Ritonavir-100 (Ritonavir-100)

Composition Pharmacodynamics Indications Carefully Contraindications Dosing and Administration Side effects Form release / dosage
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Active substanceRitonavirRitonavir
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    • Dosage form: & nbspTOthe apsules.
    Composition:

    One capsule contains:

    active substance: ritonavir - 100 mg;

    Excipients: ethanol 90 mg, macrogol glycerylricinoleate (cremophor ELP) - 45 mg, oleic acid - 664.9 mg, butylhydroxytoluene - 0.1 mg.

    Capsule shell composition: gelatin (70.41%), glycerol (28.16%), methyl parahydroxybenzoate (0.31%), propyl parahydroxybenzoate (0.08%), titanium dioxide (1.03%).

    Description:

    Soft gelatin capsules white with a creamy shade of color, oblong with a seam.

    Contents of capsules - a transparent liquid of yellow or yellow with a brownish tinge of color, with a specific odor. At a temperature of 2-8 ° C, the contents of the capsules partially crystallize.

    Pharmacotherapeutic group:antiviral [HIV] agent
    ATX: & nbsp

    J.05.A.E.   Protease Inhibitors

    J.05.A.E.03   Ritonavir

    Pharmacodynamics:

    Antiviral agent, aspartyl protease inhibitor HIV-1 and HIV-2, active peptidomimetic. Inhibition of HIV proteases inhibits rupture gag-pol the connection of the polyprotein, which leads to the formation of an immature and infectious virus. Ritonavir has a selective affinity for HIV protease and exhibits little activity with respect to aspartyl protease of a human. Increases the number CD4 + cells in the blood and reduces the concentration of viral RNA. It leads to an increase in the total number of leukocytes, platelets and lymphocytes.

    Pharmacokinetics:

    Absorption - 60-80%, time to reach a maximum concentration of 2-4 hours. The apparent volume of distribution is 0.41 l / kg and corresponds to the volume distribution of water in the body. Bioavailability - 94%.

    Metabolized by the cytochrome P450 system to hydroxylated inactive metabolites followed by their glucuronation. The main isoenzymes responsible for metabolism are CYP2B6, CYP3A4, CYP3A5, CYP3A7. Ritonavir is an inhibitor of isoenzymes CYP2D6 and CYP3A3, CYP3A5, CYP3A7. Smoking, body weight, age, sex, CYP2D6-phenotype do not affect the clearance of the drug. With multiple intake of the same dose, the minimum concentration of the drug in the plasma (Cmin), the area under the curve "concentration - time" (AUC) and half-life (T1/2) are reduced.

    It is excreted mainly through the intestine (20-40% unchanged).

    Special patient groups

    Children

    In children under the age of 14 years, the equilibrium clearance of ritonavir when taken inwards at a dose of 250 mg / m2 up to 400 mg / m2 twice a day was approximately 1.5-1.7 times higher than in adults. The concentration of ritonavir in the blood after taking doses from 350 mg / m2 up to 400 mg / m2 twice a day in children is comparable to the concentration of ritonavir in adults taking the drug at a dose of 600 mg (about 330 mg / m2) 2 times a day.

    Elderly patients

    The pharmacokinetics of ritonavir when used at a dose of 100 mg in combination with lopinavir or at higher doses but without HIV protease inhibitors does not differ in patients aged 50-70 years and in younger patients.

    Patients with impaired renal function

    At present, there is no data on the pharmacokinetics of ritonavir in patients with renal insufficiency. The renal clearance of ritonavir is negligible, so changes in overall clearance in patients with impaired renal function are not expected. Because the ritonavir actively binds to plasma proteins, it is unlikely that it will be largely excreted in hemodialysis or peritoneal dialysis.

    Patients with impaired hepatic function

    In patients with mild hepatic insufficiency, the effect of ritonavir at a dose of 400 mg on admission twice a day corresponded to that in patients of the control group at a dose of 500 mg twice a day. Thus, in patients with mild hepatic insufficiency, dose adjustment is not required. There are no sufficient data on the use of ritonavir in patients with moderate hepatic impairment. Hepatic insufficiency of mild or moderate degree does not affect the binding of ritonavir to plasma proteins.

    Indications:HIV infection in adults and children (as part of combination therapy).
    Contraindications:

    - Hypersensitivity to ritonavir or to one of the components of the drug;

    - severe hepatic impairment;

    - Children's age up to 3 years (for this dosage form);

    - simultaneous reception of the following drugs - alfuzosin, amiodarone, astemizole, bepridil, cisapride, dihydroergotamine, ergometrine, methylergomethrin, ergotamine, enkinide, flecainide, clozapine, pimozide, propafenone, quinidine, terfenadine, midazolam, triazolam, voriconazole, lovastatin, simvastatin, rifabutin, pethidine, piroxicam, dextropropoxyphene, fusidic acid, dical clorazepate, estazolam, diazepam, flurazepam, bupropion, sildenafil, salmeterol, blonanserin; saquinavir and rifampicin; preparations of St. John's wort perfumed.

    Carefully:

    Diseases of the liver (including hepatitis), increased activity of "liver" enzymes, moderate hepatic insufficiency; hemophilia; disorders of conduction of the heart, organic heart diseases, including coronary heart disease, cardiomyopathy; simultaneous reception of drugs that extend the interval PQ.

    The simultaneous use of ritonavir with certain antihistamines, sedatives, hypnotics, antiarrhythmics can lead to potentially serious and / or life-threatening side effects due to the possible effect of ritonavir on the metabolism of drugs in the liver (see section "Interaction with other medicinal products").

    Pregnancy and lactation:

    The use of ritonavir in pregnancy is possible only if the expected benefit to the mother exceeds the potential risk to the fetus.

    HIV-infected women should not breast-feed their children under any circumstances to avoid the transmission of HIV.

    Dosing and Administration:

    Adults: inside, during meals, 600 mg 2 times a day as the only protease inhibitor. To reduce side effects, the initial dose is 300 mg 2 times a day, then the dose is increased by 100 mg in each dose until a dose of 600 mg is given twice a day. When ritonavir is used in combination with saquinavir, treatment is started with a dose of ritonavir 300 mg 2 times a day. If a combination of ritonavir with indinavir is used, treatment is initiated with a dose of ritonavir 200 mg twice a day and increases twice daily intake by 100 mg to a dose of 400 mg twice a day for 2 weeks.

    Children: 400 mg / m2 2 times a day; with poor tolerance, the initial dose is 250 mg / m2, with a further increase every 2-3 days by 50 mg / m2 in each dose until a dose of 400 mg / m2 2 times a day.

    In elderly patients correction of the dose is not required.

    Side effects:

    The most common cases in adults were asthenia, gastrointestinal (nausea, diarrhea, vomiting, lack of appetite, abdominal pain, taste disorder) and neurological disorders, including perioral and peripheral paresthesia.The nature of the observed side effects in children was similar to that of adult patients.

    Disturbances from the nervous system: dizziness, headache, migraine, paresthesia, perioral paresthesia, hyperesthesia, drowsiness, insomnia, unpleasant dreams, amnesia, aphasia, ataxia, epilepsy, impaired coordination of movements, neuralgia, neuropathy, paralysis, olfaction perversion, peripheral neuropathy, peripheral sensory neuropathy, loss taste, tremor.

    Disorders of the psyche: anxiety, confusion, depression, emotional lability, euphoria, hallucinations, nervousness, personality disorders, unpleasant thoughts, anomalies of thinking.

    Hearing disorders and labyrinthine disorders: earache, hearing loss, increased ear wax, tinnitus.

    Disturbances on the part of the organ of sight: visual impairment, amblyopia / blurred vision, blepharitis, diplopia, visual field disturbance, eye pain, photophobia, iritis, uveitis, changes in electro-oculogram, electroretinogram.

    Disorders from the cardiovascular system: vasodilation, palpitation, collapse, fainting, hemorrhage, hypotension,Orthostatic hypotension, violation of peripheral circulation, tachycardia, myocardial infarction, conduction disorders of the heart.

    Violations of the blood and lymphatic system: anemia, bruising, leukopenia / leukocytosis, lymphadenopathy, lymphocytosis, neutropenia / neutrophilia, eosinophilia, thrombocytopenia.

    Disturbances from the respiratory system, chest and mediastinal organs: pharyngitis, dry cough, bronchospasm, shortness of breath, epistaxis, hypoventilation, pulmonary dysfunction, interstitial pneumonia, rhinitis, chest pain, chest pain, irritation of the larynx.

    Disorders from the gastrointestinal tract: pain in the abdomen, dyspepsia, nausea, diarrhea, vomiting, lack of appetite, impaired taste, flatulence, belching, dryness of the oral mucosa, ulceration of the oral mucosa, increased abdomen, stool disorders, stools, cheilitis, gingivitis, ileitis, colitis, constipation, dysphagia, esophagitis, gastritis, gastroenteritis, gastrointestinal bleeding, candidiasis of the oral mucosa, pancreatitis, periodontal abscesses, rectal damage, tenesmus, thirst.

    Disturbances from the liver and bile ducts: cholangitis, hepatitis, hepatomegaly, liver damage, liver failure.

    Disorders from the metabolism and nutrition: hyperlipidemia / hypercholesterolemia, weight loss, hypovolemia (dehydration), avitaminosis, cachexia, glucosuria, gout, redistribution / accumulation of subcutaneous fat.

    Disorders from the endocrine system: diabetes; decrease in free and total thyroxine (T4) in blood plasma.

    Disturbances from musculoskeletal and connective tissue: myalgia, myositis, acute necrosis of skeletal muscles, arthralgia, arthrosis, back pain, pain in the face, articular disorders, muscle cramps, muscle weakness, neck pain, neck stiffness, convulsive twitching (tick).

    Disorders from the kidneys and urinary tract: dysuria, polyuria, nocturia, hematuria, kidney stones, pain in the kidney, pyelonephritis, urethritis, increased urination, delayed urination, kidney failure.

    Disturbances from the skin and subcutaneous tissues: itching, increased sweating, skin rash, maculopapular rash, acne, contact dermatitis, dry skin, eczema,edema of the face, folliculitis, molluscum contagiosum, peripheral edema, photosensitivity, psoriasis, seborrhea, vesicle-bulbous rash.

    Immune system disorders: allergic reactions (urticaria, skin rash, angioedema); anaphylaxis, erythema multiforme bullous (Stevens-Johnson syndrome).

    General disorders and disorders at the site of administration: asthenia, pain, chills, flu-like syndrome, malaise, fever, gait disturbance.

    Other: menorrhagia, impotence, decreased libido, pain in the face, hiccups.

    Laboratory data: increase / decrease concentration of glucose, sodium, potassium, chloride, total calcium, magnesium, number of leukocytes, number of neutrophils; rise concentration of creatinine, inorganic phosphorus, uric acid, total bilirubin, triglycerides, activity of alkaline phosphatase (AFP), aspartate aminotransferase (ACT), alanine aminotransferase (ALT), lactate dehydrogenase (LDH), gamma-glutamyl transpeptidase (GGTP), amylase, creatinine phosphokinase (CK), the number of eosinophils, prothrombin time, partial activated thromboplastin time; decrease hemoglobin, hematocrit, albumin, the number of platelets.

    Overdose:

    Symptoms: paresthesia, multiple vomiting, diarrhea, dehydration (lowering blood pressure, impaired renal function), asthenia.

    Treatment: supportive activities, monitoring of vital signs and condition of the patient; gastric lavage through the probe and the introduction of activated charcoal. There is no specific antidote. The effectiveness of using dialysis to remove a large amount of the drug is unlikely.

    Interaction:

    The effects of other drugs on the pharmacokinetics of ritonavir

    Drugs that increase the activity of CYP3A, such as phenobarbital, carbamazepine, dexamethasone, phenytoin, rifampicin and rifabutin, lead to an increase in the clearance of ritonavir, as a result of which its concentration in the blood plasma decreases.

    Rifampicin leads to a decrease AUC and Cmax ritonavir, while clarithromycin and fluconazole increase the values ​​of these parameters, and didanosine and zidovudine do not affect them.

    Fluoxetine increases AUC of ritonavir, but does not affect its Cmax.

    Smoking of tobacco leads to a decrease AUC ritonavir by 18%.

    The effect of ritonavir on the pharmacokinetics of other drugs

    Ritonavir is an isoenzyme inhibitor CYP3A cytochrome P450, therefore, with simultaneous reception of ritonavir with drugs metabolized predominantly with the participation of the isozyme CYP3A, it is possible to increase their concentration in plasma (more than 3 times). The use of ritonavir with drugs, increasing concentrations in the plasma can lead to potentially serious and / or life-threatening conditions is contraindicated.

    The use of ritonavir with other substrates of the CYP3A isoenzyme may require dose adjustment and careful monitoring of patients.

    Less ritonavir inhibits the isoenzyme CYP2D6. With simultaneous administration of ritonavir and CYP2D6 isoenzyme substrates, an increase in the concentration of the latter in the plasma (2-fold) is possible, which may require correction of their dose in the direction of decrease.

    Ritonavir is probably the inducer of the isoenzymes CYP3A, CYP1A2, CYP2C9, CYP2C19 and CYP2B6, as well as a number of other enzymes, including glucuronosyltransferase, which may require an increase in the dose of preparations biotransforming under the action of this enzyme, due to a decrease in their effectiveness in joint administration.

    There are reports of the development of adverse reactions from the cardiovascular and nervous systems with the simultaneous administration of ritonavir with disopyramide, mexiletine, nefazodone or fluoxetine.

    Alprazolam: statistically significantly decreases FROMmax alprazolam (16%) and its sedative effect when taken concomitantly with ritonavir. There may also be minor psychomotor abnormalities.

    Amprenavir: the concentration rises.

    Atazanavir: ritonavir significantly increases AUC and FROMmin atazanavir.

    Boszentan: simultaneous reception of ritonavir and bosentan leads to a significant increase in the level of bosentan. In patients who received ritonavir for at least 10 days, the initial dose of bosentan is 62.5 mg once a day or every other day, depending on individual tolerability. Patients who receive bosentan, it is necessary to stop receiving it, at least 36 hours before the start of ritonavir. 10 days after the initiation of ritonavir, bosentan may be taken at an initial dose of 62.5 mg once a day or every other day, depending on the individual tolerability.

    Buspirone: first of all it is metabolized by isoenzyme CYP3A4, therefore its concentration can be significantly increased, as a result of which it is recommended to reduce the dose of buspirone on the background of its reception with ritonavir.

    Warfarin: the concentration of warfarin may change when it is used together with ritonavir - it is recommended to monitor the clotting characteristics of the blood.

    Voriconazole: while taking ritonavir 400 mg every 12 hours decreases AUC voriconazole in the equilibrium state on average by 82%, which dramatically reduces its effectiveness, so the joint administration of these drugs is not recommended.

    Delavirdine: is an inhibitor of the isoenzyme CYP3A4. Increases equilibrium FROMmax and AUC ritonavir by 50% and 75%, respectively, as a result of which a reduction in the dose of ritonavir is required. In its turn ritonavir does not affect the pharmacokinetics of delavirdine.

    Desipramine: ritonavir increases by 145% AUC desipramine, therefore, a dose reduction of desipramine should be provided for patients taking it in combination with ritonavir.

    Didanosine: ritonavir reduces equilibrium FROMmax and AUC didanosine by 16% and 13%, respectively. To avoid incompatibility, it is recommended to use drugs with an interval of not less than 2.5 hours.

    Digoxin: simultaneous reception of ritonavir (300 mg every 12 hours) and digoxin leads to a significant increase in the level of digoxin. With the simultaneous administration of digoxin and ritonavir, care should be taken to ensure adequate monitoring of the level of digoxin in the plasma.

    Disulfiram / Metronidazole: in capsules with ritonavir contains 10% of ethanol, so you should avoid the joint administration of ritonavir with disulfiram or drugs with a disulfiram-like action, such as metronidazole.

    Preparations St. John's wort perfumed (Hypericum perforatum): should not be taken in conjunction with ritonavir, since the concentration of ritonavir in the plasma is lowered due to induction of the isoenzyme CYP3A4. As a result, therapeutic effectiveness is reduced and resistance to ritonavir develops.

    Zidovudine: ritonavir reduced FROMmax and AUC zidovudine by approximately 27% and 25%, respectively. Changes in the dose of zidovudine when used with ritonavir is not required.

    Indinavir: ritonavir inhibits the metabolism of indinavir, which occurs with the participation of isoenzyme CYP3A, and leads to an increase in the concentration of indinavir in plasma.

    The risk of nephrolithiasis may increase when ritonavir is combined with indinavir at doses equal to or greater than 800 mg twice daily. It is necessary to maintain adequate hydration of patients and monitor their condition.

    Ketoconazole: The use of ritonavir in combination with ketoconazole (200 mg / day) was expressed in a marked increase in plasma ketoconazole levels: mean AUC0-24 increased by 244% and Cmax - by 55%. The mean half-life of ketoconazole increased from 2.7 to 13.2 hours. The mean AUC0-24 and Cmax ritonavir increased by 18% and 10%, respectively. Doses of ritonavir do not need to be corrected with simultaneous admission with ketoconazole, while doses of ketoconazole 200 mg / day or higher should not be used in combination with ritonavir. It is recommended to reduce the dose of ketoconazole.

    Clarithromycin: metabolism is significantly inhibited, resulting in FROMmax clarithromycin is increased by 31%, FROMmin - by 182%, AUC - by 77%. Almost completely inhibited the formation of 14-hydroxyclarithromycin (the main metabolite of clarithromycin).

    Due to the large therapeutic range of clarithromycin, there is no need to reduce the dose in patients with normal renal function.

    For patients with renal insufficiency, the following dose adjustment should be provided: with creatinine clearance (CK) from 30 to 60 ml / min, the dose of clarithromycin should be reduced by 50%, with a QC <30 ml / min the dose of clarithromycin should be reduced by 75%. Doses of clarithromycin> 1 g / day should not be given in combination with ritonavir.

    Maraviroc: with concurrent administration with ritonavir (100 mg every 12 hours), the metabolism is significantly inhibited, AUC increases by 161%, FROMmin - by 28%.

    Methadone: The use of ritonavir in combination with methadone caused a decrease in the concentration of methadone. It may be necessary to increase the dose of methadone when applied in combination with ritonavir.

    Nelfinavir: The interaction between ritonavir and nelfinavir probably occurs with both inhibition and induction of cytochrome P450 isoenzymes. There is a significant increase in the concentration of M8 (the main active metabolite of nelfinavir), while the concentration of nelfinavir itself increases to a lesser extent.

    Contraceptive preparations for oral or in the form of a patch: The use of ritonavir in combination with combined forms of ethinyl estradiol for oral administration was expressed in a decrease in the mean AUC ethinyl estradiol by 32%, and its FROMmax - by 40%. Contraceptive drugs with a higher concentration of ethinylestradiol should be used or alternative methods of contraception should be used.

    Rifabutin: The use in combination with ritonavir leads to a multiple (4 to 35 times) increase AUC and FROMmax rifabutin and its active metabolite 25-O-deacetyl rifabutin, which has clinical consequences. It is recommended to reduce the dose of rifabutin by at least 3/4 of the usual daily dose of 300 mg (ie, 150 mg every other day or 3 times a week). If necessary, further reduction of the dose is recommended.

    Saquinavir: data from pharmacokinetic studies in patients indicate that its use in combination with ritonavir causes a multiple increase in the concentration of saquinavir in the blood (AUC, A 17-fold increase). Long-term combination therapy at doses of more than 400 mg twice a day of each drug was accompanied by an increase in the frequency of adverse reactions. Do not assign saquinavir and ritonavir together with rifampicin because of the risk of severe hepatotoxicity when using these three drugs at the same time.

    Salmeterol: with the simultaneous administration of salmeterol with ritonavir, an increase in the concentration of salmeterol is noted. The joint administration of ritonavir with salmeterol is not recommended due to an increased risk of salmeterol side effects, including lengthening of the interval QT, palpitation and tachycardia.

    Means for the treatment of erectile dysfunction

    Sildenafil: it is recommended to use caution sildenafil in patients taking ritonavir. The use of sildenafil in combination with ritonavir causes a significant (11-fold) increase AUC sildenafil in the plasma, which increases the risk of adverse reactions associated with sildenafil, such as hypotension, syncope, visual impairment, prolonged erection.

    Tadalafil: should use tadalafil with caution in reduced doses - not more than 10 mg every 72 hours with enhanced monitoring of adverse events.

    Vardenafil: should use vardenafil with caution in reduced doses - no more than 2.5 mg every 72 hours with enhanced monitoring of adverse events.

    Combination of sulfamethoxazole / trimethoprim: The use of ritonavir in combination with sulfamethoxazole / trimethoprim caused a 20% reduction AUC sulfamethoxazole and a 20% increase AUC trimethoprim. Correction of the dose of sulfamethoxazole / trimethoprim when used in combination with ritonavir is usually not required.

    Theophylline: may require an increase in the dose of theophylline, since the use in combination with ritonavir caused a decrease AUC theophylline by 43%.

    Trazodone: At the same time, the use of ritonavir and trazodone may increase trazodone concentrations. There were observed such undesirable phenomena as nausea, dizziness, hypotension, fainting. Care should be taken when using trazodone and ritonavir concurrently, a dose reduction of trazodone may be required.

    Fluticasone propionate: taking ritonavir and fluticasone propionate leads to an increase in the concentration of fluticasone propionate.

    Fosamprenavir: ritonavir significantly increases AUC and FROMmin fosamprenavir.

    Fusidic acid: It is suggested that the use of ritonavir in combination with fusidic acid increases the concentration of both fusidic acid and ritonavir, as a protease inhibitor in plasma.

    Efavirenz: equilibrium AUC efavirenz increased by 21%. There was a related 17% increase AUC ritonavir.

    The effect of ritonavir on the pharmacokinetics of other drugs with simultaneous application

    Ritonavir leads to a significant increase AUC (more than 3 times) of the following drugs: alfetanil, amiodarone, atazanavir, atorvastatin, bromocriptine, buspirone, verapamil, dexamethasone, diltiazem, indinavir, isradipine, itraconazole, carbamazepine, ketoconazole, lidocaine, lovastatin, loratadine, miconazole, nefazodone, nicardipine, nimodipine, nisoldipine, nitrendipine, nifedipine, rifabutin, saquinavir, sertraline, simvastatin, sirolimus, tacrolimus, tamoxifen, felodipine, fentanyl, fluticasone, fosamprenavir, fusidic acid, quinine, ciclosporin, erythromycin.

    Ritonavir leads to a moderate increase AUC (in 1,5-3 times) the following preparations: amitriptyline, bupropion, venlafaxine, vinblastine, vincristine, haloperidol, hydrocodone, desipramine, dexfenfluramine, diazepam, disopyramide, dronabinol, zolpidem, imipramine, clarithromycin, clomipramine, clonazepam, the clorazepate dipotassium, maprotiline, maraviroc, mexiletine, methamphetamine, metoprolol, nortriptyline, oxycodone, ondansetron, paclitaxel, paroxetine, penbutolol, perphenazine, pindolol, prednisolone, dextropropoxyphene, risperidone, thioridazine, trazodone, tramadol, trimipramine, fluoxetine, flurazepam, chlorpromazine, estazolam, etoposide, ethosuximide.

    Ritonavir leads to a moderate increase or decrease AUC preparations: glyburide, glimepride, glipizide, diclofenac, ibuprofen, indomethacin, ifosfamide, lansoprazole, losartan, omeprazole, piroxicam, proguanil, propranolol, tolbutamide, flurbiprofen, cyclophosphamide.

    When used simultaneously with ritonavir, a reduction AUC following preparations: atovahon, hydromorphone, valproate semiotria, diphenoxylate, ketoprofen, ketorolac, clozapine, clofibrate, codeine, lamotrigine, loperamide, lorazepam, pethidine, methadone, metoclopramide, morphine, naproxen, oxazepam, propofol, temazepam, theophylline, phenytoin, ethinyl estradiol.

    Special instructions:

    During the treatment with ritonavir, in addition to specific immunological and virological tests, it is necessary to regularly perform clinical and biochemical blood tests.Taking ritonavir is accompanied by a change in the level of triglycerides, cholesterol, ALT, ACT, GGTP, CKK and uric acid. Appropriate laboratory tests should be performed prior to initiation of ritonavir treatment and at periodic intervals during or with clinical signs or symptoms occurring during treatment.

    Patients with haemophilia type A or B may have an increased bleeding probability (including spontaneous formation of cutaneous hematomas and hemarthrosis); after a specific treatment, ritonavir therapy can be continued under the constant monitoring of blood counts.

    In patients receiving antiretroviral therapy, there is a redistribution / accumulation of fat in the body with deposition in the back and neck ("buffalo buffalo"), a reduction in fat deposits on the face and extremities, enlargement of the mammary glands and "Cushingoid" appearance.

    Treatment with ritonavir in the form of monotherapy or in combination with saquinavir leads to a change in blood lipoproteins (a significant increase in triglycerides and total cholesterol). Determination of triglycerides and cholesterol should be performed before starting treatment with ritonavir and at periodic intervals intime for him. In case of violation of these indicators, appropriate therapy should be prescribed.

    In HIV-infected patients receiving combined antiretroviral therapy (ARVT), including ritonavir, the immune system recovery syndrome has been described. During the initial phase of ARVT, patients may exacerbate previously asymptomatic or residual opportunistic infections (including those caused by Micobacterium Avium, cytomegalovirus, pneumonia caused by Pneumocystis carinii, tuberculosis), which may require further monitoring and treatment.

    In patients receiving ritonavir as a monotherapy or in combination with other antiretroviral drugs, there are reactions from the liver: a 5-fold increase in "liver" transaminases, clinical manifestations of hepatitis and jaundice. The risk of an increase in transaminases is observed in patients who have hepatitis B or C. Therefore, patients with liver disease, changes in the activity of "hepatic" enzymes or hepatitis should be appointed ritonavir carefully.

    There are reports of a violation of liver function, and in several cases with a fatal outcome.The latter, as a rule, was observed in patients taking a large number of concomitant drugs and / or having a late stage of AIDS.

    In patients receiving ritonavir therapy, pancreatitis was observed, in some cases, with hypertriglyceridemia. Fatal cases are reported. In patients at a late stage of AIDS, the risk of increased triglycerides and pancreatitis increases. In the presence of characteristic clinical symptoms (nausea, vomiting, abdominal pain) or changes in laboratory parameters (elevated levels of lipase or amylase in the serum), the patient should be examined and, if pancreatitis is confirmed, ritonavir therapy should be discontinued.

    When taking ritonavir, some patients experienced an elongation of the interval PQ (PR). Cases of atrioventricular blockade development are described. I, II, III degrees. Caution should be exercised in prescribing ritonavir to patients with cardiac conduction abnormalities. The risk of conduction disturbances may be increased in patients with organic heart diseases, including coronary heart disease, cardiomyopathy, and with simultaneous administration of ritonavir and drugs that extend the interval PQ (including calcium channel blockers, beta-blockers, digoxin and atazanavir), especially if they are metabolized by isoenzyme CYP3A. Careful monitoring of the condition of such patients is necessary.

    Reported on the first emerging diabetes mellitus, weighting of existing diabetes mellitus and hyperglycemia in HIV-infected patients receiving protease inhibitor therapy. Some patients needed the appointment or correction of insulin dose or hypoglycemic drugs for oral administration to treat these conditions. In some cases, diabetic ketoacidosis developed. Sometimes hyperglycemia persisted even after the withdrawal of protease inhibitors. The causal relationship between these phenomena and protease inhibitor therapy has not been established.

    Caution should be exercised when ritonavir is used concomitantly with certain inhaled or intranasal glucocorticosteroid preparations. Systemic corticosteroid effects, including Cushing's syndrome and suppression of adrenal function, have been described with simultaneous administration of ritonavir with inhaled or intranasal fluticasone propionate. The development of similar symptoms in the joint use of ritonavir with other inhalationglucocorticosteroids, which are metabolized similarly to fluticasone (such as budesonide), can not be ruled out.

    Metabolism of HMG-CoA reductase inhibitors simvastatin and lovastatin strongly depends on isoenzyme CYP3A, in this regard, the joint appointment of ritonavir with simvastatin and lovastatin is not recommended because of the increased risk of myopathy, including rhabdomyolysis. Care should also be taken to reduce doses with simultaneous administration of atorvastatin and rosuvastatin, which are metabolized CYP3A4 to a lesser extent.

    The antagonist alfa1-adrenoceptor alfuzosin It is not recommended to appoint simultaneously with ritonavir because of a possible significant increase in the effects of alfuzosin.

    There are reports of the development of toxic hepatitis and hepatic decompensation with lethal outcomes while taking tipranavir and ritonavir at a dose of 200 mg. Caution should be exercised while prescribing these drugs to patients with chronic hepatitis B or C.

    With simultaneous use with ritonavir, plasma concentrations of some sedative drugs (clorazepate, diazepam, estazolam, flurazepam,midazolam and triazolam), so the risk of excessive sedation and respiratory depression increases.

    Effect on the ability to drive transp. cf. and fur:Given the possible side effects of the drug (drowsiness, dizziness), it is recommended to use caution when driving vehicles and engaging in other potentially dangerous activities that require increased concentration and speed of psychomotor reactions.
    Form release / dosage:Capsules, 100 mg.
    Packaging:

    60 capsules in a can of polymer, sealed with aluminum foil, with a screw cap that has a device that prevents children from opening the can.

    The polymer can with the instruction for use in a polyethylene bag equipped with a lock of the type zip-lock, and in a pack of cardboard. The jar inside the pack is covered with a cooling gel packaged in plastic bags and foam.

    At packing on Open Company "MAKIZ-PHARMA" or Open Company "Skopinsky pharmaceutical factory"

    The polymer can, together with the instructions for use, is placed in a pack of cardboard.

    Storage conditions:

    Store in a dry, dark place at a temperature of 2 to 8 ° C.

    Keep out of the reach of children.

    Shelf life:

    18 months.

    When stored from 8 to 25 ° C use within 30 days.

    Do not use after the expiry date printed on the package.
    Terms of leave from pharmacies:On prescription
    Registration number:LS-002290
    Date of registration:13.04.2012 / 22.11.2016
    Expiration Date:Unlimited
    The owner of the registration certificate:Heterose Labs LimitedHeterose Labs Limited India
    Manufacturer: & nbsp
    Representation: & nbspHeterose Labs LimitedHeterose Labs LimitedIndia
    Information update date: & nbsp25.12.2016
    Illustrated instructions
      Instructions
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