Immunochemical Assay of Hemoglobin with Nε-(Carboxymethyl)lysine at Lysine 66 of the β Chain

Background: N ε-(Carboxymethyl)lysine (CML), a well-characterized and major advanced glycation end product structure, is produced via a Maillard reaction by nonenzymatic glycation and/or oxidation. Although few of the carboxymethylation sites of lysine residues on proteins have been identified, it i...

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Published in	Clinical chemistry (Baltimore, Md.) Vol. 47; no. 7; pp. 1249 - 1255
Main Authors	Iwamoto, Hisahiko, Motomiya, Yoshihiro, Miura, Keisuke, Morisawa, Masayo, Yoshimura, Yoshimichi, Maruyama, Ikuro
Format	Journal Article
Language	English
Published	01.07.2001
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Abstract	Background: N ε-(Carboxymethyl)lysine (CML), a well-characterized and major advanced glycation end product structure, is produced via a Maillard reaction by nonenzymatic glycation and/or oxidation. Although few of the carboxymethylation sites of lysine residues on proteins have been identified, it is known that the possible lysine glycation site in hemoglobin (Hb) is Lys-66 on the β chain. We aimed to develop an assay for the Hb with a CML (CML-Hb) site specific to Lys-66 on the Hb β chain and to determine whether the lysine residue at that site is carboxymethylated. Methods: Ala-His-Gly-Lys-Lys(CM)-Val-Leu-Gly-Ala-Phe-Ser-Cys, the peptide derived from the β chain of human Hb, was synthesized as an immunogen, and a monoclonal antibody against the peptide was prepared. A latex immunoassay method was established using the antibody on an automatic analyzer. In this study, 20 samples from healthy subjects and 80 samples from nondiabetic patients undergoing hemodialysis (HD) were analyzed. Results: The latex immunoassay method using the antibody correlated significantly with the ELISA method using the antibody (r = 0.95; P <0.001). Between healthy subjects (n = 20) and nondiabetic HD patients (n = 80), a significant difference was seen in circulating CML-Hb (525 ± 76 vs 778 ± 137 pmol CML/mg of Hb; P <0.0001). Conclusion: The latex method for the CML-Hb site specific to Lys-66 on the β chain can measure large numbers of samples on an automatic analyzer.
AbstractList	Background: N ε-(Carboxymethyl)lysine (CML), a well-characterized and major advanced glycation end product structure, is produced via a Maillard reaction by nonenzymatic glycation and/or oxidation. Although few of the carboxymethylation sites of lysine residues on proteins have been identified, it is known that the possible lysine glycation site in hemoglobin (Hb) is Lys-66 on the β chain. We aimed to develop an assay for the Hb with a CML (CML-Hb) site specific to Lys-66 on the Hb β chain and to determine whether the lysine residue at that site is carboxymethylated. Methods: Ala-His-Gly-Lys-Lys(CM)-Val-Leu-Gly-Ala-Phe-Ser-Cys, the peptide derived from the β chain of human Hb, was synthesized as an immunogen, and a monoclonal antibody against the peptide was prepared. A latex immunoassay method was established using the antibody on an automatic analyzer. In this study, 20 samples from healthy subjects and 80 samples from nondiabetic patients undergoing hemodialysis (HD) were analyzed. Results: The latex immunoassay method using the antibody correlated significantly with the ELISA method using the antibody (r = 0.95; P <0.001). Between healthy subjects (n = 20) and nondiabetic HD patients (n = 80), a significant difference was seen in circulating CML-Hb (525 ± 76 vs 778 ± 137 pmol CML/mg of Hb; P <0.0001). Conclusion: The latex method for the CML-Hb site specific to Lys-66 on the β chain can measure large numbers of samples on an automatic analyzer.
Author	Morisawa, Masayo Yoshimura, Yoshimichi Miura, Keisuke Iwamoto, Hisahiko Maruyama, Ikuro Motomiya, Yoshihiro
Author_xml	– sequence: 1 givenname: Hisahiko surname: Iwamoto fullname: Iwamoto, Hisahiko organization: R&D for Diagnostics, A&T Corporation, 2023-1, Endo, Fujisawa-City, Kanagawa 252-0816, Japan – sequence: 2 givenname: Yoshihiro surname: Motomiya fullname: Motomiya, Yoshihiro organization: Suiyukai Clinic, 676-1, Kuzumoto-chou, Kashihara-City, Nara 634-0007, Japan – sequence: 3 givenname: Keisuke surname: Miura fullname: Miura, Keisuke organization: R&D for Diagnostics, A&T Corporation, 2023-1, Endo, Fujisawa-City, Kanagawa 252-0816, Japan – sequence: 4 givenname: Masayo surname: Morisawa fullname: Morisawa, Masayo organization: Suiyukai Clinic, 676-1, Kuzumoto-chou, Kashihara-City, Nara 634-0007, Japan – sequence: 5 givenname: Yoshimichi surname: Yoshimura fullname: Yoshimura, Yoshimichi organization: R&D for Diagnostics, A&T Corporation, 2023-1, Endo, Fujisawa-City, Kanagawa 252-0816, Japan – sequence: 6 givenname: Ikuro surname: Maruyama fullname: Maruyama, Ikuro organization: Department of Laboratory Medicine, Kagoshima University School of Medicine, Kagoshima 890-0075, Japan
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Title	Immunochemical Assay of Hemoglobin with Nε-(Carboxymethyl)lysine at Lysine 66 of the β Chain
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