Quest for the right Drug
ג'קאבי 10 מ"ג JAKAVI 10 MG (RUXOLITINIB AS PHOSPHATE)
תרופה במרשם
תרופה בסל
נרקוטיקה
ציטוטוקסיקה
צורת מתן:
פומי : PER OS
צורת מינון:
טבליה : TABLETS
עלון לרופא
מינוניםPosology התוויות
Indications תופעות לוואי
Adverse reactions התוויות נגד
Contraindications אינטראקציות
Interactions מינון יתר
Overdose הריון/הנקה
Pregnancy & Lactation אוכלוסיות מיוחדות
Special populations תכונות פרמקולוגיות
Pharmacological properties מידע רוקחי
Pharmaceutical particulars אזהרת שימוש
Special Warning עלון לרופא
Physicians Leaflet
Adverse reactions : תופעות לוואי
4.8 Undesirable effects Summary of the safety profile Myelofibrosis The most frequently reported adverse drug reactions were thrombocytopenia and anaemia. Haematological adverse drug reactions (any Common Terminology Criteria for Adverse Events [CTCAE] grade) included anaemia (83.8%), thrombocytopenia (80.5%) and neutropenia (20.8%). Anaemia, thrombocytopenia and neutropenia are dose-related effects. The three most frequent non-haematological adverse drug reactions were bruising (33.3%), other bleeding (including epistaxis, post-procedural haemorrhage and haematuria) (24.3%) and dizziness (21.9%). The three most frequent non-haematological laboratory abnormalities identified as adverse reactions were increased alanine aminotransferase (40.7%), increased aspartate aminotransferase (31.5%) and hypertriglyceridaemia (25.2%). In phase 3 clinical studies in MF, neither CTCAE grade 3 or 4 hypertriglyceridaemia or increased aspartate aminotransferase, nor CTCAE grade 4 increased alanine aminotransferase or hypercholesterolaemia were observed. Discontinuation due to adverse events, regardless of causality, was observed in 30.0% of patients. Polycythaemia vera The most frequently reported adverse drug reactions were anaemia and increased alanine aminotransferase. Haematological adverse reactions (any CTCAE grade) included anaemia (61.8%), thrombocytopenia (25.0%) and neutropenia (5.3%). Anaemia and thrombocytopenia CTCAE grade 3 or 4 were reported in 2.9% and 2.6% of the patients, respectively. The three most frequent non-haematological adverse reactions were weight gain (20.3%), dizziness (19.4%) and headache (17.9%). The three most frequent non-haematological laboratory abnormalities (any CTCAE grade) identified as adverse reactions were increased alanine aminotransferase (45.3%), increased aspartate JAK API May24 V7 EU SmPC April 2024 aminotransferase (42.6%), and hypercholesterolaemia (34.7%). No CTCAE grade 4 increased alanine aminotransferase or hypercholesterolaemia, and one CTCAE grade 4 increased aspartate aminotransferase were observed. Discontinuation due to adverse events, regardless of causality, was observed in 19.4% of patients. Acute GvHD The most frequently reported overall adverse drug reactions were thrombocytopenia, anaemia and neutropenia. Haematological laboratory abnormalities identified as adverse drug reactions included thrombocytopenia (85.2%), anaemia (75.0%) and neutropenia (65.1%). Grade 3 anaemia was reported in 47.7% of patients (grade 4 not applicable per CTCAE v4.03). Grade 3 and 4 thrombocytopenia were reported in 31.3% and 47.7% of patients, respectively. The three most frequent non-haematological adverse drug reactions were cytomegalovirus (CMV) infection (32.3%), sepsis (25.4%) and urinary tract infections (17.9%). The three most frequent non-haematological laboratory abnormalities identified as adverse drug reactions were increased alanine aminotransferase (54.9%), increased aspartate aminotransferase (52.3%) and hypercholesterolaemia (49.2%). The majority were of grade 1 and 2. Discontinuation due to adverse events, regardless of causality, was observed in 29.4% of patients. Chronic GvHD The most frequently reported overall adverse drug reactions were anaemia, hypercholesterolemia and increased aspartate aminotransferase. Haematological laboratory abnormalities identified as adverse drug reactions included anaemia (68.6%), thrombocytopenia (34.4%) and neutropenia (36.2%). Grade 3 anaemia was reported in 14.8% of patients (grade 4 not applicable per CTCAE v4.03). Grade 3 and 4 neutropenia were reported in 9.5% and 6.7% of patients, respectively. The three most frequent non-haematological adverse drug reactions were hypertension (15.0%), headache (10.2%) and urinary tract infections (9.3%). The three most frequent non-haematological laboratory abnormalities identified as adverse drug reactions were hypercholesterolaemia (52.3%), increased aspartate aminotransferase (52.2%) and increased alanine aminotransferase (43.1%). The majority were grade 1 and 2. Discontinuation due to adverse events, regardless of causality, was observed in 18.1% of patients. Tabulated list of adverse drug reactions from clinical studies The safety of Jakavi in MF patients was evaluated using the long-term follow-up data from two phase 3 studies (COMFORT-I and COMFORT-II) including data from patients initially randomised to ruxolitinib (n=301) and patients who received ruxolitinib after crossing over from control treatments (n=156). The median exposure upon which the adverse drug reaction frequency categories for MF patients are based was 30.5 months (range 0.3 to 68.1 months). The safety of Jakavi in PV patients was evaluated using the long-term follow-up data from two phase 3 studies (RESPONSE, RESPONSE 2) including data from patients initially randomised to ruxolitinib (n=184) and patients who received ruxolitinib after crossing over from control treatments (n=156). The median exposure upon which the adverse drug reaction frequency categories for PV patients are based was 41.7 months (range 0.03 to 59.7 months). JAK API May24 V7 EU SmPC April 2024 The safety of Jakavi in acute GvHD patients was evaluated in the phase 3 study REACH2, including data from patients initially randomised to Jakavi (n=152) and patients who received Jakavi after crossing over from the best available therapy (BAT) arm (n=49). The median exposure upon which the adverse drug reaction frequency categories were based was 8.9 weeks (range 0.3 to 66.1 weeks). The safety of Jakavi in chronic GvHD patients was evaluated in the phase 3 study REACH3, including data from patients initially randomised to Jakavi (n=165) and patients who received Jakavi after crossing over from BAT (n=61). The median exposure upon which the adverse drug reaction frequency categories were based was 41.4 weeks (range 0.7 to 127.3 weeks). In the clinical study programme the severity of adverse drug reactions was assessed based on the CTCAE, defining grade 1=mild, grade 2=moderate, grade 3=severe, grade 4=life-threatening or disabling, grade 5=death. Adverse drug reactions from clinical studies in MF and PV (Table 4) and in acute and chronic GvHD (Table 5) are listed by MedDRA system organ class. Within each system organ class, the adverse drug reactions are ranked by frequency, with the most frequent reactions first. In addition, the corresponding frequency category for each adverse drug reaction is based on the following convention: very common (≥1/10); common (≥1/100 to <1/10); uncommon (≥1/1,000 to <1/100); rare (≥1/10,000 to <1/1,000); very rare (<1/10,000); not known (cannot be estimated from the available data). Table 4 Frequency category of adverse drug reactions reported in the phase 3 studies in MF and PV Adverse drug reaction Frequency category for MF Frequency category for PV patients patients Infections and infestations Urinary tract infectionsd Very common Very common Herpes zosterd Very common Very common Pneumonia Very common Common Sepsis Common Uncommon Tuberculosis Uncommon Not knowne HBV reactivation Not knowne Uncommon Blood and lymphatic system disordersa,d Anaemiaa CTCAEc grade 4 Very common Uncommon (<6.5g/dl) CTCAEc grade 3 Very common Common (<8.0 – 6.5g/dl) Any CTCAEc grade Very common Very common Thrombocytopeniaa CTCAEc grade 4 Common Uncommon (<25,000/mm3) CTCAEc grade 3 Very common Common (50,000 – 25,000/mm3) Any CTCAEc grade Very common Very common Neutropeniaa CTCAEc grade 4 Common Uncommon (<500/mm3) JAK API May24 V7 EU SmPC April 2024 CTCAEc grade 3 Common Uncommon 3 (<1,000 – 500/mm ) Any CTCAEc grade Very common Common Pancytopeniaa,b Common Common Bleeding (any bleeding Very common Very common including intracranial, and gastrointestinal bleeding, bruising and other bleeding) Bruising Very common Very common Gastrointestinal bleeding Very common Common Intracranial bleeding Common Uncommon Other bleeding (including Very common Very common epistaxis, post-procedural haemorrhage and haematuria) Metabolism and nutrition disorders Hypercholesterolaemiaa Very common Very common any CTCAEc grade Hypertriglyceridaemiaa Very common Very common c any CTCAE grade Weight gain Very common Very common Nervous system disorders Dizziness Very common Very common Headache Very common Very common Gastrointestinal disorders Elevated lipase, any CTCAEc Very common Very common grade Constipation Very common Very common Flatulence Common Common Hepatobiliary disorders Increased alanine aminotransferasea CTCAEc grade 3 Common Common (> 5x – 20 x ULN) Any CTCAEc grade Very common Very common Increased aspartate aminotransferasea Any CTCAEc grade Very common Very common Vascular disorders Hypertension Very common Very common a Frequency is based on new or worsened laboratory abnormalities compared to baseline. b Pancytopenia is defined as haemoglobin level <100 g/l, platelet count <100x109/l, and neutrophil count <1.5x109/l (or low white blood cell count of grade 2 if neutrophil count is missing), simultaneously in the same lab assessment c Common Terminology Criteria for Adverse Events (CTCAE) version 3.0; grade 1 = mild, grade 2 = moderate, grade 3 = severe, grade 4 = life-threatening d These ADRs are discussed in the text. e ADR derived from post-marketing experience Upon discontinuation, MF patients may experience a return of MF symptoms such as fatigue, bone pain, fever, pruritus, night sweats, symptomatic splenomegaly and weight loss. In clinical studies in MF the total symptom score for MF symptoms gradually returned to baseline value within 7 days after JAK API May24 V7 EU SmPC April 2024 dose discontinuation (see section 4.4). Table 5 Frequency category of adverse drug reactions reported in the phase 3 studies in GvHD Acute GvHD (REACH2) Chronic GvHD (REACH3) Adverse drug reaction Frequency category Frequency category Infections and infestations CMV infections Very common Common CTCAE3 grade ≥3 Very common Common Sepsis Very common - CTCAE grade ≥3 Very common - Urinary tract infections Very common Common CTCAE grade ≥3 Common Common BK virus infections - Common CTCAE grade ≥3 - Uncommon Blood and lymphatic system disorders Thrombocytopenia1 Very common Very common CTCAE grade 3 Very common Common CTCAE grade 4 Very common Very common Anaemia1 Very common Very common CTCAE grade 3 Very common Very common Neutropenia1 Very common Very common CTCAE grade 3 Very common Common CTCAE grade 4 Very common Common Pancytopenia1,2 Very common - Metabolism and nutrition disorders Hypercholesterolaemia1 Very common Very common CTCAE grade 3 Common Common CTCAE grade 4 Common Uncommon Weight gain - Common CTCAE grade ≥3 - N/A5 Nervous system disorders Headache Common Very common CTCAE grade ≥3 Uncommon Common Vascular disorders Hypertension Very common Very common CTCAE grade ≥3 Common Common Gastrointestinal disorders Increased lipase1 - Very common CTCAE grade 3 - Common CTCAE grade 4 - Uncommon Increased amylase1 - Very common CTCAE grade 3 - Common CTCAE grade 4 - Common Nausea Very common - CTCAE grade ≥3 Uncommon - Constipation - Common CTCAE grade ≥3 - N/A5 JAK API May24 V7 EU SmPC April 2024 Hepatobiliary disorders Increased alanine Very common Very common aminotransferase1 CTCAE grade 3 Very common Common CTCAE grade 4 Common Uncommon Increased aspartate Very common Very common aminotransferase1 CTCAE grade 3 Common Common CTCAE grade 4 N/A5 Uncommon Musculoskeletal and connective tissue disorders Increased blood creatine - Very common phosphokinase1 CTCAE grade 3 - Common CTCAE grade 4 - Common Renal and urinary disorders Increased blood creatinine1 - Very common CTCAE grade 3 - Common CTCAE grade 4 - N/A5 1 Frequency is based on new or worsened laboratory abnormalities compared to baseline. 2 Pancytopenia is defined as haemoglobin level <100 g/l, platelet count <100 x 109/l, and neutrophil count <1.5 x 109/l (or low white blood cell count of grade 2 if neutrophil count is missing), simultaneously in the same laboratory assessment. 3 CTCAE Version 4.03. 4 Grade ≥3 sepsis includes 20 (10%) grade 5 events. 5 Not applicable: no cases reported Description of selected adverse drug reactions Anaemia In phase 3 clinical studies in MF, median time to onset of first CTCAE grade 2 or higher anaemia was 1.5 months. One patient (0.3%) discontinued treatment because of anaemia. In patients receiving ruxolitinib mean decreases in haemoglobin reached a nadir of approximately 10 g/litre below baseline after 8 to 12 weeks of therapy and then gradually recovered to reach a new steady state that was approximately 5 g/litre below baseline. This pattern was observed in patients regardless of whether they had received transfusion during therapy. In the randomised, placebo-controlled study COMFORT-I 60.6% of Jakavi-treated MF patients and 37.7% of placebo-treated MF patients received red blood cell transfusions during randomised treatment. In the COMFORT-II study the rate of packed red blood cell transfusions was 53.4% in the Jakavi arm and 41.1% in the best available therapy arm. In the randomised period of the pivotal studies, anaemia was less frequent in PV patients than in MF patients (40.8% versus 82.4%). In the PV population, the CTCAE grade 3 and 4 events were reported in 2.7%, while in the MF patients the frequency was 42.56%. In the phase 3 acute and chronic GvHD studies, anaemia CTCAE grade 3 was reported in 47.7% and 14.8% of patients, respectively. Thrombocytopenia In the phase 3 clinical studies in MF, in patients who developed grade 3 or 4 thrombocytopenia, the median time to onset was approximately 8 weeks. Thrombocytopenia was generally reversible with dose reduction or dose interruption. The median time to recovery of platelet counts above 50,000/mm3 was 14 days. During the randomised period, platelet transfusions were administered to 4.7% of patients receiving ruxolitinib and to 4.0% of patients receiving control regimens. Discontinuation of JAK API May24 V7 EU SmPC April 2024 treatment because of thrombocytopenia occurred in 0.7% of patients receiving ruxolitinib and 0.9% of patients receiving control regimens. Patients with a platelet count of 100,000/mm3 to 200,000/mm3 before starting ruxolitinib had a higher frequency of grade 3 or 4 thrombocytopenia compared to patients with platelet count >200,000/mm3 (64.2% versus 38.5%). In the randomised period of the pivotal studies, the rate of patients experiencing thrombocytopenia was lower in PV (16.8%) patients compared to MF (69.8%) patients. The frequency of severe (i.e. CTCAE grade 3 and 4) thrombocytopenia was lower in PV (2.7%) than in MF (11.6%) patients. In the phase 3 acute GvHD study, grade 3 and 4 thrombocytopenia was observed in 31.3% and 47.7% of patients, respectively. In the phase 3 chronic GvHD study, grade 3 and 4 thrombocytopenia was lower (5.9% and 10.7%) than in acute GvHD. Neutropenia In the phase 3 clinical studies in MF, in patients who developed grade 3 or 4 neutropenia, the median time to onset was 12 weeks. During the randomised period, dose holding or reductions due to neutropenia were reported in 1.0% of patients, and 0.3% of patients discontinued treatment because of neutropenia. In the randomised period of the phase 3 studies in PV patients, neutropenia was reported in 1.6% of patients exposed to ruxolitinib compared to 7% in reference treatments. In the ruxolitinib arm one patient developed CTCAE grade 4 neutropenia. An extended follow-up of patients treated with ruxolitinib showed 2 patients reporting CTCAE grade 4 neutropenia. In the phase 3 acute GvHD study, grade 3 and 4 neutropenia was observed in 17.9% and 20.6% of patients, respectively. In the phase 3 chronic GvHD study grade 3 and 4 neutropenia was lower (9.5% and 6.7%) than in acute GvHD. Bleeding In the phase 3 pivotal studies in MF bleeding events (including intracranial and gastrointestinal, bruising and other bleeding events) were reported in 32.6% of patients exposed to ruxolitinib and 23.2% of patients exposed to the reference treatments (placebo or best available therapy). The frequency of grade 3-4 events was similar for patients treated with ruxolitinib or reference treatments (4.7% versus 3.1%). Most of the patients with bleeding events during the treatment reported bruising (65.3%). Bruising events were more frequently reported in patients taking ruxolitinib compared with the reference treatments (21.3% versus 11.6%). Intracranial bleeding was reported in 1% of patients exposed to ruxolitinib and 0.9% exposed to reference treatments. Gastrointestinal bleeding was reported in 5.0% of patients exposed to ruxolitinib compared to 3.1% exposed to reference treatments. Other bleeding events (including events such as epistaxis, post-procedural haemorrhage and haematuria) were reported in 13.3% of patients treated with ruxolitinib and 10.3% treated with reference treatments. During the long-term follow-up of phase 3 clinical studies in MF, the cumulative frequency of bleeding events increased proportionally to the increase in the follow-up time. Bruising events were the most frequently reported bleeding events (33.3%). Intracranial and gastrointestinal bleeding events were reported in 1.3% and 10.1% of patients respectively. In the comparative period of phase 3 studies in PV patients, bleeding events (including intracranial and gastrointestinal, bruising and other bleeding events) were reported in 16.8% of patients treated with ruxolitinib, 15.3% of patients receiving best available therapy in RESPONSE study and 12.0% of patients receiving best available therapy in RESPONSE 2 study. Bruising was reported in 10.3% of patients treated with ruxolitinib, 8.1% of patients receiving best available therapy in RESPONSE study and 2.7% of patients receiving best available therapy in RESPONSE 2 study. No intracranial bleeding or gastrointestinal haemorrhage events were reported in patients receiving ruxolitinib. One patient treated with ruxolitinib experienced a grade 3 bleeding event (post-procedural bleeding); no JAK API May24 V7 EU SmPC April 2024 grade 4 bleeding was reported. Other bleeding events (including events such as epistaxis, post- procedural haemorrhage, gingival bleeding) were reported in 8.7% of patients treated with ruxolitinib, 6.3% of patients treated with best available therapy in RESPONSE study and 6.7% of patients treated with best available therapy in RESPONSE 2 study. During the long-term follow-up of phase 3 studies in PV, the cumulative frequency of bleeding events increased proportionally to the increase in the follow-up time. Bruising events were the most frequently reported bleeding events (17.4%). Intracranial and gastrointestinal bleeding events were reported in 0.3% and 3.5% of patients respectively. In the comparative period of the phase 3 acute GvHD study, bleeding events were reported in 25.0% and 22.0% of patients in the ruxolitinib and BAT arms respectively. The sub-groups of bleeding events were generally similar between treatment arms: bruising events (5.9% in ruxolitinib vs. 6.7% in BAT arm), gastrointestinal events (9.2% vs. 6.7%) and other haemorrhage events (13.2% vs. 10.7%). Intracranial bleeding events were reported in 0.7% of patients in the BAT arm and in no patients in the ruxolitinib arm. In the comparative period of the phase 3 chronic GvHD study, bleeding events were reported in 11.5% and 14.6% of patients in the ruxolitinib and BAT arms respectively. The sub-groups of bleeding events were generally similar between treatment arms: bruising events (4.2% in ruxolitinib vs. 2.5% in BAT arm), gastrointestinal events (1.2% vs. 3.2%) and other haemorrhage events (6.7% vs. 10.1%). No intracranial bleeding events were reported in either treatment arm. Infections In the phase 3 pivotal studies in MF, grade 3 or 4 urinary tract infection was reported in 1.0% of patients, herpes zoster in 4.3% and tuberculosis in 1.0%. In phase 3 clinical studies sepsis was reported in 3.0% of patients. An extended follow-up of patients treated with ruxolitinib showed no trends towards an increase in the rate of sepsis over time. In the randomised period of the phase 3 studies in PV patients, one (0.5%) CTCAE grade 3 and no grade 4 urinary tract infection was reported. The rate of herpes zoster was similar in PV (4.3%) patients and MF (4.0%) patients. There was one report of CTCAE grade 3 post-herpetic neuralgia amongst the PV patients. Pneumonia was reported in 0.5% of patients treated with ruxolitinib compared to 1.6% of patients in reference treatments. No patients in the ruxolitinib arm reported sepsis or tuberculosis. During long-term follow-up of phase 3 studies in PV, frequently reported infections were urinary tract infections (11.8%), herpes zoster (14.7%) and pneumonia (7.1%). Sepsis was reported in 0.6% of patients. No patients reported tuberculosis in long-term follow-up. In the phase 3 acute GvHD study, during the comparative period, urinary tract infections were reported in 9.9% (grade ≥3, 3.3%) of patients in the ruxolitinib arm compared to 10.7% (grade ≥3, 6.0%) in the BAT arm. CMV infections were reported in 28.3% (grade ≥3, 9.3%) of patients in the ruxolitinib arm compared to 24.0% (grade ≥3, 10.0%) in the BAT arm. Sepsis events were reported in 12.5% (grade ≥3, 11.1%) of patients in the ruxolitinib arm compared to 8.7% (grade ≥3, 6.0%) in the BAT arm. BK virus infection was reported only in the ruxolitinib arm in 3 patients with one grade 3 event. During extended follow-up of patients treated with ruxolitinib, urinary tract infections were reported in 17.9% (grade ≥3, 6.5%) of patients and CMV infections were reported in 32.3% (grade ≥3, 11.4%) of patients. CMV infection with organ involvement was seen in very few patients; CMV colitis, CMV enteritis and CMV gastrointestinal infection of any grade were reported in four, two and one patients, respectively. Sepsis events, including septic shock, of any grade were reported in 25.4% (grade ≥3, 21.9%) of patients. In the phase 3 chronic GvHD study, during the comparative period, urinary tract infections were reported in 8.5% (grade ≥3, 1.2%) of patients in the ruxolitinib arm compared to 6.3% (grade ≥3, JAK API May24 V7 EU SmPC April 2024 1.3%) in the BAT arm. BK virus infection was reported in 5.5% (grade ≥3, 0.6%) of patients in the ruxolitinib arm compared to 1.3% in the BAT arm. CMV infections were reported in 9.1% (grade ≥3, 1.8%) of patients in the ruxolitinib arm compared to 10.8% (grade ≥3, 1.9%) in the BAT arm. Sepsis events were reported in 2.4% (grade ≥3, 2.4%) of patients in the ruxolitinib arm compared to 6.3% (grade ≥3, 5.7%) in the BAT arm. During extended follow-up of patients treated with ruxolitinib, urinary tract infections and BK virus infections were reported in 9.3% (grade ≥3, 1.3%) and 4.9% (grade ≥3, 0.4%) of patients, respectively. CMV infections and sepsis events were reported in 8.8% (grade ≥3, 1.3%) and 3.5% (grade ≥3, 3.5%) of patients, respectively. Elevated lipase In the randomised period of the RESPONSE study, the worsening of lipase values was higher in the ruxolitinib arm compared to the control arm, mainly due to the differences among grade 1 elevations (18.2% vs 8.1%). Grade ≥2 elevations were similar between treatment arms. In RESPONSE 2, the frequencies were comparable between the ruxolitinib and the control arm (10.8% vs 8%). During long- term follow-up of phase 3 PV studies, 7.4% and 0.9% of patients reported grade 3 and grade 4 elevation of lipase values. No concurrent signs and symptoms of pancreatitis with elevated lipase values were reported in these patients. In phase 3 studies in MF, high lipase values were reported in 18.7% and 19.3% of patients in the ruxolitinib arms compared to 16.6% and 14.0% in the control arms in COMFORT-I and COMFORT-II studies, respectively. In patients with elevated lipase values, no concurrent signs and symptoms of pancreatitis were reported. In the comparative period of the phase 3 acute GvHD study, new or worsened lipase values were reported in 19.7% of patients in the ruxolitinib arm compared to 12.5% in the BAT arm; corresponding grade 3 (3.1% vs 5.1%) and grade 4 (0% vs 0.8%) increases were similar. During extended follow-up of patients treated with ruxolitinib, increased lipase values were reported in 32.2% of patients; grade 3 and 4 were reported in 8.7% and 2.2% of patients respectively. In the comparative period of the phase 3 chronic GvHD study, new or worsened lipase values were reported in 32.1% of patients in the ruxolitinib arm compared to 23.5% in the BAT arm; corresponding grade 3 (10.6% vs 6.2%) and grade 4 (0.6% vs 0%) increases were similar. During extended follow-up of patients treated with ruxolitinib, increased lipase values were reported in 35.9% of patients; grade 3 and 4 were observed in 9.5% and 0.4% of patients, respectively. Increased systolic blood pressure In the phase 3 pivotal clinical studies in MF an increase in systolic blood pressure of 20 mmHg or more from baseline was recorded in 31.5% of patients on at least one visit compared with 19.5% of the control-treated patients. In COMFORT-I (MF patients) the mean increase from baseline in systolic BP was 0-2 mmHg on ruxolitinib versus a decrease of 2-5 mmHg in the placebo arm. In COMFORT-II mean values showed little difference between the ruxolitinib-treated and the control-treated MF patients. In the randomised period of the pivotal study in PV patients, the mean systolic blood pressure increased by 0.65 mmHg in the ruxolitinib arm versus a decrease of 2 mmHg in the BAT arm. Paediatric patients A total of 20 patients aged 12 to <18 years with GvHD were analysed for safety: 9 patients (5 in the ruxolitinib arm and 4 in the BAT arm) in the study REACH2 and 11 patients (4 in the ruxolitinib arm and 7 in the BAT arm) in the study REACH3. Based on the similar exposure observed in adolescents and adults, the safety of ruxolitinib at the recommended dose of 10 mg twice daily is similar in frequency and severity. Elderly A total of 29 patients in study REACH2 and 25 patients in REACH3 aged >65 years and treated with JAK API May24 V7 EU SmPC April 2024 ruxolitinib were analysed for safety. Overall, no new safety concerns were identified and the safety profile in patients >65 years old is generally consistent with that of patients aged 18-65 years old. Reporting of suspected adverse reactions Reporting suspected adverse reactions after authorisation of the medicinal product is important. It allows continued monitoring of the benefit/risk balance of the medicinal product. Any suspected adverse events should be reported to the Ministry of Health according to the National Regulation by using an online form https://sideeffects.health.gov.il
פרטי מסגרת הכללה בסל
התרופה תינתן לטיפול במקרים האלה:1. מיאלופיברוזיס בדרגת סיכון intermediate 2 או high לפי IPSS על רקע:א. מיאלופיברוזיס ראשוניתב. פוליציתמיה ורהג. essential thrombocythemiaהתרופה תינתן לחולים שטרם טופלו במעכב JAK למחלתם.2. פוליציתמיה ורה עם עמידות או אי סבילות להידרוקסיאוריאה או לתרופה ממשפחת האינטרפרונים. לעניין זה עמידות תוגדר במטופל המקבל לפחות 3 חודשים טיפול ע"י הידרוקסיאוראה במינון של 2 גרם ליום או 3 חודשים במינון מקסימלי של תרופה ממשפחת האינטרפרונים, ולא מגיע לערך של המטוקריט<45 בגברים או 42 בנשים.לעניין זה אי סבילות תוגדר בחולה העונה על אחד מאלה:א. נוכחות של כיבים בגפיים התחתונות. ב. גרד קשה ועמיד לטיפול באנטיהיסטמינים ו-Pregabalin, לאחר ניסיון טיפולי בשני קווי טיפול אלו, למשך שלושה חודשים לפחות. ג. כאבים בבטן השמאלית על רקע טחול מוגדל (טחול נמדד בקוטר מירבי מעל ל20 ס"מ).ד. התפתחות תופעות לוואי של תרופות ממשפחת האינטרפרונים המחייבות הפסקת טיפול.3. טיפול בחולים מגיל 12 ומעלה עם מחלת השתל נגד המאכסן חריפה או כרונית (cGVHD או aGVHD) עם תגובה לא מספקת או הוריית נגד לטיפול בסטרואידים סיסטמיים או טיפול סיסטמי אחר.
מסגרת הכללה בסל
התוויות הכלולות במסגרת הסל
התוויה | תאריך הכללה | תחום קליני | Class Effect | מצב מחלה |
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פוליציתמיה ורה עם עמידות או אי סבילות להידרוקסיאוריאה או לתרופה ממשפחת האינטרפרונים. לעניין זה עמידות תוגדר במטופל המקבל לפחות 3 חודשים טיפול ע"י הידרוקסיאוראה במינון של 2 גרם ליום או 3 חודשים במינון מקסימלי של תרופה ממשפחת האינטרפרונים, ולא מגיע לערך של המטוקריט | 01/02/2023 | המטולוגיה | פוליציתמיה ורה, Polycythemia vera | |
א. התרופה תינתן לטיפול במיאלופיברוזיס בדרגת סיכון intermediate 2 או high לפי IPSS על רקע: 1. מיאלופיברוזיס ראשונית 2. פוליציתמיה ורה 3. essential thrombocythemia ב התרופה תינתן לחולים שטרם טופלו במעכב JAK למחלתם. | 01/03/2021 | המטולוגיה | Myelofibrosis | |
התרופה תינתן לטיפול בספלנומגליה או סימפטומים במבוגרים הסובלים ממיאלופיברוזיס בדרגת סיכון intermediate 2 או high לפי IPSS על רקע: א. מיאלופיברוזיס ראשונית ב. פוליציתמיה ורה ג. essential thrombocythemia | 09/01/2013 | המטולוגיה | Myelofibrosis | |
פוליציתמיה ורה עם עמידות או אי סבילות להידרוקסיאוריאה ותרופה ממשפחת האינטרפרונים. לעניין זה עמידות תוגדר במטופל המקבל לפחות 3 חודשים טיפול ע"י הידרוקסיאוראה במינון של 2 גרם ליום ו-3 חודשים במינון מקסימלי של תרופה ממשפחת האינטרפרונים, ולא מגיע לערך של המטוקריט | 03/02/2022 | המטולוגיה | פוליציתמיה ורה, Polycythemia vera | |
טיפול בחולים מגיל 12 ומעלה עם מחלת השתל נגד המאכסן חריפה או כרונית (cGVHD או aGVHD) עם תגובה לא מספקת או הוריית נגד לטיפול בסטרואידים סיסטמיים או טיפול סיסטמי אחר. | 01/02/2023 | המטולוגיה | GVHD, Graft versus host disease, מחלת שתל נגד מאחסן |
שימוש לפי פנקס קופ''ח כללית 1994
לא צוין
תאריך הכללה מקורי בסל
09/01/2013
הגבלות
תרופה מוגבלת לרישום ע'י רופא מומחה או הגבלה אחרת
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