Treatment with a β-2-adrenoceptor agonist stimulates glucose uptake in skeletal muscle and improves glucose homeostasis, insulin resistance and hepatic steatosis in mice with diet-induced obesity

Kalinovich, Anastasia V.; Dehvari, Nodi; Åslund, Alice; Beek, Sten van; Halleskog, Carina; Olsen, Jessica M.; Forsberg, Elisabete; Zacharewicz, Evelyn; Schaart, Gert; Rinde, Mia; Sandström, Anna L.; Berlin, Roger G.; Östenson, Claes‐Göran; Hoeks, Joris; Bengtsson, Tore

doi:10.1007/s00125-020-05171-y

Cited by 36 publications

(41 citation statements)

References 53 publications

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“…1, D-F). This is supported by a previous report studying glucose uptake in muscle cells in response to adrenergic stimulation (27,28). Furthermore, we observed, in response to increased cAMP levels, a degradation of TXNIP and the activation of GLUT1, but not GLUT4-mediated glucose uptake.…”

Section: Discussionsupporting

confidence: 92%

ATGL activity regulates GLUT1-mediated glucose uptake and lactate production via TXNIP stability in adipocytes

Beg

Zhang

McCourt

et al. 2021

Journal of Biological Chemistry

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Traditionally, lipolysis has been regarded as an enzymatic activity that liberates fatty acids as metabolic fuel. However, recent work has shown that novel substrates, including a variety of lipid compounds such as fatty acids and their derivatives, release lipolysis products that act as signaling molecules and transcriptional modulators. While these studies have expanded the role of lipolysis, the mechanisms underpinning lipolysis signaling are not fully defined. Here, we uncover a new mechanism regulating glucose uptake, whereby activation of lipolysis, in response to elevated cAMP, leads to the stimulation of thioredoxin-interacting protein (TXNIP) degradation. This, in turn, selectively induces glucose transporter 1 surface localization and glucose uptake in 3T3-L1 adipocytes and increases lactate production. Interestingly, cAMP-induced glucose uptake via degradation of TXNIP is largely dependent upon adipose triglyceride lipase (ATGL) and not hormone-sensitive lipase or monoacylglycerol lipase. Pharmacological inhibition or knockdown of ATGL alone prevents cAMP-dependent TXNIP degradation and thus significantly decreases glucose uptake and lactate secretion. Conversely, overexpression of ATGL amplifies the cAMP response, yielding increased glucose uptake and lactate production. Similarly, knockdown of TXNIP elicits enhanced basal glucose uptake and lactate secretion, and increased cAMP further amplifies this phenotype. Overexpression of TXNIP reduces basal and cAMP-stimulated glucose uptake and lactate secretion. As a proof of concept, we replicated these findings in human primary adipocytes and observed TXNIP degradation and increased glucose uptake and lactate secretion upon elevated cAMP signaling. Taken together, our results suggest a crosstalk between ATGL-mediated lipolysis and glucose uptake.

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Section: Discussionsupporting

confidence: 92%

ATGL activity regulates GLUT1-mediated glucose uptake and lactate production via TXNIP stability in adipocytes

Beg

Zhang

McCourt

et al. 2021

Journal of Biological Chemistry

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“…While our data show that endogenous macrophage B2AR signaling does not regulate local or systemic inflammation in lean and obese states, it might still be stimulated pharmacologically above its physiological threshold level to reduce inflammation and alleviate the severity of metabolic disease. Given that B2AR agonists have also been shown to improve systemic insulin sensitivity in obese animals through their action on skeletal muscle cells [ 58 ], in future it would be of interest to compare the efficacy of B2AR agonists in Adrb2 ΔLyz2 and control mice, in order to see what beneficial anti-inflammatory effects can be attributed to B2AR signaling specifically in macrophages, as compared to other cell types expressing B2ARs.…”

Section: Discussionmentioning

confidence: 99%

Macrophage beta2-adrenergic receptor is dispensable for the adipose tissue inflammation and function

Petkevicius

Bidault

Virtue

et al. 2021

Molecular Metabolism

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Objective Neuroimmune interactions between the sympathetic nervous system (SNS) and macrophages are required for the homeostasis of multiple tissues, including the adipose tissue. It has been proposed that the SNS maintains adipose tissue macrophages (ATMs) in an anti-inflammatory state via direct norepinephrine (NE) signaling to macrophages. This study aimed to investigate the physiological importance of this paradigm by utilizing a mouse model in which the adrenergic signaling from the SNS to macrophages, but not to other adipose tissue cells, was disrupted. Methods We generated a macrophage-specific B2AR knockout mouse ( Adrb2 ΔLyz2 ) by crossing Adrb2 fl/fl and Lyz2 Cre/+ mice. We have previously shown that macrophages isolated from Adrb2 ΔLyz2 animals do not respond to NE stimulation in vitro . Herein we performed a metabolic phenotyping of Adrb2 ΔLyz2 mice on either chow or high-fat diet (HFD). We also assessed the adipose tissue function of Adrb2 ΔLyz2 animals during fasting and cold exposure. Finally, we transplanted Adrb2 ΔLyz2 bone marrow to low-density lipoprotein receptor (LDLR) knockout mice and investigated the development of atherosclerosis during Western diet feeding. Results We demonstrated that SNS-associated ATMs have a transcriptional profile indicative of activated beta-2 adrenergic receptor (B2AR), the main adrenergic receptor isoform in myeloid cells. However, Adrb2 ΔLyz2 mice have unaltered energy balance on a chow or HFD. Furthermore, Adrb2 ΔLyz2 mice show similar levels of adipose tissue inflammation and function during feeding, fasting, or cold exposure, and develop insulin resistance during HFD at the same rate as controls. Finally, macrophage-specific B2AR deletion does not affect the development of atherosclerosis on an LDL receptor-null genetic background. Conclusions Overall, our data suggest that the SNS does not directly modulate the phenotype of adipose tissue macrophages in either lean mice or mouse models of cardiometabolic disease. Instead, sympathetic nerve activity exerts an indirect effect on adipose tissue macrophages through the modulation of adipocyte function.

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“…Glucose uptake, measured as DOG uptake, was increased both after acute and chronic treatment with terbutaline. This has previously been well-studied in vivo , but in vitro studies have mainly been limited to mouse ( Ito et al., 2019 ) and rat ( Kalinovich et al., 2020 ; Koziczak-Holbro et al., 2019 ; Nevzorova et al., 2006 ; Sato et al., 2014 ) skeletal muscle cells with only few reports from human myotubes ( Koziczak-Holbro et al., 2019 ; Sato et al., 2014 ). It is important to note that there are issues of translation between studies performed in rodent cells and human cells due to rodents having a higher energy expenditure and metabolic flux than human cells ( Wang et al., 2012 ).…”

Section: Discussionmentioning

confidence: 99%

Chronic treatment with terbutaline increases glucose and oleic acid oxidation and protein synthesis in cultured human myotubes

Skagen

Nyman

Peng

et al. 2021

Current Research in Pharmacology and Drug Discovery

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Objective In vivo studies have reported several beneficial metabolic effects of β-adrenergic receptor agonist administration in skeletal muscle, including increased glucose uptake, fatty acid metabolism, lipolysis and mitochondrial biogenesis. Although these effects have been widely studied in vivo , the in vitro data are limited to mouse and rat cell lines. Therefore, we sought to discover the effects of the β 2 -adrenergic receptor agonist terbutaline on metabolism and protein synthesis in human primary skeletal muscle cells. Methods Human cultured myotubes were exposed to terbutaline in various concentrations (0.01–30 μM) for 4 or 96 h. Thereafter uptake of [ 14 C]deoxy-D-glucose, oxydation of [ 14 C]glucose and [ 14 C]oleic acid were measured. Incorporation of [ 14 C]leucine, gene expression by qPCR and proteomics analyses by mass spectrometry by the STAGE-TIP method were performed after 96 h exposure to 1 and 10 μM of terbutaline. Results The results showed that 4 h treatment with terbutaline in concentrations up to 1 μM increased glucose uptake in human myotubes, but also decreased both glucose and oleic acid oxidation along with oleic acid uptake in concentrations of 10–30 μM. Moreover, administration of terbutaline for 96 h increased glucose uptake (in terbutaline concentrations up to 1 μM) and oxidation (1 μM), as well as oleic acid oxidation (0.1–30 μM), leucine incorporation into cellular protein (1–10 μM) and upregulated several pathways related to mitochondrial metabolism (1 μM). Data are available via ProteomeXchange with identifier PXD024063. Conclusion These results suggest that β 2 -adrenergic receptor have direct effects in human skeletal muscle affecting fuel metabolism and net protein synthesis, effects that might be favourable for both type 2 diabetes and muscle wasting disorders.

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Treatment with a β-2-adrenoceptor agonist stimulates glucose uptake in skeletal muscle and improves glucose homeostasis, insulin resistance and hepatic steatosis in mice with diet-induced obesity

Cited by 36 publications

References 53 publications

ATGL activity regulates GLUT1-mediated glucose uptake and lactate production via TXNIP stability in adipocytes

ATGL activity regulates GLUT1-mediated glucose uptake and lactate production via TXNIP stability in adipocytes

Macrophage beta2-adrenergic receptor is dispensable for the adipose tissue inflammation and function

Chronic treatment with terbutaline increases glucose and oleic acid oxidation and protein synthesis in cultured human myotubes

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