Article

Reactive oxygen species in the presence of high glucose alter ureteric bud morphogenesis.

University of Montreal, Centre hospitalier de l'Université de Montréal-Hôtel-Dieu, Pavillon Masson, Montreal, Quebec, Canada.
Journal of the American Society of Nephrology (impact factor: 9.66). 08/2007; 18(7):2105-15. DOI:10.1681/ASN.2006101124 pp.2105-15
Source: PubMed

ABSTRACT Renal malformations are a major cause of childhood renal failure. During the development of the kidney, ureteric bud (UB) branching morphogenesis is critical for normal nephrogenesis. These studies investigated whether renal UB branching morphogenesis is altered by a high ambient glucose environment and studied underlying mechanism(s). Kidney explants that were isolated from different periods of gestation (embryonic days 12 to 18) from Hoxb7-green fluorescence protein mice were cultured for 24 h in either normal d-glucose (5 mM) or high d-glucose (25 mM) medium with or without various inhibitors. Alterations in renal morphogenesis were assessed by fluorescence microscopy. Paired-homeobox 2 (Pax-2) gene expression was determined by real-time quantitative PCR, Western blotting, and immunohistology. The results revealed that high d-glucose (25 mM) specifically stimulates UB branching morphogenesis via Pax-2 gene expression, whereas other glucose analogs, such as d-mannitol, l-glucose, and 2-deoxy-d-glucose, had no effect. The stimulatory effect of high glucose on UB branching was blocked in the presence of catalase and inhibitors of NADPH oxidase, mitochondrial electron transport chain complex I, and Akt signaling. Moreover, in in vivo studies, it seems that high glucose induces, via Pax-2 (mainly localized in UB), acceleration of UB branching but not nephron formation. Taken together, these data demonstrate that high glucose alters UB branching morphogenesis. This occurs, at least in part, via reactive oxygen species generation, activation of Akt signaling, and upregulation of Pax-2 gene expression.

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Keywords

Akt signaling
 
ambient glucose environment
 
childhood renal failure
 
different periods
 
glucose alters UB branching morphogenesis
 
Hoxb7-green fluorescence protein mice
 
Kidney explants
 
mitochondrial electron transport chain complex
 
NADPH oxidase
 
normal d-glucose
 
normal nephrogenesis
 
Pax-2 gene expression
 
reactive oxygen species generation
 
real-time quantitative PCR
 
Renal malformations
 
renal UB branching morphogenesis
 
stimulatory effect
 
UB branching
 
ureteric bud
 
various inhibitors
 

Shao-Ling Zhang