About The Drug Mircera aka Methoxy Polyethylene glycol-epoetin beta
Find Mircera side effects, uses, warnings, interactions and indications. Mircera is also known as Methoxy Polyethylene glycol-epoetin beta.
Mircera
About Mircera aka Methoxy Polyethylene glycol-epoetin beta |
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What's The Definition Of The Medical Condition Mircera?Clinical Pharmacology CLINICAL PHARMACOLOGY Mechanism Of Action Mircera is an erythropoietin receptor activator with greater activity in vivo as well as increased half-life, in contrast to erythropoietin.
A primary growth factor for erythroid development, erythropoietin is produced in the kidney and released into the bloodstream in response to hypoxia.
In responding to hypoxia, erythropoietin interacts with erythroid progenitor cells to increase red cell production.
Production of endogenous erythropoietin is impaired in patients with CKD and erythropoietin deficiency is the primary cause of their anemia.
Pharmacodynamics Following a single-dose of Mircera in CKD patients, the onset of hemoglobin increase (defined as an increase > 0.4 g/dL from baseline) was observed 7 to 15 days following initial dose administration [see DOSAGE AND ADMINISTRATION].
Pharmacokinetics The pharmacokinetics of Mircera were studied in anemic patients with CKD including patients on dialysis and those not on dialysis.
Mircera pharmacokinetics, based on population analyses, were not altered by age, gender, race, or the use of dialysis.
Following an IV administration of Mircera 0.4 mcg/kg body weight to CKD patients receiving peritoneal dialysis, the observed terminal half-life was 134 ± 65 hours (mean ± SD), and the total systemic clearance was 0.49 ± 0.18 mL/hr/kg.
Following a SC administration of Mircera 0.8 mcg/kg to CKD patients receiving peritoneal dialysis, the terminal half-life was 139 ± 67 hours.
The maximum serum concentrations of Mircera were observed 72 hours (median value) following the SC administration.
The absolute bioavailability of Mircera after the SC administration was 62%.
In CKD patients receiving multiple Mircera doses, pharmacokinetics were studied after the first dose and on week 9 and week 19 or 21.
Multiple dosing was found to have no effect on clearance, volume of distribution or bioavailability of Mircera.
Based on population analyses of the clinical studies, Mircera did not accumulate following administration every four weeks.
However, when Mircera was administered every 2 weeks, blood concentrations at steady state increased by 12%.
A comparison of serum concentrations of Mircera measured before and after hemodialysis in 41 patients showed that hemodialysis did not alter serum concentrations.
The single-dose pharmacokinetics of Mircera in patients with severe (Child-Pugh Classification Grade C) hepatic impairment and healthy volunteers were similar.
The site of SC injection (abdomen, arm or thigh) had no clinically important effects on the pharmacokinetics or pharmacodynamics of Mircera in healthy volunteers.
Clinical Studies Patients With Chronic Kidney Disease On Dialysis: ESA Effects On Rates Of Transfusion In early clinical studies conducted in CKD patients on dialysis, ESAs have been shown to reduce the use of RBC transfusions.
These studies enrolled patients with mean baseline hemoglobin levels of approximately 7.5 g/dL and ESAs were generally titrated to achieve a hemoglobin level of approximately 12 g/dL.
Fewer transfusions were given during the ESA treatment period when compared to a pre-treatment interval.
In NHS, the yearly transfusion rate was 51.5% in the lower hemoglobin group (10 g/dL) and 32.4% in the higher hemoglobin group (14 g/dL).
Patients With Chronic Kidney Disease Not On Dialysis: ESA Effects On Rates Of Transfusion In TREAT, a randomized, double-blind trial of 4038 patients with CKD and type 2 diabetes not on dialysis, a post-hoc analysis showed that the proportion of patients receiving RBC transfusions was lower in patients administered an ESA to target a hemoglobin of 13 g/dL compared to the control arm in which the ESA was administered intermittently if hemoglobin concentration decreased to less than 9 g/dL (15% versus 25%, respectively).
In CHOIR, a randomized open-label study of 1432 patients with CKD not on dialysis, use of an ESA to target a higher (13.5 g/dL) versus lower (11.3 g/dL) hemoglobin goal did not reduce the use of RBC transfusions.
In each trial, no benefits occurred for the cardiovascular or end-stage renal disease outcomes.
In each trial, the potential benefit of ESA therapy was offset by worse cardiovascular safety outcomes resulting in an unfavorable benefit-risk profile [see WARNINGS AND PRECAUTIONS].
ESA Effects On Quality Of Life Mircera use has not been demonstrated in controlled clinical trials to improve quality of life, fatigue, or patient well-being.
ESA Effects On Rates Of Death And Other Serious Cardiac Adverse Events Three randomized outcome trials (NHS, CHOIR and TREAT) have been conducted in patients with CKD using Epogen/PROCRIT/Aranesp to target higher vs.
lower hemoglobin levels.
Though these trials were designed to establish a cardiovascular or renal benefit of targeting higher hemoglobin levels, in all 3 studies, patients randomized to the higher hemoglobin target experienced worse cardiovascular outcomes and showed no reduction in progression to ESRD.
In each trial, the potential benefit of ESA therapy was offset by worse cardiovascular safety outcomes resulting in an unfavorable benefit-risk profile [see WARNINGS AND PRECAUTIONS].
Other ESA trials The efficacy and safety of Mircera were assessed in six open-label, multi-center clinical studies that randomized patients to either Mircera or a comparator ESA.
Two studies evaluated anemic patients with CKD who were not treated with an ESA at baseline and four studies evaluated patients who were receiving an ESA for treatment of the anemia of CKD.
In all studies, patients were assessed as clinically stable at baseline and without evidence of infection or inflammation as determined by history and laboratory data, including C-reactive protein (CRP ≤ 15 mg/L for study 1 and CRP ≤ 30 mg/L for studies 2 to 6).
A CRP value above the threshold led to the exclusion of no more than 3% of the screened patients.
In the clinical studies, ESAs were administered to achieve specific hemoglobin levels (see Table 5 and Table 6).
Following stabilization of hemoglobin levels (12 g/dL), the median monthly Mircera dose was 150 mcg (range of 97 mcg to 270 mcg).
Patients Not Currently Treated with an ESA In Study 1 patients who were not receiving dialysis were randomized to Mircera or darbepoetin alfa, administered for 28 weeks.
The starting dose of Mircera was 0.6 mcg/kg administered SC once every two weeks and the starting dose of darbepoetin alfa was 0.45 mcg/kg administered SC once a week.
In Study 2, patients who were receiving dialysis were randomized to Mircera or another ESA (epoetin alfa or epoetin beta), administered for 24 weeks.
The starting dose of Mircera was 0.4 mcg/kg administered IV once every two weeks and the starting dose of the comparator was administered IV three times a week, consistent with the product's recommended dose.
In these studies, the observed median dose of Mircera once every two weeks over the course of the correction/evaluation period was 0.6 mcg/kg.
Table 5 provides the results of the two studies.
Table 5 : Clinical Studies in Patients Not Currently Treated with an ESA Group (n) Percent Achieving Goal* (95% CI) Mean Hemoglobin Change from Baseline (g/dL) RBC Transfusion, % Study 1 Mircera (n=162) 98 (94, 99) 2.1 2.5 Darbepoetin alfa (n=162) 96 (92, 99) 2.0 6.8 Study 2 Mircera (n=135) 93 (88, 97) 2.7 5.2 Epoetin alfa/beta (n=46) 91 (79, 98) 2.6 4.3 *Goal: hemoglobin increase of at least 1 g/dL and to a level of at least 11 g/dL without RBC transfusion; hemoglobin levels were to be maintained within the range of 11 to 13 g/dL.
Patients Currently Treated with an ESA Four studies assessed the ability of Mircera to maintain hemoglobin concentrations among patients currently treated with other ESAs.
Patients were randomized to receive Mircera administrations either once every two weeks or once every four weeks, or to continue their current ESA dose and schedule.
The initial Mircera dose was determined based on the patient's previous weekly ESA dose.
As shown in Table 6, treatment with Mircera once every two weeks and once every four weeks maintained hemoglobin concentrations within the targeted hemoglobin range (10 to 13.5 g/dL).
Table 6 : Clinical Studies in Patients Currently Treated with an ESA Group (n) Mean Baseline Hemoglobin Evaluation Period Hemoglobin (Mean) Between-group Difference *, g/dL (95% or 97.5% CI) Study 3 Mircera IV every 2 weeks (n=223) 12.0 11.9 0.0 (-0.2, 0.2) Mircera IV every 4 weeks (n=224) 11.9 11.9 0.1 (-0.2, 0.3) Epoetin alfa/beta IV (n=226) 12.0 11.9 n/a Study 4 Mircera SC every 2 weeks (n=190) 11.7 11.7 0.1 (-0.1, 0.4) Mircera SC every 4 weeks (n=191) 11.6 11.5 -0.0 (-0.3, 0.2) Epoetin beta SC (n=191) 11.6 11.5 n/a Study 5 Mircera IV every 2 weeks (n=157) 12.0 12.1 0.2 (-0.0, 0.4) Darbepoetin alfa IV 11.9 11.8 n/a Study 6 Mircera IV/SC every 2 weeks (n= 68) 11.8 11.9 0.1 (-0.1, 0.4) Epoetin alfa IV/SC (n=168) 11.9 11.8 0.1 (-0.1, 0.4) *Mircera versus comparator mean hemoglobin difference in the evaluation period; 97.5% CI are shown for studies that compared two Mircera groups to another ESA (Studies 3 and 4) and 95% CI are shown for the other studies.
n/a = not applicable
Drug Description Find Lowest Prices on MIRCERA® (methoxy polyethylene glycol-epoetin beta) Injection WARNINGS ESAs INCREASE THE RISK OF DEATH, MYOCARDIAL INFARCTION, STROKE, VENOUS THROMBOEMBOLISM, THROMBOSIS OF VASCULAR ACCESS, AND TUMOR PROGRESSION OR RECURRENCE Chronic Kidney Disease [see WARNINGS AND PRECAUTIONS] In controlled trials, patients experienced greater risks for death, serious adverse cardiovascular reactions, and stroke when administered erythropoiesis-stimulating agents (ESAs) to target a hemoglobin level of greater than 11 g/dL.
No trial has identified a hemoglobin target level, ESA dose, or dosing strategy that does not increase these risks.
Use the lowest Mircera dose sufficient to reduce the need for red blood cell (RBC) transfusions.
Cancer [see WARNINGS AND PRECAUTIONS] Mircera is not indicated and is not recommended for the treatment of anemia due to cancer chemotherapy.
A dose-ranging study of Mircera was terminated early because of more deaths among patients receiving Mircera than another ESA.
ESAs have shown shortened overall survival and/or increased the risk of tumor progression or recurrence in clinical studies in patients with breast, non-small cell lung, head and neck, lymphoid, and cervical cancers.
DESCRIPTION Mircera, methoxy polyethylene glycol-epoetin beta, is an ESA which differs from erythropoietin through formation of a chemical bond between either the N-terminal amino group or the ε-amino group of any lysine present in erythropoietin, predominantly Lys52 and Lys45, and methoxy polyethylene glycol (PEG) butanoic acid (approximately 30,000 daltons).
This results in a total molecular weight of approximately 60,000 daltons.
Mircera is formulated as a sterile, preservative-free protein solution for intravenous or subcutaneous administration.
Injectable solutions of Mircera in prefilled syringes (30 mcg, 50 mcg, 75 mcg, 100 mcg, 120 mcg, 150 mcg, 200 mcg, or 250 mcg in 0.3 mL) are formulated in an aqueous solution containing mannitol (9 mg), methionine (0.447 mg), poloxamer 188 (0.03 mg), sodium phosphate monobasic monohydrate (0.414 mg), and sodium sulphate (1.704 mg).
Mircera 360 mcg in 0.6 mL is formulated in an aqueous solution containing mannitol (18 mg), methionine (0.894 mg), poloxamer 188 (0.06 mg), sodium phosphate monobasic monohydrate (0.828 mg), and sodium sulphate (3.408 mg).
The solution is clear, colorless to slightly yellowish and the pH is 6.2 ± 0.2.
Indications & Dosage INDICATIONS Anemia Due To Chronic Kidney Disease Mircera is indicated for the treatment of anemia associated with chronic kidney disease (CKD) in adult patients on dialysis and patients not on dialysis.
Limitations Of Use Mircera is not indicated and is not recommended: In the treatment of anemia due to cancer chemotherapy [see WARNINGS AND PRECAUTIONS] As a substitute for RBC transfusions in patients who require immediate correction of anemia [see CLINICAL PHARMACOLOGY] Mircera has not been shown to improve symptoms, physical functioning or health-related quality of life.
DOSAGE AND ADMINISTRATION Evaluation Of Iron Stores and Nutritional Factors Evaluate the iron status in all patients before and during treatment and maintain iron repletion.
Correct or exclude other causes of anemia (e.g., vitamin deficiency, metabolic or chronic inflammatory conditions, bleeding, etc.) before initiating Mircera [see WARNINGS AND PRECAUTIONS].
Patients With Chronic Kidney Disease Individualize dosing and use the lowest dose of Mircera sufficient to reduce the need for RBC transfusions [see WARNINGS AND PRECAUTIONS].
In controlled trials, patients experienced greater risks for death, serious adverse cardiovascular reactions, and stroke when administered erythropoiesis-stimulating agents (ESAs) to target a hemoglobin level of greater than 11 g/dL.
No trial has identified a hemoglobin target level, ESA dose, or dosing strategy that does not increase these risks.
Physicians and patients should weigh the possible benefits of decreasing transfusions against the increased risks of death and other serious cardiovascular adverse events [see BOXED WARNING and Clinical Studies].
For all patients with CKD: When initiating or adjusting therapy, monitor hemoglobin levels at least weekly until stable, then monitor at least monthly.
When adjusting therapy consider hemoglobin rate of rise, rate of decline, ESA responsiveness and hemoglobin variability.
A single hemoglobin excursion may not require a dosing change.
Do not increase the dose more frequently than once every 4 weeks.
Decreases in dose can occur more frequently.
Avoid frequent dose adjustments.
If the hemoglobin rises rapidly (e.g., more than 1 g/dL in any 2-week period), reduce the dose of Mircera by 25% or more as needed to reduce rapid responses.
For patients who do not respond adequately, if the hemoglobin has not increased by more than 1 g/dL after 4 weeks of therapy, increase the dose by 25%.
For patients who do not respond adequately over a 12-week escalation period, increasing the Mircera dose further is unlikely to improve response and may increase risks.
Use the lowest dose that will maintain a hemoglobin level sufficient to reduce the need for RBC transfusions.
Evaluate other causes of anemia.
Discontinue Mircera if responsiveness does not improve.
Mircera is administered either intravenously (IV) or subcutaneously (SC).
When administered SC, Mircera should be injected in the abdomen, arm or thigh.
For Patients with CKD on dialysis: Initiate Mircera treatment when the hemoglobin level is less than 10 g/dL.
If the hemoglobin level approaches or exceeds 11 g/dL, reduce or interrupt the dose of Mircera.
The recommended starting dose of Mircera for the treatment of anemia in adult CKD patients who are not currently treated with an ESA is 0.6 mcg/kg body weight administered as a single IV or SC injection once every two weeks.
The IV route is recommended for patients receiving hemodialysis because the IV route may be less immunogenic [see ADVERSE REACTIONS].
Once the hemoglobin has been stabilized, Mircera may be administered once monthly using a dose that is twice that of the every-two-week dose and subsequently titrated as necessary.
For Patients with CKD not on dialysis: Consider initiating Mircera treatment only when the hemoglobin level is less than 10 g/dL and the following considerations apply: The rate of hemoglobin decline indicates the likelihood of requiring a RBC transfusion and, Reducing the risk of alloimmunization and/or other RBC transfusion-related risks is a goal If the hemoglobin level exceeds 10 g/dL, reduce or interrupt the dose of Mircera, and use the lowest dose of Mircera sufficient to reduce the need for RBC transfusions.
The recommended starting dose of Mircera for the treatment of anemia in adult CKD patients who are not currently treated with an ESA is 0.6 mcg/kg body weight administered as a single IV or SC injection once every two weeks.
Once the hemoglobin has been stabilized, Mircera may be administered once monthly using a dose that is twice that of the every-two-week dose and subsequently titrated as necessary.
Refer patients who self-administer Mircera to the Instructions for Use [see PATIENT INFORMATION].
Conversion From Epoetin Alfa Or Darbepoetin Alfa To Mircera In Patients With CKD Mircera can be administered once every two weeks or once monthly to patients whose hemoglobin has been stabilized by treatment with an ESA (see Table 1).
The dose of Mircera, given as a single IV or SC injection, should be based on the total weekly ESA dose at the time of conversion.
Table 1 : Mircera Starting Doses for Patients Currently Receiving an ESA Previous Weekly Epoetin alfa Dose (units/week) Previous Weekly Darbepoetin alfa Dose (mcg/week) Mircera Dose Once Monthly (mcg/month) Once Every Two Weeks (mcg/every two weeks) < 8000 < 40 120 60 8000 - 16000 40 - 80 200 100 > 16000 > 80 360 180 Preparation And Administration Of Mircera Mircera is packaged as single-dose prefilled syringes.
Mircera contains no preservatives.
Discard any unused portion.
Do not pool unused portions from the prefilled syringes.
Do not use the prefilled syringe more than one time.
Always store Mircera prefilled syringes in their original cartons.
Vigorous shaking or prolonged exposure to light should be avoided.
Do not mix Mircera with any parenteral solution.
Parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration.
Do not use any prefilled syringes exhibiting particulate matter or a coloration other than colorless to slightly yellowish.
For administration using the prefilled syringe, the plunger must be fully depressed during injection in order for the needle guard to activate.
Following administration, remove the needle from the injection site and then release the plunger to allow the needle guard to move up until the entire needle is covered.
See “Instructions for Use” for complete instructions on the preparation and administration of Mircera.
Examine each prefilled syringe for the expiration date.
Do not use Mircera after the expiration date.
HOW SUPPLIED Dosage Forms And Strengths Injection: 30 mcg, 50 mcg, 75 mcg, 100 mcg, 120 mcg, 150 mcg, 200 mcg, or 250 mcg in 0.3 mL; and 360 mcg in 0.6 mL solution in single-dose prefilled syringes Storage And Handling Mircera is available in single-dose prefilled syringes.
The syringe plungers are designated with unique colors for each dosage strength.
The prefilled syringes are supplied with a 27 gauge, ½ inch needle.
To reduce the risk of accidental needlesticks after application, each prefilled syringe is equipped with a needle guard that covers the needle during disposal.
Mircera is available in the following pack sizes: Single-Dose Prefilled Syringe (PFS) with a Needle Guard.
A 27 Gauge, ½ Inch Needle is also provided: 1 PFS/Pack 30 mcg/0.3 mL (NDC 59353-400-09) 50 mcg/0.3 mL (NDC 59353-401-09) 75 mcg/0.3 mL (NDC 59353-402-09) 100 mcg/0.3 mL (NDC 59353-403-09) 120 mcg/0.3 mL (NDC 59353-407-09) 50 mcg/0.3 mL (NDC 59353-404-09) 200 mcg/0.3 mL (NDC 59353-405-09) 250 mcg/0.3 mL (NDC 59353-406-09) 360 mcg/0.6 mL (NDC 59353-408-09) Storage The recommended storage temperature is at 2°C to 8°C (36°F to 46°F) in the original carton to protect from light.
Do not freeze or shake.
The end-user may store the product at room temperature up to 25°C (77°F) in the original carton up to 30 days.
Discard after 30 days.
Vifor (International) Inc., Rechenstrasse 37, 9014 St.
Gallen, Switzerland.
Toll-free: 1-800–576-8295.
Revised: April 2016
Medication Guide PATIENT INFORMATION MIRCERA® (mir-SER-ah) (methoxy polyethylene glycol-epoetin beta) Read this Medication Guide: before you start Mircera.
if you are told by your healthcare provider that there is new information about Mircera.
if you are told by your healthcare provider that you may inject Mircera at home, read this Medication Guide each time you receive a new supply of medicine.
This Medication Guide does not take the place of talking to your healthcare provider about your medical condition or your treatment.
Talk with your healthcare provider regularly about the use of Mircera and ask if there is new information about Mircera.
What is the most important information I should know about Mircera? Mircera may cause serious side effects that can lead to death, including: For people with cancer: Mircera is not for use to treat anemia that is caused by cancer chemotherapy.
If you have certain cancers, your tumor may grow faster and you may die sooner if you take Mircera.
Serious heart problems, such as heart attack or heart failure, and stroke.
You may die sooner if you are treated with Mircera to increase red blood cells (RBCs) to near the same level found in healthy people.
Blood clots.
Blood clots may happen at any time while taking Mircera.
If you are receiving Mircera for any reason and you are going to have surgery, talk to your healthcare provider about whether or not you need to take a blood thinner to lessen the chance of blood clots during or following surgery.
Clots can form in blood vessels (veins), especially in your leg (deep venous thrombosis or DVT).
Pieces of a blood clot may travel to the lungs and block the blood circulation in the lungs (pulmonary embolus).
Call your healthcare provider or get medical help right away if you have any of these symptoms: Chest pain Trouble breathing or shortness of breath Pain in your legs, with or without swelling A cool or pale arm or leg Sudden confusion, trouble speaking, or trouble understanding others' speech Sudden numbness or weakness in your face, arm or leg, especially on one side of your body Sudden trouble seeing Sudden trouble walking, dizziness, loss of balance or coordination Loss of consciousness (fainting) Hemodialysis vascular access stops working See “What are the possible side effects of Mircera?” below for more information.
If you decide to take Mircera, your healthcare provider should prescribe the smallest dose of Mircera that is necessary to reduce your chance of needing red blood cell transfusions.
What is Mircera? Mircera is a prescription medicine used to treat anemia.
People with anemia have a lower-thannormal number of RBCs.
Mircera works like the human protein called erythropoietin to help your body make more RBCs.
Mircera is used to reduce or avoid the need for RBC transfusion.
Mircera may be used to treat anemia if it is caused by chronic kidney disease (you may or may not be on dialysis).
If your hemoglobin level stays too high or if your hemoglobin goes up too quickly, this may lead to serious health problems which may result in death.
These serious health problems may happen if you take Mircera, even if you do not have an increase in your hemoglobin level.
Mircera is not for use for the treatment of anemia: that is caused by cancer chemotherapy in place of emergency treatment for anemia (red blood cell transfusions) Mircera has not been proven to improve the quality of life, fatigue, or well-being.
It is not known if Mircera is safe and effective in children.
Who should not take Mircera? Do not take Mircera if you: Have high blood pressure that is not controlled (uncontrolled hypertension) Have been told by your healthcare provider that you have or have ever had a type of anemia called Pure Red Cell Aplasia (PRCA) that starts after treatment with Mircera or other erythropoietin protein medicines Have had serious allergic reactions to Mircera What should I tell my healthcare provider before taking Mircera? Mircera may not be right for you.
Tell your healthcare provider about all of your medical conditions, including if you: Have heart disease Have or develop cancer Have high blood pressure Have had a seizure (convulsion) or stroke Have any other medical conditions Are pregnant or plan to become pregnant.
It is not known if Mircera may harm your unborn baby.
Are breastfeeding or plan to breastfeed.
It is not known if Mircera passes into your breast milk.
Tell your healthcare provider about all of the medicines you take, including prescription and over-the-counter medicines, vitamins, and herbal supplements.
Know the medicines you take.
Keep a list of your medicines with you and show it to your healthcare provider when you get a new medicine.
How should I take Mircera? If you or your caregiver has been trained to give Mircera shots (injections) at home: Be sure that you read, understand, and follow the “Instructions for Use” that come with Mircera.
Take Mircera exactly as your healthcare provider tells you to.
Do not change the dose of Mircera unless told to by your healthcare provider.
Your healthcare provider will show you how much Mircera to use, how to inject it, how often it should be injected, and how to safely throw away the used prefilled syringes and needles.
If you take more than your prescribed dose of Mircera, call your healthcare provider right away for instructions on what to do.
During treatment with Mircera, continue to follow your healthcare provider's instructions for diet, dialysis, and medicines, including medicines for high blood pressure.
Have your blood pressure checked as instructed by your healthcare provider.
What are possible side effects of Mircera? Mircera may cause serious side effects.
See “What is the most important information I should know about Mircera?” High blood pressure.
High blood pressure is a common side effect of Mircera in patients with chronic kidney disease.
Your blood pressure may go up or be difficult to control with blood pressure medicine while taking Mircera.
This can happen even if you have never had high blood pressure before.
Your healthcare provider should check your blood pressure often.
If your blood pressure does go up, your healthcare provider may prescribe new or more blood pressure medicine.
Seizures.
If you have any seizures while taking Mircera, get medical help right away and tell your healthcare provider.
No response or loss of your hemoglobin response to Mircera.
If your hemoglobin does not increase, or if the increase cannot be maintained, your healthcare provider will look for the cause of the problem.
Your dose of Mircera or other medicines may need to be changed.
Antibodies to Mircera.
Your body may make antibodies to Mircera.
These antibodies can block or reduce your body's ability to make red blood cells, and cause you to have severe anemia.
Call your healthcare provider if you have unusual tiredness, lack of energy, dizziness or fainting.
You may need to stop taking Mircera.
Serious allergic reaction.
Serious allergic reactions can cause a rash over your whole body, shortness of breath, wheezing, dizziness and fainting because of a drop in blood pressure, swelling around your mouth or eyes, fast pulse, or sweating.
If you have a serious allergic reaction, stop using Mircera and call your healthcare provider or get emergency medical help right away.
Common side effects of Mircera include: Diarrhea Upper respiratory tract infections (cold, cough and sinus infections) Tell your healthcare provider if you have any side effect that bothers you or that does not go away.
These are not all of the possible side effects of Mircera.
Your healthcare provider can give you a more complete list.
Tell your healthcare provider about any side effects that bother you or that do not go away.
Call your doctor for medical advice about side effects.
You may report side effects to FDA at 1800-FDA-1088.
How should I store Mircera? Store Mircera prefilled syringes in the refrigerator at 36°F to 46°F (2°C to 8°C).
If a refrigerator is not available, Mircera prefilled syringes can be stored at room temperature 77°F (25°C) for no more than 30 days.
Do not freeze Mircera.
Do not use Mircera that has been frozen or improperly refrigerated.
Keep Mircera in the original package.
Protect Mircera from light.
Do not shake Mircera.
Keep Mircera and all medicines out of the reach of children.
General information about Mircera Medicines are sometimes prescribed for purposes other than those listed in a Medication Guide.
Do not use Mircera for a condition for which it was not prescribed.
Do not give Mircera to other people, even if they have the same symptoms that you have.
It may harm them.
This Medication Guide summarizes the most important information about Mircera.
If you would like more information about Mircera, talk with your healthcare provider.
You can ask your healthcare provider or pharmacist for information about Mircera that is written for health professionals.
What are the ingredients in Mircera? Active ingredient: methoxy polyethylene glycol-epoetin beta Inactive ingredients: sodium phosphate, sodium sulphate, mannitol, methionine and poloxamer 188 Instructions for Use MIRCERA® (mir-SER-ah) (methoxy polyethylene glycol-epoetin beta) Injection Single-Dose Prefilled Syringe Read the Medication Guide that comes with Mircera for the most important information you need to know.
The following instructions explain how to give yourself or another individual an injection of Mircera using the single-dose prefilled syringe.
Be sure that you read, understand and follow these instructions before injecting a dose of Mircera so that you are able to use the prefilled syringe correctly and safely.
Your healthcare provider should show you how to correctly prepare and inject Mircera using the single-dose prefilled syringe before you use it for the first time.
Ask your healthcare provider or pharmacist if you have any questions about Mircera.
When you receive your Mircera prefilled syringes, make sure that: The name Mircera appears on the pack.
The pack is not damaged.
Do not use Mircera if the syringe, the pack or the plastic tray containing the syringe appears to be damaged.
The expiration date on the pack has not passed.
Do not use Mircera after the expiration date on the pack.
The strength (mcg/mL) on the Mircera pack is the same as the strength (mcg/mL) prescribed by your healthcare provider.
Mircera prefilled syringes come in several different strengths measured in mcg/mL.
Depending on your prescribed dose you may: receive more than one strength of Mircera prefilled syringes need to give more than one injection to receive a complete dose Important Information: Your healthcare provider may decide that you or a caregiver may give Mircera at home by an injection under your skin (subcutaneous) or by an intravenous (IV) injection.
Your healthcare provider or nurse will train you how to prepare and inject Mircera properly.
It is important that you do not try to give Mircera unless you or your caregiver has received training from your healthcare provider.
Keep the Mircera prefilled syringe in the sealed pack until you are ready to use it.
Do not hold or pull the prefilled syringe by the plunger.
Do not remove the needle shield until you are ready to give an injection.
Do not inject through clothing.
Do not touch the release clips before use (see Figure A).
Touching them may cause the needle safety device to be released too early and make the prefilled syringe unusable.
Throw away (dispose of) the used Mircera prefilled syringe right away after use.
Do not reuse a Mircera prefilled syringe or needle.
See “Disposing of used prefilled syringes and needles” at the end of this Instructions for Use.
Storage How should I store Mircera? Store Mircera in the refrigerator at 36°F to 46°F (2°C to 8°C).
If a refrigerator is not available, Mircera prefilled syringes can be stored at room temperature 77°F or less (25°C or less) for no more than 30 days.
Do not freeze Mircera.
Do not use Mircera that has been frozen.
Keep Mircera in the original package.
Protect Mircera from light.
Do not shake Mircera.
Keep Mircera and all medicines out of the reach of children.
Materials Materials included in the Mircera prefilled syringe pack (Figure A): A prefilled syringe containing Mircera A separate injection needle Figure A Materials not included in the Mircera prefilled syringe pack (Figure B): Figure B Important: Follow these instructions exactly to help avoid infections.
Preparing for an injection: 1.
Gather all of the materials you will need for an injection on a clean, well-lit, flat work surface such as a table.
2.
Allow the syringe to reach room temperature: Carefully remove your prescribed pack of Mircera from the refrigerator (see Figure C).
Keep the prefilled syringe in the pack to protect it from light and allow it to reach room temperature for about 30 minutes.
Figure C Do not warm up the prefilled syringe in any other way.
3.
Open the pack and remove the plastic tray containing the Mircera prefilled syringe without peeling back the protective film (see Figure D).
Figure D 4.
Wash your hands well with soap and warm water (see Figure E).
Figure E 5.
Remove and inspect the prefilled syringe.
Open the plastic tray by peeling back the protective film.
Remove the prefilled syringe by holding the syringe by the device body (see Figure F).
Do not touch the release clips.
Only handle the prefilled syringe by the device body.
Touching the release clips could cause the needle safety device to be released too early.
Remove the needle from the plastic tray.
Figure F 6.
Inspect the medicine and prefilled syringe (see Figure G.).
Do not use the prefilled syringe if: The prefilled syringe has been dropped or shaken Any part of the prefilled syringe appears cracked or damaged The liquid is foamy, cloudy, hazy or contains particles The expiration date has passed.
Figure G Attach needle to prefilled syringe: 7.
Grab the prefilled syringe by the finger grips.
Carefully pull the rubber tip cap away from the prefilled syringe.
It may require a strong bend and pull to remove it (see Figure H).
Figure H Throw away (dispose of) the rubber tip cap in the sharps disposal container Do not touch the release clips.
Do not push or pull on the plunger.
Place the syringe on your work surface.
Be careful that the tip of the prefilled syringe does not touch anything.
If the tip of the syringe touches anything, dispose of the prefilled syringe (see “Disposing of used prefilled syringes and needles” below) and use a new prefilled syringe and needle for the injection.
8.
Grab the packaged needle firmly in both hands.
Break the seal of the needle, using a twisting motion, and remove the plastic needle cap (see Figure I).
Throw away (dispose of) the needle cap right away in the sharps disposal container.
Do not remove the needle shield that protects the needle.
Figure I 9.
Attach the needle to the prefilled syringe by pushing it firmly onto the prefilled syringe (see Figure J).
Figure J 10.
Put the prefilled syringe on its side with the needle shield on.
This will keep the needle from touching anything before you use it.
Follow your healthcare provider's instructions for how you should inject Mircera.
Subcutaneous (under the skin) injection: If your healthcare provider tells you to inject Mircera under your skin, give your dose as described below: Selecting and preparing a subcutaneous injection site: 11.
Choose an injection site as shown in Figure K.
The three sites where you can inject Mircera include: the outer area of the upper arms the front of the middle thighs the abdomen, except for the two-inch area around the navel (belly-button) Choose a new injection site each time you inject Mircera, at least 1-inch from the area you used for the previous injection.
This helps to avoid soreness at any one site.
Figure K Do not inject Mircera into moles or into an area of your body that is tender, red, bruised, hard, or that has scars or stretch marks, or is not intact.
Do not inject into areas that could be irritated by a belt or waistband.
12.
Clean the injection site with an alcohol swab (see Figure L).
Let the skin dry for about 10 seconds.
Do not touch this area again before giving the injection.
Do not fan or blow on the clean area.
Figure L 13.
Hold the syringe firmly with one hand and pull off the needle shield with the other hand (see Figure M).
Throw away the needle shield in the sharps disposal container.
Do not touch the needle or let it touch any surface.
You may see a drop of liquid at the end of the needle.
This is normal.
Do not reattach the needle shield after removal.
Figure M 14.
Check the prefilled syringe for air bubbles.
To remove air bubbles from the prefilled syringe, hold the syringe by the body with the needle pointing up.
Tap the syringe gently to bring the air bubbles to the top (see Figure N).
Figure N 15.
Push the plunger up gently and slowly until you see a drop of liquid coming out of the needle (see Figure O).
Figure O 16.
Find a comfortable position to give an injection of Mircera.
Hold the prefilled syringe in the hand that you will use to inject Mircera.
Use the other hand to pinch a fold of loose skin at the cleaned injection site (see Figure P).
Figure P 17.
Hold the prefilled syringe like a pencil.
Fully and carefully insert the needle into the skin in a quick “dartlike” motion.
Insert straight up and down (90 degree angle) into the skin.
Keep the syringe in the skin and slowly let go of the pinch of skin.
Slowly push the plunger with your thumb all the way down while holding the syringe with the forefinger and the middle finger against the finger grips until all the medicine is injected (see Figure Q).
The plastic needle guard (a safety guard to prevent accidental needle sticks) will not move forward to cover the needle unless the full dose is given.
Do not move the needle while it is inserted in the skin.
Do not release the plunger before the end of injection or before the plunger is completely pushed down (depressed).
Figure Q 18.
Take the needle out of the skin without releasing the plunger (see Figure R).
Figure R 19.
Release the plunger after removing the needle from the skin.
This will allow the syringe to move back until the entire needle is covered with the needle guard (see Figure S).
Figure S 20.
Now the tear-off label can be removed, if necessary to keep a record of the dose taken (see Figure T).
Figure T 21.
After the injection: Place a sterile cotton ball or gauze over the injection site and press for several seconds (see Figure U).
Do not rub the injection site with an unclean hand or cloth.
If needed, you may cover the injection site with a small adhesive bandage.
Figure U 22.
Dispose of the used prefilled syringe: Throw away (dispose of) the used prefilled syringe and the attached needle in the sharps container right away.
Do not reuse your prefilled syringe or needle.
See “Disposing of used prefilled syringes and needles” below.
Intravenous (IV) injection: Injecting a dose of Mircera for people on hemodialysis using intravenous injection: Mircera can be injected in your vein through a special access (venous) port placed by your healthcare provider.
This type of Mircera injection is called an intravenous (IV) injection.
If your healthcare provider has shown you or your caregiver how to inject Mircera intravenously, you should follow the steps described below.
If you have a hemodialysis vascular access, make sure that the venous port is working by checking it as your healthcare provider has shown you.
Call your healthcare provider right away if you are having any problems or if you have any questions.
After you prepare the syringe as described in steps 7 to 10 above: Clean the venous port of the hemodialysis tubing with an alcohol swab (see Figure A).
Figure A 2.
Hold the syringe firmly with one hand and pull off the needle shield with the other hand (see Figure B).
Throw away the needle shield in the sharps disposal container.
Do not touch the needle or let it touch any surface.
You may see a drop of liquid at the end of the needle.
This is normal.
Do not reattach the needle shield after removal.
Figure B 3.
Check the prefilled syringe for air bubbles.
To remove air bubbles from the prefilled syringe, hold the syringe by the device body with the needle pointing up.
Tap the syringe gently to bring the air bubbles to the top (see Figure C).
Figure C 4.
Push the plunger up gently and slowly until you see a drop of liquid coming out of the needle (see Figure D).
Figure D 5.
Insert the needle on the prefilled syringe into the cleaned venous port (see Figure E).
Figure E 6.
Push the plunger with your thumb all the way down, while holding the syringe with the forefinger and the middle finger against the finger grips until all the medicine is injected (see Figure F).
Pull back on the syringe and remove the needle from the venous port without releasing the plunger.
Figure F The plastic needle guard (a safety guard to prevent accidental needle sticks) will not move forward to cover the needle unless the full dose is given (see Figure G).
Do not move the needle while it is inserted in the port.
Do not release the plunger before the end of injection or before the plunger is completely pushed down (depressed).
Figure G Release the plunger after removing the needle from the port.
This will allow the syringe to move back until the entire needle is covered with the needle guard (see Figure G).
7.
Now the tear-off label can be removed, if necessary to keep a record of the dose taken (see Figure H).
Figure H 8.
Dispose of the used prefilled syringe: Throw away (dispose of) the used prefilled syringe and the attached needle in the sharps container right away.
Do not reuse your prefilled syringe and needle.
See “Disposing of used prefilled syringes and needles” below.
Disposing of used prefilled syringes and needles: Put your used needles and prefilled syringes in an FDA-cleared sharps disposal container right away after use.
Do not throw away (dispose of) loose needles and prefilled syringes in your household trash.
If you do not have an FDA-cleared sharps disposal container, you may use a household container that is: made of heavy-duty plastic, can be closed with a tight-fitting, puncture-resistant lid, without sharps being able to come out, upright and stable during use, leak-resistant, and properly labeled to warn of hazardous waste inside the container.
When your sharps disposal container is almost full, you will need to follow your community guidelines for the right way to dispose of your sharps disposal container.
There may be state or local laws about how you should throw away used needles, syringes and prefilled injectors.
For more information about safe sharps disposal, and for specific information about sharps disposal in the state that you live in, go to the FDA's website at: http://www.fda.gov/safesharpsdisposal.
Do not dispose of your used sharps disposal container in your household trash unless your community guidelines permit this.
Do not recycle your used sharps disposal container.
Always keep the sharps disposal container out of the reach of children.
This Instructions for Use has been approved by the U.S.
Food and Drug Administration.
Overdosage & Contraindications Side Effects & Drug Interactions SIDE EFFECTS The following serious adverse reactions are discussed in greater detail in other sections of the labeling: Increased Mortality, Myocardial Infarction, Stroke, and Thromboembolism [see WARNINGS AND PRECAUTIONS] Increased mortality and/or tumor progression in patients with cancer [see WARNINGS AND PRECAUTIONS] Hypertension [see WARNINGS AND PRECAUTIONS] Seizures [see WARNINGS AND PRECAUTIONS] Pure red cell aplasia [see WARNINGS AND PRECAUTIONS] Serious allergic reactions [see WARNINGS AND PRECAUTIONS] Clinical Trials Experience The data described below reflect exposure to Mircera in 2737 patients, including 1451 exposed for 6 months and 1144 exposed for greater than one year.
Mircera was studied primarily in active-controlled studies (n=1789 received Mircera, and n=948 received another ESA) and in long-term follow up studies.
The population was 18 to 92 years of age, 58% male, and the percentage of Caucasian, Black (including African Americans), Asian and Hispanic patients were 73%, 20%, 5%, and 9%, respectively.
Approximately 85% of the patients were receiving dialysis.
Most patients received Mircera using dosing regimens of once every two or four weeks, administered SC or IV.
Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical studies of Mircera cannot be directly compared to rates in the clinical trials of other drugs and may not reflect the rates observed in practice.
The most commonly reported adverse reactions in ≥ 10% of patients were hypertension [see WARNINGS AND PRECAUTIONS], diarrhea, and nasopharyngitis.
The most common adverse reactions that led to treatment discontinuation in the Mircera clinical studies were: hypertension, coronary artery disease, anemia, concomitant termination of other CKD therapy and septic shock.
Some of the adverse reactions reported are typically associated with CKD, or recognized complications of dialysis, and may not necessarily be attributable to Mircera therapy.
Adverse reaction rates did not importantly differ between patients receiving Mircera or another ESA.
Table 4 summarizes the most frequent adverse reactions ( ≥ 5%) in patients treated with Mircera.
Table 4 : Adverse Reactions Occurring in ≥ 5% of CKD Patients Adverse Reaction Patients Treated with Mircera (n=1789) VASCULAR Hypertension 13% Hypotension 5% GASTROINTESTINAL Diarrhea 11% Vomiting 6% Constipation 5% INFECTIONS AND INFESTATIONS Nasopharyngitis 11% Upper Respiratory Tract Infection 9% Urinary Tract Infection 5% NERVOUS SYSTEM Headache 9% MUSCULOSKELETAL AND CONNECTIVE TISSUE Muscle Spasms 8% Back Pain 6% Pain in Extremity 5% INJURY, POISONING AND PROCEDURAL COMPLICATIONS Procedural Hypotension 8% Arteriovenous Fistula Thrombosis 5% Arteriovenous Fistula Site Complication 5% METABOLISM AND NUTRITION Fluid Overload 7% RESPIRATORY, THORACIC AND MEDIASTINAL Cough 6% In the controlled trials, the rates of serious adverse reactions did not importantly differ between patients receiving Mircera and another ESA (38% vs.
42%) except for the occurrence of serious gastrointestinal hemorrhage (1.2% vs.
0.2%).
Serious hemorrhagic adverse reactions of all types occurred among 5% and 4% of patients receiving Mircera or another ESA, respectively.
Immunogenicity As with all therapeutic proteins, there is a potential for immunogenicity.
Neutralizing antibodies to Mircera that cross-react with endogenous erythropoietin and other ESAs can result in PRCA or severe anemia (with or without other cytopenias) [see WARNINGS AND PRECAUTIONS].
Compared to SC administration, the IV route of administration may lessen the risk for development of antibodies to Mircera.
In 1789 patients treated with Mircera in clinical studies, antibody testing using an enzyme-linked immunosorbent assay (ELISA) was conducted at baseline and during treatment.
Antibody development was not detected in any of the patients.
The incidence of antibody formation is highly dependent on the sensitivity and specificity of the assay.
Additionally, the observed incidence of antibody (including neutralizing antibody) positivity in an assay may be influenced by several factors including assay methodology, sample handling, timing of sample collection, concomitant medications, and underlying disease.
For these reasons, comparison of the incidence of antibodies to Mircera with the incidence of antibodies to other ESAs may be misleading.
Postmarketing Experience The following adverse reactions have been identified during postapproval use of Mircera.
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.
Hypersensitivity Stevens-Johnson syndrome/toxic epidermal necrolysis has been reported [see WARNINGS AND PRECAUTIONS].
Pure Red Cell Aplasia (PRCA) Cases of PRCA and of severe anemia, with or without other cytopenias that arise following the development of neutralizing antibodies to erythropoietin have been reported in patients treated with Mircera [see WARNINGS AND PRECAUTIONS].
DRUG INTERACTIONS No formal drug/drug interaction studies have been performed.
Warnings & Precautions WARNINGS Included as part of the PRECAUTIONS section.
PRECAUTIONS Increased Mortality, Myocardial Infarction, Stroke, And Thromboembolism In controlled clinical trials of patients with CKD comparing higher hemoglobin targets (13 - 14 g/dL) to lower targets (9 - 11.3 g/dL), ESAs increased the risk of death, myocardial infarction, stroke, congestive heart failure, thrombosis of hemodialysis vascular access, and other thromboembolic events in the higher target groups.
Using ESAs to target a hemoglobin level of greater than 11 g/dL increases the risk of serious adverse cardiovascular reactions and has not been shown to provide additional benefit [see Clinical Studies].
Use caution in patients with coexistent cardiovascular disease and stroke [see DOSAGE AND ADMINISTRATION].
Patients with CKD and an insufficient hemoglobin response to ESA therapy may be at even greater risk for cardiovascular reactions and mortality than other patients.
A rate of hemoglobin rise of greater than 1 g/dL over 2 weeks may contribute to these risks.
In controlled clinical trials of patients with cancer, ESAs increased the risks for death and serious adverse cardiovascular reactions.
These adverse reactions included myocardial infarction and stroke.
In controlled clinical trials, ESAs increased the risk of death in patients undergoing coronary artery bypass graft surgery (CABG) and the risk of deep venous thrombosis (DVT) in patients undergoing orthopedic procedures.
The design and overall results of the 3 large trials comparing higher and lower hemoglobin targets are shown in Table 2 (Normal Hematocrit Study (NHS), Correction of Hemoglobin Outcomes in Renal Insufficiency (CHOIR) and Trial to Reduce Cardiovascular Events with Aranesp® Therapy (TREAT)).
Table 2 : Randomized Controlled Trials Showing Adverse Cardiovascular Outcomes in Patients With CKD NHS (N = 1265) CHOIR (N = 1432) TREAT (N = 4038) Time Period of Trial 1993 to 1996 2003 to 2006 2004 to 2009 Population CKD patients on hemodialysis with coexisting CHF or CAD, hematocrit 30 ± 3% on epoetin alfa CKD patients not on dialysis with hemoglobin < 11 g/dL not previously administered epoetin alfa CKD patients not on dialysis with type II diabetes, hemoglobin ≤ 11 g/dL Hemoglobin Target; Higher vs.
Lower (g/dL) 14.0 vs.
10.0 13.5 vs.
11.3 13.0 vs.
≥ 9.0 Median (Q1, Q3) Achieved Hemoglobin level (g/dL) 12.6 (11.6, 13.3) vs.
10.3 (10.0, 10.7) 13.0 (12.2, 13.4) vs.
11.4 (11.1, 11.6) 12.5 (12.0, 12.8) vs.
10.6 (9.9, 11.3) Primary Endpoint All-cause mortality or nonfatal MI All-cause mortality, MI, hospitalization for CHF, or stroke All-cause mortality, MI, myocardial ischemia, heart failure, and stroke Hazard Ratio or Relative Risk (95% CI) 1.28 (1.06 - 1.56) 1.34 (1.03 - 1.74) 1.05 (0.94 - 1.17) Adverse Outcome for Higher Target Group All-cause mortality All-cause mortality Stroke Hazard Ratio or Relative Risk (95% CI) 1.27 (1.04 - 1.54) 1.48 (0.97 - 2.27) 1.92 (1.38 - 2.68) Patients With Chronic Kidney Disease NHS: A prospective, randomized, open-label study of 1265 patients with chronic kidney disease on dialysis with documented evidence of congestive heart failure or ischemic heart disease was designed to test the hypothesis that a higher target hematocrit (Hct) would result in improved outcomes compared with a lower target Hct.
In this study, patients were randomized to epoetin alfa treatment targeted to a maintenance hemoglobin of either 14 ± 1 g/dL or 10 ± 1 g/dL.
The trial was terminated early with adverse safety findings of higher mortality in the high hematocrit target group.
Higher mortality (35% vs.
29%) was observed for the patients randomized to a target hemoglobin of 14 g/dL than for the patients randomized to a target hemoglobin of 10 g/dL.
For all-cause mortality, the HR=1.27; 95% CI (1.04, 1.54); p=0.018.
The incidence of nonfatal myocardial infarction, vascular access thrombosis, and other thrombotic events was also higher in the group randomized to a target hemoglobin of 14 g/dL.
CHOIR: In a randomized prospective trial, 1432 patients with anemia due to CKD who were not undergoing dialysis were assigned to epoetin alfa treatment targeting a maintenance hemoglobin concentration of 13.5 g/dL or 11.3 g/dL.
The trial was terminated early with adverse safety findings.
A major cardiovascular event (death, myocardial infarction, stroke, or hospitalization for congestive heart failure) occurred among 125 (18%) of the 715 patients in the higher hemoglobin group compared to 97 (14%) among the 717 patients in the lower hemoglobin group (HR 1.3, 95% CI: 1.0, 1.7 p=0.03).
TREAT: A randomized, double-blind, placebo-controlled, prospective trial of 4038 patients with: CKD not on dialysis (eGFR of 20 – 60 mL/min), anemia (hemoglobin levels ≤ 11 g/dL), and type 2 diabetes mellitus, patients were randomized to receive either darbepoetin alfa treatment or a matching placebo.
Placebo group patients also received darbepoetin alfa when their hemoglobin levels were below 9 g/dL.
The trial objectives were to demonstrate the benefit of darbepoetin alfa treatment of the anemia to a target hemoglobin level of 13 g/dL, when compared to a “placebo” group, by reducing the occurrence of either of two primary endpoints: (1) a composite cardiovascular endpoint of all-cause mortality or a specified cardiovascular event (myocardial ischemia, CHF, MI, and CVA) or (2) a composite renal endpoint of all-cause mortality or progression to end stage renal disease.
The overall risks for each of the two primary endpoints (the cardiovascular composite and the renal composite) were not reduced with darbepoetin alfa treatment (see Table 2), but the risk of stroke was increased nearly two-fold in the darbepoetin alfa -treated group versus the placebo group: annualized stroke rate 2.1% vs.
1.1%, respectively, HR 1.92; 95% CI: 1.38, 2.68; p < 0.001.
The relative risk of stroke was particularly high in patients with a prior stroke: annualized stroke rate 5.2% in the darbepoetin alfa-treated group and 1.9% in the placebo group, HR 3.07; 95% CI: 1.44, 6.54.
Also, among darbepoetin alfa-treated subjects with a past history of cancer, there were more deaths due to all causes and more deaths adjudicated as due to cancer, in comparison with the control group.
Patients With Cancer An increased incidence of thromboembolic reactions, some serious and life-threatening, occurred in patients with cancer treated with ESAs.
In a randomized, placebo-controlled study (Study 1 in Table 3 [see Increased Mortality and/or Increased Risk of Tumor Progression or Recurrence in Patients with Cancer]) of 939 women with metastatic breast cancer receiving chemotherapy, patients received either weekly epoetin alfa or placebo for up to a year.
This study was designed to show that survival was superior when epoetin alfa was administered to prevent anemia (maintain hemoglobin levels between 12 and 14 g/dL or hematocrit between 36% and 42%).
This study was terminated prematurely when interim results demonstrated a higher mortality at 4 months (8.7% vs.
3.4%) and a higher rate of fatal thrombotic reactions (1.1% vs.
0.2%) in the first 4 months of the study among patients treated with epoetin alfa.
Based on Kaplan-Meier estimates, at the time of study termination, the 12-month survival was lower in the epoetin alfa group than in the placebo group (70% vs.
76%; HR 1.37, 95% CI: 1.07, 1.75; p = 0.012).
Patients Having Surgery Mircera is not approved for reduction of RBC transfusions in patients scheduled for surgical procedures.
An increased incidence of deep vein thrombosis (DVT) in patients receiving epoetin alfa undergoing surgical orthopedic procedures has been observed.
In a randomized controlled study (referred to as the “SPINE” study), 681 adult patients, not receiving prophylactic anticoagulation and undergoing spinal surgery, received epoetin alfa and standard of care (SOC) treatment, or SOC treatment alone.
Preliminary analysis showed a higher incidence of DVT, determined by either Color Flow Duplex Imaging or by clinical symptoms, in the epoetin alfa group [16 patients (4.7%)] compared to the SOC group [7 patients (2.1%)].
In addition, 12 patients in the epoetin alfa group and 7 patients in the SOC group had other thrombotic vascular events.
Increased mortality was observed in a randomized placebo-controlled study of epoetin alfa in adult patients who were undergoing coronary artery bypass surgery (7 deaths in 126 patients randomized to epoetin alfa versus no deaths among 56 patients receiving placebo).
Four of these deaths occurred during the period of study drug administration and all four deaths were associated with thrombotic events.
Increased Mortality And/Or Increased Risk Of Tumor Progression Or Recurrence In Patients With Cancer Mircera is not indicated and is not recommended for use in the treatment of anemia due to cancer chemotherapy.
A dose-ranging trial of Mircera in 153 patients who were undergoing chemotherapy for non-small cell lung cancer was terminated prematurely because more deaths occurred among patients receiving Mircera than another ESA.
ESAs resulted in decreased locoregional control/progression-free survival and/or overall survival (see Table 3).
These findings were observed in studies of patients with advanced head and neck cancer receiving radiation therapy (Studies 5 and 6), in patients receiving chemotherapy for metastatic breast cancer (Study 1) or lymphoid malignancy (Study 2), and in patients with non-small cell lung cancer or various malignancies who were not receiving chemotherapy or radiotherapy (Studies 7 and 8).
Table 3 : Randomized, Controlled Trials with Decreased Survival and/or Decreased Locoregional Control Study/Tumor (n) Hemoglobin Target Achieved Hemoglobin (Median Q1,Q3*) Primary Endpoint Adverse Outcome for ESA-containing Arm Chemotherapy Cancer Study 1 Metastatic breast cancer (n=939) 12-14 g/dL 12.9 g/dL 12.2, 13.3 g/dL 12-month overall survival Decreased 12-month survival Cancer Study 2 Lymphoid malignancy (n=344) 13-15 g/dL (M) 13-14 g/dL (F) 11.0 g/dL 9.8, 12.1 g/dL Proportion of patients achieving a hemoglobin response Decreased overall survival Cancer Study 3 Early breast cancer (n=733) 12.5-13 g/dL 12-14 g/dL 13.1 g/dL 12.5, 13.7 g/dL 12.7 g/dL Relapse-free and overall survival Progression-free Decreased 3-year relapse-free and overall survival Decreased 3-year Cancer Study 4 Cervical cancer (n=114) 12.1, 13.3 g/dL and overall survival and locoregional control progression-free and overall survival and locoregional control Radiotherapy Alone Cancer Study 5 Head and neck cancer (n=351) > 15 g/dL (M)> 14 g/dL (F) Not available Locoregional progression-free survival (LRPFS) Decreased 5-year locoregional progression-free survival Decreased overall survival Cancer Study 6 Head and neck cancer (n=522) 14-15.5 g/dL Not available Locoregional disease control (LRC) Decreased locoregional disease control No Chemotherapy orRadiotherapy Cancer Study 7 Non-small cell lung cancer (n=70) 12-14 g/dL Not available Quality of life Decreased overall survival Cancer Study 8 Non-myeloid malignancy (n=989) 12-13 g/dL 10.6 g/dL 9.4, 11.8 g/dL RBC transfusions Decreased overall survival *Q1= 25th percentile; Q3= 75th percentile Decreased Overall Survival Cancer Study 1 (the “BEST” study) was previously described [see Increased Mortality, Myocardial Infarction, Stroke, And Thromboembolism].
Mortality at 4 months (8.7% vs.
3.4%) was significantly higher in the epoetin alfa arm.
The most common investigator-attributed cause of death within the first 4 months was disease progression; 28 of 41 deaths in the epoetin alfa arm and 13 of 16 deaths in the placebo arm were attributed to disease progression.
Investigator assessed time to tumor progression was not different between the two groups.
Survival at 12 months was significantly lower in the epoetin alfa arm (70% vs.
76%, HR 1.37, 95% CI: 1.07, 1.75; p=0.012).
Cancer Study 2 was a Phase 3, double-blind, randomized (darbepoetin alfa vs.
placebo) study conducted in 344 anemic patients with lymphoid malignancy receiving chemotherapy.
With a median follow-up of 29 months, overall mortality rates were significantly higher among patients randomized to darbepoetin alfa as compared to placebo (HR 1.36, 95% CI: 1.02, 1.82).
Cancer Study 7 was a Phase 3, multicenter, randomized (epoetin alfa vs.
placebo), double-blind study, in which patients with advanced non-small cell lung cancer receiving only palliative radiotherapy or no active therapy were treated with epoetin alfa to achieve and maintain hemoglobin levels between 12 and 14 g/dL.
Following an interim analysis of 70 of 300 patients planned, a significant difference in survival in favor of the patients on the placebo arm of the trial was observed (median survival 63 vs.
129 days; HR 1.84; p=0.04).
Cancer Study 8 was a Phase 3, double-blind, randomized (darbepoetin alfa vs.
placebo), 16-week study in 989 anemic patients with active malignant disease, neither receiving nor planning to receive chemotherapy or radiation therapy.
There was no evidence of a statistically significant reduction in proportion of patients receiving RBC transfusions.
The median survival was shorter in the darbepoetin alfa treatment group (8 months) compared with the placebo group (10.8 months); HR 1.30, 95% CI: 1.07, 1.57.
Decreased Progression-free Survival and Overall Survival Cancer Study 3 (the “PREPARE” study) was a randomized controlled study in which darbepoetin alfa was administered to prevent anemia conducted in 733 women receiving neo-adjuvant breast cancer treatment.
A final analysis was performed after a median follow-up of approximately 3 years at which time the survival rate was lower (86% vs.
90%, HR 1.42, 95% CI: 0.93, 2.18) and relapse-free survival rate was lower (72% vs.
78%, HR 1.33, 95% CI: 0.99, 1.79) in the darbepoetin alfa-treated arm compared to the control arm.
Cancer Study 4 (protocol GOG 191) was a randomized controlled study that enrolled 114 of a planned 460 cervical cancer patients receiving chemotherapy and radiotherapy.
Patients were randomized to receive epoetin alfa to maintain hemoglobin between 12 and 14 g/dL or to transfusion support as needed.
The study was terminated prematurely due to an increase in thromboembolic events in epoetin alfa-treated patients compared to control (19% vs.
9%).
Both local recurrence (21% vs.
20%) and distant recurrence (12% vs.
7%) were more frequent in epoetin alfa-treated patients compared to control.
Progression-free survival at 3 years was lower in the epoetin alfa-treated group compared to control (59% vs.
62%, HR 1.06, 95% CI: 0.58, 1.91).
Overall survival at 3 years was lower in the epoetin alfa-treated group compared to control (61% vs.
71%, HR 1.28, 95% CI: 0.68, 2.42).
Cancer Study 5 (the “ENHANCE” study) was a randomized controlled study in 351 head and neck cancer patients where epoetin beta or placebo was administered to achieve target hemoglobins of 14 and 15 g/dL for women and men, respectively.
Locoregional progression-free survival was significantly shorter in patients receiving epoetin beta (HR 1.62, 95% CI: 1.22, 2.14, p=0.0008) with a median of 406 days epoetin beta vs.
745 days placebo.
Overall survival was significantly shorter in patients receiving epoetin beta (HR 1.39, 95% CI: 1.05, 1.84; p=0.02).
Decreased Locoregional Control Cancer Study 6 (DAHANCA 10) was conducted in 522 patients with primary squamous cell carcinoma of the head and neck receiving radiation therapy randomized to darbepoetin alfa with radiotherapy or radiotherapy alone.
An interim analysis on 484 patients demonstrated that locoregional control at 5 years was significantly shorter in patients receiving darbepoetin alfa (RR 1.44, 95% CI: 1.06, 1.96; p=0.02).
Overall survival was shorter in patients receiving darbepoetin alfa (RR 1.28, 95% CI: 0.98, 1.68; p=0.08).
Hypertension Mircera is contraindicated in patients with uncontrolled hypertension.
In Mircera clinical studies, approximately 27% of patients with CKD, including patients on dialysis and patients not on dialysis, required intensification of antihypertensive therapy.
Hypertensive encephalopathy and/or seizures have been observed in patients with CKD treated with Mircera [see Seizures].
Appropriately control hypertension prior to initiation of and during treatment with Mircera.
Reduce or withhold Mircera if blood pressure becomes difficult to control.
Advise patients of the importance of compliance with antihypertensive therapy and dietary restrictions [see PATIENT INFORMATION].
Seizures Seizures have occurred in patients participating in Mircera clinical studies.
During the first several months following initiation of Mircera, monitor patients closely for premonitory neurologic symptoms.
Advise patients to contact their healthcare practitioner for new-onset seizures, premonitory symptoms, or change in seizure frequency.
Lack Or Loss Of Hemoglobin Response To Mircera For lack or loss of hemoglobin response to Mircera, initiate a search for causative factors (e.g., iron deficiency, infection, inflammation, bleeding).
If typical causes of lack or loss of hemoglobin response are excluded, evaluate for PRCA [see Pure Red Cell Aplasia].
In the absence of PRCA, follow dosing recommendations for management of patients with an insufficient response to Mircera therapy [see DOSAGE AND ADMINISTRATION].
Pure Red Cell Aplasia Cases of PRCA and of severe anemia, with or without other cytopenias that arise following the development of neutralizing antibodies to erythropoietin have been reported in the postmarketing setting in patients treated with Mircera.
This has been reported predominantly in patients with CKD receiving ESAs by SC administration.
PRCA was not observed in clinical studies of Mircera.
PRCA has also been reported in patients receiving ESAs for anemia related to hepatitis C treatment (an indication for which Mircera is not approved).
If severe anemia and low reticulocyte count develop during treatment with Mircera, withhold Mircera and evaluate patients for neutralizing antibodies to erythropoietin [see Lack or Loss of Hemoglobin Response to Mircera].
Serum samples should be obtained at least a month after the last Mircera administration to prevent interference of Mircera with the assay.
Contact Vifor at 1-800-576-8295 to perform assays for binding and neutralizing antibodies.
Permanently discontinue Mircera in patients who develop PRCA following treatment with Mircera or other erythropoietin protein drugs.
Do not switch patients to other ESAs as antibodies may cross-react [see ADVERSE REACTIONS].
Serious Allergic Reactions Serious allergic reactions, including anaphylactic reactions, angioedema, bronchospasm, tachycardia, pruritus skin rash, urticaria, and Stevens-Johnson syndrome/toxic epidermal necrolysis have been reported in patients treated with Mircera.
If a serious allergic or anaphylactic reaction occurs due to Mircera, immediately and permanently discontinue Mircera and administer appropriate therapy.
Dialysis Management Therapy with Mircera results in an increase in red blood cells and a decrease in plasma volume, which could reduce dialysis efficiency; patients may require adjustments in their dialysis prescription after initiation of Mircera.
Patients receiving Mircera may require increased anticoagulation with heparin to prevent clotting of the extracorporeal circuit during hemodialysis.
Laboratory Monitoring Evaluate transferrin saturation and serum ferritin prior to and during Mircera treatment.
Administer supplemental iron therapy when serum ferritin is less than 100 mcg/L or when serum transferrin saturation is less than 20% [see DOSAGE AND ADMINISTRATION].
The majority of patients with CKD will require supplemental iron during the course of ESA therapy.
Following initiation of therapy and after each dose adjustment, monitor hemoglobin weekly until the hemoglobin is stable and sufficient to minimize the need for RBC transfusion.
Thereafter, hemoglobin should be monitored at least monthly provided hemoglobin levels remain stable [see DOSAGE AND ADMINISTRATION].
Patient Counseling Information See Medication Guide and Instructions for Use Prior to treatment, inform patients of the risks and benefits of Mircera.
Inform patients: To read the Medication Guide and to review and discuss any questions or concerns with their healthcare provider before starting Mircera and at regular intervals while receiving Mircera Of the increased risks of mortality, serious cardiovascular reactions, thromboembolic reactions, stroke, and tumor progression [see WARNINGS AND PRECAUTIONS] To undergo regular blood pressure monitoring, adhere to prescribed anti-hypertensive regimen and follow recommended dietary restrictions To seek medical care immediately if they experience any symptoms of an allergic reaction with use of Mircera [see WARNINGS AND PRECAUTIONS] To contact their healthcare provider for new-onset neurologic symptoms or change in seizure frequency Of the need to have regular laboratory tests for hemoglobin Administer Mircera under the direct supervision of a healthcare provider or, in situations where a patient has been trained to administer Mircera at home, provide instruction on the proper use of Mircera, including instructions to: Carefully review the Medication Guide and the Instructions for Use Avoid the reuse of needles, syringes, or unused portions of the Mircera single-dose prefilled syringes and to properly dispose of these items Always keep a puncture-proof disposal container available for the disposal of used syringes and needles Nonclinical Toxicology Carcinogenesis, Mutagenesis, Impairment Of Fertility No carcinogenicity or genotoxicity studies have been conducted with Mircera.
Methoxy polyethylene glycolepoetin beta did not induce a proliferative response in either the erythropoietin receptor positive cell lines HepG2 and K562 or the erythropoietin receptor negative cell line RT112 in vitro.
In addition, using a panel of human tissues, the in vitro binding of methoxy polyethylene glycol-epoetin beta was observed only in bone marrow progenitor cells.
When methoxy polyethylene glycol-epoetin beta was administered subcutaneously to male and female rats prior to and during mating, reproductive performance, fertility, and sperm assessment parameters were not affected.
Use In Specific Populations Pregnancy Category C Risk Summary There are no adequate and well-controlled studies in pregnant women.
Mircera should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.
Animal Data When methoxy polyethylene glycol-epoetin beta was administered subcutaneously to rats and rabbits during gestation, bone malformation was observed in both species at 50 mcg/kg once every three days.
This effect was observed as missing caudal vertebrae resulting in a thread-like tail in one rat fetus, absent first digit metacarpal and phalanx on each forelimb resulting in absent pollex in one rabbit fetus, and fused fourth and fifth cervical vertebrae centra in another rabbit fetus.
Dose-related reduction in fetal weights was observed in both rats and rabbits.
At doses 5 mcg/kg once every three days and higher, methoxy polyethylene glycol-epoetin beta caused exaggerated pharmacodynamic effects in dams.
Once-weekly doses of methoxy polyethylene glycol-epoetin beta up to 50 mcg/kg/dose given to pregnant rats did not adversely affect pregnancy parameters, natural delivery or litter observations.
Increased deaths and significant reduction in the growth rate of the F1 generation were observed during lactation and early post weaning period.
However, no remarkable effect on reflex, physical and cognitive development or reproductive performance was observed in F1 generation of any dose groups.
Nursing Mothers It is not known whether Mircera is excreted into human breast milk.
In one study in rats, methoxy polyethylene glycol-epoetin beta was excreted into maternal milk.
Because many drugs are excreted in human milk, caution should be exercised when Mircera is administered to a nursing woman.
Pediatric Use The safety and efficacy of Mircera in pediatric patients have not been established.
Geriatric Use Clinical studies of Mircera did not include sufficient numbers of subjects aged 65 and over to determine whether they respond differently from younger subjects.
Other reported clinical experience has not identified differences in responses between the elderly and younger patients.
In general, dose selection for an elderly patient should be cautious, usually starting at the low end of the dosing range, reflecting the greater frequency of decreased hepatic, renal, or cardiac function and of concomitant disease or other drug therapy.
Hepatic Impairment In a study comparing 12 patients with severe (Child-Pugh Classification Grade C) hepatic impairment to 12 healthy volunteers, the single-dose pharmacokinetic disposition of Mircera was not altered in patients with hepatic impairment.
No adjustment of the starting dose is necessary in patients with hepatic impairment.
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