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Alendrostad

Document: Alendrostad 10 mg tablet SmPC change

Produktinformationen för Alendrostad 10 mg tablett, MTnr 21347, gäller vid det tillfälle då läkemedlet godkändes. Informationen kommer inte att uppdateras eftersom läkemedlet inte marknadsförs i Sverige. Av samma anledning finns inte någon svensk produktinformation.

Den engelska produktinformationen kommer dock att uppdateras när Sverige är referensland för produkten.

Om läkemedelsnamnet i följande produktinformation inte stämmer med namnet på dokumentet, beror det på att läkemedlet i Sverige är godkänt under ett annat namn.


Summary of Product Characteristics


Name of the Medicinal Product


Alendrostad 10 mg tablets


Qualitative and Quantitative Composition


Each tablet contains 10mg alendronic acid (as sodium alendronate trihydrate).


Excipients: each tablet contains 103.95 mg lactose monohydrate


For a full list of excipients, see section 6.1.


Pharmaceutical Form


Tablet


White to off-white, capsule-shaped tablet, embossed "AN 10" on one side and "Arrow logo" on the other.


Clinical Particulars


Therapeutic indications


Treatment of post-menopausal osteoporosis.

Alendronate reduces the risk of vertebral and hip fractures.


Treatment of osteoporosis in men at increased risk of fracture. A reduction in the incidence of vertebral, but not of non-vertebral fractures has been demonstrated.


Prophylaxis of glucocorticoid-induced osteoporosis

(see section 5.1).


Posology and method of administration


For oral use only.


Post-menopausal osteoporosis:

The recommended dosage is 10 mg once daily.


Osteoporosis in men at increased risk of fracture:

The recommended dosage is 10 mg once daily.


Glucocorticoid-induced osteoporosis:

For post-menopausal women who are not receiving oestrogen treatment the recommended dose is one 10 mg tablet daily. For other populations, see summary of product characteristics for preparations that contain 5 mg alendronate.


To obtain satisfactory absorption of alendronate

Alendrostad tablets must be taken on an empty stomach immediately on rising in the morning,with plain water only, at least 30 minutes before the first food, drink or other medication of the day. Other drinks (including mineral water), food and some medicines are likely to reduce the absorption of alendronate (see section 4.5).


To assist delivery to the stomach and thus reduce the risk of irritation/side effects locally and in the oesophagus (see section 4.4)


Patients should be given a calcium and vitamin D supplement if the diet is inadequate (see section 4.4).


Use in elderly patients:

In clinical trials there was no age-related difference with regard to efficacy or safety profiles of alendronate. Therefore no adjustment of the dose is necessary for elderly patients.


Use in impaired renal function

No dose adjustment is necessary in patients with a glomerular filtration rate (GFR) greater than 35 ml/min. Alendronate is not recommended for patients with impaired renal function if the GFR is less than 35 ml/min, as there is no experience of this.


Use in impaired hepatic function

No dose adjustment is necessary.


Use in children (under 18 years)

Alendronate has been studied in a small number of patients with osteogenesis imperfecta under 18 years of age. Results are insufficient to support its use in children.


Contraindications



See also section 4.4.


Special warnings and precautions for use


Alendronate can cause local irritation to the upper gastrointestinal mucosa. As there is a risk of worsening of the underlying disease, caution should be observed if alendronate is given to patients with active upper gastrointestinal tract problems, such as dysphagia, oesophageal disease, gastritis, duodenitis or ulcers, or in cases of recent (during the last year) severe gastrointestinal disease such as gastric ulcer, active gastrointestinal bleeding or surgery in the upper gastrointestinal tract other than pyloroplasty (see section 4.3).


Oesophageal side effects (in some cases severe and requiring hospitalisation) such as oesophagitis, oesophageal ulcers or oesophageal erosions, in rare cases followed by oesophageal stricture, have been reported in patients receiving treatment with alendronate. The physician should therefore be alert to any signs or symptoms of possible oesophageal reaction. The patients should be instructed to discontinue alendronate and seek medical attention if they develop symptoms of oesophageal irritation such as dysphagia, pain on swallowing, retrosternal pain or new/worsened heartburn.


The risk of severe oesophageal side effects is thought to be greater in patients who do not take alendronate correctly and/or continue to take alendronate after developing symptoms indicative of oesophageal irritation. It is very important that complete administration instructions are given to, and understood, by the patient (see section 4.2). Patients should be informed that the risk of oesophageal problems may increase if they do not follow these instructions.


Despite no increased risk having been observed in extensive clinical trials, following marketing of the original preparation there have been reports of rare cases of gastric and duodenal ulcers, some of them severe and with complications. A causal relationship cannot be excluded (see section 4.8).


Alendronate is not recommended for patients with impaired renal function if the GFR is less than 35 ml/min (see section 4.2).


Causes of osteoporosis other than oestrogen deficiency, ageing and glucocorticoid use should be considered.


Hypocalcaemia must be corrected before treatment with alendronate is initiated (see section 4.3). Other disorders of mineral metabolism (such as vitamin D deficiency and hypoparathyroidism) should also be effectively treated before starting alendronate. In patients with these conditions, serum calcium and symptoms of hypocalcaemia should be monitored during treatment with alendronate.


On account of the positive effects of alendronate on the increase in bone mineralisation, reductions in serum calcium and serum phosphate may occur. These are usually slight and asymptomatic. However, in rare cases, symptomatic hypocalcaemia has been reported which occasionally has been severe and often occurred in patients with predisposing conditions (e.g. hypoparathyroidism, vitamin D deficiency and in cases of calcium malabsorption).

It is therefore particularly important to ensure that patients taking glucocorticoids have an adequate calcium and vitamin D intake.


Osteonecrosis of the jaw, generally associated with tooth extraction and/or local infection (including osteomyelitis) has been reported in patients with cancer receiving treatment regimens including primarily intravenously administered bisphosphonates. Many of these patients were also receiving chemotherapy and corticosteroids. Osteonecrosis of the jaw has also been reported in patients with osteoporosis receiving oral bisphosphonates.

A dental examination with appropriate preventive dentistry should be considered prior to treatment with bisphosphonates in patients with concomitant risk factors (e.g. cancer, chemotherapy, radiotherapy, corticosteroids, poor oral hygiene, periodontal disease, smoking).

While on treatment, these patients should avoid invasive dental procedures if possible. For patients who develop osteonecrosis of the jaw while on bisphosphonate therapy, dental surgery may exacerbate the condition. For patients requiring dental procedures, there are no data available to suggest whether discontinuation of bisphosphonate treatment reduces the risk of osteonecrosis of the jaw.

Clinical judgement of the treating physician should guide the management plan of each patient based on individual benefit/risk assessment.


Bone, joint, and/or muscle pain has been reported in patients taking bisphosphonates. In postmarketing experience, these symptoms have rarely been severe and/or incapacitating (see section 4.8).

The time to onset of symptoms varied from one day to several months after starting treatment. Most patients had relief of symptoms after stopping. A subset had recurrence of symptoms when rechallenged with the same drug or another bisphosphonate.


Atypical stress fractures

Stress fractures (also known as insufficiency fractures) of the proximal femoral shaft have been reported in patients treated long-term with alendronic acid (time to onset ranged in the majority of cases from 18 months to 10 years). The fractures occurred after minimal or no trauma and some patients experienced thigh pain, often associated with imaging features of stress fractures, weeks to months before presenting with a completed femoral fracture. Fractures were often bilateral; therefore the contralateral femur should be examined in bisphosphonate-treated patients who have sustained a femoral shaft fracture. Poor healing of these fractures was also reported. Discontinuation of bisphosphonate therapy in patients with stress fracture is advisable pending evaluation of the patient, based on an individual benefit risk assessment.


Alendrostad 10 mg tablets contain lactose. Patients with rare hereditary problems of galactose intolerance, the Lapp lactase deficiency or glucose-galactose malabsorption should not take this medicine.


Interactions with other medicinal products and other forms of interaction


If taken at the same time, it is likely that foods and drinks (including mineral water), calcium supplements, antacids and some oral medicines will affect the absorption of alendronate. Patients must therefore wait for at least 30 minutes after taking alendronate before taking any other oral medicine (see section 4.2).


Since NSAID use is associated with gastrointestinal irritation, caution should be used during concomitant use with alendronate.


No other clinically significant drug interactions are expected. A number of patients in the clinical trials received oestrogen (intravaginally, transdermally or orally) concomitantly with alendronate. No undesirable effects could be related to the combination treatment.


No specific interaction studies have been carried out, but alendronate was used in clinical trials concomitantly with a number of other commonly prescribed medicines without any evidence of clinically unfavourable interactions.


Pregnancy and lactation


Use during pregnancy

Alendronate should not be used during pregnancy. There are no adequate data from the use of alendronate in pregnant women. Animal studies do not indicate direct harmful effects with respect to pregnancy, embryonal/fetal development, or postnatal development. Alendronate given during pregnancy in rats caused dystocia related to hypocalcemia (see 5.3 ‘Preclinical safety data’).


Use during lactation

It is not known whether alendronate is excreted into human breast milk. Alendronate should not be used by breast-feeding women.


Effects on ability to drive and use machines


No studies on the effects on the ability to drive and use machines have been performed. However, certain adverse reactions that have been reported with Alendronat STADA 10mg tablets may affect some patients' ability to drive or operate machinery. Individual responses to Alendronat STADA 10mg tablets may vary (see section 4.8)


Undesirable effects


In two three-year studies of almost identical design, with post-menopausal women (alendronate 10 mg: n=196; placebo: n= 397) the overall safety profiles for alendronate 10 mg daily and placebo were similar.


Undesirable effects reported by the investigators as possibly, probably or definitely related to the drug are presented below if they occurred in 1 % of any in the treatment groups in the one-year study or in 1 % of the patients who were treated with alendronate 10 mg per day and with an incidence higher than in patients who were treated with placebo in three-year studies.



Three-year studies

Alendronate10 mg daily

(n=196)

%

Placebo

(n=397)

%

Gastrointestinal

Abdominal pain

6.6

4.8

Dyspepsia

3.6

3.5

Acid regurgitation

2.0

4.3

Nausea

3.6

4.0

Abdominal distension

1.0

0.8

Constipation

3.1

1.8

Diarrhoea

3.1

1.8

Dysphagia

1.0

0.0

Flatulence

2.6

0.5

Gastritis

0.5

1.3

Gastric ulcer

0.0

0.0

Oesophageal ulcer

1.5

0.0

Musculoskeletal



Musculoskeletal pain

(bone, muscle or joints)

4.1

2.5

Muscle cramps

0.0

1.0

Neurological



Headache

2.6

1.5


The following undesirable effects have also been reported in clinical trials and/or post marketing:


In this section frequencies of undesirable effects are defined as follows: 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).


Immune system disorders:

Rare:Hypersensitivity reactions including urticaria and angioedema.


Metabolism and nutrition disorders:

Rare:Symptomatic hypocalcaemia, generally in connection with predisposing conditions (see. section 4.4).


Nervous system disorders:

Common:Headache

Not known:dizziness, dysgeusia


Ear and labyrinth disorders:

Not known: vertigo


Eye disorders:

Rare:Uveitis, scleritis, episcleritis


Gastrointestinal disorders:

Common: Abdominal pain, dyspepsia, constipation, diarrhoea, flatulence, oesophageal ulcers*, dysphagia*, abdominal distension, acid regurgitation.

Uncommon:Nausea, vomiting, gastritis, oesophagitis* oesophageal erosions*, melaena.

Rare:Oesophageal stricture*, oropharyngeal ulceration*, upper gastrointestinal PUB (perforations, ulcers, bleeding), a causal relationship cannot be ruled out.


Skin and subcutaneous tissue disorders:

Uncommon:Rash, pruritus, erythema,.

Rare:Skin rash with photosensitivity.


Very rare:Isolated cases of severe skin reactions including Stevens-Johnson syndrome and toxic epidermal necrolysis have been reported.

Not known: alopecia


Musculoskeletal, connective tissue and bone disorders:

Common:Musculoskeletal pain (bones, muscles or joints)

Rare: Osteonecrosis

Osteonecrosis of the jaw has been reported in patients treated by bisphosphonates. The majority of the reports refer to cancer patients, but such cases have also been reported in patients treated for osteoporosis. Osteonecrosis of the jaw is generally associated with tooth extraction and/or local infection (including osteomyelitis). Diagnosis of cancer, chemotherapy, radiotherapy, corticosteroids, and poor oral hygiene are also deemed as risk factors; severe musculoskeletal (bone, muscle or joint) pain (see 4.4 ‘Special warnings and precautions for use’).

Not known: joint swelling, stress fractures of the proximal femoral shaft (see section 4.4).


General disorders and administration site conditions:

Rare:. Transient symptoms as in an acute phase reaction (myalgia, malaise and in rare cases fever) usually in connection with the start of treatment. Not known:Asthenia, peripheral edema.


*See sections 4.4 and 4.2.


Laboratory values:In clinical trials, asymptomatic, slight and transient decreases in serum calcium and serum phosphate were observed in approx. 18 and 10 % respectively of the patients taking alendronate 10 mg/day versus 12 and 3 % respectively of those taking placebo. However, the incidence of reductions in serum calcium to <2.0 mmol/l and serum phosphate to 0.65 mmol/l was comparable in the two groups.


Overdose


Hypocalcaemia, hypophosphataemia and upper gastrointestinal side effects such as upset stomach, heartburn, oesophagitis, gastritis or ulcer can occur on oral overdosage. There is no specific information available with regard to overdosage with alendronate. Milk or antacids should be given in order to bind alendronate. On account of the risk of oesophageal irritation, vomiting should not be induced and the patient should be kept in an upright position.


Pharmacological Properties


Pharmacodynamic properties


Pharmacotherapeutic group: Drugs for treatment of bone diseases, bisphosphonates.

ATC code: M05BA04


The active substance in Alendrostad 10 mg tablets, sodium alendronate trihydrate, is a bisphosphonate that inhibits osteoclastic bone resorption without any direct effect on bone formation. Preclinical studies have demonstrated a preference for localisation of alendronate to sites where active resorption takes place. Osteoclastic activity is inhibited, but formation and binding of the osteoclasts is not affected. Bone formed during treatment with alendronate is of normal quality.


Treatment of post-menopausal osteoporosis


Osteoporosis is defined as bone mineral density (BMD) of the spine or hip 2.5 standard deviations below the mean value of a normal young population or as a previous fragility fracture, irrespective of bone mineral density.


The effects of alendronate on BMD and fracture incidence in post-menopausal women were studied in two initial efficacy studies of identical design (n=994), and in the Fracture Intervention Trial(FIT: n=6459).

In the initial efficacy studies, the increases in BMD with alendronate 10 mg daily relative to placebo after three years were 8.8 %, 5.9 % and 7.8 % at the spine, femoral neck and trochanter respectively. Total BMD also increased significantly. In the patients treated with alendronate, the proportion of patients who suffered one or more vertebral fractures was reduced by 48 % (alendronate 3.2 % versus placebo 6.2 %). In the two-year extensions of these studies the BMD in the spine and trochanter continued to increase. In addition, BMD at the femoral neck and total body was maintained.


The FIT study included two placebo-controlled trials in which alendronate was given daily (5 mg daily for two years and 10 mg daily for a further one or two years).


Osteoporosis in men with increased risk of fracture

The efficacy of alendronate 10 mg once daily in men (31-87 years, mean age 63 years, n=241) with osteoporosis was evaluated in a two-year study. After two years of treatment with alendronate 10 mg/day, BMD increased on average by 5.3 % in the spine, by 2.6 % in the femoral neck, by 3.1 % in the trochanter, and by 1.6 % for the skeleton as a whole, relative to placebo (p<0.001 for all measurement points). The effect of alendronate on BMD was independent of age, race, gonadal function, baseline BMD or baseline bone turnover. The incidence of new vertebral fractures was evaluated as a safety variable. In a retrospective analysis (assessed by quantitative radiography) one new fracture (0.8 %) was documented among patients treated with alendronate, compared with 6 new fractures (7.1 %) for placebo (p=0.017). The reduction in height was less after treatment with alendronate, relative to placebo (-0.6 mm and 2.4 mm respectively, p=0.02). No effect on non-vertebral fractures was seen.


Glucocorticoid-induced osteoporosis

Long-term use of steroids is often associated with the development of osteoporosis accompanied by fractures. This occurs in both men and women of all ages. The efficacy of alendronate 10 mg and alendronate 5 mg once daily in men and women treated with steroids (at least 7.5 mg/day of prednisone or equivalent, median dose 10 mg/day) was demonstrated in two one-year studies of practically identical design. These studies involved a total of 560 patients aged 17-83 years. The patients received calcium and vitamin D supplements. Relative to placebo, BMD increased significantly in the spine (2.41 %), femoral neck (2.19 %) and trochanter (1.65 %) in patients who were treated with alendronate 5 mg once daily. The increases in BMD with alendronate 10 mg once daily were the same as for alendronate 5 mg once daily in all patients, with the exception of post-menopausal women who were not being treated with oestrogen. In these women the increases (relative to placebo) with alendronate 10 mg once daily were greater than for alendronate 5 mg once daily in the spine (4.11 % versus 1.56 %) and trochanter (2.84 % versus 1.67 %). The fracture-preventing effect of increasing bone density with alendronate 10 mg or alendronate 5 mg in corticosteroid-induced osteoporosis has not been established.


Alendronate 10 mg and 5 mg were effective irrespective of the dose or duration of steroid use. In addition, alendronate 10 mg and alendronate 5 mg were effective irrespective of age (<65 years as against 65 years), gender, baseline BMD, baseline bone turnover and concomitant use of a number of common medicines. In the patients who received alendronate in doses up to 10 mg daily and in whom biopsy was performed after one year no signs of a disturbance of the bone mineralisation process were seen.


Pharmacokinetic properties


Absorption

Compared with an intravenous reference dose, the mean oral bioavailability of alendronate in women was 0.64 % for doses ranging from 5 to 70 mg given after an overnight fast and two hours before a standardised breakfast. Bioavailability decreased to an estimated 0.46 % and 0.39 % when alendronate was given an hour or half an hour before a standardised breakfast.

In osteoporosis studies alendronate was effective when it was given at least 30 minutes before the first meal or drink of the day. Bioavailability was negligible irrespective of whether alendronate was given together with or up to two hours after a standardised breakfast. Concomitant administration of alendronate with coffee or orange juice reduced bioavailability by approx. 60 %. In healthy persons, oral prednisolone (20 mg three times daily for five days) did not result in any clinically meaningful change in the oral bioavailability of alendronate (a mean increase ranging from 20 % to 44 %).


Distribution

Studies in rats show that alendronate is initially distributed to soft tissues after intravenous administration of 1 mg/kg, but is then rapidly redistributed to the skeleton or excreted in the urine. The mean steady-state volume of distribution, exclusive of bone, is at least 28 litres in humans. Concentrations of drug in plasma following therapeutic oral doses are too low for analytical detection (<5 ng/ml). Protein binding in human plasma is approximately 78%.


Biotransformation

There is no evidence that alendronate is metabolised in animals or humans.


Elimination

Following a single intravenous dose of (14C) alendronate, approximately 50% of the radioactivity was excreted in the urine within 72 hours and little or no radioactivity was recovered in the faeces. Following a single intravenous dose of 10 mg, the renal clearance of alendronate was 71 ml/min, and systemic clearance did not exceed 200 ml/min. Plasma concentrations fell by more than 95% within 6 hours following intravenous administration. The terminal half-life in humans is estimated to exceed ten years, reflecting release of alendronate from the skeleton. Alendronate is not excreted through the acidic or basic transport systems of the kidney in rats, and thus it is not thought to interfere with the excretion of other drugs by those systems in humans.


Characteristics in patients

Preclinical studies show that the drug that is not deposited in bone is rapidly excreted in the urine. No evidence of saturation of bone uptake was found after chronic dosing with cumulative intravenous doses up to 35 mg/kg in animals. Although no clinical information is available, it is likely that, as in animals, elimination of alendronate via the kidney will be reduced in patients with impaired renal function. Therefore, somewhat greater accumulation of alendronate in bone might be expected in patients with impaired renal function (see section 4.2).


Preclinical safety data


Conventional studies of general toxicity, genotoxicity and carcinogenicity did not reveal any special risks for humans. Studies in female rats showed that treatment with alendronate during pregnancy was associated with dystocia during parturition, which was related to hypocalcaemia. Studies in which rats were given high doses showed an increased incidence of incomplete foetal bone formation. The relevance for humans is unknown.


Pharmaceutical Particulars


List of excipients


Microcrystalline cellulose

Lactose monohydrate

Croscarmellose sodium

Magnesium stearate


Incompatibilities


Not applicable.


Shelf-life


2 years


Special precautions for storage


Do not store above 25°C. Store in the original package in order to protect from moisture.


Nature and contents of container


The tablets are supplied in triplex blister (PVC/PE/PVDC/AL) packaging.

14, 28, 30, 56, 98, 112 and 50 x 1 (unit dose).


Not all pack sizes may be marketed.


Instructions for use and handling, and for destruction


No special requirements.


Marketing Authorisation Holder


To be completed nationally


Marketing Authorisation Number


To be completed nationally


Date of First Authorisation / Renewal of Authorisation


To be completed nationally


Date of first authorisation: 2004-12-03

Date of last renewal: 2009-12-03


Date of Revision of the Text


2010-02-23