The glucose-6-phosphatase system

Schaftingen, Emile Van; Gerin, Isabelle

doi:10.1042/bj3620513

Cited by 317 publications

(225 citation statements)

References 217 publications

Supporting

Mentioning

205

Contrasting

Unclassified

Order By: Relevance

“…SLC37A1 belongs to the small human sugar-phosphate/ phosphate transporter family, an almost unexplored group of transmembrane sugar-phosphate/phosphate transporters consisting of four members. To date, only one of these four genes/proteins has been well-characterized: SLC37A4 protein also recognized as the glucose-6-phosphate transporter [26,27]. While data regarding SLC37A2 are available for mice [28], for SLC37A3 only a putative gene/protein has been identified by in silico analysis [29].…”

Section: Discussionmentioning

confidence: 99%

SLC37A1 Gene expression is up-regulated by epidermal growth factor in breast cancer cells

Iacopetta

Lappano

Cappello

et al. 2009

Breast Cancer Res Treat

View full text Add to dashboard Cite

Phospholipid biosynthesis exerts an important role in the proliferation of tumor cells; however, the regulation of the proteins involved in this context still remains to be fully evaluated. SLC37A1 protein belongs to a small family of sugar-phosphate/phosphate exchangers. The sequence homology with the bacterial glycerol-3-phosphate transporter (30%) suggests that SLC37A1 might be able to catalyze an exchange of glycerol-3-phosphate against phosphate. Glycerol-3-phosphate, found in different cellular compartments, is a fundamental substrate in phospholipid biosynthesis. In the present study, we demonstrate for the first time that epidermal growth factor (EGF) transactivates SLC37A1 promoter sequence and induces SLC37A1 mRNA, and protein expression through the EGFR/MAPK/ Fos transduction pathway in ER-negative SkBr3 breast cancer cells. These findings were corroborated by comparable results obtained in ER-positive endometrial Ishikawa tumor cells. Interestingly, we also show that SLC37A1 protein localizes in the endoplasmic reticulum, hence supporting its possible involvement in phospholipid biosynthesis. On the basis of our data, the up-regulation of SLC37A1 gene expression should be included among the well-known stimulatory action exerted by EGF in breast cancer cells. In addition, further studies are required to provide evidence concerning the potential role of EGFmediated SLC37A1 induction in breast tumor cells.

show abstract

Section: Discussionmentioning

confidence: 99%

SLC37A1 Gene expression is up-regulated by epidermal growth factor in breast cancer cells

Iacopetta

Lappano

Cappello

et al. 2009

Breast Cancer Res Treat

View full text Add to dashboard Cite

show abstract

“…However, PF-4708671 failed to significantly reduce PEPCK or G6Pase protein expression despite lower mRNA expression of these enzymes. It is possible that G6Pase and PEPCK proteins are only reduced in specific cellular compartments [38][39][40]. Indeed, we have used a PEPCK1-specific antibody that recognises the cytosolic isoform, whereas PEPCK2 is predominantly a mitochondrial form.…”

Section: Discussionmentioning

confidence: 99%

Pharmacological inhibition of S6K1 increases glucose metabolism and Akt signalling in vitro and in diet-induced obese mice

et al. 2016

View full text Add to dashboard Cite

Aims/hypothesis The mammalian target of rapamycin complex 1 (mTORC1)/p70 ribosomal S6 kinase (S6K)1 pathway is overactivated in obesity, leading to inhibition of phosphoinositide 3-kinase (PI3K)/Akt signalling and insulin resistance. However, chronic mTORC1 inhibition by rapamycin impairs glucose homeostasis because of robust induction of liver gluconeogenesis. Here, we compared the effect of rapamycin with that of the selective S6K1 inhibitor, PF-4708671, on glucose metabolism in vitro and in vivo. Methods We used L6 myocytes and FAO hepatocytes to explore the effect of PF-4708671 on the regulation of glucose uptake, glucose production and insulin signalling. We also treated high-fat (HF)-fed obese mice for 7 days with PF-4708671 in comparison with rapamycin to assess glucose tolerance, insulin resistance and insulin signalling in vivo. Results Chronic rapamycin treatment induced insulin resistance and impaired glucose metabolism in hepatic and muscle cells. Conversely, chronic S6K1 inhibition with PF-4708671 reduced glucose production in hepatocytes and enhanced glucose uptake in myocytes. Whereas rapamycin treatment inhibited Akt phosphorylation, PF-4708671 increased Akt phosphorylation in both cell lines. These opposite effects of the mTORC1 and S6K1 inhibitors were also observed in vivo. Indeed, while rapamycin treatment induced glucose intolerance and failed to improve Akt phosphorylation in liver and muscle of HF-fed mice, PF-4708671 treatment improved glucose tolerance and increased Akt phosphorylation in metabolic tissues of these obese mice. Conclusions/interpretation Chronic S6K1 inhibition by PF-4708671 improves glucose homeostasis in obese mice through enhanced Akt activation in liver and muscle. Our results suggest that specific S6K1 blockade is a valid pharmacological approach to improve glucose disposal in obese diabetic individuals.

show abstract

“…In the final steps of 78 these pathways the glucose 6-phosphate transporter (G6PT) translocates G6P into the lumen 79 of the endoplasmic reticulum (ER) where it is hydrolysed by glucose 6-phosphatase (G6Pase) 80 to glucose and inorganic phosphate (1). 81…”

Section: Introduction 73mentioning

confidence: 99%

Partial correction of neutrophil dysfunction by oral galactose therapy in glycogen storage disease type Ib

Letkemann

Wittkowski

Antonopoulos

et al. 2017

International Immunopharmacology

View full text Add to dashboard Cite

The glucose-6-phosphatase system

Cited by 317 publications

References 217 publications

SLC37A1 Gene expression is up-regulated by epidermal growth factor in breast cancer cells

SLC37A1 Gene expression is up-regulated by epidermal growth factor in breast cancer cells

Pharmacological inhibition of S6K1 increases glucose metabolism and Akt signalling in vitro and in diet-induced obese mice

Partial correction of neutrophil dysfunction by oral galactose therapy in glycogen storage disease type Ib

Contact Info

Product

Resources

About