Voltaren retard tablets p/o prolonged action 75 mg No. 10x2

Voltaren retard tablets p/o prolonged action 75 mg No. 10x2

Name

Voltaren retard.

Release forms

Pills.

INN

Diclofenac

FTG

Npvp.

Compound

active ingredient: diclofenac sodium; Each tablet contains diclofenac sodium 75 mg; excipients: tablet core - magnesium stearate, anhydrous colloidal silicon dioxide, povidone, cetyl alcohol, sucrose; tablet coating - hypromellose, red iron oxide (E 172), polysorbate 80, talc, titanium dioxide (E 171), macrogol 8000, sucrose, black ink (shellac, isopropyl alcohol, black iron oxide E172, butyl alcohol, propylene glycol, ammonium hydroxide ).

Pharmacotherapeutic group

Nonsteroidal anti-inflammatory and antirheumatic drugs. Derivatives of acetic acid. ATS code M01A B05. Clinical characteristics

Indications for use

Inflammatory and degenerative rheumatic diseases: rheumatoid arthritis, ankylosing spondylitis; arthrosis; extra-articular rheumatism. Pain and inflammation of non-rheumatic or post-traumatic origin. Symptomatic treatment of primary dysmenorrhea.

Contraindications

Known hypersensitivity to the active substance or other components of the drug, to other analgesics, antipyretics, non-steroidal anti-inflammatory drugs (NSAIDs) and, in particular, to acetylsalicylic acid; Active stomach or intestinal ulcer, bleeding or perforation. Inflammatory bowel diseases (such as Crohn's disease or ulcerative colitis); Last trimester of pregnancy; Liver failure; Renal failure (GFR

Directions for use and doses

The tablets should be taken whole, without chewing or breaking, with liquid, preferably with meals. The dose should be selected individually. Side effects can be minimized by using the lowest effective dose for the minimum period necessary to control symptoms (see Precautions). The recommended initial dose of the drug for adults is 75 - 150 mg per day (1-2 tablets of Voltaren Retard 75 mg), depending on the severity of the symptoms of the disease. For long-term therapy, as a rule, the use of 1 tablet of Voltaren Retard 75 mg per day is sufficient. If the symptoms of the disease are most pronounced at night or in the morning, Voltaren Retard should be taken in the evening. Use in special groups of patients. Children (under 18 years of age) Voltaren retard tablets, film-coated, prolonged action 75 mg are not recommended for use in children due to the high content of the active substance. Elderly patients (65 years and older). For elderly patients, no adjustment of the starting dose is usually required. However, based on generally accepted approaches, caution is required when prescribing the drug, especially in weakened or low-weight elderly patients. Patients with congestive heart failure (NYHA-I) or significant cardiovascular risk factors In patients with congestive heart failure (NYHA-I) or uncontrolled hypertension, therapy with Voltaren is generally not recommended. If necessary, the drug is prescribed to patients with cardiovascular diseases or with significant risk factors for their development only after a thorough assessment, and for a duration of therapy of more than 4 weeks - only in doses

Side effects

Adverse reactions to the drug, depending on the frequency, are described in the following order: very often (> 1/10); often (> 1/100, 1/1000, 1/10000,

Overdose

There is no typical clinical picture of diclofenac overdose. Symptoms of a diclofenac overdose may include vomiting, gastrointestinal bleeding, diarrhea, dizziness, tinnitus, and convulsions. In case of significant poisoning, acute renal failure and liver damage are possible. Treatment of acute NSAID poisoning consists of the use of supportive and symptomatic therapy. Supportive and symptomatic treatment is indicated for complications such as hypotension, renal failure, seizures, gastrointestinal disorders and respiratory depression. It is unlikely that specific therapeutic measures such as forced diuresis, dialysis or hemoperfusion will be useful for the elimination of NSAIDs, since the active substances of these drugs are largely bound to blood proteins and undergo intensive metabolism. Activated charcoal may be used after a potentially toxic overdose, as well as gastric decontamination (eg, vomiting, gastric lavage) after a potentially life-threatening overdose. Women of childbearing age, pregnancy, breastfeeding, fertility There are no data to support any recommendations for women of childbearing age. Suppression of prostaglandin synthesis can adversely affect the course of pregnancy and intrauterine development of the fetus. Epidemiological studies suggest an increased risk of miscarriage and/or fetal heart defects and gastroschisis after taking prostaglandin synthesis inhibitors in early pregnancy, but aggregated data are inconclusive. The absolute risk of cardiovascular defects increased from less than 1% to 1.5%. The risk is believed to increase with increasing dose and duration of therapy. It has been shown that in animals, the administration of prostaglandin synthesis inhibitors leads to disruption of embryo implantation. In addition, in animals receiving a prostaglandin synthesis inhibitor during the period of organogenesis, the incidence of various malformations, including developmental disorders of the cardiovascular system, increased. The use of diclofenac in pregnant women has not been studied. Therefore, Voltaren Retard should not be prescribed during the first two trimesters of pregnancy, unless the benefits of its use outweigh the risks to the fetus. As with other NSAIDs, use of the drug during the third trimester of pregnancy is contraindicated. When taking prostaglandin synthesis inhibitors in the third trimester of pregnancy, the fetus may experience: premature closure of the ductus arteriosus and pulmonary hypertension, renal dysfunction, with the progression of which renal failure with oligohydroamnion develops. When taking diclofenac at the end of pregnancy, labor weakness may develop and the duration of labor may increase. In the mother and in the fetus/newborn, bleeding time may be prolonged; the antiplatelet effect may occur even after taking very low doses of diclofenac. Thus, diclofenac is contraindicated in the third trimester of pregnancy. Like other NSAIDs, diclofenac is excreted in small quantities into breast milk. Thus, Voltaren Retard should not be used during breastfeeding in order to prevent unwanted reactions in the child. Like other NSAIDs, Voltaren Retard can adversely affect female fertility, so it is not recommended to prescribe the drug to women planning a pregnancy. In women who have difficulty conceiving or are undergoing examination for infertility, the advisability of discontinuing the drug should be considered.

Children

Voltaren Retard is not recommended for the treatment of children aged 14-18 years due to the high content of the active substance in the tablet. The drug is contraindicated in children under 14 years of age. Precautions Gastrointestinal effects With all NSAIDs, gastrointestinal bleeding, ulceration and perforation are possible, which can be fatal and occur during treatment with or without a history of warning symptoms or serious gastrointestinal disorders. In general, such phenomena are most dangerous for elderly patients. In isolated cases, when patients taking Voltaren Retard develop these complications, treatment with this drug should be discontinued. While taking the drug Voltaren Retard, medical supervision is necessary for patients who have diseases of the gastrointestinal tract or a history of gastric or intestinal ulcers, ulcerative colitis or Crohn's disease. The risk of gastrointestinal bleeding increases with increasing doses of NSAIDs and in patients with a history of ulcers, especially if the ulcer was complicated by bleeding or perforation or occurred in the elderly. To reduce the risk of toxic effects on the gastrointestinal tract in patients with a history of peptic ulcer, in particular, complicated by bleeding and perforation, as well as in elderly patients, treatment should be started with the lowest effective dose and maintained thereafter. In the above patients and patients requiring concomitant use of low doses of acetylsalicylic acid or other drugs that may increase the risk of developing adverse reactions from the gastrointestinal tract, combination therapy in combination with protective drugs (for example, proton pump inhibitors or misoprostol) should be considered. . Caution is advised in patients receiving concomitant therapy with systemic corticosteroids, anticoagulants, antiplatelet agents, or selective serotonin reuptake inhibitors. Cardiovascular Effects: Clinical studies and epidemiological data strongly suggest an increased risk of arterial thrombotic events (eg, myocardial infarction or stroke) that may be associated with the use of diclofenac, particularly when used in high doses (150 mg daily) and with long-term use. In patients with significant risk factors for cardiovascular complications (eg, hypertension, hyperlipidemia, diabetes mellitus, smoking), diclofenac should be prescribed only after careful consideration of this possibility. Due to the possible increased risk of cardiovascular events with long-term use or high doses of the drug, patients should be prescribed diclofenac at the minimum effective dose and take it for the shortest time necessary to reduce the severity of symptoms. The need for symptom relief and response to treatment should be periodically re-evaluated. In patients with congestive heart failure (NYHA-I) or significant risk factors for cardiovascular events (eg, hypertension, hyperlipidemia, diabetes mellitus, smoking), diclofenac should be used only after careful evaluation, and if the duration of therapy is more than 4 weeks - only in doses

Impact on the ability to drive vehicles and operate machinery

Patients who experience dizziness or other unpleasant sensations from the central nervous system, including visual disturbances, while taking Voltaren Retard, are not recommended to drive a car or operate machinery.

Interaction with other drugs

Caution is recommended when co-administering Voltaren Retard with CYP2C9 inhibitors (such as voriconazole), which may lead to a significant increase in peak plasma concentrations and exposure of diclofenac. Voltaren Retard may increase plasma concentrations of lithium and digoxin. It is recommended to monitor serum lithium and digoxin levels. Voltaren Retard, like other NSAIDs, may inhibit the activity of diuretics or antihypertensive drugs (for example, beta blockers, angiotensin-converting enzyme (ACE) inhibitors). Therefore, the combination should be used with caution and the blood pressure of patients, especially the elderly, should be monitored periodically. Patients should receive adequate fluid intake, and monitoring of renal function is recommended upon initiation of concomitant therapy and on a regular basis thereafter, especially when using diuretics and ACE inhibitors due to the increased risk of nephrotoxicity. Concomitant use of potassium-sparing diuretics, cyclosporine, tacrolimus or trimethoprim may lead to an increase in serum potassium levels (this indicator should be regularly monitored). Concomitant use with other systemic NSAIDs or corticosteroids may increase the incidence of adverse reactions of Voltaren Retard from the gastrointestinal tract. Concomitant use of systemic NSAIDs and SSRIs may increase the risk of bleeding in the digestive tract. Although clinical studies have not established the effect of Voltaren Retard on the action of anticoagulants, there are isolated reports of an increased risk of bleeding in patients taking Voltaren Retard and anticoagulants simultaneously. Therefore, close monitoring of such patients is recommended. Clinical studies have shown that Voltaren Retard can be used in conjunction with oral antidiabetic agents and does not change their therapeutic effect. However, there are isolated reports of the development in such cases of both hypoglycemia and hyperglycemia, which led to changes in the dose of glucose-lowering drugs during the use of Voltaren Retard. For this reason, monitoring of blood glucose levels is recommended as a precaution during concomitant therapy. Caution should be exercised when prescribing NSAIDs less than 24 hours before or after taking methotrexate, as in such cases the concentration of methotrexate in the blood may increase and its toxic effect may increase. The effect of NSAIDs, including Voltaren Retard, on the synthesis of prostaglandins in the kidneys may enhance the nephrotoxicity of cyclosporine. In this regard, Voltaren Retard should be used in lower doses than in patients who do not receive cyclosporine. When using phenytoin together with Voltaren Retard, it is recommended to monitor the concentration of phenytoin in the blood plasma due to a possible increase in phenytoin exposure. Colestipol and cholestyramine may delay or reduce the absorption of diclofenac. It is recommended to take diclofenac at least one hour before or 4-6 hours after colestipol/cholestyramine. There are isolated reports of the development of seizures in patients receiving concomitant quinolone derivatives and NSAIDs.

Pharmacological properties

Pharmacodynamics. Diclofenac, the active substance of Voltaren Retard, is a non-steroidal compound with pronounced antirheumatic, anti-inflammatory, analgesic and antipyretic effects. The main mechanism of action of diclofenac, established under experimental conditions, is considered to be inhibition of prostaglandin biosynthesis. Prostaglandins play an important role in the genesis of inflammation, pain and fever. In vitro, diclofenac sodium in concentrations equivalent to those achieved in the treatment of patients does not suppress the biosynthesis of proteoglycans in cartilage tissue. Voltaren Retard is suitable for patients in whom a daily dose of 75 mg is appropriate, taking into account the clinical picture. The ability to prescribe a drug that allows for a single dose of the entire daily dose greatly simplifies long-term treatment and helps avoid possible dosage errors. Voltaren Retard allows the use of a maximum daily dose of 150 mg in a balanced regimen twice a day. In rheumatic diseases, the anti-inflammatory and analgesic properties of Voltaren Retard provide a significant reduction in the severity of pain (both at rest and during movement), morning stiffness, swelling of the joints and, thus, improving the functional state of the patient. In the presence of inflammation caused by injury or surgery, Voltaren Retard quickly eliminates both spontaneous pain and pain during movement, and also reduces inflammatory tissue swelling and swelling at the site of the surgical wound. In clinical studies, it was found that Voltaren Retard also exhibits a strong analgesic effect in moderate and severe pain of non-rheumatic origin. Pharmacokinetics. Analysis of unchanged diclofenac and its hydroxylated metabolites excreted in urine showed that the amount of diclofenac released and absorbed was the same as when taking an equivalent dose of diclofenac sodium in the form of enteric-coated tablets. However, the systemic bioavailability of diclofenac (released from Voltaren Retard) is, on average, 82% of that after oral administration of Voltaren enteric tablets at the same dose. Due to the prolonged release of the active substance from Voltaren Retard, the maximum drug concentrations achieved in plasma are lower than after taking enteric-coated tablets. The average peak concentration of 0.4 mcg/ml or 0.5 mcg/ml (1.25 or 1.6 μmol/L) is achieved, on average, 4 hours after taking the 75 mg or 100 mg tablet. Eating does not clinically affect the absorption and systemic bioavailability of Voltaren Retard. On the other hand, a mean plasma concentration of 13 ng/mL (40 nmol/L) may be observed 24 hours (16 hours) after taking Voltaren Retard 75 mg. The amount of absorbed active substance is linearly dependent on the dose of the drug. Since about half of diclofenac is metabolized during the first passage through the liver (“first pass effect”), the area under the concentration/time curve (AUC) after taking Voltaren Retard tablet is almost half that of parenteral administration of an equivalent dose of the drug. After repeated administration of Voltaren Retard, the pharmacokinetics do not change. If the recommended intervals between doses of the drug are observed, no accumulation is observed. The corresponding concentrations are 22 ng/ml or 25 ng/ml (70 nmol/l or 80 nmol/l) when taking Voltaren Retard 75 mg 2 times a day. Pharmacokinetic behavior does not change after repeated use. There is no accumulation provided that the recommended intervals between applications are observed. Distribution. 99.7% of diclofenac is bound to serum proteins, mainly albumin (99.4%). The volume of distribution is 0.12-0.17 l/kg. Diclofenac penetrates into the synovial fluid, where its maximum concentration is reached 2-4 hours later than in plasma. The apparent half-life from synovial fluid is 3-6 hours. 2 hours after reaching maximum plasma concentrations, the concentration of the active substance in the synovial fluid is higher than in the plasma, and remains higher for 12 hours. Diclofenac was detected at low concentrations (100 ng/ml) in the breast milk of one breastfeeding woman. The amount consumed by the infant through breast milk is equivalent to a dose of 0.03 mg/kg/day. Biotransformation. Biotransformation of diclofenac occurs partly through glucuronidation of the unchanged molecule, but mainly through single and multiple hydroxylation and methoxylation, which leads to the formation of several phenolic metabolites (3′-hydroxy-, 4′-hydroxy-, 5′-hydroxy, 4′, 5-dihydroxy- and 3′-hydroxy-4′-methoxydiclofenac), most of which are conjugated with glucuronic acid. Two of these phenolic metabolites are pharmacologically active, but to a significantly lesser extent than diclofenac. Excretion. The total systemic plasma clearance of diclofenac is 263 ± 56 ml/min. The terminal half-life in plasma is 1-2 hours. The half-life of 4 metabolites, including 2 pharmacologically active ones, is also short and amounts to 1-3 hours. One of the metabolites, 3′-hydroxy-4′-methoxydiclofenac, has a longer half-life. However, this metabolite is completely inactive pharmacologically. About 60% of the applied dose of the drug is excreted in the urine in the form of glucuronic conjugates of the intact molecule of the active substance, as well as in the form of metabolites, most of which are also converted into glucuronic conjugates. Less than 1% of diclofenac is excreted unchanged. The remainder of the applied dose of the drug is excreted in the form of metabolites through bile and feces. Linearity. The amount absorbed is linearly related to the dosage. Special groups of patents. No age-related differences in drug absorption, metabolism or excretion were identified. However, in several elderly patients, a 15-minute intravenous infusion resulted in plasma concentrations 50% higher than expected based on data obtained in young healthy subjects. In patients with impaired renal function, no accumulation of unchanged active substance was detected based on single-dose kinetics data using the usual dosage regimen. When creatinine clearance is less than 10 ml/min, the calculated equilibrium levels of hydroxymetabolites in blood plasma are approximately 4 times higher than in healthy individuals. Metabolites are finally excreted in bile. In patients with chronic hepatitis or uncompensated cirrhosis, the kinetics and metabolism of diclofenac are the same as in patients without liver disease.

Pharmaceutical characteristics

Basic physical and chemical properties: tablets are pale pink, triangular, biconvex, with beveled edges, with the inscription “ID” on one side and “CG” on the other in black ink.

Best before date

3 years. Do not use after the expiration date stated on the package.

Storage conditions

Store at a temperature not exceeding 30°C, in the original packaging to protect from moisture. Keep out of the reach of children.

Package

10 tablets in a blister, 2 blisters in a cardboard box along with an insert.

Conditions for dispensing from pharmacies

On prescription.

Buy Voltaren retard tablet p/o extended d-i 75 mg in blister pack No. 10x2 in the pharmacy

Price for Voltaren retard tablet p/o extended d-i 75 mg in sheets in pack No. 10x2

Instructions for use for Voltaren retard tablet p/o extended d-ya 75 mg in sheets in pack No. 10x2

Voltaren Emulgel for back pain, muscles and joints, gel 1% 75g

A country

Switzerland
The country of production may vary depending on the batch of goods. Please check with the operator for detailed information when confirming your order.

Active substance

Diclofenac

Description

Voltaren Emulgel 75g with an innovative applicator cap - convenient to apply, leaving your hands clean.
Voltaren Emulgel is intended for pain in the joints, back, muscles, as well as inflammation and swelling of soft tissues and joints. Voltaren Emulgel has a triple effect! 1: against pain 2: against inflammation * 3: to speed up recovery ** The active substance diclofenac is a non-steroidal anti-inflammatory drug with pronounced analgesic and anti-inflammatory properties, penetrates deep into the skin, acting on both pain and its cause - inflammation. * * Instructions for medical use, RU No. P N016030/01 dated 09.09.2009 ** Limit. Musculoskeletal disorders. 2013, 14:250. Compared to using placebo.

Compound

100 g of the drug contains: Active ingredient: 1.16 g of diclofenac diethylamine, which corresponds to 1 g of diclofenac sodium. Excipients: carbomers (carbopol 974 R) 1.20 g, macrogol cetostearate (cetomacrogol 1000) 2.00 g, cocoyl caprylocaprate (cetiol LC) 2.50 g, diethylamine 0.90 g, isopropanol 20.00 g, liquid paraffin 2.50 g, aromatic cream 45 (contains benzyl benzoate) 0.10 g, propylene glycol 5.00 g, water 64.64 g.

Product description

Homogeneous, creamy gel, color from white to yellowish.

pharmachologic effect

The active component diclofenac is a non-steroidal anti-inflammatory drug with pronounced analgesic, anti-inflammatory and antipyretic properties.
By indiscriminately inhibiting cyclooxygenase types 1 and 2, it disrupts the metabolism of arachidonic acid. Voltaren Emulgel is used to eliminate pain and reduce swelling associated with the inflammatory process. Thanks to its water-alcohol base, Voltaren Emulgel has a calming and cooling effect. Pharmacokinetics Absorption The amount of diclofenac absorbed through the skin is proportional to the area of ​​the treated surface and depends both on the total dose of the drug applied and on the degree of skin hydration. After applying 2.5 g of Voltaren Emulgel to a skin area of ​​500 cm2, absorption is about 6% of the applied dose of diclofenac compared to Voltaren tablets. Distribution: 99.7% of diclofenac is bound to plasma proteins, mainly albumin (99.4%). The concentration of diclofenac in plasma, synovial membrane and synovial fluid was measured when the drug was applied to the area of ​​the affected joint. Maximum plasma concentrations were approximately 100 times lower than after oral administration of the same amount of diclofenac. Diclofenac accumulates in the skin, which plays the role of a reservoir that releases the active substance into the tissue. When applied to the area of ​​the affected joint, the concentration of synovial fluid is higher than in plasma. Diclofenac is preferentially distributed and retained deep in tissues prone to inflammation (such as joints) rather than in the bloodstream. The concentration of diclofenac in tissues is up to 20 times higher than in plasma. Metabolism The metabolism of diclofenac is carried out partly by glucuronidation of the unchanged molecule, but mainly through single and multiple hydroxylation. Excretion Most of diclofenac and its metabolites are excreted in the urine. The total systemic plasma clearance of diclofenac is 263±56 ml/min. The terminal half-life is 1-2 hours. The half-life of metabolites, including two pharmacologically active ones, is also short and amounts to 1-3 hours. One of the metabolites (3'-hydroxy-4'-methoxydiclofenac) has a longer half-life, however , this metabolite is completely inactive. Patients with renal and hepatic impairment Accumulation of diclofenac and its metabolites is not expected in patients suffering from renal impairment. In patients with chronic hepatitis or uncompensated cirrhosis, the kinetics and metabolism of diclofenac are the same as in patients without liver disease

Indications for use

Back pain due to inflammatory and degenerative diseases of the spine (sciatica, osteoarthritis, lumbago, sciatica), - joint pain (joints of the fingers, knees, etc.) with osteoarthritis, - muscle pain (due to sprains, strains, bruises, injuries) , - inflammation and swelling of soft tissues and joints due to injuries and rheumatic diseases (tenosynovitis, bursitis, lesions of periarticular tissues)

Contraindications

Hypersensitivity to diclofenac or other components of the drug; a tendency to develop attacks of bronchial asthma, Quincke's edema, urticaria or acute rhinitis when using acetylsalicylic acid or other NSAIDs; pregnancy (III trimester), breastfeeding; children's age (up to 12 years); violation of the integrity of the skin at the intended site of application.

Carefully

Hepatic porphyria (exacerbation), erosive and ulcerative lesions of the gastrointestinal tract, severe dysfunction of the liver and kidneys, chronic heart failure, bronchial asthma, old age, pregnancy (I and II trimester).

Use during pregnancy and lactation

Due to the lack of data on the use of Voltaren Emulgel in pregnant women, the use of the drug during the first and second trimester of pregnancy is recommended only as prescribed by a doctor, weighing the benefits for the mother and the risk for the fetus. The drug is contraindicated in the third trimester of pregnancy due to the possibility of decreased uterine tone, impaired fetal renal function with subsequent development of oligohydramnios and/or premature closure of the fetal ductus arteriosus. Due to the lack of data on the penetration of Voltaren Emulgel into breast milk, the use of the drug during breastfeeding is recommended only as prescribed by a doctor, weighing the benefits for the mother and the risk to the fetus. If it is still necessary to use the drug, it should not be applied to the mammary glands or large surface areas of the skin and should not be used for a long time. There are no data on the use of Voltaren Emulgel and its effect on fertility in humans.

Directions for use and doses

Externally. For adults and children over 12 years of age, the drug is applied to the skin 3-4 times a day and lightly rubbed. The required amount of the drug depends on the size of the painful area. A single dose of the drug - 2-4 g (which is comparable in volume to the size of a cherry or walnut, respectively) is sufficient to treat an area of ​​400-800 cm2. If your hands are not the area where pain is localized, your hands should be washed after applying the drug. The duration of treatment depends on the indications and the observed effect (to enhance the effect, the gel can be used together with other dosage forms of Voltaren). If after 7 days of use the therapeutic effect is not observed or the condition worsens, you should consult a doctor. The product should not be used for more than 14 days for post-traumatic inflammation and rheumatic diseases of soft tissues. Laminated tubes: To remove the protective membrane, use the screw cap as a key (the recess with ridges on the outside of the cap). Align the indentation on the outside of the cap with the shaped protective membrane of the tube and turn. The membrane should separate from the tube. Laminated tubes can have either a regular cap (round shape) or an innovative cap (triangular shape), which is especially convenient for use with limited mobility of the joints of the hands due to osteoarthritis or other joint diseases or injuries, as well as an applicator cap. Aluminum tubes: Before first use, the protective membrane of the tube must be pierced using the special protrusion on the outside of the polypropylene screw cap. Aluminum bottles: The drug is applied to the skin 3-4 times a day. Spray on the painful area for 3-6 seconds, lightly rub into the skin until the solution is completely absorbed. The required amount of the drug depends on the size of the painful area. If your hands are not the area where pain is localized, your hands should be washed after applying the drug.

Side effect

Classification of the frequency of occurrence of adverse reactions: very often (≥1/10); often (≥1/100, Infectious and parasitic diseases: Very rare: pustular rash. Immune system disorders: Very rare: hypersensitivity reactions (including urticaria), angioedema. Respiratory, thoracic and mediastinal disorders: Very rare: bronchial asthma Disorders of the skin and subcutaneous tissues: Common: dermatitis (including contact dermatitis), rash, erythema, eczema, itching Rare: bullous dermatitis Very rare: photosensitivity reactions If any of the side effects indicated in the instructions are aggravated , or you notice any other side effects not listed in the instructions, tell your doctor.

Overdose

The extremely low systemic absorption of the active components of the drug when used externally makes overdose almost impossible. However, with accidental ingestion of 100 g of gel, equivalent to 1 g of diclofenac sodium, systemic adverse reactions may develop. Treatment for accidental ingestion: gastric lavage, induction of vomiting, activated charcoal, symptomatic therapy. Hemodialysis is ineffective due to the high degree of protein binding of diclofenac (about 99%)

Interaction with other drugs

Voltaren Emulgel may enhance the effect of drugs that cause photosensitivity. Clinically significant interactions with other drugs have not been described.

special instructions

Voltaren Emulgel should be applied only to intact skin, avoiding contact with open wounds. After application, do not apply an occlusive dressing. Do not allow the drug to come into contact with the eyes or mucous membranes, and do not swallow. The drug contains propylene glycol and benzyl benzoate, which in some cases may cause mild local skin irritation. Treatment should be discontinued if a skin rash develops after application of the drug. The possibility of systemic adverse reactions (associated with the use of systemic forms of diclofenac) should be considered if diclofenac for external use is used at a higher dose or for a longer time than recommended.

Release form

Gel for external use 1%. 75 g each in an aluminum tube equipped with a protective aluminum membrane, with a screw-on plastic cap (white or blue) with a protrusion for perforating the membrane on the outside. The tube along with instructions for use are placed in a cardboard box. 75 g in a laminated tube (low-density polyethylene, aluminum, high-density polyethylene) with a shoulder and a one-piece shaped protective membrane made of high-density polyethylene and a polypropylene screw cap (white or blue), round or triangular, or with a screw-on applicator cap with transparent protective cap. The cover on the outside is equipped with a key (a recess with protrusions) for opening the protective membrane of the tube. The tube along with instructions for use are placed in a cardboard box. 75 ml in a pressurized aluminum bottle (about 73 g and 97 g, respectively), with a plastic pump dispenser on a polyethylene ring and a protective cap. The bottle along with instructions for use is placed in a cardboard box. Secondary packaging is allowed to have a first-opening control.

Storage conditions

At a temperature not exceeding 30 C, out of the reach of children.

Best before date

3 years. The drug should not be used after the expiration date indicated on the package.

Voltaren, 30 pcs., 25 mg, enteric-coated tablets

Gastrointestinal lesions

When using diclofenac, like other NSAIDs, phenomena such as bleeding or ulceration/perforation of the gastrointestinal tract, in some cases with fatal outcome, were observed. These phenomena may occur at any time when using these drugs with or without previous symptoms or a history of serious gastrointestinal diseases. In older patients, such complications can have serious consequences. If patients receiving Voltaren® develop bleeding or gastrointestinal ulceration, the drug should be discontinued.

To reduce the risk of toxic effects on the gastrointestinal tract in patients with ulcerative lesions of the gastrointestinal tract, especially those complicated by bleeding or perforation in history, as well as in elderly patients, the drug should be used in the minimum effective dose.

In patients with an increased risk of developing gastrointestinal complications, as well as in patients receiving therapy with low doses of acetylsalicylic acid, gastroprotectors (proton pump inhibitors or misoprostol) or other medications should be used during drug therapy to reduce the risk of undesirable effects on the gastrointestinal tract.

Patients with a history of gastrointestinal lesions, especially the elderly, should report all abdominal symptoms to the doctor.

Patients with bronchial asthma

Exacerbation of asthma (NSAID intolerance/NSAID-induced asthma), angioedema and urticaria are most often observed in patients with bronchial asthma, seasonal allergic rhinitis, nasal polyps, chronic obstructive pulmonary disease or chronic infectious diseases of the respiratory tract (especially those associated with allergic rhinitis). rhinitis-like symptoms). In this group of patients, as well as in patients with allergies to other drugs (skin rash and itching or urticaria), special caution should be observed when using the drug Voltaren® (preparedness for resuscitation measures).

Skin reactions

Serious dermatological reactions such as exfoliative dermatitis, Stevens-Johnson syndrome, toxic epidermal necrolysis, in some cases fatal, have been reported very rarely with the use of diclofenac. The highest risk and incidence of severe dermatological reactions were observed in the first month of treatment with diclofenac. If a patient receiving Voltaren® develops the first signs of a skin rash, damage to the mucous membranes or other symptoms of hypersensitivity, the drug should be discontinued.

In rare cases, when using Voltaren®, like other NSAIDs, anaphylactic/anaphylactoid reactions may develop in patients who have not previously received diclofenac.

Effects on the liver

Since during the period of use of the drug Voltaren® there may be an increase in the activity of one or more “liver” enzymes, monitoring of liver function is indicated as a precautionary measure during long-term therapy with the drug. If liver dysfunction persists and progresses or signs of liver disease or other symptoms occur (for example, eosinophilia, rash, etc.), the drug should be discontinued. It should be borne in mind that hepatitis during the use of the drug Voltaren® can develop without prodromal phenomena.

Effects on the kidneys

During therapy with Voltaren®, it is recommended to monitor renal function in patients with hypertension, impaired cardiac or renal function, elderly patients, patients receiving diuretics or other drugs that affect renal function, as well as in patients with a significant decrease in the volume of extracellular fluid of any etiology, for example, during the period before and after major surgical interventions. After cessation of drug therapy, normalization of renal function indicators to initial values ​​is usually observed.

Effects on the cardiovascular system

Therapy with NSAIDs, including diclofenac, particularly long-term and high-dose therapy, may be associated with a small increased risk of serious cardiovascular thrombotic events (including myocardial infarction and stroke).

In patients with diseases of the cardiovascular system and a high risk of developing diseases of the cardiovascular system (for example, with arterial hypertension, hyperlipidemia, diabetes mellitus, smokers), the drug should be used with extreme caution, at the lowest effective dose for the shortest possible duration of treatment, since the risk of thrombotic complications increases with increasing dose and duration of treatment. With long-term therapy (more than 4 weeks), the daily dose of diclofenac in such patients should not exceed 100 mg. The effectiveness of treatment and the patient's need for symptomatic therapy should be periodically assessed, especially in cases where its duration is more than 4 weeks. When the first symptoms of thrombotic disorders appear (for example, chest pain, feeling short of breath, weakness, speech impairment), the patient should immediately seek medical help.

Impact on the hematopoietic system

The drug Voltaren® may temporarily inhibit platelet aggregation, therefore, in patients with hemostasis disorders, it is necessary to carefully monitor relevant laboratory parameters.

With long-term use of the drug Voltaren®, it is recommended to conduct regular clinical tests of peripheral blood.

Masking signs of an infectious process

The anti-inflammatory effect of the drug Voltaren® may complicate the diagnosis of infectious processes.

Use simultaneously with other NSAIDs

Voltaren® should not be used concomitantly with other NSAIDs, including selective COX-2 inhibitors due to the risk of adverse events.

Voltaren, rectal suppositories 50 mg, 10 pcs.

Manufacturer

Novartis Pharma Stein AG, Switzerland

Compound

1 suppository contains:
Active substances:

diclofenac (in the form of sodium salt) - 50 mg.

Excipients:

solid fat - up to 2 g.

pharmachologic effect

Voltaren is a non-steroidal anti-inflammatory drug (NSAID). It has a pronounced analgesic, anti-inflammatory and antipyretic effect.

The main mechanism of action of diclofenac, established under experimental conditions, is considered to be inhibition of prostaglandin biosynthesis. Prostaglandins play an important role in the genesis of inflammation, pain and fever.

In vitro, diclofenac sodium in concentrations equivalent to those achieved in the treatment of patients does not suppress the biosynthesis of proteoglycans in cartilage tissue. In rheumatic diseases, the anti-inflammatory and analgesic properties of Voltaren provide a clinical effect, characterized by a significant reduction in the severity of such manifestations of diseases as pain at rest and during movement, morning stiffness and swelling of the joints, as well as an improvement in the functional state.

Indications

– inflammatory and degenerative diseases of the musculoskeletal system: rheumatoid arthritis, juvenile rheumatoid arthritis, ankylosing spondylitis, osteoarthritis, spondyloarthritis, osteoarthritis; – diseases of the spine accompanied by pain; – rheumatic diseases of extra-articular soft tissues; – post-traumatic and postoperative pain syndromes, accompanied by inflammation and swelling; – gynecological diseases accompanied by pain and inflammation (for example, primary algodismenorrhea, adnexitis); – as an additional remedy for severe infectious and inflammatory diseases of the ear, nose and throat, which occur with severe pain, for example, pharyngitis, tonsillitis, otitis media. The main treatment of the disease is carried out in accordance with generally accepted principles, incl. with the use of etiotropic therapy. Isolated fever is not an indication for the use of the drug; - migraine attacks.

Contraindications

– proctitis (only for suppositories); – hematopoietic disorders; – children under 14 years of age; – hypersensitivity to diclofenac and any other ingredients of the drug.

The drug is not recommended for use in the third trimester of pregnancy (possible suppression of uterine contractility and premature closure of the ductus arteriosus in the fetus).

Side effects

When assessing the frequency of occurrence of various adverse reactions, the following gradations were used: often - >10%, sometimes - >1-10%, rarely - >0.001-1%, in some cases

- From the digestive system: sometimes - pain in the epigastric region, nausea, vomiting, diarrhea, abdominal cramps, dyspepsia, flatulence, anorexia; rarely - gastrointestinal bleeding (vomiting blood, melena, diarrhea mixed with blood), stomach and intestinal ulcers, accompanied or not accompanied by bleeding or perforation; in some cases - aphthous stomatitis, glossitis, damage to the esophagus, the occurrence of diaphragm-like strictures in the intestine, disorders of the distal colon, such as nonspecific hemorrhagic colitis, exacerbation of ulcerative colitis or Crohn's disease, constipation, pancreatitis; sometimes - increased levels of aminotransferases in the blood serum; rarely - hepatitis, accompanied or not accompanied by jaundice; in some cases - fulminant hepatitis.

From the central nervous system and peripheral nervous system: sometimes - headache, dizziness; rarely - drowsiness; in some cases - sensitivity disorders, including paresthesia, memory disorders, disorientation, insomnia, irritability, convulsions, depression, anxiety, nightmares, tremor, psychotic reactions, aseptic meningitis.

From the senses: in some cases - visual impairment (blurred vision, diplopia), hearing impairment, tinnitus, disturbances in the sense of taste.

From the cardiovascular system: in some cases - palpitations, chest pain, increased blood pressure, worsening congestive heart failure.

Dermatological reactions: sometimes - skin rashes; rarely - urticaria; in some cases - bullous rashes, eczema, erythema multiforme, Stevens-Johnson syndrome, Lyell's syndrome (acute toxic epidermal necrolysis), erythroderma (exfoliative dermatitis), hair loss, photosensitivity reactions; purpura, incl. allergic.

From the urinary system: rarely - swelling; in some cases - acute renal failure, hematuria, proteinuria, interstitial nephritis; nephrotic syndrome; papillary necrosis.

From the hematopoietic system: in some cases - thrombocytopenia, leukopenia, hemolytic anemia, aplastic anemia, agranulocytosis.

Hypersensitivity reactions: rarely - bronchospasm, systemic anaphylactic/anaphylactoid reactions, including hypotension; in some cases - vasculitis, pneumonitis.

Interaction

Voltaren can be prescribed together with oral hypoglycemic drugs and the effectiveness of the latter does not change. However, there are isolated reports of the development in such cases of both hypoglycemia and hyperglycemia, which necessitated the need to change the dose of hypoglycemic drugs during the use of Voltaren.

Caution should be exercised when using NSAIDs less than 24 hours before starting or after stopping methotrexate therapy, because its blood levels (and therefore toxicity) may increase.

The effect of NSAIDs on the activity of prostaglandins in the kidneys may enhance the nephrotoxicity of cyclosporine.

There are isolated reports of the occurrence of seizures in patients taking NSAIDs and quinolone antibacterial drugs simultaneously.

How to take, course of administration and dosage

For adults, the recommended starting dose is 100-150 mg/day. In relatively mild cases of the disease, as well as for long-term therapy, 75-100 mg/day is sufficient. Frequency of application - 2-3 times. To relieve night pain or morning stiffness, Voltaren is prescribed in suppositories before bedtime, in addition to taking the drug in tablet form during the day; in this case, the total daily dose should not exceed 150 mg.

For primary dysmenorrhea, the daily dose is selected individually; usually it is 50-150 mg. The initial dose should be 50-100 mg; if necessary, over several menstrual cycles it can be increased to 150 mg/day. Treatment should begin when the first symptoms appear. Depending on the dynamics of clinical symptoms, treatment can be continued for several days.

For a migraine attack, the initial dose is 100 mg. The drug is prescribed at the first symptoms of an approaching attack. If necessary, on the same day you can additionally apply Voltaren in suppositories at a dose of up to 100 mg. If it is necessary to continue treatment in subsequent days, the daily dose of the drug should not exceed 150 mg (in several administrations).

Children weighing 25 kg or more are prescribed the drug at a dose of 0.5-2 mg/kg body weight/day (the daily dose, depending on the severity of the disease, should be divided into 2-3 single doses). For the treatment of juvenile rheumatoid arthritis, the daily dose can be increased to a maximum of 3 mg/kg (in several administrations).

The use of 50 mg and 100 mg suppositories in children is not recommended.

Special instructions

During the use of Voltaren, careful medical supervision is necessary for those patients who have complaints indicating gastrointestinal diseases; having a history of ulcerative lesions of the stomach or intestines; those suffering from ulcerative colitis or Crohn's disease, as well as those with impaired liver function.

During the use of Voltaren, as well as other NSAIDs, the level of one or more liver enzymes may increase. Therefore, during long-term therapy with Voltaren, monitoring of liver function is indicated as a precautionary measure. If abnormalities in liver function parameters persist or worsen, or if clinical manifestations of liver disease or other symptoms occur (for example, eosinophilia, rash, etc.), Voltaren should be discontinued. It should be borne in mind that hepatitis during the use of Voltaren can occur without prodromal phenomena.

Caution is necessary when prescribing Voltaren to patients with hepatic porphyria, because the drug can provoke attacks of porphyria.

Since prostaglandins play an important role in maintaining renal blood flow, special caution is required when treating patients with impaired cardiac or renal function, patients receiving diuretics, as well as patients who have a significant decrease in circulating blood plasma volume of any etiology, for example, in the period before and after major surgical interventions. In these cases, monitoring of renal function is recommended as a precautionary measure during the use of Voltaren. Discontinuation of the drug usually results in renal function returning to baseline levels. Caution should be exercised when using Voltaren in elderly patients. This is especially true in frail or low-weight elderly people; they are recommended to prescribe the drug at the minimum effective dose.

During the use of Voltaren, gastrointestinal bleeding may occur (for the first time or repeatedly) or ulceration/perforation of the gastrointestinal tract may develop, accompanied or not accompanied by precursor symptoms. More serious consequences of these complications may occur in older patients. In those rare cases where these complications develop in patients receiving Voltaren, the drug should be discontinued.

When using Voltaren for the first time, as well as other NSAIDs, in rare cases allergic reactions may develop, including anaphylactic and anaphylactoid reactions. Voltaren, due to its pharmacodynamic properties, can mask the manifestations of infectious diseases. Voltaren, like other NSAIDs, may temporarily inhibit platelet aggregation. Therefore, in patients with hemostasis disorders, careful monitoring of relevant laboratory parameters is necessary.

With long-term use of Voltaren, like other NSAIDs, systematic monitoring of peripheral blood patterns is indicated.

Release form

Suppositories

Storage conditions

At a temperature not exceeding 30 °C

Best before date

3 years

Active substance

Diclofenac

Conditions for dispensing from pharmacies

On prescription

Dosage form

rectal suppositories

Purpose

Pregnant women 1st and 2nd trimester as prescribed by a doctor, For adults as prescribed by a doctor

Indications

Adnexitis, Gout, Osteoarthritis, Sciatica, Arthrosis and arthritis, Tendon inflammation, Rheumatoid arthritis, Periarthritis, Swelling after injuries and operations, Bursitis, Lumbago

Barcode and weight

Barcode: 7680392549054 Weight: 0.033 kg