Acute regulation of glucose transport in a monocyte–macrophage cell line: Glut-3 affinity for glucose is enhanced during the respiratory burst

Ahmed, Nuzhat; Kansara, Maya; Berridge, Michael V.

doi:10.1042/bj3270369

Cited by 74 publications

(61 citation statements)

References 46 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…The consumption of glucose by inflammatory macrophages is mediated by glucose surface receptors and has been well characterized in numerous studies. 25,26 Those studies have shown that cellular glucose uptake agrees well with the MichaelisMenten formalism for enzymatic activity. As a result, consumption can be modeled using Michaelis-Menten kinetics with values specific to glucose uptake by macrophages.…”

Section: Modeling Early Stage Sensor Responsementioning

confidence: 76%

Modeling the Physiological Factors Affecting Glucose Sensor Function in Vivo

Novak

Reichert

2015

J Diabetes Sci Technol

View full text Add to dashboard Cite

For implantable sensors to become a more viable option for continuous glucose monitoring strategies, they must be able to persist in vivo for periods longer than the 3-to 7-day window that is the current industry standard. Recent studies have attributed such limited performance to tissue reactions resulting from implantation. While in vivo biocompatibility studies have provided much in the way of understanding histology surrounding an implanted sensor, little is known about how each constituent of the foreign body response affects sensor function. Due to the ordered composition and geometry of implantassociated tissue reactions, their effects on sensor function may be computationally modeled and analyzed in a way that would be prohibitive using in vivo studies. This review both explains how physiologically accurate computational models of implant-associated tissue reaction can be designed and shows how they have been utilized thus far. Going forward, these in silico models of implanted sensor behavior may soon complement in vivo studies to provide valuable information for improved sensor designs.

show abstract

Section: Modeling Early Stage Sensor Responsementioning

confidence: 76%

Modeling the Physiological Factors Affecting Glucose Sensor Function in Vivo

Novak

Reichert

2015

J Diabetes Sci Technol

View full text Add to dashboard Cite

show abstract

“…We found that GLUT-1 and GLUT-3, which are major isoforms of a glucose transporter in macrophages (12,13), were significantly upregulated in M1 macrophages, compared with M2 macrophages (Fig. 3) (P , 0.01 and , 0.01, respectively).…”

Section: Expression Of Glucose Metabolism-related Genes In Macrophagesmentioning

confidence: 81%

Comparison of Contrast Agents for Atherosclerosis Imaging Using Cultured Macrophages: FDG Versus Ultrasmall Superparamagnetic Iron Oxide

et al. 2013

View full text Add to dashboard Cite

Various noninvasive imaging methods have been developed to evaluate atherosclerotic plaques. Among them, 18 F-FDG PET and MR imaging with ultrasmall superparamagnetic iron oxide particles (USPIO) have been used to quantify plaque inflammation. Both methods are based on the efficient uptake of FDG and USPIO by macrophages in atherosclerotic lesions. Differently polarized macrophages have been reported to have different characteristics that are involved in the pathologic development of atherosclerosis. M1 polarized macrophages are considered the more proatherogenic phenotype than M2 polarized macrophages. However, little is known regarding the association between macrophage polarization and FDG or USPIO accumulation. In this study, we investigated intracellular FDG and USPIO accumulation in M1 and M2 polarized macrophages. Methods: THP-1 macrophages were differentiated into M1 and M2 polarized macrophages. Under optimal glucose conditions, we investigated the 3 H-labeled FDG uptake in M1 and M2 polarized macrophages. We then investigated intracellular USPIO uptake by M1 and M2 macrophages. Results: We found that M1 polarization, compared with M2 polarization, results in increased intracellular accumulation of FDG. To elucidate the mechanism by which FDG was preferentially accumulated in M1 macrophages, we examined messenger RNA expressions of glucose transporters (GLUTs) and hexokinases, which have pivotal roles in glucose uptake, and glucose-6-phosphatase (G6Pase), which catalyzes the reverse reaction of hexokinase. In M1 macrophages, GLUT-1, GLUT-3, hexokinase 1, and hexokinase 2 were upregulated and G6Pase was downregulated. In contrast to FDG, M1 polarization resulted in decreased intracellular accumulation of USPIO. We found that scavenger receptor A and CD11b, which are involved in USPIO binding and uptake, were significantly downregulated by M1 polarization. Conclusion: Compared with M2, proatherogenic M1 macrophages preferentially accumulated FDG but not USPIO, suggesting that FDG PET is a useful method for the detection of proinflammatory M1 macrophages.

show abstract

“…GLUT-1 is the major isoform found in most cells, whereas GLUT-3 leads to a substantial increase in energy needs associated with cell activation by its high affinity for glucose 30 and is a major GLUT subtype for macrophages. [31][32][33] Both GLUT-1 and GLUT-3 immunoreactivity were shown to be distributed in macrophages of the aneurysmal wall, indicating that glycolysis is the preferred energy production of these cells than the other cell types constituted of aorta. Importantly, the magnitude of GLUT-3 expression was associated with MMP-9 activity, mainly produced from macrophages in aneurysmal tissues, 34 and this was comparable in a monocytic cell line, showing the substantial increase in syntheses in GLUT-3 and MMP-9 upon the differentiation to macrophages.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of Development of Abdominal Aortic Aneurysm by Glycolysis Restriction

Tsuruda

Hatakeyama

Nagamachi

et al. 2012

ATVB

View full text Add to dashboard Cite

Objective-The mechanisms underlying abdominal aortic aneurysm development remain unknown. We hypothesized that acceleration of glucose metabolism with the upregulation of glucose transporters is associated with abdominal aortic aneurysm development. Methods and Results-Enhanced accumulation of the modified glucose analogue 18 fluoro-deoxyglucose by positron emission tomography imaging in the human abdominal aortic aneurysm was associated with protein expressions of glucose transporters-1 and -3, assessed by Western blot. The magnitude of glucose transporter-3 expression was correlated with zymographic matrix metalloproteinase-9 activity. Intraperitoneal administration of glycolysis inhibitor with 2-deoxyglucose significantly attenuated the dilatation of abdominal aorta induced by periaortic application of CaCl 2 in C57BL/6J male mice or reduced the aneurysmal formation in angiotensin II-infused apolipoprotein E knockout male mice. In monocytic cell line induced by phorbol 12-myristate 13-acetate or ex vivo culture obtained from human aneurysmal tissues, 2-deoxyglucose abrogated the matrix metalloproteinase-9 activity and interleukin-6 expression in these cells/tissues. Moreover, 2-deoxyglucose attenuated the survival/proliferation of monocytes and the adherence of them to vascular endothelial cells. Conclusion-This study suggests that the enhanced glycolytic activity in aortic wall contributes to the pathogenesis of aneurysm development. In addition, pharmacological intervention in glycolytic activity might be a potential therapeutic target for the disorder.

show abstract

Acute regulation of glucose transport in a monocyte–macrophage cell line: Glut-3 affinity for glucose is enhanced during the respiratory burst

Cited by 74 publications

References 46 publications

Modeling the Physiological Factors Affecting Glucose Sensor Function in Vivo

Modeling the Physiological Factors Affecting Glucose Sensor Function in Vivo

Comparison of Contrast Agents for Atherosclerosis Imaging Using Cultured Macrophages: FDG Versus Ultrasmall Superparamagnetic Iron Oxide

Inhibition of Development of Abdominal Aortic Aneurysm by Glycolysis Restriction

Contact Info

Product

Resources

About