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A specific and sensitive assay for blood levels of glycated CD59: A novel biomarker for diabetes
Authors:Pamela Ghosh  Rupam Sahoo  Anand Vaidya  Sonia Cantel  Amol Kavishwar  Allison Goldfine  Neil Herring  Lynn Bry  Michael Chorev  Jose A. Halperin
Affiliation:1. Division of Hematology, Department of Medicine, Brigham and Women's Hospital, Harvard Medical School, , Boston, Massachusetts;2. Division of Endocrinology, Diabetes and Hypertension, Brigham and Women's Hospital, Harvard Medical School, , Boston, Massachusetts;3. Joslin Diabetes Center, Harvard Medical School, , Boston, Massachusetts;4. Crimson Biospecimen Core, Partners Healthcare System, , Boston, Massachusetts
Abstract:
Increasing evidence links the complement system with complications of human diabetes. The complement regulatory protein CD59, an inhibitor of formation of membrane attack complex (MAC), is inhibited by hyperglycemia‐induced glycation fostering increased deposition of MAC, a major effector of complement‐mediated tissue damage. CD59, an ubiquitous GPI‐anchored membrane protein, is shed from cell membranes by phospholipases generating a soluble form present in blood and urine. We established an enzyme‐linked immunosorbent assay (ELISA) to measure serum/plasma glycated human CD59 (hCD59) (GCD59) and evaluated its potential as a diabetes biomarker. We used a synthetic peptide strategy to generate (a) a mouse monoclonal antibody to capture hCD59, (b) a rabbit monoclonal antibody to detect GCD59, and (c) a GCD59 surrogate for assay standardization. ELISA conditions were optimized for precision, reproducibility, and clinical sensitivity. The clinical utility of the assay was initially evaluated in 24 subjects with or without diabetes and further validated in a study that included 100 subjects with and 90 subjects without a diagnosis of diabetes. GCD59 (a) was significantly higher in individuals with than in individual without diabetes, (b) was independently associated with HbA1c, and (c) identified individuals with diabetes with high specificity and sensitivity. We report the development and standardization of a novel, sensitive, and specific ELISA for measuring GCD59 in blood. The assay distinguished individuals with diabetes from those without, and showed strong correlation between GCD59 and HbA1c. Because GCD59 likely contributes to the pathogenesis of diabetes complications, measurement of blood levels of GCD59 may be useful in the diagnosis and management of diabetes. Am. J. Hematol. 88:670–676, 2013. © 2013 Wiley Periodicals, Inc.
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