Increased glucose production in mice overexpressing human fructose-1,6-bisphosphatase in the liver

doi:10.1152/ajpendo.90552.2008

HOME

QUICK SEARCH:

	Author:		Keyword(s):
Year:		Vol:		Page:

Am J Physiol Endocrinol Metab 295: E1132-E1141, 2008. First published September 9, 2008; doi:10.1152/ajpendo.90552.2008
0193-1849/08 $8.00

This Article

	Full Text
	Full Text (PDF)
	All Versions of this Article: 295/5/E1132 most recent 90552.2008v1
	Alert me when this article is cited
	Alert me if a correction is posted
	Citation Map

Services

	Email this article to a friend
	Similar articles in this journal
	Similar articles in Web of Science
	Similar articles in PubMed
	Alert me to new issues of the journal
	Download to citation manager

Citing Articles

	Citing Articles via Google Scholar

Google Scholar

	Articles by Visinoni, S.
	Articles by Andrikopoulos, S.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Visinoni, S.
	Articles by Andrikopoulos, S.

Increased glucose production in mice overexpressing human fructose-1,6-bisphosphatase in the liver

Sherley Visinoni,¹ Barbara C. Fam,¹ Amy Blair,¹ Christian Rantzau,¹ Benjamin J. Lamont,¹ Russell Bouwman,¹ Matthew J. Watt,² Joseph Proietto,¹ Jenny M. Favaloro,¹^,* and Sofianos Andrikopoulos¹^,*

¹Department of Medicine, Austin Health and Northern Health, University of Melbourne, Heidelberg Heights; and ²Department of Physiology, Monash University, Clayton, Victoria, Australia

Submitted 30 June 2008 ; accepted in final form 2 September 2008

Increased endogenous glucose production (EGP) predominantlyfrom the liver is a characteristic feature of type 2 diabetes,which positively correlates with fasting hyperglycemia. Gluconeogenesisis the biochemical pathway shown to significantly contributeto increased EGP in diabetes. Fructose-1,6-bisphosphatase (FBPase)is a regulated enzyme in gluconeogenesis that is increased inanimal models of obesity and insulin resistance. However, whethera specific increase in liver FBPase can result in increasedEGP has not been shown. The objective of this study was to determinethe role of upregulated liver FBPase in glucose homeostasis.To achieve this goal, we generated human liver FBPase transgenicmice under the control of the transthyretin promoter, usinginsulator sequences to flank the transgene and protect it fromsite-of-integration effects. This resulted in a liver-specificmodel, as transgene expression was not detected in other tissues.Mice were studied under the following conditions: 1) at twoages (24 wk and 1 yr old), 2) after a 60% high-fat diet, and3) when bred to homozygosity. Hemizygous transgenic mice hadan approximately threefold increase in total liver FBPase mRNAwith concomitant increases in FBPase protein and enzyme activitylevels. After high-fat feeding, hemizygous transgenics wereglucose intolerant compared with negative littermates (P <0.02). Furthermore, when bred to homozygosity, chow-fed transgenicmice showed a 5.5-fold increase in liver FBPase levels and wereglucose intolerant compared with negative littermates, witha significantly higher rate of EGP (P < 0.006). This is thefirst study to show that FBPase regulates EGP and whole bodyglucose homeostasis in a liver-specific transgenic model. Ourhomozygous transgenic model may be useful for testing humanFBPase inhibitor compounds with the potential to treat patientswith type 2 diabetes.

endogenous glucose production; glucose intolerance

Address for reprint requests and other correspondence: S. Andrikopoulos, Univ. of Melbourne, Dept. of Medicine (AH/NH), Heidelberg Repatriation Hospital, 300 Waterdale Road, Heidelberg Heights, Victoria 3081, Australia (e-mail: sof{at}unimelb.edu.au)