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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)

Endura® contains an active substance called ‘dapoxetine’. This belongs to a group of medicines called ‘selective serotonin reuptake inhibitors’ (SSRIs). Endura® may also be known as a ‘urological’ medicine. Endura® increases the time it takes to ejaculate and can improve the control over the ejaculation. This may reduce the frustration or worry about fast ejaculation. Endura® is used to treat premature ejaculation in adult men aged 18 to 64 years. Premature ejaculation is when a man ejaculates with little sexual stimulation and before the man wants. This can cause problems for the man and may cause problems in sexual relationships.


Do not take Endura®:

If you are allergic to dapoxetine or any of the other ingredients of this medicine.

If you have heart problems, such as heart failure or problems with the heart rhythm.

If you have a history of fainting.

If you have ever had mania (symptoms include feeling over-excited, irritable or not being able to think clearly) or severe depression.

If you have moderate or severe liver problems.

If you are taking:

Medicines for depression called ‘monoamine oxidase inhibitors’ (MAOIs).

Thioridazine used for schizophrenia.

Other medicines for depression.

Lithium a medicine for bipolar disorder.

Linezolid an antibiotic used to treat infections.

Tryptophan a medicine to help you sleep.

St John’s wort a herbal medicine.

Tramadol used to treat serious pain.

Medicines used to treat migraines.

Do not take Endura® at the same time as any of the medicines listed above. If you have taken any of these medicines, you will need to wait 14 days after you stop taking it before you can start taking Endura®. Once you have stopped taking Endura®, you will need to wait 7 days before taking any of the medicines listed above.

If you are not sure about what to do, talk to your doctor or pharmacist before taking this medicine.

Certain medicines for fungal infection, including ketoconazole and itraconazole.

Certain medicines for HIV, including ritonavir, saquinavir, nelfinavir and atazanavir.

Certain antibiotics for treating infection, including telithromycin.

Nefazodone - an antidepressant.

Do not take this medicine if any of the above apply to you. If you are not sure, talk to your doctor or pharmacist before taking this medicine.

Children and adolescents

 This medicine should not be used in children or adolescents under age 18 years.

Warnings and precautions

Talk to your doctor, pharmacist or nurse before taking Endura®:

• If you have not been diagnosed with premature ejaculation.

• If you also have another sexual problem, such as erectile dysfunction.

• If you have a history of dizziness from low blood pressure.

• If you use recreational drugs such as ecstasy, LSD, narcotics or benzodiazepines.

• If you drink alcohol.

• If you have ever had a mental health problem such as depression, mania (symptoms include feeling over−excited, irritable or not being able to think clearly), bipolar disorder (symptoms include serious mood swings between mania and depression) or schizophrenia (a psychiatric disease).

• If you have epilepsy.

• If you have a history of bleeding or blood clotting problems.

• If you have kidney problems.

• If you have, or are at risk of, high pressure in the eye (glaucoma).

If any of the above apply to you (or you are not sure), talk to your doctor or pharmacist before taking this medicine.

Before you start taking this medicine, your doctor should perform a test to make sure that your blood pressure doesn’t drop too much when you stand up from lying down.

Other medicines and Endura®

Tell your doctor or pharmacist if you are taking, have recently taken, or might take any other medicines. This includes medicines you get without a prescription, such as herbal medicines. This is because Endura® can affect the way some other medicines work. Also some other medicines can affect the way Endura® works. Therefore, use of other medicines may affect the maximum dose of Endura® you’re allowed to take.

Do not take Endura® at the same time as any of the following medicines:

Medicines for depression called ‘monoamine oxidase inhibitors’ (MAOIs).

Thioridazine used for schizophrenia.

Other medicines for depression.

Lithium - a medicine for bipolar disorder.

Linezolid - an antibiotic used to treat infections.

Tryptophan - a medicine to help you sleep.

St John’s wort - a herbal medicine.

Tramadol - used to treat serious pain.

Medicines used to treat migraines.

Do not take Endura® at the same time as any of the medicines listed above. If you have taken any of these medicines, you will need to wait 14 days after you stop taking it before you can start taking Endura®.

Once you have stopped taking Endura®, you will need to wait 7 days before taking any of the medicines listed above.

If you are not sure about what to do, talk to your doctor or pharmacist before taking this medicine.

Certain medicines for fungal infection, including ketoconazole and itraconazole.

Certain medicines for HIV, including ritonavir, saquinavir, nelfinavir and atazanavir.

Certain antibiotics for treating infection, including telithromycin.

Nefazodone - an antidepressant.

Tell your doctor or pharmacist if you are taking any of the following medicines:

Medicines for mental health problems other than depression

Non-steroidal anti-inflammatory medicines such as ibuprofen or acetylsalicyclic acid.

Medicines to thin your blood, such as warfarin.

Certain medicines used to treat erectile dysfunction, such as sildenafil, tadalafil or vardenafil, as these medicines may lower your blood pressure, possibly upon standing.

Certain medicines used to treat high blood pressure and chest pain (angina) (such as verapamil and diltiazem), or enlarged prostate, as these medicines may also lower your blood pressure, possibly upon standing.

Certain other medicines for fungal infection, such as fluconazole.

Certain other medicines for HIV, such as amprenavir and fosamprenavir.

Certain other antibiotics for treating infection, such as erythromycin and clarithromycin.

Aprepitant used to treat nausea.

If you are not sure if any of the above apply to you, talk to your doctor or pharmacist before taking this medicine.

Endura® with food, drink and alcohol

Do not drink grapefruit juice within 24 hours prior to taking this medicine as this can increase the level of this medicine in your body.

This medicine can be taken with or without food.

You should take this medicine with at least one full glass of water.

Avoid alcohol when taking this medicine.

The effects of alcohol such as feeling dizzy, sleepy and having slow reactions, may be increased if taken with this medicine.

Drinking alcohol while taking this medicine may increase your risk of injury from fainting or from other side effects.

Pregnancy, breastfeeding and fertility

This medicine should not be taken by women.

Driving and using machines

You may feel sleepy, dizzy, faint, have difficulty concentrating and blurred vision while taking this medicine. If you experience any of these or similar effects, you should avoid driving or operating hazardous machinery. The effects of alcohol may be increased if taken with this medicine and you may be more at risk of injury from fainting or from other side effects if you take this medicine with alcohol.

Endura® contains lactose

This medicine contains lactose (a type of sugar). If you have been told by your doctor that you have an intolerance to some sugars, contact your doctor before taking this medicine.

Endura® contains sodium

This medicine contains less than 1 mmol sodium (23 mg) per tablet, that is to say essentially “sodium free”


Always take this medicine exactly as your doctor or pharmacist has told you. Check with your doctor or pharmacist if you are not sure.

The recommended dose is 30 mg. Your doctor may increase the dose to 60 mg.

Only take the medicine 1 to 3 hours before sexual activity is anticipated.

Do not take this medicine more than once every 24 hours or every day.

Swallow the tablets whole to avoid a bitter taste, with at least one full glass of water. This may help lower your chance of fainting.

This medicine can be taken with or without food.

This medicine should not be used by men under 18 or over 65 years of age.

Discuss your Endura® treatment with your doctor after the first 4 weeks or after 6 doses to see whether you should continue treatment. If treatment is continued, you should see your doctor again to discuss this at least every six months.

If you take more Endura® than you should

Tell your doctor or pharmacist if you have taken more tablets than you should. You may feel sick or be sick.

If you stop taking Endura®

Talk to your doctor before you stop taking this medicine. You may have problems sleeping and feel dizzy after you stop taking this medicine, even if you have not taken it every day.

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


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

Stop taking Endura® and see your doctor straight away:

If you have fits (seizures).

If you faint or feel light headed when you stand up.

If you notice any changes in your mood.

If you have any thoughts of suicide or harming yourself.

If you notice any of the above, stop taking this medicine and see your doctor straight away.

Fainting and low blood pressure

This medicine can make you faint or make your blood pressure drop when you stand up. To help lower the chance of this happening:

Take this medicine with at least one full glass of water.

Do not take this medicine if you are dehydrated (you do not have enough water in your body).

This can happen:

- If you have not had anything to drink in the past 4 to 6 hours.

- If you have been sweating for a long time.

- If you have an illness where you have a high temperature, diarrhea or being sick.

If you feel like you might faint (such as feeling sick, feeling dizzy, light headed, confused, sweaty or an abnormal heart beat), or feel light headed when you stand up, immediately lie down so your head is lower than the rest of your body or sit down with your head between your knees until you feel better. This will stop you from falling and hurting yourself if you do faint.

Do not stand up quickly after you have been sitting or lying down for a long time.

Do not drive or use any tools or machines if you feel faint when taking this medicine.

Tell your doctor if you faint when taking this medicine.

Very common side effects (may affect more than 1 in 10 men):

Feeling dizzy.

Headache.

Feeling sick.

Common side effects (may affect up to 1 in 10 men):

Feeling irritable, anxious, agitated or restless.

Feeling numb or having ‘pins and needles’.

Difficulty getting or keeping an erection.

Sweating more than normal or flushing.

Diarrhea, constipation or having wind.

Stomach pain, bloating or being sick.

Problems sleeping or strange dreams.

Feeling tired or sleepy, yawning.

Blocked nose (nasal congestion).

A rise in blood pressure.

Difficulty concentrating.

Shaking or trembling.

Lower interest in sex.

Ringing in the ears.

Blurred vision.

Indigestion.

Dry mouth.

Uncommon side effects (may affect up to 1 in 100 men):

Fainting or feeling dizzy upon standing.

Change in mood, feeling overly excited or feelings of paranoia.

Feeling confused, disoriented or unable to think clearly.

Slow or irregular heartbeat or increase in heart rate.

Loss of sex drive, problems reaching orgasm.

Feeling weak, sedated, lethargic or fatigued.

Feeling depressed, nervous or indifferent.

Feeling hot, jittery, abnormal or drunk.

Vision problems, eye pain or dilated pupils.

Low or high blood pressure.

Feeling itchy or cold sweat.

Spinning sensation.

Abnormal taste.

Teeth grinding.

Rare side effects (may affect up to 1 in 1,000 men):

Feeling dizzy following exertion.

Sudden onset of sleep.

Urgency of bowel action.

If you get any side effects, talk to your doctor, pharmacist or nurse. This includes any possible side effects not listed in this leaflet


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 carton after EXP.

The expiry date refers to the last day of that month.

Endura® Tablets: Store below 30°C.

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


The active substance is Dapoxetine (Hydrochloride) 30 mg and 60 mg.

The other ingredients are lactose monohydrate, microcrystalline cellulose, croscarmellose sodium, colloidal anhydrous silica, magnesium stearate, purified water, Opadry II Grey powder (polyvinyl alcohol-hydrolized, Talc, titanium dioxide, macrogol/PEG, lecithin, black iron oxide, red iron oxide, yellow iron oxide).

 

 


Endura® 30 mg Tablets are Grey, round normal biconvex film coated tablet, engraved with H31 on one face, presented in PVC/TE/PVDC/Alu. blisters, intended for oral use. Pack size: 3 Film Coated Tablets (3 tablets/blister, 1 blister/pack). 9 Film Coated Tablets (3 tablets/blister, 3 blisters/pack). Endura® 60 mg Tablets are Grey, round normal biconvex film coated tablet engraved with H32 on one face, presented in PVC/TE/PVDC/Alu. blisters, intended for oral use. Pack size: 3 Film Coated Tablets (3 tablets/blister, 1 blister/pack). 9 Film Coated Tablets (3 tablets/blister, 3 blisters/pack).

Med City Pharma-KSA.

1st Industrial city, Phase 5, Jeddah –KSA.

Tel: 00966920003288

Mobile: 00966555786968

P.O .Box: 4072 - Jeddah 22429

E-mail: info@medcitypharma.com


08/2024
  نشرة الدواء تحت مراجعة الهيئة العامة للغذاء والدواء (اقرأ هذه النشرة بعناية قبل البدء في استخدام هذا المنتج لأنه يحتوي على معلومات مهمة لك)

یحتوي إنديورا® على مادة فعالة تسمى “دابوكستین”. والتي تنتمي إلى مجموعة من الأدویة التي تعرف بمثبطات إعادة امتصاص السیروتونین الانتقائیة. قد یعرف إنديورا® على أنه دواء “لعلاج الجهاز البولي”.

يزيد إنديورا® من الوقت المستغرق للقذف، كما یمكنه أن یحسن التحكم في عملیة القذف. وھذا قد يقلل من الإحباط أو القلق الناتج عن سرعة القذف. يستعمل إنديورا® لعلاج سرعة القذف عند الرجال البالغین الذین تتراوح أعمارھم من 18- 64 عام.

يعد القذف سریع عند حدوث عملية القذف عند التعرض لإثارة جنسیة بسیطة أو قبل الوقت الذي یرغب فیه الرجل بذلك. وهذا قد یسبب مشاكل للرجل وقد یسبب مشاكل أثناء العلاقات الجنسیة.

يجب عدم تناول إنديورا® في الحالات التالية:

إذا كنت تعاني من تحسس لدابوكستین أو لأي مكونات أخرى في ھذا الدواء.

إذا كنت تعاني من مشاكل في القلب، مثل قصور وظيفة عضلة القلب أو مشاكل في نظمية نبضات القلب.

إذا عانيت في السابق من الإغماء.

إذا عانيت في السابق من الھوس (تتضمن الأعراض الشعور بفرط الاستثارة، الشعور بالغضب أو عدم القدرة على التفكیر بوضوح) أو إذا عانیت في السابق من اكتئاب حاد.

إذا كنت تعاني من مشاكل معتدلة أو حادة في الكبد.

إذا كنت تتناول أي من الأدویة التالیة:

- أدویة لعلاج الاكتئاب التي تسمى “مثبطات مونوأمين أوكسیدیز”.

- ثیوریدازین الي يستعمل لعلاج الفصام.

- أدویة أخرى لعلاج الاكتئاب.

- لیثیوم وهو دواء يستعمل لعلاج الاضطراب ثنائي القطب.

- لینيزولید وهو مضاد حیوي يستعمل لعلاج الالتهابات.

- تريبتوفان وهو دواء یساعد على النوم.

- نبتة سانت جون وهو دواء عشبي.

- ترامادول يستعمل لعلاج الآلام الخطیرة.

- الأدویة المستعملة لعلاج الصداع النصفي.

لا تتناول إنديورا® بالتزامن مع الأدویة المذكورة في الأعلى. إذا تناولت أي من هذه الأدویة، ستحتاج إلى الانتظار لمدة 14 یوم بعد التوقف عن تناوله لتتمكن من بدء تناول إنديورا®. بمجرد التوقف عن تناول إنديورا®، ستحتاج إلى الانتظار لمدة 7 أیام قبل تناول أي من الأدویة المذكورة في الأعلى.

إذا لم تكن متأكدا مما یجب علیك القيام به، تحدث مع طبیبك أو الصیدلي قبل تناول ھذا الدواء.

أدویة معینة لعلاج الالتهابات الفطریة، بما في ذلك كیتوكونازول وإتراكونازول.

أدویة معینة لعلاج ڤیروس نقص المناعة المكتسبة، بما في ذلك ریتوناڤیر، ساكویناڤیر، نیلفیناڤیر وأتازاناڤیر.

مضادات حیویة معينة لعلاج الالتهابات، بما في ذلك تیلیثرومایسین.

نیفازودون - مضاد للاكتئاب.

لا تتناول ھذا الدواء، إذا كان أي مما ذكر في الأعلى ينطبق علیك. إذا لم تكن متأكدا، تحدث مع طبیبك أوالصیدلي قبل تناول ھذا الدواء.

الأطفال والمراھقون
يجب عدم استعمال هذا الدواء للأطفال أو المراھقین الذین تقل أعمارھم عن 18 عاما.

الاحتياطات والمحاذير

تحدث مع طبیبك، الصیدلي أو الممرض قبل تناول إنديورا®  في الحالات الآتیة:

إذا لم يتم تشخیص إصابتك بسرعة القذف.

إذا كنت تعاني من مشكلة  جنسية أخرى مثل: ضعف الانتصاب.

إذا عانيت في السابق من الشعور بالدوار الناتج عن انخفاض ضغط الدم.

إذا كنت تستعمل بعض العقاقیر لأغراض الاستجمام مثل: إكستاسي، ثنائي إيثيل أميد حمض الليسرجيك، الناركوتيات أو بنزودیازیبین.

إذا كنت تشرب الكحول.

إذا عانيت في السابق من مشكلة تتعلق بالصحة العقلية مثل الاكتئاب، الھوس (تتضمن الأعراض الشعور بفرط الاستثارة أو الشعور بالغضب أو عدم القدرة على التفكیر بوضوح)، الاضطراب ثنائي القطب (تتضمن الأعراض التقلبات المزاجیة الخطیرة بين الھوس والاكتئاب) أو الفصام (مرض نفسي).

إذا كنت تعاني من الصرع.

إذا عانيت في السابق من الإصابة بالنزیف أو مشاكل تجلط الدم.

إذا كنت تعاني من مشاكل في الكلى.

إذا كنت تعاني من ارتفاع ضغط الدم في العین (جلوكوما)، أو كنت معرض لخطر الإصابة.

إذا كان أي مما ذكر في الأعلى ينطبق عليك (أو إذا لم تكن متأكدا)، تحدث مع طبیبك أو الصیدلي قبل تناول ھذا الدواء.

قبل البدء في تناول ھذا الدواء، یجب أن یقوم طبیبك بإجراء فحص للتأكد من عدم انخفاض ضغط الدم لدیك بشدة عند النھوض من وضعیة الاستلقاء.

 تناول الأدویة الأخرى مع إنديورا®

أخبر طبیبك أو الصیدلي إذا كنت تتناول أو قد تناولت مؤخرًا أو من الممكن أن تتناول أي أدویة أخرى. ھذا يتضمن الأدویة التي يتم الحصول عليها بدون وصفة طبیة، مثل الأدویة العشبیة. هذا لأن إنديورا® قد یؤثر على طريقة عمل بعض الأدویة الأخرى. أيضا قد تؤثر الأدویة الأخرى على طريقة عمل إنديورا®. لذلك، قد يؤثر استعمال الأدویة الأخرى على الجرعة القصوى المسموح بتناولھا من إنديورا®.

لا تتناول إنديورا®  في نفس وقت تناول الأدویة التالیة:

أدویة لعلاج الاكتئاب تسمى “مثبطات مونوأمين أوكسیدیز”.

ثیوریدازین الذي يستعمل لعلاج الفصام.

أدویة أخرى لعلاج الاكتئاب.

لیثیوم - وهو دواء يستعمل لعلاج الاضطراب ثنائي القطب.

لینيزولید - وهو مضاد حیوي يستعمل لعلاج الالتهابات.

تريبتوفان - وهو دواء یساعد على النوم.

نبتة سانت جون - وهو دواء عشبي.

ترامادول يستعمل لعلاج الآلام الخطیرة.

الأدویة المستعملة لعلاج الصداع النصفي.

لا تتناول إنديورا® بالتزامن مع الأدویة المذكورة في الأعلى. إذا تناولت أي من هذه الأدویة، ستحتاج إلى الانتظار لمدة 14 یوم بعد التوقف عن تناوله لتتمكن من بدء تناول إنديورا®. بمجرد التوقف عن تناول إنديورا®، ستحتاج إلى الانتظار لمدة 7 أیام قبل تناول أي من الأدویة المذكورة في الأعلى.

إذا لم تكن متأكدا مما یجب علیك القيام به، تحدث مع طبیبك أو الصیدلي قبل تناول ھذا الدواء.

أدویة معینة لعلاج الالتهابات الفطریة، بما في ذلك كیتوكونازول وإتراكونازول.

أدویة معینة لعلاج ڤیروس نقص المناعة المكتسبة، بما في ذلك ریتوناڤیر، ساكویناڤیر، نیلفیناڤیر وأتازاناڤیر.

مضادات حیویة معينة لعلاج الالتهابات، بما في ذلك تیلیثرومایسین.

نیفازودون - مضاد للاكتئاب.

أخبر طبیبك أو الصیدلي إذا كنت تتناول أی من الأدویة التالیة:

أدویة لعلاج مشاكل الصحة العقلیة غير الاكتئاب.

الأدویة غیر السیترویدیة المضادة للالتهابات مثل أيبوبروفین أو حمض أسیتیل سالیسیلیك.

أدویة للوقاية من تجلط الدم، مثل وارفارین.

أدویة معینة تستعمل لعلاج ضعف الانتصاب، مثل سیلدینافیل، تادالافیل أو ڤاردینافیل، حيث قد تسبب هذه الأدوية انخفاض ضغط الدم لدیك، من المحتمل عند الوقوف.

أدویة معینة تستعمل لعلاج ارتفاع ضغط الدم وألم الصدر (الذبحة الصدریة) (مثل ڤیرابامیل ودیلتیازم)، أو تضخم البروستات، حيث قد تقلل ھذه الأدویة أيضا من ضغط الدم لدیك، من المحتمل عند الوقوف.

أدویة معینة أخرى لعلاج الالتهابات الفطریة، مثل فلوكونازول.

أدویة معینة أخرى لعلاج ڤیروس نقص المناعة المكتسبة، مثل أمبریناڤیر وفوسامبریناڤیر.

مضادات حیویة معینة أخرى لعلاج الالتهابات، مثل إریثرومایسین وكلاریثرومایسین.

أبریبیتانت - دواء يستعمل لعلاج الغثیان.

 إذا لم تكن متأكدا إذا كان أي مما ذكر في الأعلى ینطبق علیك، تحدث مع طبیبك أو الصیدلي قبل تناول ھذا الدواء.

 تناول إنديورا® مع الطعام، الشراب والكحول

تجنب شرب عصير الجريب فروت خلال 24 ساعة قبل تناول هذا الدواء، حيث قد يزيد هذا من مستوى هذا الدواء في الجسم.

من الممكن تناول ھذا الدواء مع أو بدون تناول الطعام.

یجب تناول ھذا الدواء مع كوب كامل من الماء على الأقل.

تجنب شرب الكحول عند تناول ھذا الدواء.

قد يزید تأثیر الكحول مثل الشعور بالدوار، النعاس وبطء رد الفعل، إذا تم شربها بالتزامن مع تناول ھذا الدواء.

قد یزید شرب الكحول بالتزامن مع تناول ھذا الدواء من خطر التعرض للإصابات الناتجة عن الإغماء، أو تلك الناتجة عن آثار جانبیة أخرى.

الحمل والرضاعة الطبیعیة والخصوبة
يجب عدم تناول هذ الدواء من قبل النساء.

القیادة واستخدام الآلات

قد تشعر بالنعاس، الدوار، الإغماء وبصعوبة في التركیز وضبابية الرؤیة خلال فترة تناول ھذا الدواء. إذا عانیت من أي من ھذه الآثار أو من آثار مماثلة، یجب علیك تجنب القیادة أو تشغیل الآلات الخطیرة. فقد تزداد تأثیرات الكحول إذا تم شربها بالتزامن مع تناول ھذا الدواء، وقد تصبح أكثر عرضة لخطر التعرض للإصابات الناتجة عن الإغماء، أو تلك الناتجة عن آثار جانبیة أخرى عند تناول ھذا الدواء بالتزامن مع شرب الكحول.

یحتوي إنديورا على اللاكتوز

یحتوي ھذا الدواء على اللاكتوز (نوع من السكريات). إذا أخبرت من قبل طبيبك بأنك لا تستطيع تحمل بعض أنواع السكریات، اتصل مع طبيبك قبل تناول ھذا الدواء.

یحتوي إنديورا® على الصوديوم

يحتوي هذا الدواء على أقل من 1 مليمول صوديوم (23 ملغم) لكل قرص، وهذا يعني بشكل أساسي “خالٍ من الصوديوم”.

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دائما تناول ھذا الدواء تماما كما أخبرك طبيبك أو الصیدلي. تأكد من طبيبك أو الصيدلي إذا لم تكن متأكدا.

الجرعة الموصى بھا ھي 30 ملغم. وقد یزید الطبیب الجرعة لتصل إلى 60 ملغم.

فقط تناول هذا الدواء قبل ساعة إلى 3 ساعات من النشاط الجنسي المتوقع حدوثه.

لا تتناول ھذا الدواء أكثر من مرة واحدة كل 24 ساعة أو كل یوم.

تناول الأقراص كاملة؛ لتجنب الطعم المر، مع كوب كامل على الأقل من الماء. هذا قد یساعد على تقلیل فرصة الإصابة بالإغماء.

من الممكن تناول ھذا الدواء مع  أو بدون تناول الطعام.

یجب عدم استعمال ھذا الدواء من قبل الرجال الذین تقل أعمارھم عن 18 عاما أو الذین تزید أعمارھم عن 65 عاما.

ناقش العلاج باستعمال إنديورا® مع طبیبك بعد الأسابیع الأربع الأولى من العلاج أو بعد ست جرعات لترى ما إذا كان علیك الاستمرار في العلاج أم لا. في حال الاستمرار في العلاج، یجب علیك مراجعة طبیبك لمناقشة ذلك كل ستة شهور على الأقل.

إذا تناولت إنديورا® أكثر مما یجب من

أخبر طبیبك أو الصیدلي إذا تناولت كمیة من الأقراص أكثر مما یجب. قد تشعر بالغثيان أو القيء.

إذا توقفت عن تناول إنديورا®

تحدث مع طبیبك قبل التوقف عن تناول ھذا الدواء. قد تعاني من مشاكل في النوم والشعور بالدوار بعد التوقف عن تناول ھذا الدواء. حتى إذا لم تكن تتناوله كل یوم.

إذا كان لديك أي أسئلة إضافية عن استعمال هذا الدواء، إسأل الطبيب، الصيدلي أو الممرض.

مثل جميع الأدوية، قد يسبب هذا الدواء آثارا جانبية، على الرغم من عدم حدوثھا لدى الجميع.

توقف عن تناول إنديورا® وقم بزیارة طبیبك فورا في الحالات التالیة:

إذا كنت تعاني من نوبات ظهور أعراض مفاجئة (نوبات الصرع).

إذا كنت تصاب بالإغماء أو تشعر بالدوار عند الوقوف.

إذا كنت تلاحظ حدوث أي تغیرات في المزاج.

إذا كان لدیك أي أفكار متعلقة بالانتحار أو إیذاء نفسك.

إذا لاحظت حدوث أي مما ذكر في الأعلى، توقف عن تناول ھذا الدواء وقم بزیارة طبیبك فورا.

الشعور بالإغماء وانخفاض ضغط الدم

قد يسبب ھذا الدواء الشعور بالإغماء أو انخفاض في ضغط الدم عند الوقوف. لتقلیل احتمالیة حدوث ذلك:

تناول ھذا الدواء على الأقل مع كوب كامل من الماء.

لا تتناول ھذا الدواء إذا كنت تعاني من الجفاف (لیس لدیك كمیة كافیة من الماء في جسمك).

قد یحدث ھذا في الحالات التالیة:

إذا لم تكن قد تناولت أي مشروبات خلال 4 إلى 6 ساعات الماضیة. 

إذا كنت تتعرق لفترة طویلة.

إذا كنت مصابا بمرض معين يسبب ارتفاع درجة الحرارة، الإسھال أو القيء.

إذا كنت تشعر بأنك قد تصاب بالإغماء (كالشعور بالغثيان، الدوار، الدوخة، الارتباك، التعرق أو اضطراب نبضات القلب)، أو الشعور بالدوار عند الوقوف، استلق على الفور بحیث يكون رأسك منخفضة عن باقي جسمك أو اجلس بحيث يكون رأسك بین ركبتیك إلى أن تشعر بتحسن. هذا سیمنعك من السقوط وإیذاء نفسك إذا أصبت بالإغماء.

لا تقف سریعا بعد الجلوس أو الاستلقاء لوقت طویل.

تجنب القیادة أو استخدام الأدوات أو الآلات إذا شعرت بالإغماء عند تناول ھذا الدواء.

أخبر طبیبك إذا أصبت بالإغماء عند تناول ھذا الدواء.

آثار جانبیة شائعة جدا (قد تؤثر على أكثر من 1 من كل 10 رجال):

الشعور بالدوار.

صداع.

الشعور بالغثيان.

آثار جانبیة شائعة (قد تؤثر على 1 أو أقل من كل 10 رجال):

الشعور بالغضب، القلق، ھیاج أو الشعور بعدم الراحة.

الشعور بالتنمیل أو الإحساس بوخز خفيف.

صعوبة حصول الانتصاب أو الحفاظ عليه.

تعرق أكثر من الطبیعي أو احمرار الوجه يرافقه ارتفاع في درجة الحرارة.

إسھال، إمساك أو غازات.

ألم  في المعدة، انتفاخ أو قيء.

مشاكل في النوم أو أحلام غریبة.

شعور بالتعب أو النعاس، التثاؤب.

انسداد الأنف (احتقان الأنف).

ارتفاع ضغط الدم.

صعوبة في التركیز.

ارتجاف أو ارتعاش.

انخفاض الرغبة الجنسیة.

رنین في الأذنین.

ضبابية الرؤیة

عسر الھضم

جفاف الفم.

آثار جانبیة غیر شائعة (قد تُؤثر على 1 أو أقل من كل 100 رجل):

الشعور بالإغماء أو الدوار عند الوقوف.

تغیر في المزاج، شعور بفرط الاستثارة أو جنون الارتیاب.

الشعور بالارتباك أو التوھان أو عدم القدرة على التفكیر بوضوح.

بطء أو عدم انتظام نبضات القلب أو زیادة معدل نبضات القلب.

فقدان الرغبة الجنسیة، مشاكل في الوصول إلى النشوة الجنسية.

الشعور بالضعف، السكون، الكسل أو الإرھاق.

الشعور بالاكتئاب، العصبية أو اللامبالاة.

الشعور بارتفاع درجة حرارة الجسم، العصبیة، إحساس غیر طبیعي أو بالثمالة.

مشاكل في الرؤیة، ألم في العین أو اتساع حدقة العین.

انخفاض أو ارتفاع ضغط دم.

الشعور بالحكة أو بتعرق بارد.

الشعور بالدوران.

مذاق غیر طبیعي.

طحن الأسنان.

آثار جانبیة نادرة (قد تُؤثر على 1 أو أقل من كل 1000 رجل):

شعور بالدوار بعد بذل مجھود.

نوم مفاجئ.

حاجة ملحة للإخراج.

إذا حصل لديك أي آثار جانبية، تحدث مع طبيبك، الصيدلي أو الممرض. هذا يتضمن أي آثار جانبية محتملة غير مذكورة في هذه النشرة

يحفظ بعيدا عن متناول الأطفال و نظرهم.

لا تستخدم أقراص إنديورا® بعد تاريخ انتهاء الصلاحية المذكورعلى الشريط و العلبة الخارجية.

تاريخ الانتهاء يشير إلى اليوم الأخير من ذلك الشهر.

أقراص إنديورا® :يحفظ بدرجة حرارة دون 30 °م.

يجب أن لا يتم التخلص من الأدوية عن طريق مياه الصرف الصحي أو النفايات المنزلية. اسأل الصيدلي عن كيفية التخلص من الأدوية التي لم تعد مطلوبة. وسوف تساعد هذه التدابير في حماية البيئة.

ماذا تحتوي أقراص إنديورا®

المادة الفعالة هي دابوكستین (هيدروكلوريد) 30 ملغم و 60 ملغم.

المكونات الأخرى هي لاكتوز أحادي الھیدرات، ميكروكريستالين سلیلوز، كروسكارمیلوز الصودیوم، ثاني أكسید السیلیكون الغروي، ستیرات المغنيسیوم، ماء نقي، مسحوق أوبادري رمادي (بولي فينيل الكحول، تلك، ثاني أكسيد التيتانيوم، ماكروجول/بولي إيثيلين جلايكول، ليسيثين، أكسيد الحديد الأسود، أكسيد الحديد الأصفر، أكسيد الحديد الأحمر).

إنديورا® 30 ملغم هي أقراص مغلفة دائرية الشكل ذات لون رمادي، محدبة الوجهين، محفور على أحد الأوجه H31، معبأة في أشرطة بي ڤي سي/تي إي/بي ڤي دي سي/ألومنيوم معدة للاستعمال عن طريق الفم. 

حجم العبوة: 3 أقراص مغلفة (3 أقراص/شريط، 1 شريط/ عبوة).

9 أقراص مغلفة (3 أقراص/شريط، 3 شريط/ عبوة).

إنديورا® 60 ملغم هي أقراص مغلفة دائرية الشكل ذات لون رمادي، محدبة الوجهين، محفور على أحد الأوجه H32، معبأة في أشرطة بي ڤي سي/تي إي/بي ڤي دي سي/ألومنيوم معدة للاستعمال عن طريق الفم. 

حجم العبوة: 3 أقراص مغلفة (3 أقراص/شريط، 1 شريط/ عبوة).

9 أقراص مغلفة (3 أقراص/شريط، 3 شريط/ عبوة).

مدينة الدواء للصناعات الدوائية - المملكة العربية السعودية.

المدينة الصناعية األولى، المرحلة الخامسة، جدة - المملكة العربية السعودية.

هاتف: 00966920003288

جوال: 00966555786968

ص.ب: 4072 - جدة 22429

بريد الكتروني: info@medcitypharma.com 

08/2024
 Read this leaflet carefully before you start using this product as it contains important information for you

Endura® 30 mg Film Coated Tablets. Endura® 60 mg Film Coated Tablets.

Endura® 30 mg: Each film coated tablet contains Dapoxetine 30 mg. Endura® 60 mg: Each film coated tablet contains Dapoxetine 60 mg. For a full list of excipients, see section 6.1.

Film Coated Tablet. Endura® 30 mg Film Coated Tablet: grey round normal biconvex film coated tablets engraved with H31 on one face, presented in PVC/TE/PVDC/AIu blister intended for oral use. Endura® 60 mg Film Coated Tablet: grey round normal biconvex film coated tablets engraved with H32 on one face, presented in PVC/TE/PVDC/AIu blister intended for oral use.

Endura® is indicated for the treatment of premature ejaculation (PE) in adult men 18 to 64 years.

Endura® should only be prescribed to patients who meet all the following criteria:

·       An intravaginal ejaculatory latency time (IELT) of less than two minutes.

·       Persistent or recurrent ejaculation with minimal sexual stimulation before, on, or shortly after penetration and before the patient wishes.

·       Marked personal distress or interpersonal difficulty as a consequence of PE.

·       Poor control over ejaculation.

·       A history of premature ejaculation in the majority of intercourse attempts over the prior 6 months.

Endura® should be administered only as on-demand treatment before anticipated sexual activity. Endura® should not be prescribed to delay ejaculation in men who have not been diagnosed with PE.


Posology

Adult men (18 to 64 years of age)

The recommended starting dose for all patients is 30 mg, taken as needed approximately 1 to 3 hours prior to sexual activity. Treatment with Endura® should not be initiated with the 60 mg dose.

Endura® is not intended for continuous daily use. Endura® should be taken only when sexual activity is anticipated. Endura® must not be taken more frequently than once every 24 hours.

If the individual response to 30 mg is insufficient and the patient has not experienced moderate or severe adverse reactions or prodromal symptoms suggestive of syncope, the dose may be increased to a maximum recommended dose of 60 mg taken as needed approximately 1 to 3 hours prior to sexual activity. The incidence and severity of adverse events is higher with the 60 mg dose.

If the patient experienced orthostatic reactions on the starting dose, no dose escalation to 60 mg should be performed (see section 4.4).

A careful appraisal of individual benefit risk of Endura® should be performed by the physician after the first four weeks of treatment (or at least after 6 doses of treatment) to determine whether continuing treatment with Endura® is appropriate.

Data regarding the efficacy and safety of Endura® beyond 24 weeks are limited. The clinical need of continuing and the benefit risk balance of treatment with Endura® should be re-evaluated at least every six months.

Elderly (age 65 years and over)

The efficacy and safety of Endura® have not been established in patients age 65 years and over (see section 5.2).

Paediatric population

There is no relevant use of Endura® in this population in the indication of premature ejaculation.

Patients with renal impairment

Caution is advised in patients with mild or moderate renal impairment. Endura® is not recommended for use in patients with severe renal impairment (see sections 4.4 and 5.2).

Patients with Hepatic Impairment

Endura® is contraindicated in patients with moderate and severe hepatic impairment (Child-Pugh Class B and C) (see sections 4.3 and 5.2).

Known CYP2D6 poor metabolizers or patients treated with potent CYP2D6 inhibitors

Caution is advised if increasing the dose to 60 mg in patients known to be of CYP2D6 poor metabolizer genotype or in patients concomitantly treated with potent CYP2D6 inhibitors (see sections 4.4, 4.5 and 5.2).

Patients treated with moderate or potent inhibitors of CYP3A4

Concomitant use of potent CYP3A4 inhibitors is contraindicated. The dose should be restricted to 30 mg in patients concomitantly treated with moderate CYP3A4 inhibitors and caution is advised (see sections 4.3, 4.4 and 4.5).

Method of administration

For oral use. Tablets should be swallowed whole to avoid the bitter taste. It is recommended that tablets be taken with at least one full glass of water. Endura® may be taken with or without food (see section 5.2).

Precautions to be taken before handling or administering the medicinal product

Before treatment is initiated, see section 4.4 regarding orthostatic hypotension.


Hypersensitivity to the active substance or to any of the excipients listed in section 6.1. Significant pathological cardiac conditions such as: • Heart failure (NYHA class II-IV). • Conduction abnormalities such as AV block or sick sinus syndrome. • Significant ischemic heart disease. • Significant valvular disease. • A history of syncope. • A history of mania or severe depression. Concomitant treatment with monoamine oxidase inhibitors (MAOIs), or within 14 days of discontinuing treatment with an MAOI. Similarly, an MAOI should not be administered within 7 days after Endura® has been discontinued (see section 4.5). Concomitant treatment with thioridazine, or within 14 days of discontinuing treatment with thioridazine. Similarly, thioridazine should not be administered within 7 days after Endura® has been discontinued (see section 4.5). Concomitant treatment with serotonin reuptake inhibitors [selective serotonin reuptake inhibitors (SSRIs), serotonin-norepinephrine reuptake inhibitors (SNRIs), tricyclic antidepressants (TCAs)] or other medicinal/herbal products with serotonergic effects [e.g., L-tryptophan, triptans, tramadol, linezolid, lithium, St. John's Wort (Hypericum perforatum)] or within 14 days of discontinuing treatment with these medicinal/herbal products. Similarly, these medicinal/herbal products should not be administered within 7 days after Endura® has been discontinued (see section 4.5). Concomitant treatment of potent CYP3A4 inhibitors such as ketoconazole, itraconazole, ritonavir, saquinavir, telithromycin, nefazadone, nelfinavir, atazanavir, etc. (see section 4.5). Moderate and severe hepatic impairment.

General recommendations

Endura® is only indicated in men with Premature Ejaculation who meet all the criteria listed in sections 4.1 and 5.1. Endura® should not be prescribed to men who have not been diagnosed with Premature Ejaculation. Safety has not been established and there are no data on the ejaculation-delaying effects in men without Premature Ejaculation.

Other forms of sexual dysfunction

Before treatment, subjects with other forms of sexual dysfunction, including erectile dysfunction, should be carefully investigated by physicians. Endura® should not be used in men with erectile dysfunction (ED) who are using PDE5 inhibitors (see section 4.5).

Orthostatic hypotension

Before treatment initiation, a careful medical examination including history of orthostatic events should be performed by the physician. An orthostatic test should be performed before initiating therapy (blood pressure and pulse rate, supine and standing). In case of a history of documented or suspected orthostatic reaction, treatment with Endura® should be avoided.

Orthostatic hypotension has been reported in clinical trials. The prescriber should counsel the patient in advance that if he experiences possibly prodromal symptoms, such as lightheadedness soon after standing, he should immediately lie down so his head is lower than the rest of his body or sit down with his head between his knees until the symptoms pass. The prescriber should also inform the patient not to rise quickly after prolonged lying or sitting.

Suicide/suicidal thoughts

Antidepressants, including SSRIs, increased the risk compared to placebo of suicidal thinking and suicidality in short-term studies in children and adolescents with Major Depressive Disorder and other psychiatric disorders. Short-term studies did not show an increase in the risk of suicidality with antidepressants compared to placebo in adults beyond age 24. In clinical trials with dapoxetine for the treatment of premature ejaculation, there was no clear indication of treatment-emergent suicidality in evaluation of possibly suicide-related adverse events evaluated by the Columbia Classification Algorhythm of Suicide Assessment (C-CASA), Montgomery-Asberg Depression Rating Scale, or Beck Depression Inventory-II.

Syncope

Patients should be cautioned to avoid situations where injury could result, including driving or operating hazardous machinery, should syncope or its prodromal symptoms such as dizziness or lightheadedness occur (see section 4.8).

Possibly prodromal symptoms such as nausea, dizziness/lightheadedness, and diaphoresis were reported more frequently among patients treated with dapoxetine compared to placebo.

In the clinical trials, cases of syncope characterized as loss of consciousness, with bradycardia or sinus arrest observed in patients wearing Holter monitors, were considered vasovagal in etiology and the majority occurred during the first 3 hours after dosing, after the first dose, or associated with study-related procedures in the clinic setting (such as blood draw and orthostatic maneuvers and blood pressure measurements). Possibly prodromal symptoms, such as nausea, dizziness, lightheadedness, palpitations, asthenia, confusion and diaphoresis generally occurred within the first 3 hours following dosing, and often preceded the syncope. Patients need to be made aware that they could experience syncope at any time with or without prodromal symptoms during their treatment with dapoxetine. Prescribers should counsel patients about the importance of maintaining adequate hydration and about how to recognize prodromal signs and symptoms to decrease the likelihood of serious injury associated with falls due to loss of consciousness. If the patient experiences possibly prodromal symptoms, the patient should immediately lie down so his head is lower than the rest of his body or sit down with his head between his knees until the symptoms pass, and be cautioned to avoid situations where injury could result, including driving or operating hazardous machinery, should syncope or other CNS effects occur (see section 4.7).

Patients with cardiovascular risk factors

Subjects with underlying cardiovascular disease were excluded from Phase 3 clinical trials. The risk of adverse cardiovascular outcomes from syncope (cardiac syncope and syncope from other causes) is increased in patients with underlying structural cardiovascular disease (e.g., documented outflow obstruction, valvular heart disease, carotid stenosis and coronary artery disease). There are insufficient data to determine whether this increased risk extends to vasovagal syncope in patients with underlying cardiovascular disease.

Use with recreational drugs

Patients should be advised not to use Endura® in combination with recreational drugs.

Recreational drugs with serotonergic activity such as ketamine, methylenedioxymethamphetamine (MDMA) and lysergic acid diethylamide (LSD) may lead to potentially serious reactions if combined with dapoxetine. These reactions include, but are not limited to, arrhythmia, hyperthermia, and serotonin syndrome. Use of dapoxetine with recreational drugs with sedative properties such as narcotics and benzodiazepines may further increase somnolence and dizziness.

Ethanol

Patients should be advised not to use Endura® in combination with alcohol.

Combining alcohol with dapoxetine may increase alcohol-related neurocognitive effects and may also enhance neurocardiogenic adverse events such as syncope, thereby increasing the risk of accidental injury; therefore, patients should be advised to avoid alcohol while taking Endura® (see sections 4.5 and 4.7).

Medicinal products with vasodilatation properties

Endura® should be prescribed with caution in patients taking medicinal products with vasodilatation properties (such as alpha adrenergic receptor antagonists and nitrates) due to possible reduced orthostatic tolerance (see section 4.5).

Moderate CYP3A4 inhibitors

Caution is advised in patients taking moderate CYP3A4 inhibitors and the dose is restricted to 30 mg (see sections 4.2 and 4.5).

Potent CYP2D6 inhibitors

Caution is advised if increasing the dose to 60 mg in patients taking potent CYP2D6 inhibitors or if increasing the dose to 60 mg in patients known to be of CYP2D6 poor metabolizer genotype, as this may increase exposure levels, which may result in a higher incidence and severity of dose dependent adverse events (see sections 4.2, 4.5 and 5.2).

Mania

Endura® should not be used in patients with a history of mania/hypomania or bipolar disorder and should be discontinued in any patient who develops symptoms of these disorders.

Seizure

Due to the potential of SSRIs to lower the seizure threshold, Endura® should be discontinued in any patient who develops seizures and avoided in patients with unstable epilepsy. Patients with controlled epilepsy should be carefully monitored.

Paediatric population

Endura® should not be used in individuals below 18 years of age.

Depression and/or psychiatric disorders

Men with underlying signs and symptoms of depression should be evaluated prior to treatment with Endura® to rule out undiagnosed depressive disorders. Concomitant treatment of Endura® with antidepressants, including SSRIs and SNRIs, is contraindicated (see section 4.3). Discontinuation of treatment for ongoing depression or anxiety in order to initiate Endura® for the treatment of PE is not recommended. Endura® is not indicated for psychiatric disorders and should not be used in men with these disorders, such as schizophrenia, or in those suffering with co-morbid depression, as worsening of symptoms associated with depression cannot be excluded. This could be the result of underlying psychiatric disorder or might be a result of medicinal product therapy. Physicians should encourage patients to report any distressing thoughts or feelings at any time and if signs and symptoms of depression develop during treatment, Endura® should be discontinued.

Haemorrhage

There have been reports of bleeding abnormalities with SSRIs. Caution is advised in patients taking Endura®, particularly in concomitant use with medicinal products known to affect platelet function (e.g., atypical antipsychotics and phenothiazines, acetylsalicylic acid, nonsteroidal anti-inflammatory drugs [NSAIDs], anti-platelet agents) or anticoagulants (e.g., warfarin), as well as in patients with a history of bleeding or coagulation disorders (see section 4.5).

Renal impairment

Endura® is not recommended for use in patients with severe renal impairment and caution is advised in patients with mild or moderate renal impairment (see sections 4.2 and 5.2).

Withdrawal effects

Abrupt discontinuation of chronically administered SSRIs used to treat chronic depressive disorders has been reported to result in the following symptoms: dysphoric mood, irritability, agitation, dizziness, sensory disturbances (e.g., paresthesias such as electric shock sensations), anxiety, confusion, headache, lethargy, emotional lability, insomnia and hypomania.

A double-blind clinical trial in subjects with PE designed to assess the withdrawal effects of 62 days of daily or as needed dosing with 60 mg dapoxetine showed mild withdrawal symptoms with a slightly higher incidence of insomnia and dizziness in subjects switched to placebo after daily dosing (see section 5.1).

Eye disorders

The use of Endura® has been associated with ocular effects such as mydriasis and eye pain. Endura® should be used with caution in patients with raised intraocular pressure or those at risk of angle closure glaucoma.

Lactose intolerance

Patients with rare hereditary problems of galactose intolerance, total lactase deficiency or glucose-galactose malabsorption should not take this medicine.

This medicine contains less than 1 mmol sodium (23 mg) per tablet, that is to say essentially 'sodium free'.


Potential for interaction with monoamine oxidase inhibitors

In patients receiving an SSRI in combination with a monoamine oxidase inhibitor (MAOI), there have been reports of serious, sometimes fatal, reactions including hyperthermia, rigidity, myoclonus, autonomic instability with possible rapid fluctuations of vital signs, and mental status changes that include extreme agitation progressing to delirium and coma. These reactions have also been reported in patients who have recently discontinued an SSRI and have been started on an MAOI. Some cases presented with features resembling neuroleptic malignant syndrome. Animal data on the effects of combined use of an SSRI and MAOIs suggest that these medicinal products may act synergistically to elevate blood pressure and evoke behavioural excitation. Therefore, Endura® should not be used in combination with an MAOI, or within 14 days of discontinuing treatment with an MAOI. Similarly, an MAOI should not be administered within 7 days after Endura® has been discontinued (see section 4.3).

Potential for interaction with thioridazine

Thioridazine administration alone produces prolongation of the QTc interval, which is associated with serious ventricular arrhythmias. Medicinal products such as dapoxetine that inhibit the CYP2D6 isoenzyme appear to inhibit the metabolism of thioridazine and the resulting elevated levels of thioridazine are expected to augment the prolongation of the QTc interval. Endura® should not be used in combination with thioridazine or within 14 days of discontinuing treatment with thioridazine. Similarly, thioridazine should not be administered within 7 days after Endura® has been discontinued (see section 4.3).

Medicinal/herbal products with serotonergic effects

As with other SSRIs, co-administration with serotonergic medicinal/herbal products (including MAOIs, L-tryptophan, triptans, tramadol, linezolid, SSRIs, SNRIs, lithium and St. John's Wort (Hypericum perforatum) preparations) may lead to an incidence of serotonin associated effects. dapoxetine should not be used in combination with other SSRIs, MAOIs or other serotonergic medicinal/herbal products or within 14 days of discontinuing treatment with these medicinal/herbal products. Similarly, these medicinal/herbal products should not be administered within 7 days after Endura® has been discontinued (see section 4.3).

CNS active medicinal products

The use of dapoxetine in combination with CNS active medicinal products (e.g., antiepileptics, antidepressants, antipsychotics, anxiolytics, sedative hypnotics) has not been systematically evaluated in patients with premature ejaculation. Consequently, caution is advised if the concomitant administration of Endura® and such medicinal products is required.

Pharmacokinetic interactions

Effects of co-administered medicinal products on the pharmacokinetics of dapoxetine

In vitro studies in human liver, kidney, and intestinal microsomes indicate dapoxetine is metabolized primarily by CYP2D6, CYP3A4 and flavin monooxygenase 1 (FMO1). Therefore, inhibitors of these enzymes may reduce dapoxetine clearance.

CYP3A4 inhibitors

Potent CYP3A4 inhibitors. Administration of ketoconazole (200 mg twice daily for 7 days) increased the Cmax and AUCinf of dapoxetine (60 mg single dose) by 35% and 99%, respectively. Considering the contribution of both unbound dapoxetine and desmethyldapoxetine, the Cmax of the active fraction may be increased by approximately 25% and the AUC of the active fraction may be doubled if taken with potent CYP3A4 inhibitors.

The increases in the Cmax and AUC of the active fraction may be markedly increased in a part of the population which lack a functional CYP2D6 enzyme, i.e., CYP2D6 poor metabolizers, or in combination with potent inhibitors of CYP2D6.

Therefore, concomitant use of Endura® and potent CYP3A4 inhibitors, such as ketoconazole, itraconazole, ritonavir, saquinavir, telithromycin, nefazodone, nelfinavir and atazanavir, is contraindicated. Grapefruit juice is also a potent CYP3A4 inhibitor and should be avoided within 24 hours prior to taking Endura® (see section 4.3).

Moderate CYP3A4 inhibitors. Concomitant treatment with moderate CYP3A4 inhibitors (e.g., erythromycin, clarithromycin, fluconazole, amprenavir, fosamprenavir, aprepitant, verapamil, diltiazem) may also give rise to significantly increased exposure of dapoxetine and desmethyldapoxetine, especially in CYP2D6 poor metabolizers. The maximum dose of dapoxetine should be 30 mg if dapoxetine is combined with any of these drugs (see sections 4.2, 4.4 and below).

These two measures apply to all patients unless the patient has been verified to be a CYP2D6 extensive metabolizer by geno- or phenotyping. In patients verified to be CYP2D6 extensive metabolizers, a maximum dose of 30 mg is advised if dapoxetine is combined with a potent CYP3A4 inhibitor and caution is advised if dapoxetine in 60 mg doses is taken concomitantly with a moderate CYP3A4 inhibitor.

Potent CYP2D6 inhibitors

The Cmax and AUCinf of dapoxetine (60 mg single dose) increased by 50% and 88%, respectively, in the presence of fluoxetine (60 mg/day for 7 days). Considering the contribution of both unbound dapoxetine and desmethyldapoxetine, the Cmax of the active fraction may be increased by approximately 50% and the AUC of the active fraction may be doubled if taken with potent CYP2D6 inhibitors. These increases in the Cmax and AUC of the active fraction are similar to those expected for CYP2D6 poor metabolizers and may result in a higher incidence and severity of dose dependent adverse events (see section 4.4).

PDE5 inhibitors

dapoxetine should not be used in patients using PDE5 inhibitors due to possible reduced orthostatic tolerance (see section 4.4). The pharmacokinetics of dapoxetine (60 mg) in combination with tadalafil (20 mg) and sildenafil (100 mg) were evaluated in a single dose crossover study. Tadalafil did not affect the pharmacokinetics of dapoxetine. Sildenafil caused slight changes in dapoxetine pharmacokinetics (22% increase in AUCinf and 4% increase in Cmax), which are not expected to be clinically significant.

Concomitant use of Endura® with PDE5 inhibitors may result in orthostatic hypotension (see section 4.4). The efficacy and safety of Endura® in patients with both premature ejaculation and erectile dysfunction concomitantly treated with Endura® and PDE5 inhibitors have not been established.

Effects of dapoxetine on the pharmacokinetics of co-administered medicinal products

Tamsulosin

Concomitant administration of single or multiple doses of 30 mg or 60 mg dapoxetine to patients receiving daily doses of tamsulosin did not result in changes in the pharmacokinetics of tamsulosin. The addition of dapoxetine to tamsulosin did not result in a change in the orthostatic profile and there were no differences in orthostatic effects between tamsulosin combined with either 30 or 60 mg dapoxetine and tamsulosin alone; however, Endura® should be prescribed with caution in patients who use alpha adrenergic receptor antagonists due to possible reduced orthostatic tolerance (see section 4.4).

Medicinal products metabolized by CYP2D6

Multiple doses of dapoxetine (60 mg/day for 6 days) followed by a single 50 mg dose of desipramine increased the mean Cmax and AUCinf of desipramine by approximately 11% and 19%, respectively, compared to desipramine administered alone. Dapoxetine may give rise to a similar increase in the plasma concentrations of other drugs metabolized by CYP2D6. The clinical relevance is likely to be small.

Medicinal products metabolized by CYP3A4

Multiple dosing of dapoxetine (60 mg/day for 6 days) decreased the AUCinf of midazolam (8 mg single dose) by approximately 20% (range -60 to +18%). The clinical relevance of the effect on midazolam is likely to be small in most patients. The increase in CYP3A activity may be of clinical relevance in some individuals concomitantly treated with a medicinal product mainly metabolized by CYP3A and with a narrow therapeutic window.

Medicinal products metabolized by CYP2C19

Multiple dosing of dapoxetine (60 mg/day for 6 days) did not inhibit the metabolism of a single 40 mg dose of omeprazole. Dapoxetine is unlikely to affect the pharmacokinetics of other CYP2C19 substrates.

Medicinal products metabolized by CYP2C9

Multiple dosing of dapoxetine (60 mg/day for 6 days) did not affect the pharmacokinetics or pharmacodynamics of a single 5 mg dose of glibenclamide. Dapoxetine is unlikely to affect the pharmacokinetics of other CYP2C9 substrates.

Warfarin and medicinal products that are known to affect coagulation and/or platelet function

There are no data evaluating the effect of chronic use of warfarin with dapoxetine; therefore, caution is advised when dapoxetine is used in patients taking warfarin chronically (see section 4.4). In a pharmacokinetic study, dapoxetine (60 mg/day for 6 days) did not affect the pharmacokinetics or pharmacodynamics (PT or INR) of warfarin following a single 25 mg dose.

There have been reports of bleeding abnormalities with SSRIs (see section 4.4).

Ethanol

Coadministration of a single dose of ethanol, 0.5 g/kg (approximately 2 drinks), did not affect the pharmacokinetics of dapoxetine (60 mg single dose); however, dapoxetine in combination with ethanol increased somnolence and significantly decreased self-rated alertness. Pharmacodynamic measures of cognitive impairment (Digit Vigilance Speed, Digit Symbol Substitution Test) also showed an additive effect when dapoxetine was coadministered with ethanol. Concomitant use of alcohol and dapoxetine increases the chance or severity of adverse reactions such as dizziness, drowsiness, slow reflexes, or altered judgment. Combining alcohol with dapoxetine may increase these alcohol-related effects and may also enhance neurocardiogenic adverse events such as syncope, thereby increasing the risk of accidental injury; therefore, patients should be advised to avoid alcohol while taking Endura® (see sections 4.4 and 4.7).


Endura® is not indicated for use by women.

Animal studies do not indicate direct or indirect harmful effects with respect to fertility, pregnancy or embryonal/foetal development (see section 5.3).

It is not known if either dapoxetine or its metabolites are excreted in human milk.

 


Dapoxetine has minor or moderate influence on the ability to drive and use machines. Dizziness, disturbance in attention, syncope, blurred vision and somnolence have been reported in subjects receiving dapoxetine in clinical trials. Therefore, patients should be warned to avoid situations where injury could result, including driving or operating hazardous machinery.

Combining alcohol with dapoxetine may increase alcohol-related neurocognitive effects and may also enhance neurocardiogenic adverse events such as syncope, thereby increasing the risk of accidental injury; therefore, patients should be advised to avoid alcohol while taking Endura® (see sections 4.4 and 4.5).

 


Summary of the safety profile

Syncope and orthostatic hypotension have been reported in clinical trials (see section 4.4).

The following adverse drug reactions were reported during Phase 3 clinical trials most commonly and were dose related: nausea (11.0% and 22.2% in 30 mg and 60 mg prn dapoxetine groups, respectively), dizziness (5.8% and 10.9%), headache (5.6% and 8.8%), diarrhoea (3.5% and 6.9%), insomnia (2.1% and 3.9%) and fatigue (2.0% and 4.1%). The most common adverse events leading to discontinuation were nausea (2.2% of dapoxetine-treated subjects) and dizziness (1.2% of dapoxetine-treated subjects).

Tabulated list of adverse reactions

The safety of dapoxetine was evaluated in 4224 subjects with premature ejaculation who participated in five double-blind, placebo-controlled clinical trials. Of the 4224 subjects, 1616 received dapoxetine 30 mg as needed and 2608 received 60 mg, either as needed or once daily.

Table 1 presents the adverse reactions that have been reported.

Table 1: Frequency of Adverse Reactions (MedDRA)

System Organ Class

Very common

(> 1/10)

Common

(≥ 1/100 to < 1/10)

Uncommon

(≥ 1/1000 to < 1/100)

Rare

(≥ 1/10000 to < 1/1000)

Psychiatric disorders

 

Anxiety, Agitation, Restlessness, Insomnia, Abnormal dreams, Libido decreased

Depression, Depressed mood, Euphoric mood, Mood altered, Nervousness, Indifference, Apathy, Confusional state, Disorientation, Thinking abnormal, Hypervigilance, Sleep disorder, Initial insomnia, Middle insomnia, Nightmare, Bruxism, Loss of libido, Anorgasmia

 

Nervous system disorders

Dizziness, Headache

Somnolence, Disturbance in attention, Tremor, Paraesthesia

Syncope, Syncope vasovagal, Dizziness postural, Akathisia, Dysgeusia, Hypersomnia, Lethargy, Sedation, Depressed level of consciousness

Dizziness exertional, Sudden onset of sleep

Eye disorders

 

Vision blurred

Mydriasis (see section 4.4), Eye pain, Visual disturbance

 

Ear and labyrinth disorders

 

Tinnitus

Vertigo

 

Cardiac disorders

  

Sinus arrest, Sinus bradycardia, Tachycardia

 

Vascular disorders

 

Flushing

Hypotension, Systolic hypertension, Hot flush

 

Respiratory, thoracic and mediastinal disorders

 

Sinus congestion, Yawning

  

Gastrointestinal disorders

Nausea

Diarrhoea, Vomiting, Constipation, Abdominal pain, Abdominal pain upper, Dyspepsia, Flatulence, Stomach discomfort, Abdominal distension, Dry mouth

Abdominal discomfort, Epigastric discomfort

Defaecation urgency

Skin and subcutaneous tissue disorders

 

Hyperhidrosis

Pruritis, Cold sweat

 

Reproductive system and breast disorders

 

Erectile dysfunction

Ejaculation failure, Male orgasmic disorder, Paraesthesia of genital male

 

General disorders and administration site conditions

 

Fatigue, Irritability

Asthenia, Feeling hot, Feeling jittery, Feeling abnormal, Feeling drunk

 

Investigations

 

Blood pressure increased

Heart rate increased, Blood pressure diastolic increased, Blood pressure orthostatic increased

 

Adverse drug reactions reported in the 9-month long-term open-label extension trial were consistent with those reported in the double-blind studies and no additional adverse drug reactions were reported.

Description of selected adverse reactions

Syncope characterized as loss of consciousness, with bradycardia or sinus arrest observed in patients wearing Holter monitors, has been reported in clinical trials and is considered medicinal product-related. The majority of cases occurred during the first 3 hours after dosing, after the first dose or associated with study-related procedures in the clinical setting (such as blood draw and orthostatic maneuvers and blood pressure measurements). Prodromal symptoms often preceded the syncope (see section 4.4).

The occurrence of syncope and possibly prodromal symptoms appears dose dependent as demonstrated by higher incidence among patients treated with higher than recommended doses in Phase 3 clinical trials.

Orthostatic hypotension has been reported in clinical trials (see section 4.4).The frequency of syncope characterized as loss of consciousness in the dapoxetine clinical development program varied depending on the population studied and ranged from 0.06% (30 mg) to 0.23% (60 mg) for subjects enrolled in the Phase 3 placebo-controlled clinical trials to 0.64% (all doses combined) for Phase 1 non-PE healthy volunteer studies.

Other special populations

Caution is advised if increasing the dose to 60 mg in patients taking potent CYP2D6 inhibitors or if increasing the dose to 60 mg in patients known to be of CYP2D6 poor metabolizer genotype (see sections 4.2, 4.4, 4.5 and 5.2).

Withdrawal effects

Abrupt discontinuation of chronically administered SSRIs used to treat chronic depressive disorders has been reported to result in the following symptoms: dysphoric mood, irritability, agitation, dizziness, sensory disturbances (e.g., paresthesias such as electric shock sensations), anxiety, confusion, headache, lethargy, emotional lability, insomnia and hypomania.

Results of a safety study showed a slightly higher incidence of withdrawal symptoms of mild or moderate insomnia and dizziness in subjects switched to placebo after 62 days of daily dosing.

 

To report any side effect (s):

•Saudi Arabia:

The National Pharmacovigilance Center (NPC):

SFDA Call Center: 19999

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

Website: https://ade.sfda.gov.sa

•Other GCC States:

Please contact the relevant competent authority.


No case of overdose has been reported.

There were no unexpected adverse events in a clinical pharmacology study of dapoxetine with daily doses up to 240 mg (two 120 mg doses given 3 hours apart). In general, symptoms of overdose with SSRIs include serotonin-mediated adverse reactions such as somnolence, gastrointestinal disturbances such as nausea and vomiting, tachycardia, tremor, agitation and dizziness.

In cases of overdose, standard supportive measures should be adopted as required. Due to high protein binding and large volume of distribution of dapoxetine hydrochloride, forced diuresis, dialysis, hemoperfusion and exchange transfusion are unlikely to be of benefit. No specific antidotes for dapoxetine are known.


Pharmacotherapeutic group: Other Urologicals, ATC code: G04BX14

Mechanism of action

Dapoxetine is a potent selective serotonin reuptake inhibitor (SSRI) with an IC50 of 1.12 nM, while its major human metabolites, desmethyldapoxetine (IC50 < 1.0 nM) and didesmethyldapoxetine (IC50 = 2.0 nM) are equivalent or less potent (dapoxetine-N-oxide (IC50 = 282 nM)).

Human ejaculation is primarily mediated by the sympathetic nervous system. The ejaculatory pathway originates from a spinal reflex centre, mediated by the brain stem, which is influenced initially by a number of nuclei in the brain (medial preoptic and paraventricular nuclei).

The mechanism of action of dapoxetine in premature ejaculation is presumed to be linked to the inhibition of neuronal reuptake of serotonin and the subsequent potentiation of the neurotransmitter's action at pre- and postsynaptic receptors.

In the rat, dapoxetine inhibits the ejaculatory expulsion reflex by acting at a supraspinal level within the lateral paragigantocellular nucleus (LPGi). Post ganglionic sympathetic fibers that innervate the seminal vesicles, vas deferens, prostate, bulbourethral muscles and bladder neck cause them to contract in a coordinated fashion to achieve ejaculation. Dapoxetine modulates this ejaculatory reflex in rats.

Clinical efficacy and safety

The effectiveness of dapoxetine in the treatment of premature ejaculation has been established in five double-blind, placebo-controlled clinical trials, in which a total of 6081 subjects were randomized. Subjects were 18 years of age or older and had a history of PE in the majority of intercourse experiences in the 6-month period prior to enrolment. Premature ejaculation was defined according to the DSM-IV diagnostic criteria: short ejaculatory time (an intravaginal ejaculatory latency time [IELT; time from vaginal penetration to the moment of intravaginal ejaculation] of ≤ 2 minutes measured using a stopwatch in four studies), poor control over ejaculation, marked distress or interpersonal difficulty due to the condition.

Subjects with other forms of sexual dysfunction, including erectile dysfunction, or those using other forms of pharmacotherapy for the treatment of PE were excluded from all studies.

Results of all randomized studies were consistent. Efficacy was demonstrated after 12 weeks of treatment. One study enrolled patients both outside and within the EU and had a treatment duration of 24 weeks. In the study, 1162 subjects were randomized, 385 to placebo, 388 to dapoxetine 30 mg as needed, and 389 to dapoxetine 60 mg as needed. The mean and median Average IELT at study end are presented in Table 2 below and the cumulative distribution of subjects who achieved at least a specific level in Average IELT at study end are presented in Table 3 below. Other studies and pooled analysis of the data at Week 12 gave consistent results.

Table 2: Least squares mean and median Average IELT at study end*

Average IELT

Placebo

Dapoxetine 30 mg

Dapoxetine 60 mg

Median

1.05 min

1.72 min

1.91 min

Difference from placebo [95% CI]

 

0.6 min**

[0.37, 0.72]

0.9 min**

[0.66, 1.06]

Least Squares Mean

1.7 min

2.9 min

3.3 min

Difference from placebo [95% CI]

 

1.2 min**

[0.59, 1.72]

1.6 min**

[1.02, 2.16]

*Baseline value carried forward for subjects with no post-baseline data.

**Difference was statistically significant (p-value <= 0.001).

Table 3: Subjects achieving at least a specific level in Average IELT at study end*

IELT

(mins)

Placebo

%

Dapoxetine 30 mg

%

Dapoxetine 60 mg

%

≥1.0

51.6

68.8

77.6

≥2.0

23.2

44.4

47.9

≥3.0

14.3

26.0

37.4

≥4.0

10.4

18.4

27.6

≥5.0

7.6

14.3

19.6

≥6.0

5.0

11.7

14.4

≥7.0

3.9

9.1

9.8

≥8.0

2.9

6.5

8.3

* Baseline value carried forward for subjects with no post-baseline data.

The magnitude of IELT prolongation was related to baseline IELT and was variable between individual subjects. The clinical relevance of dapoxetine treatment effects was further demonstrated in terms of various patient reported outcome measures and a responder analysis.

A responder was defined as a subject who had at least a 2-category increase in control over ejaculation plus at least a 1-category decrease in ejaculation-related distress. A statistically significantly greater percentage of subjects responded in each of the dapoxetine groups versus placebo at the end of the study Week 12 or 24. There was a higher percentage of responders in the dapoxetine 30 mg (11.1% - 95% CI [7.24; 14.87]) and 60 mg (16.4% - 95% CI [13.01; 19.75]) groups compared with the placebo group at Week 12 (pooled analysis).

The clinical relevance of dapoxetine treatment effects is represented by treatment group for the subject's Clinical Global Impression of Change (CGIC) outcome measure, in which patients were asked to compare their premature ejaculation from the start of the study, with response options ranging from much better to much worse. At study end (Week 24), 28.4% (30 mg group) and 35.5% (60 mg group) of subjects reported their condition to be “better” or “much better”, compared to 14% for placebo, while 53.4% and 65.6% of subjects treated with dapoxetine 30 mg and 60 mg, respectively, reported their condition to be at least “slightly better”, compared to 28.8% for placebo.


Absorption

Dapoxetine is rapidly absorbed with maximum plasma concentrations (Cmax) occurring approximately 1-2 hours after tablet intake. The absolute bioavailability is 42% (range 15-76%), and dose proportional increases in exposure (AUC and Cmax) are observed between the 30 and 60 mg dose strengths. Following multiple doses, AUC values for both dapoxetine and the active metabolite desmethyldapoxetine (DED) increase by approximately 50% when compared to single dose AUC values.

Ingestion of a high fat meal modestly reduced the Cmax (by 10%) and modestly increased the AUC (by 12%) of dapoxetine and slightly delayed the time for dapoxetine to reach peak concentrations. These changes are not clinically significant. Endura® can be taken with or without food.

Distribution

More than 99% of dapoxetine is bound in vitro to human serum proteins. The active metabolite desmethyldapoxetine (DED) is 98.5% protein bound. Dapoxetine has a mean steady state volume of distribution of 162 L.

Biotransformation

In vitro studies suggest that dapoxetine is cleared by multiple enzyme systems in the liver and kidneys, primarily CYP2D6, CYP3A4, and flavin monooxygenase (FMO1). Following oral dosing of 14C-dapoxetine, dapoxetine was extensively metabolized to multiple metabolites primarily through the following biotransformational pathways: N-oxidation, N-demethylation, naphthyl hydroxylation, glucuronidation and sulfation. There was evidence of presystemic first-pass metabolism after oral administration.

Intact dapoxetine and dapoxetine-N-oxide were the major circulating moieties in the plasma. In vitro binding and transporter studies show that dapoxetine-N-oxide is inactive. Additional metabolites including desmethyldapoxetine and didesmethyldapoxetine account for less than 3% of the total circulating drug –related materials in plasma. In vitro binding studies indicate that DED is equipotent to dapoxetine and didesmethyldapoxetine has approximately 50% of the potency of dapoxetine (see section 5.1). The unbound exposures (AUC and Cmax) of DED are approximately 50% and 23%, respectively, of the unbound exposure of dapoxetine.

Elimination

The metabolites of dapoxetine were primarily eliminated in the urine as conjugates. Unchanged active substance was not detected in the urine. Following oral administration, dapoxetine has an initial (disposition) half-life of approximately 1.5 hours, with plasma levels less than 5% of peak concentrations by 24 hours post-dose, and a terminal half-life of approximately 19 hours. The terminal half-life of DED is approximately 19 hours.

Pharmacokinetics in special populations

The metabolite DED contributes to the pharmacological effect of dapoxetine, particularly when the exposure of DED is increased. Below, in some populations, the increase in active fraction parameters is presented. This is the sum of the unbound exposure of dapoxetine and DED. DED is equipotent to dapoxetine. The estimation assumes equal distribution of DED to the CNS but it is unknown whether this is the case.

Race

Analyses of single dose clinical pharmacology studies using 60 mg dapoxetine indicated no statistically significant differences between Caucasians, Blacks, Hispanics and Asians. A clinical study conducted to compare the pharmacokinetics of dapoxetine in Japanese and Caucasian subjects showed 10% to 20% higher plasma levels (AUC and peak concentration) of dapoxetine in Japanese subjects due to lower body weight. The slightly higher exposure is not expected to have a meaningful clinical effect.

Elderly (age 65 years and over)

Analyses of a single dose clinical pharmacology study using 60 mg dapoxetine showed no significant differences in pharmacokinetic parameters (Cmax, AUCinf, Tmax) between healthy elderly males and healthy young adult males. The efficacy and safety has not been established in this population (see section 4.2).

Renal impairment

A single-dose clinical pharmacology study using a 60 mg dapoxetine dose was conducted in subjects with mild (CrCL 50 to 80 mL/min), moderate (CrCL 30 to < 50 mL/min), and severe renal impairment (CrCL < 30 mL/min) and in subjects with normal renal function (CrCL > 80 mL/min). No clear trend for an increase in dapoxetine AUC with decreasing renal function was observed. AUC in subjects with severe renal impairment was approximately 2-fold that of subjects with normal renal function, although there are limited data in patients with severe renal impairment. Dapoxetine pharmacokinetics have not been evaluated in patients requiring renal dialysis (see sections 4.2 and 4.4).

Hepatic impairment

In patients with mild hepatic impairment, unbound Cmax of dapoxetine is decreased by 28% and unbound AUC is unchanged. The unbound Cmax and AUC of the active fraction (the sum of the unbound exposure of dapoxetine and desmethyldapoxetine) were decreased by 30% and 5%, repectively. In patients with moderate hepatic impairment, unbound Cmax of dapoxetine is essentially unchanged (decrease of 3%) and unbound AUC is increased by 66%. The unbound Cmax and AUC of the active fraction were essentially unchanged and doubled, respectively.

In patients with severe hepatic impairment, the unbound Cmax of dapoxetine was decreased by 42% but the unbound AUC was increased by approximately 223%. The Cmax and AUC of the active fraction had similar changes (see sections 4.2 and 4.3).

CYP2D6 Polymorphism

In a single dose clinical pharmacology study using 60 mg dapoxetine, plasma concentrations in poor metabolizers of CYP2D6 were higher than in extensive metabolizers of CYP2D6 (approximately 31% higher for Cmax and 36% higher for AUCinf of dapoxetine and 98% higher for Cmax and 161% higher for AUCinf of desmethyldapoxetine). The active fraction of dapoxetine may be increased by approximately 46% at Cmax and by approximately 90% at AUC. This increase may result in a higher incidence and severity of dose dependent adverse events (see section 4.2). The safety of dapoxetine in poor metabolizers of CYP2D6 is of particular concern with concomitant administration of other medicinal products that may inhibit the metabolism of dapoxetine such as moderate and potent CYP3A4 inhibitors (see sections 4.2 and 4.3).


A full assessment of the safety pharmacology, repeat dose toxicology, genetic toxicology, carcinogenicity, dependence/withdrawal liability, phototoxicity and developmental reproductive toxicology of dapoxetine was conducted in preclinical species (mouse, rat, rabbit, dog and monkey) up to the maximum tolerated doses in each species. Due to the more rapid bioconversion in the preclinical species than in man, pharmacokinetic exposure indices (Cmax and AUC0-24 hr) at the maximum tolerated doses in some studies approached those observed in man. However, the body weight normalized dose multiples were greater than 100-fold. There were no clinically relevant safety hazards identified in any of these studies.

In studies with oral administration, dapoxetine was not carcinogenic to rats when administered daily for approximately two years at doses up to 225 mg/kg/day, yielding approximately twice the exposures (AUC) seen in human males given the Maximum Recommended Human Dose (MRHD) of 60 mg. Dapoxetine also did not cause tumors in Tg.rasH2 mice when administered at the maximum possible doses of 100 mg/kg for 6 months and 200 mg/kg for 4 months. The steady state exposures of dapoxetine in mice following 6-months oral administration at 100 mg/kg/day were less than the single dose exposures observed clinically at 60 mg.

There were no effects on fertility, reproductive performance or reproductive organ morphology in male or female rats and no adverse signs of embryotoxicity or fetotoxicity in the rat or rabbit. Reproductive toxicity studies did not include studies to assess the risk of adverse effects after exposure during the peri-post-natal period.


Lactose monohydrate, microcrystalline cellulose, croscarmellose sodium, colloidal anhydrous silica, magnesium stearate, purified water, Opadry II Grey powder (polyvinyl alcohol-hydrolized, Talc, titanium dioxide, macrogol/PEG, lecithin, black iron oxide, red iron oxide, yellow iron oxide).

 


Not applicable.


2 years

Store below 30°C.


Endura® 30 mg Film Coated Tablet: grey round normal biconvex film coated tablets engraved with H31 on one face, presented in PVC/TE/PVDC/AIu blister intended for oral use.

Pack size: 3 Film Coated Tablets (3 tablets/blister, 1 blister/pack).

9 Film Coated Tablets (3 tablets/blister, 3 blisters/pack)

Endura® 60 mg Film Coated Tablet: grey round normal biconvex film coated tablets engraved with H32 on one face, presented in PVC/TE/PVDC/AIu blister intended for oral use.

Pack size: 3 Film Coated Tablets (3 tablets/blister, 1 blister/pack).

9 Film Coated Tablets (3 tablets/blister, 3 blisters/pack)


No special requirements.


Med City Pharma-KSA. 1st Industrial city, Phase 5, Jeddah –KSA. Tel: 0096698003288 Mobile: 00966555786968 P.O .Box: 4072 - Jeddah 22429 E-mail: info@medcitypharma.com

08/2024
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