Source: Medicines & Healthcare Products Regulatory Agency (GB) Revision Year: 2022 Publisher: Takeda UK Limited, 1 Kingdom Street, London, W2 6BD, United Kingdom
Hypersensitivity to the active substance, any of the excipients or to synthetic gonadotrophin releasing homone (Gn-RH) or Gn-RH derivatives.
Women: PROSTAP 3 is contra-indicated in women who are or may become pregnant while receiving the drug. PROSTAP 3 should not be used in women who are breastfeeding or have undiagnosed abnormal vaginal bleeding.
In the pre- and perimenopausal breast cancer setting: Initiation of aromatase inhibitor treatment before adequate ovarian suppression with leuprorelin has been achieved (see sections 4.2 and 4.4).
Men: There are no known contra-indications to the use of PROSTAP 3 in men.
In girls with central precocious puberty:
PROSTAP 3 injectable suspension must be prepared at the time of use and, after reconstitution, used immediately.
PROSTAP 3 contains sodium. This medicine contains less than 1 mmol sodium (23 mg) per injection, this is to say it is essentially ‘sodium free’.
Depression: There is an increased risk of incident depression (which may be severe) in patients undergoing treatment with GnRH agonists, such as leuprorelin. Patients should be informed and monitored accordingly and treated as appropriate if symptoms occur.
Seizure: Postmarketing reports of seizures have been observed in patients treated with leuprorelin acetate and these events have been reported in both children and adults, and in those with or without a history of epilepsy, seizure disorders or risk disorders for seizures.
Adults: Epidemiological data have shown that during androgen deprivation therapy in males and estrogen deprivation therapy in females, changes in the metabolic condition (e.g. reduction in glucose tolerance or aggravation of pre-existing diabetes) as well as an increased risk for cardiovascular diseases may occur. However, prospective data did not confirm a link between treatment with GnRH analogues and an increase in cardiovascular mortality. Patients at high risk for metabolic or cardiovascular diseases should be appropriately monitored. Diabetic patients may require more frequent monitoring of blood glucose during treatment with PROSTAP 3.
Hepatic dysfunction and jaundice with elevated liver enzyme have been reported. Therefore, close observation should be made and appropriate measures taken if necessary.
Spinal fracture, paralysis and hypotension have been reported.
Bone mineral loss: Long-term estrogen deprivation either by bilateral oophorectomy, ovarian ablation or administration of GnRH analogues, or long-term androgen deprivation either by bilateral orchiectomy or administration of GnRH analogues is associated with increased risk of bone mineral loss which, in patients with additional risk factors, may lead to osteoporosis and an increased risk of bone fracture (see section 4.8).
An induced hypo-estrogenic state results in a loss in bone density over the course of treatment, some of which may not be reversible e.g. the extent of bone demineralisation due to hypo-estrogenaemia is proportional to time. The generally accepted level of bone loss with GnRH analogues such as PROSTAP 3 is 5%. In clinical studies with PROSTAP 3 the levels varied between 2.3% and 15.7% depending on the method of measurement. During one treatment period e.g. six months, this bone loss should not be important.
In patients with major risk factors for decreased bone mineral content such as chronic alcohol and/or tobacco use, strong family history of osteoporosis, or chronic use of drugs that can reduce bone mass such as anticonvulsants or corticosteroids, PROSTAP SR therapy may pose an additional risk. In these patients, the risks and benefits must be weighed carefully before therapy with PROSTAP 3 is instituted. This is particularly important in women with uterine fibroids where age related bone loss may have already begun to occur.
Idiopathic intracranial hypertension (pseudotumor cerebri) has been reported in patients receiving leuprorelin. Patients should be warned for signs and symptoms of idiopathic intracranial hypertension, including severe or recurrent headache, vision disturbances and tinnitus. If idiopathic intracranial hypertension occurs, discontinuation of leuprorelin should be considered.
In the initial stages of therapy, a transient rise in levels of testosterone, dihydrotestosterone and acid phosphatase may occur. In some cases, this may be associated with a “flare” or exacerbation of the tumour growth resulting in temporary deterioration of the patient’s condition. These symptoms usually subside on continuation of therapy. “Flare” may manifest itself as systemic or neurological symptoms in some cases.
In order to reduce the risk of “flare”, an anti-androgen may be administered beginning 3 days prior to leuprorelin acetate therapy and continuing for the first two to three weeks of treatment. This has been reported to prevent the sequelae of an initial rise in serum testosterone. If an anti-androgen is used over a prolonged period, due attention should be paid to the contra-indications and precautions associated with its extended use.
In the rare event of an abscess occurring at the injection site, testosterone level should be monitored as there may be inadequate absorption of leuprorelin from the depot formulation.
Patients at risk of or with ureteric obstruction or spinal cord compression due to metastasis, should be considered carefully and closely supervised in the first few weeks of treatment as bone pain, weakness of the lower extremities and paraesthesia (as neurologic symptom) may occur. These patients should be considered for prophylactic treatment with anti-androgens. Should urological/neurological complications occur, these should be treated by appropriate specific measures.
Whilst the development of pituitary adenomas has been noted in chronic toxicity studies at high doses in some animal species, this has not been observed in long term clinical studies with leuprorelin acetate.
Androgen deprivation therapy may prolong the QT interval.
In patients with a history of or risk factors for QT prolongation and in patients receiving concomitant medicinal products that might prolong the QT interval (see section 4.5) physicians should assess risk and benefits including the potential for Torsade de pointes prior to initiating treatment with PROSTAP 3.
Initial increase in sex steroids:
During the early phase of therapy, sex steroids temporarily rise above baseline because of the physiological effect of the drug. Therefore, a worsening of clinical signs and symptoms may be observed during the initial days of therapy, but these will dissipate with continued therapy.
Endometriosis:
When receiving GnRH analogues for the treatment of endometriosis, the duration of administration of leuprorelin acetate should be limited to 6 months, as its use is associated with an increased risk of bone mineral loss (see Bone Mineral loss, section 4.4). The addition of HRT (an estrogen and progestogen) has been shown to reduce bone mineral density loss and vasomotor symptoms. Therefore, if appropriate, HRT may be co-administered with leuprorelin acetate, taking into account the risks and benefits of each medicinal product, for up to 6 months if clinically appropriate. If it is necessary to resume administration of leuprorelin acetate, changes in bone parameters should be closely followed.
Abnormal bleeding:
In women with submucous fibroids there have been reports of severe vaginal bleeding following administration of PROSTAP 3 as a consequence of the acute degeneration of the fibroids. Patients should be warned of the possibility of abnormal bleeding or pain in case earlier surgical intervention is required.
Cervical resistance:
PROSTAP 3 may cause an increase in uterine cervical resistance, which may result in difficulty in dilating the cervix for intrauterine surgical procedures.
Breast cancer:
Advanced and early breast cancer:
In order to ensure adequate ovarian suppression in pre- and perimenopausal women, treatment with leuprorelin should be administered for at least 6-8 weeks prior to commencement of an aromatase inhibitor, and 3 monthly leuprorelin injections should be administered on schedule and without interruption throughout aromatase inhibitor treatment.
Women who are premenopausal at breast cancer diagnosis and who become amenorrhoeic following chemotherapy may or may not have continued estrogen production from the ovaries. Irrespective of menstrual status, premenopausal status should be confirmed following chemotherapy and before commencement of leuprorelin, by blood concentrations of estradiol and FSH within the reference ranges for premenopausal women, in order to avoid unnecessary treatment with leuprorelin in the event of a chemotherapy-induced menopause.
Following commencement of leuprorelin, it is important to confirm adequate ovarian suppression (gonadotrophin analogue- induced menopause) by serial assessment of circulating FSH, and estradiol if this subset of women is to be considered for therapy with an aromatase inhibitor, in accordance with current clinical practice recommendations. Accordingly, ovarian suppression should be confirmed by low blood concentrations of FSH and estradiol prior to starting aromatase inhibitor treatment and measurements should be repeated every three months during combination therapy with leuprorelin and an aromatase inhibitor. This is to avoid aromatase inhibitor-induced rebound increase in circulating estrogen, with consequential implications for the breast cancer. Of note, circulating FSH levels are lowered in response to gonadotrophin analogue-induced ovarian suppression (induced menopause), unlike in a natural menopause where FSH levels are elevated.
Patients who have discontinued leuprorelin treatment should also discontinue aromatase inhibitors within 3 months of the last PROSTAP 3 administration.
Particular attention should also be paid to the prescribing information of co-administered medicinal products, such as aromatase inhibitors, tamoxifen, CDK4/6 inhibitors, for relevant safety information when administered in combination with leuprorelin.
Bone mineral density should be assessed before starting treatment with leuprorelin, particularly in women who have additional risk factors for osteoporosis. These patients should be closely monitored and treatment for, or prophylaxis of, osteoporosis should be initiated when appropriate
The risk of musculoskeletal disorders (including joint or musculoskeletal pain) when a GnRH agonist is used in combination with either an aromatase inhibitor or tamoxifen is approximately 89% with the aromatase inhibitor and approximately 76% with tamoxifen.
Hypertension has been reported as a targeted adverse event at a very common frequency with GnRH agonist in combination with either exemestane or tamoxifen.
Premenopausal women with breast cancer receiving GnRH agonist in combination with either exemestane or tamoxifen should have regular monitoring of cardiovascular risk factors and blood pressure.
Hyperglycaemia and diabetes were reported as targeted adverse events at a common frequency with a GnRH agonist in combination with either exemestane or tamoxifen. Premenopausal women with breast cancer receiving a GnRH agonist in combination with either exemestane or tamoxifen should have regular monitoring of risk factors for diabetes with blood glucose monitoring on a regular basis and appropriate anti-diabetic treatment initiated, if appropriate, according to national guidelines.
Depression has been reported to occur in approximately 50% of patients treated with a GnRH agonist in combination with either tamoxifen or exemestane, but less than 5% of patients had severe depression (grade 3-4). Patients should be informed accordingly and treated as appropriate if symptoms occur. Patients with known depression or depression history should be carefully monitored during therapy.
Treatment of premenopausal women with endocrine responsive early stage breast cancer with leuprorelin in combination with tamoxifen or an aromatase inhibitor should follow a careful individual appraisal of the risks and benefits.
Men: Patients with urinary obstruction and patients with metastatic vertebral lesions should begin PROSTAP 3 therapy under close supervision for the first few weeks of treatment.
Women: Before starting treatment with leuprorelin acetate, pregnancy must be excluded (see section 4.3) and undiagnosed abnormal vaginal bleeding must be investigated, diagnosis confirmed and relevant management initiated. During treatment with leuprorelin acetate, patients should be instructed to prevent conception e.g. with the use of non-hormonal methods. Since menstruation should stop with effective doses of PROSTAP 3, the patient should notify her physician if regular menstruation persists.
Children with central precocious puberty: Before starting treatment with leuprorelin acetate, a precise diagnosis of idiopathic and/or neurogenic central precocious should be made and in girls, pregnancy must be excluded (see section 4.3).
The therapy is a long-term treatment, adjusted individually. PROSTAP 3 should be administered as precisely as possible in regular 3-monthly periods. An exceptional delay of the injection date for a few days (90 ± 2 days) does not influence the results of the therapy.
In the event of a sterile abscess at the injection site (mostly reported after i.m. injection of higher than the recommended dosage) the absorption of leuprorelin acetate from the depot can be decreased. In this case the hormonal parameters (testosterone, oestradiol) should be monitored at 2-week intervals (see 4.2).
The treatment of children with progressive brain tumours should follow a careful individual appraisal of the risks and benefits.
The occurrence of vaginal bleeding, spotting and discharge after the first injection may occur as a sign of hormone withdrawal in girls. Vaginal bleeding beyond the first/second month of treatment needs to be investigated.
Bone mineral density (BMD) may decrease during GnRH therapy for central precocious puberty. However, after cessation of treatment subsequent bone mass accrual is preserved, and peak bone mass in late adolescence does not seem to be affected by treatment.
Slipped femoral epiphysis can be seen after withdrawal of GnRH treatment. The suggested theory is that the low concentrations of estrogen during treatment with GnRH agonists weakens the epiphysial plate. The increase in growth velocity after stopping the treatment subsequently results in a reduction of the shearing force needed for displacement of the epiphysis.
No interaction studies have been performed.
No known interactions.
Since androgen deprivation treatment may prolong the QT interval, the concomitant use of PROSTAP 3 with medicinal products known to prolong the QT interval or associated with Torsade de pointes such as class IA (e.g. quinidine, disopyramide) or class III (e.g. amiodarone, sotalol, dofetilide, ibutilide) antiarrhythmic medicinal products, methadone, moxifloxacin, antipsychotics, etc. should be carefully evaluated (see section 4.4).
Safe use of leuprorelin acetate in pregnancy has not been established clinically.
Studies in animals have shown reproductive toxicity (see section 5.3). Before starting treatment with PROSTAP 3, pregnancy must be excluded. There have been reports of foetal malformation when PROSTAP 3 has been given during pregnancy.
PROSTAP 3 must not be used in women who are pregnant or breastfeeding (see section 4.3).
When used 3-monthly at the recommended dose, PROSTAP 3 usually inhibits ovulation and stops menstruation. Contraception is not ensured, however, by taking PROSTAP 3 and therefore patients should use non-hormonal methods of contraception during treatment and after cessation of treatment until the return of menses.
Patients should be advised that if they miss successive doses of PROSTAP 3, breakthrough bleeding or ovulation may occur with the potential for conception. Patients should be advised to see their physician if they believe they may be pregnant. If a patient becomes pregnant during treatment, the drug must be discontinued. The patient must be apprised of this evidence and the potential for an unknown risk to the foetus.
See section 4.3 Contraindications.
PROSTAP 3 can influence the ability to drive and use machines due to visual disturbances and dizziness.
Adverse reactions seen with PROSTAP 3 are due mainly to the specific pharmacological action, namely increases and decreases in certain hormone levels.
The following tables list adverse reactions with leuprorelin based on experience from clinical trials as well as from post-marketing experience. Adverse reactions are grouped by MedDRA System Organ Classes and frequency classification. Frequencies are defined as: very common (≥1/10); common (≥1/100 to <1/10); uncommon (≥1/1,000 to <1/100); rare (≥1/10,000 to <1/1,000); very rare (<1/10,000); not known (cannot be estimated from the available data).
In cases where a “tumour flare” occurs after PROSTAP 3 therapy, an exacerbation may occur in any symptoms or signs due to disease. Adverse events, which may occur particularly at the beginning of treatment include urinary tract obstruction (as urinary symptoms). In patients with spinal cord compression, bone pain, weakness of the lower extremities and paraesthesia (as neurologic symptom) may also occur (see section 4.4). These symptoms subside on continuation of therapy.
Tabulated list of adverse reactions in Men:
SOC | Very common | Common | Uncommon | Rare | Very rare | Not known |
---|---|---|---|---|---|---|
Blood and lymphatic system disorders | anaemia (reported in medicinal products of this class), thrombocytopaenia, leucopenia | |||||
Immune system disorders | hypersensitivity reactions (including rash, pruritus, urticaria, wheezing, fever, chills and anaphylactic reactions) | |||||
Metabolism and nutrition disorders | weight fluctuation | decreased appetite | Metabolic syndrome (including hypertension, dyslipidaemia, insulin resistance, abnormal glucose tolerance) | |||
Psychiatric disorders | insomnia, depression (see Section 4.4), mood changes (long-term use**) | mood changes (short term use**) | ||||
Nervous system disorders | headache (occasionally severe) | dizziness, paraesthesia | pituitary apoplexy has been reported following initial administration in patients with pituitary adenoma, pituitary haemorrhage | paralysis (see Section 4.4), seizure, idiopathic intracranial hypertension (pseudotumor cerebri) (see section 4.4) | ||
Eye disorders | visual impairment | |||||
Cardiac disorders | palpitations, QT prolongation (see Sections 4.4 and 4.5) | |||||
Vascular disorders | hot flush | pulmonary embolism, hypertension, hypotension (see Sections 4.4 and 4.5) | ||||
Gastrointestinal disorders | nausea | diarrhoea, vomiting | ||||
Hepatobiliary disorders | hepatic function abnormal, hepatic function test abnormal (usually transient) | jaundice | ||||
Skin and subcutaneous tissue disorders | hyperhydrosis | |||||
Musculoskeletal, connective tissue and bone disorders | muscle weakness, bone pain | arthralgia | myalgia, weakness of lower extremities | spinal fracture, reduction in bone mineral density, osteoporosis (including spinal fracture, see Section 4.4) | ||
Respiratory, thoracic and mediastinal disorders | Interstitial lung disease | |||||
Renal and urinary disorders | urinary tract obstruction | |||||
Reproductive system and breast disorders | Libido decreased, erectile dysfunction, testicular atrophy | gynaecomastia | ||||
General disorders and administration site conditions | Fatigue, injection site reaction, e.g., induration, erythema, pain, abscesses, swelling, nodules, ulcers and necrosis | oedema peripheral | pyrexia |
** mood changes (long term use: frequency of ‘common’ and short term use: frequency of ‘uncommon’)
Those adverse events occurring most frequently with PROSTAP 3 are associated with hypo-estrogenism; the most frequently reported are hot flushes, mood swings including depression (occasionally severe), and vaginal dryness. Estrogen levels return to normal after treatment is discontinued.
The induced hypo-estrogenic state results in a loss in bone density over the course of treatment, some of which may not be reversible (see Section 4.4).
Vaginal haemorrhage may occur during therapy due to acute degeneration of submucous fibroids (see Section 4.4).
Tabulated list of adverse reactions in Women:
SOC | Very common | Common | Uncommon | Rare | Very rare | Not known |
---|---|---|---|---|---|---|
Blood and lymphatic system disorders | Anaemia (reported in medicinal products of this class), thrombocytopaenia, leucopenia | |||||
Immune system disorders | hypersensitivity reactions (including rash, pruritus, urticaria, wheezing, fever, chills and anaphylactic reactions) | |||||
Metabolism and nutrition disorders | weight fluctuation | decreased appetite, lipids abnormal | Metabolic syndrome (including hypertension, dyslipidaemia, insulin resistance, abnormal glucose tolerance) | |||
Psychiatric disorders | insomnia | depression (see Section 4.4), mood changes (long-term use**) | mood changes (short term use**) | |||
Nervous system disorders | headache (occasionally severe) | paraesthesia, dizziness | pituitary apoplexy has been reported following initial administration in patients with pituitary adenoma, pituitary haemorrhage | paralysis (see Section 4.4), seizure, idiopathic intracranial hypertension (pseudotumor cerebri) (see section 4.4) | ||
Eye disorders | visual impairment | |||||
Cardiac disorders | palpitations | |||||
Vascular disorders | hot flush | pulmonary embolism, hypertension, hypotension (see Section 4.4) | ||||
Gastrointestinal disorders | nausea | diarrhoea, vomiting | ||||
Hepatobiliary disorders | hepatic function test abnormal (usually transient) | hepatic function abnormal (including jaundice) | ||||
Skin and subcutaneous tissue disorders | hyperhidrosis | hair loss | ||||
Musculoskeletal, connective tissue and bone disorders | bone pain | arthralgia, muscle weakness | myalgia | reduction in bone mineral density, osteoporosis (including spinal fracture, see Section 4.4) | ||
Respiratory, thoracic and mediastinal disorders | Interstitial lung disease | |||||
Reproductive system and breast disorders | breast tenderness , breast atrophy, vulvovaginal dryness | vulvovaginitis, libido decreased, vaginal haemorrhage | ||||
General disorders and administration site conditions | Oedema peripheral, injection site reaction e.g.injection site induration, erythema, pain, abscesses, swelling, nodules, ulcers and necrosis | pyrexia, fatigue |
** mood changes (long term use: frequency of ‘common’ and short term use: frequency of ‘uncommon’)
In women with early breast cancer treated with a GnRH agonist, in combination with tamoxifen or an aromatase inhibitor, the following side effects have been seen:
Very common: Nausea, fatigue, musculoskeletal disorders, osteoporosis, hot flushes, hyperhidrosis, insomnia, depression, libido decreased, vulvovaginal dryness, dyspareunia, urinary incontinence, hypertension.
Common: Diabetes mellitus, hyperglycaemia, injection site reaction, hypersensitivity fracture, embolism.
Uncommon: myocardial ischaemia, cerebral ischaemia, central nervous system haemorrhage.
Rare: QT prolongation
In the initial phase of therapy, a short-term increase as flare-up of the sex hormone level occurs, followed by a decrease to values within the pre-pubertal range. Due to this pharmacological effect, adverse events may occur particularly at the beginning of treatment.
Tabulated list of adverse reactions in Children:
SOC | Very common | Common | Uncommon | Rare | Very rare | Not known |
---|---|---|---|---|---|---|
Immune system disorders | Hypersensitivity (rash, pruritus, urticaria, wheezing, fever, chills and anaphylactic reactions) | |||||
Psychiatric disorders | depression (see Section 4.4), emotional lability | |||||
Nervous system disorders | headache | pituitary apoplexy has been reported following initial administration in patients with pituitary adenoma, pituitary haemorrhage | seizure | |||
Gastrointestinal disorders | abdominal pain / abdominal cramps, nausea/vomiting | |||||
Skin and subcutaneous tissue disorders | acne | |||||
Respiratory, thoracic and mediastinal disorders | Interstitial lung disease | |||||
Reproductive system and breast disorders | vaginal haemorrhage, spotting**, vaginal discharge | |||||
General disorders and administration site conditions | injection site reactions (e.g. induration, erythema, pain, abscess, swelling, nodules and necrosis) |
** In general, the occurrence of vaginal spotting with continued treatment (subsequent to possible withdrawal bleeding in the first month of treatment) should be assessed as a sign of potential underdosage. The pituitary suppression should then be determined by gonadotropin releasing hormone (GnRH) stimulating test.
Reporting suspected adverse reactions after authorisation of the medicinal product is important. It allows continued monitoring of the benefit/risk balance of the medicinal product. Healthcare professionals are asked to report any suspected adverse reactions via the Yellow Card Scheme. Website: www.mhra.gov.uk/yellowcard or search for MHRA Yellow Card in the Google Play or Apple App Store.
This drug must be injected alone.
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