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  5. Information for Epogen/Procrit (Epoetin alfa)
  1. Postmarket Drug Safety Information for Patients and Providers

Information for Epogen/Procrit (Epoetin alfa)

FDA announced on April 13, 2017 the elimination of the risk evaluation and mitigation strategy (REMS) for Epogen/Procrit (epoetin alfa).

Epogen/Procrit was approved on June 1, 1989 for the treatment of anemia associated with chronic renal failure, including patients on dialysis and patients not on dialysis and on April 1, 1993 for the treatment of anemia due to the effects of concomitant myelosuppressive chemotherapy. Aranesp is an Erythropoiesis-Stimulating Agents (ESAs). ESAs work like the human protein erythropoietin, which stimulates bone marrow to make red blood cells. Epogen/Procrit is also indicated for anemia due to zidovudine in patients with HIV and reduction of RBC transfusions in patients certain surgeries.

Epogen/Procrit increases the risk of death, myocardial infarction, stroke, venous thromboembolism, and thrombosis of vascular access and tumor progession or recurrence. Epogen/Procrit can also lead to an increase in adverse cardiovascular events, hypertension, seizures, and severe anemia.

In 2008, FDA determined a REMS was necessary for the ESAs, Epogen/Procrit (epoetin alfa) and Aranesp (darbopoetin alfa), to ensure the benefits for use as treatment for anemia associated with myelosuppressive chemotherapy outweigh its risks of shortened overall survival and/or increased risk of tumor progression or recurrence in patients with cancer. The REMS was approved in 2010. Under the REMS program, referred to as the ESA APPRISE Oncology Program, healthcare providers that prescribed and/or dispensed Aranesp to patients with cancer and hospitals that dispensed Aranesp to patients with cancer were required to enroll and become certified in the ESA REMS. The ESA REMS also required a Patient and Healthcare Provider Acknowledgement Form be completed for each patient with cancer before the new ESA treatment course to ensure patients were counseled about the benefits and risks of these products.

The FDA determined that the ESA REMS, which was limited to the use of Epogen/Procrit and Aranesp to treat patients with anemia due to associated myelosuppressive chemotherapy is no longer necessary to ensure that the benefits of Epogen/Procrit and Aranesp outweigh its risks of shortened overall survival and/or increased risk of tumor progression or recurrence in patients with cancer.

The agency made this determination based on an evaluation of the results of the REMS Assessments submitted by Amgen, Inc., and additional FDA analyses to understand the impact of the various regulatory and other actions on the use of ESAs.

The REMS Assessment showed that:

  • The results from surveyed prescribers demonstrate acceptable knowledge of the product risks of decreased survival and/or the increased risk of tumor progression or recurrence and the need to counsel patients about these risks.
  • The drug utilization data that indicates appropriate prescribing of ESAs consistent with the FDA approved indication.

FDA conducted an evaluation of the impact of multiple actions, including the ESA REMS, on the utilization of the ESAs using sponsor-submitted data from outpatient oncology practices between 2006 and 2014. During 2004-2009, FDA took multiple regulatory actions, including labeling changes. In 2007, the Center for Medicare and Medicaid Services (CMS) made a National Coverage Determination (NCD) to limit coverage of the ESAs for on-renal disease indications. These actions coincided with:

  • A decrease in the proportion of patients receiving chemotherapy using ESAs,
  • An increase in the proportion of patients receiving chemotherapy who initiate ESAs at a hemoglobin level 10g>
  • An increase in the proportion of patients who initiate ESAs at a dosage consistent with product prescribing information.

Full implementation of the ESA REMS in 2011 had minimal impact on trends in these three ESA utilization metrics beyond the changes observed after the CMS coverage determination and multiple other FDA regulatory actions.

This information led FDA to conclude that it is no longer necessary to require the certification of prescribers and hospitals that prescribe and/or dispense ESAs to patients with cancer in order to ensure the benefits outweigh the risks.

The FDA has released the REMS requirements for the ESA products, Epogen/Procrit and Aranesp, and the risks can be communicated by the current product prescribing information. The appropriate use of ESAs is supported by the CMS NCD, the American Society of Clinical Oncology (ASCO) and American Society of Hematology (ASH) clinical guidelines which are evidence-based guidelines intended to provide a basis for the standard of care in clinical oncology.

Prescribers should continue to follow the labeled directions for initiation and dose selection of Epogen/Procrit in order to treat anemia associated with chemotherapy in patients with cancer

By eliminating the Epogen/Procrit REMS:

  • Health care professionals who prescribe Epogen/Procrit for the treatment of anemia due to myelosuppressive chemotherapy will no longer be required to enroll and become certified in the ESA REMS to prescribe or dispense Aranesp.
  • Prescribers will no longer be required to complete a Patient and Healthcare Provider Acknowledgement Form for each patient with cancer before the new Epogen/Procrit treatment course.
  • Hospitals that dispense Epogen/Procrit to patients with cancer will no longer be required to enroll and become certified to dispense Epogen/Procrit.

While the REMS is no longer necessary to ensure the benefits outweigh the risks, the serious risks of shortened overall survival and/or increased risk of tumor progression or recurrence associated with Epogen/Procrit remains a concern. The prescribing information continues to note an increased risk of tumor progression or recurrence, as well as death, myocardial infarction, stroke, venous thromboembolism, and thrombosis of vascular access.

Prescribing Information and Regulatory History from Drugs@FDA

 
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