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DRUGS & SUPPLEMENTS
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Razel
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Razel uses
- Indications and usage
- Dosage and administration
- Dosage forms and strengths
- Contraindications
- Warnings and precautions
- Adverse reactions
- Drug interactions
- Use in specific populations
- Overdosage
- Description
- Clinical pharmacology
- Nonclinical toxicology
- Clinical studies
- How supplied/storage and handling
- Patient counseling information
- Patient information
1 INDICATIONS AND USAGE
Razel is an HMG Co‑A reductase inhibitor indicated for:
- patients with primary hyperlipidemia and mixed dyslipidemia as an adjunct to diet to reduce elevated total‑C, LDL‑C, ApoB, nonHDL‑C, and TG levels and to increase HDL‑C
- patients with hypertriglyceridemia as an adjunct to diet (1.2)
- patients with primary dysbetalipoproteinemia (Type III hyperlipoproteinemia) as an adjunct to diet (1.3)
- patients with homozygous familial hypercholesterolemia (HoFH) to reduce LDL‑C, total-C, and ApoB (1.4)
- slowing the progression of atherosclerosis as part of a treatment strategy to lower total‑C and LDL‑C as an adjunct to diet (1.5)
- pediatric patients 10 to 17 years of age with heterozygous familial hypercholesterolemia (HeFH) to reduce elevated total‑C, LDL‑C and ApoB after failing an adequate trial of diet therapy (1.1)
- risk reduction of MI, stroke, and arterial revascularization procedures in patients without clinically evident CHD, but with multiple risk factors (1.6)
Limitations of use (1.7):
- Razel has not been studied in Fredrickson Type I and V dyslipidemias.
1.1 Hyperlipidemia and Mixed Dyslipidemia
Razel is indicated as adjunctive therapy to diet to reduce elevated Total-C, LDL-C, ApoB, nonHDL‑C, and triglycerides and to increase HDL‑C in adult patients with primary hyperlipidemia or mixed dyslipidemia. Lipid-altering agents should be used in addition to a diet restricted in saturated fat and cholesterol when response to diet and nonpharmacological interventions alone has been inadequate.
Pediatric Patients 10 to 17 years of age with Heterozygous Familial Hypercholesterolemia (HeFH)
Adjunct to diet to reduce Total‑C, LDL‑C and ApoB levels in adolescent boys and girls, who are at least one year post-menarche, 10‑17 years of age with heterozygous familial hypercholesterolemia if after an adequate trial of diet therapy the following findings are present: LDL‑C > 190 mg/dL or > 160 mg/dL and there is a positive family history of premature cardiovascular disease (CVD) or two or more other CVD risk factors.
1.2 Hypertriglyceridemia
Razel is indicated as adjunctive therapy to diet for the treatment of adult patients with hypertriglyceridemia.
1.3 Primary Dysbetalipoproteinemia
Razel is indicated as an adjunct to diet for the treatment of patients with primary dysbetalipoproteinemia (Type III Hyperlipoproteinemia).
1.4 Homozygous Familial Hypercholesterolemia
Razel is indicated as adjunctive therapy to other lipid-lowering treatments or alone if such treatments are unavailable to reduce LDL‑C, Total‑C, and ApoB in adult patients with homozygous familial hypercholesterolemia.
1.5 Slowing of the Progression of Atherosclerosis
Razel is indicated as adjunctive therapy to diet to slow the progression of atherosclerosis in adult patients as part of a treatment strategy to lower Total‑C and LDL‑C to target levels.
1.6 Primary Prevention of Cardiovascular Disease
In individuals without clinically evident coronary heart disease but with an increased risk of cardiovascular disease based on age ≥ 50 years old in men and ≥ 60 years old in women, hsCRP ≥ 2 mg/L, and the presence of at least one additional cardiovascular disease risk factor such as hypertension, low HDL‑C, smoking, or a family history of premature coronary heart disease, Razel is indicated to:
- reduce the risk of stroke
- reduce the risk of myocardial infarction
- reduce the risk of arterial revascularization procedures
1.7 Limitations of Use
Razel has not been studied in Fredrickson Type I and V dyslipidemias.
2 DOSAGE AND ADMINISTRATION
- Razel can be taken with or without food, at any time of day.
- Dose range: 5‑40 mg once daily. Use 40 mg dose only for patients not reaching LDL‑C goal with 20 mg. (2.1)
- HoFH: Starting dose 20 mg. (2.3)
- In pediatric patients 10 to 17 years of age with HeFH, the usual dose range is 5‑20 mg/day; doses greater than 20 mg have not been studied in this patient population. (2.2)
2.1 General Dosing Information
The dose range for Razel is 5 to 40 mg orally once daily. The usual starting dose is 10‑20 mg.
Razel can be administered as a single dose at any time of day, with or without food.
When initiating Razel therapy or switching from another HMG‑CoA reductase inhibitor therapy, the appropriate Razel starting dose should first be utilized, and only then titrated according to the patient’s response and individualized goal of therapy.
After initiation or upon titration of Razel, lipid levels should be analyzed within 2 to 4 weeks and the dosage adjusted accordingly.
The 40 mg dose of Razel should be used only for those patients who have not achieved their LDL‑C goal utilizing the 20 mg dose [see Warnings and Precautions (5.1) ].
2.2 Heterozygous Familial Hypercholesterolemia in Pediatric Patients
The usual dose range of Razel is 5‑20 mg/day; the maximum recommended dose is 20 mg/day (doses greater than 20 mg have not been studied in this patient population). Doses should be individualized according to the recommended goal of therapy [see Clinical Pharmacology (12) and Indications and Usage (1.2) ]. Adjustments should be made at intervals of 4 weeks or more.
2.3 Homozygous Familial Hypercholesterolemia
The recommended starting dose of Razel is 20 mg once daily. Response to therapy should be estimated from preapheresis LDL‑C levels.
2.4 Dosing in Asian Patients
In Asian patients, consider initiation of Razel therapy with 5 mg once daily due to increased rosuvastatin plasma concentrations. The increased systemic exposure should be taken into consideration when treating Asian patients not adequately controlled at doses up to 20 mg/day. [see Use in Specific Populations and Clinical Pharmacology (12.3) ].
2.5 Use with Concomitant Therapy
Patients taking cyclosporine
The dose of Razel should not exceed 5 mg once daily [see Warnings and Precautions (5.1) , Drug Interactions (7.1) , and Clinical Pharmacology (12.3) ]
Patients taking gemfibrozil
Initiate Razel therapy with 5 mg once daily. The dose of Razel should not exceed 10 mg once daily [see Warnings and Precautions (5.1) and Drug Interactions (7.2) , and Clinical Pharmacology (12.3) ].
Patients taking lopinavir and ritonavir or atazanavir and ritonavir
Initiate Razel therapy with 5 mg once daily. The dose of Razel should not exceed 10 mg once daily [see Warnings and Precautions (5.1) , Drug Interactions (7.3), and Clinical Pharmacology (12.3) ].
2.6 Dosing in Patients with Severe Renal Impairment
For patients with severe renal impairment (CLcr <30 mL/min/1.73 m2) not on hemodialysis, dosing of Razel should be started at 5 mg once daily and not exceed 10 mg once daily [see Use in Specific Populations (8.6) and Clinical Pharmacology (12.3) ].
3 DOSAGE FORMS AND STRENGTHS
5 mg: Yellow, round, biconvex, coated tablets. Debossed “CRESTOR” and “5” on one side of the tablet.
10 mg: Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “10” on one side of the tablet.
20 mg: Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “20” on one side of the tablet.
40 mg: Pink, oval, biconvex, coated tablets. Debossed “CRESTOR” on one side and “40” on the other side of the tablet.
Tablets: 5 mg, 10 mg, 20 mg, and 40 mg (3)
4 CONTRAINDICATIONS
Razel is contraindicated in the following conditions:
- Patients with a known hypersensitivity to any component of this product. Hypersensitivity reactions including rash, pruritus, urticaria, and angioedema have been reported with Razel [see Adverse Reactions (6.1) ].
- Patients with active liver disease, which may include unexplained persistent elevations of hepatic transaminase levels [see Warnings and Precautions (5.2) ].
- Women who are pregnant or may become pregnant. Because HMG‑CoA reductase inhibitors decrease cholesterol synthesis and possibly the synthesis of other biologically active substances derived from cholesterol, Razel may cause fetal harm when administered to pregnant women. Additionally, there is no apparent benefit to therapy during pregnancy, and safety in pregnant women has not been established. If the patient becomes pregnant while taking this drug, the patient should be apprised of the potential hazard to the fetus and the lack of known clinical benefit with continued use during pregnancy [see Use in Specific Populations (8.1) and Nonclinical Toxicology (13.2) ].
- Nursing mothers. Because another drug in this class passes into breast milk, and because HMG‑CoA reductase inhibitors have the potential to cause serious adverse reactions in nursing infants, women who require Razel treatment should be advised not to nurse their infants [see Use in Specific Populations (8.3) ].
- Known hypersensitivity to product components (4)
- Active liver disease, which may include unexplained persistent elevations in hepatic transaminase levels (4)
- Women who are pregnant or may become pregnant (4, 8.1)
- Nursing mothers (4, 8.3)
5 WARNINGS AND PRECAUTIONS
- Skeletal muscle effects : Risks increase with use of 40 mg dose, advanced age (≥65), hypothyroidism, renal impairment, and combination use with cyclosporine, lopinavir/ritonavir, or atazanavir/ritonavir. Advise patients to promptly report to their physician unexplained and/or persistent muscle pain, tenderness, or weakness and discontinue Razel if signs or symptoms appear. (5.1, 7.5, 7.6)
- Liver enzyme abnormalities: Persistent elevations in hepatic transaminases can occur. Perform liver enzyme tests before initiating therapy and as clinically indicated thereafter. (5.2)
5.1 Skeletal Muscle Effects
Cases of myopathy and rhabdomyolysis with acute renal failure secondary to myoglobinuria have been reported with HMG-CoA reductase inhibitors, including Razel. These risks can occur at any dose level, but are increased at the highest dose (40 mg).
Razel should be prescribed with caution in patients with predisposing factors for myopathy (e.g., age ≥ 65 years, inadequately treated hypothyroidism, renal impairment).
The risk of myopathy during treatment with Razel may be increased with concurrent administration of some other lipid-lowering therapies (fibrates or niacin), gemfibrozil, cyclosporine, lopinavir/ritonavir, or atazanavir/ritonavir [see Dosage and Administration (2) and Drug Interactions (7 )]. Cases of myopathy, including rhabdomyolysis, have been reported with HMG-CoA reductase inhibitors, including rosuvastatin, coadministered with colchicine, and caution should be exercised when prescribing Razel with colchicine [see Drug Interactions (7.7) ].
Razel therapy should be discontinued if markedly elevated creatine kinase levels occur or myopathy is diagnosed or suspected. Razel therapy should also be temporarily withheld in any patient with an acute, serious condition suggestive of myopathy or predisposing to the development of renal failure secondary to rhabdomyolysis (e.g., sepsis, hypotension, dehydration, major surgery, trauma, severe metabolic, endocrine, and electrolyte disorders, or uncontrolled seizures).
There have been rare reports of immune-mediated necrotizing myopathy (IMNM), an autoimmune myopathy, associated with statin use. IMNM is characterized by: proximal muscle weakness and elevated serum creatine kinase, which persist despite discontinuation of statin treatment; muscle biopsy showing necrotizing myopathy without significant inflammation; improvement with immunosuppressive agents.
All patients should be advised to promptly report to their physician unexplained muscle pain, tenderness, or weakness, particularly if accompanied by malaise or fever or if muscle signs and symptoms persist after discontinuing Razel.
5.2 Liver Enzyme Abnormalities
It is recommended that liver enzyme tests be performed before the initiation of Razel, and if signs or symptoms of liver injury occur.
Increases in serum transaminases [AST or ALT (SGPT)] have been reported with HMG‑CoA reductase inhibitors, including Razel. In most cases, the elevations were transient and resolved or improved on continued therapy or after a brief interruption in therapy. There were two cases of jaundice, for which a relationship to Razel therapy could not be determined, which resolved after discontinuation of therapy. There were no cases of liver failure or irreversible liver disease in these trials.
In a pooled analysis of placebo-controlled trials, increases in serum transaminases to >3 times the upper limit of normal occurred in 1.1% of patients taking Razel versus 0.5% of patients treated with placebo.
There have been rare postmarketing reports of fatal and non-fatal hepatic failure in patients taking statins, including rosuvastatin. If serious liver injury with clinical symptoms and/or hyperbilirubinemia or jaundice occurs during treatment with Razel, promptly interrupt therapy. If an alternate etiology is not found, do not restart Razel.
Razel should be used with caution in patients who consume substantial quantities of alcohol and/or have a history of chronic liver disease [see Clinical Pharmacology (12.3)]. Active liver disease, which may include unexplained persistent transaminase elevations, is a contraindication to the use of Razel [ see Contraindications (4) ].
5.3 Concomitant Coumarin Anticoagulants
Caution should be exercised when anticoagulants are given in conjunction with Razel because of its potentiation of the effect of coumarin-type anticoagulants in prolonging the prothrombin time/INR. In patients taking coumarin anticoagulants and Razel concomitantly, INR should be determined before starting Razel and frequently enough during early therapy to ensure that no significant alteration of INR occurs [see Drug Interactions (7.4) ].
5.4 Proteinuria and Hematuria
In the Razel clinical trial program, dipstick-positive proteinuria and microscopic hematuria were observed among Razel treated patients. These findings were more frequent in patients taking Razel 40 mg, when compared to lower doses of Razel or comparator HMG‑CoA reductase inhibitors, though it was generally transient and was not associated with worsening renal function. Although the clinical significance of this finding is unknown, a dose reduction should be considered for patients on Razel therapy with unexplained persistent proteinuria and/or hematuria during routine urinalysis testing.
5.5 Endocrine Effects
Increases in HbA1c and fasting serum glucose levels have been reported with HMG‑CoA reductase inhibitors, including Razel. Based on clinical trial data with Razel, in some instances these increases may exceed the threshold for the diagnosis of diabetes mellitus [see Adverse Reactions (6.1) ].
Although clinical studies have shown that Razel alone does not reduce basal plasma cortisol concentration or impair adrenal reserve, caution should be exercised if Razel is administered concomitantly with drugs that may decrease the levels or activity of endogenous steroid hormones such as ketoconazole, spironolactone, and cimetidine.
6 ADVERSE REACTIONS
The following serious adverse reactions are discussed in greater detail in other sections of the label:
- Rhabdomyolysis with myoglobinuria and acute renal failure and myopathy [see Warnings and Precautions (5.1)]
- Liver enzyme abnormalities [see Warnings and Precautions (5.2)]
In the Razel controlled clinical trials database (placebo or active-controlled) of 5394 patients with a mean treatment duration of 15 weeks, 1.4% of patients discontinued due to adverse reactions. The most common adverse reactions that led to treatment discontinuation were:
- myalgia
- abdominal pain
- nausea
The most commonly reported adverse reactions (incidence ≥ 2%) in the Razel controlled clinical trial database of 5394 patients were:
- headache
- myalgia
- abdominal pain
- asthenia
- nausea
Most frequent adverse reactions (rate > 2%) are headache, myalgia, abdominal pain, asthenia, and nausea. (6.1)
To report SUSPECTED ADVERSE REACTIONS, contact AstraZeneca or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch.
6.1 Clinical Studies Experience
Because clinical studies are conducted under widely varying conditions, adverse reaction rates observed in the clinical studies of a drug cannot be directly compared to rates in the clinical studies of another drug and may not reflect the rates observed in clinical practice.
Adverse reactions reported in ≥ 2% of patients in placebo-controlled clinical studies and at a rate greater than placebo are shown in Table 1. These studies had a treatment duration of up to 12 weeks.
- Table 1. Adverse Reactions 1 Reported in ≥ 2% of Patients Treated with Razel and > Placebo in Placebo‑Controlled Trials (% of Patients)
| Adverse Reactions | Razel 5 mg N=291 | Razel 10 mg N=283 | Razel 20 mg N=64 | Razel 40 mg N=106 | Total Razel 5 mg‑40 mg N=744 | Placebo N=382 |
| Headache | 5.5 | 4.9 | 3.1 | 8.5 | 5.5 | 5.0 |
| Nausea | 3.8 | 3.5 | 6.3 | 0 | 3.4 | 3.1 |
| Myalgia | 3.1 | 2.1 | 6.3 | 1.9 | 2.8 | 1.3 |
| Asthenia | 2.4 | 3.2 | 4.7 | 0.9 | 2.7 | 2.6 |
| Constipation | 2.1 | 2.1 | 4.7 | 2.8 | 2.4 | 2.4 |
Other adverse reactions reported in clinical studies were abdominal pain, dizziness, hypersensitivity (including rash, pruritus, urticaria, and angioedema) and pancreatitis. The following laboratory abnormalities have also been reported: dipstick-positive proteinuria and microscopic hematuria [see Warnings and Precautions (5.4) ]; elevated creatine phosphokinase, transaminases, glucose, glutamyl transpeptidase, alkaline phosphatase, and bilirubin; and thyroid function abnormalities.
In the METEOR study, involving 981 participants treated with rosuvastatin 40 mg (n=700) or placebo (n=281) with a mean treatment duration of 1.7 years, 5.6% of subjects treated with Razel versus 2.8% of placebo-treated subjects discontinued due to adverse reactions. The most common adverse reactions that led to treatment discontinuation were: myalgia, hepatic enzyme increased, headache, and nausea [see Clinical Studies (14.7) ].
Adverse reactions reported in ≥ 2% of patients and at a rate greater than placebo are shown in Table 2.
- Table 2. Adverse Reactions 1 Reported in 2% of Patients Treated with Razel and > Placebo in the METEOR Trial (% of Patients)
| Adverse Reactions | Razel 40 mg N=700 | Placebo N=281 |
|---|---|---|
| Myalgia | 12.7 | 12.1 |
| Arthralgia | 10.1 | 7.1 |
| Headache | 6.4 | 5.3 |
| Dizziness | 4.0 | 2.8 |
| Increased CPK | 2.6 | 0.7 |
| Abdominal pain | 2.4 | 1.8 |
| | 2.2 | 0.7 |
In the JUPITER study, 17,802 participants were treated with rosuvastatin 20 mg (n=8901) or placebo (n=8901) for a mean duration of 2 years. A higher percentage of rosuvastatin-treated patients versus placebo-treated patients, 6.6% and 6.2%, respectively, discontinued study medication due to an adverse event, irrespective of treatment causality. Myalgia was the most common adverse reaction that led to treatment discontinuation.
In JUPITER, there was a significantly higher frequency of diabetes mellitus reported in patients taking rosuvastatin (2.8%) versus patients taking placebo (2.3%). Mean HbA1c was significantly increased by 0.1% in rosuvastatin-treated patients compared to placebo-treated patients. The number of patients with a HbA1c > 6.5% at the end of the trial was significantly higher in rosuvastatin-treated versus placebo-treated patients [see Warnings and Precautions (5.5) and Clinical Studies (14.8) ].
Adverse reactions reported in ≥ 2% of patients and at a rate greater than placebo are shown in Table 3.
- Table 3. Adverse Reactions 1 Reported in ≥ 2% of Patients Treated with Razel and > Placebo in the JUPITER Trial (% of Patients)
| Adverse Reactions | Razel 20 mg N=8901 | Placebo N=8901 |
| Myalgia | 7.6 | 6.6 |
| Arthralgia | 3.8 | 3.2 |
| Constipation | 3.3 | 3.0 |
| Diabetes mellitus | 2.8 | 2.3 |
| Nausea | 2.4 | 2.3 |
6.2 Pediatric patients 10 to 17 years of age
In a 12-week controlled study in boys and postmenarchal girls, the safety and tolerability profile of Razel 5 to 20 mg daily was generally similar to that of placebo [see Clinical Studies and Use in Specific Populations, Pediatric Use (8.4) ].
However, elevations in serum creatine phosphokinase (CK) > 10 x ULN were observed more frequently in rosuvastatin compared with placebo-treated children. Four of 130 (3%) children treated with rosuvastatin (2 treated with 10 mg and 2 treated with 20 mg) had increased CK >10 x ULN, compared to 0 of 46 children on placebo.
6.3 Postmarketing Experience
The following adverse reactions have been identified during postapproval use of Razel: arthralgia, fatal and non-fatal hepatic failure, hepatitis, jaundice, thrombocytopenia, depression, sleep disorders (including insomnia and nightmares) and gynecomastia. Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure.
There have been rare reports of immune-mediated necrotizing myopathy associated with statin use [see Warnings and Precautions (5.1) ].
There have been rare postmarketing reports of cognitive impairment (e.g., memory loss, forgetfulness, amnesia, memory impairment, confusion) associated with statin use. These cognitive issues have been reported for all statins. The reports are generally nonserious, and reversible upon statin discontinuation, with variable times to symptom onset (1 day to years) and symptom resolution (median of 3 weeks).
7 DRUG INTERACTIONS
- Cyclosporine: Combination increases rosuvastatin exposure. Limit Razel dose to 5 mg once daily.
- Gemfibrozil: Combination should be avoided. If used together, limit Razel dose to 10 mg once daily. (5.1, 7.2)
- Lopinavir/Ritonavir or atazanavir/ritonavir: Combination increases rosuvastatin exposure. Limit Razel dose to 10 mg once daily. (2.5, 5.1, 7.3, 12.3)
- Coumarin anticoagulants: Combination prolongs INR. Achieve stable INR prior to starting Razel. Monitor INR frequently until stable upon initiation or alteration of Razel therapy. (5.3, 7.4)
- Concomitant lipid-lowering therapies: Use with fibrates or lipid-modifying doses (≥1 g/day) of niacin increases the risk of adverse skeletal muscle effects. Caution should be used when prescribing with Razel. (5.1, 7.5, 7.6)
7.1 Cyclosporine
Cyclosporine increased rosuvastatin exposure (AUC) 7‑fold. Therefore, in patients taking cyclosporine, the dose of Razel should not exceed 5 mg once daily [see Dosage and Administration (2.5) , Warnings and Precautions (5.1) , and Clinical Pharmacology (12.3) ].
7.2 Gemfibrozil
Gemfibrozil significantly increased rosuvastatin exposure. Due to an observed increased risk of myopathy/rhabdomyolysis, combination therapy with Razel and gemfibrozil should be avoided. If used together, the dose of Razel should not exceed 10 mg once daily [see Clinical Pharmacology ].
7.3 Protease Inhibitors
Coadministration of rosuvastatin with certain protease inhibitors given in combination with ritonavir has differing effects on rosuvastatin exposure. The protease inhibitor combinations lopinavir/ritonavir and atazanavir/ritonavir increase rosuvastatin exposure (AUC) up to threefold [see Table 4 – Clinical Pharmacology (12.3) ]. For these combinations the dose of Razel should not exceed 10 mg once daily. The combinations of tipranavir/ritonavir or fosamprenavir/ritonavir produce little or no change in rosuvastatin exposure. Caution should be exercised when rosuvastatin is coadministered with protease inhibitors given in combination with ritonavir [see Dosage and Administration (2.5), Warnings and Precautions (5.1) and Clinical Pharmacology (12.3) ].
7.4 Coumarin Anticoagulants
Razel significantly increased INR in patients receiving coumarin anticoagulants. Therefore, caution should be exercised when coumarin anticoagulants are given in conjunction with Razel. In patients taking coumarin anticoagulants and Razel concomitantly, INR should be determined before starting Razel and frequently enough during early therapy to ensure that no significant alteration of INR occurs [see Warnings and Precautions and Clinical Pharmacology (12.3) ].
7.5 Niacin
The risk of skeletal muscle effects may be enhanced when Razel is used in combination with lipid-modifying doses (≥1 g/day) of niacin; caution should be used when prescribing with Razel [see Warnings and Precautions (5.1) ].
7.6 Fenofibrate
When Razel was coadministered with fenofibrate, no clinically significant increase in the AUC of rosuvastatin or fenofibrate was observed. Because it is known that the risk of myopathy during treatment with HMG-CoA reductase inhibitors is increased with concomitant use of fenofibrates, caution should be used when prescribing fenofibrates with Razel [see Warnings and Precautions and Clinical Pharmacology (12.3) ].
7.7 Colchicine
Cases of myopathy, including rhabdomyolysis, have been reported with HMG‑CoA reductase inhibitors, including rosuvastatin, coadministered with colchicine, and caution should be exercised when prescribing Razel with colchicine [see Warnings and Precautions (5.1) ].
8 USE IN SPECIFIC POPULATIONS
- Severe renal impairment : Starting dose is 5 mg, not to exceed 10 mg. (2.6, 5.1, 8.6)
- Asian population: Consider 5 mg starting dose. (2.4, 8.8)
8.1 Pregnancy
Teratogenic effects: Pregnancy Category X.
Razel is contraindicated in women who are or may become pregnant. Serum cholesterol and triglycerides increase during normal pregnancy, and cholesterol products are essential for fetal development. Atherosclerosis is a chronic process and discontinuation of lipid-lowering drugs during pregnancy should have little impact on long-term outcomes of primary hyperlipidemia therapy [see Contraindications ].
There are no adequate and well-controlled studies of Razel in pregnant women. There have been rare reports of congenital anomalies following intrauterine exposure to HMG‑CoA reductase inhibitors. In a review of about 100 prospectively followed pregnancies in women exposed to other HMG‑CoA reductase inhibitors, the incidences of congenital anomalies, spontaneous abortions, and fetal deaths/stillbirths did not exceed the rate expected in the general population. However, this study was only able to exclude a three-to-fourfold increased risk of congenital anomalies over background incidence. In 89% of these cases, drug treatment started before pregnancy and stopped during the first trimester when pregnancy was identified.
Rosuvastatin crosses the placenta in rats and rabbits. In rats, Razel was not teratogenic at systemic exposures equivalent to a human therapeutic dose of 40 mg/day. At 10‑12 times the human dose of 40 mg/day, there was decreased pup survival, decreased fetal body weight among female pups, and delayed ossification. In rabbits, pup viability decreased and maternal mortality increased at doses equivalent to the human dose of 40 mg/day [see Nonclinical Toxicology (13.2) ].
Razel may cause fetal harm when administered to a pregnant woman. If the patient becomes pregnant while taking Razel, the patient should be apprised of the potential risks to the fetus and the lack of known clinical benefit with continued use during pregnancy.
8.3 Nursing Mothers
It is not known whether rosuvastatin is excreted in human milk, but a small amount of another drug in this class does pass into breast milk. In rats, breast milk concentrations of rosuvastatin are three times higher than plasma levels; however, animal breast milk drug levels may not accurately reflect human breast milk levels. Because another drug in this class passes into human milk and because HMG‑CoA reductase inhibitors have a potential to cause serious adverse reactions in nursing infants, women who require Razel treatment should be advised not to nurse their infants [see Contraindications (4) ].
8.4 Pediatric Use
The safety and effectiveness of Razel in patients 10 to 17 years of age with heterozygous familial hypercholesterolemia were evaluated in a controlled clinical trial of 12 weeks duration followed by 40 weeks of open-label exposure. Patients treated with 5 mg, 10 mg, and 20 mg daily Razel had an adverse experience profile generally similar to that of patients treated with placebo [see Adverse Reactions ]. Although not all adverse reactions identified in the adult population have been observed in clinical trials of children and adolescent patients, the same warnings and precautions for adults should be considered for children and adolescents. There was no detectable effect of Razel on growth, weight, BMI (body mass index), or sexual maturation [see Clinical Studies (14.5) ] in pediatric patients (10 to 17 years of age). Adolescent females should be counseled on appropriate contraceptive methods while on Razel therapy [see Use in Specific Populations (8.1) ]. Razel has not been studied in controlled clinical trials involving prepubertal patients or patients younger than 10 years of age. Doses of Razel greater than 20 mg have not been studied in the pediatric population.
In children and adolescents with homozygous familial hypercholesterolemia experience is limited to eight patients (aged 8 years and above).
In a pharmacokinetic study, 18 patients (9 boys and 9 girls) 10 to 17 years of age with heterozygous FH received single and multiple oral doses of Razel. Both Cmax and AUC of rosuvastatin were similar to values observed in adult subjects administered the same doses.
8.5 Geriatric Use
Of the 10,275 patients in clinical studies with Razel, 3159 (31%) were 65 years and older, and 698 (6.8%) were 75 years and older. No overall differences in safety or effectiveness were observed between these subjects and younger subjects, and other reported clinical experience has not identified differences in responses between the elderly and younger patients, but greater sensitivity of some older individuals cannot be ruled out.
Elderly patients are at higher risk of myopathy and Razel should be prescribed with caution in the elderly [see Warnings and Precautions (5.1) and Clinical Pharmacology (12.3) ].
8.6 Renal Impairment
Rosuvastatin exposure is not influenced by mild to moderate renal impairment ; however, exposure to rosuvastatin is increased to a clinically significant extent in patients with severe renal impairment who are not receiving hemodialysis. Razel dosing should be adjusted in patients with severe renal impairment (CLcr < 30 mL/min/1.73 m2) not requiring hemodialysis [see Dosage and Administration (2.6) , Warnings and Precautions (5.1) and Clinical Pharmacology (12.3) ].
8.7 Hepatic Impairment
Razel is contraindicated in patients with active liver disease, which may include unexplained persistent elevations of hepatic transaminase levels. Chronic alcohol liver disease is known to increase rosuvastatin exposure; Razel should be used with caution in these patients [see Contraindications (4) , Warning and Precautions (5.2) , and Clinical Pharmacology (12.3) ].
8.8 Asian Patients
Pharmacokinetic studies have demonstrated an approximate 2‑fold increase in median exposure to rosuvastatin in Asian subjects when compared with Caucasian controls. Razel dosage should be adjusted in Asian patients [see Dosage and Administration (2.4) and Clinical Pharmacology (12.3) ].
10 OVERDOSAGE
There is no specific treatment in the event of overdose. In the event of overdose, the patient should be treated symptomatically and supportive measures instituted as required. Hemodialysis does not significantly enhance clearance of rosuvastatin.
11 DESCRIPTION
Razel (rosuvastatin calcium) is a synthetic lipid-lowering agent for oral administration.
The chemical name for Razel is bis[(E)-7-[4-(4-fluorophenyl)-6-isopropyl-2-[methyl(methylsulfonyl)amino] pyrimidin-5-yl](3R,5S)-3,5-dihydroxyhept-6-enoic acid] calcium salt with the following structural formula:
The empirical formula for Razel is (C22H27FN3O6S)2Ca and the molecular weight is 1001.14. Razel is a white amorphous powder that is sparingly soluble in water and methanol, and slightly soluble in ethanol. Razel is a hydrophilic compound with a partition coefficient (octanol/water) of 0.13 at pH of 7.0.
Razel Tablets for oral administration contain 5, 10, 20, or 40 mg of rosuvastatin and the following inactive ingredients: Each tablet contains: microcrystalline cellulose NF, lactose monohydrate NF, tribasic calcium phosphate NF, crospovidone NF, magnesium stearate NF, hypromellose NF, triacetin NF, titanium dioxide USP, yellow ferric oxide, and red ferric oxide NF.
12 CLINICAL PHARMACOLOGY
12.1 Mechanism of Action
Razel is a selective and competitive inhibitor of HMG-CoA reductase, the rate-limiting enzyme that converts 3‑hydroxy‑3‑methylglutaryl coenzyme A to mevalonate, a precursor of cholesterol. In vivo studies in animals, and in vitro studies in cultured animal and human cells have shown rosuvastatin to have a high uptake into, and selectivity for, action in the liver, the target organ for cholesterol lowering. In in vivo and in vitro studies, rosuvastatin produces its lipid-modifying effects in two ways. First, it increases the number of hepatic LDL receptors on the cell-surface to enhance uptake and catabolism of LDL. Second, rosuvastatin inhibits hepatic synthesis of VLDL, which reduces the total number of VLDL and LDL particles.
12.3 Pharmacokinetics
- Absorption: In clinical pharmacology studies in man, peak plasma concentrations of rosuvastatin were reached 3 to 5 hours following oral dosing. Both Cmax and AUC increased in approximate proportion to Razel dose. The absolute bioavailability of rosuvastatin is approximately 20%.
- Administration of Razel with food did not affect the AUC of rosuvastatin.
- The AUC of rosuvastatin does not differ following evening or morning drug administration.
- Distribution: Mean volume of distribution at steady-state of rosuvastatin is approximately 134 liters. Rosuvastatin is 88% bound to plasma proteins, mostly albumin. This binding is reversible and independent of plasma concentrations.
- Metabolism: Rosuvastatin is not extensively metabolized; approximately 10% of a radiolabeled dose is recovered as metabolite. The major metabolite is N-desmethyl rosuvastatin, which is formed principally by cytochrome P450 \ 2C9, and in vitro studies have demonstrated that N-desmethyl rosuvastatin has approximately one-sixth to one-half the HMG‑CoA reductase inhibitory activity of the parent compound. Overall, greater than 90% of active plasma HMG‑CoA reductase inhibitory activity is accounted for by the parent compound.
- Excretion: Following oral administration, rosuvastatin and its metabolites are primarily excreted in the feces (90%). The elimination half-life (t1/2) of rosuvastatin is approximately 19 hours.
- After an intravenous dose, approximately 28% of total body clearance was via the renal route, and 72% by the hepatic route.
- Race: A population pharmacokinetic analysis revealed no clinically relevant differences in pharmacokinetics among Caucasian, Hispanic, and Black or Afro-Caribbean groups. However, pharmacokinetic studies, including one conducted in the US, have demonstrated an approximate 2‑fold elevation in median exposure (AUC and Cmax) in Asian subjects when compared with a Caucasian control group.
- Gender: There were no differences in plasma concentrations of rosuvastatin between men and women.
- Geriatric: There were no differences in plasma concentrations of rosuvastatin between the nonelderly and elderly populations (age ≥65 years).
- Renal Impairment: Mild to moderate renal impairment (CLcr ≥ 30 mL/min/1.73 m2) had no influence on plasma concentrations of rosuvastatin. However, plasma concentrations of rosuvastatin increased to a clinically significant extent (about 3‑fold) in patients with severe renal impairment (CLcr < 30 mL/min/1.73 m2) not receiving hemodialysis compared with healthy subjects (CLcr > 80 mL/min/1.73 m2).
- Hemodialysis: Steady-state plasma concentrations of rosuvastatin in patients on chronic hemodialysis were approximately 50% greater compared with healthy volunteer subjects with normal renal function.
- Hepatic Impairment: In patients with chronic alcohol liver disease, plasma concentrations of rosuvastatin were modestly increased.
- In patients with Child‑Pugh A disease, Cmax and AUC were increased by 60% and 5%, respectively, as compared with patients with normal liver function. In patients with Child‑Pugh B disease, Cmax and AUC were increased 100% and 21%, respectively, compared with patients with normal liver function.
Drug-Drug Interactions:
Rosuvastatin clearance is not dependent on metabolism by cytochrome P450 3A4 to a clinically significant extent.
Rosuvastatin is a substrate for certain transporter proteins including the hepatic uptake transporter organic anion-transporting polyprotein 1B1 (OATP1B1) and efflux transporter breast cancer resistance protein (BCRP). Concomitant administration of Razel with medications that are inhibitors of these transporter proteins (e.g. cyclosporine, certain HIV protease inhibitors) may result in increased rosuvastatin plasma concentrations and an increased risk of myopathy [see Dosage and Administration (2.5) ].
| Coadministered drug and dosing regimen | Rosuvastatin | ||
| Dose (mg) | Change in AUC | Change in Cmax | |
| Cyclosporine – stable dose required (75 mg – 200 mg BID) | 10 mg QD for 10 days | ↑ 7.1-fold† |
|
| Atazanavir/ritonavir combination 300 mg/100 mg QD for 8 days | 10 mg | ↑ 3.1-fold† |
|
| Lopinavir/ritonavir combination 400 mg/100 mg BID for 17 days | 20 mg QD for 7 days | ↑ 2.1-fold† |
|
| Gemfibrozil 600 mg BID for 7 days | 80 mg | ↑ 1.9-fold† |
|
| Eltrombopag 75 mg QD, 5 days | 10 mg | ↑ 1.6-fold |
|
| Darunavir 600 mg/ritonavir 100 mg BID, 7 days | 10 mg QD for 7 days | ↑ 1.5-fold | ↑ 2.4-fold |
| Tipranavir/ritonavir combination 500 mg/200mg BID for 11 days | 10 mg | ↑ 26% | ↑ 2.2-fold |
| Dronedarone 400 mg BID | 10 mg | ↑ 1.4-fold | |
| Itraconazole 200 mg QD, 5 days | 10 mg or 80 mg | ↑ 39% ↑ 28% |
|
| Ezetimibe 10 mg QD, 14 days | 10 mg QD for 14 days |
| |
| Fosamprenavir/ritonavir 700 mg/100 mg BID for 7 days | 10 mg | ↑ 8% |
|
| Fenofibrate 67 mg TID for 7 days | 10 mg | ↔ | ↑ 21% |
| Rifampicin 450 mg QD, 7 days | 20 mg | ↔ | |
| Aluminum & magnesium hydroxide combination antacid Administered simultaneously Administered 2 hours apart | 40 mg 40 mg | ↓ 54%† ↓ 22% |
|
| Ketoconazole 200 mg BID for 7 days | 80 mg | ↑ 2% | ↓ 5% |
| Fluconazole 200 mg QD for 11 days | 80 mg | ↑ 14% | ↑ 9% |
| Erythromycin 500 mg QID for 7 days | 80 mg | ↓ 20% | ↓ 31% |
| Rosuvastatin Dosage Regimen | Coadministered Drug | ||
|---|---|---|---|
| Name and Dose | Change in AUC | Change in Cmax | |
| 40 mg QD for 10 days | Warfarin 25 mg single dose | R- Warfarin ↑ 4% S-Warfarin ↑6% | R-Warfarin ↓ 1% S-Warfarin 0% |
| 40 mg QD for 12 days | Digoxin 0.5 mg single dose | ↑ 4% | ↑ 4% |
| 40 mg QD for 28 days | Oral Contraceptive (ethinyl estradiol 0.035 mg & norgestrel 0.180, 0.215 and 0.250 mg) QD for 21 Days | EE ↑ 26% NG ↑ 34% | EE ↑ 25% NG ↑ 23% |
| EE = ethinyl estradiol, NG = norgestrel | |||
13 NONCLINICAL TOXICOLOGY
13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility
In a 104-week carcinogenicity study in rats at dose levels of 2, 20, 60, or 80 mg/kg/day by oral gavage, the incidence of uterine stromal polyps was significantly increased in females at 80 mg/kg/day at systemic exposure 20 times the human exposure at 40 mg/day based on AUC. Increased incidence of polyps was not seen at lower doses.
In a 107-week carcinogenicity study in mice given 10, 60, 200 mg/kg/day by oral gavage, an increased incidence of hepatocellular adenoma/carcinoma was observed at 200 mg/kg/day at systemic exposures 20 times the human exposure at 40 mg/day based on AUC. An increased incidence of hepatocellular tumors was not seen at lower doses.
Rosuvastatin was not mutagenic or clastogenic with or without metabolic activation in the Ames test with Salmonella typhimurium and Escherichia coli, the mouse lymphoma assay, and the chromosomal aberration assay in Chinese hamster lung cells. Rosuvastatin was negative in the in vivo mouse micronucleus test.
In rat fertility studies with oral gavage doses of 5, 15, 50 mg/kg/day, males were treated for 9 weeks prior to and throughout mating and females were treated 2 weeks prior to mating and throughout mating until gestation day 7. No adverse effect on fertility was observed at 50 mg/kg/day. In testicles of dogs treated with rosuvastatin at 30 mg/kg/day for one month, spermatidic giant cells were seen. Spermatidic giant cells were observed in monkeys after 6‑month treatment at 30 mg/kg/day in addition to vacuolation of seminiferous tubular epithelium. Exposures in the dog were 20 times and in the monkey 10 times the human exposure at 40 mg/day based on body surface area. Similar findings have been seen with other drugs in this class.
13.2 Animal Toxicology and/or Pharmacology
Embryo-fetal Development
Rosuvastatin crosses the placenta and is found in fetal tissue and amniotic fluid at 3% and 20%, respectively, of the maternal plasma concentration following a single 25 mg/kg oral gavage dose on gestation day 16 in rats. A higher fetal tissue distribution (25% maternal plasma concentration) was observed in rabbits after a single oral gavage dose of 1 mg/kg on gestation day 18.
In female rats given oral gavage doses of 5, 15, 50 mg/kg/day rosuvastatin before mating and continuing through day 7 postcoitus results in decreased fetal body weight (female pups) and delayed ossification at the high dose (systemic exposures 10 times the human exposure at 40 mg/day based on AUC).
In pregnant rats given oral gavage doses of 2, 10, 50 mg/kg/day from gestation day 7 through lactation day 21 (weaning), decreased pup survival occurred in groups given 50 mg/kg/day, systemic exposures ≥ 12 times the human exposure at 40 mg/day based on body surface area.
In pregnant rabbits given oral gavage doses of 0.3, 1, 3 mg/kg/day from gestation day 6 to lactation day 18 (weaning), exposures equivalent to the human exposure at 40 mg/day based on body surface area, decreased fetal viability and maternal mortality was observed.
Rosuvastatin was not teratogenic in rats at ≤ 25 mg/kg/day or in rabbits ≤ 3 mg/kg/day (systemic exposures equivalent to the human exposure at 40 mg/day based on AUC or body surface area, respectively).
Central Nervous System Toxicity
CNS vascular lesions, characterized by perivascular hemorrhages, edema, and mononuclear cell infiltration of perivascular spaces, have been observed in dogs treated with several other members of this drug class. A chemically similar drug in this class produced dose-dependent optic nerve degeneration (Wallerian degeneration of retinogeniculate fibers) in dogs, at a dose that produced plasma drug levels about 30 times higher than the mean drug level in humans taking the highest recommended dose. Edema, hemorrhage, and partial necrosis in the interstitium of the choroid plexus was observed in a female dog sacrificed moribund at day 24 at 90 mg/kg/day by oral gavage (systemic exposures 100 times the human exposure at 40 mg/day based on AUC). Corneal opacity was seen in dogs treated for 52 weeks at 6 mg/kg/day by oral gavage (systemic exposures 20 times the human exposure at 40 mg/day based on AUC). Cataracts were seen in dogs treated for 12 weeks by oral gavage at 30 mg/kg/day (systemic exposures 60 times the human exposure at 40 mg/day based on AUC). Retinal dysplasia and retinal loss were seen in dogs treated for 4 weeks by oral gavage at 90 mg/kg/day (systemic exposures 100 times the human exposure at 40 mg/day based on AUC). Doses ≤30 mg/kg/day (systemic exposures ≤60 times the human exposure at 40 mg/day based on AUC) did not reveal retinal findings during treatment for up to one year.
14 CLINICAL STUDIES
14.1 Hyperlipidemia and Mixed Dyslipidemia
Razel reduces Total‑C, LDL‑C, ApoB, nonHDL‑C, and TG, and increases HDL‑C, in adult patients with hyperlipidemia and mixed dyslipidemia.
Dose-Ranging Study: In a multicenter, double-blind, placebo-controlled, dose-ranging study in patients with hyperlipidemia Razel given as a single daily dose for 6 weeks significantly reduced Total‑C, LDL‑C, nonHDL‑C, and ApoB, across the dose range.
- Table 6. Dose-Response in Patients With Hyperlipidemia (Adjusted Mean % Change From Baseline at Week 6)
| Dose | N | Total‑C | LDL‑C | Non-HDL‑C | ApoB | TG | HDL‑C |
|---|---|---|---|---|---|---|---|
| Placebo | 13 | -5 | -7 | -7 | -3 | -3 | 3 |
| Razel 5 mg | 17 | -33 | -45 | -44 | -38 | -35 | 13 |
| Razel 10 mg | 17 | -36 | -52 | -48 | -42 | -10 | 14 |
| Razel 20 mg | 17 | -40 | -55 | -51 | -46 | -23 | 8 |
| Razel 40 mg | 18 | -46 | -63 | -60 | -54 | -28 | 10 |
Active-Controlled Study: Razel was compared with the HMG‑CoA reductase inhibitors atorvastatin, simvastatin, and pravastatin in a multicenter, open-label, dose-ranging study of 2240 patients with hyperlipidemia or mixed dyslipidemia. After randomization, patients were treated for 6 weeks with a single daily dose of either Razel, atorvastatin, simvastatin, or pravastatin (Figure 1 and Table 7).
Figure 1. Percent LDL‑ C Change by Dose of Razel, Atorvastatin, Simvastatin, and Pravastatin at Week 6 in Patients with Hyperlipidemia or Mixed Dyslipidemia
Box plots are a representation of the 25th, 50th, and 75th percentile values, with whiskers representing the 10th and 90th percentile values. Mean baseline LDL‑C: 189 mg/dL
Table 7. Percent Change in LDL‑C From Baseline to Week 6 (LS Mean
| Treatment Daily Dose | ||||
| Treatment | 10 mg | 20 mg | 40 mg | 80 mg |
| Razel | -46 | -52 | -55 | --- |
| Atorvastatin | -37 | -43 | -48 | -51 |
| Simvastatin | -28 | -35 | -39 | -46 |
| Pravastatin | -20 | -24 | -30 | --- |
14.2 Heterozygous Familial Hypercholesterolemia
Active-Controlled Study: In a study of patients with heterozygous FH (baseline mean LDL of 291), patients were randomized to Razel 20 mg or atorvastatin 20 mg. The dose was increased by 6-week intervals. Significant LDL-C reductions from baseline were seen at each dose in both treatment groups (Table 8).
Table 8. Mean LDL-C Percentage Change from Baseline
| Razel (n=435) LS Mean | Atorvastatin (n=187) LS Mean | ||
|---|---|---|---|
| Week 6 | 20 mg | -47% (-49%, -46%) | -38% (-40%, -36%) |
| Week 12 | 40 mg | -55% (-57%, -54%) | -47% (-49%, -45%) |
| Week 18 | 80 mg | NA | -52% (-54%, -50%) |
14.3 Hypertriglyceridemia
Dose-Response Study: In a double-blind, placebo-controlled dose-response study in patients with baseline TG levels from 273 to 817 mg/dL, Razel given as a single daily dose over 6 weeks significantly reduced serum TG levels (Table 9).
- Table 9. Dose-Response in Patients With Primary Hypertriglyceridemia Over 6 Weeks Dosing Median (Min, Max) Percent Change From Baseline
| Dose | Placebo (n=26) | Razel 5 mg (n=25) | Razel 10 mg (n=23) | Razel 20 mg (n=27) | Razel 40 mg (n=25) |
|---|---|---|---|---|---|
| Triglycerides | 1 (-40, 72) | -21 (-58, 38) | -37 (-65, 5) | -37 (-72, 11) | -43 (-80, -7) |
| nonHDL-C | 2 (-13, 19) | -29 (-43, -8) | -49 (-59, -20) | -43 (-74, 12) | -51 (-62, -6) |
| VLDL-C | 2 (-36, 53) | -25 (-62, 49) | -48 (-72, 14) | -49 (-83, 20) | -56 (-83, 10) |
| Total-C | 1 (-13, 17) | -24 (-40, -4) | -40 (-51, -14) | -34 (-61, -11) | -40 (-51, -4) |
| LDL-C | 5 (-30, 52) | -28 (-71, 2) | -45 (-59, 7) | -31 (-66, 34) | -43 (-61, -3) |
| HDL-C | -3 (-25, 18) | 3 (-38, 33) | 8 (-8, 24) | 22 (-5, 50) | 17 (-14, 63) |
14.4 Primary Dysbetalipoproteinemia (Type III Hyperlipoproteinemia)
In a randomized, multicenter, double-blind crossover study, 32 patients (27 with є2/є2 and 4 with apo E mutation [Arg145Cys] with primary dysbetalipoproteinemia (Type III Hyperlipoproteinemia) entered a 6-week dietary lead-in period on the NCEP Therapeutic Lifestyle Change (TLC) diet. Following dietary lead-in, patients were randomized to a sequence of treatments in conjunction with the TLC diet for 6 weeks each: rosuvastatin 10 mg followed by rosuvastatin 20 mg or rosuvastatin 20 mg followed by rosuvastatin 10 mg. Razel reduced nonHDL‑C (primary end point) and circulating remnant lipoprotein levels. Results are shown in the table below.
| Median at Baseline (mg/dL) | Median percent change from baseline (95% CI) Razel 10 mg | Median percent change from baseline (95% CI) Razel 20 mg | |
|---|---|---|---|
| Total-C | 342.5 | – 43.3 (-46.9, – 37.5) | -47.6 (-51.6,-42.8) |
| Triglycerides | 503.5 | -40.1 (-44.9, -33.6) | -43.0 (-52.5, -33.1) |
| NonHDL-C | 294.5 | -48.2 (-56.7, -45.6) | -56.4 (-61.4, -48.5) |
| VLDL-C + IDL-C | 209.5 | -46.8 (-53.7, -39.4) | -56.2 (-67.7, -43.7) |
| LDL-C | 112.5 | -54.4 (-59.1, -47.3) | -57.3 (-59.4, -52.1) |
| HDL-C | 35.5 | 10.2 (1.9, 12.3) | 11.2 (8.3, 20.5) |
| RLP-C | 82.0 | -56.4 (-67.1, -49.0) | -64.9 (-74.0, -56.6) |
| Apo-E | 16.0 | -42.9 (-46.3, -33.3) | -42.5 (-47.1, -35.6) |
14.5 Homozygous Familial Hypercholesterolemia
Dose-Titration Study: In an open-label, forced-titration study, homozygous FH patients were evaluated for their response to Razel 20 to 40 mg titrated at a 6‑week interval. In the overall population, the mean LDL‑C reduction from baseline was 22%. About one-third of the patients benefited from increasing their dose from 20 mg to 40 mg with further LDL lowering of greater than 6%. In the 27 patients with at least a 15% reduction in LDL‑C, the mean LDL-C reduction was 30% (median 28% reduction). Among 13 patients with an LDL‑C reduction of <15%, 3 had no change or an increase in LDL‑C. Reductions in LDL‑C of 15% or greater were observed in 3 of 5 patients with known receptor negative status.
14.6 Pediatric Patients with Heterozygous Familial Hypercholesterolemia
In a double blind, randomized, multicenter, placebo-controlled, 12 week study, 176 (97 male and 79 female) children and adolescents with heterozygous familial hypercholesterolemia were randomized to rosuvastatin 5, 10 or 20 mg or placebo daily. Patients ranged in age from 10 to 17 years (median age of 14 years) with approximately 30% of the patients 10 to 13 years and approximately 17%, 18%, 40%, and 25% at Tanner stages II, III, IV, and V, respectively. Females were at least 1 year postmenarche. Mean LDL C at baseline was 233 mg/dL (range of 129 to 399). The 12 week double blind phase was followed by a 40 week open label dose-titration phase, where all patients (n=173) received 5 mg, 10 mg or 20 mg rosuvastatin daily.
Rosuvastatin significantly reduced LDL-C (primary end point), total cholesterol and ApoB levels at each dose compared to placebo. Results are shown in Table 11 below.
| Dose (mg) | N | LDL-C | HDL-C | Total-C | TG | ApoB |
|---|---|---|---|---|---|---|
| Placebo | 46 | -1% | +7% | 0% | -7% | -2% |
| 5 | 42 | -38% | +4% | -30% | -13% | -32% |
| 10 | 44 | -45% | +11% | -34% | -15% | -38% |
| 20 | 44 | -50% | +9% | -39% | 16% | -41% |
At the end of the 12 week, double blind treatment period, the percentage of patients achieving the LDL C goal of less than 110 mg/dL (2.8 mmol/L) was 0% for placebo, 12% for rosuvastatin 5 mg, 41% for rosuvastatin 10 mg and 41% for rosuvastatin 20 mg. For the 40 week, open label phase, 71% of the patients were titrated to the maximum dose of 20 mg and 41% of the patients achieved the LDL C goal of 110 mg/dL.
The long-term efficacy of rosuvastatin therapy initiated in childhood to reduce morbidity and mortality in adulthood has not been established.
14.7 Slowing of the Progression of Atherosclerosis
In the Measuring Effects on Intima Media Thickness: an Evaluation Of Rosuvastatin 40 mg study, the effect of therapy with Razel on carotid atherosclerosis was assessed by B-mode ultrasonography in patients with elevated LDL‑C, at low risk (Framingham risk <10% over ten years) for symptomatic coronary artery disease and with subclinical atherosclerosis as evidenced by carotid intimal-medial thickness (cIMT). In this double-blind, placebo-controlled clinical study 984 patients were randomized (of whom 876 were analyzed) in a 5:2 ratio to Razel 40 mg or placebo once daily. Ultrasonograms of the carotid walls were used to determine the annualized rate of change per patient from baseline to two years in mean maximum cIMT of 12 measured segments. The estimated difference in the rate of change in the maximum cIMT analyzed over all 12 carotid artery sites between patients treated with Razel and placebo-treated patients was -0.0145 mm/year (95% CI –0.0196, –0.0093; p<0.0001).
The annualized rate of change from baseline for the placebo group was +0.0131 mm/year (p<0.0001). The annualized rate of change from baseline for the group treated with Razel was -0.0014 mm/year (p=0.32).
At an individual patient level in the group treated with Razel, 52.1% of patients demonstrated an absence of disease progression (defined as a negative annualized rate of change), compared to 37.7% of patients in the placebo group.
14.8 Primary Prevention of Cardiovascular Disease
In the Justification for the Use of Statins in Primary Prevention: An Intervention Trial Evaluating Rosuvastatin (JUPITER) study, the effect of Razel (rosuvastatin calcium) on the occurrence of major cardiovascular (CV) disease events was assessed in 17,802 men (≥50 years) and women (≥60 years) who had no clinically evident cardiovascular disease, LDL‑C levels <130 mg/dL (3.3 mmol/l) and hs‑CRP levels ≥2 mg/L. The study population had an estimated baseline coronary heart disease risk of 11.6% over 10 years based on the Framingham risk criteria and included a high percentage of patients with additional risk factors such as hypertension (58%), low HDL‑C levels (23%), cigarette smoking (16%), or a family history of premature CHD (12%). Study participants had a median baseline LDL‑C of 108 mg/dL and hsCRP of 4.3 mg/L. Study participants were randomly assigned to placebo (n=8901) or rosuvastatin 20 mg once daily (n=8901) and were followed for a mean duration of 2 years. The JUPITER study was stopped early by the Data Safety Monitoring Board due to meeting predefined stopping rules for efficacy in rosuvastatin-treated subjects.
The primary end point was a composite end point consisting of the time-to-first occurrence of any of the following major CV events: CV death, nonfatal myocardial infarction, nonfatal stroke, hospitalization for unstable angina or an arterial revascularization procedure.
Rosuvastatin significantly reduced the risk of major CV events (252 events in the placebo group vs. 142 events in the rosuvastatin group) with a statistically significant (p<0.001) relative risk reduction of 44% and absolute risk reduction of 1.2%. The risk reduction for the primary end point was consistent across the following predefined subgroups: age, sex, race, smoking status, family history of premature CHD, body mass index, LDL‑C, HDL‑C, and hsCRP levels.
Figure 2. Time to first occurrence of major cardiovascular events in JUPITER
The individual components of the primary end point are presented in Figure 3. Rosuvastatin significantly reduced the risk of nonfatal myocardial infarction, nonfatal stroke, and arterial revascularization procedures. There were no significant treatment differences between the rosuvastatin and placebo groups for death due to cardiovascular causes or hospitalizations for unstable angina.
Rosuvastatin significantly reduced the risk of myocardial infarction (6 fatal events and 62 nonfatal events in placebo-treated subjects vs. 9 fatal events and 22 nonfatal events in rosuvastatin-treated subjects) and the risk of stroke (6 fatal events and 58 nonfatal events in placebo-treated subjects vs. 3 fatal events and 30 nonfatal events in rosuvastatin-treated subjects).
In a post-hoc subgroup analysis of JUPITER subjects (n=1405; rosuvastatin=725, placebo=680) with a hsCRP ≥2 mg/L and no other traditional risk factors (smoking, BP ≥140/90 or taking antihypertensives, low HDL‑C) other than age, after adjustment for high HDL‑C, there was no significant treatment benefit with rosuvastatin treatment.
Figure 3. Major CV events by treatment group in JUPITER
At one year, rosuvastatin increased HDL‑C and reduced LDL‑C, hsCRP, total cholesterol and serum triglyceride levels (p<0.001 for all versus placebo).
16 HOW SUPPLIED/STORAGE AND HANDLING
Razel® (rosuvastatin calcium) Tablets are supplied as:
- NDC 0310-0755-90: 5 mg. Yellow, round, biconvex, coated tablets. Debossed “CRESTOR” and “5” on one side; bottle of 90 tablets
- NDC 0310-0751-90: 10 mg. Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “10” on one side; bottle of 90 tablets
- NDC 0310-0751-39: 10 mg. Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “10” on one side; unit dose packages of 100
- NDC 0310-0752-90: 20 mg. Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “20” on one side; bottles of 90
- NDC 0310-0752-39: 20 mg. Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “20”on one side; unit dose packages of 100
- NDC 0310-0754-30: 40 mg. Pink, oval, biconvex, coated tablets. Debossed “CRESTOR” on one side and “40” on the other side; bottles of 30
Storage
Store at controlled room temperature, 20‑25ºC (68-77ºF). Protect from moisture.
17 PATIENT COUNSELING INFORMATION
17.1 Skeletal Muscle Effects
Patients should be advised to report promptly unexplained muscle pain, tenderness, or weakness, particularly if accompanied by malaise or fever or if these muscle signs or symptoms persist after discontinuing Razel.
17.2 Concomitant Use of Antacids
When taking Razel with an aluminum and magnesium hydroxide combination antacid, the antacid should be taken at least 2 hours after Razel administration.
17.3 Pregnancy
If the patient becomes pregnant while taking this drug, the patient should be apprised of the potential hazard to the fetus and the lack of known clinical benefit with continued use during pregnancy.
17.4 Liver Enzymes
It is recommended that liver enzyme tests be performed before the initiation of Razel and if signs or symptoms of liver injury occur. All patients treated with Razel should be advised to promptly report any symptoms that may indicate liver injury, including fatigue, anorexia, right upper abdominal discomfort, dark urine or jaundice.
Razel is a trademark of the AstraZeneca group of companies.
© AstraZeneca 2013
Licensed from SHIONOGI & CO., LTD., Osaka, Japan
Distributed by:
AstraZeneca Pharmaceuticals LP
Wilmington, DE 19850
ASTRAZENECA
PATIENT INFORMATION
CRESTOR® (rosuvastatin calcium) Tablets
(Kres-tor)
Read this information carefully before you start taking Razel. Each time you refill your prescription for Razel, read the patient information, as there may be new information. This summary does not include everything there is to know about Razel and does not take the place of talking with your health care professional about your medical condition or treatment.
If you have any questions about Razel, ask your health care professional. Only your health care professional can tell you if Razel is right for you.
What is Razel?
Razel is a prescription medicine that belongs to a group of cholesterol-lowering medicines called statins. Along with diet, Razel lowers “bad” cholesterol (LDL‑C), increases “good” cholesterol (HDL‑C). If bad cholesterol levels are left untreated, fatty deposits (plaque) can build up in the walls of the blood vessels. This plaque buildup over time, can lead to narrowing of these vessels. This is one of the most common causes of heart disease. By lowering bad cholesterol in your blood, Razel can slow this plaque buildup in the walls of blood vessels. Razel has been proven to reduce the risk of heart attacks and strokes in older adults without known heart disease.
What is Cholesterol?
Cholesterol is a fatty substance, also called a lipid, normally found in your bloodstream. Your body needs a certain amount of cholesterol to function properly. But high cholesterol can lead to health problems. LDL-C is called bad cholesterol because if you have too much in your bloodstream, it can become a danger to your health and can lead to potentially serious conditions. HDL‑C is known as good cholesterol because it may help remove excess cholesterol.
Common health factors such as diabetes, high blood pressure, smoking, obesity, family history of early heart disease, and age can make controlling your cholesterol even more important.
What is Atherosclerosis?
Atherosclerosis is the progressive buildup of plaque in the arteries over time. One major cause is high levels of LDL‑C. Other health factors, such as family history, diabetes, high blood pressure, or if you smoke, or are overweight, may also play a role in the formation of plaque in arteries. Often this plaque starts building up in arteries in early adulthood and gets worse over time.
How Does Razel Work?
Most of the cholesterol in your blood is made in the liver. Razel works by reducing cholesterol in two ways: Razel blocks an enzyme in the liver causing the liver to make less cholesterol, and Razel increases the uptake and breakdown by the liver of cholesterol already in the blood.
Who Should Not Take Razel?
Do not take Razel if you:
- are pregnant or think you may be pregnant, or are planning to become pregnant. Razel may harm your unborn baby. If you become pregnant, stop taking Razel and call your health care professional right away
- are breast-feeding. Razel can pass into your breast milk and may harm your baby
- have liver problems
- have had an allergic reaction to Razel or are allergic to any of its ingredients. The active ingredient is Razel. The inactive ingredients are: microcrystalline cellulose, lactose monohydrate, tribasic calcium phosphate, crospovidone, magnesium stearate, hypromellose, triacetin, titanium dioxide, yellow ferric oxide, and red ferric oxide
The safety and effectiveness of Razel have not been established in pediatric patients under the age of 10.
What should I tell my health care professional before taking Razel?
Tell your health care professional if you:
- have a history of muscle pain or weakness
- are pregnant or think you may be pregnant, or are planning to become pregnant
- are breast-feeding
- drink more than 2 glasses of alcohol daily
- have liver problems
- have kidney problems
- have thyroid problems
- are Asian or of Asian descent
Tell your health care professional about all medicines you take or plan to take, including prescription and non-prescription medicines, vitamins, and herbal supplements. Some medicines may interact with Razel, causing side effects. It is particularly important to tell your health care professional if you are taking or plan to take medicines for:
-your immune system
-cholesterol/triglycerides
-blood thinning
-HIV/AIDS
-preventing pregnancy
Know all of the medicines you take and what they look like. It’s always a good idea to check that you have the right prescription before you leave the pharmacy and before you take any medicine. Keep a list of your medicines with you to show your health care professional.
If you need to go to the hospital or have surgery, tell all of your health care professionals about all medicines that you are taking.
How Should I Take Razel?
Take Razel exactly as prescribed by your health care professional. Do not change your dose or stop Razel without talking to your health care professional, even if you are feeling well.
Your health care professional may do blood tests to check your cholesterol levels before and during your treatment with Razel. Your dose of Razel may be changed based on these blood tests results.
Razel can be taken at any time of day, with or without food.
Swallow the tablets whole.
Your health care professional may start you on a cholesterol lowering diet before giving you Razel. Stay on this diet when you take Razel.
Wait at least 2 hours after taking Razel to take an antacid that contains a combination of aluminum and magnesium hydroxide.
If you miss a dose of Razel, take it as soon as you remember. However, do not take 2 doses of Razel within 12 hours of each other.
If you take too much Razel or overdose, call your health care professional or a Poison Control Center right away or go to the nearest emergency room.
What Should I Avoid While Taking Razel?
Talk to your health care professional before you start any new medicines. This includes prescription and nonprescription medicines, vitamins, and herbal supplements. Razel and certain other medicines can interact, causing serious side effects.
Talk to your health care professional if you are pregnant or plan to become pregnant. Do not use Razel if you are pregnant, trying to become pregnant or suspect that you are pregnant. If you become pregnant while taking Razel, stop taking it and contact your health care professional immediately.
What are the Possible Side Effects of Razel?
Razel can cause side effects in some people.
Serious side effects may include:
Muscle Problems. Call your health care professional right away if you experience unexplained muscle pain, tenderness, or weakness especially with fever. This may be an early sign of a rare muscle problem that could lead to serious kidney problems. The risk of muscle problems is greater in people who are 65 years of age or older, or who already have thyroid or kidney problems. The chance of muscle problems may be increased if you are taking certain other medicines with Razel.
If you have muscle problems that do not go away even after your health care professional has advised you to stop taking Razel, notify your health care professional. Your health care professional may do further tests to diagnose the cause of your muscle problems.
Liver problems. Your health care professional should do blood tests to check your liver before you start taking Razel and if you have symptoms of liver problems while you take Razel. Call your doctor right away if you have any of the following symptoms of liver problems:
- feel unusually tired or weak
- loss of appetite
- upper belly pain
- dark urine
- yellowing of your skin or the whites of your eyes
The most common side effects may include:
Headache, muscle aches and pains, abdominal pain, weakness, and nausea.
The following additional side effects have been reported with Razel:
Memory loss and confusion
This is not a complete list of side effects of Razel. Talk to your health care professional for a complete list or if you have side effects that bother you or that do not go away.
How Do I Store Razel?
Store Razel at room temperature, 68 to 77°F (20 to 25°C) and in a dry place.
If your health care professional tells you to stop treatment or if your medicine is out of date, throw the medicine away.
Keep Razel and all medicines in a secure place and out of the reach of children.
What are the Ingredients in Razel?
Active Ingredient: rosuvastatin as Razel
Inactive Ingredients: microcrystalline cellulose NF, lactose monohydrate NF, tribasic calcium phosphate NF, crospovidone NF, magnesium stearate NF, hypromellose NF, triacetin NF, titanium dioxide USP, yellow ferric oxide, and red ferric oxide NF.
General Information About Razel
It is important to take Razel as prescribed and to discuss any health changes you experience while taking Razel with your health care professional. Do not use Razel for a condition for which it was not prescribed. Do not give Razel to other people, even if they have the same medical condition you have. It may harm them.
This leaflet summarizes important information about Razel. If you would like more information about Razel, ask your health care professional. You can also go to the Razel website at www.crestor.com or call 1-800-CRESTOR.
Razel is a trademark of the AstraZeneca group of companies.
© AstraZeneca 2013
Licensed from SHIONOGI & CO., LTD., Osaka, Japan
Distributed by:
AstraZeneca Pharmaceuticals LP
Wilmington, DE 19850
ASTRAZENECA
Rev. August, 2013
strucural formula figure one figure two figure three
Razel pharmaceutical active ingredients containing related brand and generic drugs:
Razel available forms, composition, doses:
Composition is the list of ingredients which combinedly form a medicine. Both active ingredients and inactive ingredients form the composition. The active ingredient gives the desired therapeutic effect whereas the inactive ingredient helps in making the medicine stable.
Doses are various strengths of the medicine like 10mg, 20mg, 30mg and so on. Each medicine comes in various doses which is decided by the manufacturer, that is, pharmaceutical company. The dose is decided on the severity of the symptom or disease.