Giacavi - instructions for use, dose, side effects, contraindications

Active substanceРусосолитинибРусосолитиниб

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Jakavi®

pills inwards

Novartis Pharma AG Switzerland

Jakavi®

pills inwards

Novartis Pharma AG Switzerland

Dosage form: & nbsppills

Composition:

1 tablet contains:

active substance: rutzolitinib phosphate (corresponding to the ratsolitinib base) - 6.60 (5) mg, 19.80 (15) mg and 26.40 (20) mg;

Excipients: lactose monohydrate 71.45 mg, 214.35 mg and 285.80 mg, microcrystalline cellulose 68.35 mg, 205.05 mg, 273.40 mg; sodium carboxymethyl starch (type A) 4.80 mg, 14.40 mg, 19.20 mg; giprolose - 3.20 mg, 9.60 mg, 12.80 mg; povidone - 3.20 mg, 9.60 mg, 12.80 mg; silicon colloidal dioxide - 1.60 mg, 4.80 mg, 6.40 mg; magnesium stearate - 0.80 mg, 2.40 mg and 3.20 mg.

Description:

Tablets 5 mg:

Round tablets white or almost white without chamfer. On one side is engraved "L5", another - "NVR".

Tablets 15 mg:

Oval biconvex tablets white or almost white without chamfer. On one side is engraved "L15", another - "NVR".

Tablets of 20 mg:

Oblong biconvex tablets white or almost white without chamfer. On one side is engraved "L20", another - "NVR".

Pharmacotherapeutic group:Antitumor agent - protein kinase inhibitor

ATX: & nbsp

L.01.X.E Protein kinase inhibitors

L.01.X.E.18 Русосолитиниб

Pharmacodynamics:

Mechanism of action

Ruxolitinib is a selective inhibitor JAK-Kinase (Janus Associated Kinases - JAKs), JAK1 and JAK2. These kinases contribute to the transmission of signals from numerous cytokines and growth factors that play an important role in hematopoiesis and the function of the immune system.

Activated JAK-kinase, acting on cytokine receptors, activate STATproteins (STATs) (signal carriers and transcription activators) that, as a result of activation, are transported into the nucleus and modulate gene expression. Dysregulation of the path JAK-STAT is associated with some types of malignant neoplasms and an increase in proliferation and survival of malignant cells.

Myelofibrosis and true polycythemia - myeloproliferative diseases associated with the dysregulation of the signaling pathway JAK1 and JAK2. It is believed that the basis for dysregulation is a high level of circulating cytokines that activate the JAK-STAT pathway, leading to pathological functional mutations, such as JAK2V617F, and to suppression of negative regulatory mechanisms. In patients with myelofibrosis, dysregulation of the JAK signaling pathway is detected, regardless of the presence of the JAK2V617F mutation. Activating mutations of the signal pathway JAK2 (V617F or exon 12) are detected in> 95% of patients with true polycythemia.Ruksolinib suppresses holding JAK-STAT signal and cell proliferation in cytokine-dependent hematologic models, and in Ba / F3 cytokine-independent cells (due to expression of a mutant protein JAK2V617F) with a value of 50% inhibitory concentration (IC₅₀) in the range of 80-320 nmol. In studies of JAK2V617F-pozitivnyx animal models of hematological when applying ruksolitiniba inwardly at doses do not cause myelosuppression effects, it prevents the development of splenomegaly, selectively reduces the number of mutant JAK2V617F- spleen cells and the concentration of circulating cytokines (e.g., tumor necrosis factor-alpha (TNF-alpha) and interleukin-6 (IL-6), and resulted in a significant increase in survival time.

Pharmacodynamics

Ruxolitinib inhibits cytokine-induced phosphorylation STAT3 whole blood in both healthy volunteers and in patients with myelofibrosis and polycythemia vera. Maximum inhibition of STAT3 phosphorylation ruksolitinibom achieved by 2 hours after application with recovery to baseline levels after 8 hours in healthy volunteers and in patients with myelofibrosis, indicating the absence of accumulation as a starting material, and its metabolites.

Initial increase in the concentration of markers of the inflammatory process, such as TNF-alpha, IL-6 and C-reactive protein (CRP) observed in patients with myelofibrosis decreases after treatment with rutzolithinib.

In patients with myelofibrosis, there was no evidence of resistance to the pharmacodynamic effects of rutzolitinib. Similarly, in patients with true polycythemia, an initial increase in the concentration of markers of the inflammatory process was observed, which decreased after treatment with rutzolithinib.

In the clinical study there was no lengthening QT/QTc interval when using rutzolitinib once in supra-therapeutic doses (200 mg), which indicates the absence of influence on repolarization myocardium.

Pharmacokinetics:

Absorption

Ruxolitinib belongs to the first class of molecules in the biopharmaceutical classification system (Biopharmaceutical Classification System) with high permeability, high solubility and rapid dissolution. In clinical trials rosolitinib quickly absorbed after oral administration with time reaching the maximum concentration (C_max) is approximately 1 hour. The absorption of rutzolitinib is 95% or more. Average C_maxand the area under the concentration-time curve (AUC) increases proportionally in the dose range of 5 to 200 mg. When using rutzolitinib simultaneously with high-fat food, clinically insignificant changes in the pharmacokinetics of rutzolitinib were observed: mean C_max slightly decreased (24%), while the AUC remained practically unchanged (rising by 4%).

Distribution

The average volume of distribution in equilibrium state was 72 l in patients with myelofibrosis with interindividual variability of 29.4% and 75 l in patients with true polycythemia, Interindividual variability in these patients was 22.6%.

In clinically significant concentrations, the association of rutzolithinib with proteins in vitro (mainly with albumin) was approximately 97%. In a study in animals, it was shown that rosolitinib does not penetrate the blood-brain barrier.

Biotransformation / metabolism

Ruxolitinib is a substrate of isoenzyme CYP3A4. After receiving the drug into the blood circulating 60% ruksolitiniba unchanged. 2 main active metabolite ruksolitiniba identified in human blood, constituting 25% and 11% AUC.

The pharmacological activity of rutzolitinib is 18% of the activity of its metabolites. In clinically significant concentrations rosolitinib does not inhibit isozymes CYP1A2, CYP2B6, CYP2C8, CYP2C9, CYP2C19, CYP2D6 or CYP3A4 and is a potent inducer isozymes CYP1A2, CYP2B6 and CYP3A4.

Elimination

After administration of a single dose of radiolabelled ruksolitiniba majority (74%) of the radioactivity in the urine was determined (output of the kidneys), and 22% is excreted through the intestines. The unchanged substance was less than 1% of the total withdrawn drug. The half-life of rutzolitinib is approximately 3 hours.

Linearity / nonlinearity of pharmacokinetics

Pharmacokinetics ruksolitiniba varies proportionally administered (single, multiple) doses.

Pharmacokinetics in selected patient groups

The influence of age, sex or race

No significant differences in the pharmacokinetics ruksolitiniba based on gender and race. The clearance of rutzolitinib in patients with myelofibrosis is 17.7 l / h in women and 22.1 l / h in men (interindividual variability is 39%).

In patients with polycythemia vera ruksolitiniba clearance was 12.7 L / h (interindividual variability of 42%); revealed no influence of gender, age or race on the clearance of the ingestion of the drug.

Patients aged ≤18 years

The efficacy and safety of the Giacavi® preparation in patients younger than 18 years of age is not established.

Impaired renal function

AUC metabolites of rutzolitinib increases with increasing severity of renal dysfunction and reaches significant values in patients with terminal stage of renal failure who need hemodialysis. Русосолитиниб not output by dialysis. For patients with severe and terminal stages of renal failure (QC less than 30 mL / min), dose adjustment is recommended rusolitinib.

Impaired liver function

AUC rutzolitinib increased in patients with mild, moderate and severe hepatic impairment by 87%, 28% and 65%, respectively, compared with normal liver function, and there is no apparent correlation with the severity of liver function impairment as determined by the Child-Pugh scale. The final half-life is prolonged in patients with impaired liver function in comparison with healthy volunteers (4.1-5.0 h versus 2.8 h). In patients with impaired liver function, a dose reduction of rutzolitinib is recommended.

Indications:

Myelofibrosis

Treatment of patients with myelofibrosis, including primary myelofibrosis and secondary myelofibrosis, developed due to true polycythemia and essential thrombocythemia.

Polycythemia true

Treatment of patients with true polycythemia, resistant to hydroxyurea drugs or with their intolerance.

Contraindications:

- Hypersensitivity to ratsolitinib or any other component of the drug;

- pregnancy and the period of breastfeeding;

- The age is under 18 years.

Carefully:

Caution should be exercised when using Jakavi ® in patients with violation of the function of the kidneys of a serious degree, including those on hemodialysis or receiving a hemodialysis procedure, in patients with a violation of the liver, in patients with severe infectious diseases in the acute stage, also in patients with thrombocytopenia, anemia and neutropenia, in patients with lactase deficiency, lactose intolerance, glucose-galactose malabsorption.

Caution should be exercised when using the Jakavi ® preparation simultaneously with potent inhibitors of the isoenzyme CYP3A4.

Pregnancy and lactation:

The drug Giacavi® is contraindicated for use during pregnancy and breastfeeding.

Patients with saved reproductive potential It is recommended to use reliable contraceptive methods during therapy with Giacavi®. If pregnancy occurs during therapy with Giacavi®, the benefit / risk ratio should be carefully assessed for each individual patient, taking into account the latest known data on the embryotoxicity of the drug.

Studies of the influence of rutzolitinib on embryo-fetal development of teratogenic phenomena have not been revealed. However, the phenomena of embryo and fetotoxicity (an increase in postimplantation loss and a decrease in fetal body mass) are noted.

In preclinical studies, russoleinib and / or its metabolites were found in the milk of lactating animals at concentrations 13 times higher than the concentration in the blood plasma of the mother. It is not known whether the saline is secreted into human breast milk.

There is no data on the effect of rutzolitinib on fertility in humans. In studies in animals, no effect on fertility was found.

Dosing and Administration:

The drug Giacavi^® take inside, regardless of the time you eat.

Initial dose

The recommended initial dose of the drug Giacavi ® in the treatment of patients with myelofibrosis is 15 mg 2 times a day for patients with a platelet count of 100-200 x 10⁹/ l; and 20 mg twice daily for patients with platelet count> 200 x 10⁹/ l.

The maximum recommended initial dose in patients with platelet counts 50-100 x 10⁹/ l is 5 mg 2 once a day inside, followed by correction dose that is performed with caution (see Table 1).

Table 1. The recommended initial dose of Jakavi® in the treatment of patients with myelofibrosis

Number of platelets	Initial dose
> 200 x 10⁹	20 mg 2 times a day
100-200 x 10⁹	15 mg 2 times a day
50 - less than 100 x 10⁹	5 mg 2 times a day

The recommended initial dose of Giacavi® in the treatment of patients from true polycythemia is 10 mg 2 times a day inside.

Dose selection

Dose of Jakavi® is adjusted based on the safety and effectiveness of the treatment. Treatment of patients with myelofibrosis should be suspended if a platelet count is less than 50 x 10⁹/ l or with a decrease in the absolute number of neutrophils less than 0,5x 10⁹/ l.

After the restoration of the platelet count and neutrophils above these values, the use of the Giacavi® preparation can be resumed at a dose of 5 mg twice a day, a further gradual increase in the dose with a careful control of the amount shaped blood elements (see Table 2).

Table 2. Myelofibrosis: the maximum dose of the drug Giacavi® with the resumption of therapy after suspension of its use due to thrombocytopenia (for patients with a platelet count of 100 x 10⁹/ l and more to the beginning of therapy)

Number of platelets	The maximum dose of the drug Giacavi® with the resumption of therapy
125 x 10⁹/ l and more	20 mg 2 times a day
100 - less than 125 х 10⁹/ l	15 mg 2 times a day
75 - less than 100 х 10⁹/ l	10 mg 2 times a day for 2 weeks minimum; further, with the preservation of the number of platelets, it is possible to increase to 15 mg 2 times a day
50 - less than 75 x 10⁹/ l	5 mg 2 times a day for 2 weeks minimum; further, if the number of platelets is maintained, it is possible to increase to 10 mg 2 times a day
less than 50 x 10⁹/ l	Suspension of use

* When resuming the use of the drug, Giacavi® should be started with a dose of at least 5 mg twice a day below that used before the suspension of its use.

It is recommended to reduce the dose of the drug with a decrease in the number of platelets less than 100 x 10⁹/ l, in avoid the suspension of therapy due to developed thrombocytopenia (see Table 3).

Table 3. Myelofibrosis: the recommended dose of the drug Giacavi® (for patients with a platelet count of 100 x 10⁹/ l and more to the top therapy)

Dose, used before the decrease in the number of platelets

Number of platelets

25 mg

2 times a day

20 mg

2 times a day

15 mg

2 times a day

10 mg

2 times a day

5 mg

2 times a day

Reduced dose

100 - less than 125 х 10⁹/ l

20 mg

2 times a day

15 mg

2 times a day

Without changes

75 - less than 100 х 10⁹/ l

10 mg

2 times a day

10 mg

2 times a day

10 mg

2 times a day

Without changes

50 - less than 75 х 10⁹/ l

5 mg

2 times a day

5 mg

2 times a day

5 mg

2 times a day

5 mg

2 times a day

Without changes

less than 50 x 10⁹/ l

Suspension of use

FROMIt is advisable to consider the possibility of dose reduction with a decrease in hemoglobin concentration in blood <120 g / l in patients with true polycythemia, with a decrease in hemoglobin concentration in the blood <100 g / l - a dose reduction is recommended.

Treatment should be suspended with a decrease in hemoglobin concentration in the blood <80 g / l in patients with true polycythemia (see Table 4).

Table 4. Dose reduction in patients with true polycythemia

The concentration of hemoglobin and / or the number of platelets	Recommended dose
The concentration of hemoglobin ≥ 120 g / l and the number of platelets ≥ 100 x 10⁹/ l	Dose correction is not required
The concentration of hemoglobin 100 - <120 g / l and the number of platelets 75 <100 x 10⁹/ l	Consider the possibility of reducing the dose of the drug, in order to avoid the suspension of therapy due to developing anemia and thrombocytopenia.
Concentration of hemoglobin 80 - <100 g / l OR the number of platelets is 50 - <75 x 10⁹/ l	Reduction of the dose by 5 mg 2 times a day. In patients taking 5 mg 2 times a day, a dose reduction of up to 5 mg 1 time per day is recommended.
Concentration of hemoglobin <80 g / l OR number of platelets <50 x 10⁹/ l	Suspension of use

AT and if the amount of platelets and neutrophils in patients with myelofibrosis or hemoglobin concentration in patients with true polycythemia is sufficient, the dose of the drug Giacavi^® can be increased as much as 5 mg 2 times a day, up to a maximum dose of 25 mg 2 times a day. Do not increase the initial dose of the drug in during the first 4 weeks of treatment, and then no more often than once in 2 weeks.

The maximum dose of the drug Giacavi * is 25 mg 2 times a day inside.

In case of missed intake of the next dose of the drug, the patient should not take an additional dose, the next dose should be taken at the usual prescribed time.

Treatment with the drug is continued as long as the therapeutic effect remains.

Monitoring Recommendations

Counting blood cells: Before calculating the Giacavi® preparation, the number of blood cells should be counted.

Absolute number of blood elements should be monitored every 2-4 weeks during the selection of the dose of rutzolitinib and further on the clinical indications.

Correction of the dose while using powerful inhibitors of the isoenzyme CYP3A4 or fluconazole.

In the case of simultaneous application with potent inhibitors of the isoenzyme CYP3A4 (clarithromycin, indinavir, itraconazole, ketoconazole, lopinavir / ritonavir, nelfinavir, ritonavir, saquinavir, telithromycin, voriconazole, grapefruit juice) or with double moderate inhibitors of CYP2C9 and CYP3A4 isoenzymes (for example, fluconazole), the total daily dose of the Giacavi® preparation should be reduced by approximately 50%, by decreasing the daily dose divided into 2 doses, or by appropriately reducing the frequency of administration to 1 time per day (in the case that such a regimen is possible). It should avoid simultaneous use of the drug with fluconazole at a dose of more than 200 mg per day.

More frequent monitoring of hematological parameters and clinical signs and symptoms associated with adverse reactions to the Giacavi® preparation is recommended at the beginning of simultaneous use of potent inhibitors of the CYP3A4 isoenzyme or double moderate inhibitors of the CYP2C9 and CYP3A4 isoenzymes (see Table 5).

Table 5. Correction of the dose while using powerful inhibitors of the CYP3A4 isoenzyme or double moderate inhibitors of CYP2C9 isoenzymes and CYP3A4

The use of the drug Giacavi® simultaneously with the powerful inhibitors of CYP3A4	Recommended dose adjustment
Initial dose in patients with myelofibrosis and platelet count
100 x 10⁹/ l and more	10 mg 2 times a day
50 - less than 100 х 10⁹/ l	5 mg once a day
Initial dose in patients with true polycythemia	5 mg 2 times a day
Patients taking the drug at a dose established on the basis of safety and effectiveness of the treatment:
≥10 mg 2 times a day	Dose reduction by 50%
5 mg 2 times a day	5 mg once a day
5 mg once a day	The use of powerful inhibitors of CYP3A4 or the preparation of Giacavi® should be stopped for the time of the use of powerful inhibitors of CYP3A4

ABOUTevent of a group of patients

Impaired renal function

In patients with myelofibrosis and violation of the function of heavy-colored nights (QC less than 30 ml / min), the recommended initial dose based on the number of platelets should be reduced by approximately 50%. The recommended initial dose for treatment of patients with true polycythemia and impaired renal function of severe degree is 5 mg 2 times a day inwards.

Patients with impaired renal function of severe degree receiving the preparation of Giacavi ® should be carefully observed, if necessary, the dose of the drug should be reduced in order to avoid the development of unwanted drug reactions.

There are limited data on the use of rutzolithinib in patients with terminal stage of renal failure on hemodialysis.In this category of patients with myelofibrosis, treatment should start with a single dose of 15 mg or 20 mg (based on the number of platelets) followed by single doses only after each hemodialysis and with a thorough assessment of the benefit / risk ratio.

In patients with true polycythemia and terminal stage of renal failure on hemodialysis treatment should start with a single dose of 10 mg after hemodialysis procedures only on the day of its conduct with careful monitoring of the condition and evaluation of the benefit / risk ratio (see Table 6).

Table 6. The recommended dose of Jakavi® in patients with impaired function kidneys

Degree of severity of renal dysfunction	Number of platelets	Recommended initial dose
Patients with myelofibrosis: Average (QC 30-59 ml / min) or Heavy (SC 15-29 ml / min)	More than 150 x 10⁹/ l	Dose correction is not required
	100x10⁹/ l - 150 x 10⁹/ l	10 mg 2 times a day
	50 - less than 100 х 10⁹/ l	5 mg once a day
	Less than 50 x 10⁹/ l	Suspension of use
Patients with true polycythemia: Average (QC 30-59 ml / min) or Heavy (SC 15-29 ml / min)	Any	5 mg 2 times a day

Hhepatic function

In patients with impaired hepatic function, the recommended initial dose, based on the number of platelets, should be reduced by approximately 50%. Patients with diagnosed severe liver dysfunction who receive Giacavi ® should be carefully observed, if necessary, the dose of the drug should be reduced to avoid the development of unwanted drug reactions (see Table 7).

Table 7. Recommended dose of Giacavi® in patients with impaired hepatic function

Degree of severity of liver dysfunction	Number of platelets	Recommended initial dose
Patients with myelofibrosis: mild, moderate or severe (Child-Pugh class A, B or C)	More than 150 x 10⁹/ l	Dose correction is not required
	100 х10⁹/ l - 150 x 10⁹/ l	10 mg 2 times a day
	50 - less than 100 x10⁹/ l	5 mg once a day
	Less than 50 x 10⁹/ l	Suspension of use
Patients with true polycythemia: mild, moderate or severe (Child-Pugh class A, B or C)	Any	5 mg 2 times a day

Patients aged ≤ 18 years

The safety and efficacy of Giacavi® in patients <18 years of age have not been established.

Patients ≥65 years of age

Correction of the dose is not required.

Side effects:

Undesirable phenomena (AEs), noted when the drug is used during clinical research

AEs are grouped according to the classification of organs and systems of MedDRA organs, within each group are listed in order of decreasing frequency of occurrence.

The following criteria were used to estimate the frequency (according to the classification of the World Health Organization (WHO)): very often (≥1 / 10); often (≥1 / 100, <1/10); infrequently (≥1 / 1000, <1/100); rarely (≥1 / 10000, <1/1000); very rarely (<1/10000).

In clinical studies, the severity of AE was assessed according to the General terminology of criteria for adverse events *

Myelofibrosis

Infectious and parasitic diseases: very often - urinary tract infections, particularly cystitis, urosepsis, pyuria, kidney infections; often - Herpes zoster; infrequently - tuberculosis.

Violations from the blood and lymphatic system: very often - anemia (including 3 degrees of severity (> 80 - 65 g / l), 4 degrees of severity (<65 g / l)) thrombocytopenia, neutropenia, bleeding, including gastrointestinal bleeding, intracranial hemorrhage, subcutaneous hemorrhage, bruising, including bruises, ecchymoses, hematomas, including periorbital hematoma, increased tendency with bruises, petechiae, purpura; often - thrombocytopenia of the 4th degree of severity (<25 x 10⁹/ l), the third degree of severity (50-25 x 10⁹/ l), neutropenia of the 4th degree of severity (<0.5x10⁹/ l), the third degree of severity (<1- 0.5 x 10⁹/ l).

Disorders from the metabolism and nutrition: very often - hypercholesterolemia (1, 2 degrees of severity), weight gain.

Disorders from the nervous system: very often - dizziness, vertigo, headache; often - disturbance of balance; infrequently - Ménière's disease.

Disorders from the gastrointestinal tract: often - Flatulence.

Disorders from the liver and biliary tract: very often - increased ALT activity, increased activity ACT; often - increased ALT activity of the third degree (5-20 times higher than normal).

With the use of the drug Giacavi ®, a report was received on the case of the development of progressive multifocal leukoencephalopathy (PML). If suspected development of PML should stop using the drug.

After discontinuation of therapy with Giacavi®, some patients with myelofibrosis experienced the following AEs: fever, respiratory distress syndrome, arterial hypotension, disseminated vi- trus-vascular coagulation syndrome (DIC syndrome), or multiple organ failure.

True polycythemia

Infectious and parasitic diseases: often - nasopharyngitis, herpes zoster, urinary tract infections.

Violations from the blood and lymphatic system: very often - anemia, thrombocytopaedy; often - thrombocytopaedy of the 3rd degree of severity (50-25 x 10⁹/l); infrequently anemia 3 severity (> 80-65 g / l), 4 degrees of severity (<65 g / l), thrombocytopaedy of the 4th degree of severity (<25 x 10⁹/l).

Disorders from the metabolism and nutrition: very often - hypercholesterolemia (1,2 degrees of severity), hypertriglyceridemia (1 degree of severity); often - increase in body weight.

Disorders from the nervous system: very often - headache, dizziness.

Disturbances from the respiratory system, chest markers and mediastinum: very often - shortness of breath, including number of dyspnoea with physical exertion; often - cough, nosebleeds.

Disorders from the gastro-intestinal tract: very often - abdominal pain, diarrhea; often - constipation, nausea.

Disorders from the liver and bile ducts: very often - PIncreased ALT activity, increased ACT activity; infrequently - rise ALT activity of the 3rd degree (5-20 times higher norms).

Disturbances from the musculoskeletal and connective tissue: very often - muscle spasms; often - Arthralgia.

Vascular disorders: often - marked increase in arterial pressure.

General disorders and disorders in place introduction: very often - fatigue; often - asthenia, edema, including peripheral edema.

* - classification of severity of undesirable phenomena

1 - mild degree

2 - medium degree

3 - heavy degree

4 - extremely severe (life-threatening) degree

If any of the instructions specified in the instruction side effects are aggravated, or you notice any other side effects not listed in the instructions, inform the doctor about it.

Overdose:

Symptoms: The use of rutzolitinib once in a dose of up to 200 mg was tolerated satisfactorily. Exceeding the recommended doses was associated with increased myelosuppression, which was manifested by leukopenia, anemia and thrombocytopenia.

Treatment: with the development of adverse events associated with overdose of the drug, it is necessary to apply appropriate supportive treatment. It is expected that hemodialysis does not help accelerate the removal of rutzolitinib from the body. Antidote to ratsolitinibu is unknown.

Interaction:

Remedies that can change the concentration of rusolitnib in the blood plasma

Powerful inhibitors of isoenzyme CYP3A4: in healthy volunteers, the administration of ketoconazole, a potent inhibitor of the isoenzyme CYP3A4, at a dose of 200 mg twice daily for 4 days, resulted in an increase in the AUC of ratsolitinib by 91% and an elongation of the nil elimination period from 3.7 h to 6.0 h.

In the case of use with potent inhibitors of isoenzyme CYP3A4, the total daily dose of rutzolitinib should be reduced by approximately 50%.

Patients should be carefully monitored to reduce the number of blood cells, if necessary, further correction of the dose is recommended based on efficacy and safety data.

Weak and moderate inhibitors isoenzyme CYP3A4: reception of erythromycin, a moderate isoenzyme inhibitor CYP3A4. in a dose of 500 mg twice a day for healthy volunteers for 4 days led to an increase of 27% AUC rusolitinib.

Dose correction is not required when the Jakavi drug is used concomitantly with weak or moderate isofermine inhibitors CYP3A4 (including erythromycin). At the beginning of therapy with rutzolitinib simultaneously with moderate inhibitors of isofermene CYP3A4 It requires careful monitoring of patients and evaluation of the number of blood cells.

Double Moderate Inhibitors isozymes CYP2C9 and CYP3A4: on Based on the results of modeling of drug interactions, an increase is expected AUC rutzolitinib in 2,9 and 4,3 times with simultaneous application with fluconazole in doses of 200 mg and 400 mg respectively. The dose of the drug should be reduced to 50% with simultaneous application with double-moderated inhibitors of isoenzymes CYP2C9 and CYP3A4. Avoid simultaneous use of rutzolitinib with fluconazole at a dose exceeding 200 mg per day.

Inductors of isoferment CYP3A4: at the beginning treatment simultaneously with isofermeng inducers CYP3A4 dose adjustment is not recommended. If the effectiveness of therapy with the drug Giacavi® decreases with simultaneous therapy with inducers of isoenzyme CYP3A4 it is necessary to consider a gradual increase in the dose of Jakavi®.

In healthy volunteers who received rifampicin, a powerful isoenzyme inducer CYP3A4, in a dose of 600 mg once a day for 10 days AUC of the drug Giacavi® after a single dose was reduced by 71% and the half-life decreased from 3.3 hours to 1.7 hours. The relative amount of active metabolites increased with respect to the starting material.

P-glyco-protein and other carrier proteins: It is not recommended to correct the dose when using the drug Giacavi® concomitantly with drugs interacting with P-glycoprotein and other carrier proteins.

Other studied drug interactions

Substrates CYP3A4: study the healthy volunteers demonstrated the absence of clinically significant pharmacokinetic interaction of rutzolithinib with midazolam (substrate isoenzyme CYP3A4).

Oral contraceptives: a study in healthy volunteers demonstrated the lack of influence of rutzolitinib on the pharmacokinetics of oral contraceptives containing ethinyl estradiol and levonorgestrel, in connection with which the effectiveness of oral contraceptives with this combination of active substances is not expected to decrease with simultaneous use with rutzolitinib.

Special instructions:

Reducing the number of blood elements

Treatment with Jakav® can lead to the development of hematological adverse reactions including thrombocytopenia, anemia and neutropenia. Before starting treatment with Giacavi ®, a general blood test should be performed.

Thrombocytopenia

In patients with a reduced number of platelets (<200 x 10⁹/ l) at the beginning of therapy approximately 2-fold increases the likelihood of thrombocytopenia during treatment with ratsolitinibom. In clinical studies in patients with myelofibrosis, grade 3 or 4 thrombocytopenia developed around the 8th week of therapy.

Thrombocytopenia, as a whole, is reversible and is usually corrected by a decrease in dose or a temporary discontinuation of the Giacavi® drug. The number of platelets was restored to values greater than 50 x 10⁹/ l for 14 days. However, in some cases transfusion of platelet concentrates may be required.

In patients with true polycythemia, thrombocytopenia was less frequent (24.5%) than in patients with myelofibrosis (69.8%). Thrombocytopenia of the 3rd and 4th degree of severity was noted in 5.54% of patients with true polycythemia and in 11.6% of patients with myelofibrosis.

Anemia

If anemia develops, a red blood cell transfusion may be required. In addition, it is necessary to assess the need for dose adjustment or discontinuation of treatment with Giacavi®. Approximately 50% of patients with myelofibrosis who participated in CI and received the preparation of Giacavi ®, and 37% of patients in the control group during the study required red blood cell transfusion.In patients receiving the preparation of Giacavi ®, the hemoglobin concentration reached the lowest possible level (by 15-20 g / L below the initial value) at the 8-12th week of therapy. Subsequently, the hemoglobin concentration gradually increased and remained at a level of 10 g / l below the baseline (before treatment). This trend was observed regardless of whether the patient received blood transfusion during therapy.

In patients with true polycythemia, anemia was less frequent (46.8%) than in patients with myelofibrosis (82.4%). Anemia of the 3rd and 4th degree of severity was noted in 1.8% of patients with true polycythemia and in 42.5% of patients with myelofibrosis.

Neutropenia

In patients with myelofibrosis, grade 3 and 4 neutropenia developed around the 12th week of therapy. In general, neutropenia (absolute number of neutrophils (ACHN) <0.5 x 10⁹/ l), in the case of its development, was reversible and corrected by the temporary withdrawal of the drug Jakavi®.

In patients with true polycythemia, neutropenia was noted in 2 patients, while one patient noted development of grade 4 neutropenia.

Bleeding

Bleeding (including intracranial hemorrhage,Gastrointestinal hemorrhage, subcutaneous hemorrhage, petechiae, purpura and other bleeding) were reported in 32.6% of patients receiving the Giacavi ® preparation. 65.3% of all bleeding were cases of development of subcutaneous hematomas, which were noted in 21.3% of patients. The incidence of bleeding of grade 3 and 4 was 4.7%. Cases of intracranial hemorrhage were noted in 1% of patients, gastrointestinal bleeding - in 5.0% of patients, bleeding due to other causes (including nasal bleeding, postoperative bleeding and hematuria) in 13.3% of patients receiving the drug Giacavi ®.

Infections

Patients treated with Giacavi® have been diagnosed with serious bacterial, mycobacterial, fungal, viral and other opportunistic infections. Before using Giacavi ®, the risk of developing serious infections. Patients receiving the Giacavi® preparation should be closely monitored to identify symptoms of infection and, if necessary, to begin appropriate treatment immediately.

In patients who received the preparation Giacavi ® about myelofibrosis, reported cases of tuberculosis. It should be remembered about the possibility of developing an active or latent form of tuberculosis. Before starting therapy, the drug should be examined by the patient to identify an active or latent form of tuberculosis in accordance with local clinical guidelines.

Do not start therapy with the drug until the resolution of a severe active infection. In patients with chronic viral hepatitis B receiving the preparation of Giacavi, there was an increase in the titer of the DNA of the hepatitis B virus with or without an accompanying increase in activity ACT and ALT. The effect of Jakavi® on the replication of hepatitis B virus DNA is unknown. Treatment and monitoring of patients with chronic viral hepatitis B should be carried out in accordance with generally accepted standards of clinical practice.

Shingles Herpes

Before using the Giacavi® drug, the physician should be trained in the timely detection of early symptoms of herpes zoster, reporting the need for early treatment.

Progressive multifocal leukoencephalopathy

With the use of the drug Giacavi, a case report was received PML.

If suspected development of PML, discontinue use of Giacavi ® before the deletion of this diagnosis.

Malignant neoplasms of the skin, with the exception of melanoma

With the use of the drug Giacavi®, cases of development of malignant tumors of the skin were reported, with the exception of melanoma, including basal cell and squamous cell carcinoma, as well as carcinomas from Merkel cells. In most cases, such patients had a history of long-term treatment with hydroxyurea preparations or previously had malignant skin lesions, with the exception of melanoma, or precancerous skin lesions. The causal relationship with the use of rutzolitinib was not established. It is recommended to conduct periodic examination of skin in patients with an increased risk of developing malignant skin tumors.

Change in lipid profile

An increase in the concentration of lipids, including an increase in the concentration of total cholesterol, high and low-density lipoproteins and triglycerides associated with treatment with Giacavi®, has been noted.Recommended control lipid profile and correction of dyslipidemia in accordance with local clinical recommendations.

The "cancellation" syndrome

After discontinuing therapy with Giacavi, symptoms of myelofibrosis (such as fatigue, bone pain, fever, pruritus, night sweats, symptomatic splenomegaly, and weight loss) may return. In clinical trials, the overall scale of symptoms of myelofibrosis gradually returned to baseline values within 7 days after discontinuation of use.

Effect on the ability to drive transp. cf. and fur:

Studies of the effect of the drug on the ability to drive vehicles and / or mechanisms were not carried out. Given the possibility of developing some side effects when taking Jakavi ® (dizziness), patients should be careful when driving vehicles and engaging in other potentially hazardous activities that require increased concentration.

Form release / dosage:

Tablets, 5 mg, 15 mg and 20 mg.

Packaging:

For 14 tablets per blister PVC / PCTFE / Al.

4 blisters together with instructions for use in a cardboard box.

Storage conditions:

Store at a temperature not exceeding 30 ° C.

Keep out of the reach of children.

Shelf life:

3 years.

Do not use after the expiration date.

Terms of leave from pharmacies:On prescription

Registration number:LP-002028

Date of registration:21.03.2013 / 09.01.2017

Expiration Date:21.03.2018

The owner of the registration certificate:Novartis Pharma AGNovartis Pharma AG Switzerland

Manufacturer: & nbsp

NOVARTIS PHARMA STEIN, AG Switzerland

Representation: & nbspNOVARTIS PHARMA LLCNOVARTIS PHARMA LLC

Information update date: & nbsp25.04.2017

Illustrated instructions

Instructions

Jakavi® (Jaakafi®)