Subscribe to RSS
Download PDF
DOI: 10.1055/s-2002-33256
Up-Regulation of Liver Glucose-6-Phosphatase in X-Linked Hypophosphatemic Mice
Publication History
Received 18 September 2001
Accepted after Revision 6 March 2002
Publication Date:
12 August 2002 (online)
Abstract
We previously showed that a phosphate-deficient diet resulting in hypophosphatemia upregulated the catalytic subunit p36 of rat liver glucose-6-phosphatase, which is responsible for hepatic glucose production. A possible association between phosphate and glucose homeostasis was now further evaluated in the Hyp mouse, a murine homologue of human X-linked hypophosphatemia. We found that in the Hyp mouse as in the dietary Pi deficiency model, serum insulin was reduced while glycemia was increased, and that liver glucose-6-phosphatase activity was enhanced as a consequence of increased mRNA and protein levels of p36. In contrast, the Hyp model had decreased mRNA and protein levels of the putative glucose-6-phosphate translocase p46 and liver cyclic AMP was not increased as in the phosphate-deficient diet rats. It is concluded that in genetic as in dietary hypophosphatemia, elevated glucose-6-phosphatase activity could be partially responsible for the impaired glucose metabolism albeit through distinct mechanisms.
Key words
Glucose Intolerance - Phosphate Homeostasis - Mouse Liver
References
- 1 Foster J DF, Pederson B A, Nordlie R C. Glucose-6-phosphatase structure, regulation, and function: an update. Proc Soc Exp Biol Med. 1997; 215 314-332
- 2 Lei K J, Shelly L L, Pan C J, Sidbury J B, Chou J Y. Mutations in the glucose-6-phosphatase gene that cause glycogen storage disease type 1a. Science. 1993; 262 580-583
- 3 Gerin I, Veiga-da-Cunha M, Achouri Y, Collet J F, van Schaftingen E. Sequence of a putative glucose-6-phosphate translocase, mutation in glycogen storage disease type Ib. FEBS Lett. 1997; 419 235-238
- 4 van de Werve G, Lange A, Newgard C, Méchin M C, Li Y, Berteloot A. New lessons in the regulation of glucose metabolism taught by the glucose 6-phosphatase system. Eur J Biochem. 2000; 267 1533-1549
- 5 Li Y, Méchin M C, van de Werve G. Diabetes affects similarly the catalytic subunit and putative glucose-6-phosphate translocase of glucose-6-phosphatase. J Biol Chem. 1999; 274 33 866-33 868
- 6 Li Y, van de Werve G. Distinct hormone stimulation and counteraction by insulin of the expression of the two components of glucose 6-phosphatase in HepG2 cells. Biochem Biophys Res Commun. 2000; 272 41-44
- 7 Trinh K Y, O’Doherty R M, Anderson P, Lange A J, Newgard C B. Perturbation of fuel homeostasis caused by over-expression of the glucose-6-phosphatase catalytic subunit in liver of normal rats. J Biol Chem. 1998; 273 31 615-31 620
- 8 Econs M J. New insights into the pathogenesis of inherited phosphate wasting disorders. Bone. 1999; 25 131-135
- 9 Lajeunesse D, Meyer Jr. R A, Hamel L. Direct demonstration of a humorally-mediated inhibition of renal phosphate transport in the Hyp mouse. Kidney Int. 1996; 50 1531-1538
- 10 The HYP Consortium . A gene (PEX) with homologies to endopeptidases is mutated in patients with X-linked hypophosphatemic rickets. Nature Genet. 1995; 11 130-136
- 11 Du L, Desbarats M, Viel J, Glorieux F H, Cawthorn C, Ecarot B. cDNA cloning of the murine Pex gene implicated in X-linked hypophosphatemia and evidence for expression in bone. Genomics. 1996; 36 22-28
- 12 Guo R, Quarles L D. Cloning and sequencing of human PEX from a bone cDNA library: evidence for its developmental stage-specific regulation in osteoblasts. J Bone Miner Res. 1997; 12 1009-1017
- 13 DeFronzo R A, Lang R. Hypophosphatemia and glucose intolerance: evidence for tissue insensitivity to insulin. N Engl J Med. 1980; 303 1259-1263
- 14 Paula F J, Plens A E, Foss M C. Effects of hypophosphatemia on glucose tolerance and insulin secretion. Horm Metab Res. 1998; 30 281-284
- 15 Xie W S, Li Y, Méchin M C, van de Werve G. Upregulation of liver glucose-6-phosphatase in rats fed with a Pi-deficient diet. Biochem J. 1999; 343 393-396
- 16 Xie W S, Tran T L, Finegood D T, van de Werve G. Dietary phosphate deprivation in rats affects liver cyclic AMP, glycogen, key steps of gluconeogenesis and glucose production. Biochem J. 2000; 352 227-232
- 17 Méchin M C, Annabi B, Pegorier J P, van de Werve G. Ontogeny of the catalytic subunit and putative glucose-6-phosphate transporter proteins of the rat microsomal liver glucose-6-phosphatase system. Metabolism. 2000; 49 1200-1203
- 18 Tenenhouse H S. X-linked hypophosphatemia: a homologous disorder in humans and mice. Nephrol Dial Transplant. 1999; 14 333-341
- 19 Kido S, Miyamoto K, Mizobuchi H, Taketani Y, Ohkido I, Ogawa N, Kaneko Y, Harashima S, Takeda E. Identification of regulatory sequences and binding proteins in the type II sodium/phosphate cotransporter NPT2 gene responsive to dietary phosphate. J Biol Chem. 1999; 274 28 256-28 263
- 20 Cowgill L D, Goldfarb S, Lau K, Slatopolsky E. Evidence for an intrinsic renal tubular defect in mice with genetic hypophosphatemic rickets. J Clin Invest. 1979; 63 1203-1210
- 21 Kiebzak G M, Roos B A, Meyer Jr. R A. Secondary hyperparathyroidism in X-linked hypophosphatemic mice. Endocrinol. 1982; 111 650-652
- 22 Zhou X J, Fadda G Z, Perna A F, Massry S G. Phosphate depletion impairs insulin secretion by pancreatic islets. Kidney Int. 1991; 39 120-128
- 23 Moore E E, Kuestner R E, Conklin D C, Whitmore T E, Downey W, Buddle M M, Adams R L, Bell L A, Thompson D L, Wolf A, Chen L, Stamm M R, Grant F J, Lok S, Ren H, de Jongh K S. Stanniocalcin 2: characterization of the protein and its localization to human pancreatic alpha cells. Horm Metab Res. 1999; 31 406-414
- 24 Drezner M K. PHEX gene and hypophosphatemia. Kidney Int. 2000; 57 9-18
- 25 Shimada T, Mizutani S, Muto T, Vonega T, Hino R, Takeda S, Takeuchi Y, Fujita T, Fukumoto S, Yamashita T. Cloning and characterization of FGF-23 as a causative factor of tumor-induced osteomalacia. Proc Natl Acad Sci. 2001; 98 6500-6505
- 26 Bowe A E, Finnegan R, Jan de Beur S M, Cho J, Levine M A, Kumar R, Schiavi S C. FGF-23 inhibits renal tubular phosphate transport and is a PHEX substrate. Biochem Biophysical Res Comm. 2001; 284 977-981
- 27 Rowe P S, de Zoysa P A, Dong R, Wang H R, White K E, Econs M J, Oudet C L. MEPE, a new gene expressed in bone marrow and tumors causing osteomalacia. Genomics. 2000; 67 54-68
- 28 Argiro L, Desbarats M, Glorieux F H, Ecarot B. MEPE, the gene encoding a tumor-secreted protein in oncogenic hypophosphatemic osteomalacia, is expressed in bone. Genomics. 2001; 74 342-351
G. van de Werve, Ph.D.
Département de Nutrition · Centre de Recherche du CHUM · Hôpital Notre-Dame ·
8ième Pavillon Malloux · 1560 rue Sherbrooke Est · Montréal · Québec H2L 4M1 · Canada
·
Fax: + 1 (514) 412 76 03
Email: gerald_van_de_werve@hotmail.com