Commercial assays for serum osteocalcin give clinically discordant results

Serum samples from 9 healthy controls and from subjects with primary hyperparathyroidism (n = 5), Paget disease (n = 3), pregnancy (n = 5), glucocorticoid therapy (n = 5), postmenopausal osteoporosis (n = 10), and renal failure (n = 10) were used to assess the clinical agreement among eight commerci...

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Published in	Clinical chemistry (Baltimore, Md.) Vol. 40; no. 3; pp. 358 - 363
Main Authors	Masters, PW, Jones, RG, Purves, DA, Cooper, EH, Cooney, JM
Format	Journal Article
Language	English
Published	Washington, DC Am Assoc Clin Chem 01.03.1994 American Association for Clinical Chemistry
Subjects	Adult Aged Analysis of complex biological substances Analytical, structural and metabolic biochemistry Biological and medical sciences Blood and biological fluids Female Fundamental and applied biological sciences. Psychology Glucocorticoids - therapeutic use Humans Hyperparathyroidism - blood Immunoradiometric Assay - standards Immunoradiometric Assay - statistics & numerical data Male Middle Aged Osteitis Deformans - blood Osteocalcin - blood Osteoporosis, Postmenopausal - blood Pregnancy Radioimmunoassay - standards Radioimmunoassay - statistics & numerical data Reagent Kits, Diagnostic - standards Reagent Kits, Diagnostic - statistics & numerical data Renal Insufficiency - blood Biological fluid Osteoporosis Serum Osteocalcin Analysis method
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Abstract	Serum samples from 9 healthy controls and from subjects with primary hyperparathyroidism (n = 5), Paget disease (n = 3), pregnancy (n = 5), glucocorticoid therapy (n = 5), postmenopausal osteoporosis (n = 10), and renal failure (n = 10) were used to assess the clinical agreement among eight commercially available assay kits for osteocalcin (OC). These kits differ in their assay configurations (six radioimmunoassays, two immunoradiometric assays), standards (five bovine, three human), and antibodies (six polyclonal, two monoclonal). Individual results were divided by the mean OC of the control subjects for each assay and expressed as percentage deviations. The expected wide variation in absolute OC concentrations between kits was only partially reduced by this transformation. Agreement was equally poor when absolute OC concentrations were compared with the reference ranges quoted by the manufacturers. The discordance was particularly marked in renal failure, presumably because of immunoreactive fragments, and in osteoporosis. Systematic differences could not be attributed to assay format, species source of standard, or antibody specificity. We conclude that results cannot be compared between assays even when normalized against healthy subjects, and that standardization is needed.
AbstractList	Serum samples from 9 healthy controls and from subjects with primary hyperparathyroidism (n = 5), Paget disease (n = 3), pregnancy (n = 5), glucocorticoid therapy (n = 5), postmenopausal osteoporosis (n = 10), and renal failure (n = 10) were used to assess the clinical agreement among eight commercially available assay kits for osteocalcin (OC). These kits differ in their assay configurations (six radioimmunoassays, two immunoradiometric assays), standards (five bovine, three human), and antibodies (six polyclonal, two monoclonal). Individual results were divided by the mean OC of the control subjects for each assay and expressed as percentage deviations. The expected wide variation in absolute OC concentrations between kits was only partially reduced by this transformation. Agreement was equally poor when absolute OC concentrations were compared with the reference ranges quoted by the manufacturers. The discordance was particularly marked in renal failure, presumably because of immunoreactive fragments, and in osteoporosis. Systematic differences could not be attributed to assay format, species source of standard, or antibody specificity. We conclude that results cannot be compared between assays even when normalized against healthy subjects, and that standardization is needed. Serum samples from 9 healthy controls and from subjects with primary hyperparathyroidism (n = 5), Paget disease (n = 3), pregnancy (n = 5), glucocorticoid therapy (n = 5), postmenopausal osteoporosis (n = 10), and renal failure (n = 10) were used to assess the clinical agreement among eight commercially available assay kits for osteocalcin (OC). These kits differ in their assay configurations (six radioimmunoassays, two immunoradiometric assays), standards (five bovine, three human), and antibodies (six polyclonal, two monoclonal). Individual results were divided by the mean OC of the control subjects for each assay and expressed as percentage deviations. The expected wide variation in absolute OC concentrations between kits was only partially reduced by this transformation. Agreement was equally poor when absolute OC concentrations were compared with the reference ranges quoted by the manufacturers. The discordance was particularly marked in renal failure, presumably because of immunoreactive fragments, and in osteoporosis. Systematic differences could not be attributed to assay format, species source of standard, or antibody specificity. We conclude that results cannot be compared between assays even when normalized against healthy subjects, and that standardization is needed.Serum samples from 9 healthy controls and from subjects with primary hyperparathyroidism (n = 5), Paget disease (n = 3), pregnancy (n = 5), glucocorticoid therapy (n = 5), postmenopausal osteoporosis (n = 10), and renal failure (n = 10) were used to assess the clinical agreement among eight commercially available assay kits for osteocalcin (OC). These kits differ in their assay configurations (six radioimmunoassays, two immunoradiometric assays), standards (five bovine, three human), and antibodies (six polyclonal, two monoclonal). Individual results were divided by the mean OC of the control subjects for each assay and expressed as percentage deviations. The expected wide variation in absolute OC concentrations between kits was only partially reduced by this transformation. Agreement was equally poor when absolute OC concentrations were compared with the reference ranges quoted by the manufacturers. The discordance was particularly marked in renal failure, presumably because of immunoreactive fragments, and in osteoporosis. Systematic differences could not be attributed to assay format, species source of standard, or antibody specificity. We conclude that results cannot be compared between assays even when normalized against healthy subjects, and that standardization is needed.
Author	Purves, DA Jones, RG Cooper, EH Cooney, JM Masters, PW
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SubjectTerms	Adult Aged Analysis of complex biological substances Analytical, structural and metabolic biochemistry Biological and medical sciences Blood and biological fluids Female Fundamental and applied biological sciences. Psychology Glucocorticoids - therapeutic use Humans Hyperparathyroidism - blood Immunoradiometric Assay - standards Immunoradiometric Assay - statistics & numerical data Male Middle Aged Osteitis Deformans - blood Osteocalcin - blood Osteoporosis, Postmenopausal - blood Pregnancy Radioimmunoassay - standards Radioimmunoassay - statistics & numerical data Reagent Kits, Diagnostic - standards Reagent Kits, Diagnostic - statistics & numerical data Renal Insufficiency - blood
Title	Commercial assays for serum osteocalcin give clinically discordant results
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