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  • CRESTOR ROSUVASTATIN CALCIUM 10 mg/1 AstraZeneca Pharmaceuticals LP
FDA Drug information

CRESTOR

Read time: 3 mins
Marketing start date: 03 Dec 2024

Summary of product characteristics


Adverse Reactions

6 ADVERSE REACTIONS The following important adverse reactions are described below and elsewhere in the labeling: Myopathy and Rhabdomyolysis [see Warnings and Precautions (5.1) ] Immune-Mediated Necrotizing Myopathy [see Warnings and Precautions (5.2) ] Hepatic Dysfunction [see Warnings and Precautions (5.3) ] Proteinuria and Hematuria [see Warnings and Precautions (5.4) ] Increases in HbA1c and Fasting Serum Glucose Levels [see Warnings and Precautions (5.5) ] Most frequent adverse reactions (rate ≥2%) are headache, nausea, myalgia, asthenia, and constipation. ( 6.1 ) To report SUSPECTED ADVERSE REACTIONS, contact AstraZeneca at 1-800-236-9933 or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch. 6.1 Clinical Trials Experience Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials 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 2. These studies had a treatment duration of up to 12 weeks. Table 2: Adverse Reactions Reported in ≥2% of Patients Treated with CRESTOR and > Placebo in Placebo-Controlled Trials Adverse Reactions Placebo N=382 % CRESTOR 5 mg N=291 % CRESTOR 10 mg N=283 % CRESTOR 20 mg N=64 % CRESTOR 40 mg N=106 % Total CRESTOR 5 mg ‑ 40 mg N=744 % Headache 5.0 5.5 4.9 3.1 8.5 5.5 Nausea 3.1 3.8 3.5 6.3 0 3.4 Myalgia 1.3 3.1 2.1 6.3 1.9 2.8 Asthenia 2.6 2.4 3.2 4.7 0.9 2.7 Constipation 2.4 2.1 2.1 4.7 2.8 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; elevated creatine phosphokinase, transaminases, glucose, glutamyl transpeptidase, alkaline phosphatase, and bilirubin; and thyroid function abnormalities. In the METEOR study, patients were treated with CRESTOR 40 mg (n=700) or placebo (n=281) with a mean treatment duration of 1.7 years. Adverse reactions reported in ≥2% of patients and at a rate greater than placebo are shown in Table 3. Table 3: Adverse Reactions Reported in ≥2% of Patients Treated with CRESTOR and > Placebo in the METEOR Trial Adverse Reactions Placebo N=281 % CRESTOR 40 mg N=700 % Myalgia 12.1 12.7 Arthralgia 7.1 10.1 Headache 5.3 6.4 Dizziness 2.8 4.0 Increased CPK 0.7 2.6 Abdominal pain 1.8 2.4 ALT greater than 3x ULN Frequency recorded as abnormal laboratory value. 0.7 2.2 In the JUPITER study, patients were treated with CRESTOR 20 mg (n=8901) or placebo (n=8901) for a mean duration of 2 years. In JUPITER, there was a significantly higher frequency of diabetes mellitus reported in patients taking CRESTOR (2.8%) versus patients taking placebo (2.3%). Mean HbA1c was significantly increased by 0.1% in CRESTOR-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 CRESTOR-treated versus placebo-treated patients [see Warnings and Precautions (5.5) and Clinical Studies (14) ] . Adverse reactions reported in ≥2% of patients and at a rate greater than placebo are shown in Table 4. Table 4: Adverse Reactions Reported in ≥2% of Patients Treated with CRESTOR and > Placebo in the JUPITER Trial Adverse Reactions Placebo N=8901 % CRESTOR 20 mg N=8901 % Myalgia 6.6 7.6 Arthralgia 3.2 3.8 Constipation 3.0 3.3 Diabetes mellitus 2.3 2.8 Nausea 2.3 2.4 Pediatric Patients with HeFH In a 12‑week controlled study in pediatric patients 10 to 17 years of age with HeFH with CRESTOR 5 to 20 mg daily [see Use in Specific Populations (8.4) and Clinical Studies (14) ] , elevations in serum CK greater than 10 x ULN were observed more frequently in CRESTOR-treated patients compared with patients receiving placebo. Four of 130 (3%) patients treated with CRESTOR (2 treated with 10 mg and 2 treated with 20 mg) had increased CK greater than 10 x ULN, compared to 0 of 46 patients on placebo. 6.2 Postmarketing Experience The following adverse reactions have been identified during postapproval use of CRESTOR. 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. Blood Disorders : thrombocytopenia Hepatobiliary Disorders : hepatitis, jaundice, fatal and non-fatal hepatic failure Musculoskeletal Disorders : arthralgia, rare reports of immune-mediated necrotizing myopathy associated with statin use Nervous System Disorders : peripheral neuropathy, rare postmarketing reports of cognitive impairment (e.g., memory loss, forgetfulness, amnesia, memory impairment, and confusion) associated with the use of 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). Psychiatric Disorders : depression, sleep disorders (including insomnia and nightmares) Reproductive System and Breast Disorders : gynecomastia Respiratory Disorders : interstitial lung disease Skin and Subcutaneous Tissue Disorders : drug reaction with eosinophilia and systemic symptoms (DRESS), lichenoid drug eruption

Contraindications

4 CONTRAINDICATIONS CRESTOR is contraindicated in the following conditions: • Acute liver failure or decompensated cirrhosis [see Warnings and Precautions (5.3) ] . • Hypersensitivity to rosuvastatin or any excipients in CRESTOR. Hypersensitivity reactions including rash, pruritus, urticaria, and angioedema have been reported with CRESTOR [see Adverse Reactions (6.1) ]. Acute liver failure or decompensated cirrhosis. ( 4 ) Hypersensitivity to rosuvastatin or any excipients in CRESTOR. ( 4 )

Description

11 DESCRIPTION CRESTOR (rosuvastatin) is a 3-hydroxy-3-methylglutaryl coenzyme A (HMG CoA)-reductase inhibitor. The chemical name for rosuvastatin calcium 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 rosuvastatin calcium is (C 22 H 27 FN 3 O 6 S) 2 Ca and the molecular weight is 1001.14. Rosuvastatin calcium is a white amorphous powder that is sparingly soluble in water and methanol, and slightly soluble in ethanol. Rosuvastatin calcium is a hydrophilic compound with a partition coefficient (octanol/water) of 0.13 at pH of 7.0. CRESTOR tablets for oral use contain rosuvastatin 5 mg, 10 mg, 20 mg, or 40 mg (equivalent to 5.2 mg, 10.4 mg, 20.8 mg, and 41.6 mg rosuvastatin calcium) and the following inactive ingredients: crospovidone NF, hypromellose NF, lactose monohydrate NF, magnesium stearate NF, microcrystalline cellulose NF, red ferric oxide NF, titanium dioxide USP, triacetin NF, tribasic calcium phosphate NF and yellow ferric oxide. strucural formula

Dosage And Administration

2 DOSAGE AND ADMINISTRATION Take orally with or without food, at any time of day. ( 2.1 ) Assess LDL-C when clinically appropriate, as early as 4 weeks after initiating CRESTOR, and adjust dosage if necessary. ( 2.1 ) Adults : Recommended dosage range is 5 to 40 mg once daily. ( 2.1 ) Pediatric Patients with HeFH : Recommended dosage range is 5 to 10 mg once daily for patients aged 8 to less than 10 years of age, and 5 to 20 mg once daily for patients aged 10 years and older. ( 2.2 ) Pediatric Patients with HoFH : Recommended dosage is 20 mg once daily for patients aged 7 years and older. ( 2.2 ) Asian Patients : Initiate at 5 mg once daily. Consider risks and benefits of treatment if not adequately controlled at doses up to 20 mg once daily. ( 2.4 ) Patients with Severe Renal Impairment (not on hemodialysis) : Initiate at 5 mg once daily; do not exceed 10 mg once daily. ( 2.5 , 5.1 , 8.6 ) See full prescribing information for CRESTOR dosage and administration modifications due to drug interactions. ( 2.6 ) 2.1 General Dosage and Administration Information • Administer CRESTOR orally as a single dose at any time of day, with or without food. The tablet should be swallowed whole. • Assess LDL-C when clinically appropriate, as early as 4 weeks after initiating CRESTOR, and adjust the dosage if necessary. • If a dose is missed, advise patients not take an extra dose. Resume treatment with the next dose. 2.2 Recommended Dosage in Adult Patients • The dosage range for CRESTOR is 5 to 40 mg orally once daily. • The recommended dose of CRESTOR depends on a patient’s indication for usage, LDL-C, and individual risk for cardiovascular events. 2.3 Recommended Dosage in Pediatric Patients Dosage in Pediatric Patients 8 Years of Age and Older with HeFH The recommended dosage range is 5 mg to 10 mg orally once daily in patients aged 8 years to less than 10 years and 5 mg to 20 mg orally once daily in patients aged 10 years and older. Dosage in Pediatric Patients 7 Years of Age and Older with HoFH The recommended dosage is 20 mg orally once daily. 2.4 Dosing in Asian Patients Initiate CRESTOR at 5 mg once daily due to increased rosuvastatin plasma concentrations. Consider the risks and benefits of CRESTOR when treating Asian patients not adequately controlled at doses up to 20 mg once daily [see Warnings and Precautions (5.1) , Use in Specific Populations (8.8) , and Clinical Pharmacology (12.3) ] . 2.5 Recommended Dosage in Patients with Renal Impairment In patients with severe renal impairment (CL cr less than 30 mL/min/1.73 m 2 ) not on hemodialysis, the recommended starting dosage is 5 mg once daily and should not exceed 10 mg once daily [see Warnings and Precautions (5.1) and Use in Specific Populations (8.6) ] . There are no dosage adjustment recommendations for patients with mild and moderate renal impairment. 2.6 Dosage and Administration Modifications Due to Drug Interactions CRESTOR Dosage Modifications Due to Drug Interactions Table 1 displays dosage modifications for CRESTOR due to drug interactions [see Warnings and Precautions (5.1) and Drug Interactions (7.1) ] . Table 1: CRESTOR Dosage Modifications Due to Drug Interactions Concomitantly Used Drug CRESTOR Dosage Modifications Cyclosporine Do not exceed 5 mg once daily. Teriflunomide Do not exceed 10 mg once daily. Capmatinib Do not exceed 10 mg once daily. Fostamatinib Do not exceed 20 mg once daily. Febuxostat Do not exceed 20 mg once daily. Gemfibrozil Avoid concomitant use. If used concomitantly, initiate at 5 mg once daily and do not exceed 10 mg once daily. Tafamidis Avoid concomitant use. If used concomitantly, initiate at 5 mg once daily and do not exceed 10 mg once daily. Antiviral Medications ∘ Sofbuvir/velpatasvir/voxilaprevir ∘ Ledipasvir/sofosbuvir Concomitant use not recommended. ∘ Simeprevir ∘ Dasabuvir/ombitasvir/paritaprevir/ritonavir ∘ Elbasvir/Grazoprevir ∘ Sofosbuvir/Velpatasvir ∘ Glecaprevir/Pibrentasvir ∘ Atazanavir/Ritonavir ∘ Lopinavir/Ritonavir Initiate at 5 mg once daily. Do not exceed 10 mg once daily. Darolutamide Do not exceed 5 mg once daily. Regorafenib Do not exceed 10 mg once daily. CRESTOR Administration Modifications Due to Drug Interactions When taking CRESTOR with an aluminum and magnesium hydroxide combination antacid, administer CRESTOR at least 2 hours before the antacid [see Drug Interactions (7.2) ] .

Indications And Usage

1 INDICATIONS AND USAGE CRESTOR is indicated: • To reduce the risk of stroke, myocardial infarction, and arterial revascularization procedures in adults without established coronary heart disease who are at increased risk of cardiovascular (CV) disease based on age, hsCRP ≥2 mg/L, and at least one additional CV risk factor. • As an adjunct to diet to: ∘ Reduce LDL-C in adults with primary hyperlipidemia. ∘ Reduce low-density lipoprotein cholesterol (LDL-C) and slow the progression of atherosclerosis in adults. ∘ Reduce LDL-C in adults and pediatric patients aged 8 years and older with heterozygous familial hypercholesterolemia (HeFH). • As an adjunct to other LDL-C-lowering therapies, or alone if such treatments are unavailable, to reduce LDL-C in adults and pediatric patients aged 7 years and older with homozygous familial hypercholesterolemia (HoFH). • As an adjunct to diet for the treatment of adults with: ∘ Primary dysbetalipoproteinemia. ∘ Hypertriglyceridemia. CRESTOR is an HMG Co-A reductase inhibitor (statin) indicated: ( 1 ) • To reduce the risk of stroke, myocardial infarction, and arterial revascularization procedures in adults without established coronary heart disease who are at increased risk of cardiovascular (CV) disease based on age, hsCRP ≥2 mg/L, and at least one additional CV risk factor. • As an adjunct to diet to reduce LDL-C in adults with primary hyperlipidemia. • As an adjunct to diet to reduce low-density lipoprotein cholesterol (LDL-C) and slow the progression of atherosclerosis in adults. • As an adjunct to diet to reduce LDL-C in adults and pediatric patients aged 8 years and older with heterozygous familial hypercholesterolemia (HeFH). • As an adjunct to other LDL-C-lowering therapies, or alone if such treatments are unavailable, to reduce LDL-C in adults and pediatric patients aged 7 years and older with homozygous familial hypercholesterolemia (HoFH). • As an adjunct to diet for the treatment of adults with: ∘ Primary dysbetalipoproteinemia. ∘ Hypertriglyceridemia.

Overdosage

10 OVERDOSAGE No specific antidotes for CRESTOR are known. Hemodialysis does not significantly enhance clearance of rosuvastatin. Contact Poison Control (1‑800‑222‑1222) for latest recommendations.

Adverse Reactions Table

Table 2: Adverse Reactions Reported in ≥2% of Patients Treated with CRESTOR and > Placebo in Placebo-Controlled Trials

Adverse Reactions

Placebo

N=382

%

CRESTOR

5 mg

N=291

%

CRESTOR

10 mg

N=283

%

CRESTOR

20 mg

N=64

%

CRESTOR

40 mg

N=106

%

Total

CRESTOR

5 mg40 mg

N=744

%

Headache

5.0

5.5

4.9

3.1

8.5

5.5

Nausea

3.1

3.8

3.5

6.3

0

3.4

Myalgia

1.3

3.1

2.1

6.3

1.9

2.8

Asthenia

2.6

2.4

3.2

4.7

0.9

2.7

Constipation

2.4

2.1

2.1

4.7

2.8

2.4

Drug Interactions

7 DRUG INTERACTIONS See full prescribing information for details regarding concomitant use of CRESTOR with other drugs that increase the risk of myopathy and rhabdomyolysis. ( 2.6 , 7.1 ) Aluminum and Magnesium Hydroxide Combination Antacids : Administer CRESTOR at least 2 hours after the antacid. ( 2.6 , 7.2 ) Wafarin : Obtain INR prior to starting CRESTOR. Monitor INR frequently until stable upon initiation, dose titration or discontinuation. ( 7.3 ) 7.1 Drug Interactions that Increase the Risk of Myopathy and Rhabdomyolysis with CRESTOR Rosuvastatin is a substrate of CYP2C9 and transporters (such as OATP1B1, BCRP). Rosuvastatin plasma levels can be significantly increased with concomitant administration of inhibitors of CYP2C9 and transporters. Table 5 includes a list of drugs that increase the risk of myopathy and rhabdomyolysis when used concomitantly with CRESTOR and instructions for preventing or managing them [see Warnings and Precautions (5.1) and Clinical Pharmacology (12.3) ] . Table 5: Drug Interactions that Increase the Risk of Myopathy and Rhabdomyolysis with CRESTOR Cyclosporine Clinical Impact: Cyclosporine increased rosuvastatin exposure 7-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use of cyclosporine or gemfibrozil with CRESTOR. Intervention: If used concomitantly, do not exceed a dose of CRESTOR 5 mg once daily. Teriflunomide Clinical Impact: Teriflunomide increased rosuvastatin exposure more than 2.5-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use. Intervention: In patients taking teriflunomide, do not exceed a dose of CRESTOR 10 mg once daily. Capmatinib Clinical Impact: Capmatinib increased rosuvastatin exposure more than 2.1-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use. Intervention: In patients taking capmatinib, do not exceed a dose of CRESTOR 10 mg once daily. Fostamatinib Clinical Impact: Fostamatinib increased rosuvastatin exposure more than 2.0-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use. Intervention: In patients taking fostamatinib, do not exceed a dose of CRESTOR 20 mg once daily. Febuxostat Clinical Impact: Febuxostat increased rosuvastatin exposure more than 1.9-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use. Intervention: In patients taking febuxostat, do not exceed a dose of CRESTOR 20 mg once daily. Gemfibrozil Clinical Impact: Gemfibrozil significantly increased rosuvastatin exposure and gemfibrozil may cause myopathy when given alone. The risk of myopathy and rhabdomyolysis is increased with concomitant use of gemfibrozil with CRESTOR. Intervention: Avoid concomitant use of gemfibrozil with CRESTOR. If used concomitantly, initiate CRESTOR at 5 mg once daily and do not exceed a dose of CRESTOR 10 mg once daily. Tafamidis Clinical Impact: Tafamidis significantly increased rosuvastatin exposure and tafamidis may cause myopathy when given alone. The risk of myopathy and rhabdomyolysis is increased with concomitant use of tafamidis with CRESTOR. Intervention: Avoid concomitant use of tafamidis with CRESTOR. If used concomitantly, initiate CRESTOR at 5 mg once daily and do not exceed a dose of CRESTOR 10 mg once daily. Monitor for signs of myopathy and rhabdomyolysis if used concomitantly with CRESTOR. Anti-Viral Medications Clinical Impact: Rosuvastatin plasma levels were significantly increased with concomitant administration of many anti-viral drugs, which increases the risk of myopathy and rhabdomyolysis. Intervention: • Sofosbuvir/velpatasvir/voxilaprevir • Ledipasvir/sofosbuvir Avoid concomitant use with CRESTOR. • Simeprevir • Dasabuvir/ombitasvir/paritaprevir/ritonavir • Elbasvir/grazoprevir • Sofosbuvir/velpatasvir • Glecaprevir/pibrentasvir • Atazanavir/ritonavir • Lopinavir/ritonavir Initiate with CRESTOR 5 mg once daily, and do not exceed a dose of CRESTOR 10 mg once daily. Darolutamide Clinical Impact: Darolutamide increased rosuvastatin exposure more than 5-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use. Intervention: In patients taking darolutamide, do not exceed a dose of CRESTOR 5 mg once daily. Regorafenib Clinical Impact: Regorafenib increased rosuvastatin exposure and may increase the risk of myopathy. Intervention: In patients taking regorafenib, do not exceed a dose of CRESTOR 10 mg once daily. Fenofibrates (e.g., fenofibrate and fenofibric acid) Clinical Impact: Fibrates may cause myopathy when given alone. The risk of myopathy and rhabdomyolysis is increased with concomitant use of fibrates with CRESTOR. Intervention: Consider if the benefit of using fibrates concomitantly with CRESTOR outweighs the increased risk of myopathy and rhabdomyolysis. If concomitant use is decided, monitor patients for signs and symptoms of myopathy, particularly during initiation of therapy and during upward dose titration of either drug. Niacin Clinical Impact: Cases of myopathy and rhabdomyolysis have occurred with concomitant use of lipid-modifying doses (≥1 g/day) of niacin with CRESTOR. Intervention: Consider if the benefit of using lipid-modifying doses (≥1 g/day) of niacin concomitantly with CRESTOR outweighs the increased risk of myopathy and rhabdomyolysis. If concomitant use is decided, monitor patients for signs and symptoms of myopathy, particularly during initiation of therapy and during upward dose titration of either drug. Colchicine Clinical Impact: Cases of myopathy and rhabdomyolysis have been reported with concomitant use of colchicine with CRESTOR. Intervention: Consider if the benefit of using colchicine concomitantly with CRESTOR outweighs the increased risk of myopathy and rhabdomyolysis. If concomitant use is decided, monitor patients for signs and symptoms of myopathy, particularly during initiation of therapy and during upward dose titration of either drug. 7.2 Drug Interactions that Decrease the Efficacy of CRESTOR Table 6 presents drug interactions that may decrease the efficacy of CRESTOR and instructions for preventing or managing them. Table 6: Drug Interactions that Decrease the Efficacy of CRESTOR Antacids Clinical Impact: Concomitant aluminum and magnesium hydroxide combination antacid administration decreased the mean exposure of rosuvastatin 50% [see Clinical Pharmacology (12.3) ] . Intervention: In patients taking antacid, administer CRESTOR at least 2 hours after the antacid . 7.3 CRESTOR Effects on Other Drugs Table 7 presents CRESTOR’s effect on other drugs and instructions for preventing or managing them. Table 7: CRESTOR Effects on Other Drugs Warfarin Clinical Impact: Rosuvastatin significantly increased the INR in patients receiving warfarin [see Clinical Pharmacology (12.3) ] . Intervention: In patients taking warfarin, obtain an INR before starting CRESTOR and frequently enough after initiation, dose titration or discontinuation to ensure that no significant alteration in INR occurs. Once the INR is stable, monitor INR at regularly recommended intervals.

Drug Interactions Table

Table 5: Drug Interactions that Increase the Risk of Myopathy and Rhabdomyolysis with CRESTOR

Cyclosporine

Clinical Impact:

Cyclosporine increased rosuvastatin exposure 7-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use of cyclosporine or gemfibrozil with CRESTOR.

Intervention:

If used concomitantly, do not exceed a dose of CRESTOR 5 mg once daily.

Teriflunomide

Clinical Impact:

Teriflunomide increased rosuvastatin exposure more than 2.5-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use.

Intervention:

In patients taking teriflunomide, do not exceed a dose of CRESTOR 10 mg once daily.

Capmatinib

Clinical Impact:

Capmatinib increased rosuvastatin exposure more than 2.1-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use.

Intervention:

In patients taking capmatinib, do not exceed a dose of CRESTOR 10 mg once daily.

Fostamatinib

Clinical Impact:

Fostamatinib increased rosuvastatin exposure more than 2.0-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use.

Intervention:

In patients taking fostamatinib, do not exceed a dose of CRESTOR 20 mg once daily.

Febuxostat

Clinical Impact:

Febuxostat increased rosuvastatin exposure more than 1.9-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use.

Intervention:

In patients taking febuxostat, do not exceed a dose of CRESTOR 20 mg once daily.

Gemfibrozil

Clinical Impact:

Gemfibrozil significantly increased rosuvastatin exposure and gemfibrozil may cause myopathy when given alone. The risk of myopathy and rhabdomyolysis is increased with concomitant use of gemfibrozil with CRESTOR.

Intervention:

Avoid concomitant use of gemfibrozil with CRESTOR. If used concomitantly, initiate CRESTOR at 5 mg once daily and do not exceed a dose of CRESTOR 10 mg once daily.

Tafamidis

Clinical Impact:

Tafamidis significantly increased rosuvastatin exposure and tafamidis may cause myopathy when given alone. The risk of myopathy and rhabdomyolysis is increased with concomitant use of tafamidis with CRESTOR.

Intervention:

Avoid concomitant use of tafamidis with CRESTOR. If used concomitantly, initiate CRESTOR at 5 mg once daily and do not exceed a dose of CRESTOR 10 mg once daily. Monitor for signs of myopathy and rhabdomyolysis if used concomitantly with CRESTOR.

Anti-Viral Medications

Clinical Impact:

Rosuvastatin plasma levels were significantly increased with concomitant administration of many anti-viral drugs, which increases the risk of myopathy and rhabdomyolysis.

Intervention:

  • Sofosbuvir/velpatasvir/voxilaprevir
  • Ledipasvir/sofosbuvir
  • Avoid concomitant use with CRESTOR.

  • Simeprevir
  • Dasabuvir/ombitasvir/paritaprevir/ritonavir
  • Elbasvir/grazoprevir
  • Sofosbuvir/velpatasvir
  • Glecaprevir/pibrentasvir
  • Atazanavir/ritonavir
  • Lopinavir/ritonavir
  • Initiate with CRESTOR 5 mg once daily, and do not exceed a dose of CRESTOR 10 mg once daily.

    Darolutamide

    Clinical Impact:

    Darolutamide increased rosuvastatin exposure more than 5-fold. The risk of myopathy and rhabdomyolysis is increased with concomitant use.

    Intervention:

    In patients taking darolutamide, do not exceed a dose of CRESTOR 5 mg once daily.

    Regorafenib

    Clinical Impact:

    Regorafenib increased rosuvastatin exposure and may increase the risk of myopathy.

    Intervention:

    In patients taking regorafenib, do not exceed a dose of CRESTOR 10 mg once daily.

    Fenofibrates (e.g., fenofibrate and fenofibric acid)

    Clinical Impact:

    Fibrates may cause myopathy when given alone. The risk of myopathy and rhabdomyolysis is increased with concomitant use of fibrates with CRESTOR.

    Intervention:

    Consider if the benefit of using fibrates concomitantly with CRESTOR outweighs the increased risk of myopathy and rhabdomyolysis. If concomitant use is decided, monitor patients for signs and symptoms of myopathy, particularly during initiation of therapy and during upward dose titration of either drug.

    Niacin

    Clinical Impact:

    Cases of myopathy and rhabdomyolysis have occurred with concomitant use of lipid-modifying doses (≥1 g/day) of niacin with CRESTOR.

    Intervention:

    Consider if the benefit of using lipid-modifying doses (≥1 g/day) of niacin concomitantly with CRESTOR outweighs the increased risk of myopathy and rhabdomyolysis. If concomitant use is decided, monitor patients for signs and symptoms of myopathy, particularly during initiation of therapy and during upward dose titration of either drug.

    Colchicine

    Clinical Impact:

    Cases of myopathy and rhabdomyolysis have been reported with concomitant use of colchicine with CRESTOR.

    Intervention:

    Consider if the benefit of using colchicine concomitantly with CRESTOR outweighs the increased risk of myopathy and rhabdomyolysis. If concomitant use is decided, monitor patients for signs and symptoms of myopathy, particularly during initiation of therapy and during upward dose titration of either drug.

    Clinical Pharmacology

    12 CLINICAL PHARMACOLOGY 12.1 Mechanism of Action CRESTOR is an inhibitor of HMG-CoA reductase, the rate-limiting enzyme that converts 3‑hydroxy‑3‑methylglutaryl coenzyme A to mevalonate, a precursor of cholesterol. 12.2 Pharmacodynamics Inhibition of HMG-CoA reductase by rosuvastatin accelerates the expression of LDL-receptors, followed by the uptake of LDL-C from blood to the liver, leading to a decrease in plasma LDL-C and total cholesterol. Sustained inhibition of cholesterol synthesis in the liver also decreases levels of very-low-density lipoproteins. The maximum LDL-C reduction of CRESTOR is usually achieved by 4 weeks and is maintained after that. 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 C max and AUC increased in approximate proportion to CRESTOR dose. The absolute bioavailability of rosuvastatin is approximately 20%. The AUC of rosuvastatin does not differ following evening or morning drug administration. Effect of food Administration of CRESTOR with food did not affect the AUC of rosuvastatin. 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. Elimination 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%). After an intravenous dose, approximately 28% of total body clearance was via the renal route, and 72% by the hepatic route. The elimination half-life of rosuvastatin is approximately 19 hours. Specific Populations Geriatric Patients There were no differences in plasma concentrations of rosuvastatin between the nonelderly and elderly populations (age ≥65 years). Pediatric Patients In a population pharmacokinetic analysis of two pediatric trials involving patients with heterozygous familial hypercholesterolemia 10 to 17 years of age and 8 to 17 years of age, respectively, rosuvastatin exposure appeared comparable to or lower than rosuvastatin exposure in adult patients. Male and Female Patients There were no differences in plasma concentrations of rosuvastatin between men and women. Racial or Ethnic Groups 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 C max ) in Asian subjects when compared with a Caucasian control group. Patients with Renal Impairment Mild to moderate renal impairment (CL cr ≥30 mL/min/1.73 m 2 ) 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 (CL cr <30 mL/min/1.73 m 2 ) not receiving hemodialysis compared with healthy subjects (CL cr >80 mL/min/1.73 m 2 ). Steady-state plasma concentrations of rosuvastatin in patients on chronic hemodialysis were approximately 50% greater compared with healthy volunteer subjects with normal renal function. Patients with Hepatic Impairment In patients with chronic alcohol liver disease, plasma concentrations of rosuvastatin were modestly increased. In patients with Child‑Pugh A disease, C max and AUC were increased by 60% and 5%, respectively, as compared with patients with normal liver function. In patients with Child‑Pugh B disease, C max and AUC were increased 100% and 21%, respectively, compared with patients with normal liver function. Drug Interactions Studies 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 CRESTOR with medications that are inhibitors of these transporter proteins (e.g. cyclosporine, certain HIV protease inhibitors) may result in increased rosuvastatin plasma concentrations [see Dosage and Administration (2.6) and Drug Interactions (7.1) ] . Table 8: Effect of Coadministered Drugs on Rosuvastatin Systemic Exposure Coadministered drug and dosing regimen Rosuvastatin Mean Ratio (ratio with/without coadministered drug) No Effect=1.0 Dose (mg) Single dose unless otherwise noted. Change in AUC Change in C max Sofosbuvir/velpatasvir/voxilaprevir (400 mg -100 mg-100 mg) + Voxilaprevir (100 mg) once daily for 15 days 10 mg, single dose 7.39 Clinically significant [see Dosage and Administration (2) and Warnings and Precautions (5) ] (6.68-8.18) Mean ratio with 90% CI (with/without coadministered drug, e.g., 1= no change, 0.7 = 30% decrease, 11=11‑fold increase in exposure) 18.88 (16.23-21.96) Cyclosporine – stable dose required (75 mg - 200 mg BID) 10 mg, QD for 10 days 7.1 11 Darolutamide 600 mg BID, 5 days 5 mg, single dose 5.2 ~5 Regorafenib 160 mg OD, 14 days 5 mg, single dose 3.8 4.6 Atazanavir/ritonavir combination 300 mg/100 mg QD for 8 days 10 mg 3.1 7 Simeprevir 150 mg QD, 7 days 10 mg, single dose 2.8 (2.3-3.4) 3.2 (2.6-3.9) Velpatasvir 100 mg once daily 10 mg, single dose 2.69 (2.46-2.94) 2.61 (2.32-2.92) Ombitasvir 25 mg/paritaprevir 150 mg/ ritonavir 100 mg + dasabuvir 400 mg BID 5 mg, single dose 2.59 (2.09-3.21) 7.13 (5.11-9.96) Teriflunomide Not available 2.51 2.65 Elbasvir 50 mg/grazoprevir 200 mg once daily 10 mg, single dose 2.26 (1.89-2.69) 5.49 (4.29-7.04) Glecaprevir 400 mg/pibrentasvir 120 mg once daily 5 mg, once daily 2.15 (1.88-2.46) 5.62 (4.80-6.59) Lopinavir/ritonavir combination 400 mg/100 mg BID for 17 days 20 mg, QD for 7 days 2.1 (1.7-2.6) 5 (3.4-6.4) Capmatinib 400 mg BID 10 mg, single dose 2.08 (1.56-2.76) 3.04 (2.36-3.92) Fostamatinib 100 mg BID 20 mg, single dose 1.96 (1.77-2.15) 1.88 (1.69-2.09) Febuxostat 120 mg OD for 4 days 10 mg, single dose 1.9 (1.5-2.5) 2.1 (1.8-2.6) Gemfibrozil 600 mg BID for 7 days 80 mg 1.9 (1.6-2.2) 2.2 (1.8-2.7) Tafamidis 61 mg QD, 7 days 10 mg 1.97 (1.68-2.31) 1.86 (1.59-2.16) Eltrombopag 75 mg QD, 5 days 10 mg 1.6 (1.4-1.7) 2 (1.8-2.3) Darunavir 600 mg/ritonavir 100 mg BID, 7 days 10 mg, QD for 7 days 1.5 (1.0-2.1) 2.4 (1.6-3.6) Tipranavir/ritonavir combination 500 mg/200 mg BID for 11 days 10 mg 1.4 (1.2-1.6) 2.2 (1.8-2.7) Dronedarone 400 mg BID 10 mg 1.4 Itraconazole 200 mg QD, 5 days 10 mg or 80 mg 1.4 (1.2-1.6) 1.3 (1.1-1.4) 1.4 (1.2-1.5) 1.2 (0.9-1.4) Ezetimibe 10 mg QD, 14 days 10 mg, QD for 14 days 1.2 (0.9-1.6) 1.2 (0.8-1.6) Fosamprenavir/ritonavir 700 mg/100 mg BID for 7 days 10 mg 1.1 1.5 Fenofibrate 67 mg TID for 7 days 10 mg ↔ 1.2 (1.1-1.3) Rifampicin 450 mg QD, 7 days 20 mg ↔ Aluminum & magnesium hydroxide combination antacid Administered simultaneously Administered 2 hours apart 40 mg 40 mg 0.5 (0.4-0.5) 0.8 (0.7-0.9) 0.5 (0.4-0.6) 0.8 (0.7-1.0) Ketoconazole 200 mg BID for 7 days 80 mg 1.0 (0.8-1.2) 1.0 (0.7-1.3) Fluconazole 200 mg QD for 11 days 80 mg 1.1 (1.0-1.3) 1.1 (0.9-1.4) Erythromycin 500 mg QID for 7 days 80 mg 0.8 (0.7-0.9) 0.7 (0.5-0.9) QD= Once daily, BID= Twice daily, TID= Three times daily, QID= Four times daily Table 9: Effect of Rosuvastatin Coadministration on Systemic Exposure to Other Drugs Rosuvastatin Dosage Regimen Coadministered Drug Mean Ratio (ratio with/without coadministered drug) No Effect=1.0 Name and Dose Change in AUC Change in C max 40 mg QD for 10 days Warfarin Clinically significant pharmacodynamic effects [see Drug Interactions (7.3) ] 25 mg single dose R- Warfarin 1.0 (1.0-1.1) Mean ratio with 90% CI (with/without coadministered drug, e.g., 1= no change, 0.7=30% decrease, 11=11-fold increase in exposure) S-Warfarin 1.1 (1.0-1.1) R-Warfarin 1.0 (0.9-1.0) S-Warfarin 1.0 (0.9-1.1) 40 mg QD for 12 days Digoxin 0.5 mg single dose 1.0 (0.9-1.2) 1.0 (0.9-1.2) 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 1.3 (1.2-1.3) NG 1.3 (1.3-1.4) EE 1.3 (1.2-1.3) NG 1.2 (1.1-1.3) EE = ethinyl estradiol, NG = norgestrel, QD= Once daily 12.5 Pharmacogenomics Disposition of rosuvastatin, involves OATP1B1 and other transporter proteins. Higher plasma concentrations of rosuvastatin have been reported in very small groups of patients (n=3 to 5) who have two reduced function alleles of the gene that encodes OATP1B1 ( SLCO1B1 521T > C). The frequency of this genotype (i.e., SLCO1B1 521 C/C) is generally lower than 5% in most racial/ethnic groups. The impact of this polymorphism on efficacy and/or safety of CRESTOR has not been clearly established.

    Clinical Pharmacology Table

    Table 8: Effect of Coadministered Drugs on Rosuvastatin Systemic Exposure

    Coadministered drug and dosing regimen

    Rosuvastatin

    Mean Ratio (ratio with/without coadministered drug) No Effect=1.0

    Dose (mg)Single dose unless otherwise noted.

    Change in AUC

    Change in Cmax

    Sofosbuvir/velpatasvir/voxilaprevir (400 mg -100 mg-100 mg) + Voxilaprevir (100 mg) once daily for 15 days

    10 mg, single dose

    7.39Clinically significant [see Dosage and Administration (2) and Warnings and Precautions (5)]

    (6.68-8.18)Mean ratio with 90% CI (with/without coadministered drug, e.g., 1= no change, 0.7 = 30% decrease, 11=11‑fold increase in exposure)

    18.88

    (16.23-21.96)

    Cyclosporine – stable dose required (75 mg - 200 mg BID)

    10 mg, QD for 10 days

    7.1

    11

    Darolutamide 600 mg BID, 5 days

    5 mg, single dose

    5.2

    ~5

    Regorafenib 160 mg OD, 14 days

    5 mg, single dose

    3.8

    4.6

    Atazanavir/ritonavir combination 300 mg/100 mg QD for 8 days

    10 mg

    3.1

    7

    Simeprevir 150 mg QD, 7 days

    10 mg, single dose

    2.8

    (2.3-3.4)

    3.2

    (2.6-3.9)

    Velpatasvir 100 mg once daily

    10 mg, single dose

    2.69

    (2.46-2.94)

    2.61

    (2.32-2.92)

    Ombitasvir 25 mg/paritaprevir 150 mg/ ritonavir 100 mg + dasabuvir 400 mg BID

    5 mg, single dose

    2.59

    (2.09-3.21)

    7.13

    (5.11-9.96)

    Teriflunomide

    Not available

    2.51

    2.65

    Elbasvir 50 mg/grazoprevir 200 mg once daily

    10 mg, single dose

    2.26

    (1.89-2.69)

    5.49

    (4.29-7.04)

    Glecaprevir 400 mg/pibrentasvir 120 mg once daily

    5 mg, once daily

    2.15

    (1.88-2.46)

    5.62

    (4.80-6.59)

    Lopinavir/ritonavir combination 400 mg/100 mg BID for 17 days

    20 mg, QD for 7 days

    2.1

    (1.7-2.6)

    5

    (3.4-6.4)

    Capmatinib 400 mg BID

    10 mg, single dose

    2.08

    (1.56-2.76)

    3.04

    (2.36-3.92)

    Fostamatinib 100 mg BID

    20 mg, single dose

    1.96

    (1.77-2.15)

    1.88

    (1.69-2.09)

    Febuxostat 120 mg OD for 4 days

    10 mg, single dose

    1.9

    (1.5-2.5)

    2.1

    (1.8-2.6)

    Gemfibrozil 600 mg BID for 7 days

    80 mg

    1.9

    (1.6-2.2)

    2.2

    (1.8-2.7)

    Tafamidis 61 mg QD, 7 days

    10 mg

    1.97

    (1.68-2.31)

    1.86

    (1.59-2.16)

    Eltrombopag 75 mg QD, 5 days

    10 mg

    1.6

    (1.4-1.7)

    2

    (1.8-2.3)

    Darunavir 600 mg/ritonavir 100 mg BID, 7 days

    10 mg, QD for 7 days

    1.5

    (1.0-2.1)

    2.4

    (1.6-3.6)

    Tipranavir/ritonavir combination 500 mg/200 mg BID for 11 days

    10 mg

    1.4

    (1.2-1.6)

    2.2

    (1.8-2.7)

    Dronedarone 400 mg BID

    10 mg

    1.4

    Itraconazole 200 mg QD, 5 days

    10 mg or 80 mg

    1.4

    (1.2-1.6)

    1.3

    (1.1-1.4)

    1.4

    (1.2-1.5)

    1.2

    (0.9-1.4)

    Ezetimibe 10 mg QD, 14 days

    10 mg, QD for 14 days

  • 1.2
  • (0.9-1.6)
  • 1.2

    (0.8-1.6)

    Fosamprenavir/ritonavir 700 mg/100 mg BID for 7 days

    10 mg

    1.1

    1.5

    Fenofibrate 67 mg TID for 7 days

    10 mg

    1.2

    (1.1-1.3)

    Rifampicin 450 mg QD, 7 days

    20 mg

    Aluminum & magnesium hydroxide combination antacid

    Administered simultaneously Administered 2 hours apart

    40 mg 40 mg

    0.5

    (0.4-0.5) 0.8

    (0.7-0.9)

    0.5

    (0.4-0.6) 0.8

    (0.7-1.0)

    Ketoconazole 200 mg BID for 7 days

    80 mg

    1.0

    (0.8-1.2)

    1.0

    (0.7-1.3)

    Fluconazole 200 mg QD for 11 days

    80 mg

    1.1

    (1.0-1.3)

    1.1

    (0.9-1.4)

    Erythromycin 500 mg QID for 7 days

    80 mg

    0.8

    (0.7-0.9)

    0.7

    (0.5-0.9)

    QD= Once daily, BID= Twice daily, TID= Three times daily, QID= Four times daily

    Mechanism Of Action

    12.1 Mechanism of Action CRESTOR is an inhibitor of HMG-CoA reductase, the rate-limiting enzyme that converts 3‑hydroxy‑3‑methylglutaryl coenzyme A to mevalonate, a precursor of cholesterol.

    Pharmacodynamics

    12.2 Pharmacodynamics Inhibition of HMG-CoA reductase by rosuvastatin accelerates the expression of LDL-receptors, followed by the uptake of LDL-C from blood to the liver, leading to a decrease in plasma LDL-C and total cholesterol. Sustained inhibition of cholesterol synthesis in the liver also decreases levels of very-low-density lipoproteins. The maximum LDL-C reduction of CRESTOR is usually achieved by 4 weeks and is maintained after that.

    Pharmacokinetics

    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 C max and AUC increased in approximate proportion to CRESTOR dose. The absolute bioavailability of rosuvastatin is approximately 20%. The AUC of rosuvastatin does not differ following evening or morning drug administration. Effect of food Administration of CRESTOR with food did not affect the AUC of rosuvastatin. 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. Elimination 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%). After an intravenous dose, approximately 28% of total body clearance was via the renal route, and 72% by the hepatic route. The elimination half-life of rosuvastatin is approximately 19 hours. Specific Populations Geriatric Patients There were no differences in plasma concentrations of rosuvastatin between the nonelderly and elderly populations (age ≥65 years). Pediatric Patients In a population pharmacokinetic analysis of two pediatric trials involving patients with heterozygous familial hypercholesterolemia 10 to 17 years of age and 8 to 17 years of age, respectively, rosuvastatin exposure appeared comparable to or lower than rosuvastatin exposure in adult patients. Male and Female Patients There were no differences in plasma concentrations of rosuvastatin between men and women. Racial or Ethnic Groups 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 C max ) in Asian subjects when compared with a Caucasian control group. Patients with Renal Impairment Mild to moderate renal impairment (CL cr ≥30 mL/min/1.73 m 2 ) 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 (CL cr <30 mL/min/1.73 m 2 ) not receiving hemodialysis compared with healthy subjects (CL cr >80 mL/min/1.73 m 2 ). Steady-state plasma concentrations of rosuvastatin in patients on chronic hemodialysis were approximately 50% greater compared with healthy volunteer subjects with normal renal function. Patients with Hepatic Impairment In patients with chronic alcohol liver disease, plasma concentrations of rosuvastatin were modestly increased. In patients with Child‑Pugh A disease, C max and AUC were increased by 60% and 5%, respectively, as compared with patients with normal liver function. In patients with Child‑Pugh B disease, C max and AUC were increased 100% and 21%, respectively, compared with patients with normal liver function. Drug Interactions Studies 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 CRESTOR with medications that are inhibitors of these transporter proteins (e.g. cyclosporine, certain HIV protease inhibitors) may result in increased rosuvastatin plasma concentrations [see Dosage and Administration (2.6) and Drug Interactions (7.1) ] . Table 8: Effect of Coadministered Drugs on Rosuvastatin Systemic Exposure Coadministered drug and dosing regimen Rosuvastatin Mean Ratio (ratio with/without coadministered drug) No Effect=1.0 Dose (mg) Single dose unless otherwise noted. Change in AUC Change in C max Sofosbuvir/velpatasvir/voxilaprevir (400 mg -100 mg-100 mg) + Voxilaprevir (100 mg) once daily for 15 days 10 mg, single dose 7.39 Clinically significant [see Dosage and Administration (2) and Warnings and Precautions (5) ] (6.68-8.18) Mean ratio with 90% CI (with/without coadministered drug, e.g., 1= no change, 0.7 = 30% decrease, 11=11‑fold increase in exposure) 18.88 (16.23-21.96) Cyclosporine – stable dose required (75 mg - 200 mg BID) 10 mg, QD for 10 days 7.1 11 Darolutamide 600 mg BID, 5 days 5 mg, single dose 5.2 ~5 Regorafenib 160 mg OD, 14 days 5 mg, single dose 3.8 4.6 Atazanavir/ritonavir combination 300 mg/100 mg QD for 8 days 10 mg 3.1 7 Simeprevir 150 mg QD, 7 days 10 mg, single dose 2.8 (2.3-3.4) 3.2 (2.6-3.9) Velpatasvir 100 mg once daily 10 mg, single dose 2.69 (2.46-2.94) 2.61 (2.32-2.92) Ombitasvir 25 mg/paritaprevir 150 mg/ ritonavir 100 mg + dasabuvir 400 mg BID 5 mg, single dose 2.59 (2.09-3.21) 7.13 (5.11-9.96) Teriflunomide Not available 2.51 2.65 Elbasvir 50 mg/grazoprevir 200 mg once daily 10 mg, single dose 2.26 (1.89-2.69) 5.49 (4.29-7.04) Glecaprevir 400 mg/pibrentasvir 120 mg once daily 5 mg, once daily 2.15 (1.88-2.46) 5.62 (4.80-6.59) Lopinavir/ritonavir combination 400 mg/100 mg BID for 17 days 20 mg, QD for 7 days 2.1 (1.7-2.6) 5 (3.4-6.4) Capmatinib 400 mg BID 10 mg, single dose 2.08 (1.56-2.76) 3.04 (2.36-3.92) Fostamatinib 100 mg BID 20 mg, single dose 1.96 (1.77-2.15) 1.88 (1.69-2.09) Febuxostat 120 mg OD for 4 days 10 mg, single dose 1.9 (1.5-2.5) 2.1 (1.8-2.6) Gemfibrozil 600 mg BID for 7 days 80 mg 1.9 (1.6-2.2) 2.2 (1.8-2.7) Tafamidis 61 mg QD, 7 days 10 mg 1.97 (1.68-2.31) 1.86 (1.59-2.16) Eltrombopag 75 mg QD, 5 days 10 mg 1.6 (1.4-1.7) 2 (1.8-2.3) Darunavir 600 mg/ritonavir 100 mg BID, 7 days 10 mg, QD for 7 days 1.5 (1.0-2.1) 2.4 (1.6-3.6) Tipranavir/ritonavir combination 500 mg/200 mg BID for 11 days 10 mg 1.4 (1.2-1.6) 2.2 (1.8-2.7) Dronedarone 400 mg BID 10 mg 1.4 Itraconazole 200 mg QD, 5 days 10 mg or 80 mg 1.4 (1.2-1.6) 1.3 (1.1-1.4) 1.4 (1.2-1.5) 1.2 (0.9-1.4) Ezetimibe 10 mg QD, 14 days 10 mg, QD for 14 days 1.2 (0.9-1.6) 1.2 (0.8-1.6) Fosamprenavir/ritonavir 700 mg/100 mg BID for 7 days 10 mg 1.1 1.5 Fenofibrate 67 mg TID for 7 days 10 mg ↔ 1.2 (1.1-1.3) Rifampicin 450 mg QD, 7 days 20 mg ↔ Aluminum & magnesium hydroxide combination antacid Administered simultaneously Administered 2 hours apart 40 mg 40 mg 0.5 (0.4-0.5) 0.8 (0.7-0.9) 0.5 (0.4-0.6) 0.8 (0.7-1.0) Ketoconazole 200 mg BID for 7 days 80 mg 1.0 (0.8-1.2) 1.0 (0.7-1.3) Fluconazole 200 mg QD for 11 days 80 mg 1.1 (1.0-1.3) 1.1 (0.9-1.4) Erythromycin 500 mg QID for 7 days 80 mg 0.8 (0.7-0.9) 0.7 (0.5-0.9) QD= Once daily, BID= Twice daily, TID= Three times daily, QID= Four times daily Table 9: Effect of Rosuvastatin Coadministration on Systemic Exposure to Other Drugs Rosuvastatin Dosage Regimen Coadministered Drug Mean Ratio (ratio with/without coadministered drug) No Effect=1.0 Name and Dose Change in AUC Change in C max 40 mg QD for 10 days Warfarin Clinically significant pharmacodynamic effects [see Drug Interactions (7.3) ] 25 mg single dose R- Warfarin 1.0 (1.0-1.1) Mean ratio with 90% CI (with/without coadministered drug, e.g., 1= no change, 0.7=30% decrease, 11=11-fold increase in exposure) S-Warfarin 1.1 (1.0-1.1) R-Warfarin 1.0 (0.9-1.0) S-Warfarin 1.0 (0.9-1.1) 40 mg QD for 12 days Digoxin 0.5 mg single dose 1.0 (0.9-1.2) 1.0 (0.9-1.2) 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 1.3 (1.2-1.3) NG 1.3 (1.3-1.4) EE 1.3 (1.2-1.3) NG 1.2 (1.1-1.3) EE = ethinyl estradiol, NG = norgestrel, QD= Once daily

    Pharmacokinetics Table

    Table 8: Effect of Coadministered Drugs on Rosuvastatin Systemic Exposure

    Coadministered drug and dosing regimen

    Rosuvastatin

    Mean Ratio (ratio with/without coadministered drug) No Effect=1.0

    Dose (mg)Single dose unless otherwise noted.

    Change in AUC

    Change in Cmax

    Sofosbuvir/velpatasvir/voxilaprevir (400 mg -100 mg-100 mg) + Voxilaprevir (100 mg) once daily for 15 days

    10 mg, single dose

    7.39Clinically significant [see Dosage and Administration (2) and Warnings and Precautions (5)]

    (6.68-8.18)Mean ratio with 90% CI (with/without coadministered drug, e.g., 1= no change, 0.7 = 30% decrease, 11=11‑fold increase in exposure)

    18.88

    (16.23-21.96)

    Cyclosporine – stable dose required (75 mg - 200 mg BID)

    10 mg, QD for 10 days

    7.1

    11

    Darolutamide 600 mg BID, 5 days

    5 mg, single dose

    5.2

    ~5

    Regorafenib 160 mg OD, 14 days

    5 mg, single dose

    3.8

    4.6

    Atazanavir/ritonavir combination 300 mg/100 mg QD for 8 days

    10 mg

    3.1

    7

    Simeprevir 150 mg QD, 7 days

    10 mg, single dose

    2.8

    (2.3-3.4)

    3.2

    (2.6-3.9)

    Velpatasvir 100 mg once daily

    10 mg, single dose

    2.69

    (2.46-2.94)

    2.61

    (2.32-2.92)

    Ombitasvir 25 mg/paritaprevir 150 mg/ ritonavir 100 mg + dasabuvir 400 mg BID

    5 mg, single dose

    2.59

    (2.09-3.21)

    7.13

    (5.11-9.96)

    Teriflunomide

    Not available

    2.51

    2.65

    Elbasvir 50 mg/grazoprevir 200 mg once daily

    10 mg, single dose

    2.26

    (1.89-2.69)

    5.49

    (4.29-7.04)

    Glecaprevir 400 mg/pibrentasvir 120 mg once daily

    5 mg, once daily

    2.15

    (1.88-2.46)

    5.62

    (4.80-6.59)

    Lopinavir/ritonavir combination 400 mg/100 mg BID for 17 days

    20 mg, QD for 7 days

    2.1

    (1.7-2.6)

    5

    (3.4-6.4)

    Capmatinib 400 mg BID

    10 mg, single dose

    2.08

    (1.56-2.76)

    3.04

    (2.36-3.92)

    Fostamatinib 100 mg BID

    20 mg, single dose

    1.96

    (1.77-2.15)

    1.88

    (1.69-2.09)

    Febuxostat 120 mg OD for 4 days

    10 mg, single dose

    1.9

    (1.5-2.5)

    2.1

    (1.8-2.6)

    Gemfibrozil 600 mg BID for 7 days

    80 mg

    1.9

    (1.6-2.2)

    2.2

    (1.8-2.7)

    Tafamidis 61 mg QD, 7 days

    10 mg

    1.97

    (1.68-2.31)

    1.86

    (1.59-2.16)

    Eltrombopag 75 mg QD, 5 days

    10 mg

    1.6

    (1.4-1.7)

    2

    (1.8-2.3)

    Darunavir 600 mg/ritonavir 100 mg BID, 7 days

    10 mg, QD for 7 days

    1.5

    (1.0-2.1)

    2.4

    (1.6-3.6)

    Tipranavir/ritonavir combination 500 mg/200 mg BID for 11 days

    10 mg

    1.4

    (1.2-1.6)

    2.2

    (1.8-2.7)

    Dronedarone 400 mg BID

    10 mg

    1.4

    Itraconazole 200 mg QD, 5 days

    10 mg or 80 mg

    1.4

    (1.2-1.6)

    1.3

    (1.1-1.4)

    1.4

    (1.2-1.5)

    1.2

    (0.9-1.4)

    Ezetimibe 10 mg QD, 14 days

    10 mg, QD for 14 days

  • 1.2
  • (0.9-1.6)
  • 1.2

    (0.8-1.6)

    Fosamprenavir/ritonavir 700 mg/100 mg BID for 7 days

    10 mg

    1.1

    1.5

    Fenofibrate 67 mg TID for 7 days

    10 mg

    1.2

    (1.1-1.3)

    Rifampicin 450 mg QD, 7 days

    20 mg

    Aluminum & magnesium hydroxide combination antacid

    Administered simultaneously Administered 2 hours apart

    40 mg 40 mg

    0.5

    (0.4-0.5) 0.8

    (0.7-0.9)

    0.5

    (0.4-0.6) 0.8

    (0.7-1.0)

    Ketoconazole 200 mg BID for 7 days

    80 mg

    1.0

    (0.8-1.2)

    1.0

    (0.7-1.3)

    Fluconazole 200 mg QD for 11 days

    80 mg

    1.1

    (1.0-1.3)

    1.1

    (0.9-1.4)

    Erythromycin 500 mg QID for 7 days

    80 mg

    0.8

    (0.7-0.9)

    0.7

    (0.5-0.9)

    QD= Once daily, BID= Twice daily, TID= Three times daily, QID= Four times daily

    Effective Time

    20230113

    Version

    44

    Dosage And Administration Table

    Sofbuvir/velpatasvir/voxilaprevir
  • Ledipasvir/sofosbuvirSimeprevir
  • Dasabuvir/ombitasvir/paritaprevir/ritonavir
  • Elbasvir/Grazoprevir
  • Sofosbuvir/Velpatasvir
  • Glecaprevir/Pibrentasvir
  • Atazanavir/Ritonavir
  • Lopinavir/Ritonavir
    Table 1: CRESTOR Dosage Modifications Due to Drug Interactions

    Concomitantly Used Drug

    CRESTOR Dosage Modifications

    Cyclosporine

    Do not exceed 5 mg once daily.

    Teriflunomide

    Do not exceed 10 mg once daily.

    Capmatinib

    Do not exceed 10 mg once daily.

    Fostamatinib

    Do not exceed 20 mg once daily.

    Febuxostat

    Do not exceed 20 mg once daily.

    Gemfibrozil

    Avoid concomitant use. If used concomitantly, initiate at 5 mg once daily and do not exceed 10 mg once daily.

    Tafamidis

    Avoid concomitant use. If used concomitantly, initiate at 5 mg once daily and do not exceed 10 mg once daily.

    Antiviral Medications

  • Concomitant use not recommended.

  • Initiate at 5 mg once daily. Do not exceed 10 mg once daily.

    Darolutamide

    Do not exceed 5 mg once daily.

    Regorafenib

    Do not exceed 10 mg once daily.

    Dosage Forms And Strengths

    3 DOSAGE FORMS AND STRENGTHS CRESTOR tablets: • 5 mg of rosuvastatin: yellow, round, biconvex, coated tablets. Debossed “CRESTOR” and “5” on one side of the tablet. • 10 mg of rosuvastatin: pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “10” on one side of the tablet. • 20 mg of rosuvastatin: pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “20” on one side of the tablet. • 40 mg of rosuvastatin: 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 of rosuvastatin. ( 3 )

    Spl Product Data Elements

    CRESTOR Rosuvastatin calcium ROSUVASTATIN CALCIUM ROSUVASTATIN LACTOSE MONOHYDRATE MICROCRYSTALLINE CELLULOSE HYPROMELLOSE, UNSPECIFIED TRIACETIN TITANIUM DIOXIDE FERRIC OXIDE YELLOW biconvex 5;crestor CRESTOR Rosuvastatin calcium ROSUVASTATIN CALCIUM ROSUVASTATIN LACTOSE MONOHYDRATE MICROCRYSTALLINE CELLULOSE TRIBASIC CALCIUM PHOSPHATE CROSPOVIDONE, UNSPECIFIED MAGNESIUM STEARATE HYPROMELLOSE, UNSPECIFIED TRIACETIN TITANIUM DIOXIDE FERRIC OXIDE RED biconvex 10;crestor CRESTOR Rosuvastatin calcium ROSUVASTATIN CALCIUM ROSUVASTATIN LACTOSE MONOHYDRATE MICROCRYSTALLINE CELLULOSE TRIBASIC CALCIUM PHOSPHATE CROSPOVIDONE, UNSPECIFIED MAGNESIUM STEARATE HYPROMELLOSE, UNSPECIFIED TRIACETIN TITANIUM DIOXIDE FERRIC OXIDE RED biconvex 20;crestor CRESTOR Rosuvastatin calcium ROSUVASTATIN CALCIUM ROSUVASTATIN LACTOSE MONOHYDRATE MICROCRYSTALLINE CELLULOSE TRIBASIC CALCIUM PHOSPHATE CROSPOVIDONE, UNSPECIFIED MAGNESIUM STEARATE HYPROMELLOSE, UNSPECIFIED TRIACETIN TITANIUM DIOXIDE FERRIC OXIDE RED biconvex 40;crestor

    Carcinogenesis And Mutagenesis And Impairment Of Fertility

    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, or 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 (systemic exposures up to 10 times the human exposure at 40 mg/day based on AUC). 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.

    Nonclinical Toxicology

    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, or 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 (systemic exposures up to 10 times the human exposure at 40 mg/day based on AUC). 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.

    Application Number

    NDA021366

    Brand Name

    CRESTOR

    Generic Name

    Rosuvastatin calcium

    Product Ndc

    0310-0751

    Product Type

    HUMAN PRESCRIPTION DRUG

    Route

    ORAL

    Package Label Principal Display Panel

    Package/Label Display Panel – 5 mg NDC 0310-0755-90 90 tablets CRESTOR® rosuvastatin calcium 5 mg tablets Rx only Mfd. for: AstraZeneca Pharmaceuticals LP Wilmington, DE 19850 By: IPR Pharmaceuticals, Inc. Canóvanas, PR 00729 Product of UK AstraZeneca Crestor 5 mg tablet 90 count bottle label

    Recent Major Changes

    Contraindications, Pregnancy and Lactation ( 4 ) Removed 01/2023 Warnings and Precautions ( 5.2 ) 01/2023 Warnings and Precautions, Concomitant Coumarin Anticoagulants ( 5.4 ) Removed 01/2023

    Information For Patients

    17 PATIENT COUNSELING INFORMATION Advise the patient to read the FDA-approved patient labeling (Patient Information). Myopathy and Rhabdomyolysis Advise patients that CRESTOR may cause myopathy and rhabdomyolysis. Inform patients that the risk is also increased when taking certain types of medication and they should discuss all medication, both prescription and over the counter, with their healthcare provider. Instruct patients to promptly report any unexplained muscle pain, tenderness or weakness particularly if accompanied by malaise or fever [see Warnings and Precautions (5.1) , and Drug Interactions (7.1) ] . Hepatic Dysfunction Inform patients that CRESTOR may cause liver enzyme elevations and possibly liver failure. Advise patients to promptly report fatigue, anorexia, right upper abdominal discomfort, dark urine or jaundice [see Warnings and Precautions (5.3) ] . Increases in HbA1c and Fasting Serum Glucose Levels Inform patients that increases in HbA1c and fasting serum glucose levels may occur with CRESTOR. Encourage patients to optimize lifestyle measures, including regular exercise, maintaining a healthy body weight, and making healthy food choices [see Warnings and Precautions (5.5) ] . Pregnancy Advise pregnant patients and patients who can become pregnant of the potential risk to a fetus. Advise patients to inform their healthcare provider of a known or suspected pregnancy to discuss if CRESTOR should be discontinued [see Use in Specific Populations (8.1) ] . Lactation Advise patients that breastfeeding during treatment with CRESTOR is not recommended [see Use in Specific Populations (8.2) ] . Concomitant Use of Antacids When taking CRESTOR with an aluminum and magnesium hydroxide combination antacid, the antacid should be taken at least 2 hours after CRESTOR administration. Missed Doses If a dose is missed, advise patients not take an extra dose. Just resume the usual schedule. CRESTOR is a trademark of the AstraZeneca group of companies. © AstraZeneca 2023 Licensed from SHIONOGI & CO., LTD., Osaka, Japan Distributed by: AstraZeneca Pharmaceuticals LP Wilmington, DE 19850

    Spl Patient Package Insert Table

    lower the level of low-density lipoprotein (LDL) cholesterol or “bad” cholesterol in adults with primary hyperlipidemia.
  • slow the buildup of fatty deposits (plaque) in the walls of blood vessels.
  • treat adults and children 8 years of age and older with high blood cholesterol due to heterozygous familial hypercholesterolemia (an inherited condition that causes high levels of LDL).
  • along with other cholesterol lowering treatments or alone if such treatments are unavailable in adults and children 7 years of age and older with homozygous familial hypercholesterolemia (an inherited condition that causes high levels of LDL).
  • treat adults with a type of high cholesterol called primary dysbetalipoproteinemia (type III hyperlipoproteinemia).
  • lower the level of fat in your blood (triglycerides) in adults with hypertriglyceridemia.
  • The safety and effectiveness of CRESTOR has not been established in children younger than 8 years of age with heterozygous familial hypercholesterolemia or children younger than 7 years of age with homozygous familial hypercholesterolemia or in children with other types of hyperlipidemias (other than HeFH or HoFH).
  • lopinavir, ritonavir, fosamprenavir, tipranavir, atazanavir, simeprevir
  • combination of
  • sofosbuvir/velpatasvir/voxilaprevir
  • dasabuvir/ombitasvir/paritaprevir/ritonavir
  • elbasvir/grazoprevir
  • sofosbuvir/velpatasvir
  • glecaprevir/pibrentasvir and
  • all other combinations with ledipasvir including ledipasvir/sofosbuvir
  • certain anti-fungal medicines (such as itraconazole, ketoconazole and fluconazole)
  • coumarin anticoagulants (medicines that prevent blood clots, such as warfarin)
  • niacin or nicotinic acid
  • fibric acid derivatives (such as fenofibrate)
  • colchicine (a medicine used to treat gout)
  • Ask your doctor or pharmacist for a list of these medicines if you are not sure. Know the medicines you take.

    Keep a list of them to show your doctor and pharmacist when you get new medicine.

    you have unexplained muscle pain, tenderness, or weakness, especially if you have a fever or feel more tired than usual, while you take CRESTOR.
  • you have muscle problems that do not go away even after your doctor has told you to stop taking CRESTOR. Your doctor may do further tests to diagnose the cause of your muscle problems.
  • Your chances of getting muscle problems are higher if you:
  • are taking certain other medicines while you take CRESTOR
  • are 65 years of age or older
  • have thyroid problems (hypothyroidism) that are not controlled
  • have kidney problems
  • are taking higher doses of CRESTOR
  • Liver problems. Your doctor should do blood tests to check your liver before you start taking CRESTOR and if you have symptoms of liver problems while you take CRESTOR. 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
  • Protein and blood in the urine. CRESTOR may cause you to have protein and blood in your urine. If you develop protein or blood in your urine, your doctor may decrease your dose of CRESTOR.
  • Increase in blood sugar (glucose) levels. CRESTOR may cause an increase in your blood sugar levels.
  • The most common side effects may include: headache, muscle aches and pains, abdominal pain, weakness, and nausea.

    Tell your doctor if you have any side effect that bothers you or that does not go away.

    For more information, ask your doctor or pharmacist.

    Call your doctor for medical advice about side effects. You may report side effects to FDA at 1-800-FDA-1088.

    PATIENT INFORMATION

    CRESTOR® (Kres-tor)

    rosuvastatin

    Tablets

    Read this Patient Information carefully before you start taking CRESTOR and each time you get a refill. If you have any questions about CRESTOR, ask your doctor. Only your doctor can determine if CRESTOR is right for you.

    What is CRESTOR?

    CRESTOR is a prescription medicine that contains a cholesterol-lowering medicine called rosuvastatin.

  • CRESTOR is used to:
  • reduce the risk of stroke, heart attack, and the need for procedures to improve blood flow to the heart called arterial revascularization in adults who do not have known heart disease but do have certain additional risk factors.
  • CRESTOR is used along with diet to:
  • Who should not take CRESTOR?

    Do not take CRESTOR if you:

  • have liver problems.
  • are allergic to rosuvastatin or any of the ingredients in CRESTOR. See the end of this leaflet for a complete list of ingredients in CRESTOR. Symptoms of allergic reactions include rash, itching, hives, and swelling.
  • What should I tell my doctor before and while taking CRESTOR?

    Tell your doctor if you:

  • have unexplained muscle aches or weakness.
  • have or have had kidney problems.
  • have or have had liver problems.
  • drink more than 2 glasses of alcohol daily.
  • have thyroid problems.
  • are 65 years of age or older.
  • are of Asian descent.
  • are pregnant or think you may be pregnant, or are planning to become pregnant. If you become pregnant while taking CRESTOR, call your healthcare provider right away to discuss your CRESTOR treatment.
  • are breastfeeding. CRESTOR can pass into your breast milk. Breastfeeding is not recommended while taking CRESTOR.
  • Tell your doctor about all the medicines you take, including prescription and over-the-counter medicines, vitamins, and herbal supplements.

    Taking CRESTOR with certain other medicines may affect each other causing side effects. CRESTOR may affect the way other medicines work, and other medicines may affect how CRESTOR works.

    Especially tell your doctor if you take:

  • cyclosporine (a medicine for your immune system)
  • gemfibrozil (a fibric acid medicine for lowering cholesterol)
  • fostamatinib (a medicine used to treat low platelet counts)
  • febuxostat (a medicine used to treat and prevent high blood levels of uric acid)
  • teriflunomide (a medicine used to treat relapsing remitting multiple sclerosis)
  • capmatinib (a medicine for the treatment of non-small cell lung cancer)
  • tafamidis (used to treat cardiomyopathy [enlarged and thickened heart muscle])
  • darolutamide (a medicine for the treatment of prostate cancer)
  • regorafenib (a medicine used to treat cancer of the colon and rectum)
  • anti-viral medicines including certain HIV or hepatitis C virus drugs such as:
  • How should I take CRESTOR?

  • Take CRESTOR exactly as your doctor tells you to take it.
  • Take CRESTOR, by mouth, 1 time each day. Swallow the tablet whole.
  • CRESTOR can be taken at any time of day, with or without food.
  • Do not change your dose or stop CRESTOR without talking to your doctor, even if you are feeling well.
  • Your doctor may do blood tests to check your cholesterol levels before and during your treatment with CRESTOR. Your doctor may change your dose of CRESTOR if needed.
  • Your doctor may start you on a cholesterol lowering diet before giving you CRESTOR. Stay on this diet when you take CRESTOR.
  • Wait at least 2 hours after taking CRESTOR to take an antacid that contains a combination of aluminum and magnesium hydroxide.
  • If you miss a dose of CRESTOR, take your next dose at your normal scheduled time. Do not take an extra dose of CRESTOR.
  • If you take too much CRESTOR or overdose, call your doctor or go to the nearest hospital emergency room right away.
  • What are the possible side effects of CRESTOR?

    CRESTOR may cause serious side effects, including:

  • Muscle pain, tenderness and weakness (myopathy). Muscle problems, including muscle breakdown, can be serious in some people and rarely cause kidney damage that can lead to death. Tell your doctor right away if:
  • How should I store CRESTOR?

  • Store CRESTOR at room temperature, between 68°F to 77°F (20°C to 25°C) and in a dry place.
  • Safely throw away medicine that is out of date or no longer needed.
  • Keep CRESTOR and all medicines out of the reach of children.

    General Information about the safe and effective use of CRESTOR

    Medicines are sometimes prescribed for purposes other than those listed in a Patient Information leaflet. Do not use CRESTOR for a condition for which it was not prescribed. Do not give CRESTOR to other people, even if they have the same medical condition you have. It may harm them.

    You can ask your pharmacist or doctor for information about CRESTOR that is written for health professionals.

    What are the Ingredients in CRESTOR?

    Active Ingredient: rosuvastatin as rosuvastatin calcium

    Inactive Ingredients: crospovidone NF, hypromellose NF, lactose monohydrate NF, magnesium stearate NF, microcrystalline cellulose NF, red ferric oxide NF, titanium dioxide USP, triacetin NF, tribasic calcium phosphate NF and yellow ferric oxide.

    CRESTOR is a trademark of the AstraZeneca group of companies.

    © AstraZeneca 2023

    Licensed from SHIONOGI & CO., LTD., Osaka, Japan

    Distributed by:

    AstraZeneca Pharmaceuticals LP

    Wilmington, DE 19850

    For more information, go to the CRESTOR website at www.crestor.com or call 1-800-CRESTOR

    Clinical Studies

    14 CLINICAL STUDIES 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 CRESTOR 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 and hsCRP 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%). Patients had a median baseline LDL‑C of 108 mg/dL and hsCRP of 4.3 mg/L. Patients were randomly assigned to placebo (n=8901) or CRESTOR 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 CRESTOR-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. CRESTOR 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% (see Figure 1). 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 1. Time to First Occurrence of Major Cardiovascular Events in JUPITER The individual components of the primary end point are presented in Figure 3. CRESTOR significantly reduced the risk of nonfatal myocardial infarction, nonfatal stroke, and arterial revascularization procedures. There were no significant treatment differences between the CRESTOR and placebo groups for death due to cardiovascular causes or hospitalizations for unstable angina. CRESTOR 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 CRESTOR-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 CRESTOR-treated subjects). In a post-hoc subgroup analysis of JUPITER subjects (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 CRESTOR treatment. Figure 2. Major CV Events by Treatment Group in JUPITER At one year, CRESTOR increased HDL‑C and reduced LDL‑C, hsCRP, total cholesterol and serum triglyceride levels (p<0.001 for all versus placebo). Primary Hyperlipidemia in Adults CRESTOR reduces Total‑C, LDL‑C, ApoB, non-HDL‑C, and TG, and increases HDL‑C, in adult patients with hyperlipidemia and mixed dyslipidemia. In a multicenter, double-blind, placebo-controlled study in patients with hyperlipidemia, CRESTOR given as a single daily dose (5 to 40 mg) for 6 weeks significantly reduced Total‑C, LDL‑C, non-HDL‑C, and ApoB, across the dose range (Table 10). Table 10: Lipid-modifying Effect of CRESTOR in Adult 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 CRESTOR 5 mg 17 -33 -45 -44 -38 -35 13 CRESTOR 10 mg 17 -36 -52 -48 -42 -10 14 CRESTOR 20 mg 17 -40 -55 -51 -46 -23 8 CRESTOR 40 mg 18 -46 -63 -60 -54 -28 10 CRESTOR was compared with the statins (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 CRESTOR, atorvastatin, simvastatin, or pravastatin (Figure 3 and Table 11). Figure 3. Percent LDL‑C Change by Dose of CRESTOR, Atorvastatin, Simvastatin, and Pravastatin at Week 6 in Adult 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 11: Percent Change in LDL-C by Dose of CRESTOR, Atorvastatin, Simvastatin, and Pravastatin From Baseline to Week 6 (LS Mean Corresponding standard errors are approximately 1.00. ) in Adult Patients with Hyperlipidemia or Mixed Dyslipidemia (Sample Sizes Ranging from 156–167 Patients Per Group) Treatment Daily Dose Treatment 10 mg 20 mg 40 mg 80 mg CRESTOR -46 CRESTOR 10 mg reduced LDL-C significantly more than atorvastatin 10 mg; pravastatin 10 mg, 20 mg, and 40 mg; simvastatin 10 mg, 20 mg, and 40 mg. (p<0.002) -52 CRESTOR 20 mg reduced LDL-C significantly more than atorvastatin 20 mg and 40 mg; pravastatin 20 mg and 40 mg; simvastatin 20 mg, 40 mg, and 80 mg. (p<0.002) -55 CRESTOR 40 mg reduced LDL-C significantly more than atorvastatin 40 mg; pravastatin 40 mg; simvastatin 40 mg, and 80 mg. (p<0.002) --- Atorvastatin -37 -43 -48 -51 Simvastatin -28 -35 -39 -46 Pravastatin -20 -24 -30 --- Slowing of the Progression of Atherosclerosis In the Measuring Effects on Intima Media Thickness: an Evaluation Of Rosuvastatin 40 mg (METEOR) study, the effect of therapy with CRESTOR 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 adult patients were randomized (of whom 876 were analyzed) in a 5:2 ratio to CRESTOR 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 CRESTOR 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 CRESTOR was -0.0014 mm/year (p=0.32). At an individual patient level in the group treated with CRESTOR, 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. HeFH in Adults In a study of adult patients with HeFH (baseline mean LDL of 291 mg/dL), patients were randomized to CRESTOR 20 mg or atorvastatin 20 mg. The dose was increased at 6-week intervals. Significant LDL-C reductions from baseline were seen at each dose in both treatment groups (Table 12). Table 12: LDL-C Percent Change from Baseline CRESTOR (n=435) LS Mean LS Means are least square means adjusted for baseline LDL-C (95% CI) Atorvastatin (n=187) LS Mean (95% CI) 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%) HeFH in Pediatric Patients 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 mg, 10 mg 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 13 below. Table 13: Lipid-Modifying Effects of CRESTOR in Pediatric Patients 10 to 17 years of Age with Heterozygous Familial Hypercholesterolemia (Least-Squares Mean Percent Change from Baseline To Week 12) Dose (mg) N LDL-C HDL-C Total-C TG Median percent change ApoB Placebo 46 -1% +7% 0% -7% -2% 5 42 -38% +4% Difference from placebo not statistically significant -30% -13% -32% 10 44 -45% +11% -34% -15% -38% 20 44 -50% +9% -39% 16% -41% Rosuvastatin was also studied in a two-year open‑label, uncontrolled, titration-to-goal trial that included 175 children and adolescents with heterozygous familial hypercholesterolemia who were 8 to 17 years old (79 boys and 96 girls). All patients had a documented genetic defect in the LDL receptor or in ApoB. Approximately 89% were White, 7% were Asian, 1% were Black, and fewer than 1% were Hispanic. Mean LDL-C at baseline was 236 mg/dL. Fifty-eight (33%) patients were prepubertal at baseline. The starting rosuvastatin dosage for all children and adolescents was 5 mg once daily. Children 8 to less than 10 years of age (n=41 at baseline) could titrate to a maximum dosage of 10 mg once daily, and children and adolescents 10 to 17 years of age could titrate to a maximum dosage of 20 mg once daily. The reductions in LDL‑C from baseline were generally consistent across age groups within the trial as well as with previous experience in both adult and pediatric controlled trials. HoFH in Adult and Pediatric Patients In an open-label, forced-titration study, HoFH patients (n=40, 8‑63 years) were evaluated for their response to CRESTOR 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-C 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. HoFH in Pediatric Patients CRESTOR was studied in a randomized, double-blind, placebo-controlled, multicenter, cross-over study in 14 pediatric patients with HoFH. The study included a 4‑week dietary lead‑in phase during which patients received CRESTOR 10 mg daily, a cross‑over phase that included two 6‑week treatment periods with either CRESTOR 20 mg or placebo in random order, followed by a 12‑week open‑label phase during which all patients received CRESTOR 20 mg. Patients ranged in age from 7 to 15 years of age (median 11 years), 50% were male, 71% were White, 21% were Asian, 7% were Black, and no patients were of Hispanic ethnicity. Fifty percent were on apheresis therapy and 57% were taking ezetimibe. Patients who entered the study on apheresis therapy or ezetimibe continued the treatment throughout the entire study. Mean LDL‑C at baseline was 416 mg/dL (range 152 to 716 mg/dL). A total of 13 patients completed both treatment periods of the randomized cross-over phase; one patient withdrew consent due to inability to have blood drawn during the cross-over phase. CRESTOR 20 mg significantly reduced LDL-C, total cholesterol, ApoB, and non-HDL-C compared to placebo (Table 14). Table 14: Lipid-modifying Effects of CRESTOR in Pediatric Patients 7 to 15 years of Age with Homozygous Familial Hypercholesterolemia After 6 Weeks Placebo (N=13) CRESTOR 20 mg (N=13) Percent difference (95% CI) LDL-C (mg/dL) 481 396 -22.3% (-33.5, -9.1) p=0.005 Total-C (mg/dL) 539 448 -20.1% (-29.7, -9.1) p=0.003 Non-HDL-C (mg/dL) 505 412 -22.9% (-33.7, ‑10.3) ApoB (mg/dL) 268 235 -17.1% (-29.2, -2.9) p=0.024 % Difference estimates are based on transformations of the estimated mean difference in log LDL measurements between CRESTOR and placebo using a mixed model adjusted for study period. Primary Dysbetalipoproteinemia in Adults In a randomized, multicenter, double-blind crossover study, 32 adult patients (27 with є2/є2 and 4 with apo E mutation [Arg145Cys] with primary dysbetalipoproteinemia 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 for 6 weeks each: rosuvastatin 10 mg followed by rosuvastatin 20 mg or rosuvastatin 20 mg followed by rosuvastatin 10 mg. CRESTOR reduced non-HDL‑C (primary end point) and circulating remnant lipoprotein levels. Results are shown in the table below. Table 15: Lipid-modifying Effects of CRESTOR 10 mg and 20 mg in Adult Patients with Primary Dysbetalipoproteinemia (Type III hyperlipoproteinemia) After Six Weeks by Median Percent Change (95% CI) from Baseline (N=32) Median at Baseline (mg/dL) Median percent change from baseline (95% CI) CRESTOR 10 mg Median percent change from baseline (95% CI) CRESTOR 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) Non‑HDL-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) Hypertriglyceridemia in Adults In a double-blind, placebo-controlled study in adult patients with baseline TG levels from 273 to 817 mg/dL, CRESTOR given as a single daily dose (5 to 40 mg) over 6 weeks significantly reduced serum TG levels (Table 16). Table 16: Lipid-Modifying Effect of CRESTOR in Adult Patients with Primary Hypertriglyceridemia After Six Weeks by Median (Min, Max) Percent Change from Baseline to Week 6 Dose Placebo (n=26) CRESTOR 5 mg (n=25) CRESTOR 10 mg (n=23) CRESTOR 20 mg (n=27) CRESTOR 40 mg (n=25) Triglycerides 1 (-40, 72) -21 (-58, 38) -37 (-65, 5) -37 (-72, 11) -43 (-80, -7) Non-HDL-C 2 (-13, 19) -29 (-43, -8) -49 (-59, -20) -43 (-74, 12) -51 (-62, -6) 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) figure1 Figure__2 figure_3

    Clinical Studies Table

    Table 10: Lipid-modifying Effect of CRESTOR in Adult Patients with Hyperlipidemia (Adjusted Mean % Change from Baseline at Week 6)

    Dose

    N

    TotalC

    LDLC

    Non-HDLC

    ApoB

    TG

    HDLC

  • Placebo
  • 13

    -5

    -7

    -7

    -3

    -3

    3

    CRESTOR 5 mg

    17

    -33

    -45

    -44

    -38

    -35

    13

    CRESTOR 10 mg

    17

    -36

    -52

    -48

    -42

    -10

    14

    CRESTOR 20 mg

    17

    -40

    -55

    -51

    -46

    -23

    8

    CRESTOR 40 mg

    18

    -46

    -63

    -60

    -54

    -28

    10

    Geriatric Use

    8.5 Geriatric Use Of the total number of CRESTOR-treated patients in clinical studies, 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. Advanced age (≥65 years) is a risk factor for CRESTOR-associated myopathy and rhabdomyolysis. Dose selection for an elderly patient should be cautious, recognizing the greater frequency of decreased hepatic, renal, or cardiac function, and of concomitant disease or other drug therapy and the higher risk of myopathy. Monitor geriatric patients receiving CRESTOR for the increased risk of myopathy [see Warnings and Precautions (5.1) ] .

    Pediatric Use

    8.4 Pediatric Use The safety and effectiveness of CRESTOR as an adjunct to diet to reduce LDL-C have been established in pediatric patients 8 years of age and older with HeFH. Use of CRESTOR for this indication is based on one 12-week controlled trial with a 40-week open-label extension period in 176 pediatric patients 10 years of age and older with HeFH and one 2-year open-label, uncontrolled trial in 175 pediatric patients 8 years of age and older with HeFH [see Clinical Studies (14) ] . In the 1-year trial with a 12-week controlled phase, there was no detectable effect of CRESTOR on growth, weight, BMI (body mass index), or sexual maturation in patients aged 10 to 17 years. The safety and effectiveness of CRESTOR as an adjunct to other LDL-C-lowering therapies to reduce LDL-C have been established pediatric patients 7 years of age and older with HoFH. Use of CRESTOR for this indication is based on a randomized, placebo-controlled, cross-over study in 14 pediatric patients 7 years of age and older with HoFH [see Clinical Studies (14) ] . The safety and effectiveness of CRESTOR have not been established in pediatric patients younger than 8 years of age with HeFH, younger than 7 years of age with HoFH, or in pediatric patients with other types of hyperlipidemia (other than HeFH or HoFH).

    Pregnancy

    8.1 Pregnancy Risk Summary Discontinue CRESTOR when pregnancy is recognized. Alternatively, consider the ongoing therapeutic needs of the individual patient. CRESTOR decreases synthesis of cholesterol and possibly other biologically active substances derived from cholesterol; therefore, CRESTOR may cause fetal harm when administered to pregnant patients based on the mechanism of action [see Clinical Pharmacology (12.1) ] . In addition, treatment of hyperlipidemia is not generally necessary during pregnancy. Atherosclerosis is a chronic process and the discontinuation of lipid-lowering drugs during pregnancy should have little impact on the outcome of long-term therapy of primary hyperlipidemia for most patients. Available data from case series and prospective and retrospective observational cohort studies over decades of use with statins in pregnant women have not identified a drug-associated risk of major congenital malformations. Published data from prospective and retrospective observational cohort studies with CRESTOR use in pregnant women are insufficient to determine if there is a drug-associated risk of miscarriage (see Data) . In animal reproduction studies, no adverse developmental effects were observed in pregnant rats or rabbits orally administered rosuvastatin during the period of organogenesis at doses that resulted in systemic exposures equivalent to human exposures at the maximum recommended human dose (MRHD) of 40 mg/day, based on AUC and body surface area (mg/m 2 ), respectively (see Data). The estimated background risk of major birth defects and miscarriage for the indicated population is unknown. In the U.S. general population, the estimated background risk of major birth defects and miscarriage in clinically recognized pregnancies is 2 to 4% and 15 to 20%, respectively. Data Human Data A Medicaid cohort linkage study of 1152 statin-exposed pregnant women compared to 886,996 controls did not find a significant teratogenic effect from maternal use of statins in the first trimester of pregnancy, after adjusting for potential confounders – including maternal age, diabetes mellitus, hypertension, obesity, and alcohol and tobacco use – using propensity score‑based methods. The relative risk of congenital malformations between the group with statin use and the group with no statin use in the first trimester was 1.07 (95% confidence interval 0.85 to 1.37) after controlling for confounders, particularly pre-existing diabetes mellitus. There were also no statistically significant increases in any of the organ-specific malformations assessed after accounting for confounders. In the majority of pregnancies, statin treatment was initiated prior to pregnancy and was discontinued at some point in the first trimester when pregnancy was identified. Study limitations include reliance on physician coding to define the presence of a malformation, lack of control for certain confounders such as body mass index, use of prescription dispensing as verification for the use of a statin, and lack of information on non-live births. Animal Data In female rats given 5, 15 and 50 mg/kg/day before mating and continuing through to gestation day 7 resulted in decreased fetal body weight (female pups) and delayed ossification at 50 mg/kg/day (10 times the human exposure at the MRHD dose of 40 mg/day based on AUC). In pregnant rats given 2, 10 and 50 mg/kg/day of rosuvastatin from gestation day 7 through lactation day 21 (weaning), decreased pup survival occurred at 50 mg/kg/day (dose equivalent to 12 times the MRHD of 40 mg/day based body surface area). In pregnant rabbits given 0.3, 1, and 3 mg/kg/day of rosuvastatin from gestation day 6 to day 18, decreased fetal viability and maternal mortality was observed at 3 mg/kg/day (dose equivalent to the MRHD of 40 mg/day based on body surface area). Rosuvastatin crosses the placenta in rats and rabbits 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. In rabbits, fetal tissue distribution was 25% of maternal plasma concentration after a single oral gavage dose of 1 mg/kg on gestation day 18.

    Use In Specific Populations

    8 USE IN SPECIFIC POPULATIONS • Pregnancy : May cause fetal harm. ( 8.1 ) • Lactation : Breastfeeding not recommended during treatment with CRESTOR. ( 8.2 ) 8.1 Pregnancy Risk Summary Discontinue CRESTOR when pregnancy is recognized. Alternatively, consider the ongoing therapeutic needs of the individual patient. CRESTOR decreases synthesis of cholesterol and possibly other biologically active substances derived from cholesterol; therefore, CRESTOR may cause fetal harm when administered to pregnant patients based on the mechanism of action [see Clinical Pharmacology (12.1) ] . In addition, treatment of hyperlipidemia is not generally necessary during pregnancy. Atherosclerosis is a chronic process and the discontinuation of lipid-lowering drugs during pregnancy should have little impact on the outcome of long-term therapy of primary hyperlipidemia for most patients. Available data from case series and prospective and retrospective observational cohort studies over decades of use with statins in pregnant women have not identified a drug-associated risk of major congenital malformations. Published data from prospective and retrospective observational cohort studies with CRESTOR use in pregnant women are insufficient to determine if there is a drug-associated risk of miscarriage (see Data) . In animal reproduction studies, no adverse developmental effects were observed in pregnant rats or rabbits orally administered rosuvastatin during the period of organogenesis at doses that resulted in systemic exposures equivalent to human exposures at the maximum recommended human dose (MRHD) of 40 mg/day, based on AUC and body surface area (mg/m 2 ), respectively (see Data). The estimated background risk of major birth defects and miscarriage for the indicated population is unknown. In the U.S. general population, the estimated background risk of major birth defects and miscarriage in clinically recognized pregnancies is 2 to 4% and 15 to 20%, respectively. Data Human Data A Medicaid cohort linkage study of 1152 statin-exposed pregnant women compared to 886,996 controls did not find a significant teratogenic effect from maternal use of statins in the first trimester of pregnancy, after adjusting for potential confounders – including maternal age, diabetes mellitus, hypertension, obesity, and alcohol and tobacco use – using propensity score‑based methods. The relative risk of congenital malformations between the group with statin use and the group with no statin use in the first trimester was 1.07 (95% confidence interval 0.85 to 1.37) after controlling for confounders, particularly pre-existing diabetes mellitus. There were also no statistically significant increases in any of the organ-specific malformations assessed after accounting for confounders. In the majority of pregnancies, statin treatment was initiated prior to pregnancy and was discontinued at some point in the first trimester when pregnancy was identified. Study limitations include reliance on physician coding to define the presence of a malformation, lack of control for certain confounders such as body mass index, use of prescription dispensing as verification for the use of a statin, and lack of information on non-live births. Animal Data In female rats given 5, 15 and 50 mg/kg/day before mating and continuing through to gestation day 7 resulted in decreased fetal body weight (female pups) and delayed ossification at 50 mg/kg/day (10 times the human exposure at the MRHD dose of 40 mg/day based on AUC). In pregnant rats given 2, 10 and 50 mg/kg/day of rosuvastatin from gestation day 7 through lactation day 21 (weaning), decreased pup survival occurred at 50 mg/kg/day (dose equivalent to 12 times the MRHD of 40 mg/day based body surface area). In pregnant rabbits given 0.3, 1, and 3 mg/kg/day of rosuvastatin from gestation day 6 to day 18, decreased fetal viability and maternal mortality was observed at 3 mg/kg/day (dose equivalent to the MRHD of 40 mg/day based on body surface area). Rosuvastatin crosses the placenta in rats and rabbits 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. In rabbits, fetal tissue distribution was 25% of maternal plasma concentration after a single oral gavage dose of 1 mg/kg on gestation day 18. 8.2 Lactation Risk Summary Limited data from case reports in published literature indicate that CRESTOR is present in human milk. There is no available information on the effects of the drug on the breastfed infant or the effects of the drug on milk production. Statins, including CRESTOR, decrease cholesterol synthesis and possibly the synthesis of other biologically active substances derived from cholesterol and may cause harm to the breastfed infant. Because of the potential for serious adverse reactions in a breastfed infant, based on the mechanism of action, advise patients that breastfeeding is not recommended during treatment with CRESTOR [see Use in Specific Populations (8.1) and Clinical Pharmacology (12.1) ] . 8.4 Pediatric Use The safety and effectiveness of CRESTOR as an adjunct to diet to reduce LDL-C have been established in pediatric patients 8 years of age and older with HeFH. Use of CRESTOR for this indication is based on one 12-week controlled trial with a 40-week open-label extension period in 176 pediatric patients 10 years of age and older with HeFH and one 2-year open-label, uncontrolled trial in 175 pediatric patients 8 years of age and older with HeFH [see Clinical Studies (14) ] . In the 1-year trial with a 12-week controlled phase, there was no detectable effect of CRESTOR on growth, weight, BMI (body mass index), or sexual maturation in patients aged 10 to 17 years. The safety and effectiveness of CRESTOR as an adjunct to other LDL-C-lowering therapies to reduce LDL-C have been established pediatric patients 7 years of age and older with HoFH. Use of CRESTOR for this indication is based on a randomized, placebo-controlled, cross-over study in 14 pediatric patients 7 years of age and older with HoFH [see Clinical Studies (14) ] . The safety and effectiveness of CRESTOR have not been established in pediatric patients younger than 8 years of age with HeFH, younger than 7 years of age with HoFH, or in pediatric patients with other types of hyperlipidemia (other than HeFH or HoFH). 8.5 Geriatric Use Of the total number of CRESTOR-treated patients in clinical studies, 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. Advanced age (≥65 years) is a risk factor for CRESTOR-associated myopathy and rhabdomyolysis. Dose selection for an elderly patient should be cautious, recognizing the greater frequency of decreased hepatic, renal, or cardiac function, and of concomitant disease or other drug therapy and the higher risk of myopathy. Monitor geriatric patients receiving CRESTOR for the increased risk of myopathy [see Warnings and Precautions (5.1) ] . 8.6 Renal Impairment Rosuvastatin exposure is not influenced by mild to moderate renal impairment (CL cr ≥30 mL/min/1.73 m 2 ). Exposure to rosuvastatin is increased to a clinically significant extent in patients with severe renal impairment (CL cr <30 mL/min/1.73 m 2 ) who are not receiving hemodialysis [see Clinical Pharmacology (12.3) ] . Renal impairment is a risk factor for myopathy and rhabdomyolysis. Monitor all patients with renal impairment for development of myopathy. In patients with severe renal impairment not on hemodialysis, the recommended starting dosage is 5 mg daily and should not exceed 10 mg daily [see Dosage and Administration (2.5) and Warnings and Precautions (5.1) ] . 8.7 Hepatic Impairment CRESTOR is contraindicated in patients with acute liver failure or decompensated cirrhosis. Chronic alcohol liver disease is known to increase rosuvastatin exposure. Patients who consume substantial quantities of alcohol and/or have a history of liver disease may be at increased risk for hepatic injury [see Contraindications (4) , Warning and Precautions (5.3) 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 White controls. Adjust the CRESTOR dosage in Asian patients [see Dosage and Administration (2.4) and Clinical Pharmacology (12.3) ] .

    How Supplied

    16 HOW SUPPLIED/STORAGE AND HANDLING CRESTOR tablets are supplied as: Strength How Supplied NDC Tablet Description 5 mg bottles of 90 tablets 0310-755-90 Yellow, round, biconvex, coated tablets. Debossed “CRESTOR” and “5” on one side 10 mg bottles of 90 tablets 0310-751-90 Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “10” on one side 20 mg bottles of 90 tablets 0310-752-90 Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “20” on one side 40 mg bottles of 30 tablets 0310-754-30 Pink, oval, biconvex, coated tablets. Debossed “CRESTOR” on one side and “40” on the other side Storage Store at controlled room temperature, 20ºC to 25ºC (68ºF to 77ºF); excursions permitted between 15°C and 30°C (59°F and 86°F) [see USP Controlled Room Temperature]. Protect from moisture.

    How Supplied Table

    Strength

    How Supplied

    NDC

    Tablet Description

    5 mg

    bottles of 90 tablets

    0310-755-90

    Yellow, round, biconvex, coated tablets. Debossed “CRESTOR” and “5” on one side

    10 mg

    bottles of 90 tablets

    0310-751-90

    Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “10” on one side

    20 mg

    bottles of 90 tablets

    0310-752-90

    Pink, round, biconvex, coated tablets. Debossed “CRESTOR” and “20” on one side

    40 mg

    bottles of 30 tablets

    0310-754-30

    Pink, oval, biconvex, coated tablets. Debossed “CRESTOR” on one side and “40” on the other side

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