Comparison of methodologies to define hemodialysis patients hyporesponsive to epoetin and impact on counts and characteristics

David T. Gilbertson; Yi Peng; Thomas J. Arneson; Stephan Dunning; Allan J. Collins

doi:10.1186/1471-2369-14-44

Comparison of methodologies to define hemodialysis patients hyporesponsive to epoetin and impact on counts and characteristics

David T. Gilbertson, Yi Peng, Thomas J. Arneson, Stephan Dunning, Allan J. Collins

Medicine - Renal and Hypertension Division

Research output: Contribution to journal › Article › peer-review

22 Scopus citations

Abstract

Background: Some hemodialysis patients require large doses of erythropoiesis-stimulating agents (ESAs) to manage anemia. These patients, termed "ESA hyporesponsive," have been characterized using various definitions. We applied three definitions of hyporesponsiveness to a large, national cohort of hemodialysis patients to assess the impact of definition on counts and on characteristics associated with hyporesponsiveness. Methods. We studied point-prevalent hemodialysis patients on May 1, 2008, with Medicare as primary payer, who survived through December 31, 2008. Included patients received recombinant human erythropoietin (EPO) in each month, August-December. Hyporesponsiveness definitions were: above the ninetieth percentile of total monthly EPO dose; above the ninetieth percentile of total monthly EPO dose divided by weight in kg; above the ninetieth percentile of total monthly EPO dose divided by hemoglobin level. Hyporesponsiveness was further classified as chronic, acute, or other. Comorbid conditions were assessed before and concurrent with the hyporesponsive period. Results: Women, African Americans, and patients aged <40 years, with cause of renal failure other than diabetes or hypertension, or longer dialysis duration, were more likely to be hyporesponsive. Antecedent comorbid conditions most predictive of any subsequent hyporesponsiveness were congestive heart failure, peripheral vascular disease, other cardiac disease, gastrointestinal bleeding, and cancer. Concurrent comorbid conditions most strongly associated with any hyporesponsiveness were gastrointestinal bleeding and cancer. All conditions were somewhat more likely when ascertained concurrently. Comorbidity burdens were lowest for non-hyporesponsive patients. Conclusions: As associations were similar between patient characteristics and three methods of characterizing EPO hyporesponsiveness, the simplest definition using EPO dose can be used.

Original language	English (US)
Article number	44
Journal	BMC Nephrology
Volume	14
Issue number	1
DOIs	https://doi.org/10.1186/1471-2369-14-44
State	Published - 2013

Bibliographical note

Funding Information:
This study was supported by a research contract from Takeda Pharmaceuticals International, Inc., Deerfield, Illinois. The contract provides for the authors to have final determination of manuscript content. Yi Peng has no conflicts of interest. Dr. Gilbertson has provided consultation to Amgen, DaVita Clinical Research, and Affymax. Dr. Arneson has an ownership interest in Johnson & Johnson. Stephan Dunning has provided consultation to Amgen. Dr. Collins has provided consultation to Merck, Amgen, Takeda, and NxStage.

Keywords

Epidemiology
Epoetin
Hemodialysis

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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title = "Comparison of methodologies to define hemodialysis patients hyporesponsive to epoetin and impact on counts and characteristics",

abstract = "Background: Some hemodialysis patients require large doses of erythropoiesis-stimulating agents (ESAs) to manage anemia. These patients, termed {"}ESA hyporesponsive,{"} have been characterized using various definitions. We applied three definitions of hyporesponsiveness to a large, national cohort of hemodialysis patients to assess the impact of definition on counts and on characteristics associated with hyporesponsiveness. Methods. We studied point-prevalent hemodialysis patients on May 1, 2008, with Medicare as primary payer, who survived through December 31, 2008. Included patients received recombinant human erythropoietin (EPO) in each month, August-December. Hyporesponsiveness definitions were: above the ninetieth percentile of total monthly EPO dose; above the ninetieth percentile of total monthly EPO dose divided by weight in kg; above the ninetieth percentile of total monthly EPO dose divided by hemoglobin level. Hyporesponsiveness was further classified as chronic, acute, or other. Comorbid conditions were assessed before and concurrent with the hyporesponsive period. Results: Women, African Americans, and patients aged <40 years, with cause of renal failure other than diabetes or hypertension, or longer dialysis duration, were more likely to be hyporesponsive. Antecedent comorbid conditions most predictive of any subsequent hyporesponsiveness were congestive heart failure, peripheral vascular disease, other cardiac disease, gastrointestinal bleeding, and cancer. Concurrent comorbid conditions most strongly associated with any hyporesponsiveness were gastrointestinal bleeding and cancer. All conditions were somewhat more likely when ascertained concurrently. Comorbidity burdens were lowest for non-hyporesponsive patients. Conclusions: As associations were similar between patient characteristics and three methods of characterizing EPO hyporesponsiveness, the simplest definition using EPO dose can be used.",

keywords = "Epidemiology, Epoetin, Hemodialysis",

author = "Gilbertson, {David T.} and Yi Peng and Arneson, {Thomas J.} and Stephan Dunning and Collins, {Allan J.}",

note = "Funding Information: This study was supported by a research contract from Takeda Pharmaceuticals International, Inc., Deerfield, Illinois. The contract provides for the authors to have final determination of manuscript content. Yi Peng has no conflicts of interest. Dr. Gilbertson has provided consultation to Amgen, DaVita Clinical Research, and Affymax. Dr. Arneson has an ownership interest in Johnson & Johnson. Stephan Dunning has provided consultation to Amgen. Dr. Collins has provided consultation to Merck, Amgen, Takeda, and NxStage.",

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AU - Gilbertson, David T.

AU - Peng, Yi

AU - Arneson, Thomas J.

AU - Dunning, Stephan

AU - Collins, Allan J.

N1 - Funding Information: This study was supported by a research contract from Takeda Pharmaceuticals International, Inc., Deerfield, Illinois. The contract provides for the authors to have final determination of manuscript content. Yi Peng has no conflicts of interest. Dr. Gilbertson has provided consultation to Amgen, DaVita Clinical Research, and Affymax. Dr. Arneson has an ownership interest in Johnson & Johnson. Stephan Dunning has provided consultation to Amgen. Dr. Collins has provided consultation to Merck, Amgen, Takeda, and NxStage.

PY - 2013

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N2 - Background: Some hemodialysis patients require large doses of erythropoiesis-stimulating agents (ESAs) to manage anemia. These patients, termed "ESA hyporesponsive," have been characterized using various definitions. We applied three definitions of hyporesponsiveness to a large, national cohort of hemodialysis patients to assess the impact of definition on counts and on characteristics associated with hyporesponsiveness. Methods. We studied point-prevalent hemodialysis patients on May 1, 2008, with Medicare as primary payer, who survived through December 31, 2008. Included patients received recombinant human erythropoietin (EPO) in each month, August-December. Hyporesponsiveness definitions were: above the ninetieth percentile of total monthly EPO dose; above the ninetieth percentile of total monthly EPO dose divided by weight in kg; above the ninetieth percentile of total monthly EPO dose divided by hemoglobin level. Hyporesponsiveness was further classified as chronic, acute, or other. Comorbid conditions were assessed before and concurrent with the hyporesponsive period. Results: Women, African Americans, and patients aged <40 years, with cause of renal failure other than diabetes or hypertension, or longer dialysis duration, were more likely to be hyporesponsive. Antecedent comorbid conditions most predictive of any subsequent hyporesponsiveness were congestive heart failure, peripheral vascular disease, other cardiac disease, gastrointestinal bleeding, and cancer. Concurrent comorbid conditions most strongly associated with any hyporesponsiveness were gastrointestinal bleeding and cancer. All conditions were somewhat more likely when ascertained concurrently. Comorbidity burdens were lowest for non-hyporesponsive patients. Conclusions: As associations were similar between patient characteristics and three methods of characterizing EPO hyporesponsiveness, the simplest definition using EPO dose can be used.

AB - Background: Some hemodialysis patients require large doses of erythropoiesis-stimulating agents (ESAs) to manage anemia. These patients, termed "ESA hyporesponsive," have been characterized using various definitions. We applied three definitions of hyporesponsiveness to a large, national cohort of hemodialysis patients to assess the impact of definition on counts and on characteristics associated with hyporesponsiveness. Methods. We studied point-prevalent hemodialysis patients on May 1, 2008, with Medicare as primary payer, who survived through December 31, 2008. Included patients received recombinant human erythropoietin (EPO) in each month, August-December. Hyporesponsiveness definitions were: above the ninetieth percentile of total monthly EPO dose; above the ninetieth percentile of total monthly EPO dose divided by weight in kg; above the ninetieth percentile of total monthly EPO dose divided by hemoglobin level. Hyporesponsiveness was further classified as chronic, acute, or other. Comorbid conditions were assessed before and concurrent with the hyporesponsive period. Results: Women, African Americans, and patients aged <40 years, with cause of renal failure other than diabetes or hypertension, or longer dialysis duration, were more likely to be hyporesponsive. Antecedent comorbid conditions most predictive of any subsequent hyporesponsiveness were congestive heart failure, peripheral vascular disease, other cardiac disease, gastrointestinal bleeding, and cancer. Concurrent comorbid conditions most strongly associated with any hyporesponsiveness were gastrointestinal bleeding and cancer. All conditions were somewhat more likely when ascertained concurrently. Comorbidity burdens were lowest for non-hyporesponsive patients. Conclusions: As associations were similar between patient characteristics and three methods of characterizing EPO hyporesponsiveness, the simplest definition using EPO dose can be used.

KW - Epidemiology

KW - Epoetin

KW - Hemodialysis

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Comparison of methodologies to define hemodialysis patients hyporesponsive to epoetin and impact on counts and characteristics

Abstract

Bibliographical note

Keywords

UN SDGs

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