Quantitative Differences in the Urinary Proteome of Siblings Discordant for Type 1 Diabetes Include Lysosomal Enzymes

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• 作者：Moo-Jin Suh ; Andrey Tovchigrechko ; Vishal Thovarai ; Melanie A. Rolfe ; Manolito G. Torralba ; Junmin Wang ; Joshua N. Adkins ; Bobbie-Jo M. Webb-Robertson ; Whitney Osborne ; Fran R. Cogen ; Paul B. Kaplowitz ; Thomas O. Metz ; Karen E. Nelson ; Ramana Madupu ; Rembert Pieper
• 刊名：Journal of Proteome Research
• 出版年：2015
• 出版时间：August 7, 2015
• 年：2015
• 卷：14
• 期：8
• 页码：3123-3135
• 全文大小：441K
• ISSN：1535-3907

文摘

Individuals with type 1 diabetes (T1D) often have higher than normal blood glucose levels, causing advanced glycation end product formation and inflammation and increasing the risk of vascular complications years or decades later. To examine the urinary proteome in juveniles with T1D for signatures indicative of inflammatory consequences of hyperglycemia, we profiled the proteome of 40 T1D patients with an average of 6.3 years after disease onset and normal or elevated HbA_1C levels, in comparison with a cohort of 41 healthy siblings. Using shotgun proteomics, 1036 proteins were identified, on average, per experiment, and 50 proteins showed significant abundance differences using a Wilcoxon signed-rank test (FDR q-value 鈮?0.05). Thirteen lysosomal proteins were increased in abundance in the T1D versus control cohort. Fifteen proteins with functional roles in vascular permeability and adhesion were quantitatively changed, including CD166 antigen and angiotensin-converting enzyme 2. 伪-N-Acetyl-galactosaminidase and 伪-fucosidase 2, two differentially abundant lysosomal enzymes, were detected in western blots with often elevated quantities in the T1D versus control cohort. Increased release of proteins derived from lysosomes and vascular epithelium into urine may result from hyperglycemia-associated inflammation in the kidney vasculature.