe hepatic impairment (serum bilirubin values of > 3.0 mg/dl) (see section 4.3).
Renal impairment
On the basis of pharmacokinetic data, no dose adjustment is necessary in patients with a creatinine clearance of > 10 mL/min. Experience in patients with severe renal impairment is limited.
Paediatric population
The safety and efficacy of Bendamustine hydrochloride in children have not yet been established. Current available data is not sufficient to make a recommendation on posology.
Elderly patients
There is no evidence that dose adjustments are necessary in elderly patients (see also section 5.2).
Method of administration
For intravenous infusion over 30 - 60 minutes (see section 6.6).
Infusion must be administered under the supervision of a physician qualified and experienced in the use of chemotherapeutic agents.
Poor bone marrow function is related to increased chemotherapy-induced haematological toxicity. Treatment should not be started if leukocyte and/or platelet values dropped to < 3,000/µl or < 75,000/µl, respectively (see section 4.3).
Treatment should be terminated or delayed if leukocyte and/or platelet values dropped to < 3,000/µl or < 75,000/µl, respectively. Treatment can be continued after leukocyte values have increased to > 4,000/µl and platelet values to > 100,000/µl.
The leukocyte and platelet Nadir is reached after 14-20 days with regeneration after 3-5 weeks. During therapy free intervals strict monitoring of the blood count is recommended (see section 4.4).
In case of non-haematological toxicity dose reductions have to be based on the worst CTC grades in the preceding cycle. A 50% dose reduction is recommended in case of CTC grade 3 toxicity. An interruption of treatment is recommended in case of CTC grade 4 toxicity.
If a patient requires a dose modification the individually calculated reduced dose must be given on day 1 and 2 of the respective treatment cycle.
For instructions on reconstitution of the medicinal product before administration, see section 6.6.
Yellow fever vaccination
Myelosuppression
Patients treated with Bendamustine hydrochloride may experience myelosuppression. In the event of treatment-related myelosuppression, leukocytes, platelets, haemoglobin, and neutrophils must be monitored at least weekly. Prior to the initiation of the next cycle of therapy, the following parameters are recommended: Leukocyte and/or platelet values > 4,000/µl or > 100,000/µl, respectively.
Infections
Serious and fatal infections have occurred with Bendamustine hydrochloride, including bacterial (sepsis, pneumonia) and opportunistic infections such as Pneumocystis jirovecii pneumonia (PJP), varicella zoster virus (VZV) and cytomegalovirus (CMV). Treatment with Bendamustine hydrochloride may cause prolonged lymphocytopenia (< 600/μl) and low CD4-positive T-cell (T-helper cell) counts (< 200/μl) for at least 7–9 months after the completion of treatment.
Lymphocytopenia and CD4-positive T-cell depletion are more pronounced when Bendamustine is combined with rituximab Patients with lymphopenia and low CD4-positive T-cell count following treatment with Bendamustine hydrochloride are more susceptible to (opportunistic) infections. In case of low CD4-positive T-cell counts (< 200/μl) Pneumocystis jirovecii pneumonia (PJP) prophylaxis should be considered. All patients should be monitored for respiratory signs and symptoms throughout treatment. Patients should be advised to report new signs of infection, including fever or respiratory symptoms promptly. Discontinuation of Bendamustine hydrochloride should be considered if there are signs of (opportunistic) infections.
Hepatitis B reactivation
Reactivation of hepatitis B in patients who are chronic carriers of this virus has occurred after these patients received Bendamustine hydrochloride. Some cases resulted in acute hepatic failure or a fatal outcome. Patients should be tested for HBV infection before initiating treatment with Bendamustine hydrochloride. Experts in liver disease and in the treatment of hepatitis B should be consulted before treatment is initiated in patients with positive hepatitis B tests (including those with active disease) and for patients who test positive for HBV infection during treatment. Carriers of HBV who require treatment with Bendamustine hydrochloride should be closely monitored for signs and symptoms of active HBV infection throughout therapy and for several months following termination of therapy (see section 4.8).
Skin reactions
A number of skin reactions have been reported. These events have included rash, severe cutaneous reactions and bullous exanthema. Cases of Stevens – Johnson syndrome (SJS) and Toxic Epidermal Necrolysis (TEN) and Drug Reaction with Eosinophilia and Systemic Symptoms (DRESS), some fatal, have been reported with the use of Bendamustine hydrochloride. 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. Some events occurred when Bendamustine hydrochloride was given in combination with other anticancer agents, so the precise relationship is uncertain. When skin reactions occur, they may be progressive and increase in severity with further treatment. If skin reactions are progressive, Bendamustine should be withheld or discontinued. For severe skin reactions with suspected relationship to Bendamustine hydrochloride, treatment should be discontinued.
Cardiac disorders
During treatment with Bendamustine hydrochloride the concentration of potassium in the blood of patients with cardiac disorders must be closely monitored and potassium supplement must be given when K+ <3.5 mEq/l and ECG measurement must be performed.
Fatal cases of myocardial infarction and cardiac failure have been reported with Bendamustine hydrochloride treatment. Patients with concurrent or history of cardiac disease should be observed closely.
Nausea, vomiting
An antiemetic may be given for the symptomatic treatment of nausea and vomiting.
Tumour lysis syndrome
Tumour lysis syndrome (TLS) associated with Bendamustine treatment has been reported in patients in clinical trials. The onset tends to be within 48 hours of the first dose of Bendamustine and, without intervention, may lead to acute renal failure and death. Preventive measures such as adequate hydration, close monitoring of blood chemistry, particularly potassium and uric acid levels and the use of hypouricemic agents (allopurinol and rasburicase) should be considered prior to therapy. There have been a few cases of Stevens-Johnson Syndrome and Toxic Epidermal Necrolysis reported when Bendamustine and allopurinol were administered concomitantly.
Anaphylaxis
Infusion reactions to Bendamustine hydrochloride have occurred commonly in clinical trials. Symptoms are generally mild and include fever, chills, pruritus and rash. In rare instances severe anaphylactic and anaphylactoid reactions have occurred. Patients must be asked about symptoms suggestive of infusion reactions after their first cycle of therapy. Measures to prevent severe reactions, including antihistamines, antipyretics and corticosteroids must be considered in subsequent cycles in patients who have previously experienced infusion reactions.
Patients who experienced Grade 3 or worse allergic-type reactions were typically not re-challenged.
Contraception
Bendamustine hydrochloride is teratogenic and mutagenic.
Women should not become pregnant during treatment. Male patients should not father a child during and up to 6 months after treatment. They should seek advice about sperm conservation prior to treatment with Bendamustine hydrochloride because of possible irreversible infertility.
Extravasation
An extravasal injection should be stopped immediately. The needle should be removed after a short aspiration. Thereafter the affected area of tissue should be cooled. The arm should be elevated. Additional treatments like the use of corticosteroids are not of clear benefit.
No in-vivo interaction studies have been performed.
When Bendamustine is combined with myelosuppressive agents, the effect of Bendamustine and/or the co-administered medicinal products on the bone marrow may be potentiated. Any treatment reducing the patient's performance status or impairing bone marrow function can increase the toxicity of Bendamustine.
Combination of Bendamustine with cyclosporine or tacrolimus may result in excessive immunosuppression with risk of lymphoproliferation.
Cytostatics can reduce antibody formation following live-virus vaccination and increase the risk of infection which may lead to fatal outcome. This risk is increased in subjects who are already immunosuppressed by their underlying disease.
Bendamustine metabolism involves cytochrome P450 (CYP) 1A2 isoenzyme (see section 5.2). Therefore, the potential for interaction with CYP1A2 inhibitors such as fluvoxamine, ciprofloxacin, acyclovir and cimetidine exists.
Paediatric population
Interaction studies have only been performed in adults.
Pregnancy
There are insufficient data from the use of Bendamustine in pregnant women. In nonclinical studies Bendamustine hydrochloride was embryo-/fetolethal, teratogenic and genotoxic (see section 5.3). During pregnancy Bendamustine should not be used unless clearly necessary. The mother should be informed about the risk to the foetus. If treatment with Bendamustine is absolutely necessary during pregnancy or if pregnancy occurs during treatment, the patient should be informed about the risks for the unborn child and be monitored carefully. The possibility of genetic counselling should be considered.
Fertility
Women of childbearing potential must use effective methods of contraception both before and during Bendamustine therapy.
Men being treated with Bendamustine are advised not to father a child during and for up to 6 months following cessation of treatment. Advice on conservation of sperm should be sought prior to treatment because of the possibility of irreversible infertility due to therapy with Bendamustine.
Breast feeding
It is not known whether Bendamustine passes into the breast milk, therefore, Bendamustine is contraindicated during breast feeding (see section 4.3). Breast feeding must be discontinued during treatment with Bendamustine.
Bendamustine has major influence on the ability to drive and use machines. Ataxia, peripheral neuropathy and somnolence have been reported during treatment with Bendamustine (see section 4.8). Patients should be instructed that if they experience these symptoms they should avoid potentially hazardous tasks such as driving and using machines.
Summary of the safety profile
The most common adverse reactions with Bendamustine hydrochloride are hematological adverse reactions (leukopenia, thrombopenia), dermatologic toxicities (allergic reactions), constitutional symptoms (fever), gastrointestinal symptoms (nausea, vomiting).
The table below reflects the data obtained with Bendamustine hydrochloride.
Table 1: Adverse reactions in patients treated with Bendamustine hydrochloride.
Very common ≥1/10 | Common ≥1/100 to <1/10 | Uncommon ≥1/1,000 to <1/100 | Rare ≥1/10,000 to <1/1, 000 | Very rare <1/10, 000 | Not known (cannot be estimated from the available data) | MedDRA system organ class |
| |
Infection NOS Including Opportunistic infection (e.g. Herpes zoster, cytomegalovirus, hepatitis B) |
| Pneumocystis jirovecii pneumonia | Sepsis | Pneumonia primary atypical |
| Infections and infestations |
| |
| Tumour lysis syndrome | Myelodysplastic syndrome, acute myeloid leukemia |
|
|
| Neoplasma benign, malignant and unspecified (including cyst and polyp) |
| |
Leukopenia NOS, Thrombocytopenia Lymphopenia | Haemorrhage, Anaemia, Neutropenia | Pancytopenia | Bone marrow failure | Haemolysis |
| Blood and lymphatic system disorders |
| |
| Hypersensitivity NOS |
| Anaphylactic reaction, Anaphylactoid reaction | Anaphylactic shock |
| Immune system disorders |
| |
Headache | Insomnia Dizziness |
| Somnolence, Aphonia | Dysgeusia, Paraesthesia, Peripheral sensory neuropathy, Anticholinergic syndrome, Neurological disorders, Ataxia, Encephalitis |
| Nervous system disorders |
| |
| Cardiac dysfunction, such as palpitations, angina pectoris, Arrhythmia | Pericardial effusion Myocardial infarction, Cardiac failure |
| Tachycardia | Atrial fibrillation | Cardiac disorders |
| |
| Hypotension, Hypertension |
| Acute circulatory failure | Phlebitis |
| Vascular disorders |
| |
| Pulmonary dysfunction |
|
| Pulmonary fibrosis | Pneumonitis Pulmonary alveolar haemorrhage | Respiratory, thoracic and media-stinal disorders |
| |
Nausea, Vomiting | Diarrhoea, Constipation, Stomatitis |
|
| haemorrhagic oesophagitis, Gastrointestinal haemorrhage |
| Gastrointestinal disorders |
| |
| Alopecia, Skin disorders NOS Urticaria |
| Erythema, Dermatitis, Pruritus, Maculopapular Rash, Hyperhidrosis |
| Stevens – Johnson syndrome, Toxic Epidermal Necrolysis (TEN) Drug reaction with eosinophilia and systemic symptoms (DRESS)* | Skin and subcutaneous tissue disorders |
NOS = Not otherwise specified (*=combination therapy with rituximab)
Description of selected adverse reactions There have been isolated reports of necrosis after accidental extra-vascular administration and tumour lysis syndrome, and anaphylaxis. The risk of myelodysplastic syndrome and acute myeloid leukaemias is increased in patients treated with alkylating agents (including Bendamustine). The secondary malignancy may develop several years after chemotherapy has been discontinued.
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. To report any side effects Saudi Arabia:
|
After application of a 30 min infusion of Bendamustine once every 3 weeks the maximum tolerated dose (MTD) was 280 mg/m². Cardiac events of CTC grade 2 which were compatible with ischaemic ECG changes occurred which were regarded as dose limiting.
In a subsequent study with a 30 min infusion of Bendamustine at day 1 and 2 every 3 weeks the MTD was found to be 180 mg/m2. The dose limiting toxicity was grade 4 thrombocytopenia. Cardiac toxicity was not dose limiting with this schedule.
Counter measures
There is no specific antidote. Bone marrow transplantation and transfusions (platelets, concentrated erythrocytes) may be made or haematological growth factors may be given as effective countermeasures to control haematological side effects.
Bendamustine hydrochloride and its metabolites are dialyzable to a small extent.
Pharmacotherapeutic group: Antineoplastic agents, alkylating agents.
ATC code: L01AA09
Bendamustine hydrochloride is an alkylating antitumour agent with unique activity. The antineoplastic and cytocidal effect of Bendamustine hydrochloride is based essentially on a cross-linking of DNA single and double strands by alkylation. As a result, DNA matrix functions and DNA synthesis and repair are impaired. The antitumour effect of Bendamustine hydrochloride has been demonstrated by several in vitro studies in different human tumour cell lines (breast cancer, non-small cell and small cell lung cancer, ovarian carcinoma and different leukaemia) and in vivo in different experimental tumour models with tumours of mouse, rat and human origin (melanoma, breast cancer, sarcoma, lymphoma, leukaemia and small cell lung cancer).
Bendamustine hydrochloride showed an activity profile in human tumour cell lines different to that of other alkylating agents. The active substance revealed no or very low cross-resistance in human tumour cell lines with different resistance mechanisms at least in part due to a comparatively persistent DNA interaction. Additionally, it was shown in clinical studies that there is no complete cross-resistance of Bendamustine with anthracyclines, alkylating agents or rituximab. However, the number of assessed patients is small.
Chronic lymphocytic leukaemia
The indication for use in chronic lymphocytic leukaemia is supported by a single open label study comparing Bendamustine with chlorambucil. In the prospective, multi-centre, randomised study, 319 previously untreated patients with chronic lymphocytic leukaemia stage Binet B or C requiring therapy were included. The first line therapy with Bendamustine hydrochloride 100 mg/m² i.v. on days 1 and 2 (BEN) was compared to treatment with chlorambucil 0.8 mg/kg days 1 and 15 (CLB) for 6 cycles in both arms. Patients received allopurinol in order to prevent tumour lysis syndrome.
Patients with BEN had a significantly longer median progression free survival than patients with CLB treatment (21.5 versus 8.3 months, p < 0.0001 in the latest follow-up). Overall survival was not statistically significantly different (median not reached). The median duration of remission was 19 months with BEN and 6 months with CLB treatment (p < 0.0001). The safety evaluation in both treatment arms did not reveal any unexpected undesirable effects in nature and frequency. The dose of BEN was reduced in 34% of the patients. Treatment with BEN was discontinued in 3.9% of patients due to allergic reactions.
Indolent non-Hodgkin's lymphomas
The indication for indolent non-Hodgkin's lymphomas relied on two uncontrolled phase II trials.
In the pivotal prospective, multi-centre, open study 100 patients with indolent B-cell non-Hodgkin´s lymphomas refractory to rituximab mono- or combination therapy were treated with BEN single agent. Patients had received a median of 3 previous chemotherapy or biological therapy courses. The median number of previous rituximab-containing courses was 2. The patients had had no response or there had been progression within 6 months after rituximab treatment. The dose of BEN was 120 mg/m² i.v. on days 1 and 2 planned for at least 6 cycles. Duration of treatment depended on response (6 cycles planned). The overall response rate was 75% including 17% complete (CR and CRu) and 58% partial response as assessed by independent review committee. The median duration of remission was 40 weeks. BEN was generally well tolerated when given in this dose and schedule.
The indication is further supported by another prospective, multi-centre, open study including 77 patients. The patient population was more heterogeneous including: indolent or transformed B-cell non-Hodgkin's lymphomas refractory to rituximab mono- or combination therapy. The patients had no response or there had been progression within 6 months or had had an untoward reaction to prior rituximab treatment. Patients had received a median of 3 previous chemotherapy or biological therapy courses. The median number of previous rituximab-containing courses had been 2. The overall response rate was 76% with a median duration of response of 5 months (29 [95% CI 22.1, 43.1] weeks).
Multiple myeloma
In a prospective, multi-centre, randomised, open study 131 patients with advanced multiple myeloma (Durie-Salmon stage II with progression or stage III) were included. The first line therapy with Bendamustine hydrochloride in combination with prednisone (BP) was compared to treatment with melphalan and prednisone (MP). Tolerability in both treatment arms was in line with the known safety profile of the respective medicinal products with significantly more dose reductions in the BP arm. The dose was Bendamustine hydrochloride 150 mg/m² i.v. on days 1 and 2 or melphalan 15 mg/m² i.v. on day 1 each in combination with prednisone. Duration of treatment depended on response and averaged 6.8 cycles in the BP and 8.7 cycles in the MP group.
Patients with BP treatment had a longer median progression free survival than patients with MP (15 [95% CI 12-21] versus 12 [95% CI 10-14] months) (p=0.0566). The median time to treatment failure was 14 months with BP and 9 months with MP treatment. The duration of remission was 18 months with BP and 12 months with MP treatment. The difference in overall survival was not significantly different (35 months BP versus 33 months MP). Tolerability in both treatment arms was in line with the known safety profile of the respective medicinal products with significantly more dose reductions in the BP arm.
Distribution
The elimination half-life t1/2ß after 30 min i.v. infusion of 120 mg/m2 area to 12 subjects was 28.2 minutes.
Following 30 min i.v. infusion the central volume of distribution was 19.3 l. Under steady-state conditions following i.v. bolus injection the volume of distribution was 15.8-20.5 l.
More than 95% of the substance is bound to plasma proteins (primarily albumin).
Biotransformation
A major route of clearance of Bendamustine is the hydrolysis to monohydroxy- and dihydroxy-Bendamustine. Formation of N-desmethyl-Bendamustine and gamma-hydroxy-Bendamustine by hepatic metabolism involves cytochrome P450 (CYP) 1A2 isoenzyme. Another major route of Bendamustine metabolism involves conjugation with glutathione.
In-vitro Bendamustine does not inhibit CYP 1A4, CYP 2C9/10, CYP 2D6, CYP 2E1 or CYP 3A4.
Elimination
The mean total clearance after 30 min i.v. infusion of 120 mg/m2 body surface area to 12 subjects was 639.4 mL/minute. About 20% of the administered dose was recovered in urine within 24 hours. Amounts excreted in urine were in the order monohydroxy-Bendamustine > Bendamustine > dihydroxy-Bendamustine > oxidised metabolite > N-desmethyl Bendamustine. In the bile, primarily polar metabolites are eliminated.
Hepatic impairment
In patients with 30 - 70% tumour infestation of the liver and mild hepatic impairment (serum bilirubin < 1.2 mg/dl) the pharmacokinetic behaviour was not changed. There was no significant difference to patients with normal liver and kidney function with respect to Cmax, tmax, AUC, t1/2ß , volume of distribution and clearance. AUC and total body clearance of Bendamustine correlate inversely with serum bilirubin.
Renal impairment
In patients with creatinine clearance > 10 mL/min including dialysis dependent patients, no significant difference to patients with normal liver and kidney function was observed with respect to Cmax, tmax, AUC, t1/2ß, volume of distribution and clearance.
Elderly subjects
Subjects up to 84 years of age were included in pharmacokinetic studies. Higher age does not influence the pharmacokinetics of Bendamustine
Adverse reactions not observed in clinical studies, but seen in animals at exposure levels similar to clinical exposure levels and with possible relevance to clinical use were as follows:
Histological investigations in dogs showed macroscopic visible hyperaemia of the mucosa and haemorrhagia in the gastrointestinal tract. Microscopic investigations showed extensive changes of the lymphatic tissue indicating an immunosuppression and tubular changes of kidneys and testis, as well as atrophic, necrotic changes of the prostate epithelium.
Animal studies showed that Bendamustine is embryotoxic and teratogenic.
Bendamustine induces aberrations of the chromosomes and is mutagenic in vivo as well as in vitro. In long-term studies in female mice Bendamustine is carcinogenic.
Mannitol
Tertiary Butanol
This medicinal product must not be mixed with other medicinal products except those mentioned in section 6.6.
Store below 30°C.
Keep the vial in the outer carton in order to protect from light.
For storage conditions of the reconstituted or diluted medicinal product, see section 6.3.
Type I Amber glass vials of 26 mL or 60 mL with rubber stopper and an aluminium flip-off cap.
Pack of 1 vial.
When handling Bendamustine, inhalation, skin contact or contact with mucous membranes should be avoided (wear gloves and protective clothes!). Contaminated body parts should be carefully rinsed with water and soap, the eyes should be rinsed with physiological saline solution. If possible it is recommended to work on special safety workbenches (laminar flow) with liquid-impermeable, absorbent disposable foil. Pregnant personnel should be excluded from handling cytostatics.
The powder for concentrate for solution for infusion has to be reconstituted with water for injection, diluted with sodium chloride 9 mg/mL (0.9%) solution for injection and then administered by intravenous infusion. Aseptic technique is to be used.
1. Reconstitution
Reconstitute each vial of Bendamustine containing 25 mg Bendamustine hydrochloride in 10 mL water for injection by shaking;
Reconstitute each vial of Bendamustine containing 100 mg Bendamustine hydrochloride in 40 mL water for injection by shaking.
The reconstituted concentrate contains 2.5 mg Bendamustine hydrochloride per mL and appears as a clear colourless solution.
2. Dilution
As soon as a clear solution is obtained dilute the total recommended dose of Bendamustine immediately with 0.9% NaCl solution to produce a final volume of about 500 mL.
Bendamustine must be diluted with 0.9% NaCl solution and not with any other injectable solution.
3. Administration
The solution is administered by intravenous infusion over 30-60 min.
The vials are for single use only.
Any unused product or waste material should be disposed of in accordance with local requirements.
