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نشرة الممارس الصحي نشرة معلومات المريض بالعربية نشرة معلومات المريض بالانجليزية صور الدواء بيانات الدواء
  SFDA PIL (Patient Information Leaflet (PIL) are under review by Saudi Food and Drug Authority)

Duodart is used to treat men with an enlarged prostate (benign prostatic hyperplasia) - a non-cancerous growth of the prostate gland, caused by producing too much of a hormone called dihydrotestosterone.

 

Duodart is a combination of two different medicines called dutasteride and tamsulosin. Dutasteride belongs to a group of medicines called 5-alpha reductase inhibitors and tamsulosin belongs to a group of medicines called alpha-blockers.

 

As the prostate grows, it can lead to urinary problems, such as difficulty in passing urine and a need to go to the toilet frequently. It can also cause the flow of the urine to be slower and less forceful. If left untreated, there is a risk that your urine flow will be completely blocked (acute urinary retention). This requires immediate medical treatment. Sometimes surgery is necessary to remove or reduce the size of the prostate gland.

 

Dutasteride lowers the production of a hormone called dihydrotestosterone, which helps to shrink the prostate and relieve the symptoms. This will reduce the risk of acute urinary retention and the need for surgery. Tamsulosin acts by relaxing the muscles in your prostate gland, making it easier to pass urine and rapidly improving your symptoms.


Do not take Duodart

-        if you’re a woman (because this medicine is for men only).

-        if you’re a child or adolescent less than 18 years old.

-        if you’re allergic to dutasteride, other 5-alpha reductase inhibitors, tamsulosin, soya, peanut or to any of the other ingredients of this medicine (listed in section 6).

-        if you have low blood pressure which makes you feel dizzy, lightheaded or faint (orthostatic hypotension).

-        if you have a severe liver disease.

 è If you think any of these apply to you, don’t take this medicine until you have checked with your doctor.

 

 

Take special care with Duodart

Talk to your doctor before taking Duodart

-          In some clinical studies, more patients taking dutasteride and another medicine called an alpha-blocker, like tamsulosin, experienced heart failure than patients taking only dustasteride or only an alpha blocker. Heart failure means your heart does not pump blood as well as it should.  

 

-          Make sure your doctor knows about liver problems. If you have had any illness affecting your liver, you may need some additional check-ups while you are taking Duodart.

 

-          Make sure your doctor knows if you have severe problems with your kidney.

 

-          Cataract (cloudy lens) surgery.  If you are going to have surgery to remove a cataract, your doctor may ask you to stop taking Duodart for a while before your operation.  Tell your eye specialist before your operation that you are taking Duodart or tamsulosin (or have previously taken it).  Your specialist will need to take appropriate precautions to help prevent complications during your operation.

 

-          Women, children and adolescents must not handle leaking Duodart capsules, because the active ingredient can be absorbed through the skin. Wash the affected area immediately with soap and water if there is any contact with the skin.

 

-          Use a condom during sexual intercourse. Dutasteride has been found in the semen of men taking Duodart. If your partner is or may be pregnant, you must avoid exposing her to your semen as dutasteride may affect the normal development of a male baby. Dutasteride has been shown to decrease sperm count, semen volume and sperm motility. This could reduce your fertility.

 

-          Duodart affects a blood test for PSA (prostate-specific antigen), which is sometimes used to detect prostate cancer. Your doctor should be aware of this effect and can still use the test to detect prostate cancer.  If you are having a blood test for PSA, tell your doctor that you are taking Duodart. Men taking Duodart should have their PSA tested regularly.

 

-          In a clinical study of men at increased risk of prostate cancer, men taking dutasteride had a serious form of prostate cancer more often than men who did not take dutasteride. The effect of dutasteride on this serious form of prostate cancer is not clear.

 

-          Duodart may cause breast enlargement and tenderness.  If this becomes troublesome, or if you notice breast lumps or nipple discharge you should talk to your doctor about these changes as these may be signs of a serious condition, such as breast cancer.

 

 è Contact your doctor or pharmacist if you have any questions about taking Duodart.

 

Other medicines and Duodart

Tell your doctor or pharmacist if you are taking, have recently taken or might take any other medicines.

 

Don’t take Duodart with these medicines:

-          other alpha blockers (for enlarged prostate or high blood pressure)

 

Duodart is not recommended with these medicines:

-          ketoconazole (used to treat fungal infections)

 

Some medicines can react with Duodart and may make it more likely that you’ll have side-effects. These medicines include:

-          PDE5 inhibitors (used to help achieve or maintain an erection) such as vardenafil, sildenafil citrate and tadalafil                    

-          verapamil or diltiazem (for high blood pressure)

-          ritonavir or indinavir (for HIV)

-          itraconazole or ketaconazole (for fungal infections)

-          nefazodone (an antidepressant)

-          cimetidine (for stomach ulcers)

-          warfarin (for blood clotting)

-          erythromycin (an antibiotic used to treat infections)

-          paroxetine (an antidepressant)

-          terbinafine (used to treat fungal infections)

-          diclofenac (used to treat pain and inflammation)

 è Tell your doctor if you are taking any of these medicines.

 

Duodart with food and drink

Duodart should be taken 30 minutes after the same meal each day.

 

Pregnancy, breast-feeding and fertility

Duodart must not be taken by women.

 

Women who are pregnant (or may be) must not handle leaking capsules. Dutasteride is absorbed through the skin and can affect the normal development of a male baby. This is a particular risk in the first 16 weeks of pregnancy.

 

Use a condom during sexual intercourse. Dutasteride has been found in the semen of men taking Duodart. If your partner is or may be pregnant, you must avoid exposing her to your semen.

 

Duodart has been shown to reduce sperm count, semen volume and sperm movement. Therefore male fertility may be reduced.

 è Contact your doctor for advice if a pregnant woman has come into contact with Duodart.

 

Driving and using machines

Duodart makes some people feel dizzy, so it may affect your ability to drive or operate machinery safely.

 è Don’t drive or operate machinery if you are affected in this way.

 

Important information about some of the ingredients of Duodart

Duodart contains the colouring agent Sunset Yellow (E110) which may cause allergic reactions.

Duodart contains lecithin from soya. If you are allergic to peanut or soya, do not use this medicinal product.


Always take Duodart exactly as your doctor or pharmacist has told you to. If you do not take it regularly the monitoring of your PSA levels may be affected. Check with your doctor or pharmacist if you are not sure.

 

How much to take

The recommended dose is one capsule taken once a day, 30 minutes after the same meal each day.

 

How to take

Swallow the capsules whole with water. Do not chew or break open the capsule. Contact with the contents of the capsules may make your mouth or throat sore.

 

If you take more Duodart than you should

Contact your doctor or pharmacist for advice if you take too many Duodart capsules.

 

If you forget to take Duodart

Do not take a double dose to make up for a forgotten dose. Just take your next dose at the usual time.

 

Don’t stop Duodart without advice

Don’t stop taking Duodart without talking to your doctor first.

 

If you have any further questions on the use of this product, ask your doctor or pharmacist.


Like all medicines, this medicine can cause side effects, although not everybody gets them.

 

Allergic reaction

The signs of allergic reactions can include:

-          skin rash (which can be itchy)

-          hives (like a nettle rash)

-          swelling of the eyelids, face, lips, arms or legs.

 è Contact your doctor immediately if you get any of these symptoms, and stop using Duodart.

 

Dizziness, light-headedness and fainting

Duodart can cause dizziness, lightheadedness and on rare occasions fainting. Take care when moving from a lying down or sitting position to sitting or standing, particularly if you wake up in the night, until you know how this medicine affects you. If you feel dizzy or lightheaded at any time during treatment, sit or lie down until the symptoms pass.

 

Serious skin reactions

The signs of serious skin reactions can include:

 

-          a widespread rash with blisters and peeling skin, particularly around the mouth, nose, eyes and genitals (Stevens-Johnson syndrome).

è      Contact a doctor immediately if you get these symptoms and stop using Duodart.

 

Common side effects

These may affect up to 1 in 10 men taking Duodart:

-          impotence (not able to achieve or maintain an erection)*

-          decreased sex drive (libido)*

-          difficulty with ejaculation, such as a decrease in the amount of semen released during sex*

-          breast enlargement or tenderness (gynecomastia)

-          dizziness.

-          * In a small number of people some of these events may continue after you stop taking Duodart.

 

Uncommon side effects

These may affect up to 1 in 100 men

-          heart failure (heart becomes less efficient at pumping blood around the body. You may have symptoms such as shortness of breath, extreme tiredness and swelling in your ankles and legs)

-          low blood pressure on standing

-          fast heart beat (palpitations)

-          constipation, diarrhoea, vomiting, feeling sick (nausea)

-          weakness or loss of strength

-          headache

-          itchy, blocked or runny nose (rhinitis)

-          skin rash, hives, itching

-          hair loss (usually from the body) or hair growth.

 

Rare side effects

These may affect up to 1 in 1,000 men

-          swelling of the eyelids, face, lips, arms or legs (angioedema)

-          fainting.

 

Very rare side effects

These may affect up to 1 in 10,000 men

-          persistent painful erection of the penis (priapism)

-          serious skin reactions (Stevens-Johnson syndrome)

 

Other side effects

Other side effects have occurred in a small number of men, but their exact frequency is not known (the frequency cannot be estimated from the available data):

-          abnormal or fast heartbeat (arrhythmia or tachycardia or atrial fibrillation)

-          shortness of breath (dyspnoea)

-          depression

-          pain and swelling in your testicles

-          nose bleeds

-          severe skin rash

-          changes in vision (blurred vision or visual impairment)

-          dry mouth

 

è  If any of the side effects gets serious, or if you notice any side effects not listed in this leaflet,

                Please tell your doctor or pharmacist.


 

·         Keep out of the reach and sight of children.

·         Do not use Duodart after the expiry date which is stated on the pack after ‘Exp’.

·         Don’t store Duodart above 25°C.

·         If your doctor tells you to stop taking Duodart, it is important to return any tablets which are left over to your pharmacist.

·         Medicines should not be disposed of via wastewater or household waste. Ask your pharmacist how to dispose of medicines no longer required. These measures will help to protect the environment.


What Duodart contains

The active substances are dutasteride and tamsulosin hydrochloride. Each capsule contains 0.5 mg dutasteride and 0.4 mg tamsulosin hydrochloride.

The other ingredients are:

*      hard capsule shell: hypromellose, carrageenan (E407), potassium chloride, titanium dioxide (E171), iron oxide red (E172), sunset yellow (E110), carnauba wax, maize starch.

*      inside the hard capsule: mono-di-glycerides of caprylic/capric acid and butylhydroxytoluene (E321), gelatin, glycerol, titanium dioxide (E171), iron oxide yellow (E172), triglycerides (medium chain), lecithin(may contain soya oil), cellulose microcrystalline, methacrylic acid - ethyl acrylate copolymer (containing polysorbate 80 and sodium laurilsulfate), talc, triethyl citrate.

*      black print ink (SW-9010 or SW-9008): shellac, propylene glycol, iron oxide black (E172), potassium hydroxide (in Black Ink SW-9008 only).


This medicine is an oblong hard capsule with a brown body and an orange cap printed with GS 7CZ in black ink. They are available in packs of 7, 30 and 90 capsules. Not all pack sizes may be available in your country. Duodart is a trademark owned by or licensed of the GlaxoSmithKline group of companies © 2019 GlaxoSmithKline, all rights reserved

Marketing Authorisation Holder and Manufacturer

GlaxoSmithKline Export Limited

Address: 980 Great West Road, Brentford, Middlesex, TW8 9GS, England

 

Manufacturer:

Catalent Germany Schorndorf GmbH

Steinbeisstrasse 2

73614 Schorndorf

Germany

To report any side effect(s):

Kingdom of Saudi Arabia

-National Pharmacovigilance centre (NPC)

•Fax:  +966-11-205-7662

• Call NPC at +966-11-2038222, Ext: 2317-2356-2340

• Reporting hotline: 19999

• E-mail: npc.drug@sfda.gov.sa

• Website: www.sfda.gov.sa/npc

-GlaxoSmithKline - Head Office, Jeddah

• Tel: +966-12-6536666

• Mobile: +966-56-904-9882

• Email: sa.aermi-saudi@gsk.com

• website: https://healthksa.gsk.com/

• P.O. Box 55850, Jeddah 21544, Saudi Arabia

 

THIS IS A MEDICAMENT

- Medicament is a product which affects your health, and its consumption contrary to instructions is dangerous for you.

- Follow strictly the doctor’s prescription, the method of use and the instructions of the pharmacist who sold the medicament.

- The doctor and the pharmacist are experts in medicine, its benefits and risks.

- Do not by yourself interrupt the period of treatment prescribed for you.

- Do not repeat the same prescription without consulting your doctor.

- Keep all medicine out of reach of children

Council of Arab Health Ministers

Union of Arab Pharmacists

 

 


Version number: EU v12 Date of issue: 17 November 2017
  نشرة الدواء تحت مراجعة الهيئة العامة للغذاء والدواء (اقرأ هذه النشرة بعناية قبل البدء في استخدام هذا المنتج لأنه يحتوي على معلومات مهمة لك)

ديودارت يستعمل لعلاج الرجال المصابين بتضخم البروستاتة (فرط تنسج البروستاتة الحميد) – وهو نمو غير سرطاني لغدة البروستاتة، ناتج عن الإنتاج المفرط لهرمون يدعى دايهيدروتيستوستيرون.

ديودارت هو عبارة عن توليفة لدواءين مختلفين وهما دوتاستيرايد وتامسولوسين. دوتاستيرايد ينتمي لمجموعة أدوية تدعى مثبطات مختزلة الألفا-5 وتامسولوسين ينتمي لمجموعة أدوية تدعى أدوية حاصرات لمستقبلات ألفا.

كلما ازداد حجم البروستاتة، قد يؤدي ذلك إلى مشاكل بولية، مثل صعوبة بالتبول والحاجة إلى الذهاب للمرحاض على نحو متكرر. وقد يسفر أيضاً عن سريان البول على نحو أبطأ وأقل قوة. في حالة عدم العلاج، يوجد خطر بتوقف سريان البول تماماً (الاحتباس البولي الحاد). وذلك يقتضي علاج طبي فوري. وقد يلزم أحيانأ إجراء جراحة لإستئصال غدة البروستاتة أو تقليص حجمها.

دوتاستيرايد يخفض إنتاج هرمون يدعى دايهيدروتيستوستيرون، مما يساعد على تقليص حجم البروستاتة وزوال الأعراض. وذلك يؤدي إلى انخفاض خطر الإصابة بالاحتباس البولي الحاد والحاجة لإجراء جراحة. تامسولوسين يزاول مفعوله عن طريق إرخاء العضلات بغدة البروستاتة، مما يسهل التبول وتحسن الأعراض بسرعة.

ديودارت يستعمل لعلاج الرجال المصابين بتضخم البروستاتة (فرط تنسج البروستاتة الحميد) – وهو نمو غير سرطاني لغدة البروستاتة، ناتج عن الإنتاج المفرط لهرمون يدعى دايهيدروتيستوستيرون.

ديودارت هو عبارة عن توليفة لدواءين مختلفين وهما دوتاستيرايد وتامسولوسين. دوتاستيرايد ينتمي لمجموعة أدوية تدعى مثبطات مختزلة الألفا-5 وتامسولوسين ينتمي لمجموعة أدوية تدعى أدوية حاصرات لمستقبلات ألفا.

كلما ازداد حجم البروستاتة، قد يؤدي ذلك إلى مشاكل بولية، مثل صعوبة بالتبول والحاجة إلى الذهاب للمرحاض على نحو متكرر. وقد يسفر أيضاً عن سريان البول على نحو أبطأ وأقل قوة. في حالة عدم العلاج، يوجد خطر بتوقف سريان البول تماماً (الاحتباس البولي الحاد). وذلك يقتضي علاج طبي فوري. وقد يلزم أحيانأ إجراء جراحة لإستئصال غدة البروستاتة أو تقليص حجمها.

دوتاستيرايد يخفض إنتاج هرمون يدعى دايهيدروتيستوستيرون، مما يساعد على تقليص حجم البروستاتة وزوال الأعراض. وذلك يؤدي إلى انخفاض خطر الإصابة بالاحتباس البولي الحاد والحاجة لإجراء جراحة. تامسولوسين يزاول مفعوله عن طريق إرخاء العضلات بغدة البروستاتة، مما يسهل التبول وتحسن الأعراض بسرعة.

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ديودارت يجب تناوله دائماً على النحو الذي أخبرك به الطبيب أو الصيدلي تماماً. في حالة عدم تناوله بانتظام، قد تتأثر مراقبة مستويات المستضد الخاص بالبروستاتة لديك. يرجى الرجوع إلى الطبيب أو الصيدلي إذا لم تكن متأكداً.

الجرعة التي يجب تناولها

الجرعة الموصى بها هي كبسولة واحدة تؤخذ مرة واحدة في اليوم، بعد 30 دقيقة من نفس الوجبة كل يوم.

كيفية تناول العقار

يجب ابتلاع الكبسولات كاملةً مع بعض الماء. لا يجوز مضغ أو فتح الكبسولة. ملامسة مكونات الكبسولات قد يؤدي إلى احتقان الفم أو الحلق.

إذا تناولت من ديودارت أكثر مما يجب

اتصل بالطبيب أو الصيدلي لاستشارته إذا تناولت أكثر مما يجب تناوله من كبسولات ديودارت.

 

إذا نسيت أن تتناول ديودارت

لا تتناول جرعة مضاعفة للتعويض عن جرعة منسية. تناول فقط الجرعة التالية في الموعد المعتاد.

لا يجوز وقف تناول ديودارت دون استشارة

لا يجوز وقف تناول ديودارت دون استشارة الطبيب أولاً.

إذا كانت لديك أية أسئلة أخرى عن استعمال هذا المستحضر، اسأل الطبيب أو الصيدلي.

كشأن كافة الأدوية، ديودارت قد يسبب آثاراً جانبية، إلا أنها لا تصيب كل فرد.

ردود فعل تحسسية

علامات الإصابة بردود فعل تحسسية قد تشتمل على:

·      طفح جلدي (قد يكون مصحوباً بحكة).

·      شَرَى (مثل طفح جلدي ناتج عن نبات القُرَّاص).

·      تورم الجفنين، أو الوجه، أو الشفتين، أو الذراعين، أو الساقين.

ç اتصل بالطبيب على الفور في حالة الإصابة بأي من هذه الأعراض، وتوقف عن استعمال ديودارت.

الدوخة، الدوار والإغماء

ديودارت قد يسبب دوخة، ودواراً، وقد يسبب إغماء في أحيان نادرة. يجب توخي الحذر عند تغيير وضع الاستلقاء أو الجلوس إلى الجلوس أو الوقوف، خاصةً في حالة الاستيقاظ أثناء الليل، حتى تعرف كيف يؤثر هذا الدواء عليك. في حالة الشعور بدوخة أو دوار في أي وقت خلال فترة العلاج، يجب الجلوس أو الاستلقاء حتى زوال الأعراض.

 

تفاعلات جلدية خطيرة

علامات التفاعلات الجلدية الخطيرة قد تحتوى على:

-       إنتشار واسع لطفح مصحوب بفقاعات وتقشر الجلد، خصوصاً حول الفم، الأنف، العين والأعضاء التناسلية (متلازمة ستيڤينز-جونسون).

ç إتصل بطبيبك فوراً إذا حدثت لك هذه الأعراض وتوقف عن تناول ديودارت.

 

آثار جانبية شائعة

قد تؤثر حتى شخص واحد من بين 10 أشخاص يتناولون ديودارت

·      عَنَانَة (عدم القدرة على تحقيق انتصاب أو الحفاظ عليه).

·      انخفاض الإثارة الجنسية (الرغبة الجنسية)*.

·      صعوبة بالقذف، مثل انخفاض كمية السائل المنوي المنطلق أثناء ممارسة الجنس *

·      تضخم أو مضض الثدي (تثدي الرجل).

·      دوخة.

* في عدد صغير من الأشخاص قد تستمر بعض هذه الأعراض بعد التوقف عن تناول ديودارت.

 

آثار جانبية غير شائعة

قد تؤثر حتى شخص واحد من بين 100 شخص

·      فشل قلبي (حيث تنخفض كفاءة القلب في ضخ الدم حول الجسم. قد تصاب بأعراض مثل ضيق النفس، وإرهاق شديد، وتورم بالكاحلين والساقين).

·      انخفاض ضغط الدم عند الوقوف.

·      ضربات قلب سريعة (خفقان).

·      إمساك، إسهال، قيء، شعور بغثيان (غثيان).

·      وهن أو فقدان القوة.

·      صداع.

·      حكة، أو انسداد، أو رشح أنفي (التهاب الأنف).

·      طفح جلدي، شَرَى، حكة.

·      فقدان الشعر (غالباً من الجسم) أو نمو الشعر.

 

آثار جانبية نادرة

قد تؤثر حتى شخص واحد من بين 1000 شخص

·      تورم الجفنين، أو الوجه، أو الشفتين، أو الذراعين، أو الساقين (وذمة وعائية).

·      إغماء.

 

آثار جانبية نادرة جداً

قد تؤثر حتى شخص واحد من بين 10.000 شخص

·      انتصاب القضيب على نحو مستديم ومؤلم (إنتصاب مستمر).

·      تفاعلات جلدية خطيرة (متلازمة ستيڤينز-جونسون).

 

آثار جانبية أخرى

آثار جانبية أخرى قد حدثت في عدد صغير من الأشخاص، ولكن معدل حدوثها غير معروف بالتحديد (لا يمكن تقدير المعدل من البيانات المتاحة):

·      ضربات قلب غير طبيعية أو سريعة (عدم انتظام ضربات القلب، سرعة ضربات القلب أو رجفان أذيني).

·      ضيق في التنفس (ضيق النفس).

·      إكتئاب.

·      ألم وتورم في الخيصيتين.

·      نزيف الأنف.

·      طفح جلدي شديد.

·      تغيرات في الرؤية (زغللة أو ضعف النظر).

·      جفاف الفم.

 

ç إذا أصبح أي من الآثار الجانبية خطيراً، أو إذا لاحظت أية آثار جانبية غير مدرجة في هذه النشرة، يرجى إبلاغ الطبيب أو الصيدلي.

·       احتفظ بالأدوية بعيداً عن متناول ونظر الأطفال.

·       لا تستخدم ديودارت بعد تاريخ انتهاء الصلاحية المذكور على العبوة بعد كلمة "Exp".

·       لا يجوز حفظ ديودارت في درجة حرارة تزيد عن 25°م.

·       إذا أخبرك الطبيب بوقف تناول هذا الدواء، فمن المهم أن تعيد أي كمية متبقية إلى الصيدلي.

·       لا ينبغي التخلص من الأدوية عن طريق مياة الصرف الصحي أو المخلفات المنزلية. إسأل الصيدلي عن كيفية التخلص من الأدوية التي لم تعد بحاجة إليها. سوف تساعد هذه التدابير في حماية البيئة.

المادتان الفعالتان هما دوتاستيرايد وتامسولوسين هيدروكلورايد. كل كبسولة تحتوي على 0.5 مجم دوتاستيرايد و0.4 مجم تامسولوسين هيدروكلورايد.

المكونات الأخرى هي:

·      غلاف الكبسولة الصلبة: هيپروميلوز، كاراچينان (E407)، كلوريد البوتاسيوم، ثاني أكسيد التيتانيوم (E171)، أكسيد الحديد الأحمر، (E172)، صبغ أصفر غروب الشمس (E110)، شمع كارنوبا، نشا الذرة.

·      داخل الكبسولة الصلبة: أول وثاني جليسريدات حمض الكپريليك/الكپريك وبيوتيل هيدروكسي الطولوين (E321)، چيلاتين، جليسرول، ثاني أكسيد التيتانيوم (E171)، أكسيد الحديد الأصفر (E172)، ثالث الجليسريدات (سلسلة متوسطة)، ليسيثين (قد يحتوي على زيت الصويا)، سليولوز دقيق التبلور، بلمر حمض الميثاكريليك- أكريلات الإيثيل المشترك (يحتوي على پولي سوربات 80 ولوريل سلفات الصوديوم)، تالك، ثالث إيثيل السترات.

·      حبر طباعة أسود (SW-9010 أو SW-9008): شيلاك، جلايكول الپروپيلين، أكسيد الحديد الأسود (E172)، هيدروكسيد البوتاسيوم (في الحبر الأسود SW-9008 فقط).

هذا الدواء هو عبارة عن كبسولة صلبة مستطيلة الشكل ذات جسم بني وغطاء برتقالي منقوش عليها GS 7CZ بالحبر الأسود. العقار متوفر في عبوات تحتوي على 7 كبسولات، و30، و90 كبسولة. قد لا تتوفر جميع أحجام العبوات في السوق. ديودارت علامة تجارية مملوكة اومرخصة لمجموعة شركات جلاكسو سميث كلاين. © 2019 جلاكسو سميث كلاين، جميع الحقوق محفوظة.

صاحبة رخصة التسويق وإنتاج

جلاكسو سميث كلاين للتصدير المحدودة

العنوان: 980 طريق جريت ويست، برينتفورد، ميدلسكس، TW8 9GS، إنكلترا

 

إنتاج:

كاتالانت ألمانيا شورندورف Gmbh

ستئينبيستراسي 2

73614 شورندورف

ألمانيا

للإبلاغ عن أي آثار جانبية:

المملكة العربية السعودية

- - المركز الوطني للتيقظ والسلامة الدوائية

·         فاكس: 7662-205-11-966 +

·         الاتصال بالمركز الوطني للتيقظ والسلامة الدوائية. هاتف:2038222-11-966+ تحويلة:2340-2356-2317

·         الخط الساخن:19999

·         البريد الإلكتروني: npc.drug@sfda.gov.sa

·         الموقع الإلكتروني: www.sfda.gov.sa/npc

- جلاكسو سميث كلاين المكتب الرئيسي، جدة.

·         هاتف: 6536666 (12) 966 +

·         المحمول : 9882-904-56  966 +

·         البريد اللكتروني : sa.aermi-saudi@gsk.com

·         الموقع الإلكتروني: https://healthksa.gsk.com/

·         ص.ب 55850، جدة 21544، المملكة العربية السعودية.

 

إن هذا الدواء

- الدواء مستحضر يؤثر على صحتك، واستهلاكه خلافا للتعليمات يعرضك للخطر.

- اتبع بدقة وصفة الطبيب، وطريقة الاستعمال المنصوص عليها، وتعليمات الصيدلانى الذى صرفها لك.

- فالطبيب و الصيدلانى هما الخبيران بالدواء، وبنفعه و ضرره.

- لا تقطع مدة العلاج المحددة لك من تلقاء نفسك.

- لا تكرر صرف الدواء بدون استشارة الطبيب.

- احتفظ بجميع الأدوية بعيداً عن متناول لأطفال.   

                                                                                                مجلس وزراء الصحة العرب

                                                                                                   اتحاد الصيادلة العرب

 

 

 

رقم الإصدار:EU v12 تاريخ الإصدار:17 نوفمبر 2017
 Read this leaflet carefully before you start using this product as it contains important information for you

Duodart 0.5 mg / 0.4 mg hard capsules

Each hard capsule contains 0.5 mg dutasteride and 0.4 mg tamsulosin hydrochloride, (equivalent to 0.367 mg tamsulosin). Excipients with known effect Each capsule contains lecithin (which may contain soya oil) and Sunset Yellow (E 110). Each capsule contains ≤ 0.1 mg sunset yellow. For the full list of excipients, see section 6.1.

Capsule, hard. Oblong, hard capsules with a brown body and an orange cap imprinted with GS 7CZ in black ink. Each hard capsule contains tamsulosin hydrochloride modified release pellets and one dutasteride soft gelatin capsule.

Treatment of moderate to severe symptoms of benign prostatic hyperplasia (BPH).

 

Reduction in the risk of acute urinary retention (AUR) and surgery in patients with moderate to severe symptoms of BPH.

 

For information on effects of treatment and patient populations studied in clinical trials please see section 5.1.


Posology

 

Adults (including elderly)

 

The recommended dose of Duodart is one capsule (0.5 mg/ 0.4 mg) once daily.

 

Where appropriate, Duodart may be used to substitute concomitant dutasteride and tamsulosin hydrochloride in existing dual therapy to simplify treatment.

 

Where clinically appropriate, direct change from dutasteride or tamsulosin hydrochloride monotherapy to Duodart may be considered.

 

Renal impairment

 

The effect of renal impairment on dutasteride-tamsulosin pharmacokinetics has not been studied. No adjustment in dosage is anticipated for patients with renal impairment (see section 4.4 and 5.2).

 

Hepatic impairment

 

The effect of hepatic impairment on dutasteride-tamsulosin pharmacokinetics has not been studied so caution should be used in patients with mild to moderate hepatic impairment (see section 4.4 and section 5.2). In patients with severe hepatic impairment, the use of Duodart is contraindicated (see section 4.3).

 

Paediatric population

 

Dutasteride-tamsulosin is contraindicated in the paediatric population (under 18 years of age) (see section 4.3).

 

Method of administration

 

For oral use.

 

Patients should be instructed to swallow the capsules whole, approximately 30 minutes after the same meal each day. The capsules should not be chewed or opened. Contact with the contents of the dutasteride capsule contained within the hard-shell capsule may result in irritation of the oropharyngeal mucosa.


Duodart is contraindicated in: - women and children and adolescents (see section 4.6 ). - patients with hypersensitivity to dutasteride, other 5-alpha reductase inhibitors, tamsulosin (including tamsulosin-induced angio-edema), soya, peanut or any of the other excipients listed in section 6.1. - patients with a history of orthostatic hypotension. - patients with severe hepatic impairment.

Combination therapy should be prescribed after careful benefit risk assessment due to the potential increased risk of adverse events (including cardiac failure) and after consideration of alternative treatment options including monotherapies.

 

Prostate cancer and high grade tumours

 

The REDUCE study, a 4-year, multicentre, randomised, double-blind, placebo controlled study investigated the effect of dutasteride 0.5 mg daily on patients with a high risk for prostate cancer (including men 50 to 75 years of age with PSA levels of 2.5 to 10 ng/ml and a negative prostate biopsy 6 months before study enrolment) compared to placebo. Results of this study revealed a higher incidence of Gleason 8 – 10 prostate cancers in dutasteride treated men (n=29, 0.9%) compared to placebo (n=19, 0.6%). The relationship between dutasteride and Gleason 8 – 10 prostate cancers is not clear. Thus, men taking Duodart should be regularly evaluated for prostate cancer (see section 5.1).

 

Prostate specific antigen (PSA)

 

Serum prostate-specific antigen (PSA) concentration is an important component in the detection of prostate cancer.  Duodart causes a decrease in mean serum PSA levels by approximately 50%, after 6 months of treatment. 

 

Patients receiving Duodart should have a new PSA baseline established after 6 months of treatment with Duodart.  It is recommended to monitor PSA values regularly thereafter.  Any confirmed increase from lowest PSA level while on Duodart may signal the presence of prostate cancer or noncompliance to therapy with Duodart and should be carefully evaluated, even if those values are still within the normal range for men not taking a 5-alpha reductase inhibitor (see section 5.1).  In the interpretation of a PSA value for a patient taking dutasteride, previous PSA values should be sought for comparison.

 

Treatment with Duodart does not interfere with the use of PSA as a tool to assist in the diagnosis of prostate cancer after a new baseline has been established.

 

Total serum PSA levels return to baseline within 6 months of discontinuing treatment.  The ratio of free to total PSA remains constant even under the influence of Duodart.  If clinicians elect to use percent free PSA as an aid in the detection of prostate cancer in men undergoing Duodart therapy, no adjustment to its value appears necessary.

 

Digital rectal examination, as well as other evaluations for prostate cancer or other conditions which can cause the same symptoms as BPH, must be performed on patients prior to initiating therapy with Duodart and periodically thereafter.

 

Cardiovascular adverse events

 

In two 4-year clinical studies, the incidence of cardiac failure (a composite term of reported events, primarily cardiac failure and congestive cardiac failure) was marginally higher among subjects taking the combination of dutasteride and an alpha1- adrenoceptor antagonist, primarily tamsulosin, than it was among subjects not taking the combination.  However, the incidence of cardiac failure in these trials was lower in all actively treated groups compared to the placebo group, and other data available for dutasteride or alpha1-adrenoceptor antagonists do not support a conclusion on increased cardiovascular risks (see section 5.1).

 

Breast neoplasia

 

There have been rare reports of male breast cancer reported in men taking dutasteride in clinical trials and during the post-marketing period.  However, epidemiological studies showed no increase in the risk of developing male breast cancer with the use of 5-alpha reductase inhibitors (see section 5.1).  Physicians should instruct their patients to promptly report any changes in their breast tissue such as lumps or nipple discharge.

 

Renal impairment

 

The treatment of patients with severe renal impairment (creatinine clearance of less than 10 ml/min) should be approached with caution as these patients have not been studied.

 

Hypotension

 

Orthostatic: As with other alpha1- adrenoceptor antagonists, a reduction in blood pressure can occur during treatment with tamsulosin, as a result of which, rarely, syncope can occur. Patients beginning treatment with Duodart should be cautioned to sit or lie down at the first signs of orthostatic hypotension (dizziness, weakness) until the symptoms have resolved.

 

In order to minimise the potential for developing postural hypotension the patient should be haemodynamically stable on an alpha1- adrenoceptor antagonist prior to initiating use of PDE5 inhibitors.

Symptomatic: Caution is advised when alpha adrenergic blocking agents including tamsulosin are co-administered with PDE5 inhibitors (e.g. sildenafil, tadalafil, vardenafil). Alpha1- adrenoceptor antagonists and PDE5 inhibitors are both vasodilators that can lower blood pressure. Concomitant use of these two drug classes can potentially cause symptomatic hypotension (see section 4.5).

 

Intraoperative Floppy Iris Syndrome

 

Intraoperative Floppy Iris Syndrome (IFIS, a variant of small pupil syndrome) has been observed during cataract surgery in some patients on or previously treated with tamsulosin. IFIS may increase the risk of eye complications during and after the operation. The initiation of therapy with Duodart in patients for whom cataract surgery is scheduled is therefore not recommended.

 

During pre-operative assessment, cataract surgeons and ophthalmic teams should consider whether patients scheduled for cataract surgery are being or have been treated with Duodart in order to ensure that appropriate measures will be in place to manage the IFIS during surgery.

 

Discontinuing tamsulosin 1 – 2 weeks prior to cataract surgery is anecdotally considered helpful, but the benefit and duration of stopping therapy prior to cataract surgery has not yet been established.

 

Leaking capsules

 

Dutasteride is absorbed through the skin, therefore, women, children and adolescents must avoid contact with leaking capsules (see section 4.6).  If contact is made with leaking capsules, the contact area should be washed immediately with soap and water.

 

Inhibitors of CYP3A4 and CYP2D6

 

Concomitant administration of tamsulosin hydrochloride with strong inhibitors of CYP3A4 (e.g. ketoconazole), or to a lesser extent, with strong inhibitors of CYP2D6 (e.g. paroxetine) can increase tamsulosin exposure (see section 4.5). Tamsulosin hydrochloride is therefore not recommended in patients taking a strong CYP3A4 inhibitor and should be used with caution in patients taking a moderate CYP3A4 inhibitor, a strong or moderate CYP2D6 inhibitor, a combination of both CYP3A4 and CYP2D6 inhibitors, or in patients known to be poor metabolisers of CYP2D6.

 

Hepatic impairment

 

Duodart has not been studied in patients with liver disease.  Caution should be used in the administration of Duodart to patients with mild to moderate hepatic impairment (see section 4.2, section 4.3 and section 5.2).

 

Excipients

 

This medicinal product contains the colouring agent Sunset Yellow (E110), which may cause allergic reactions.


There have been no drug interaction studies for Duodart. The following statements reflect the information available on the individual components.

 

Dutasteride

 

For information on the decrease of serum PSA levels during treatment with dutasteride and guidance concerning prostate cancer detection, please see section 4.4.

 

Effects of other drugs on the pharmacokinetics of dutasteride

 

Dutasteride is mainly eliminated via metabolism.  In vitro studies indicate that this metabolism is catalysed by CYP3A4 and CYP3A5.  No formal interaction studies have been performed with potent CYP3A4 inhibitors.  However, in a population pharmacokinetic study, dutasteride serum concentrations were on average 1.6 to 1.8 times greater, respectively, in a small number of patients treated concurrently with verapamil or diltiazem (moderate inhibitors of CYP3A4 and inhibitors of P-glycoprotein) than in other patients.

 

Long-term combination of dutasteride with drugs that are potent inhibitors of the enzyme CYP3A4 (e.g. ritonavir, indinavir, nefazodone, itraconazole, ketoconazole administered orally) may increase serum concentrations of dutasteride. Further inhibition of 5-alpha reductase at increased dutasteride exposure, is not likely.  However, a reduction of the dutasteride dosing frequency can be considered if side effects are noted.  It should be noted that in the case of enzyme inhibition, the long half-life may be further prolonged and it can take more than 6 months of concurrent therapy before a new steady state is reached.

 

Administration of 12 g cholestyramine one hour after a 5 mg single dose of dutasteride did not affect the pharmacokinetics of dutasteride.

 

Effects of dutasteride on the pharmacokinetics of other drugs

 

In a small study (n=24) of two weeks duration in healthy men, dutasteride (0.5 mg daily) had no effect on the pharmacokinetics of tamsulosin or terazosin. There was also no indication of a pharmacodynamic interaction in this study.

 

Dutasteride has no effect on the pharmacokinetics of warfarin or digoxin. This indicates that dutasteride does not inhibit/induce CYP2C9 or the transporter P-glycoprotein.  In vitro interaction studies indicate that dutasteride does not inhibit the enzymes CYP1A2, CYP2D6, CYP2C9, CYP2C19 or CYP3A4.

 

Tamsulosin

 

Concomitant administration of tamsulosin hydrochloride with drugs which can reduce blood pressure, including anaesthetic agents, PDE5 inhibitors and other alpha1- adrenoceptor antagonists could lead to enhanced hypotensive effects. Dutasteride-tamsulosin should not be used in combination with other alpha1- adrenoceptor antagonists.

 

Concomitant administration of tamsulosin hydrochloride and ketoconazole (a strong CYP3A4 inhibitor) resulted in an increase of the Cmax and AUC of tamsulosin hydrochloride by a factor of 2.2 and 2.8 respectively. Concomitant administration of tamsulosin hydrochloride and paroxetine (a strong CYP2D6 inhibitor) resulted in an increase of the Cmax and AUC of tamsulosin hydrochloride by a factor of 1.3 and 1.6 respectively.  A similar increase in exposure is expected in CYP2D6 poor metabolisers as compared to extensive metabolisers when co-administered with a strong CYP3A4 inhibitor.  The effects of co-administration of both CYP3A4 and CYP2D6 inhibitors with tamsulosin hydrochloride have not been evaluated clinically, however there is a potential for significant increase in tamsulosin exposure (see section 4.4).

 

Concomitant administration of tamsulosin hydrochloride (0.4 mg) and cimetidine (400 mg every six hours for six days) resulted in a decrease in the clearance (26%) and an increase in the AUC (44%) of tamsulosin hydrochloride. Caution should be used when dutasteride-tamsulosin is used in combination with cimetidine.

 

A definitive drug-drug interaction study between tamsulosin hydrochloride and warfarin has not been conducted. Results from limited in vitro and in vivo studies are inconclusive. Diclofenac and warfarin, however, may increase the elimination rate of tamsulosin. Caution should be exercised with concomitant administration of warfarin and tamsulosin hydrochloride.

 

No interactions have been seen when tamsulosin hydrochloride was given concomitantly with either atenolol, enalapril, nifedipine or theophylline. Concomitant furosemide brings about a fall in plasma levels of tamsulosin, but as levels remain within the normal range posology need not be adjusted.

 

In vitro neither diazepam nor propranolol, trichlormethiazide, chlormadinon, amitryptyline, diclofenac, glibenclamide and simvastatin change the free fraction of tamsulosin in human plasma. Neither does tamsulosin change the free fractions of diazepam, propranolol, trichlormethiazide, and chlormadinon.


Duodart is contraindicated for use by women. There have been no studies to investigate the effect of Duodart on pregnancy, lactation and fertility. The following statements reflect the information available from studies with the individual components (see section 5.3).

 

Pregnancy

 

As with other 5 alpha reductase inhibitors, dutasteride inhibits the conversion of testosterone to dihydrotestosterone and may, if administered to a woman carrying a male foetus, inhibit the development of the external genitalia of the foetus (see section 4.4).  Small amounts of dutasteride have been recovered from the semen in subjects receiving dutasteride. It is not known whether a male foetus will be adversely affected if his mother is exposed to the semen of a patient being treated with dutasteride (the risk of which is greatest during the first 16 weeks of pregnancy).

 

As with all 5 alpha reductase inhibitors, when the patient's partner is or may potentially be pregnant it is recommended that the patient avoids exposure of his partner to semen by use of a condom.

 

Administration of tamsulosin hydrochloride to pregnant female rats and rabbits showed no evidence of foetal harm.

 

For information on preclinical data, see section 5.3.

 

Breast-feeding

 

It is not known whether dutasteride or tamsulosin are excreted in human milk.

 

Fertility

 

Dutasteride has been reported to affect semen characteristics (reduction in sperm count, semen volume, and sperm motility) in healthy men (see section 5.1). The possibility of reduced male fertility cannot be excluded.

 

Effects of tamsulosin hydrochloride on sperm counts or sperm function have not been evaluated.


No studies on the effects of Duodart on the ability to drive and use machines have been performed. However, patients should be informed about the possible occurrence of symptoms related to orthostatic hypotension such as dizziness when taking Duodart.


The data presented here relate to the co-administration of dutasteride and tamsulosin from the 4 year analysis of the CombAT (Combination of Avodart and Tamsulosin) study, a comparison of dutasteride 0.5mg and tamsulosin 0.4mg once daily for four years as co-administration or as monotherapy. Bioequivalence of Duodart with co-administered dutasteride and tamsulosin has been demonstrated (see section 5.2). Information on the adverse event profiles of the individual components (dutasteride and tamsulosin) is also provided. Note that not all the adverse events reported with the individual components have been reported with Duodart and these are included for information for the prescriber.

Data from the 4 year CombAT study have shown that the incidence of any investigator-judged drug-related adverse event during the first, second, third and fourth years of treatment respectively was 22% 6%, 4% and 2% for dutasteride + tamsulosin co-administration therapy, 15%, 6%, 3% and 2%  for dutasteride monotherapy and 13%, 5%, 2% and 2% for tamsulosin monotherapy. The higher incidence of adverse events in the co-administration therapy group in the first year of treatment was due to a higher incidence of reproductive disorders, specifically ejaculation disorders, observed in this group.

 

The investigator-judged drug-related adverse events have been reported with an incidence of greater than or equal to 1% during the first year of treatment in the CombAT Study, BPH monotherapy clinical studies and REDUCE study are shown in the table below.

In addition the undesirable effects for tamsulosin below are based on information available in the public domain. The frequencies of adverse events may increase when the combination therapy is used.

 

The frequency of adverse reactions identified from clinical trials:

Common; ≥1/100 to <1/10, Uncommon; ≥1/1000 to <1/100, Rare; ≥1/10,000 to <1/1000, Very rare; <1/10,000. Within each SOC grouping, undesirable effects are presented in order of decreasing seriousness.

System organ class

Adverse reactions

Dutasteride+

tamsulosina

Dutasteride

Tamsulosinc

Nervous system disorders

Syncope

-

-

Rare

 

Dizziness

Common

-

Common

 

Headache

-

-

Uncommon

Cardiac disorders

Cardiac failure (Composite term1)

 

Uncommon

Uncommond

-

 

Palpitations

-

-

Uncommon

Vascular disorders

Orthostatic hypotension

 

-

-

Uncommon

Respiratory, thoracic and mediastinal disorders

Rhinitis

 

-

-

Uncommon

Gastrointestinal disorders

Constipation

 

-

-

Uncommon

Diarrhoea

 

-

-

Uncommon

Nausea

-

-

Uncommon

Vomiting

-

-

Uncommon

Skin and subcutaneous disorders

Angioedema

 

-

-

Rare

Stevens-Johnson syndrome

 

-

-

Very rare

 

Urticaria

 

-

-

Uncommon

 

Rash   

-

-

Uncommon

 

Pruritus

-

-

Uncommon

Reproductive system and breast disorders

Priapism

 

-

-

Very rare

Impotence3

Common

Commonb

-

Altered (decreased) libido3

 

Common

Commonb

-

Ejaculation disorders3 ^

 

Common

Commonb

Common

Breast disorders2

 

Common

Commonb

-

General disorders and administration site disorders

Asthenia

 

-

-

Uncommon

a. Dutasteride + tamsulosin: from CombAT study - the frequencies of these adverse events decrease over time of treatment, from year 1 to year 4.

b. Dutasteride: from BPH monotherapy clinical studies.

c. Tamsulosin: from EU Core Safety Profile for tamsulosin.

d. REDUCE study (see section 5.1).

1. Cardiac failure composite term comprised of cardiac failure congestive, cardiac failure, left ventricular failure, cardiac failure acute, cardiogenic shock, left ventricular failure acute, right ventricular failure, right ventricular failure acute, ventricular failure, cardiopulmonary failure, congestive cardiomyopathy.

2. Includes breast tenderness and breast enlargement.

3. These sexual adverse events are associated with dutasteride treatment (including monotherapy and combination with tamsulosin). These adverse events may persist after treatment discontinuation. The role of dutasteride in this persistence is not known.

^. Includes semen volume decreased.

 

OTHER DATA

 

The REDUCE study revealed a higher incidence of Gleason 8-10 prostate cancers in dutasteride treated men compared to placebo (see sections 4.4 and 5.1). Whether the effect of dutasteride to reduce prostate volume, or study related factors, impacted the results of this study has not been established.

 

The following has been reported in clinical trials and post-marketing use: male breast cancer (see section 4.4).

 

Post marketing Data

 

Adverse events from world-wide post-marketing experience are identified from spontaneous post-marketing reports; therefore the true incidence is not known.

 

Dutasteride

 

Immune system disorders

Not known: Allergic reactions, including rash, pruritus, urticaria, localised oedema, and angioedema.

 

Psychiatric disorders

Not known: Depression

 

Skin and subcutaneous tissue disorders

Uncommon: Alopecia (primarily body hair loss), hypertrichosis.

 

Reproductive system and breast disorders

Not known: Testicular pain and testicular swelling

 

Tamsulosin

 

During postmarketing surveillance, reports of Intraoperative Floppy Iris Syndrome (IFIS), a variant of small pupil syndrome, during cataract surgery have been associated with alpha1- adrenoceptor antagonists, including tamsulosin (see section 4.4).

 

In addition atrial fibrillation, arrhythmia, tachycardia, dyspnoea, epistaxis, vision blurred, visual impairment, erythema multiforme, dermatitis exfoliative, ejaculation disorder, retrograde ejaculation, ejaculation failure and dry mouth have been reported in association with tamsulosin use. The frequency of events and the role of tamsulosin in their causation cannot be reliably determined.

 

 

To report any side effect(s):

Kingdom of Saudi Arabia

-National Pharmacovigilance centre (NPC)

•          Fax: +966-11-205-7662

•          Call NPC at +966-11-2038222, Ext: 2317-2356-2340

•          Reporting hotline: 19999

•          E-mail: npc.drug@sfda.gov.sa

•          Website: www.sfda.gov.sa/npc

 

-GlaxoSmithKline - Head Office, Jeddah

•          Tel: +966-12-6536666

•          Mobile: +966-56-904-9882

•          Email: sa.aermi-saudi@gsk.com

•          website: https://healthksa.gsk.com/

•          P.O. Box 55850, Jeddah 21544, Saudi Arabia

 


No data are available with regard to overdosage of Duodart. The following statements reflect the information available on the individual components.

 

Dutasteride

 

In volunteer studies, single daily doses of dutasteride up to 40 mg/day (80 times the therapeutic dose) have been administered for 7 days without significant safety concerns.  In clinical studies, doses of 5 mg daily have been administered to subjects for 6 months with no additional adverse effects to those seen at therapeutic doses of 0.5 mg.  There is no specific antidote for dutasteride, therefore, in suspected overdosage symptomatic and supportive treatment should be given as appropriate. 

 

Tamsulosin

 

Acute overdose with 5 mg tamsulosin hydrochloride has been reported. Acute hypotension (systolic blood pressure 70 mm Hg), vomiting and diarrhoea were observed which were treated with fluid replacement and the patient could be discharged the same day. In case of acute hypotension occurring after overdosage cardiovascular support should be given. Blood pressure can be restored and heart rate brought back to normal by lying the patient down. If this does not help then volume expanders, and when necessary, vasopressors could be employed. Renal function should be monitored and general supportive measures applied. Dialysis is unlikely to be of help as tamsulosin is very highly bound to plasma proteins.

 

Measures, such as emesis, can be taken to impede absorption. When large quantities are involved, gastric lavage can be applied and activated charcoal and an osmotic laxative, such as sodium sulphate, can be administered.


Pharmacotherapeutic group: Alpha-adrenoreceptor antagonists, ATC code: G04CA52

 

Dutasteride-tamsulosin is a combination of two drugs: dutasteride, a dual 5 α-reductase inhibitor (5 ARI) and tamsulosin hydrochloride, an antagonist of α1a and α1d adrenoreceptors.  These drugs have complementary mechanisms of action that rapidly improve symptoms, urinary flow and reduce the risk of acute urinary retention (AUR) and the need for BPH related surgery.

 

Dutasteride inhibits both type 1 and type 2, 5 alpha-reductase isoenzymes, which are responsible for the conversion of testosterone to dihydrotestosterone (DHT). DHT is the androgen primarily responsible for prostate growth and BPH development. Tamsulosin inhibits α1a and α1d adrenergic receptors in the stromal prostatic smooth muscle and bladder neck.  Approximately 75% of the α1-receptors in the prostate are of the α1a subtype.

 

Dutasteride co-administration with tamsulosin

 

The following statements reflect the information available on dutasteride and tamsulosin co-administration therapy.

 

Dutasteride 0.5 mg/day (n = 1,623), tamsulosin 0.4 mg/day (n = 1,611) or the co-administration of Dutasteride 0.5 mg plus tamsulosin 0.4 mg (n = 1,610) were evaluated in male subjects with moderate to severe symptoms of BPH who had prostates ³30ml and a PSA value within the range 1.5 - 10 ng/mL in a 4 year multicentre, multinational, randomized double‑blind, parallel group study. Approximately 53% of subjects had previous exposure to 5-alpha reductase inhibitor or alpha1- adrenoceptor antagonist. The primary efficacy endpoint during the first 2 years of treatment was change in International Prostate Symptom Score (IPSS), an 8-item instrument based on AUA-SI with an additional question on quality of life.  Secondary efficacy endpoints at 2 years included maximum urine flow rate (Qmax) and prostate volume. The combination achieved significance for IPSS from Month 3 compared to dutasteride and from Month 9 compared to tamsulosin.  For Qmax combination achieved significance from Month 6 compared to both dutasteride and tamsulosin.

 

The combination of dutasteride and tamsulosin provides superior improvement in symptoms than either component alone. After 2 years of treatment, co-administration therapy showed a statistically significant adjusted mean improvement in symptom scores from baseline of -6.2 units.

 

The adjusted mean improvement in flow rate from baseline was 2.4 ml/sec for co-administration therapy, 1.9 ml/sec for dutasteride and 0.9 ml/sec for tamsulosin.  The adjusted mean improvement in BPH Impact Index (BII) from baseline was -2.1 units for co-administration therapy, -1.7 for dutasteride and -1.5 for tamsulosin. These improvements in flow rate and BII were statistically significant for co-administration therapy compared to both monotherapies.

 

The reduction in total prostate volume and transition zone volume after 2 years of treatment was statistically significant for co-administration therapy compared to tamsulosin monotherapy alone.

 

The primary efficacy endpoint at 4 years of treatment was time to first event of AUR or BPH-related surgery. After 4 years of treatment, combination therapy statistically significantly reduced the risk of AUR or BPH-related surgery (65.8% reduction in risk p<0.001 [95% CI 54.7% to 74.1%]) compared to tamsulosin monotherapy. The incidence of AUR or BPH-related surgery by Year 4 was 4.2% for combination therapy and 11.9% for tamsulosin (p<0.001). Compared to dutasteride monotherapy, combination therapy reduced the risk of AUR or BPH-related surgery by 19.6% (p=0.18 [95% CI -10.9% to 41.7%]). The incidence of AUR or BPH-related surgery by Year 4 was 5.2% for dutasteride.

 

Secondary efficacy endpoints after 4 years of treatment included time to clinical progression (defined as a composite of: IPSS deterioration by ³4 points, BPH-related events of AUR, incontinence, urinary tract infection (UTI), and renal insufficiency) change in International Prostate Symptom Score (IPSS), maximum urine flow rate (Qmax) and prostate volume. IPSS is an 8-item instrument based on the AUA-SI with an additional question on quality of life. Results following 4 years of treatment are presented below:

Parameter

 

Time-point

Combination

Dutasteride

Tamsulosin

AUR or BPH related surgery (%)

Incidence at Month 48

4.2

5.2

11.9a

Clinical progression* (%)

Month 48

12.6

17.8b

21.5a

IPSS (units)

[Baseline]

Month 48 (Change from Baseline)

[16.6]

-6.3

[16.4]

-5.3b

[16.4]

-3.8a

Qmax (mL/sec)

[Baseline]

Month 48 (Change from Baseline)

[10.9]

2.4

[10.6]

2.0

[10.7]

0.7a

Prostate Volume (ml)

[Baseline]

Month 48 (% Change from Baseline)

[54.7]

-27.3

[54.6]

-28.0

[55.8]

+4.6a

Prostate Transition Zone Volume (ml)#

[Baseline]

Month 48 (% Change from Baseline)

[27.7]

-17.9

[30.3]

-26.5

[30.5]

18.2a

BPH Impact Index (BII) (units)

[Baseline]

Month 48 (Change from Baseline)

[5.3]

-2.2

[5.3]

-1.8b

[5.3]

-1.2a

IPSS Question 8 (BPH-related Health Status) (units)

 

[Baseline]

Month 48 (Change from Baseline)

[3.6]

-1.5

[3.6]

-1.3b

[3.6]

-1.1a

Baseline values are mean values and changes from baseline are adjusted mean changes.

* Clinical progression was defined as a composite of: IPSS deterioration by ³4 points, BPH-related events of AUR, incontinence, UTI, and renal insufficiency.

# Measured at selected sites (13% of randomized patients)

a. Combination achieved significance (p<0.001) vs. tamsulosin at Month 48

b. Combination achieved significance (p<0.001) vs. dutasteride at Month 48

 

Dutasteride

 

Dutasteride 0.5 mg/day or placebo was evaluated in 4325 male subjects with moderate to severe symptoms of BPH who had prostates ≥30ml and a PSA value within the range 1.5 - 10 ng/mL in three primary efficacy 2-year multicenter, multinational, placebo controlled, double-blind studies. The studies then continued with an open-label extension to 4 years with all patients remaining in the study receiving dutasteride at the same 0.5 mg dose. 37% of initially placebo-randomized patients and 40% of dutasteride-randomized patients remained in the study at 4 years. The majority (71%) of the 2,340 subjects in the open-label extensions completed the 2 additional years of open-label treatment.

 

The most important clinical efficacy parameters were American Urological Association Symptom Index (AUA-SI), maximum urinary flow (Qmax) and the incidence of acute urinary retention and BPH-related surgery.

 

AUA-SI is a seven-item questionnaire about BPH-related symptoms with a maximum score of 35.  At baseline the average score was approx. 17.  After six months, one and two years treatment the placebo group had an average improvement of 2.5, 2.5 and 2.3 points respectively while the Avodart group improved 3.2, 3.8 and 4.5 points respectively.  The differences between the groups were statistically significant. The improvement in AUA-SI seen during the first 2 years of double-blind treatment was maintained during an additional 2 years of open-label extension studies.

 

Qmax (maximum urine flow)

 

Mean baseline Qmax for the studies was approx 10 ml/sec (normal Qmax ³ 15 ml/sec). After one and two years treatment the flow in the placebo group had improved by 0.8 and 0.9 ml/sec respectively and 1.7 and 2.0 ml/sec respectively in the Avodart group.  The difference between the groups was statistically significant from Month 1 to Month 24. The increase in maximum urine flow rate seen during the first 2 years of double-blind treatment was maintained during an additional 2 years of open-label extension studies.

 

Acute Urinary Retention and Surgical Intervention

 

After two years of treatment, the incidence of AUR was 4.2% in the placebo group against 1.8% in the Avodart group (57% risk reduction).  This difference is statistically significant and means that 42 patients (95% CI 30-73) need to be treated for two years to avoid one case of AUR.

 

The incidence of BPH-related surgery after two years was 4.1% in the placebo group and 2.2% in the Avodart group (48% risk reduction).  This difference is statistically significant and means that 51 patients (95% CI 33-109) need to be treated for two years to avoid one surgical intervention.

 

Hair distribution

The effect of dutasteride on hair distribution was not formally studied during the phase III programme, however, 5 alpha-reductase inhibitors could reduce hair loss and may induce hair growth in subjects with male pattern hair loss (male androgenetic alopecia).

 

Thyroid function

Thyroid function was evaluated in a one year study in healthy men.  Free thyroxine levels were stable on dutasteride treatment but TSH levels were mildly increased (by 0.4 MCIU/mL) compared to placebo at the end of one year's treatment.  However, as TSH levels were variable, median TSH ranges (1.4 - 1.9 MCIU/mL) remained within normal limits (0.5 - 5/6 MCIU/mL), free thyroxine levels were stable within the normal range and similar for both placebo and dutasteride treatment, the changes in TSH were not considered clinically significant.  In all the clinical studies, there has been no evidence that dutasteride adversely affects thyroid function.

 

Breast neoplasia

 

In the 2 year clinical trials, providing 3374 patient years of exposure to dutasteride, and at the time of registration in the 2 year open label extension, there were 2 cases of male breast cancer reported in dutasteride-treated patients and 1 case in a patient who received placebo. In the 4 year CombAT and REDUCE clinical trials providing 17489 patient years exposure to dutasteride and 5027 patient years exposure to dutasteride and tamsulosin combination there were no cases of breast cancer reported in any treatment groups.

 

Two case control, epidemiological studies, one conducted in a US (n=339 breast cancer cases and n=6,780 controls) and the other in a UK (n=398 breast cancer cases and n=3,930 controls) healthcare database, showed no increase in the risk of developing male breast cancer with the use of 5 ARIs (see section 4.4).  Results from the first study did not identify a positive association for male breast cancer (relative risk for ³ 1 year of use before breast cancer diagnosis compared with < 1 year of use: 0.70: 95% CI 0.34, 1.45).  In the second study, the estimated odds ratio for breast cancer associated with the use of 5 ARIs compared with non-use was 1.08: 95% CI 0.62, 1.87). 

 

A causal relationship between the occurrence of male breast cancer and long term use of dutasteride has not been established.

 

Effects on male fertility:

 

The effects of dutasteride 0.5 mg/day on semen characteristics were evaluated in healthy volunteers aged 18 to 52 (n=27 dutasteride, n=23 placebo) throughout 52 weeks of treatment and 24 weeks of post-treatment follow-up. At 52 weeks, the mean percent reduction from baseline in total sperm count, semen volume and sperm motility were 23%, 26% and 18%, respectively, in the dutasteride group when adjusted for changes from baseline in the placebo group. Sperm concentration and sperm morphology were unaffected. After 24 weeks of follow-up, the mean percent change in total sperm count in the dutasteride group remained 23% lower than baseline. While mean values for all parameters at all time points remained within the normal ranges and did not meet the predefined criteria for a clinically significant change (30%), two subjects in the dutasteride group had decreases in sperm count of greater than 90% from baseline at 52 weeks, with partial recovery at the 24 week follow-up. The possibility of reduced male fertility cannot be excluded.

 

Cardiovascular adverse events

 

In a 4 year BPH study of dutasteride in combination with tamsulosin in 4844 men (the CombAT study) the incidence of the composite term cardiac failure in the combination group (14/1610, 0.9%) was higher than in either monotherapy group:  dutasteride, (4/1623, 0.2%) and tamsulosin, (10/1611, 0.6%).

 

In a separate 4-year study in 8231 men aged 50 to 75, with a prior negative biopsy for prostate cancer and baseline PSA between 2.5 ng/mL and 10.0 ng/mL in the case of men 50 to 60 years of age, or 3 ng/mL and 10.0 ng/mL in the case of men older than 60 years of age) (the REDUCE study), there was a higher incidence of the composite term cardiac failure in subjects taking dutasteride 0.5 mg once daily (30/4105, 0.7%) compared to subjects taking placebo (16/4126, 0.4%).  A post-hoc analysis of this study showed a higher incidence of the composite term cardiac failure in subjects taking dutasteride and an alpha1- adrenoceptor antagonist concomitantly (12/1152, 1.0%), compared to subjects taking dutasteride and no alpha1- adrenoceptor antagonist (18/2953, 0.6%), placebo and an alpha1- adrenoceptor antagonist (1/1399, <0.1%), or placebo and no alpha1- adrenoceptor antagonist (15/2727, 0.6%).

 

In a meta-analysis of 12-randomised, placebo- or comparator-controlled clinical studies (n=18,802) that evaluated the risks of developing cardiovascular adverse events from the use of dutasteride (by comparison with controls), no consistent statistically significant increase in the risk of heart failure (RR 1.05; 95% CI 0.71, 1.57), acute myocardial infarction (RR 1.00; 95% CI 0.77, 1.30) or stroke (RR 1.20; 95% CI 0.88, 1.64) were found.

 

Prostate cancer and high grade tumours

 

In a 4-year comparison of placebo and dutasteride in 8231 men aged 50 to 75, with a prior negative biopsy for prostate cancer and baseline PSA between 2.5 ng/mL and 10.0 ng/mL in the case of men 50 to 60 years of age, or 3 ng/mL and 10.0 ng/mL in the case of men older than 60 years of age) (the REDUCE study), 6,706 subjects had prostate needle biopsy (primarily protocol mandated) data available for analysis to determine Gleason Scores. There were 1517 subjects diagnosed with prostate cancer in the study.  The majority of biopsy-detectable prostate cancers in both treatment groups were diagnosed as low grade (Gleason 5-6, 70%).

 

There was a higher incidence of Gleason 8-10 prostate cancers in the dutasteride group (n=29, 0.9%) compared to the placebo group (n=19, 0.6%) (p=0.15).  In Years 1-2, the number of subjects with Gleason 8-10 cancers was similar in the dutasteride group (n=17, 0.5%) and the placebo group (n=18, 0.5%).  In Years 3-4, more Gleason 8-10 cancers were diagnosed in the dutasteride group (n=12, 0.5%) compared with the placebo group (n=1, <0.1%) (p=0.0035).  There are no data available on the effect of dutasteride beyond 4 years in men at risk of prostate cancer.  The percentage of subjects diagnosed with Gleason 8-10 cancers was consistent across study time periods (Years 1-2 and Years 3-4) in the dutasteride group (0.5% in each time period), while in the placebo group, the percentage of subjects diagnosed with Gleason 8-10 cancers was lower during Years 3-4 than in Years 1-2 (<0.1% versus 0.5%, respectively) (see section 4.4). There was no difference in the incidence of Gleason 7-10 cancers (p=0.81).

 

The additional 2-year follow-up study of the REDUCE trial did not identify any new cases of Gleason 8–10 prostate cancers.

 

In a 4 year BPH study (CombAT) where there were no protocol-mandated biopsies and all diagnoses of prostate cancer were based on for-cause biopsies, the rates of Gleason 8-10 cancer were (n=8, 0.5%) for dutasteride, (n=11, 0.7%) for tamsulosin and (n=5, 0.3%) for combination therapy.

 

Four different epidemiological, population-based studies (two of which were based on a total population of 174,895, one on a population of 13,892, and one on a population of 38,058) showed that the use of 5-alpha reductase inhibitors is not associated with the occurrence of high grade prostate cancer, nor with prostate cancer, or overall mortality.

 

The relationship between dutasteride and high grade prostate cancer is not clear.

 

Effects on sexual function:

 

The effects of Duodart on sexual function were assessed in a double-blind, placebo-controlled study in sexually active men with BPH (n=243 Duodart, n=246 placebo). A statistically significant (p<0.001) greater reduction (worsening) in the Men’s Sexual Health Questionnaire (MSHQ) score was observed at 12 months in the combination group. The reduction was mainly related to a worsening of the ejaculation and overall satisfaction domains rather than the erection domains. These effects did not affect study participants’ perception of Duodart, which was rated with a statistically significant greater satisfaction throughout 12 months compared with placebo (p<0.05). In this study the sexual adverse events occurred during the 12 months of treatment and approximately half of these resolved within 6 months post-treatment.

 

Dutasteride-tamsulosin combination and dutasteride monotherapy are known to cause sexual function adverse effects (see section 4.8).

 

As observed in other clinical studies, including CombAT and REDUCE, the incidence of adverse events related to sexual function decreases over time with continued therapy.

 

Tamsulosin

 

Tamsulosin increases the maximum urinary flow rate. It relieves obstruction by relaxing smooth muscle in the prostate and urethra, thereby improving voiding symptoms. It also improves the storage symptoms in which bladder instability plays an important role. These effects on storage and voiding symptoms are maintained during long-term therapy.  The need for surgery or catheterization is significantly delayed.

 

Α1-adrenoreceptor antagonists can reduce blood pressure by lowering peripheral resistance.  No reduction in blood pressure of any clinical significance was observed during studies with tamsulosin.


 

Bioequivalence was demonstrated between dutasteride-tamsulosin and concomitant dosing with separate dutasteride and tamsulosin capsules.

 

The single dose bioequivalence study was performed in both the fasted and fed states. A 30% reduction in Cmax was observed for the tamsulosin component of dutasteride-tamsulosin in the fed state compared to the fasted state. Food had no effect on AUC of tamsulosin.

 

Absorption

 

Dutasteride

Following oral administration of a single 0.5 mg dutasteride dose, the time to peak serum concentrations of dutasteride is 1 to 3 hours.  The absolute bioavailability is approximately 60%. The bioavailability of dutasteride is not affected by food.

 

Tamsulosin

Tamsulosin is absorbed from the intestine and is almost completely bioavailable. Both the rate and extent of absorption of tamsulosin are reduced when taken within 30 minutes of a meal. Uniformity of absorption can be promoted by the patient always taking Duodart after the same meal. Tamsulosin shows dose proportional plasma exposure. 

 

After a single dose of tamsulosin in the fed state, plasma concentrations of tamsulosin peak at around 6 hours and, in the steady state, which is reached by day 5 of multiple dosing, the mean steady state Cmax in patients is about two thirds higher than that reached after a single dose. Although this was observed in elderly patients, the same finding would also be expected in younger patients.

 

Distribution

 

Dutasteride

Dutasteride has a large volume of distribution (300 to 500 L) and is highly bound to plasma proteins (>99.5%).  Following daily dosing, dutasteride serum concentrations achieve 65% of steady state concentration after 1 month and approximately 90% after 3 months.

Steady state serum concentrations (Css) of approximately 40 ng/mL are achieved after 6 months of dosing 0.5 mg once a day.  Dutasteride partitioning from serum into semen averaged 11.5%.

 

Tamsulosin

In man tamsulosin is about 99% bound to plasma proteins.  The volume of distribution is small (about 0.2l/kg).

 

Biotransformation

 

Dutasteride

Dutasteride is extensively metabolised in vivo.  In vitro, dutasteride is metabolised by the cytochrome P450 3A4 and 3A5 to three monohydroxylated metabolites and one dihydroxylated metabolite.

 

Following oral dosing of dutasteride 0.5 mg/day to steady state, 1.0% to 15.4% (mean of 5.4%) of the administered dose is excreted as unchanged dutasteride in the faeces.  The remainder is excreted in the faeces as 4 major metabolites comprising 39%, 21%, 7%, and 7% each of drug-related material and 6 minor metabolites (less than 5% each).  Only trace amounts of unchanged dutasteride (less than 0.1% of the dose) are detected in human urine.

 

Tamsulosin

There is no enantiomeric bioconversion from tamsulosin hydrochloride [R(-) isomer] to the S(+) isomer in humans. Tamsulosin hydrochloride is extensively metabolised by cytochrome P450 enzymes in the liver and less than 10% of the dose is excreted in urine unchanged. However, the pharmacokinetic profile of the metabolites in humans has not been established. In vitro results indicate that CYP3A4 and CYP2D6 are involved in metabolism of tamsulosin as well as some minor participation of other CYP isoenzymes. Inhibition of hepatic drug metabolising enzymes may lead to increased exposure to tamsulosin (see section 4.4 and 4.5). The metabolites of tamsulosin hydrochloride undergo extensive conjugation to glucuronide or sulfate prior to renal excretion.

 

Elimination

 

Dutasteride

The elimination of dutasteride is dose dependent and the process appears to be described by two elimination pathways in parallel, one that is saturable at clinically relevant concentrations and one that is non saturable.

At low serum concentrations (less than 3 ng/mL), dutasteride is cleared rapidly by both the concentration dependent and concentration independent elimination pathways.  Single doses of 5 mg or less showed evidence of rapid clearance and a short half-life of 3 to 9 days. 

 

At therapeutic concentrations, following repeat dosing of 0.5 mg/day, the slower, linear elimination pathway is dominating and the half-life is approx. 3-5 weeks.

 

Tamsulosin

Tamsulosin and its metabolites are mainly excreted in the urine with about 9% of a dose being present in the form of unchanged active substance.

 

Following intravenous or oral administration of an immediate-release formulation, the elimination half life of tamsulosin in plasma ranges from 5 to 7 hours. Due to the absorption rate-controlled pharmacokinetics with tamsulosin modified release capsules, the apparent elimination half life of tamsulosin in the fed state is approximately 10 hours and in the steady state is approximately 13 hours.

 

Elderly

 

Dutasteride

Dutasteride pharmacokinetics were evaluated in 36 healthy male subjects between the ages of 24 and 87 years following administration of a single 5 mg dose of dutasteride.  No significant influence of age was seen on the exposure of dutasteride but the half-life was shorter in men under 50 years of age.  Half-life was not statistically different when comparing the 50-69 year old group to the greater than 70 years old.

 

Tamsulosin

Cross-study comparison of tamsulosin hydrochloride overall exposure (AUC) and half-life indicate that the pharmacokinetic disposition of tamsulosin hydrochloride may be slightly prolonged in elderly males compared to young, healthy male volunteers. Intrinsic clearance is independent of tamsulosin hydrochloride binding to AAG, but diminishes with age, resulting in a 40% overall higher exposure (AUC) in subjects of age 55 to 75 years compared to subjects of age 20 to 32 years.

 

Renal impairment

 

Dutasteride

The effect of renal impairment on dutasteride pharmacokinetics has not been studied.  However, less than 0.1% of a steady-state 0.5 mg dose of dutasteride is recovered in human urine, so no clinically significant increase of the dutasteride plasma concentrations is anticipated for patients with renal impairment (see section 4.2).

 

Tamsulosin

The pharmacokinetics of tamsulosin hydrochloride have been compared in 6 subjects with mild-moderate (30 ≤ CLcr < 70 mL/min/1.73m2) or moderate-severe (10 ≤ CLcr < 30 mL/min/1.73m2) renal impairment and 6 normal subjects (CLcr > 90 mL/min/1.73m2). While a change in the overall plasma concentration of tamsulosin hydrochloride was observed as the result of altered binding to AAG, the unbound (active) concentration of tamsulosin hydrochloride, as well as the intrinsic clearance, remained relatively constant. Therefore, patients with renal impairment do not require an adjustment in tamsulosin hydrochloride capsules dosing. However, patients with endstage renal disease (CLcr < 10 mL/min/1.73m2) have not been studied.

 

Hepatic impairment

 

Dutasteride

The effect on the pharmacokinetics of dutasteride in hepatic impairment has not been studied (see section 4.3).  Because dutasteride is eliminated mainly through metabolism the plasma levels of dutasteride are expected to be elevated in these patients and the half-life of dutasteride be prolonged (see section 4.2 and section 4.4).

 

Tamsulosin

The pharmacokinetics of tamsulosin hydrochloride have been compared in 8 subjects with moderate hepatic dysfunction (Child-Pugh's classification: Grades A and B) and 8 normal subjects. While a change in the overall plasma concentration of tamsulosin hydrochloride was observed as the result of altered binding to AAG, the unbound (active) concentration of tamsulosin hydrochloride does not change significantly with only a modest (32%) change in intrinsic clearance of unbound tamsulosin hydrochloride. Therefore, patients with moderate hepatic dysfunction do not require an adjustment in tamsulosin hydrochloride dosage. Tamsulosin hydrochloride has not been studied in patients with severe hepatic dysfunction.


Non-clinical studies have not been conducted with Duodart. Dutasteride and tamsulosin hydrochloride individually have been extensively evaluated in animal toxicity tests and findings were consistent with the known pharmacological actions of 5 alpha‑reductase inhibitors and alpha1- adrenoceptor antagonists. The following statements reflect the information available on the individual components.

 

Dutasteride

 

Current studies of general toxicity, genotoxicity and carcinogenicity did not show any particular risk to humans.

 

Reproduction toxicity studies in male rats have shown a decreased weight of the prostate and seminal vesicles, decreased secretion from accessory genital glands and a reduction in fertility indices (caused by the pharmacological effect of dutasteride). The clinical relevance of these findings is unknown.

 

As with other 5 alpha reductase inhibitors, feminisation of male foetuses in rats and rabbits has been noted when dutasteride was administered during gestation. Dutasteride has been found in blood from female rats after mating with dutasteride treated males. When dutasteride was administered during gestation to primates, no feminisation of male foetuses was seen at blood exposures sufficiently in excess of those likely to occur via human semen. It is unlikely that a male foetus will be adversely affected following seminal transfer of dutasteride.

 

Tamsulosin

 

Studies of general toxicity and genotoxicity did not show any particular risk to humans other than those related to the pharmacological properties of tamsulosin.

 

In carcinogenicity studies in rats and mice, tamsulosin hydrochloride produced an increased incidence of proliferative changes of the mammary glands in females.  These findings, which are probably mediated by hyperprolactinaemia and only occurred at high dose levels, are regarded as not clinically relevant

 

High doses of tamsulosin hydrochloride resulted in a reversible reduction in fertility in male rats considered possibly due to changes of semen content or impairment of ejaculation.  Effects of tamsulosin on sperm counts or sperm function have not been evaluated.

 

Administration of tamsulosin hydrochloride to pregnant female rats and rabbits at higher than the therapeutic dose showed no evidence of foetal harm.


Hard Capsule Shell:

Hypromellose

Carrageenan (E407)

Potassium Chloride

Titanium Dioxide (E171)

Iron Oxide Red (E172)

Sunset Yellow (E110)

Carnauba Wax

Maize Starch

 

Contents in Dutasteride Soft Capsule:

Mono-di-glycerides of caprylic/capric acid

Butylhydroxytoluene (E321)

 

Soft Capsule Shell:

Gelatin

Glycerol

Titanium dioxide (E171)

Iron Oxide Yellow (E172)

Triglycerides, medium chain

Lecithin (may contain soya oil)

 

Tamsulosin Pellets:

Cellulose, Microcrystalline

Methacrylic acid - ethyl acrylate copolymer 1:1 dispersion 30 per cent (also contains polysorbate 80 and sodium laurilsulfate)

Talc

Triethyl citrate

 

Black Inks (SW-9010 or SW-9008):

Shellac

Propylene Glycol

Iron Oxide Black (E172)

Potassium Hydroxide (in Black Ink SW-9008 only)


Not applicable.


18 months

Do not store above 25°C.


Opaque, white high density polyethylene (HDPE) bottles with polypropylene child-resistant closures with polyethylene-faced, foil induction heat-seal liners:

7 hard capsules in 40 ml bottle

30 hard capsules in 100 ml bottle

90 hard capsules in 200 ml bottle

Not all pack sizes may be marketed.


Dutasteride is absorbed through the skin, therefore contact with leaking capsules must be avoided.  If contact is made with leaking capsules, the contact area should be washed immediately with soap and water (see section 4.4).

 

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


MARKETING AUTHORISATION HOLDER GlaxoSmithKline Export Limited Address: 980 Great West Road, Brentford, Middlesex, TW8 9GS, England DUODART is a trademark owned by or licensed to GSK group of companies. © 2019 GSK group of companies, all rights reserved. MANUFACTURER Catalent Germany Schorndorf GmbH Steinbeisstrasse 2 73614 Schorndorf Germany

TEXT VERSION: EU SPC v12 DATE OF REVISION OF THE TEXT:17-November-2017
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