TY - JOUR
T1 - The First 2 Years of Biosimilar Epoetin for Cancer and Chemotherapy-Induced Anemia in the U.S.
T2 - A Review from the Southern Network on Adverse Reactions
AU - Bennett, Charles L.
AU - Nagai, Sumimasa
AU - Bennett, Andrew C.
AU - Hoque, Shamia
AU - Nabhan, Chadi
AU - Schoen, Martin W.
AU - Hrushesky, William J.
AU - Luminari, Stefano
AU - Ray, Paul
AU - Yarnold, Paul R.
AU - Witherspoon, Bart
AU - Riente, Josh
AU - Bobolts, Laura
AU - Brusk, John
AU - Tombleson, Rebecca
AU - Knopf, Kevin
AU - Fishman, Marc
AU - Yang, Y. Tony
AU - Carson, Kenneth R.
AU - Djulbegovic, Benjamin
AU - Restaino, John
AU - Armitage, James O.
AU - Sartor, Oliver A.
N1 - Funding Information:
Robert C. Kane, M.D., the 2016 recipient of the Food and Drug Administration's Frances Kelsey Award for Pharmaceutical Safety Efforts, died after the submission of the first draft of this manuscript. The article is submitted in his honor. This study was funded partly by the National Institutes of Health (grant R01CA16509), the American Cancer Society (IRG‐13‐043‐01), the South Carolina SmartState Program, and Oncology Analytics, Inc. No funds were accepted from a pharmaceutical manufacturer or a pharmaceutical distributor. The views expressed represent independent work of the authors and should not be considered to represent the views or policy of any other entity or agency. Parts of this study were presented at the Asia Oncology Summit in Kyoto, Japan, March 3–7, 2016 (travel fees were supported by ), and at the American Society of Hematology conference in San Diego, California, December 1–4, 2018, and at Hematology/Oncology Grand Rounds at the George Washington Medical Center in Washington DC on July 31, 2020. Lancet Oncology
Funding Information:
Robert C. Kane, M.D., the 2016 recipient of the Food and Drug Administration's Frances Kelsey Award for Pharmaceutical Safety Efforts, died after the submission of the first draft of this manuscript. The article is submitted in his honor. This study was funded partly by the National Institutes of Health (grant R01CA16509), the American Cancer Society (IRG-13-043-01), the South Carolina SmartState Program, and Oncology Analytics, Inc. No funds were accepted from a pharmaceutical manufacturer or a pharmaceutical distributor. The views expressed represent independent work of the authors and should not be considered to represent the views or policy of any other entity or agency. Parts of this study were presented at the Asia Oncology Summit in Kyoto, Japan, March 3–7, 2016 (travel fees were supported by Lancet Oncology), and at the American Society of Hematology conference in San Diego, California, December 1–4, 2018, and at Hematology/Oncology Grand Rounds at the George Washington Medical Center in Washington DC on July 31, 2020.
Publisher Copyright:
© 2021 AlphaMed Press.
PY - 2021/8
Y1 - 2021/8
N2 - Biosimilars are biologic drug products that are highly similar to reference products in analytic features, pharmacokinetics and pharmacodynamics, immunogenicity, safety, and efficacy. Biosimilar epoetin received Food and Drug Administration (FDA) approval in 2018. The manufacturer received an FDA nonapproval letter in 2017, despite receiving a favorable review by FDA's Oncologic Drugs Advisory Committee (ODAC) and an FDA nonapproval letter in 2015 for an earlier formulation. We discuss the 2018 FDA approval, the 2017 FDA ODAC Committee review, and the FDA complete response letters in 2015 and 2017; review concepts of litigation, naming, labeling, substitution, interchangeability, and pharmacovigilance; review European and U.S. oncology experiences with biosimilar epoetin; and review the safety of erythropoiesis-stimulating agents. In 2020, policy statements from AETNA, United Health Care, and Humana indicated that new epoetin oncology starts must be for biosimilar epoetin unless medical need for other epoetins is documented. Empirical studies report that as of 2012, reference epoetin use decreased from 40%–60% of all patients with cancer with chemotherapy-induced anemia to <5% of such patients because of safety concerns. Between 2018 and 2020, biosimilar epoetin use varied, increasing to 81% among one private insurer's patients covered by Medicare whose cancer care is administered with Oncology Analytics and to 41% with the same private insurer's patients with cancer covered by commercial health insurance and administered by the private insurer, to 0% in several Veterans Administration Hospitals, increasing to 100% in one large county hospital in California, and with yet-to-be-reported data from most oncology settings. We conclude that biosimilar epoetin appears to have overcome some barriers since 2015, although current uptake in the U.S. is variable. Pricing and safety considerations for all erythropoiesis-stimulating agents are primary determinants of biosimilar epoetin oncology uptake. Implications for Practice: Few oncologists understand substitution and interchangeability of biosimilars with reference drugs. Epoetin biosimilar is new to the market, and physician and patient understanding is limited. The development of epoetin biosimilar is not familiar to oncologists.
AB - Biosimilars are biologic drug products that are highly similar to reference products in analytic features, pharmacokinetics and pharmacodynamics, immunogenicity, safety, and efficacy. Biosimilar epoetin received Food and Drug Administration (FDA) approval in 2018. The manufacturer received an FDA nonapproval letter in 2017, despite receiving a favorable review by FDA's Oncologic Drugs Advisory Committee (ODAC) and an FDA nonapproval letter in 2015 for an earlier formulation. We discuss the 2018 FDA approval, the 2017 FDA ODAC Committee review, and the FDA complete response letters in 2015 and 2017; review concepts of litigation, naming, labeling, substitution, interchangeability, and pharmacovigilance; review European and U.S. oncology experiences with biosimilar epoetin; and review the safety of erythropoiesis-stimulating agents. In 2020, policy statements from AETNA, United Health Care, and Humana indicated that new epoetin oncology starts must be for biosimilar epoetin unless medical need for other epoetins is documented. Empirical studies report that as of 2012, reference epoetin use decreased from 40%–60% of all patients with cancer with chemotherapy-induced anemia to <5% of such patients because of safety concerns. Between 2018 and 2020, biosimilar epoetin use varied, increasing to 81% among one private insurer's patients covered by Medicare whose cancer care is administered with Oncology Analytics and to 41% with the same private insurer's patients with cancer covered by commercial health insurance and administered by the private insurer, to 0% in several Veterans Administration Hospitals, increasing to 100% in one large county hospital in California, and with yet-to-be-reported data from most oncology settings. We conclude that biosimilar epoetin appears to have overcome some barriers since 2015, although current uptake in the U.S. is variable. Pricing and safety considerations for all erythropoiesis-stimulating agents are primary determinants of biosimilar epoetin oncology uptake. Implications for Practice: Few oncologists understand substitution and interchangeability of biosimilars with reference drugs. Epoetin biosimilar is new to the market, and physician and patient understanding is limited. The development of epoetin biosimilar is not familiar to oncologists.
KW - Epoetin Biosimilars Interchangeable Substitution Guidelines
UR - http://www.scopus.com/inward/record.url?scp=85102719400&partnerID=8YFLogxK
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U2 - 10.1002/onco.13713
DO - 10.1002/onco.13713
M3 - Article
C2 - 33586299
AN - SCOPUS:85102719400
SN - 1083-7159
VL - 26
SP - e1418-e1426
JO - Oncologist
JF - Oncologist
IS - 8
ER -
