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نشرة الممارس الصحي | نشرة معلومات المريض بالعربية | نشرة معلومات المريض بالانجليزية | صور الدواء | بيانات الدواء |
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SOPORIDEX contains an active substance called dexmedetomidine, which belongs to a medicine group called sedatives. It is used to provide sedation (a state of calm, drowsiness or sleep) for adult patients in hospital intensive care settings or awake sedation during different diagnostic or surgical procedures.
You must not be given SOPORIDEX:
- if you are allergic to dexmedetomidine or any of the other ingredients of this medicine (listed in section 6).
- if you have some disorders of heart rhythm (heart block grade 2 or 3).
- if you have very low blood pressure which does not respond to treatment.
- if you have recently had a stroke or other serious condition affecting blood supply to the brain.
Warnings and precautions
Before you are given this medicine, tell your doctor or nurse if any of the following apply as SOPORIDEX should be used cautiously:
- if you have an abnormally slow heart rate (either due to illness or high levels of physical fitness)
- if you have low blood pressure
- if you have low blood volume, for example after bleeding
- if you have certain heart disorders
- if you are elderly
- if you have a neurological disorder (for instance head or spinal cord injury or stroke)
- if you have severe liver problems
- if you have ever developed a serious fever after some medicines, especially anesthetics
Other medicines and SOPORIDEX
Tell your doctor or nurse if you are taking, have recently taken or might take any other medicines.
The following medicines may enhance the effect of SOPORIDEX:
- medicines that help you sleep or cause sedation (e.g. midazolam, propofol)
- strong pain medicines (e.g. opioids such as morphine, codeine)
- anesthetic medicines (e.g. sevoflurane, isoflurane)
If you are using medicines, which lower your blood pressure and heart rate, co-administration with SOPORIDEX may enhance this effect. SOPORIDEX should not be used with medicines that cause temporary paralysis.
Pregnancy and breast-feeding
SOPORIDEX should not be used during pregnancy or breast-feeding unless clearly necessary.
Ask your doctor for advice before having this medicine.
Driving and using machines
SOPORIDEX has major impact on the ability to drive and use machines.
After you have been given SOPORIDEX you must not drive, operate machinery, or work in dangerous situations. Ask your doctor when you can start doing these activities again and when you can go back to this kind of work.
SOPORIDEX contains sodium
Each ml of SOPORIDEX contains less than 1 mmol (approximately 3.5 mg) sodium.
Hospital intensive care
SOPORIDEX is administered to you by a doctor or nurse in hospital intensive care.
Procedural sedation/awake sedation
SOPORIDEX is administered to you by a doctor or nurse prior to and/or during diagnostic or surgical procedures requiring sedation, i.e. procedural/awake sedation.
Your doctor will decide on a suitable dose for you. The amount of SOPORIDEX depends on your age, size, general condition of health, the level of sedation needed and how you respond to the medicine. Your doctor may change your dose if needed and will monitor your heart and blood pressure during the treatment.
SOPORIDEX is diluted and it is given to you as an infusion (drip) into your veins.
After sedation/wake-up
· The doctor will keep you under medical supervision for some hours after the sedation to make sure that you feel well.
· You should not go home unaccompanied.
· Medicines to help you sleep, cause sedation or strong painkillers may not be appropriate for some time after you have been given SOPORIDEX. Talk to your doctor about the use of these medicines and about the use of alcohol.
If you have been given more SOPORIDEX than you should
If you are given too much SOPORIDEX, your blood pressure may drop, your heartbeat may slow down and you may feel more drowsy. Your doctor will know how to treat you based on your condition.
If you have any further questions on the use of this medicine, ask your doctor.
Like all medicines, this medicine can cause side effects, although not everybody gets them.
Very common (affects more than 1 user in 10)
- slow heart rate
- low or high blood pressure
- change in breathing pattern or stopping breathing
Common (affects 1 to 10 users in 100)
- chest pain or heart attack
- fast heart rate
- low or high blood sugar
- nausea, vomiting or dry mouth
- restlessness
- symptoms after stopping the medicine
- high temperature
Uncommon (affects 1 to 10 users in 1,000)
- a condition where there is too much acid in the body
- low albumin level in blood
- hallucinations
- reduced heart function
- shortness of breath and transient cessation of respiration
- the medicine is not effective enough.
- swelling of the stomach
- thirst
Not known (frequency cannot be estimated from the available data)
- increased need to pass urine
Reporting of side effects
If you get any side effects, talk to your doctor, pharmacist, or nurse. This includes any possible side effects not listed in this leaflet. By reporting side effects you can help provide more information on the safety of this medicine.
To report any side effect(s):
Saudi Arabia
The National Pharmacovigilance and Drug Safety Centre (NPC)
- Fax: +966-11-205-7662
- Call NPC at +966-11-2038222, Exts: 2317-2356-2353-2354-2334-2340.
- Toll free phone: 8002490000
- E-mail: npc.drug@sfda.gov.sa
- Website: www.sfda.gov.sa/npc
Other GCC States
Please contact the relevant competent authority
Keep this medicine out of the sight and reach of children.
Do not use this medicine after the expiry date, which is stated on the label and carton after EXP.
Store below 30 °C. Keep the vials in the outer carton in order to protect from light.
- The active substance is dexmedetomidine.
- Each ml of concentrate contains dexmedetomidine hydrochloride equivalent to 100 micrograms dexmedetomidine.
- The other ingredients are sodium chloride and water for injections.
Each 2 ml vial contains 200 micrograms of dexmedetomidine (as hydrochloride).
Each 4 ml vial contains 400 micrograms of dexmedetomidine (as hydrochloride).
Each 10 ml vial contains 1000 micrograms of dexmedetomidine (as hydrochloride).
The concentration of the final solution after dilution should be either 4 micrograms/ml or 8 micrograms/ml.
Marketing Authorisation Holder:
EVER Valinject GmbH
Oberburgau 3
4866 Unterach am Attersee
Austria
Manufacturer:
EVER Pharma Jena GmbH
Otto-Schott-Strasse 15
07745 Jena
Germany
For any information about this medicinal product, please contact the local representative of the Marketing Authorisation Holder:
Cigalah Group
P.O.Box 50622
11533 Riyadh
Saudi Arabia
يحتوي سوبوريديكس على مادة فعالة تسمى دكسميديتوميدين، وهي تنتمي إلى المجموعة الطبية التي تسمى المسكنات. وتستعمل للتخدير (حالة من الهدوء أو النعاس أو النوم) للبالغين من المرضى في قسم العناية المركزة بالمستشفيات أو التخدير الواعي أثناء مختلف حالات التشخيص أو الإجراءات الجراحية.
لا يستعمل سوبوريديكس في الحالات التالية:" | |
- | الحساسية ضد سوبوريديكس أو ضد أي من العناصر الأخرى المكونة لهذا الدواء والواردة في القسم رقم "6" أدناه من هذه النشرة. |
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- | إضطرابات نظم القلب (إحصار القلب من الدرجة الثانية أو الثالثة). |
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- | الانخفاض الشديد في ضغط الدم الذي لا يستجيب للعلاج. |
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- | التعرض لأي جلطة قبل فترة وجيزة من الزمن أو اي حالة خطرة تؤثر على تدفق الدم إلى الدماغ. |
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| قبل تناول هذا الدواء يجب تبليغ الطبيب أو الممرض بوجود أي مما يلي ذكره، حيث يجب توخي الحيطة والحذر عندما تستعمل معها سوبوريديكس: |
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- | إنخفاض في ضغط الدم. |
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- | إنخفاض كمية الدم، مثل في حالة النزيف. |
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- | بعض اضطرابات القلب. |
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- | تقدم العمــر. |
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- | الاضطرابات العصبية (مثلا إصابة الرأس أو النخاع الشوكي أو الجلطة). |
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- | مشاكل الكبد الحادة. |
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- | الإصابة بحمى خطرة بعد تناول بعض الأدوية وخاصة أدوية التخدير. |
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سوبوريديكس والأدوية الأخرى: | |
يجب تبليغ الطبيب في حالة تناول أدوية أخرى مؤخرا أو احتمال تناولها. | |
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| الأدوية المذكورة أدناه قد تقوي من مفعول سوبوريديكس: |
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- | الأدوية المساعدة للنوم أو المسببة للتخدير، مثل: ميدازولم و بروبوفول. |
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- | أدوية الألم الشديد. |
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- | الأدوية المخدرة، مثل: سيفوفلورين و إيسوفلورين. |
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في حالة تناول أي من الأدوية المؤدية إلى تخفيض ضغط الدم أو معدل ضربات القلب، فإنها استخدامها مع سوبوريديكس قد يزيد من مفعول هذا الأثر. ويجب عدم استعمال سوبوريديكس مع الأدوية المسببة للشلل المؤقت. | |
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الحمــل والرضــاعة: | |
لا يستعمل سوبوريديكس أثناء فترة الحمل والرضاعة ما لم تستدعي الضرورة الملحة ذلك. ويجب استشارة الطبيب قبل تناول هذا الدواء. | |
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القيــادة وتشغيل الآليات: | |
يؤثر سوبوريديكس تأثيرا كبيرا على القدرة على قيادة السيارات وتشغيل الآليات. وبعـد تناول سوبوريديكس يجب عدم قيادة السيارات وعدم تشغيل الآليات وكذلك عدم ممارسة أي عمل في الأوضاع الخطرة. ويجب استشارة الطبيب عن متى يمكن استئناف مزوالة تلك النشاطات ومتى يمكن العودة لمثل هذا النوع من العمل. | |
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سوبوريديكس يحتوي على الصوديوم | |
كل ملتر من سوبوريديكس يحتوي على أقل من ملتر (تقريبا 3.5 ملجرام) من الصوديوم. |
العناية المركزة في المستشفى |
يُصرف سوبوريديكس للمريض بواسطة الطبيب أو الممرض في مستشفى العناية المركزة. |
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التخدير الإجرائي/التخدير مع اليقظة |
يُعطى سوبوريديكس للمريض بواسطة الطبيب أو الممرض قبل الإجراءات التشخيصية أو الجراحية أو أثنائها عندما تتطلب تلك الإجراءات الخدير، وذلك مثل التخدير الإجرئي أو التخدير مع اليقظة. |
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يحدد الطبيب الجرعة المناسبة للمريض. وتعتمد كمية الجرعة على عمر المريض وحجمه وحالته الصحية ومستوى التخدير المطلوب، واستجابه المريض للدواء. وقد يعدل الطبيب الجرعة المقررة للمريض في حالة الضرورة، وأنه سوف يراقب القلب وضغط الدم للمريض أثناء العلاج. |
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يتم تخفيف سوبوريديكس ، ويعطى بالحقن بواسطة الدرب من خلال الوريد. |
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بعــد التخدير/اليقظــة: |
يظل المريض تحت المراقبة الطبية من الطبيب لبعض الساعات بعد التخدير للتأكيــد من أنه بحالة جيدة. |
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لا يذهب المريض إلى منزله دون مرافق له. |
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من المستحسن عدم تناول الأدوية المنومة والمخدرة المسكنة للآلام لفترة من الزمن بعد تناول سوبوريديكس. ويجب التحدث مع الطبيب بخصوص استعمال تلك الأدوية وعن تعاطي الكحول. |
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إعطاء جرعــة زائدة من سوبوريديكس: |
إعطاء جرعة زائدة من سوبوريديكس يؤدي إلى إنخفاض ضغط الدم وكذلك إنخفاض ضربات القلب، وقد يشعر المريض بالنعاس. ويعرف الطبيب طريقة العلاج حسب حالة المريض. |
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توجه إلى الطبيب أي استفسارات أخرى بخصوص استعمال هذا الدواء. |
أن هذا الدواء – مثله مثل بقية الأدوية – يمكن أن يسبب آثار جانبية، والتي قد لا تظهر عند كل شخص. | ||||||||||||
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الآثار الجانبية الغالبة الشــيوع (بمعدل أكثر من مريض بين كل 10 مرضى): | ||||||||||||
أنخفاض معدل ضربات القلب. | ||||||||||||
إنخفاض أو ارتفاع ضغط الدم. | ||||||||||||
تغييرات في نمط التنفس أو توقف التنفس. | ||||||||||||
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الآثار الجانبية الشائعة (بمعدل 1 إلى 10 مريض بين كل 100 مريض) | ||||||||||||
آلام في الصدر أو نوبة قلبية. | ||||||||||||
تسرع ضربات القلب. | ||||||||||||
إنخفاض أو ارتفاع سكر الدم. | ||||||||||||
الغيثان أو التقيؤ أو جفاف الفم. | ||||||||||||
الأرق. | ||||||||||||
الأعراض بعد توقف استعمال الدواء. | ||||||||||||
إرتفاع درجة الحرارة | ||||||||||||
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الآثار الجانبية الشائعة (بمعدل 1 إلى 10 مريض في 1000 مريض) | ||||||||||||
ارتفاع مستوى الحامض في الجسم. | ||||||||||||
إنخفاض مستوى الألبومين في الدم. | ||||||||||||
الهذيــان. | ||||||||||||
إنخفاض مستوى أداء القلب لوظيفته. | ||||||||||||
ضيق التنفس والتوقف المؤقت للتنفس. | ||||||||||||
عدم الفعالية الكافية للدواء. | ||||||||||||
إنتفاخ البطن. | ||||||||||||
العطش. | ||||||||||||
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الآثار الجانبية غير المعروفة (لا يمكن تقدير تكرارها من واقع البيانات المتوفرة) | ||||||||||||
الشعور بالحاجة الزائدة للتبول. | ||||||||||||
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التبليغ عن الآثار الجانبية: | ||||||||||||
يجب تبليغ الطبيب أو الصيدلي أو الممرض في حالة ظهور أي من الآثار الجانبية لهذا الدواء، وبما فيها أي من تلك الآثار الجانبية التي لم ترد ذكرها في هذه النشرة. حيث أن التبليغ عنها يساعد في توفير المزيد المعلومات بخصوص سلامة هذا الدواء.
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يحفظ الدواء بعيــدا عن متناول الأطفال. |
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لا يستخدم العقــار بعد تاريخ إنتهاء صلاحيته المحدد في البطاقة العلبة. |
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يحفظ الدواء تحت أقل من 30 درجة حرارة. وتحفظ القارورة الصندوق الخارجي لأجل حمايتها من الضوء. |
يحتوي سوبوريديكس على المادة الفعالة دكسميديتوميدين. |
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كل ملتر من التركيز يحتوي على هيدروكلوريد دكسميديتوميدين بما يعادل 100 ميكروجرام من دكسميديتوميدين. |
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المكونات الأخرى تشمل كلوريد الصوديوم والماء للحقن. |
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كل قارورة سعة 2 ملتر تحتوي على 200 ميكروجرام من دكسميديتوميدين (عبارة عن هيدروكلوريد). |
كل قارورة سعة 4 ملتر تحتوي على 400 ميكروجرام من دكسميديتوميدين (عبارة عن هيدروكلوريد). |
كل قارورة سعة 10 ملتر تحتوي على 1000 ميكروجرام من دكسميديتوميدين (عبارة عن هيدروكلوريد). |
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التركيز للمحلول النهائي بعد التخفيف إما 4 ميكروجرام/ملتر أو 8 ميكروجرام/ملتر. |
المادة المركزة المحلول للحقن (المادة المركزة معقم) |
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المادة المركزة عبارة عن محلول شفاف عديم اللون. |
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الحاويات: |
قوارير زجاجية شفافة سعة 2.5 أو 10 ملتر. |
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أحجام العبوات: |
قوارير 5× 2 مل. |
قوارير 5× 4 مل. |
قوارير 5× 10 مل. |
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ليس من المحتمل تسويق جميع العبوات. |
صاحب ترخيص التسويق | ||||
أيفــر فالنجيكت جي.إم.بي.إتش. | ||||
أوبربارقــو 3 | ||||
4866 أنتراتش آم أترسي | ||||
أســتراليا | ||||
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الشركة المنتجة | ||||
أيفــر فالنجيكت جي.إم.بي.إتش. | ||||
15 شارع أوتو-شوت | ||||
07745 جينا | ||||
ألمانيا
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1. For sedation of adult ICU (Intensive Care Unit) patients requiring sedation level not deeper than arousal in response to verbal stimulation (corresponding to Richmond Agitation-Sedation Scale (RASS) 0 to -3).
2. For sedation of non-intubated adult patients prior to and/or during diagnostic or surgical procedures requiring sedation, i.e. procedural/awake sedation.
Indication 1. For sedation of adult ICU (Intensive Care Unit) patients requiring a sedation level not deeper than arousal in response to verbal stimulation (corresponding to Richmond Agitation-Sedation Scale (RASS) 0 to -3).
Posology ICU sedation
For hospital use only. SOPORIDEX should be administered by healthcare professionals skilled in the management of patients requiring intensive care.
Patients already intubated and sedated may switch to dexmedetomidine with an initial infusion rate of 0.7 micrograms/kg/h which may then be adjusted stepwise within the dose range 0.2 to 1.4 micrograms/kg/h in order to achieve the desired level of sedation, depending on the patient's response. A lower starting infusion rate should be considered for frail patients. Dexmedetomidine is very potent and the infusion rate is given per hour. After dose adjustment, a new steady state sedation level may not be reached for up to one hour.
Maximum dose
The maximum dose of 1.4 micrograms/kg/h should not be exceeded. Patients failing to achieve an adequate level of sedation with the maximum dose of dexmedetomidine should be switched to an alternative sedative agent.
Use of a loading dose of SOPORIDEX in ICU sedation is not recommended and is associated with increased adverse reactions. Propofol or midazolam may be administered if needed until clinical effects of dexmedetomidine are established.
Duration
There is no experience in the use of SOPORIDEX for more than 14 days. The use of SOPORIDEX for longer than this period should be regularly reassessed.
Indication 2. For sedation of non-intubated adult patients prior to and/or during diagnostic or surgical procedures requiring sedation, i.e. procedural/awake sedation.
SOPORIDEX should be administered only by health care professionals skilled in the anaesthetic management of patients in the operating room or during diagnostic procedures. When SOPORIDEX is administered for conscious sedation, patients should be continuously monitored by persons not involved in the conduct of the diagnostic or surgical procedure. Patients should be monitored continuously for early signs of hypotension, hypertension, bradycardia, respiratory depression, airway obstruction, apnoea, dyspnoea and/or oxygen desaturation (see section 4.8).
Supplemental oxygen should be immediately available and provided when indicated. The oxygen saturation should be monitored by pulse oximetry.
SOPORIDEX is given as a loading infusion followed by maintenance infusion. Depending on the procedure, concomitant local anaesthesia or analgesia may be needed in order to achieve the desired clinical effect. Additional analgesia or sedatives (e.g. midazolam, propofol and opioids) are recommended in case of painful procedures or if increased depth of sedation is necessary. The pharmacokinetic distribution half –life of dexmedetomidine has been estimated to be around 6 min, which can be taken into consideration, together with the effects of other administered medications, when assessing the appropriate time needed for titration to desired clinical effect of SOPORIDEX.
Initiation of Procedural Sedation:
- A loading infusion of 1.0 microgram/kg over 10 minutes. For less invasive procedures such as ophthalmic surgery, a loading infusion of 0.5 micrograms/kg given over 10 minutes may be suitable.
Maintenance of Procedural Sedation:
- The maintenance infusion is generally initiated at 0.6 microgram/kg/hour and titrated to achieve desired clinical effect with doses ranging from 0.2 to 1 microgram/kg/hour. The rate of the maintenance infusion should be adjusted to achieve the targeted level of sedation.
Special populations
Elderly: No dose adjustment is normally required for elderly patients (see section 5.2). Elderly patients appear to have an increased risk for hypotension (see section 4.4) but the limited data available from procedural sedation do not suggest a clear dose dependency.
Renal impairment: No dose adjustment is required for patients with renal impairment.
Hepatic impairment: Dexmedetomidine is metabolised in the liver and should be used with caution in patients with hepatic impairment. A reduced maintenance dose may be considered (see sections 4.4 and 5.2).
Paediatric population:
The safety and efficacy of SOPORIDEX in children aged 0 to 18 years have not been established.
Currently available data are described in sections 4.8, 5.1 and 5.2 but no recommendation on a posology can be made.
Method of administration
SOPORIDEX must be administered only as a diluted intravenous infusion using a controlled infusion device. For instructions on dilution of the medicinal product before administration, see section 6.6.
Monitoring
Based on the indications, SOPORIDEX is intended for use in an intensive care setting, operating room and during diagnostic procedures. The use in other environments is not recommended. All patients should have continuous cardiac monitoring during SOPORIDEX infusion. Respiration should be monitored in non-intubated patients due to the risk of respiratory depression and in some case apnoea (see section 4.8).
The time to recovery after the use of dexmedetomidine was reported to be approximately one hour.
When used in an outpatient setting close monitoring should continue for at least one hour (or longer based on the patient condition), with medical supervision continued for at least one furtherhour to ensure the safety of the patient.
General precautions
SOPORIDEX should not be given as a bolus dose and in the ICU a loading dose is not recommended. Users should generally be ready to use an alternative sedative for acute control of agitation or during procedures, especially during the first few hours of treatment. During procedural sedation a small bolus of another sedative may be used if a rapid increase in sedation level is required.
Some patients receiving SOPORIDEX have been observed to be arousable and alert when stimulated. This alone should not be considered as evidence of lack of efficacy in the absence of other clinical signs and symptoms.
Dexmedetomidine normally does not cause deep sedation and patients may be easily roused. Dexmedetomidine is therefore not suitable in patients who will not tolerate this profile of effects, for example those requiring continuous deep sedation.
SOPORIDEX should not be used as a general anaesthetic induction agent for intubation or to provide sedation during muscle relaxant use.
Dexmedetomidine lacks the anticonvulsant action of some other sedatives and so will not suppress underlying seizure activity.
Care should be taken if combining dexmedetomidine with other substances with sedative or cardiovascular actions as additive effects may occur.
SOPORIDEX is not recommended for patient controlled sedation. Adequate data is not available.
When SOPORIDEX is used in an outpatient setting patients should normally be discharged into the care of a suitable third party. Patients should be advised to refrain from driving or other hazardous tasks and where possible to avoid the use of other agents that may sedate (e.g, benzodiazepines, opioids, alcohol) for a suitable period of time based on observedeffects of dexmedetomidine, the procedure, concomitant medications, the age and the condition of the patient.
Caution should be exercised when administering dexmedetomidine to elderly patients.
Elderly patients over 65 years of age may be more prone to hypotension with the administration of dexmedetomidine, including a loading dose, for procedures. A dose reduction should be considered. Please refer to section 4.2.
Cardio-vascular effects and precautions
Dexmedetomidine reduces heart rate and blood pressure through central sympatholysis but at higher concentrations causes peripheral vasoconstriction leading to hypertension (see section 5.1). Dexmedetomidine is therefore not suitable in patients with severe cardiovascular instability.
Caution should be exercised when administering dexmedetomidine to patients with pre-existing bradycardia. Data on the effects of SOPORIDEX in patients with heart rate <60 are very limited and particular care should be taken with such patients. Bradycardia does not normally require treatment but has commonly responded to anti-cholinergic medicine or dose reduction where needed. Patients with high physical fitness and slow resting heart rate may be particularly sensitive to bradycardic effects of alpha-2 receptor agonists and cases of transient sinus arrest have been reported.
The hypotensive effects of dexmedetomidine may be of greater significance in those patients with pre-existing hypotension (especially if not responsive to vasopressors), hypovolaemia, chronic hypotension or reduced functional reserve such as patients with severe ventricular dysfunction and the elderly and special care is warranted in these cases (see section 4.3). Hypotension does not normally require specific treatment but, where needed, users should be ready to intervene with dose reduction, fluids and/or vasoconstrictors.
Patients with impaired peripheral autonomic activity (e.g. due to spinal cord injury) may have more pronounced haemodynamic changes after starting dexmedetomidine and so should be treated with care.
Transient hypertension has been observed primarily during the loading dose in association with the peripheral vasoconstrictive effects of dexmedetomidine and a loading dose is not recommended in ICU sedation. Treatment of hypertension has generally not been necessary but decreasing the continuous infusion rate may be advisable.
Local vasoconstriction at higher concentration may be of greater significance in patients with ischaemic heart disease or severe cerebrovascular disease who should be monitored closely. Dose reduction or discontinuation should be considered in a patient developing signs of myocardial or cerebral ischaemia.
Caution is advised when administering dexmedetomidine together with spinal or epidural anaesthesia due to possible increased risk of hypotension or bradycardia.
Patients with hepatic impairment
Care should be taken in severe hepatic impairment as excessive dosing may increase the risk of adverse reactions, over-sedation or prolonged effect as a result of reduced dexmedetomidine clearance.
Patients with neurological disorders
Experience of dexmedetomidine in severe neurological disorders such as head injury and after neurosurgery is limited and it should be used with caution here, especially if deep sedation is required. Dexmedetomidine may reduce cerebral blood flow and intracranial pressure and this should be considered when selecting therapy.
Other
Alpha-2 agonists have rarely been associated with withdrawal reactions when stopped abruptly after prolonged use. This possibility should be considered if the patient develops agitation and hypertension shortly after stopping dexmedetomidine.
Dexmedetomidine may induce hyperthermia that may be resistant to traditional cooling methods. Dexmedetomidine treatment should be discontinued in the event of a sustained unexplained fever and is not recommended for use in malignant hyperthermia-sensitive patients.
Excipient with known effect:
SOPORIDEX contains less than 1 mmol sodium (23 mg) per ml.
Interaction studies have only been performed in adults.
Co-administration of dexmedetomidine with anaesthetics, sedatives, hypnotics, and opioids is likely to lead to an enhancement of effects, including sedative, anaesthetic and cardiorespiratory effects. Specific studies have confirmed enhanced effects with isoflurane, propofol, alfentanil, and midazolam.
No pharmacokinetic interactions between dexmedetomidine and isoflurane, propofol, alfentanil and midazolam have been demonstrated. However, due to possible pharmacodynamic interactions, when co-administered with dexmedetomidine, a reduction in dosage of dexmedetomidine or the concomitant anaesthetic, sedative, hypnotic or opioid may be required.
Inhibition of CYP enzymes including CYP2B6 by dexmedetomidine has been studied in human liver microsome incubations. In vitro study suggests that interaction potential in vivo exists between dexmedetomidine and substrates with dominant CYP2B6 metabolism.
Induction of dexmedetomidine in vitro was observed on CYP1A2, CYP2B6, CYP2C8, CYP2C9 and CYP3A4, and induction in vivo cannot be excluded. The clinical significance is unknown.
The possibility of enhanced hypotensive and bradycardic effects should be considered in patients receiving other medicinal products causing these effects, for example beta-blockers, although additional effects in an interaction study with esmolol were modest.
Pregnancy
There are no adequate data from the use of dexmedetomidine in pregnant women.
Studies in animals have shown reproductive toxicity (see section 5.3). SOPORIDEX is not recommended during pregnancy and in women of childbearing potential not using contraception.
Breastfeeding
Available data in the rat have shown excretion of dexmedetomidine or metabolites in milk. A risk to infants cannot be excluded. A decision must be made whether to discontinue breastfeeding or to discontinue dexmedetomidine therapy taking into account the benefit of breastfeeding for the child and the benefit of therapy for the woman.
Fertility
In the rat fertility study, dexmedetomidine had no effect on male or female fertility.
Dexmedetomidine EVER Pharma has major impact on the ability to drive and use machines.
ummary of the safety profile
Indication 1: Sedation of adult ICU (Intensive Care Unit) patients:
The most frequently reported adverse reactions with dexmedetomidine in ICU setting are hypotension, hypertension and bradycardia, occurring in approximately 25 %, 15 % and 13 % of patients respectively.
Hypotension and bradycardia were also the most frequent dexmedetomidine-related serious adverse reactions occurring in 1.7 % and 0.9 % of randomised Intensive Care Unit (ICU) patients respectively.
Indication 2: Procedural/awake sedation
The most frequently reported adverse reactions with dexmedetomidine in procedural sedation are:
- Hypotension (55 % in dexmedetomidine-group vs. 30 % in placebo-group receiving rescue midazolam and fentanyl)
- Respiratory depression (38 % in dexmedetomidine-group vs. 35 % in placebo-group receiving rescue midazolam and fentanyl)
- Bradycardia (14 % in dexmedetomidine-group vs. 4 % in placebo-group receiving rescue midazolam and fentanyl)
Tabulated list of adverse reactions
The adverse reactions listed in Table 1 have been accumulated from pooled data of clinical trials in intensive care.
Adverse reactions are ranked under headings of frequency, the most frequent first, using the following convention: Very common (≥1/10); Common (≥1/100 to <1/10); Uncommon (≥1/1,000 to <1/100); Not known (frequency cannot be estimated from available data).
Table 1: Adverse reactions (Indication 1 and Indication 2)
Metabolism and nutrition disorders | |
Common: | Hyperglycaemia, hypoglycaemia |
Uncommon: | Metabolic acidosis, hypoalbuminaemia |
Psychiatric disorders | |
Common: | Agitation |
Uncommon: | Hallucination |
Cardiac disorders | |
Very common: | Bradycardia1,2 |
Common: | Myocardial ischaemia or infarction, tachycardia |
Uncommon: | Atrioventricular block first degree, cardiac output decreased |
Vascular disorders: | |
Very common: | Hypotension1,2, hypertension1,2 |
Respiratory, thoracic and mediastinal disorders | |
Very common: | Respiratory depression2,3 |
Uncommon: | Dyspnoea, apnoea |
Gastrointestinal disorders | |
Common: | Nausea2, vomiting, dry mouth2 |
Uncommon: | Abdominal distension |
Renal and urinary disorders | |
Not known: | Polyuria |
General disorders and administration site conditions | |
Common: | Withdrawal syndrome, hyperthermia |
Uncommon: | Drug ineffective, thirst |
1 See section on Description of selected adverse reactions
2 Adverse reaction observed also in procedural sedation studies
3 Incidence 'common' in ICU sedation studies
Description of selected adverse reactions
Clinically significant hypotension or bradycardia should be treated as described in section 4.4.
In relatively healthy non-ICU subjects treated with dexmedetomidine, bradycardia has occasionally led to sinus arrest or pause. The symptoms responded to leg raising and anticholinergics such as atropine or glycopyrrolate. In isolated cases, bradycardia has progressed to periods of asystole in patients with pre-existing bradycardia.
Hypertension has been associated with the use of a loading dose and this reaction can be reduced by avoiding such a loading dose or reducing the infusion rate or size of the loading dose.
Paediatric population
Children > 1 month post-natal, predominantly post-operative, have been evaluated for treatment up to 24 hours in the ICU and demonstrated a similar safety profile as in adults. Data in new-born infants (28 – 44 weeks gestation) is very limited and restricted to maintenance doses ≤ 0.2 micrograms/kg/h. A single case of hypothermic bradycardia in a neonate has been reported in the literature.
Reporting of suspected adverse reactions
Reporting suspected adverse reactions after authorisation of the medicinal product is important. It allows continued monitoring of the benefit/risk balance of the medicinal product. Healthcare professionals are asked to report any suspected adverse reactions via the national reporting system.
To report any side effect(s):
Saudi Arabia
The National Pharmacovigilance and Drug Safety Centre (NPC)
- Fax: +966-11-205-7662
- Call NPC at +966-11-2038222, Exts: 2317-2356-2353-2354-2334-2340.
- Toll free phone: 8002490000
- E-Mail: npc.drug@sfda.gov.sa
- Website: www.sfda.gov.sa/npc
Other GCC States
Please contact the relevant competent authority
Symptoms
Several cases of dexmedetomidine overdose have been reported in both the clinical trial and the post-marketing data. The reported highest infusion rates of dexmedetomidine in these cases have reached up to 60 µg/kg/h for 36 minutes and 30 µg/kg/h for 15 minutes in a 20-month-old child and in an adult, respectively. The most common adverse reactions reported in conjunction with overdose in these cases included bradycardia, hypotension, oversedation, somnolence and cardiac arrest.
Management
In cases of overdose with clinical symptoms, dexmedetomidine infusion should be reduced or stopped. Expected effects are primarily cardiovascular and should be treated as clinically indicated (see section 4.4). At high concentration, hypertension may be more prominent than hypotension. In clinical studies, cases of sinus arrest reversed spontaneously or responded to treatment with atropine and glycopyrrolate. Resuscitation was required in isolated cases of severe overdose resulting in cardiac arrest.
Pharmacotherapeutic group: Psycholeptics, other hypnotics and sedatives, ATC code: N05CM18
Dexmedetomidine is a selective alpha-2 receptor agonist with a broad range of pharmacological properties. It has a sympatholytic effect through decrease of the release of noradrenaline in sympathetic nerve endings. The sedative effects are mediated through decreased firing of locus coeruleus, the predominant noradrenergic nucleus, situated in the brainstem.
Dexmedetomidine has analgesic and anaesthetic/analgesic-sparing effects. The cardiovascular effects depend on the dose; with lower infusion rates the central effects dominate leading to decrease in heart rate and blood pressure. With higher doses, peripheral vasoconstricting effects prevail leading to an increase in systemic vascular resistance and blood pressure, while the bradycardic effect is further emphasised. Dexmedetomidine is relatively free from respiratory depressive effects when given as monotherapy to healthy subjects.
Indication 1: Sedation of adult ICU (Intensive Care Unit) patients
In placebo controlled trials in a post-operative ICU population previously intubated and sedated with midazolam or propofol, dexmedetomidine significantly reduced the requirement for both rescue sedative (midazolam or propofol) and opioids during sedation for up to 24 hours. Most dexmedetomidine patients required no additional sedative treatment. Patients could be successfully extubated without stopping the dexmedetomidine infusion. Studies from outside the ICU have confirmed that dexmedetomidine can be administered safely to patients without endotracheal intubation provided adequate monitoring is in place.
Dexmedetomidine was similar to midazolam (Ratio 1.07; 95 % CI 0.971, 1.176) and propofol (Ratio 1.00; 95 % CI 0.922, 1.075) on the time in target sedation range in a predominantly medical population requiring prolonged light to moderate sedation (RASS 0 to -3) in the ICU for up to 14 days, reduced the duration of mechanical ventilation compared to midazolam and reduced the time to extubation compared to midazolam and propofol. Compared to both propofol and midazolam, patients were more easily roused, more cooperative and better able to communicate whether or not they had pain. Dexmedetomidine treated patients had more frequent hypotension and bradycardia but less tachycardia than those receiving midazolam and more frequent tachycardia but similar hypotension to propofol-treated patients. Delirium measured by the CAM-ICU scale was reduced in a study compared to midazolam and delirium-related adverse events were lower on dexmedetomidine compared to propofol. Those patients who withdrew due to insufficient sedation were switched to either propofol or midazolam. The risk of insufficient sedation was increased in patients who were difficult to sedate with standard care immediately prior to switching.
Evidence of paediatric efficacy was seen in a dose-controlled ICU study in a largely post-operative population aged 1 month to ≤ 17 years. Approximately 50 % of patients treated with dexmedetomidine did not require rescue addition of midazolam during a median treatment period of 20.3 hours, not exceeding 24 hours. Data on treatment for > 24 hours is not available. Data in new-born infants (28 – 44 weeks gestation) is very limited and restricted to low doses (≤ 0.2 micrograms/kg/h) (see sections 5.2 and 4.4). New-born infants may be particularly sensitive to the bradycardic effects of dexmedetomidine in the presence of hypothermia and in conditions of heart rate-dependent cardiac output.
In double blind comparator controlled ICU studies the incidence of cortisol suppression in patients treated with dexmedetomidine (n=778) was 0.5 % compared with 0 % in patients treated with either midazolam (n=338) or propofol (n=275). The event was reported as mild in 1 and moderate in 3 cases.
Indication 2: Procedural/awake sedation
The safety and efficacy of dexmedetomidine for sedation of non-intubated patients prior to and/or during surgical and diagnostic procedures was evaluated in two randomized, double-blind, placebo-controlled multicentre clinical trials.
· Study 1 randomised patients undergoing elective surgeries/procedures under monitored anaesthesia care and local/regional anaesthesia to receive a loading infusion of either dexmedetomidine 1 µg/kg (n=129), dexmedetomidine 0.5 µg/kg (n=134), or placebo (normal saline) (n=63) given over 10 minutes and followed by a maintenance infusion started at 0.6 µg/kg/h. The maintenance infusion of study drug could be titrated from 0.2 mµ/kg/h to 1 µg/kg/h. The proportion of patients that achieved the targeted sedation score (Observer’s Assessment of Alertness/Sedation Scale ≤4). Without need for rescue midazolam was 54 % of the patients receiving dexmedetomidine 1 µg/kg and 40 % of the patients receiving dexmedetomidine 0.5 µg/kg compared to 3 % of patients receiving the placebo.
The risk difference in proportion of subjects randomised to dexmedetomidine 1 μg/kg group and dexmedetomidine 0.5 μg/kg group not requiring rescue midazolam was 48% (95% CI: 37 % - 57%) and 40% (95% CI: 28 % - 48%), respectively compared placebo. The median (range) midazolam rescue dose was 1.5 (0.5-7.0) mg in the dexmedetomidine1.0 µg/kg group, 2.0 (0.5-8.0) mg in the dexmedetomidine 0.5 µg/kg group, and 4.0 (0.5-14.0) mg in the placebo group. The difference in means in dose of rescue midazolam in dexmedetomidine 1 μg/kg and dexmedetomidine 0.5 μg/kg group compared to placebo was -3.1 mg (95% CI: -3.8 - -2.5) and -2.7 mg (95% CI: -3.3 - -2.1), respectively favouring dexmedetomidine. The median time to first rescue dose was 114 minutes in the dexmedetomidine 1.0 µg/kg group, 40 minutes in the dexmedetomidine 0.5 µg/kg group, and 20 minutes in the placebo group.
· Study 2 randomised patients undergoing awake fibreoptic intubation under topical anaesthesia to receive a loading infusion of dexmedetomidine 1 µg/kg (n=55) or placebo (normal saline) (n=50) given over 10 minutes and followed by a fixed maintenance infusion of 0.7 µg/kg/h. To maintain a Ramsay Sedation Scale ≥2 53% of the patients receiving dexmedetomidine did not require midazoloam rescue vs. 14% of patients receiving placebo. The risk difference in proportion of subjects randomised to dexmedetomidine not requiring rescue midazolam was 43% (95% CI: 23 % - 57%) compared placebo. The mean midazolam rescue dose was 1.1 mg in the dexmedetomidine group, and 2.8 mg in the placebo group. The difference in means in dose of rescue midazolam was -1.8 mg (95% CI: -2.7 - -0.86) favouring dexmedetomidine.
The pharmacokinetics of dexmedetomidine has been assessed following short-term IV administration in healthy volunteers and long-term infusion in ICU population.
Distribution
Dexmedetomidine exhibits a two-compartment disposition model. In healthy volunteers, it exhibits a rapid distribution phase with a central estimate of the distribution half-life (t1/2α) of about 6 minutes. The mean estimate of the terminal elimination half-life (t1/2) is approximately 1.9 to 2.5 h (min 1.35, max 3.68 h) and the mean estimate of the steady-state volume of distribution (Vss) is approximately 1.16 to 2.16 l/kg (90 to 151 litres). Plasma clearance (Cl) has a mean estimated value of 0.46 to 0.73 l/h/kg (35.7 to 51.1 l/h). The mean body weight associated with these Vss and Cl estimates was 69 kg. Plasma pharmacokinetics of dexmedetomidine is similar in the ICU population following infusion >24 h. The estimated pharmacokinetic parameters are: t1/2 approximately 1.5 hours, Vss approximately 93 litres and Cl approximately 43 l/h. The pharmacokinetics of dexmedetomidine is linear in the dosing range from 0.2 to 1.4 µg/kg/h and it does not accumulate in treatments lasting up to 14 days. Dexmedetomidine is 94 % bound to plasma proteins. Plasma protein binding is constant over the concentration range of 0.85 to 85 ng/ml. Dexmedetomidine binds to both human serum albumin and Alpha-1-acid glycoprotein with serum albumin as the major binding protein of dexmedetomidine in plasma.
Biotransformation and Elimination
Dexmedetomidine is eliminated by extensive metabolism in the liver. There are three types of initial metabolic reactions; direct N-glucuronidation, direct N-methylation and cytochrome P450 catalysed oxidation. The most abundant circulating dexmedetomidine metabolites are two isomeric N-glucuronides. Metabolite H-1, N-methyl 3-hydroxymethyl dexmedetomidine O-glucuronide, is also a major circulating product of dexmedetomidine biotransformation. Cytochrome P-450 catalyses the formation of two minor circulating metabolites, 3-hydroxymethyl dexmedetomidine produced by hydroxylation at the 3-methyl group of dexmedetomidine and H-3 produced by oxidation in the imidazole ring. Available data suggest that the formation of the oxidised metabolites is mediated by several CYP forms (CYP2A6, CYP1A2, CYP2E1, CYP2D6 and CYP2C19). These metabolites have negligible pharmacological activity.
Following IV administration of radiolabelled dexmedetomidine an average 95 % of radioactivity was recovered in the urine and 4% in the faeces after nine days. The major urinary metabolites are the two isomeric N-glucuronides, which together accounted for approximately 34 % of the dose and N-methyl 3-hydroxymethyl dexmedetomidine O-glucuronide that accounted for 14.51% of the dose. The minor metabolites dexmedetomidine carboxylic acid, 3-hydroxymethyl dexmedetomidine and its O-glucuronide individually comprised 1.11 to 7.66 % of the dose. Less than 1 % of unchanged parent drug was recovered in the urine. Approximately 28 % of the urinary metabolites are unidentified minor metabolites.
Special Populations
No major pharmacokinetic differences have been observed based on gender or age.
Dexmedetomidine plasma protein binding is decreased in subjects with hepatic impairment compared with healthy subjects. The mean percentage of unbound dexmedetomidine in plasma ranged from 8.5 % in healthy subjects to 17.9 % in subjects with severe hepatic impairment. Subjects with varying degrees of hepatic impairment (Child-Pugh Class A, B, or C) had decreased hepatic clearance of dexmedetomidine and prolonged plasma elimination t1/2. The mean plasma clearance values of unbound dexmedetomidine for subjects with mild, moderate, and severe hepatic impairment were 59 %, 51 % and 32 % of those observed in the normal healthy subjects, respectively. The mean t1/2 for the subjects with mild, moderate or severe hepatic impairment was prolonged to 3.9, 5.4, and 7.4 hours, respectively. Although dexmedetomidine is administered to effect, it may be necessary to consider initial/maintenance dose reduction in patients with hepatic impairment depending on the degree of impairment and the response.
The pharmacokinetics of dexmedetomidine in subjects with severe renal impairment (creatinine clearance <30 ml/min) is not altered relative to healthy subjects.
Data in new-born infants (28 - 44 weeks gestation) to children 17 years of age are limited. Dexmedetomidine half-life in children (1 month to 17 years) appears similar to that seen in adults, but in new-born infants (under 1 month), it appears higher. In the age groups 1 month to 6 years, body weight-adjusted plasma clearance appeared higher but decreased in older children. Body weight-adjusted plasma clearance in new-born infants (under 1 month) appeared lower (0.9 l/h/kg) than in the older groups due to immaturity. The available data is summarised in the following table:
|
| Mean (95% CI) | |
Age | N | Cl (l/h/kg) | t1/2 (h) |
Under 1 month | 28 | 0.93 (0.76, 1.14) | 4.47 (3.81, 5.25) |
1 to < 6 months | 14 | 1.21 (0.99, 1.48) | 2.05 (1.59, 2.65) |
6 to < 12 months | 15 | 1.11 (0.94, 1.31) | 2.01 (1.81, 2.22) |
12 to < 24 months | 13 | 1.06 (0.87, 1.29) | 1.97 (1.62, 2.39) |
2 to < 6 years | 26 | 1.11 (1.00, 1.23) | 1.75 (1.57, 1.96) |
6 to < 17 years | 28 | 0.80 (0.69, 0.92) | 2.03 (1.78, 2.31) |
Non-clinical data reveal no special hazard for humans based on conventional studies of safety pharmacology, single and repeated dose toxicity and genotoxicity.
In the reproductive toxicity studies, dexmedetomidine had no effect on male or female fertility in the rat, and no teratogenic effects were observed in the rat or rabbit. In the rabbit study intravenous administration of the maximum dose, 96 µg/kg/day, produced exposures that are similar to those observed clinically. In the rat, subcutaneous administration at the maximum dose, 200 µg/kg/day, caused an increase in embryofoetal death and reduced the foetal body weight. These effects were associated with clear maternal toxicity. Reduced foetal body weight was noted also in the rat fertility study at dose 18 µg/kg/day and was accompanied with delayed ossification at dose 54 µg/kg/day. The observed exposure levels in the rat are below the clinical exposure range.
Sodium chloride
Water for injections
This medicinal product must not be mixed with other medicinal products except those mentioned in section 6.6.
Compatibility studies have shown potential for adsorption of dexmedetomidine to some types of natural rubber. Although dexmedetomidine is dosed to effect, it is advisable to use components with synthetic or coated natural rubber gaskets
Store below 30 °C
Keep the vials in the outer carton in order to protect from light.
For storage conditions after dilution of the medicinal product, see section 6.3
2, 5 or 10 ml Type I colourless glass vials (with filling volumes of 2, 4 and 10 ml), bromobutyl rubber closure with fluoropolymer coating
Pack sizes
5 x 2 ml vials
5 x 4 ml vials
5 x 10 ml vials
Not all pack sizes may be marketed.
Vials are intended for single patient use only.
Preparation of solution
SOPORIDEX can be diluted in glucose 50 mg/ml (5 %), Ringers, mannitol or sodium chloride 9 mg/ml (0.9 %) solution for injection to achieve the required concentration of either 4 micrograms/ml or 8 micrograms/ml prior to administration. Please see below in tabulated form the volumes needed to prepare the infusion.
In case the required concentration is 4 micrograms/ml:
Volume of SOPORIDEX 100 micrograms/ml concentrate for solution for infusion | Volume of diluent | Total volume of infusion |
2 ml | 48 ml | 50 ml |
4 ml | 96 ml | 100 ml |
10 ml | 240 ml | 250 ml |
20 ml | 480 ml | 500 ml |
In case the required concentration is 8 micrograms/ml:
Volume of SOPORIDEX 100 micrograms/ml concentrate for solution for infusion | Volume of diluent | Total volume of infusion |
4 ml | 46 ml | 50 ml |
8 ml | 92 ml | 100 ml |
20 ml | 230 ml | 250 ml |
40 ml | 460 ml | 500 ml |
The solution should be shaken gently to mix well.
SOPORIDEX should be inspected visually for particulate matter and discoloration prior to administration.
SOPORIDEX has been shown to be compatible when administered with the following intravenous fluids and medicinal products:
Lactated Ringers, 5 % glucose solution, sodium chloride 9 mg/ml (0.9 %) solution for injection, mannitol 200 mg/ml (20 %), thiopental sodium, etomidate, vecuronium bromide, pancuronium bromide, succinylcholine, atracurium besylate, mivacurium chloride, rocuronium bromide, glycopyrrolate bromide, phenylephrine HCl, atropine sulfate, dopamine, noradrenaline, dobutamine, midazolam, morphine sulfate, fentanyl citrate, and a plasma-substitute.
Any unused medicinal product or waste material should be disposed of in accordance with local requirements.