Using a Targeted Proteomics Chip to Explore Pathophysiological Pathways for Incident Diabetes– The Malmö Preventive Project

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作者
John Molvin
Manan Pareek
Amra Jujic
Olle Melander
Lennart Råstam
Ulf Lindblad
Bledar Daka
Margrét Leósdóttir
Peter M. Nilsson
Michael H. Olsen
Martin Magnusson
机构
[1] Clinical Research Center,Department of Clinical Sciences, Lund University
[2] Skåne University Hospital Malmö,Department of Cardiology
[3] Holbæk Hospital,Cardiology Section, Department of Internal Medicine
[4] Harvard Medical School,Brigham and Women’s Hospital Heart & Vascular Center
[5] Skåne University Hospital,Department of Internal Medicine
[6] University of Gothenburg,Institute of Medicine, Department of Public Health and Community Medicine, Sahlgrenska Academy
[7] University of Southern Denmark,Centre for Individualized Medicine in Arterial Diseases (CIMA), Odense University Hospital
[8] Lund University,Wallenberg Center for Molecular Medicine
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Multiplex proteomic platforms provide excellent tools for investigating associations between multiple proteins and disease (e.g., diabetes) with possible prognostic, diagnostic, and therapeutic implications. In this study our aim was to explore novel pathophysiological pathways by examining 92 proteins and their association with incident diabetes in a population-based cohort (146 cases of diabetes versus 880 controls) followed over 8 years. After adjusting for traditional risk factors, we identified seven proteins associated with incident diabetes. Four proteins (Scavenger receptor cysteine rich type 1 protein M130, Fatty acid binding protein 4, Plasminogen activator inhibitor 1 and Insulin-like growth factor-binding protein 2) with a previously established association with incident diabetes and 3 proteins (Cathepsin D, Galectin-4, Paraoxonase type 3) with a novel association with incident diabetes. Galectin-4, with an increased risk of diabetes, and Paraoxonase type 3, with a decreased risk of diabetes, remained significantly associated with incident diabetes after adjusting for plasma glucose, implying a glucose independent association with diabetes.
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