Literature DB >> 30802485

Harmonization of immunoassays for biomarkers in diabetes mellitus.

Sebastian Hörber1, Peter Achenbach2, Erwin Schleicher3, Andreas Peter1.   

Abstract

Harmonization of biomarkers is important for the comparability of laboratory results as it allows the definition of universal reference values and clinical decision limits. In diabetology, immunoassays are widely used to determine HbA1c, C-peptide, insulin, and autoantibodies to beta cell proteins, which are essential biomarkers for the diagnosis and classification of diabetes mellitus. Furthermore, as large clinical studies have identified HbA1c as a predictor for the development of diabetic complications, HbA1c has evolved as the general treatment target. For decades, the use of non-harmonized assays caused confusion. After the standardization of HbA1c, the worldwide comparability improved and increased the confidence in this laboratory biomarker. Insulin and C-peptide are not only valuable biomarkers to assess beta-cell function, but may also be used to evaluate insulin resistance, a metabolic feature of type 2 diabetes often occurring before its manifestation. Long-lasting efforts led to substantial improvements in the harmonization process of C-peptide assays, but harmonization of insulin assays is still ongoing. Therefore, C-peptide is now sometimes used as a surrogate biomarker for insulin. Furthermore, autoantibodies against beta cell components are important biomarkers for the accurate differentiation of type 1, type 2, and other special types of diabetes. Owing to the heterogeneity of these autoantibodies against beta cell proteins, harmonization is very difficult to achieve. International efforts are in progress to harmonize the current assays, as the presence of autoantibodies against beta cell proteins predicts the development of type 1 diabetes in early life. In conclusion, clinical studies linking diagnosis, classification, prediction, and treatment to laboratory values of the respective biomarkers need to be harmonized to avoid misdiagnosis and incorrect clinical decisions, thus improving patient care and safety.
Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Autoantibodies; Biomarker; C-peptide; Classification; Diabetes mellitus; Glycated hemoglobin; Harmonization; Immunoassay; Insulin; Prediction; Standardization

Year:  2019        PMID: 30802485     DOI: 10.1016/j.biotechadv.2019.02.015

Source DB:  PubMed          Journal:  Biotechnol Adv        ISSN: 0734-9750            Impact factor:   14.227


  5 in total

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Authors:  Sapna Bhoria; Jyoti Yadav; Honey Yadav; Darshna Chaudhary; Ranjana Jaiwal; Pawan K Jaiwal
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2.  Measurement comparability of insulin assays using conventional immunoassay kits.

Authors:  Nordiana Rosli; Ha-Jeong Kwon; Jinsook Lim; Young Ahn Yoon; Ji-Seon Jeong
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4.  Increase in glycemic set point, alongside a decrease in waist circumference, in the non-diabetic population during the Japanese National Intervention Program for metabolic syndrome: A single-center, large-scale, matched-pair analysis.

Authors:  Takuya Sugiyama; Yuya Yamada; Yoshito Ito; Ryohei Mineo; Ryuya Iwamoto; Sachiko Tamba; Takashi Fujimoto; Koji Yamamoto; Yuji Matsuzawa
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5.  Considering Insulin Secretory Capacity as Measured by a Fasting C-Peptide/Glucose Ratio in Selecting Glucose-Lowering Medications.

Authors:  Andreas Fritsche; Martin Heni; Andreas Peter; Baptist Gallwitz; Monika Kellerer; Andreas L Birkenfeld; Hans-Ulrich Häring; Robert Wagner
Journal:  Exp Clin Endocrinol Diabetes       Date:  2020-09-18       Impact factor: 2.949

  5 in total

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