Carnosine attenuates the development of both type 2 diabetes and diabetic nephropathy in BTBR ob/ob mice

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Veröffentlicht in:	Scientific reports 7(2017) Artikel-Nummer 44492, 16 Seiten
Personen und Körperschaften:	Albrecht, Thomas (VerfasserIn), Zhang, Shiqi (VerfasserIn), Braun, Jana D. (VerfasserIn), Qiu, Jiedong (VerfasserIn), Rodriguez-Niño, Angelica (VerfasserIn), Pastene, Diego O. (VerfasserIn), Krämer, Bernhard (VerfasserIn), Köppel, Hannes (VerfasserIn), Yard, Benito A. (VerfasserIn), Hauske, Sibylle J. (VerfasserIn)
Titel:	Carnosine attenuates the development of both type 2 diabetes and diabetic nephropathy in BTBR ob/ob mice/ Thomas Albrecht, Maaike Schilperoort, Shiqi Zhang, Jana D. Braun, Jiedong Qiu, Angelica Rodriguez, Diego O. Pastene, Bernhard K. Krämer, Hannes Köppel, Hans Baelde, Emile de Heer, Alessandra Anna Altomare, Luca Regazzoni, Alessandra Denisi, Giancarlo Aldini, Jacob van den Born, Benito A. Yard & Sibylle J. Hauske
Format:	E-Book-Kapitel
Sprache:	Englisch
veröffentlicht:	10 March 2017
Gesamtaufnahme:	: Scientific reports, 7(2017) Artikel-Nummer 44492, 16 Seiten , volume:7
Quelle:	Verbunddaten SWB Lizenzfreie Online-Ressourcen

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Zusammenfassung:	We previously demonstrated that polymorphisms in the carnosinase-1 gene (CNDP1) determine the risk of nephropathy in type 2 diabetic patients. Carnosine, the substrate of the enzyme encoded by this gene, is considered renoprotective and could possibly be used to treat diabetic nephropathy (DN). In this study, we examined the effect of carnosine treatment in vivo in BTBR (Black and Tan, BRachyuric) ob/ob mice, a type 2 diabetes model which develops a phenotype that closely resembles advanced human DN. Treatment of BTBR ob/ob mice with 4 mM carnosine for 18 weeks reduced plasma glucose and HbA1c, concomitant with elevated insulin and C-peptide levels. Also, albuminuria and kidney weights were reduced in carnosine-treated mice, which showed less glomerular hypertrophy due to a decrease in the surface area of Bowman's capsule and space. Carnosine treatment restored the glomerular ultrastructure without affecting podocyte number, resulted in a modified molecular composition of the expanded mesangial matrix and led to the formation of carnosine-acrolein adducts. Our results demonstrate that treatment with carnosine improves glucose metabolism, albuminuria and pathology in BTBR ob/ob mice. Hence, carnosine could be a novel therapeutic strategy to treat patients with DN and/or be used to prevent DN in patients with diabetes.
Beschreibung:	Gesehen am 17.04.2018
Umfang:	16
ISSN:	2045-2322
DOI:	10.1038/srep44492