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DOI: 10.1055/s-2003-44710
J. A. Barth Verlag in Georg Thieme Verlag Stuttgart · New York
Effect of α-Ketobutyrate on Microvascular Thickness in the Diabetic Rat Kidney
Publication History
Received: September 4, 2002
First decision: November 24, 2002
Accepted: April 22, 2003
Publication Date:
09 January 2004 (online)
Abstract
The first objective of this study was to examine the intermediary metabolism of plasma amino acids and keto acids in streptozotocin (STZ)-treated rats. Plasma α-aminobutyrate (α-ABA) concentration in STZ rats was 1.5-fold greater than in control (CNT) animals at 1 month. In contrast, the level of plasma α-ketobutyrate (KB), which is transaminated to α-ABA, did not differ significantly between STZ and CNTs at 1 month, and also increased with age. Additionally, HPLC analysis revealed consistent profiles containing peaks of unknown origin. Two pathways exist for the formation of α-KB, either from the action of threonine dehydratase or via homocysteine, the latter metabolite being closely associated with the development of cardiovascular disease. These observations suggest that uncharacterized metabolites, including plasma α-KB, may be potential risk factors for the development of diabetic complications. We carried out preparatory experiments on non-diabetic rats to investigate the influence of α-KB and confirmed this metabolite had no adverse effects. The second aim of the study was to compare vascular wall thickness in diabetic rats treated or untreated with α-KB with CNT animals in order to determine the effects of α-KB on the renal microvasculature. The thickness of the medial wall of arterioles and small arteries differed significantly among all groups and was increased, especially in the small arterial walls of the diabetic rats treated with α-KB. Plasma renin activities (PRA) in both diabetic rats treated or untreated with α-KB were decreased significantly compared to CNT animals, while diabetic rats treated with α-KB had higher angiotensin converting enzyme (ACE) activity than the CNT group (p < 0.01). These results suggest that α-KB may have a role in the renal microvascular complications of diabetes.
Key words
α-ketobutyrate (KB) - diabetes mellitus - medial thickness - arteriole - angiotensin converting enzyme (ACE) activity
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Rei Hirota PhD.
Department of Biochemistry
Nihon University School of Medicine
Itabashi
Tokyo
173-8610, Japan
Phone: + 81339728111, ex. -2243
Fax: + 81 3 39 72 00 27
Email: rhirota@med.nihon-u.ac.jp